Survey
* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project
Download VOLUME 149 - No. 3 - JUNE 2014 OFFICIAL
Document related concepts
Transcript
BY U S EX E D IC ) I N D EX E D E D M I N N I) I N EX DL IO ( I S D E TAT D I N ( M C I DE E N C A N XP E SC IE OFFICIAL JOURNAL OF THE SOCIETÀ ITALIANA DI DERMATOLOGIA MEDICA, CHIRURGICA, ESTETICA E DELLE MALATTIE SESSUALMENTE TRASMESSE (SIDeMaST) VOLUME 149 - No. 3 - JUNE 2014 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA Official Journal of the “Società Italiana di Dermatologia Medica, Chirurgica, Estetica e delle Malattie Sessualmente Trasmesse (SIDeMaST)” Honorary Editor Mario PIPPIONE Editor in Chief Andrea PESERICO Assistant Editors Nicola PIMPINELLI - Pietro Quaglino Honorary Members and Editorial Committee M. Bagot (Paris, France) - L. Borradori (Bern, Switzerland) - R. Cerio (London, UK) - K. D. Cooper (Cleveland, USA) P. M. Elias (San Francisco, USA) - J. Hercogova (Prague, Czech Republic) - F. Kerdel (Miami, USA) - C. Paul (Tolouse, France) M. R. Pittelkow (Rochester, USA) - R. Schwartz (Newark; USA) - W. Sterry (Berlin, Germany) - E. Tschachler (Vienna, Austria) Editorial Board P. Amerio (Chieti) - G. Argenziano (Reggio Emilia) - A. Belloni Fortina (Padova) - N. Cassano (Bari) - A. Costanzo (Roma) E. Cozzani (Genova) - M. C. Fargnoli (L’Aquila) - F. Lacarrubba (Catania), D. Linder (Padova) - I. Neri (Bologna) F. Rongioletti (Genova) - F. Sampogna (Roma) - C. Tomasini (Torino) - M. Venturini (Brescia) - G. Zambruno (Roma) Società Italiana di Dermatologia Medica, Chirurgica, Estetica e delle Malattie Sessualmente Trasmesse (SIDeMaST) Board of Directors Andrea Peserico (President) - Gianfranco Altomare - Emilio Berti - Sergio Chimenti - Clara De Simone Alberico Motolese - Aurora Parodi - Giovanni Pellacani Nicola Pimpinelli - Carlo Pincelli - Anna Virgili Managing Editor Alberto OLIARO This journal is peer reviewed and is indexed by: Embase, PubMed/MEDLINE, Science Citation Index Expanded (SciSearch), Scopus The “Giornale Italiano di Dermatologia e Venereologia”, Bi-monthly Journal of Dermatology and Venereology, was founded in 1866 by G.B. Soresina, formerly “Giornale di Dermatologia e Sifilologia”, “Minerva Dermatologica”, “Giornale Italiano di Dermatologia”, “Il Dermosifilografo”, “Dermatologia”, “Cosmetologia”. Editorial, business, graphic and advertising address - Edizioni Minerva Medica - Corso Bramante 83-85 - I-10126 Torino (Italy) - Tel. +39 011 678282 - Fax +39 011 674502 E-mail: [email protected] - Web Site: www.minervamedica.it Typesetting and printed - Edizioni Minerva Medica - Tipografia di Saluzzo - Corso IV Novembre 29-31 - I-12037 Saluzzo (Italy) - Tel. +39 0175 249405 - Fax +39 0175 249407 Annual subscription: Italy: Individual: Online € 105.00, Print € 110.00, Print+Online € 115.00; Institutional: Print € 145.00, Online (Small € 272.00, Medium € 310.00, Large € 356.00, Extra-Large € 372.00), Print+Online (Small € 280.00, Medium € 325.00, Large € 370.00, Extra-Large € 385.00). European Union: Individual: Online € 180.00, Print € 185.00, Print+Online € 195.00; Institutional: Print € 255.00, Online (Small € 272.00, Medium € 310.00, Large € 356.00, ExtraLarge € 372.00), Print+Online (Small € 290.00, Medium € 335.00, Large € 380.00, Extra-Large € 395.00). Outside the European Union: Individual: Online € 200.00, Print € 210.00, Print+Online € 220.00; Institutional: Print € 280.00, Online (Small € 290.00, Medium € 325.00, Large € 375.00, Extra-Large € 390.00), Print+Online (Small € 305.00, Medium € 345.00, Large € 395.00, Extra-Large € 410.00). Subscribers: Payment to be made in Italy: a) by check; b) by bank transfer to: Edizioni Minerva Medica, INTESA SANPAOLO Branch no. 18 Torino. IBAN: IT45 K030 6909 2191 0000 0002 917 c) through postal account no. 00279109 in the name of Edizioni Minerva Medica, Corso Bramante 83-85, 10126 Torino; d) by credit card Diners Club International, Master Card, VISA, American Express. Foreign countries: a) by check; b) by bank transfer to: Edizioni Minerva Medica, INTESA SANPAOLO Branch no. 18 Torino. IBAN: IT45 K030 6909 2191 0000 0002 917; BIC: BCITITMM c) by credit card Diners Club International, Master Card, VISA, American Express. Notification of changes to mailing addresses, e-mail addresses or any other subscription information must be received in good time. Notification can be made by sending the new and old information by mail, fax or e-mail or directly through the website www.minervamedica.it at the section “Your subscriptions - Contact subscriptions department”. Complaints regarding missing issues must be made within six months of the issue’s publication date. Prices for back issues and years are available upon request. © Edizioni Minerva Medica - Torino 2014 All rights reserved. No part of this publication may be reproduced, stored or transmitted in any form or by any means, without the prior permission of the copyright owner Bi-monthly publication. Authorized by Turin Court no. 277 of July 2, 1948. Registered in the national press register as per law no. 416 art. 11 dated 5-8-1981 with number 00 148 vol. 2 sheet 377 dated 18-8-1982. Bi-monthly publication - Poste Italiane S.p.A. - Shipped on a subscription basis - Decree Law 353/2003 (converted in Law 27/02/2004 n° 46) art. 1, para 1, DCB/CN. Pubblicazione associata a La Rivista aderisce al Codice di Autodisciplina degli Editori Medico Sportivi associati a FARMAMEDIA e può essere oggetto di pianificazione pubblicitaria INSTRUCTIONS TO AUTHORS The journal Giornale Italiano di Dermatologia e Venereologia publishes scientific papers on dermatology and sexually transmitted diseases. Manuscripts may be submitted in the form of editorials, original articles, review articles, case reports, therapeutical notes, special articles and letters to the Editor. Manuscripts are expected to comply with the instructions to authors which conform to the Uniform Requirements for Manuscripts Submitted to Biomedical Editors by the International Committee of Medical Journal Editors (www.icmje.org). Articles not conforming to international standards will not be considered for acceptance. Papers should be submitted directly to the online Editorial Office at the Edizioni Minerva Medica website: www.minervamedica.it Submission of the manuscript means that the paper is original and has not yet been totally or partially published and, if accepted, will not be published elsewhere either wholly or in part. All illustrations should be original. Illustrations taken from other publications must be accompanied by the publisher’s permission. The Authors agree to transfer the ownership of copyright to Giornale Italiano di Dermatologia e Venereologia in the event the manuscript is published. The journal adheres to the principles set forth in the Helsinki Declaration and states that all reported research concerning human beings should be conducted in accordance with such principles. The journal also adheres to the International Guiding Principles for Biomedical Research Involving Animals recommended by the WHO and requires that all research on animals be conducted in accordance with these principles. The Authors, if necessary, must indicate that the study has been approved by the ethics committee and that patients have given their informed consent. Authors must also indicate whether they have any financial agreement with any organization that were involved in the research by filling the relevant form. Papers must be accompanied by the following authors’ statement relative to copyright, ethics and conflicts of interest, signed by all authors: “The undersigned authors transfer the ownership of copyright to Giornale Italiano di Dermatologia e Venereologia should their work be published in this journal. They state that the article is original, has not been submitted for publication in other journals and has not yet been published either wholly or in part. They state that they are responsible for the research that they have designed and carried out; that they have participated in drafting and revising the manuscript submitted, whose contents they approve. In the case of studies carried out on human beings, the authors confirm that the study was approved by the ethics committee and that the patients gave their informed consent. They also state that the research reported in the paper was undertaken in compliance with the Helsinki Declaration and the International Principles governing research on animals. They agree to inform Edizioni Minerva Medica of any conflict of interest that might arise, particularly any financial agreements they may have with pharmaceutical or biomedical firms whose products are pertinent to the subject matter dealt with in the manuscript”. The authors implicitly agree to their paper being peer-reviewed. All manuscripts will be reviewed by Editorial Board members who reserve the right to reject the manuscript without entering the review process in the case that the topic, the format or ethical aspects are inappropriate. Once accepted, all manuscripts are subjected to copy editing. If modifications to the manuscript are requested, the corrected version should be sent to the online Editorial Office with the modified parts underlined and highlighted. The revised version should be accompanied by a letter with point-by-point responses to the reviewers’ comments. Correction of proofs should be limited to typographical errors. Substantial changes in content (changes of title and authorship, new results and corrected values, changes in figures and tables) are subject to editorial review. Changes that do not conform to the journal’s style are not accepted. Corrected proofs must be sent back within 3 working days to the online Editorial Office of Giornale Italiano di Dermatologia e Venereologia. In case of delay, the editorial staff of the journal may correct the proofs on the basis of the original manuscript. Publication of manuscripts is free of charge. Colour figures, linguistic revision, and excessive alterations to proofs will be charged to the authors. If one of the authors is a SIDEMAST member, colour figures will be published free of charge. Authors will receive instructions on how to order reprints and a copy of the manuscript in PDF For further information about publication terms please contact the Editorial Office of Giornale Italiano di Dermatologia e Venereologia, Edizioni Minerva Medica, Corso Bramante 83-85, 10126 Torino, Italy – Phone +39-011-678282 – Fax +39-011-674502 – E-mail: [email protected]. ARTICLE TYPES Instructions for the most frequent types of articles submitted to the journal. Editorials. Commissioned by the Editor in Chief or the Managing Editor, editorials deal with a subject of topical interest about which the author expresses his/her personal opinion. No more than 1000 words (3 typed, double-spaced pages) and up to 15 references will be accepted. Original articles. These should be original contributions to the subject. The text should be 3000-5500 words (8 to 16 typed, double-spaced pages) not including references, tables, figures. No more than 50 references will be accepted. The article must be subdivided into the following sections: introduction, materials and methods, results, discussion, conclusions. In the introduction the aim of the study should be clearly summed up. The materials and methods section should describe in a logical sequence how the study was designed and carried out, how the data were analyzed (what hypothesis was tested, what type of study was carried out, how randomization was done, how the subjects were recruited and chosen, provide accurate details of the main features of treatment, of the materials used, of drug dosages, of unusual equipments, of the statistical method ...). In the results section the answers to the questions posed in the introduction should be given. The results should be reported fully, clearly and concisely supported, if necessary, by figures, graphs and tables. The discussion section should sum up the main results, critically analyze the methods used, compare the results obtained with other published data and discuss the implications of the results. The conclusions should briefly sum up the significance of the study and its future implications. Review articles. Generally commissioned by the Editor in Chief or the Managing Editor, review articles should discuss a topic of current interest, outline current knowledge of the subject, analyze different opinions regarding the problem discussed, be up-to-date on the latest data in the literature. The text should be 6000-12000 words (17 to 34 typed, doublespaced pages) not including references, tables, figures. No more than 100 references will be accepted. Case reports. These give a description of particularly interesting cases. The text should be 2000-3000 words (6 to 8 typed, double-spaced pages) not including references, tables, figures. No more than 30 references will be accepted. The article must be subdivided into the following sections: introduction, case report or clinical series, discussion, conclusions. Therapeutical notes. These are intended for the presentation and assessment of new medical and surgical treatments. The text should be 3000-5500 words (8 to 16 typed, double-spaced pages) not including references, tables, figures. No more than 30 references will be accepted. The article must be subdivided into the following sections: introduction, materials and methods, results, discussion, conclusions. Special articles. These are articles on the history of medicine, health care delivery, ethics, economic policy and law concerning dermatology. The text should be 3000-7000 words (8 to 20 typed, double-spaced pages) not including references, tables, figures. No more than 50 references will be accepted. Letters to the Editor. These may refer to articles already published in the journal or to a subject of topical interest that the authors wish to present to readers in a concise form. The text should be 500-1000 words (1 to 3 typed, double-spaced pages) not including references, tables, figures. No more than 5 references will be accepted. Guidelines. These are documents drawn up by special committees or authoritative sources. The number of figures and tables should be appropriate for the type and length of the paper. PREPARATION OF MANUSCRIPTS Text file Manuscripts must be drafted according to the template for each type of paper (editorial, original article, review, case report, therapeutical note, special article, letter to the Editor). The formats accepted are Word and RFT. The text file must contain title, authors’ details, notes, abstract, key words, text, references and titles of tables and figures. Tables and figures should be submitted as separate files. Title and authors’ details •Short title, with no abbreviations. •First name and surname of the authors. •Affiliation (section, department and institution) of each author. Notes •Dates of any congress where the paper has already been presented. •Mention of any funding or research contracts or conflict of interest. •Acknowledgements. •Name, address, e-mail of the corresponding author. Abstract and key words Articles should include an abstract of between 200 and 250 words. For original articles and therapeutical notes, the abstract should be structured as follows: aim (aim of the study), methods (experimental design, patients and interventions), results (what was found), conclusion (meaning of the study). Key words should refer to the terms from Medical Subject Headings (MeSH) of MEDLINE/PubMed. No abstracts are required for editorials or letters to the Editor. Text Identify methodologies, equipment (give name and address of manufacturer in brackets) and procedures in sufficient detail to allow other researchers to reproduce results. Specify well-known methods including statistical procedures; mention and provide a brief description of published methods which are not yet well known; describe new or modified methods at length; justify their use and evaluate their limits. For each drug generic name, dosage and administration routes should be given. Brand names for drugs should be given in brackets. Units of measurement, symbols and abbreviations must conform to international standards. Measurements of length, height, weight and volume should be given in metric units (meter, kilogram, liter) or their decimal multiples. Temperatures must be expressed in degrees Celsius. Blood pressure must be expressed in millimeters of mercury. All clinical chemistry measurements should be expressed in metric units using the International System of Units (SI). The use of unusual symbols or abbreviations is strongly discouraged. The first time an abbreviation appears in the text, it should be preceded by the words for which it stands. References It is expected that all cited references will have been read by the authors. The references must contain only the authors cited in the text, be numbered in Arabic numerals and consecutively as they are cited. Bibliographical entries in the text should be quoted using superscripted Arabic numerals. References must be set out in the standard format approved by the International Committee of Medical Journal Editors (www.icmje.org). Journals Each entry must specify the author’s surname and initials (list all authors when there are six or fewer; when there are seven or more, list only the first six and then “et al.”), the article’s original title, the name of the Journal (according to the abbreviations used by MEDLINE/PubMed), the year of publication, the volume number and the number of the first and last pages. When citing references, please follow the rules for international standard punctuation carefully. Examples: – Standard article. Sutherland DE, Simmons RL, Howard RJ. Intracapsular technique of transplant nephrectomy. Surg Gynecol Obstet 1978;146:951-2. – Organization as author International Committee of Medical Journal Editors. Uniform requirements for manuscripts submitted to biomedical journals. Ann Int Med 1988;108:258-65. – Issue with supplement Payne DK, Sullivan MD, Massie MJ. Women’s psychological reactions to breast cancer. Semin Oncol 1996;23(1 Suppl 2):89-97. Books and monographs For occasional publications, the names of authors, title, edition, place, publisher and year of publication must be given. Examples: – Books by one or more authors Rossi G. Manual of Otorhinolaryngology. Turin: Edizioni Minerva Medica; 1987. – Chapter from book De Meester TR. Gastroesophageal reflux disease. In: Moody FG, Carey LC, Scott Jones R, Ketly KA, Nahrwold DL, Skinner DB, editors. Surgical treatment of digestive diseases. Chicago: Year Book Medical Publishers; 1986. p. 132-58. – Congress proceedings Kimura J, Shibasaki H, editors. Recent advances in clinical neurophysiology. Proceedings of the 10th International Congress of EMG and Clinical Neurophysiology; 1995 Oct 15-19; Kyoto, Japan. Amsterdam: Elsevier; 1996. Electronic material – Standard journal article on the Internet Kaul S, Diamond GA. Good enough: a primer on the analysis and interpretation of noninferiority trials. Ann Intern Med [Internet]. 2006 Jul 4 [cited 2007 Jan 4];145(1):62-9. Available from: http://www.annals.org/cgi/reprint/145/1/62.pdf – Standard citation to a book on CD-ROM or DVD Kacmarek RM. Advanced respiratory care [CD-ROM]. Version 3.0. Philadelphia: Lippincott Williams & Wilkins; ©2000. 1 CD-ROM: sound, color, 4 3/4 in. – Standard citation to a homepage AMA: helping doctors help patients [Internet]. Chicago: American Medical Association; ©1995-2007 [cited 2007 Feb 22]. Available from: http://www.ama-assn.org/. Footnotes and endnotes of Word must not be used in the preparation of references. References first cited in a table or figure legend should be numbered so that they will be in sequence with references cited in the text taking into consideration the point where the table or figure is first mentioned. Therefore, those references should not be listed at the end of the reference section but consecutively as they are cited. Titles of tables and figures Titles of tables and figures should be included both in the text file and in the file of tables and figures. File of tables Each table should be submitted as a separate file. Formats accepted are Word and RTF. Each table must be typed correctly and prepared graphically in keeping with the page layout of the journal, numbered in Roman numerals and accompanied by the relevant title. Notes should be inserted at the foot of the table and not in the title. Tables should be referenced in the text sequentially. File of figures Each figure should be submitted as a separate file. Formats accepted: JPEG set at 300 dpi resolution preferred; other formats accepted are TIFF and PDF (high quality). Figures should be numbered in Arabic numerals and accompanied by the relevant title. Figures should be referenced in the text sequentially. Reproductions should be limited to the part that is essential to the paper. Histological photographs should always be accompanied by the magnification ratio and the staining method. If figures are in color, it should always be specified whether color or black and white reproduction is required. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA Vol. 149 June 2014 No. 3 CONTENTS DRUG ERUPTIONS - Part II 317 281 Grasso V., Vassallo C., Croci G., Brazzelli V. Guest Editors: G. BORRONI, C. TOMASINI Acute generalized exanthematous pustulosis: report of five cases and systematic review of clinical and histopathological findings Vassallo C., Derlino F., Brazzelli V., D’Ospina R. M., Borroni G. Tyrosine kinase inhibitors: muco-cutaneous side effects at the microscope 329 Thalidomide-induced granuloma annulare Ferreli C., Atzori L., Manunza F., Pau M., Caddori A. 335 291 Histopathologic spectrum of Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS): a diagnosis that needs clinico-pathological correlation Borroni G., Torti S., Pezzini C., Vassallo C., Rosso R., D’Ospina R. M., Tomasini C., Brazzelli V. ORIGINAL ARTICLES Topical lactoferrin can improve stable psoriatic plaque Saraceno R., Gramiccia T., Chimenti S., Valenti P., Pietropaoli M., Bianchi L. 341 301 Drug-induced lupus erythematosus Clinically and/or histologically pigmented poromas in Caucasian patients Marzano A. V., Tavecchio S., Menicanti C., Crosti C. Betti R., Bombonato C., Cerri A., Moneghini L., Abramo P., Menni S. 311 347 Inflammatory/infectious cutaneous side effects of biological drugs in patients with psoriasis: a general review with personal data Rongioletti F., Burlando M., Parodi A. Vol. 149 - No. 3 In vivo and in vitro evaluation of topical formulations containing physiological lipid mixture for replacement of skin barrier function Barba C., Parra J. L., Coderch L., Semenzato A. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA XV CONTENTS 355 372 Crosta M. L., Caldarola G., Fraietta S., Craba A., Benedetti C., Coco V., Janiri L., Rinaldi L., De Simone C. Lo Schiavo A., Brancaccio G., Romano F., Caccavale S. Psychopathology and eating disorders in patients with psoriasis Lymphangiomas arising on lymphedema: first step of malignant development 374 A rare association between neurofibromatosis type 1 and vulvar sarcoma 363 CASE REPORTS Periungual pyogenic granulomas due to topical tazarotene for nail psoriasis Piraccini B. M., Venturi M., Patrizi A. Miraglia E., Pecorella I., Persechino F., Visconti B., Calvieri S., Giustini S. 376 A clinical case of cutaneous silica granuloma 367 Onesti M. G., Fino P., Amorosi V., Piro F., Pedace D., Carella S., Latini C. Carlesimo M., Pennica A., Muscianese M., Bottoni U., Abruzzese C., Giubettini M., Pranteda G., Pranteda G. 378 Multiple skin ulcers due to Serratia marcescens in a immunocompetent patient Merkel cell carcinoma of the lower limb De Paola M., Poggiali S., Miracco C., Pisani C., Batsikosta A., Bilenchi R. 371 CORRESPONDENCE A case of superimposed segmental giant melanocytic nevus Piccolo V., Russo T., Picciocchi R., Ametrano O., Moscarella E. XVI 381 Yellow urticaria in a patient with hepatic cirrhosis Chiba T., Hayashi F., Shinmura M., Kiyomatsu M., Tatematsu S., Nakao M., Furue M. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 DRUG ERUPTIONS - Part II Guest Editors: G. Borroni, C. Tomasini G ITAL DERMATOL VENEREOL 2014;149:281-90 Acute generalized exanthematous pustulosis: report of five cases and systematic review of clinical and histopathological findings C. VASSALLO, F. DERLINO, V. BRAZZELLI, R. M. D’OSPINA, G. BORRONI Acute generalized exanthematous pustulosis (AGEP) is a rare, drug-related pustular eruption usually starting from folds with edema and erythema and with subsequent spreading. Clinically AGEP is characterized by the sudden appearance of dozen of sterile, non follicular, small pustules on erythematous and edematous skin. Mild non erosive mucosal involvement, mostly oral, may sometimes occur. Fever, neutrophilia and peripheral blood eosinophilia (in a third of patients) are present. Other skin signs such as facial edema, purpura, target-like lesions and blisters have been described but are not typical for AGEP. Diagnostic criteria for AGEP were established by an international committee of experts, the European Study of Severe Cutaneous Adverse Reactions (EuroSCAR). The most relevant histopathological feature is represented by the detection of non-follicular subcorneal and/or intracorneal spongiform pustules that are usually large, contiguous and tend to coalesce. After elimination of the causative drug, pustules usually spontaneously disappear in a few days with desquamation and the reaction fully resolves within 15 days. Internal organs are not usually involved and no systemic treatment is required. Withdrawal of the culprit drug is mandatory. Although AGEP is a self-limiting disease with a favourable prognosis, secondary infections are a not infrequent complication in patients in poor general medical conditions. The reported mortality is about 5%. The most severe cases are associated with drug rechallenge. Key words: Acute generalized exanthematous pustulosis - Pathology - Diagnosis. A cute generalized exanthematous pustulosis (AGEP) is a rare, acute, febrile eruption, characterized by the occurrence of numerous small, nonfollicular, sterile pustules, arising within large areas Corrisponding author: C. Vassallo, MD, Department of Dermatology, University of Pavia, Policlinico San Matteo IRCCS Foundation, Viale C. Golgi 19, 27100 Pavia, Italy. E-mail [email protected] Vol. 149 - No. 3 Dermatology Unit, Department of Clinical‑Surgical Diagnostic and Pediatric Sciences, University of Pavia Policlinico San Matteo IRCCS Foundation, Pavia, Italy of oedematous erythema, associated with peripheral blood leukocytosis. In 1968 Baker and Ryan identified 5 patients with drug-related pustular eruptions with an acute course, who had no history of psoriasis. Over time, cases with similar clinical characteristics have been described using different names, such as “generalized toxic pustuloderma”, “blistering drug eruptions”, and “generalized pustular dermatosis”.1 The term acute generalized exanthematous pustulosis (AGEP) was first introduced by Beylot et al. in 1980.2, 3 AGEP was better defined later by Roujeau et al.4 and Chang et al.5 In most cases (more than 90%) it arises as an adverse drug reaction even if other rarer toxical and infectious causes have been reported (Table I). The incidence of AGEP is estimated at one to five cases per million people per year, even though this figure may be underestimated and misdiagnosed as pustular psoriasis.6, 7 Although AGEP is generally accepted as a distinct entity, clinical, etiologic and histopathologic features may hardly be distinguished from drug-induced psoriasis and, to a lesser extent, from other pustular widespread neutrophilic dermatosis. Materials and methods We conducted a retrospective study of all patients admitted to our department for AGEP between 2008 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 281 VASSALLO ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS Table I.—Some of the most frequently involved drugs causing AGEP. Group Specific Agent Antibiotics Amoxicillin (with or without clavulanic acid) propicillin, imipenem, cephalexin and cephradine, co-trimoxazole, doxycycline, chloramphenicol, ciprofloxacin, norfloxacin, ofloxacin, teicoplanin, streptomycin, isoniazid, metronidazole Terbinafine, fluconazole, itraconazole, nystatin Sertraline, chlorpromazine, nitrazepam Diltiazem, captopril, enalapril, furosemide, hydrochlorothiazide Hydroxychloroquine, pyrimethamine, salazopyrine, mesalazine, azathioprine, cytarabine, piperazine ethionamate, pseudoephedrine, allopurinol, dextropropoxyphene, icodextrin, mexiletine, morphine, acetylsalicylic acid, naproxen, deltaeparin, intravenous non-ionic contrast agents Antimycotics Anticonvulsant Antihypertensive Others and 2013 (6-year period): a series of seven patients has been considered. All the patients were rated with the EuroSCAR score and five out of seven were classified as affected by AGEP. Three male and two female patients are reported (mean age 66.6). All the patients had different comorbidities requiring a therapy with a specific drug that in each case was of recent introduction. In each case reported the patient presented a rather abrupt occurrence of erythematous patches quickly followed by the appearance of dozens of millimetric non follicular, monomorphous pustules, associated with a burning sensation and pruritus. In all cases lesions had focal distribution with a tendency to spread rapidly and to coalesce. In two patients, a palmar involvement was observed, while in one woman mucosal (oral) involvement was evident. Admission to our in-patient department was required in two cases. Patients were all investigated for laboratory findings, including full blood count, creatinine, transaminases, bilirubin, gammaglutamyl peptidase and inflammatory markers. In each case two punch biopsies were performed, respectively for histopathological examination and direct immunofluorescence; a pustular smear was made from a recent lesion in order to exclude an infectious etiology. In all cases the culprit drug was suspended and a systemic and/or topical corticosteroidal therapy was started. Resolution of cutaneous lesions with superficial desquamation was observed in all cases. Results Results are reported and summarized in Table II, where clinical features, causative drugs, histopathological and immunopathological findings are reported for each patient. Microbiological examinations from pustular smears always proved negative. In all cases direct immunofluorescence was negative and histopathological examination (Table III) was always consistent with a diagnosis of AGEP presenting with subcorneal and intracorneal pustules with only scant spongiosis and few necrotic keratinocytes. Rare eosinophils in superficial dermis were evident in three patients. Table II.—Main clinical features of five patients affected by AGEP. Patient gender age 1 (CR), F 70 yrs-o 2 (CG), M 76 yrs-o 3 (DL), M 60 yrs-o 4 (CG), F 68 yrs-o 5 (GF), M 59 yrs-o 282 Main comorbidities Causative drug Cutaneous involvement Rheumatoid arthritis Hydroxychloroquine Trunk, arms, legs, face Mucosal involvement Systemic involvement Lips Fever, 38 °C, leukocytosis with neutrophilia, elevation of inflammatory markers (hospitalized) Leukocytosis with neutrophilia, elevation of inflammatory markers Fever; rhabdomyolysis (hospitalized) Dermatomyositis Hydroxychloroquine Arms, legs, palms // Hairy cell leukaemia Pentostatin Neck, trunk, legs // Diabetes mellitus arthrosis Hypertension Naproxen sodium Trunk, palms // Amoxicillin + clavulanic acid Face, trunk (folds) // Leukocytosis with eosinophilia, slight elevation of inflammatory markers Slight elevation of inflammatory markers GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS VASSALLO Table III.—Histopathological findings in five patients affected by AGEP. Immunopathological features Histopathological features: epidermal changes Histopathological features: dermal changes 1 DIF negative 2 DIF negative Basket-wave corneum, scant sub/intraepidermal non spongiform pustules, spongiosis, neutrophilic exocytosis Subcorneal pustules, focal spongiosis, neutrophils at dermo-epidermal junction 3 DIF negative Parakeratosis, focal scale-crust, subcorneal pustules, spongiosis, rare single necrotic keratinocytes 4 DIF negative Subcorneal pustules, scant focal spongiosis, neutrophils exocytosis, rare single necrotic keratinocytes 5 DIF negative Confluent subcorneal pustules, slight spongiosis, neutrophils along the dermo-epidermal junction Slight edema of papillary dermis, scant interstitial inflammatory infiltrate composed of lymphocytes, neutrophils, and few eosinophils Edema of sub-papillary dermis, extravasation of erythrocytes, interstitial infiltrate of neutrophils and lymphocytes, no eosinophils Slight edema of papillary dermis, scant inflammatory infiltrate composed of lymphocytes, neutrophils and many eosinophils. Erythrocytes extravasation Edema of sub-papillary dermis, erythrocytes extravasation, interstitial infiltrate of neutrophils and lymphocytes, few eosinophils Scarce infiltrate of lymphocytes and neutrophils in an oedematous superficial dermis. No eosinophils Patient Clinicopathologic correlations in the five AGEP pa‑ tients considered Case 1 A 70-year-old woman, affected by rheumatoid arthritis developed erythematous and edematous patches, quickly covered by pustular lesions. She was in treatment with hydroxychloroquine for one month before cutaneous eruption. These manifestations began on the trunk and rapidly spread to legs, arms, face and oral mucous membranes (lips) (Figure 1). These widespread cutaneous lesions were associated with fever (38 °C), pruritus and burning sensation and altered blood clotting analysis. Hospitalization was necessary. Laboratory findings showed leucocytosis with neutrophilia and elevation of inflammatory markers. No other internal organ involvement was documented. A pustular smear from a new lesion was performed and allowed us to exclude an infectious cause of lesion. Two punch biopsies were performed, on for direct immunofluorescence (negative) and one for histopathologic examination, confirming the clinical diagnosis of AGEP. In particular basket-wave corneum, scant sub/intraepidermal non spongiform pustules, spongiosis, neutrophilic exocytosis were observed. The dermis was characterised by slight oedema of papillary dermis, scant interstitial superficial inflammatory infiltrate composed of lymphocytes, neutrophils, and few eosinophils. Case 2 Figure 1.—AGEP: mucous membrane involvement. Mucosal localization is reported in only one third of cases, being almost exclusively oral. Pustular lesions evolve into superficial erosions. Vol. 149 - No. 3 A 76-year-old man affected by dermatomyositis in therapy with systemic corticosteroids started also a therapy with hydroxychloroquine, developing within some days erythematous and edematous patches with small, monomorphous pustular lesions all over the body surface (Figure 2) with even a palmar involvement. No mucosal localization was present and good clinical general conditions were documented. Only leukocytosis with neutrophilia and slight elevation of inflammatory markers were detectable. A pustular smear was performed from a recent lesion and resulted negative for micro-organisms. Two punch biopsies were taken: the first one for DIF proved negative and the other one was consistent with a diagnosis of AGEP. The histopathologic GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 283 VASSALLO ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS Figure 3.—Subcorneal pustule filled by several neutrophils (hematoxylin-eosin). Figure 2.—AGEP: early stage. Presence of erythematous and oedematous patches on the neck and on the trunk. Lesions were associated with hitch. Within a few hours the occurrence of several, monomorphous, millimetric pustules could be documented. features presented with subcorneal pustules (Figure 3), focal spongiosis, neutrophils at dermo-epidermal junction (Figure 4), edema of sub-papillary dermis, extravasation of erythrocytes, interstitial infiltrate of neutrophils and lymphocytes, no eosinophils. Case 3 A 60-year-old man affected by hairy cell leukemia started chemotherapy with granulocyte colony stimulating factors (GCSF) and pentostatin. About 15 days later he developed erythematous patches covered by small, monomorphous pustules, localized 284 Figure 4.—Neutrophils along dermal-epidermal junction (hematoxylin-eosin). to trunk, neck and legs. Mucous membrane was not involved. A systemic involvement was documented by the presence of fever (>38 °C), elevation of inflammatory markers and rhabdomyolysis, that could be interpreted as due to chemotherapy. The patient was admitted to our in-patient department. Pustular smear was performed and resulted negative as well as direct immunofluorescence. Histopathology showed parakeratosis, focal crusty lesions, subcorneal pustules, spongiosis, rare single necrotic keratinocytes, slight oedema of papillary dermis, extravasation of erythrocytes scant inflammatory infiltrate composed of lymphocytes, neutrophils and many eosinophils. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS Case 4 A 68-year-old woman affected by diabetes mellitus and arthrosis took naproxen sodium because of joint pain and developed within some hours a diffuse burning and itchy sensation associated the following day to the occurrence of erythematous patches mainly localized on the trunk and on arms with also a palmar involvement, and covered by tiny confluent pustules. These pustular lesions were extremely fragile and were associated to a scaling evolution (Figure 5), particularly marked on palms. Neither mucosal nor systemic involvement was observed. VASSALLO Laboratory findings showed a slight elevation of inflammatory markers and moderate leukocytosis. A pustular smear from a new lesion was performed and allowed us to exclude an infectious cause of lesion. Two punch biopsies were performed for direct immunofluorescence, resulted negative, and histopathological examination. Histopathology revealed the presence of subcorneal pustules (Figure 6), scant focal spongiosis, neutrophils exocytosis, rare single necrotic keratinocytes, oedema of sub-papillary dermis, erythrocytes extravasation, interstitial infiltrate of neutrophils and lymphocytes, few eosinophils. Case 5 A 59-year-old patient affected by hypertension, after the intake of amoxicillin and clavulanic acid for a Figure 5.—AGEP: late stage. After the withdrawal of the culprit drug the disease usually resolves spontaneously with superficial desquamation within fifteen days. Here typical involvement of arm fold is reported. Vol. 149 - No. 3 Figure 6.—Patient 4: a small, subcorneal pustule associated with parakeratosis (hematoxylin-eosin). GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 285 VASSALLO ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS Figure 8.—Histopathological findings are characterized by confluent pustules and underlying psoriasiform epidermal hyperplasia (hematoxylin-eosin). Figure 7.—Patient affected by amoxicillin and clavulanic-induced AGEP with confluent pustules on his left thigh. dental abscess, within a few hours developed an erythematous papulo-pustular eruption on trunk, with a peculiar distribution on folds (Figure 7), quickly involving his face. The patient was apyretic and laboratory examinations did not reveal any significant alteration. Histopathological findings were characterized by confluent subcorneal pustules (Figure 8), slight spongiosis of epidermis, neutrophils along the dermo-epidermal junction, a scarce infiltrate of lymphocytes and neutrophils in an oedematous superficial dermis. No eosinophils were present. Discussion AGEP is a rare, acute, pustular, usually febrile eruption. The current estimated incidence rate of AGEP is one to five cases per million per year.6, 8 Previous studies have shown that AGEP can occur at any age, also in childhood, even if the mean age of occurrence has been assessed between the fourth and the fifth decade.8 AGEP affects men and women equally, even if a trend toward female predominance would be revealed by more recent studies,4, 5, 6, 9 being perfectly consistent with the recognized female predominance in drug eruption in general.8 These data are consistent with those observed in our study, even if in our series of cases patients were older than the mean age reported in literature. According to lit- 286 erature seasonality would play a role in AGEP occurrence since a clustering of cases in the summer has been reported in a series of cases from Israel, albeit further studies would be necessary to clarify this finding.9, 10 As far as we know from our observation seasonality does not play a relevant role since our patients developed AGEP in months different from summer, even showing a predilection for autumn and winter. Clinically, pustular manifestations usually occur rapidly: from hours (usually within 24 hours) to few days after drug intake. Lesions usually start on face on flexural areas and disseminate over few hours with development of systemic symptoms. The pustular eruption is represented by dozens to hundreds of small (pinhead sized, 5 mm) non follicular, sterile pustules, arising on an strongly erythematous and oedematous skin surface. Sometimes confluence of pustules and their evolution with desquamation may mimic a positive Nikolsky’s sign simulating, in severe cases, toxic epidermal necrolysis (TEN). The occurrence of lesions is usually associated to a burning sensation or to pruritus or both. Other skin signs like marked edema of the face, purpura lesions (especially on the legs), Stevens-Johnson-syndromelike “atypical targets”, blisters and vesicles have been observed in more than 50% of patients with AGEP, even if they are not typical for it. Mucous membrane involvement may occur in about 20% of the cases but usually is mild and remains limited to one location (mostly oral). Systemic symptoms are almost always presents and include: fever above 38 °C, lymphadenopathy and leukocytosis with blood neutrophil count above 7 X109/L. Hypocalcaemia can be detected and a mild to moderate eosinophilia GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS may be present in about one third of the patients.7 In about 30% of cases a slight reduction of the creatinine clearance, leading in some cases to a transient renal failure, may be detected. A mild elevation of aminotransferases may also be found.9 Cutaneous lesions last 1 to 2 weeks after the withdrawal of the involved drug and are followed by a desquamation.7 The course of the disease is usually favourable with a spontaneous regression of cutaneous and systemic symptoms (even if topical steroid and systemic antipyretics may help). In some rare cases a widespread TEN-like picture can develop with a more severe prognosis that can be worsened also by secondary infections. Rare fatalities are documented: reported mortality rate is about 5%.8 These clinical manifestations and this clinical behaviour are perfectly consistent with those observed in our case series, therefore their stereotypical features, associated to the acute and abrupt onset have to be recognised in order to immediately suspect a diagnosis of AGEP facing a pustular manifestation of sudden appearance. Histopathology of AGEP, despite its relative aspecificity, is a useful means of diagnostic integration with the history of patients and their clinical features. Biopsy specimen should be obtained from early pustular lesions. A relevant histopathological feature is the presence of non-follicular subcorneal and/or intracorneal spongiform pustules encompassing more than 15 keratinocytes. Pustules may coalesce. These pustular lesions are typically sterile and no bacterial, viral or fungal proliferation can be detected at haematoxylin-eosin staining or PAS stain. In a wide histopathological study performed in 2010 on 102 patients with a definite or probable diagnosis of AGEP (according to AGEP validation score), 23% of cases also presented with follicular pustules that are not typical of AGEP, although the diagnosis could not be excluded for this.8 We could not observe any follicular pustule in our cases. Other relevant epidermal features typically associated to pustular lesions in AGEP are the presence of necrotic keratinocytes and neutrophil exocytosis. In our series of patients, two had few, single necrotic keratinocytes and one neutrophilic exocytosis. In two cases presence of neutrophils along the dermo-epidermal junction was detectable. The main dermal features were papillary oedema and mixed superficial, interstitial, and mid/ deep-dermal infiltrates containing neutrophils and eosinophils. No sign of vasculitis is usually evident, even if in more than 50% of cases leukocytoclasia Vol. 149 - No. 3 VASSALLO and erythrocyte extravasation can be detected with their misinterpretation as vasculitis and with a consequent diagnostic confusion of AGEP with pustular vasculitis.8 In three out five of our patients it was possible to observe erythrocyte extravasation. Additional features that can be observed are: parakeratosis and rete-ridges elongation (mild to moderate);8 in our patient affected by hairy cell leukaemia, parakeratosis could be seen, but probably is to address to previous chemotherapy that he received. Despite the neutrophilic inflammation observed in AGEP is unusual in allergic drug reactions, many of the other mentioned aspects are typical of drug adverse reactions, such as the prominent presence of eosinophils in the skin of patients, both within the pustules and in the dermis, but also blood eosinophilia, observed in about a third of patients with AGEP, is a hallmark of many drug-induced allergic reactions, suggests that AGEP is a hypersensitivity reaction. Furthermore the mid/deep-dermal perivascular infiltrates and extravasation of erythrocytes, the absence of vasculitis and especially the presence of necrotic keratinocytes in AGEP has been reported also in other drug eruptions including exanthematic drug eruptions and drug eruptions characterized primarily by interface dermatitis such as lichenoid drug eruptions, such as Stevens-Johnson syndrome (SJS), TEN and fixed drug eruptions.8 In more than 90% of cases AGEP is caused by drug intake.7 The onset of AGEP is rapid, often occurring within 24 hours after drug intake. Recently, a large-scale multinational case-control study (the EuroSCAR study) pointed out that the latent period is different for each drug, being for instance, shorter (about 24 hours) for antibiotics and longer (even 11 days) for other drugs.9 Longer latent periods (1-3 months to 1 year), were reported in a few AGEP cases with an underlying malignancy, that conceivably would play a role in extending latent period.10, 11-13 Spontaneous resolution usually begins once the causative drug is no longer used, even if in exceptional cases a severe evolution in TEN-like picture has been reported.13 A prior sensitization (including a contact sensitization) to the inducing drug may explain the short interval between drug administration and the onset of the eruption; the short interval suggests an immunologic recall phenomenon in a patient with strong prior sensitization. According to this hypothesis, in many cases there may be a positive patch test reaction to the suspected drug. Other than this, a genetic predisposition has also GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 287 VASSALLO ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS been documented, since HLA-B5, -DR11 and -DQ3 have been found more frequently in patients with AGEP.7 Among drugs antibiotics are the most frequent causative agents, especially penicillins or macrolides (ampicillin/amoxicillin±clavulanic acid and pristinamycin), quinolones, anti-infective sulphonamides, terbinafine, and spiramycin±metronidazole, even if also other drugs such as (hydroxy)chloroquine, diltiazem, carbamazepine have been frequently mentioned as responsible agents. In the table 1 we list all the main drug that have been associated with AGEP during years. The absolutely relevant role of drugs in determining AGEP is underlined also by ours case series where eache patient had an history of recent drug intake. Besides drug intake which is the most frequent cause, AGEP can occur also after viral infections (e.g., enteroviruses parvovirus B19, cytomegalovirus and Coxsackie B4), UV radiation, heavy metal exposure (e.g., hypersensitivity to mercury) and spider bites.12, 13 Pathogenetic mechanisms are now quite known and have been mainly elucidated by patch and in vitro tests. The first step would be represented by activation, expansion and subsequent migration of drug specific CD4 and CD8 cells to the skin. Presentation of the drug bound to major histocompatibility complex (MHC) class I by keratinocytes to T CD 8 cells result in apoptosis of keratinocytes derived from the release of granzyme and perforin by TCD8 cells and in a subsequent formation of subcorneal vescicles. Infiltration of TCD4 cells would also contribute to this process, since the presentation of the drug bound to major histocompatibility complex (MHC), class II, by keratinocytes to drug-specific TCD4 cells determine the release of CXCL-8 and of granulocyte macrophage-colony stimulating factor (GM-CSF), respectively able to induce the recruitment of neutrophils and to prevent of neutrophils apoptosis. This result in the conversion of subcorneal vescicles into sterile pustules. CD4 cells also release interferon (IFN-γ), which stimulates keratinocytes to secrete CXCL-8 and interleukin-5, which contributes to the eosinophilia observed in some patients. Resident Langerhans cells may present drug antigens to CD4 cells and keratinocytes may act as antigen presenting cells to CD8 cells, increasing the neutrophil-mediated inflammatory response.14 AGEP diagnosis is based on clinical, histopathological and immunopathological features but also on personal history (e.g. history of psoriasis, history of recent drug intake). In a retrospective 288 analysis of 63 cases of AGEP, performed in 2001, suggested five criteria for AGEP recognition: 1) several dozens of small, mostly non follicular pustules arising on a widespread oedematous erythema; 2) typical histopathologic change; 3) fever (38 °C); 4) blood neutrophil count above 7 X 109/L and 5) acute evolution with spontaneous resolution of pustules in less than 15 days, elaborating then even a more sophisticated score system for AGEP diagnosis (AGEP validation score).15, 16 The AGEP validation score is a standardized scoring system composed of a set of data related to clinical features (morphology and clinical course) and histopathology. On the basis of this score is possible to categorize cases as no AGEP, possible AGEP, probable AGEP and definite AGEP.8-12 The AGEP validation score has been used to diagnose AGEP in many case reports and case series but in everyday clinical practice the five criteria first suggested can be often satisfactory in order to make a diagnosis. Once suspected AGEP, other more specific tests such as in vivo and in vitro tests can be performed for the identification of culprit drugs, always keeping in mind that they are consistent in some cases but not in others.17 In vivo tests consist on patch tests that are considered well-tolerated (although a generalized AGEPlike reaction has been reported) 12 and, over recent years, have been created for a wider and wider variety of medications and chemicals, proving strongly positive in more than 50% of AGEP cases. Concerning in vitro tests, drug specific CD4+ and CD8+ T cells can be isolated and cultured from patch test sites and blood from AGEP patients. A positive diagnostic sign was represented by the observation of the in vitro release of the Th1-type cytokine IFNγ, of the lymphokine macrophage migration inhibition factor and of the mast cell degranulation test. Differential diagnosis of AGEP includes a wide number of vescico-pustular dermatoses. The main differential diagnoses according to clinical and histopathological features are represented by: pustular psoriasis (von Zumbusch type), subcorneal pustular dermatosis (Sneddon-Wilkinson disease), pustular vasculitis, drug hypersensivity syndrome and toxic epidermal necrolysis. Distinction of AGEP from pustular psoriasis (von Zumbush type) is probably the hardest and still most debated differential diagnosis because of their clinical and histopathological similarity diseases so that GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS to be considered in some cases a same entity. In this case, the history of the patient proves fundamental. Usually in pustular psoriasis a positive history of pre-existent and even long-dating psoriasis is often present, while in AGEP is possible but not so frequent, a positive history for recent drug intake is uncommon and systemic symptoms and cutaneous manifestation are referred by the patient to have a longer duration. Moreover, from a clinical point of view in pustular psoriasis, pustules and erythema usually have a more generalized distribution and show a tendency to persist until a therapy is started. On the contrary, in AGEP, pustular lesions are mainly localized, with a particular predominance in the folds and have a more fading behaviour/course, since they often spontaneously resolve with drug withdrawal. Moreover, even though both AGEP and pustular psoriasis at histopathological examination show a spongiform subcorneal and/or intraepidermal sterile pustule, in pustular psoriasis more typical aspects, such as papillomatosis and regular acanthosis can be detected. Finally in AGEP the presence of an inflammatory infiltrate of both neutrophils and eosinophils on the one hand differentiate from psoriasis and on the other hand underline once again AGEP nature as drug-adverse reaction. Recent genetic studies on pustular psoriasis underline the presence of recessive mutations of IL36RN in generalized pustular psoriasis; the same defect was also find in some patients affected by AGEP, suggesting that the two condition might have in common at least one pathway.18 Sneddon-Wilkinson’s subcorneal pustular dermatosis may resemble AGEP, especially for its prevalent folds involvement. Despite that SneddonWilkinson’s disease have a less acute course and at histopathological examination pustular lesions, that are also wider than in AGEP, are not spongiform. Considering the spectrum of bullous diseases also pemphigus foliaceus/IgA pemphigus and toxic epidermal necrolysis have to be excluded. Usually pemphigus foliaceus and IgA pemphigus have a less acute course, more diffuse distribution, present with subcorneal bullous lesions with a scant neutrophilic infiltrate and have a positive direct immunofluorescence. On the other hand in some cases the presence of “atypical” target lesions and the confluence of pustules mimicking a positive Nikolsky-sign may suggest the diagnosis of TEN in severe cases of AGEP. In these cases a distinction can be made because usu- Vol. 149 - No. 3 VASSALLO ally AGEP presents a more superficial epidermal detachment and mucous membrane involvement is less pronounced. Whereas differentiation in some cases might be difficult on clinical grounds alone, histology is significantly different in TEN typically showing full thickness epidermal necrosis and only a very sparse inflammatory infiltrate. Yet, even some overlap cases might exist that fulfil the criteria for both diseases both clinically and histologically. Drug hypersensitivity syndrome, also referred to as DRESS (an acronym for drug rash with eosinophilia and systemic symptoms) may also show papulo-vesicles and/or papulo-pustules, the pustular component being usually less pronounced than in AGEP. In addition patients usually show show more severe systemic symptoms with: fever, lymphadenopathy, eosinophilia, and often severe visceral involvement like hepatitis, nephritis, pneumonitis, and/or myocarditis. Also pustular vasculitis should be excluded, since bullous and/or pustular lesions may arise in purpura lesions of leukocytoclastic vasculitis. In addition there seems to be a special variant of leukocytoclastic vasculitis which is characterized by the development of many small pustules which, as opposed to AGEP, are localized mainly on the dorsum of the hands and which might also be drug-induced. A marked leukocytoclastic vasculitis, not detectable in AGEP, can be observed in histology. The occurrence of systemic symptoms like fever, lymphoadenomegaly and blood leukocytosis with neutrophilia, associated with an elevated amount of neutrophils detectable at histopathology should lead also to rule out an infection (bacterial or fungal) presenting as primary or secondary on a preexistent dermatosis. Bacterial folliculitis, dermatophyte infections, pyoderma vegetans, Kaposi’s varicelliform eruption, impetigo, impetiginized eczema and staphylococcal scalded skin syndrome have to be excluded performing a pustular smear. Conclusions AGEP is a rare, acute, pustular, usually febrile eruption induced by drugs. All our patients with AGEP improved within a few days after drug withdrawal, symptom management and systemic/topical corticosteroids. None of our patients died, despite two required hospitalization for systemic involvement. All of them presented comorbidities, and three GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 289 VASSALLO ACUTE GENERALIZED EXANTHEMATOUS PUSTULOSIS autoimmune diseases. Hydroxychloroquine-induced AGEP was observed in two out of five patients. One patient presented pentostatin-induced AGEP, never described before. The histopathological findings were consistent with AGEP in all cases and in two of them a new histological feature could be described, namely the presence of neutrophils along the dermoepidermal junction. Clinicopathological correlation allows a specific diagnosis in most of cases, albeit the rapid evolution of pustules may sometimes infer in obtaining a representative biopsy of the process, making more difficult the diagnosis. References 1. Guevara-Gutierrez E, Uribe-Jimenez E, Diaz-Canchola M, Tlacuilo-Parra A. Acute generalized exanthematous pustulosis: report of 12 cases and literature review. Int J Dermatol 2 009;48:253-8. 2. Choi MJ, Kim HS, Park HJ, Park CJ, Lee JD, Lee JY et al. Clinicopathologic manifestations of 36 korean patients with acute generalized exanthematous pustulosis: a case series and review of the literature. Ann Dermatol 2010;22:163-9. 3. Beylot C, Bioulac P, Doutre MS. Acute generalized exanthematic pustuloses (four cases). Ann Dermatol Venereol 1980;107:37-48. 4. Roujeau JC, Bioulac-Sage P, Bourseau C, Guillaume JC, Bernard P, Lok C et al. Acute generalized exanthematous pustulosis. Analysis of 63 cases. Arch Dermatol 1991;127:1333-8. 5. Chang SL, Huang YH, Yang CH, Hu S, Hong HS. Clinical manifestations and characteristics of patients with acute generalized exanthematous pustulosis in Asia. Acta Derm Venereol 2008;88:363-5. 6. Bailey K, McKee D, Wismer J, Shear N. Acute generalized exanthematous pustulosis induced by hydroxychloroquine: first case report in Canada and review of the literature. J Cutan Med Surg 2013;17:414-8. 290 7. Revuz J, Valeyrie-Allanore L. Drug reactions. In: Bolognia JL, Jorizzo JL, Rapini RP, editors. Dermatology. 2nd edition. Vol 1. St Louis, MO: Mosby Elsevier; 2008. p. 301-20. 8. Hlevy S. Acute generalized exanthematous pustulosis. Curr Opin Allergy Clin Immunol 2009;9:322-8. 9. Sidoroff A, Dunant A, Viboud C, Halevy S, Bavinck JN, Naldi L et al. Risk factors for acute generalized exanthematous pustulosis (AGEP)-results of a multinational case-control study (EuroSCAR). Br J Dermatol 2007;157:989-96 10. Davidovici B, Dodiuk- Gad R, Rozenman D, Halevy S; Israeli RegiSCAR Network. Profile of acute generalized exanthematous pustulosis in Israel during 2002-2005: results of the RegiSCAR Study. Isr Med Assoc J 2008;10:410-2. 11. Tamir E, Wohl Y, Mashiah J, Brenner S. Acute generalized exanthematous pustulosis: a retrospective analysis showing a clear predilection for women. Skinmed 2006;5:186-8. 12. Halevy S, Kardaun SH, Davidovici B, Wechsler J; EuroSCAR and RegiSCAR study group. The spectrum of histopathological features in acute generalized exanthematous pustulosis: a study of 102 cases. Br J Dermatol 2010;163:1245-52. 13. Peermohamed S, Haber RM. Acute generalized exanthematous pustulosis simulating toxic epidermal necrolysis: a case report and review of the literature. Arch Dermatol 2011;147:697-701. 14. Fernando SL. Acute generalised exanthematous pustulosis. Australas J Dermatol 2012;53:87-92. 15. Roujeau JC, Bioulac-Sage P, Bourseau C, Guillaume JC, Bernard P, Lok C et al. Acute generalized exanthematous pustulosis. Analysis of 63 cases. Arch Dermatol 1991;127:1333-8. 16. Sidoroff A, Halevy S, Bavinck JN, Vaillant L, Roujeau JC. Acute generalized exanthematous pustulosis (AGEP) -a clinical reaction pattern. J Cutan Pathol 2001;28:113-9. 17. Mashiah J, Brenner S. A systemic reaction to patch testing for the evaluation of acute generalized exanthematous pustulosis. Arch Dermatol 2003;139:1181-3. 18. Sugiura K. The genetic background of generalized pustular psoriasis: IL36RN mutations and CARD14 gain-of-function variants. J Dermatol Sci 2014;14:S0923-1811 Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 G ITAL DERMATOL VENEREOL 2014;149:291-300 Histopathologic spectrum of Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS): a diagnosis that needs clinico-pathological correlation G. BORRONI 1, S. TORTI 1, C. PEZZINI 1, C. VASSALLO 1, R. ROSSO 2 R. M. D’OSPINA 1, C. TOMASINI 3, V. BRAZZELLI 1 Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS) is characterized by an heterogeneous group of severe dermatologic manifestations and systemic involvement, due to several groups of medicaments. A series of 9 consecutive cases, observed from 2008 to 2013 in the Department of Dermatology, University of Pavia, is reported, all satisfying the clinical, hematological and systemic diagnostic criteria of DRESS. Clinically, 4 out of 9 patients had an urticarial and papular eruption, 2 an erythema-multiforme-like (EMlike) pattern, 2 erythroderma and 1 had an erythematous and macular reaction. Aim of the study was to describe the histopathologic features of DRESS and to trace a possible correlation between the four clinical recognized types of the syndrome and the histopathological patterns. Predominantly, a superficial perivascular lymphocytic infiltrate, extravasation of erythrocytes, and focal interface changes characterized DRESS cases. Less frequently, histopathology revealed the presence of necrotic keratinocytes; surprisingly, only in 2 cases the presence of rare dermal eosinophils was detected, even if all the patients had significant peripheral eosinophilia. A histopathological diagnosis of DRESS seems per se, according to our data, not feasible, since the main histopathological changes (interface changes, superficial perivascular dermatitis, focal spongiosis, lichenoid infiltrate, rare presence of necrotic keratinocytes) can be interpreted generically as a drug induced dermatitis. The above mentioned histopathological changes, however, when associated with clinical information on cutaneous and systemic involvement of the patient, allow the pathologist or the dermatopathologist to make a diagnosis of DRESS with a reliable margin of certainty. Key words: Drug hypersensitivity syndrome - Diagnosis Drug-related side effects and adverse reactions. Corresponding author: G. Borroni, MD, Department of Dermatology, University of Pavia, Fondazione IRCCS Policlinico San Matteo, Viale C. Golgi 19, 27100 Pavia, Italy. E-mail: [email protected] Vol. 149 - No. 3 1Department of Clinical‑Surgical, Diagnostic and Pediatric Sciences Dermatology Section, University of Pavia Foundation IRCCS Policlinico San Matteo, Pavia, Italy 2Anatomic Pathology Foundation IRCCS Policlinico San Matteo University of Pavia, Italy 34th Section of Human Pathology Training‑Centre in Dermatopathology San Giovanni Battista University Hospital, Turin, Italy T he syndrome characterized by cutaneous Drug Reaction with Eosinophilia and Systemic Symptoms, defined by the acronym DRESS, has been firstly described by Bocquet et al. in 1996.1 The syndrome encompasses an heterogeneous group of severe and systemic reactions (liver, kidney, heart, lung, central nervous system, blood, lymph nodes), caused by different drugs, associated with fever and extensive skin manifestations. The genetic susceptibility factors of DRESS have not yet been fully identified. However, some HLA alleles have been correlated with DRESS in some ethnic groups, but not in others. In fact, in Japanese patients with carbamazepine induced DRESS a correlation with HLA-B*4801 have been demonstrated. An association between allopurinol and HLAB*5801 has not been found in Japanese patients with DRESS.2 On the contrary, some other alleles, such as HLA-A*31:01 showed a significant association with carbamazepine-induced DRESS both in European and Chinese population.3-7 The role of causal drugs 8 and susceptibility GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 291 BORRONI HISTOPATHOLOGIC SPECTRUM OF DRESS to viruses, such as HHV-7,9 Epstein-Barr Virus (EBV),10 cytomegalovirus (CMV),11 HHV-6 and Varicella-Zoster Virus (VZV),12 reactivated during the relatively long period of drug administration (from 3 weeks to 2 month), and T-cell response 13 are as many factors that play a crucial role in the complex pathogenesis of the syndrome. The severity of systemic signs and symptoms have, to some extent, put aside the dermatological features. Cutaneous eruption, however, is one of the main diagnostic criteria of DRESS. Despite its protean dermatological presentation, four main clinical patterns have been proposed:1, 14 I) urticarial and papular manifestation; II) erithemamultiforme-like reaction (EM-reaction); III) macular and erythematous features; and IV) erythrodermalike pattern. Histopathologic findings of DRESS have been referred as polymorphous, to the point of making a diagnosis of DRESS on the histopathologic grounds alone, virtually impossible to the pathologist. The EM-like reaction has been related to a poorer prognosis, with more severe hepatic involvement.14 ered in RegiSCAR grading system for DRESS,15 were used in our cases. Histopathology showed a wide spectrum of changes including 1) necrotic keratinocytes; 2) exocytosis of lymphocytes; 3) spongiosis/vesciculation; 4) focal interface changes with vacuolar alterations; 5) superficial perivascular lymphocytic infiltrate; 6) atypical lymphocytes; 7) eosinophils in the dermis; 8) lichenoid infiltrate; 9) dilated blood vessels; and 10) extravasation of erythrocytes. They have been graded according to their presence (%) and severity (scoring), with an evaluation of every change from 0 to 3. Low grade incidence of changes was defined by a total score <0.30; slight changes were defined by a scoring between 0.30 and 0.60; moderate changes between 0.60 and 0.90; high grade of changes >0.90. Aim of the study was to investigate the histopathological findings of DRESS, to describe the main characteristics, and to trace a correlation between the clinical presentation and histopathological pattern. Every patient was assessed by two dermatologists at least and by one pathologist for the above mentioned purposes, and assisted in the clinical course by several specialists of different medical disciplines. Material and methods Over a 6-year period (2008-2013) a series of nine consecutive cases of DRESS, all satisfying the clinical, haematological and systemic criteria of the Syndrome, have been considered. Six male and three female patients, all Caucasians, are reported (mean age: 59.5). Four cases had urticarial and papular manifestations, two had a diffuse EM-reaction, one had a macular and erythematous eruption and two had an erythroderma-like pattern. In every case medical history showed previous and recent exposure to drugs (from two weeks to two months), and a sequential series of worsening clinical findings in the development of the disease. Patients were all investigated for laboratory findings, including full blood count, creatinine, transaminases (AST, ALT) and gamma-glutamyl transpeptidase, bilirubin and virological analyses (HIV, hepatitis B and C, Epstein-Barr Virus, Human Herpes Virus 6 and 7, Cytomegalovirus), ECG and chest Rx. Biopsies were taken after patients consent and processed for routine histopathology. All the clinical and laboratory findings, consid- 292 Results Results are reported and summarized in Table I, were clinical features, causative drugs, systemic involvement and peripheral eosinophilia percentage have been reported for every patient. Clinicopathologic correlations in the nine DRESS patients considered Case 1 A 40-year-old man, presented with widespread, erythematous-papular confluent lesions, involving more than 50% of the body surface and affecting trunk and extremities (Figure 1A). He had been in treatment with allopurinol for 3 weeks, before cutaneous manifestation. Afterwards, he developed also hepatic and renal dysfunction, fever and diffuse lymphadenopathy and he was hospitalized. The peripheral eosinophilia was >20%. Histopathology revealed a superficial dense perivascular lymphocytic dermatitis, with several lymphocytes with hyperchromatic nuclei, focal interface changes, mild exocytosis and slight focal spongiosis. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 HISTOPATHOLOGIC SPECTRUM OF DRESS BORRONI Table I.—Clinical features, causative drug, systemic involvement in the 9 patients observed. Patient’s gender and age Type and % of cutaneous clinical involvement 1 M 40 y-o Diffuse macular and erythematous eruption >50% 2 M 58 y-o Diffuse urticarial persistent erythematous eruption >50% 3 F 35 y-o Implicated drug/drugs Systemic involvement Eosinophilia Allopurinol Hepatic dysfunction Renal dysfunction Lymphadenopathy Fever >20% Carbamazepine Hepatic dysfunction Acute pancreatitis Lymphadenopathy Fever >20% Erythroderma and confluent EM-like eruption >50% Diclofenac Hepatic dysfunction Lymphadenopathy 10-19% 4 M 65 y-o Diffuse erythematous erythroderma-like reaction Extent >50% Allopurinol Hepatic dysfunction Renal dysfunction Lung involvement Pericarditis Fever >20% 5 M 72 y-o Diffuse erythematous erythroderma-like reaction with facial HSV infection Extent >50% Carbamazepine Hepatic dysfunction Renal dysfunction Lymphadenopathy Fever >20% 6 M 67 y-o Severe and persistent urticarial reaction Extent >50% Valproic Acid Hepatic dysfunction Lymphadenopathy 10-19% 7 F 58 y-o Diffuse papular and erythematous eruption Extent >50% Amoxicylline + Clavulanic Acid Hepatic dysfunction Lymphadenopathy Fever 10-19% 8 F 76 y-o EM-like eruption Extent >50% Hydroxychloroquine Hepatic dysfunction Lymphadenopathy Fever >20% 9 M 65 y-o Diffuse papular and erythematous eruption Extent <50% Perindopril + Indapamide Hepatic dysfunction >20% A B Figure 1.—A) Diffuse erythematous and macular eruption, involving more than 50% of the body surface; B) dense superficial perivascular and interstitial lymphocytic infiltrate, with focal exocytosis and slight spongiosis. Erythrocyte extravasation in the upper part dermis, (H&E). Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 293 BORRONI HISTOPATHOLOGIC SPECTRUM OF DRESS Erythrocyte extravasation was seen in the upper dermis. No eosinophils were present in the inflammatory infiltrate (Figure 1B). Case 2 A 58-year-old male patient, with personal history of carbamazepine medication 4 weeks before, showed a diffuse urticarial erythematous eruption from the onset involving upper trunk, with later involvement to limbs and face, associated with intense pruritus, asthenia and fever (Figure 2A). During hospitalization, he developed hepatic dysfunction A and acute pancreatitis and we detected a peripheral eosinophilia >20%. A skin biopsy from the trunk was taken. Histopathology was characterized by a lichenoid lymphocytic infiltrate, involving focally dermo-epidermal junction and dermal interstitium. Furthermore, a dense perivascular lymphocytic infiltrate was seen around superficial blood vessels, with many hyperchromatic nuclei. Slight vasodilation with few extravasated erythrocytes, no eosinophils in the dermal infiltrate. Epidermal changes were characterized by incipient and frank focal spongiosis with exocytosis of lymphocytes, without necrotic keratinocytes (Figure 2B). B Figure 2.—A) Diffuse urticarial persistent erythematous eruption (>50%); B) relatively dense lichenoid lymphocytic infiltrate, and dense superficial perivascular lymphocytic infiltrate with many hyperchromatic nuclei. Focal epidermal spongiosis, (H&E). A B C Figure 3.—A) Erythroderma-like pattern of DRESS involving trunk and proximal arms; B) EM-like features of DRESS in the same patient on upper arms and lower legs (>50%); C) absence of necrotic keratinocytes, vacuolar changes at dermo-epidermal junction, with a hint of sub-epidermal vesiculation and a dense mid-dermal perivascular and interstitial lymphocytic infiltrate, without eosinophils (trunk), (H&E). 294 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 HISTOPATHOLOGIC SPECTRUM OF DRESS Case 3 A 35-year-old woman developed diffuse figurate targetoid, discrete and confluent erithema-multiforme-like lesions, with erythroderma-like reaction, involving neck, face, trunk and extremities (Figure 3A, B), about 3 weeks after diclofenac treatment. Moreover, she developed hepatic dysfunction and diffuse lymphadenopathy; peripheral eosinophilia was 16%. A biopsy was taken, and histopathology revealed absence of necrotic keratinocytes with a dense perivascular superficial lymphocytic infiltrate, and some atypical lymphocytes with hyperchromatic nuclei, focal interface vacuolar changes and a hint of sub-epidermal vesiculation. No eosinophils were detectable in the inflammatory infiltrate (Figure 3C). Case 4 A 65-year-old man showed a diffuse erythematous eruption with oedema and focal vesiculation, with later diffuse desquamation (Figure 4A, B). He was treated with allopurinol since one month for hyperuricemia. Few days after hospitalization, he developed a renal and hepatic dysfunction, with lung involvement and pericarditis. Peripheral eosinophilia was >20%. A skin biopsy was done from his left thigh. Histopathology was characterized by a true spongiotic dermatitis with intraepidermal vesiculation and focal and confluent necrotic keratinocytes, either immediately beneath the stratum corneum and within the spongiotic foci. Oedema of the sub-papillary dermis was prominent. In the dermis a mild perivascular A B BORRONI lymphocytic infiltrate with rare hyperchromatic nuclei, without eosinophils, was seen, associated with moderate erythrocyte extravasation (Figure 4C). Case 5 A 72-year-old-male patient was in treatment with carbamazepine for bipolar disorder. After 6 weeks of carbamazepine therapy, he developed a macular confluent and erythroderma-like reaction, involving more than 50% of the skin (Figure 5A, B). For the appearance of hepatic and renal dysfunction, the patient was hospitalized. His peripheral eosinophilia was >20%. A skin biopsy was taken and histopathology revealed epidermal atrophy with necrotic keratinocytes and interface changes, a lymphocytic superficial perivascular infiltrate with some hyperchromatic nuclei. The stratum corneum was characterized by hyperkeratosis with parakeratosis and scale crusts with neutrophils (Figure 5C). Case 6 A 67-year-old-man showed a severe erythematomacular and confluent urticarial reaction, involving more than 50% of cutaneous surface (Figure 6A, B). The drug involved was valproic acid, which the patient had been taking for 3 weeks. Moreover, he developed severe hepatic dysfunction and lymphadenopathy and he had peripheral eosinophilia 17%. A skin biopsy was taken from the trunk. Histopatholo- C Figure 4.—A, B) Diffuse erythroderma-like reaction (>50%); C) spongiotic dermatitis, with oedema of the papillary dermis and mild perivascular lymphocytic infiltrate with hyperchromatic nuclei, without eosinophils. Few extravasated erythrocytes, (H&E). Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 295 BORRONI HISTOPATHOLOGIC SPECTRUM OF DRESS A B C Figure 5.—A, B) Erythroderma-like diffuse reaction (>50%), with late stage HSV-infection on the face; C) Epidermal atrophy with few necrotic keratinocytes and focal interface changes. Lymphocytic superficial perivascular infiltrate with hyperchromatic nuclei (H&E). A B C Figure 6.—A, B) Severe and persistent urticarial-like reaction (>50%); C) dense and diffuse lymphocytic superficial perivascular infiltrate, with few necrotic keratinocytes, in touch with lymphocytes, (H&E). gy was characterized by a dense diffuse lymphocytic superficial perivascular dermatitis, incipient spongiosis with rare necrotic keratinocytes, surrounded by lymphocytes (Figure 6C). Case 7 A 58-year-old female patient developed erythematous confluent oedematous lesions, involving more than 50% of the body surface and confluent widespread papular eruption (Figure 7A, B). She had a personal history of amoxicylline + clavulanic acid treatment for a previous dental work about 20 days before. The patient was hospitalized for the development of hepatic dysfunction, fever and diffuse lymphadenopathy. She had a peripheral eosinophilia 13%. A skin biopsy was taken from her right leg. Histopathology was characterized by compact and 296 basket waved orthokeratosis and parakeratosis, slight atrophy of the epidermidis, focal interface changes without necrotic keratinocytes, lymphocytic exocytosis, oedema of the papillary dermis, and a perivascular superficial and mid-dermal lymphocytic infiltrate, with some interstitial changes, vasodilatation and erythrocytes extravasation. No eosinophils were detected (Figure 7C). Case 8 A 76-year-old woman showed an EM-like reaction, involving more than 50% of body surface about 6 weeks after starting therapy with hydroxychloroquine for dermatomyositis (Figure 8A). In few days, the patient developed hepatic dysfunction and fever, so she was hospitalized. Her peripheral eosinophilia was >20%. Histopathology (left forearm), revealed GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 HISTOPATHOLOGIC SPECTRUM OF DRESS A BORRONI B C Figure 7.—A, B) Diffuse papular and confluent erythematous and oedematous features (>50%); C) Focal interface changes, without necrotic keratinocytes, lymphocytic exocytosis, oedema of the papillary dermis, and superficial and mid-dermal lymphocytic infiltrate, with some eosinophils and extravasation of erythrocytes, (H&E). A B Figure 8.—A) Confluent EM-like lesions, involving more than 50% of the body surface; B) moderate atrophy of the epidermis, focal interface changes, no necrotic keratinocytes, mild perivascular lymphocytic infiltrate, with eosinophils and erythrocytes extravasation (left upper arm), (H&E). moderate atrophy of the epidermis, focal interface changes, without necrotic keratinocytes, superficial perivascular lymphocytic infiltrate, with eosinophils, vasodilatation and moderate erythrocytes extravasation (Figure 8B). dermis. No eosinophils were detected in the infiltrate (Figure 9B). Case 9 On the basis of the clinical classification of DRESS into four main patterns,1, 14 4 out of 9 patients had diffuse urticarial and papular eruption, 2 had erythroderma, 2 EM-like reaction and 1 erythematous and macular pattern. However, at least 6 of our patients had, to some extent, overlapping mixed features, and only 3 had either defined papular or urticarial diffuse lesions. Allopurinol (2 cases), carbamazepine (2 cases) and diclofenac, valproic acid, amoxicylline + clavulanic acid, hydroxychloroquine, perindopril + indapamide (1 case respectively) were the causative About a month after starting treatment with perindopril-indapamide, a 65-year-old man developed a diffuse urticarial and papular eruption and hepatic dysfunction (Figure 9A). He had peripheral eosinophilia >20%. A skin biopsy from the trunk was taken, and histopathology revealed slight atrophy of the epidermis, without necrotic keratinocytes, scant interface changes, moderately dense lichenoid lymphocytic infiltrate in the papillary and sub-papillary Vol. 149 - No. 3 Discussion GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 297 BORRONI HISTOPATHOLOGIC SPECTRUM OF DRESS A B Figure 9.—A) Diffuse urticarial and papular eruption (<50%); B) Irregular acanthosis, no necrotic keratinocytes, focal interface changes and moderately dense lichenoid lymphocytic infiltrate in the papillary and sub-papillary dermis, (H&E). drugs of DRESS in our series. Hepatic dysfunction and eosinophilia were found in 100% of the cases, while fever (>38 °C) was recorded in 6 out of 9 cases and lymphadenopathy in 7 out of 9. Some rarer clinical features, such as pericarditis and acute pancreatitis, were recorded in cases 4 and 2. None of the patients died of the disease. In case 9, a particularly long course was characterized by the resolution of systemic signs and symptoms, but by the persistence of an erythroderma-like appearance at several month after diagnosis of DRESS. The patient 1 with diffuse macular erythema- Table II.—Histopathologic changes found in the epidermis and dermis of the 9 DRESS patients. Case 1 2 3 4 5 6 7 8 9 Sc % Av Sc Necr KC 0 0 0 2 2 1 0 0 0 5 33.3 0.55 Exoc Lymph 1 2 0 2 0 1 2 0 0 8 55.5 0.88 Spong Vesic 1 2 1 3 0 1 0 0 0 8 55.5 0.88 Focal Interface Changes Lymph Sup Periv Infiltrate 1 2 1 0 2 0 2 1 1 10 77.7 1.1 3 3 3 1 1 3 2 0 0 16 77.7 1.7 Atyp Lymph 0 2 2 1 1 0 0 0 0 6 44.4 0.66 Eos 0 0 0 0 0 0 1 2 0 3 22.2 0.33 Lichenoid infiltrate 0 1 0 0 1 0 0 0 2 4 33.3 0.44 Dilated blood vess 1 2 0 1 1 0 2 1 0 8 66.6 0.88 Extrav erythr 2 1 0 1 0 0 2 1 0 7 55.5 0.77 Score (Sc) expresses the sum of the severity of every single histopathological change out of the total cases considered. Percentage (%) defines the relationship between the number of the cases showing that specific histopathologic change out of the total number of the patients considered for that change. Average Score (Av Sc) represent the ratio between the scoring of a single histopathologic change and the total number of the cases. Legend: Necr KC: necrotic keratinocytes. Exoc Lymph: exocytosis of lymphocytes. Spong Vesic: spongiosis and vesiculation. Focal Interface Changes: focal interface changes. Lymph Sup Periv Infiltrate: lymphocytic superficial perivascular infiltrate. Atyp Lymph: atypical lymphocytes. Eos: eosinophils. Lichenoid infiltrate: lichenoid infiltrate. Dilated blood vess: dilated blood vessels. Extrav eryth: extravasation of erythrocytes. 298 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 HISTOPATHOLOGIC SPECTRUM OF DRESS tous eruption had histopathology characterized by a dense superficial perivascular lymphocytic infiltrate with a mixture of changes of the interface and spongiosis. The EM-like clinical presentation had histologically either a dense perivascular superficial infiltrate with focal interface changes and atypical lymphocytes (case 3) and slight focal interface changes with eosinophils (case 8). None of the 2 cases had necrotic keratinocytes. Erythroderma-like pattern (cases 4 and 5) had both atypical lymphocytes in the dermal infiltrate and a moderate number of necrotic keratinocytes. Spongiosis characterized case 4, while focal interface changes characterized mostly case 5. The urticarial clinical pattern was mostly associated with a superficial perivascular lymphocytic infiltrate (3 out of 4 cases) and spongiosis (2 out of 4) and by focal interface changes (3 out of 4). An inconstant presence of lichenoid infiltrate, dilated blood vessels, extravasation of erythrocytes and necrotic keratinocytes was found in an erratic way throughout the four cases. A constant relationship between the clinical type of DRESS and the histopathologic pattern could not be traced in our patients. This does not mean that DRESS has no histopathologic specific changes. Histopathological features (Table II) were mostly characterized by focal interface changes, with slight vacuolar alteration of basal layer (seven out of nine patients; 77.7%, with an average score of 1.1) and by a superficial variably dense perivascular lymphocytic infiltrate (7 out of 9 patients; 77.7%, average score 1.5). Atypical lymphocytes, with hyperchromatic nuclei, were a relatively common feature, found in 4 out of 9 cases (44.4%, average score 0.66). Spongiosis, as well as exocytosis of lymphocytes, were both found in 55.5%, average score 0.88. Necrotic keratinocytes were found only rarely (33.3%, average score 0.55). On the contrary, dilated blood vessels in the upper part of the dermis and a variable degree of extravasation of erythrocytes were found in about 66% of the cases, with an average score 0.88. True lichenoid infiltrate was found only in 2 cases. Eosinophils were surprisingly a rare histopathological finding (2 cases with very few cells), while all the 9 patients had constant peripheral eosinophilia. We have no reliable explanation of this dissociation between the peripheral eosinophilic pattern and the virtual absence of the eosinophils in the skin. Vol. 149 - No. 3 BORRONI Conclusions Our data cannot confirm a more severe prognosis for patients with EM-like clinical presentation, as reported by some authors.14 The most severe and prolonged course characterized, on the contrary, the erythroderma-like presentation in cases 4 and 5, and in case 9, who had long lasting erythroderma-like changes. In those 3 cases, the severe course of the disease could be referred to a series of several preexisting comorbidities. One of the patients (case 5) also showed HSV vesiculation and crusting on his face. The well known attitude of drugs in inducing a vast and variegate number of clinical reactions (erythematous, exanthema-like, urticarial, EMlike, erythrodermal, papular, macular and oedematous, vesico-bullous) and histopathological variants (spongiotic, bullous, lichenoid, interface dermatitis, perivascular superficial dermatitis with or without necrotic keratinocytes), is confirmed by this study on histology of DRESS. An aspecific diagnosis of drug induced dermatitis may be suspected and done on histopathologic grounds alone, but a specific histopathologic diagnosis of DRESS does not seem feasible for the pathologist or the dermatopathologist, without mandatory and accurate clinical information. References 1. Bocquet H, Bagot M, Roujeau JC. Drug-induced pseudolymphoma and drug hypersensitivity syndrome (drug rash with eosinophilia and systemic symptoms: DRESS). Semin Cutan Med Surg 1996;15:250-7. 2. Kano Y, Hirahara K, Asano Y, Shiohara T. HLA-B allele associations with certain drugs are not confirmed in Japanese patients with severe cutaneous drug reactions. Acta Derm Venereol 2008;88:6168. 3. Genin E1, Chen DP, Hung SI, Sekula P, Schumacher M, Chang PY et al. HLA-A*31:01 and different types of carbamazepine-induced severe cutaneous adverse reactions: an international study and meta-analysis. Pharmacogenomics J 2013 [Epub ahead of print]. 4. McCormack M, Alfirevic A, Bourgeois S, Farrell JJ, Kasperavičiūtė D, Carrington M et al. HLA-A*3101 and carbamazepine-induced hypersensitivity reactions in Europeans. N Engl J Med 2011;364:1134-43. 5. Hetherington S, Hughes AR, Mosteller M, Shortino D, Baker KL, Spreen W et al. Genetic variations in HLA-B region and hypersensitivity reactions to abacavir. Lancet 2002;359:1121-2. 6. Gonçalo M, Coutinho I, Teixeira V, Gameiro AR, Brites MM, Nunes R et al. HLA-B*58:01 is a risk factor for allopurinol-induced DRESS and Stevens-Johnsonsyndrome/toxic epidermal necrolysis in a Portuguese population. Br J Dermatol 2013;169:660-5. 7. Amstutz U1, Shear NH, Rieder MJ, Hwang S, Fung V, Nakamura GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 299 BORRONI HISTOPATHOLOGIC SPECTRUM OF DRESS H et al. Recommendations for HLA-B*15:02 and HLA-A*31:01 genetic testing to reduce the risk of carbamazepine-induced hypersensitivity reactions. Epilepsia 2014 [Epub ahead of print]. 8. Roujeau JC, Stern RS. Severe adverse cutaneous reactions to drugs. N Engl J Med 1994;331:1272-85. 9. Seishima M, Yamanaka S, Fujisawa T, Tohyama M, Hashimoto K. Reactivation of human herpesvirus (HHV) family members other than HHV-6 in drug-induced hypersensitivity syndrome. Br J Dermatol 2006;155:344-9. 10. Kano Y, Hiraharas K, Sakuma K, Shiohara T. Several Herpesviruses can reactivate in a severe drug-induced multiorgan reaction in the same sequential order as in graft-versus-host disease. Br J Dermatol 2006;155:301-6. 11. Kano Y, Shiohara T. Sequential Reactivation of herpesvirus in drug-induced hypersensitivity syndrome. Acta Derm Venereol 2004;84:484-5. 12. Kano Y, Horie C, Inaoka M, Tadashi I, Mizukawa Y, Shiohara T. 300 Herpes Zoster in patients with drug-induced hypersensitivity syndrome/DRESS. Acta Derm Venereol 2012;92:206-7. 13. Gerber BO, Pichler WJ. Cellular mechanisms of T cell mediated drug hypersensitivity. Curr Opin Immunol 2004;16:732-7. 14. Walsh S, Diaz-Cano S, Higgins E, Morris-Jones R, Bashir S, Bernal W et al. Drug reaction with eosinophilia and systemic symptoms: is cutaneous phenotype a prognostic marker for outcome? A review of clinicopathological features of 27 cases. Br J Dermatol 2013;168:391-401. 15. Kardaun SH, Sidoroff A, Valeyrie-Allanore L, Halevy S, Davidovici BB, Mockenhaupt M et al. Variability in the clinical pattern of cutaneous side-effects of drugs with systemic symptoms: does a DRESS syndrome really exist? Br J Dermatol 2007;156:609-11. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 G ITAL DERMATOL VENEREOL 2014;149:301-9 Drug-induced lupus erythematosus A. V. MARZANO, S. TAVECCHIO, C. MENICANTI, C. CROSTI Drug-induced lupus erythematosus (DI-LE) is defined as an entity characterized by clinical manifestations and immunopathological serum findings similar to those of idiopathic lupus but which is temporally related to drug exposure and resolves after withdrawal of the implicated drug. Similarly to idiopathic lupus, DI-LE can be divided into systemic LE, subacute cutaneous LE (SCLE), chronic cutaneous LE (CCLE) and cutaneous LE tumidus. DI-SCLE is the most frequent variant of drug-induced cutaneous LE and presents mainly with annular-polycyclic lesions; the clinical picture is often widespread, with involvement of the lower legs that are usually spared in idiopathic SCLE. ANA and anti-Ro/SSA antibodies are typically present, whereas antihistone antibodies are uncommonly found. We have recently addressed the question whether DI-SCLE differs significantly from its idiopathic counterpart by virtue of clinical features and, based on our findings, we have suggested that the frequent occurrence of malar rash and bullous, erythema multiforme-like and vasculitic manifestations can be regarded as the hallmark of DI-SCLE. In contrast, the histology is not a useful diagnostic criterion for DI-SCLE, considering that the typical pattern of lichenoid interface dermatitis is seen only in the early stage of disease and tissue eosinophilia does not represent a differentiating histopathological feature. DI-CCLE and DI-LE tumidus, albeit possibly misdiagnosed, are rarely observed and are characterized by classic discoid lesions and erythematous-oedematous plaques on sun exposed areas, respectively. Management of DI-LE is based on the discontinuation of the offending drug; topical and/or systemic corticosteroids and other immunomodulating/immunosuppressive agents should be reserved for resistant cases. Key words: Lupus erythematosus - Antibodies, antinuclear Antibodies - Dermatitis - Drug eruptions. Corresponding author: A. V. Marzano, Operative Unit of Dermatology, Department of Pathophysiology and Transplantation, University of Milan, Fondazione IRCCS Ca’ Granda Ospedale Maggiore Policlinico, via Pace 9, 20122 Milan, Italy. E-mail: [email protected] Vol. 149 - No. 3 Operative Unit of Dermatology Department of Pathophysiology and Transplantation University of Milan, Fondazione IRCCS Ca’ Granda Ospedale Maggiore Policlinico, Milan, Italy D rug-induced lupus erythematosus (DI-LE) was first reported in 1945 in association with sulfadiazine.1 It is defined by the following diagnostic criteria: 1) absence of signs and symptoms of lupus erythematosus (LE) before exposure to a drug; 2) appearance of one or more clinical manifestations of LE in combination with antinuclear antibodies (ANA) positivity after exposure to it; 3) resolution of clinical symptoms accompanied by reduction or reverting to normal of ANA titers following drug withdrawal; 4) and recurrence of symptoms once the implicated drug is retaken.2 There are a number of reports in literature concerning patients with preexisting LE in whom the drug acts as a factor inducing exacerbation of the disease or unmasking latent lupus; in these cases, there is lack of resolution of LE symptoms and signs in spite of drug discontinuation.3, 4 As for idiopathic LE, DI-LE may present with systemic symptoms (with or without cutaneous manifestations) or with predominant skin involvement; the cutaneous variants include subacute cutaneous lupus erythematosus (SCLE) and chronic cutaneous lupus erythematosus (CCLE) or discoid LE; there are only few reported cases of cutaneous lupus erythematosus tumidus (DI-LE tumidus) induced by drugs.3-7 This review discusses the dermatological aspects of DI-LE, focusing on its cutaneous variants, particularly the most common presentation, GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 301 MARZANO Drug-induced lupus erythematosus DI-SCLE, suggesting that the latter differs clinically from the idiopathic counterpart; moreover, we provide an update on postulated pathomechanisms for the DI-SCLE skin lesion and DI-LE in general as well as on triggering drugs. Pathogenesis of DI-LE The pathogenesis of DI-LE is not fully understood yet and available data suggest that there is no single mechanism responsible for the induction of autoimmunity. Four main pathomechanisms have been hypothesized:8 1) the drug (or its metabolite) binds itself to a “self” protein making it “foreign” and triggering an autoreactive immune response against this autoantigen by virtue of the so-called molecular mimicry phenomenon;9 2) reactive drug metabolites cause cell death by direct cytotoxicity;10, 11 3) disruption of the central immune tolerance occurs;12, 13 4) autoreactive T-lymphocytes develop owing to DNA hypomethylation;14, 15 all the aforesaid pathomechanisms could co-exist and cross-talk. Some drugs such as anti-tumor necrosis factor (TNF)-alpha agents deserve a separate discussion. Indeed, it has been suggested that these drugs alter the regulatory role of TNF-alpha on antigen presenting cells, inhibiting apoptosis of potentially autoreactive T cells;16 in addition, TNF-alpha blockers could impair the activity of cytotoxic T cells with functions of immunosurveillance, leading to production of pathogenic autoantibodies.14, 17 Another hypothesis is that these drugs inhibit the function of regulatory T (Treg) lymphocytes which are responsible for immunosurveillance. It has also been demonstrated that during treatment with TNF-alpha antagonists there is a reduced expression of CD44 antigen, which contributes to inducing apoptosis of autoreactive T cells. Moreover, the inhibition of T helper (Th) 1 immune response by anti-TNF-alpha agents can determine a shift to a predominantly Th2 response; finally, infections in patients under anti-TNF-alpha therapy may lead to a polyclonal activation of B cells with consequent production of autoantibodies.18, 19 Pathogenesis of DI-SCLE skin lesion The pathogenesis of the DI-SCLE skin lesion remains speculative too. Immune response to skin an- 302 tigens modified by drugs (or ultraviolet radiations) and Fas-dependent apoptosis of epidermal basal keratinocytes are currently proposed as pathomechanisms for inducing and perpetuing skin lesions in SCLE,20-22 as well as in other drug-induced immunemediated cutaneous disorders such as StevensJohnson syndrome, toxic epidermal necrolysis and erythema multiforme (EM).23 The release of soluble pro-inflammatory epidermal and dermal mediators (which may be genetically regulated) and increased expression of cellular adhesion molecules on keratinocytes and subepidermal endothelial cells are also involved. In particular in SCLE, nuclear antigens such as Ro/SSA, translocated to the keratinocyte surfaces, possibly involving the heat-shock proteins are targeted by circulating anti-Ro/SSA antibodies and cytotoxic T cells. These mechanisms are able to upregulate cellular apoptosis.24 An additional pathomechanism may consist in a reduced expression of Bcl-2, a protein known as blocking apoptosis, which has been demonstrated by means of immunohistochemical methods along the epidermal basal layer in lesional skin from patients with LE compared with normal skin.22 Low number of Treg cells has recently been demonstrated in skin lesions of patients with cutaneous LE,25 suggesting that a defective global function of these cells may trigger a crescendo of autoimmunity potentially culminating in the skin illness. In fact, Treg lymphocytes are responsible for immunologic self-tolerance by suppressing potentially autoreactive T cells. Thus, although the exact role of the offending drug in triggering keratinocyte apoptosis and recruiting inflammatory cells into the DI-SCLE skin lesion remains to be elucidated, the above findings suggest that the extent of both epidermal apoptosis and inflammation may correlate with the chronological development and severity of LE skin lesions. DI-SCLE Idiopathic SCLE was recognized in 1979 as a distinct subtype of cutaneous LE with unique clinical, immunological and genetic features.26, 27 Clinically, SCLE typically presents with nonscarring annular or papulosquamous eruptions on sun exposed skin, mainly the upper back, chest, dorsal arms and lateral neck. However, a number of unusual variants have been described, including pityriasiform, bullous, GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Drug-induced lupus erythematosus erythrodermic, poikilodermatous, toxic epidermal necrolysis-like and erythema multiforme (EM)-like subtypes.28-33 Anti-Ro/SSA antibodies are classically regarded as the serological marker for this subset.34, 35 DI-SCLE was described for the first time in 1985 by Reed et al.36 in association with hydrochlorothiazide; they reported 5 patients with DI-SCLE, one of whom was affected by systemic LE since 25 years without skin lesions and another one complained of arthralgias.36 Several drugs have been reported as causative agents of DI-SCLE, including antihypertensive drugs such as diuretics, calcium channel blockers and angiotensin converting enzyme inhibitors, antifungals such as terbinafine,37-39 statins and chemotherapeutics;16, 40-47 recently, there were several reported cases of SCLE induced by TNF-alpha antagonists and their number is progressively increasing 48, 49 (Table I). From a meta-analysis of the literature published by Lowe et al. in 2011 50 comes that there were 117 reported cases of DI-SCLE with a prevalence in females (72% of cases) and a mean age at disease onset of 58 years; in this study, the mean incubation period for all drug classes combined was 27.9 weeks (range: 3 days to 11 years) and the mean overall time to resolution of DI-SCLE after drug discontinuation was 7.3 weeks (range: 1 week to 32 weeks). These authors concluded that there was adequate published experience to suggest that DI-SCLE did not differ clinically, histopathologi- MARZANO cally or immunologically from idiopathic SCLE.50 We have seen and followed-up in our department 11 cases of DI-SCLE between 2001 and 2010, whose clinical features, immunological findings, course and therapy are summarized in Table II. The cutaneous features were compared with those of our 79 patients with idiopathic SCLE to address the question whether DI-SCLE differs significantly from its idiopathic counterpart.51 Clinical manifestations Unlike the literature data coming from the metaanalysis by Lowe et al.,50 DI-SCLE manifested as widespread skin lesions involving also lower extremities in nine out of eleven patients of our case series (82%), while generalized involvement was observed in only five out of our 79 patients with idiopathic SCLE (6%).51 In eight patients (73%), DI-SCLE presented with annular-polycyclic eruptions, while in two patients it was characterized by papulosquamous lesions (18%); coexistence of annular-polycyclic and papulosquamous features was observed in only one patient (9%). Unlike the data reported by Lowe et al.,50 in our case series DISCLE significantly differed from idiopathic SCLE by virtue of distinctive cutaneous features, particularly the frequent occurrence of malar rash and bullous, EM-like and vasculitic manifestations. Indeed, Table I.—Drugs associated with drug-induced subacute cutaneous lupus erythematosus. Thiazidic diuretics Calcium channel blockers ACE inhibitors β-blockers Statins Biologics Antibiotics Chemotherapics Antifungals NSAIDs Antidepressant Proton pump inhibitors Anticonvulsants Antiaggregants Immunosuppressants Antihistamines Antiemetics Ranitidine Hydroclorothiazide Diltiazem, verapamil, nifedipine, nitrendipine Cilazapril Acebutolol Simvastatin TNF-α antagonists (infliximab, etanercept, adalimumab, golimumab), efalizumab, rituximab Rifabutin/rifamycin, doxycycline Gemcitabine, doxorubicin, capecitabine, fluorouracil, tamoxifen, docetaxel, paclitaxel, interferon β, interferon α, leuprorelin Terbinafine, griseofulvin Piroxicam, naproxen Bupropion Lansoprazole, pantoprazole, esomeprazole, omeprazole Carbamazepine, sodium valproate, lamotrigine, phenytoin Ticlopidine Leflunomide Cinnarizine Thiethylperazine ACE: angiotensin converting enzyme; NSAID: non-steroidal anti-inflammatory drugs; TNF: tumor necrosis factor. Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 303 MARZANO Drug-induced lupus erythematosus Table II.—Summary of the clinical features, immunological findings, course and treatment in our 11 cases of drug-induced subacute cutaneous lupus erythematosus (modified from Marzano AV et al.51). Patient Sex Age at onset (years) Offending drug Incubation time (weeks) Cutaneous features Annularpolycyclic; bullous Annularpolycyclic; bullous; EM-like; malar rash Papulosquamous Annularpolycyclic; bullous; purpuric; malar rash Annularpolycyclic; EM-like; purpuric; malar rash Annularpolycyclic; EM-like; purpuric; malar rash Annularpolycyclic; EM-like; malar rash Annularpolycyclic; bullous; purpuric and necroticulcerative Annularpolycyclic; bullous; EM-like; purpuric and necroticulcerative Papulosquamous Annularpolycyclic/ papulosquamous overlap 1 M 66 Nitrendipine 3 2 F 24 Leflunomide 3 3 F 70 Etanercept 3 4 M 60 Piroxicam 3 5 F 80 Allopurinol 4 6 M 62 Amoxicillin plus clavulanic acid 2 7 F 72 Hydroxychloroquine 6 8 F 85 Ramipril 4 9 M 90 Carbamazepine 2 10 F 68 Enalapril 6 11 F 58 Hydroxychloroquine 6 Immunological findings Treatment Resolution time (weeks) Follow-up (years) ANA; Ro/SSA; La/SSB; AHA; Sm; aCL; LAC ANA None 4 9 Pred 3 4 ANA; Ro/SSA None 3 4 ANA; Ro/SSA Pred 24 5 ANA; Ro/SSA None 3 3 Absent ANA; Ro/SSA; La/SSB; AHA None 3 2 Absent ANA; Ro/SSA; La/SSB None 8 3 Absent ANA; Ro/SSA; La/SSB; RNP; Scl-70 None 8 1 Absent ANA; Ro/SSA; La/SSB; aCL Pred 10 1 ANA; Ro/SSA None 4 6 ANA; Ro/SSA None 4 5 Extracutaneous involvement Absent Absent Absent Absent Absent Absent Absent M: male, F: female; EM: erythema multiforme; ANA: antinuclear antibodies; Ro/SSA: Ro/Sjögren’s syndrome associated antigen; La/SSB: La/Sjögren’s syndrome associated antigen B; AHA: antihistone antibodies; aCL: anticardiolipin antibodies; LAC: lupus anticoagulant; RNP: anti-ribonucleoprotein antibodies; Sm: Smith antigen; pred: oral prednisone. bullous lesions, typically occurring over the edge of annular-polycyclic eruptions (Figure 1A), were observed in five of 11 patients with DI-SCLE (45%) and in only one patient with idiopathic SCLE (1%). 304 Five of 11 patients with DI-SCLE (45%) presented with targetoid EM-like lesions (Figure 1B), which were present in only one patient with idiopathic SCLE (1%). Vasculitic manifestations, namely only GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Drug-induced lupus erythematosus purpuric (Figure 1C) or purpuric and necrotic-ulcerative lesions, on the lower legs were seen in five of 11 patients with DI-SCLE (45%); in contrast, only two of 79 patients with idiopathic SCLE (3%) exhibited vasculitic lesions. Finally, malar rash (Figure 1D) was evident in five of 11 patients with DI-SCLE (45%), while it was seen in five of 79 patients with the idiopathic counterpart (6%). As regards systemic symptoms and signs, arthralgias or arthritis, serositis and other visceral involvement as well as Raynaud phenomenon were lacking in all our 11 patients with DI-SCLE; on the other hand, in none of the 11 patients were the American College of Rheumatology criteria 52 for the diagnosis of systemic LE fulfilled.51 Histopathological aspects In the early stages of disease, skin biopsy specimens taken from both annular-polycyclic and papulosquamous lesions show a typical pattern of lichenoid interface dermatitis: it consists in an upper dermal lympho-histiocytic infiltrate invading the dermoepidermal junction with hydropic degeneration of the epidermal basal cell layer; numerous necrotic keratinocytes are also present (Figure 2A). In papulosquamous lesions there is also psoriasiform hyperplasia of the epidermis. Dermoepidermal detachment is seen in patients having annular-polycyclic lesions associated with blisters. In EM-like lesions, the histological picture is similar to that found in DI-SCLE but with stronger hydropic degeneration of the basal layer. Purpuric as well as necrotic-ulcerative lesions reveal typical histopathological features of leukocytoclastic vasculitis. In the late stages of disease, nonspecific changes are usually observed, namely mononuclear cell inflammatory infiltrates in the upper dermis without epidermal alterations.51 Some authors have recently reviewed skin biopsy specimens of 59 patients with SCLE, 15 of whom were drug-induced and 44 idiopathic, concluding that tissue eosinophilia does not represent a differentiating histopathological feature of DI-SCLE.53 MARZANO Laboratory findings It is well known that SCLE is characterized by distinctive immunological profile consisting in positivity of ANA (81-100% of cases) and Ro/SSA (81-90% of cases); SSB/La positivity is observed in a lesser percentage of cases (45-48%);3, 50, 51 antihistone antibodies can be detected in 33% of cases and, unlike druginduced systemic LE, are not considered a serological marker of DI-SCLE.54, 55 According to Lowe et al.,50 anti-Ro/SSA antibodies, re-evaluated in clinical remission, remain positive in 66.7% of cases; in our case series however, these autoantibodies were negative in 73% of patients when re-assessed at least one year after DI-SCLE resolution.51 Antidouble stranded (ds) DNA antibodies are usually absent, whereas anticardiolipin antibodies in combination with anti-beta2-glycoprotein I and lupus anticoagulant have been found in one case reported by ourselves.56 Anemia, leukopenia and thrombocytopenia are rarely reported.3, 51 Treatment and course The management of DI-SCLE consists in the discontinuation of the implicated drug. Pharmacological treatment should be reserved for either severe or refractory cases, these last sometimes representing a preexisting lupus exacerbated by the offending drug. Systemic corticosteroids at the doses commonly used for idiopathic SCLE are the first-choice therapy; topical steroids and/or hydroxychloroquine may be associated. In more resistant cases, other immunomodulating/immunosuppressive agents such as thalidomide, azathioprine, cyclophosphamide or mycophenolate can be used.3 In our case series, DI-SCLE healed upon drug discontinuation after a mean resolution time of 7 weeks (range 3–24); the three patients showing the most severe clinical presentation were given oral prednisone 0.5 mg/kg/day at progressively tapering dosages until stopping after SCLE resolution. At the time of writing, all patients were alive and free of disease after a mean time of follow-up of 4 years (range 1-9), with neither relapses nor evolution into idiopathic systemic LE having occurred.51 Direct immunofluorescence features Direct immunofluorescence on sun exposed skin usually reveals granular deposits of immunoglobulin (Ig) M (Figure 2B) and/or IgG and/or complement (C) 3 at the dermoepidermal junction.51 Vol. 149 - No. 3 DI-CCLE DI-CCLE is a rare entity originally reported as caused by fluororuracile agents like tegafur and GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 305 MARZANO Drug-induced lupus erythematosus A C B D Figure 1.—A) Bullae evolved in crusts covering the edge of annular polycyclic lesions on the lower extremities in a patient with druginduced subacute cutaneous lupus erythematosus (DI-SCLE); B-D) DI-SCLE patients. Targetoid erythema multiforme-like lesions extensively involving the back and gluteal regions (B). Vasculitic features manifesting as purpura on the legs (C). Typical malar rash (D). 306 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Drug-induced lupus erythematosus A MARZANO B Figure 2.—A) Skin biopsy specimens taken from a patient with drug-induced subacute cutaneous lupus erythematosus (DI-SCLE) showing a lichenoid interface dermatitis histopathological pattern (hematoxylin-eosin stain; original magnification, x 200); B) direct immunofluorescence studies on sun exposed lesional skin of a DI-SCLE patient revealing immunoglobulin (Ig) M deposits along the dermoepidermal junction (fluoresceine isothiocyanate stain; original magnification, x 200). uraciltegafur (UFT).57 More recently, some cases triggered by TNF-alpha antagonists, such as infliximab or etanercept, have been described.4, 16, 44-47, 58 The clinical features are those of the idiopathic counterpart, namely classic discoid lesions presenting with a photosensitive distribution on the face, upper trunk and arms. Systemic symptoms such as fever, arthralgia or myalgia are typically lacking. Concerning immunological findings, ANA have been reported to be present in 66% of cases whereas anti-extractable nuclear antigen (ENA) and anti-dsDNA antibodies are usually absent as well as antihistone antibodies. As for idiopathic CCLE, anaemia, leukopenia and thrombocytopenia are generally not found.3 Treatment and course of DI-CCLE and DI-LE tumidus The treatment of choice for DI-CCLE and DI-LE tumidus consists in the withdrawal of the implicated drug. Cutaneous manifestations usually heal within 8 weeks; sometimes the complete resolution can be slower, making useful a drug treatment. Hydroxychloroquine at the doses commonly used for the idiopathic counterparts, in combination with topical corticosteroids, is the first-line therapy. Systemic corticosteroids or thalidomide can be used in resistant cases.3 Conclusions DI-LE tumidus To the best of our knowledge, only six cases of DI-LE tumidus presenting with typical erythematous-oedematous plaques on sun exposed areas have been reported: three cases were due to TNF-alpha blockers, two triggered by bortezomib, a proteasome inhibitor approved for the treatment of multiple myeloma, and another one occurred following assumption of an angiotensin-converting enzyme inhibitor. Extracutaneous involvement was lacking in all the aforesaid cases.4, 47, 58-62 Vol. 149 - No. 3 DI-SCLE is the most frequent variant of druginduced cutaneous LE and presents mainly with annular-polycyclic manifestations; the clinical picture is often generalized, with involvement of the lower legs that are usually spared in idiopathic SCLE. ANA and anti-Ro/SSA antibodies are usually present, whereas antihistone antibodies are uncommonly found. We have recently addressed the question whether DI-SCLE differs significantly from its idiopathic counterpart by virtue of clinical aspects and, on the basis of our findings, we have suggested that the frequent occurrence of ma- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 307 MARZANO Drug-induced lupus erythematosus lar rash and bullous, EM-like and vasculitic manifestations can be considered distinctive features marking the drug-induced variant. In contrast, the histology is not a verifying criterion for DI-SCLE, considering that the typical pattern of lichenoid interface dermatitis is seen only in the early phase of disease. DI-CCLE, albeit possibly misdiagnosed, is rarely observed and its picture is characterized by the occurrence of classic discoid lesions typically involving sun exposed sites; aspects of lupus tumidus, whose actual incidence may also be underestimated, have rarely been reported, particularly in patients treated with TNF-alpha antagonists. In conclusion, although DI-SCLE seems to represent a subset different clinically from the idiopathic counterpart, careful review of a patient’s drug history in correlation with clinical findings remains the standard for identifying a drug as an etiologic or exacerbating factor in patients with LE. References 1. Hoffman BJ. Sensitivity to sulfadiazine resembling acute disseminated lupus erythematosus. Arch Derm Syphilol 1945;51:190-2. 2. Hess E. Drug-related lupus. N Engl J Med 1988; 318:1460-2. 3. Marzano AV, Vezzoli P, Crosti C. Drug-induced lupus: an update on its dermatologic aspects. Lupus 2009;18:935-40. 4. Callen JP. Drug-induced subacute cutaneous lupus erythemaosus. Lupus 2010;19:1107-11. 5. Dalle Vedove C, Del Giglio M, Schena D, Girolomoni G. Druginduced lupus erythematosus. Arch Dermatol Res 2009;301:99105. 6. Sarzi-Puttini P, Atzeni F, Capsoni F, Lubrano E, Doria A. Druginduced lupus erythematosus. Autoimmunity 2005;38:507-18. 7. Schneider SW, Staender S, Schlüter B, Luger TA, Bonsmann G. Infliximab-induced lupus erythematosus tumidus in a patient with rheumatoid arthritis. Arch Dermatol 2006;142:115-6. 8. Uetrecht J. Current trends in drug-induced autoimmunity. Toxicology 2005;4:309-14. 9. Griem P, Wulferink M, Sachs B, Gonzalez JB, Gleichmann E. Allergic and autoimmune reactions to xenobiotics: how do they arise. Immunol Today 1998;19:133-41. 10. Williams DP, Pirmohamed M, Naisbitt DJ, Utrecht JP, Park BK. Induction of metabolism dependent and independent neutrophil apoptosis by clozapine. Mol Pharmacol 2000;58:207-16. 11. Hess DA, Sisson ME, Suria MJ, Wijsman J, Puvanesasingham R, Madrenas J et al. Cytotoxicity of sulphonamide reactive metabolities: apoptosis and selective toxicity of CD8+ cells by the hydroxylamine of sulfamethoxazole. FASEB J 1999;13:1688-98. 12. Kretz-Rommel A, Duncan SR, Rubin RL. Autoimmunity caused by disruption of central T cell tolerance: a murine model of druginduced lupus. J Clin Invest 1997;99:1888-96. 13. Kretz-Rommel A, Rubin RL. Disruption of positive selection of thymocytes causing autoimmunity. Nat Med 2000;6:298-305. 14.Yung RL, Quddus J, Chrisp CE, Johnson KJ, Richardson BC. Mechanism of drug-induced lupus. Cloned Th2 cells modified with DNA methylation inhibitors in vitro cause autoimmunity in vivo. J Immunol 1995;154:3025-35. 308 15.Yung R, Chang S, Hemati H, Johnson KJ, Richardson BC. Mechanism of drug-induced lupus. Comparison of procainamide and hydralazine with analogs in vitro and in vivo. Arthritis Rheum 1997;40:1436-43. 16. Costa MF, Said NR, Zimmermann B. Drug-induced lupus due to anti-tumor necrosis factor alpha agents. Semin Arthritis Rheum 2008;37:381-7. 17.Yung R, Powers D, Johnson K, Amento E, Carr D, Laing T et al. Mechanisms of drug-induced lupus. II. T cells overexpressing lymphocyte function-associated antigen 1 become autoreactive and cause a lupuslike disease in syngeneic mice. J Clin Invest 1996;97:2866-71. 18. William EL, Gadola S, Edwards CJ. Anti-TNF-induced lupus. Rheumatology (Oxford). 2009;48:716-20. 19. Caramaschi P, Biasi D, Colombatti M, Pieropan S, Martinelli N, Carletto A et al. Anti-TNFalpha therapy in rheumatoid arthritis and autoimmunity. Rheumatol Int 2006;26:209-14. 20. Bennion SD, Middleton MH, David-Bajar KM, Brice S, Norris DA. In three types of interface dermatitis, different patterns of expression of intercellular adhesion molecule-1 (ICAM-1) indicate different triggers of disease. J Invest Dermatol 1995;105:71-9. 21. Norris D, Bennion S, David-Bajar K. Pathomechanisms of cutaneous lupus erythematosus. In: Wallace DJ, Hahn BH, editors. Dubois’ lupus erythematosus. 5th ed. Baltimore, MD: Williams & Wilkins; 1997. p. 549-67. 22. Baima B, Sticherling M. Apoptosis in different cutaneous manifestations of lupus erythematosus. Br J Dermatol 2001;144:958-66. 23. Marzano AV, Frezzolini A, Caproni M, Parodi A, Fanoni D, Quaglino P et al. Immunohistochemical expression of apoptotic markers in drug-induced erythema multiforme, Stevens–Johnson syndrome and toxic epidermal necrolysis. Int J Immunopathol Pharmacol 2007;20:557-66. 24. Nyberg F, Stephansson E. The role of T cells and adhesion molecules in cutaneous lupus erythematosus. In: Kuhn A, Lehmann P, Ruzika T, editors. Cutaneous lupus erythematosus. Berlin: Springer-Verlag; 2005. p. 267-81. 25. Franz B, Fritzsching B, Riehl A, Oberle N, Klemke CD, Sykora J et al. Low number of regulatory T cells in skin lesions of patients with cutaneous lupus erythematosus. Arthritis Rheum 2007;56:191020. 26. Sontheimer RD, Thomas JR, Gilliam JN. Subacute cutaneous lupus erythematosus: a cutaneous marker for a distinct lupus erythematosus subset. Arch Dermatol 1979;115:1409-15. 27. Sontheimer RD, Maddison PJ, Reichlin M, Jordon RE, Stastny P, Gilliam JN. Serologic and HLA associations in subacute cutaneous lupus erythematosus, a clinical subset of lupus erythematosus. Ann Intern Med 1982;97:664-71. 28. Sontheimer RD. Subacute cutaneous lupus erythematosus. A quarter century’s perspective. In: Sarzi-Puttini P, Doria A, Girolomoni G, Kuhn A, editors. The skin in systemic autoimmune disease. Amsterdam: Elsevier; 2006. p. 65-86. 29. Marzano AV, Facchetti M, Alessi E. Poikilodermatous subacute cutaneous lupus erythematosus. Dermatology 2003;207:285-90. 30. Marzano AV, Berti E, Gasparini G, Caputo R. Lupus erythematosus with antiphospholipid syndrome and erythema multiforme-like lesions. Br J Dermatol 1999;141:720-4. 31. Caproni M, Cardinali C, Salvatore E, Fabbri P. Subacute cutaneous lupus erythematosus with pityriasis-like cutaneous manifestations. Int J Dermatol 2001;40:59-62. 32. Torchia D, Caproni M, Massi D, Chella A, Fabbri P. Paraneoplastic toxic epidermal necrolysis-like subacute cutaneous lupus erythematosus. Clin Exp Dermatol 2010;35:455-6. 33. Aydogan K, Karadogan S, Balaban Adim S, Tunali S. Lupus erythematosus associated with erythema multiforme: report of two cases and review of the literature. J Eur Acad Dermatol Venereol 2005;19:621-7. 34. Lee LA, Roberts CM, Frank MB, McCubbin VR, Reichlin M. The GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Drug-induced lupus erythematosus autoantibody response to Ro/SSA in cutaneous lupus erythematosus. Arch Dermatol 1994;130:1262-8. 35. Marzano AV, Lazzari R, Polloni I, Boneschi V, Crosti C. Rosacealike cutaneous lupus erythematosus: an atypical presentation responding to antimalarials. Acta Derm Venereol 2013;93:106-7 36. Reed BR, Huff JC, Jones SK, Orton PW, Lee LA, Norris DA. Subacute cutaneous lupus erythematosus associated with hydrochlorothiazide therapy. Ann Intern Med 1985;103:49-51. 37. Bonsmann G, Schiller M, Luger TA, Stander S. Terbinafine-induced subacute cutaneous lupus erythematosus. J Am Acad Dermatol 2001;44:925-31. 38. Farhi D, Viguier M, Cosnes A, Reygagne P, Dubertret L, Revuz J et al. Terbinafine-induced subacute cutaneous lupus erythematosus. Dermatology 2006;212:59-65. 39. Callen JP, Hughes AP, Kulp-Shorten C. Subacute cutaneous lupus erythematosus induced or exacerbated by terbinafine: a report of 5 cases. Arch Dermatol 2001;137:1196-8. 40. Cassis TB, Callen JP. Bupropion-induced subacute cutaneous lupus erythematosus. Australas J Dermatol 2005;46:266-9. 41. Fenniche S, Dhaoui A, Ammar FB, Benmously R, Marrak H, Mokhtar I. Acebutolol-induced subacute cutaneous lupus erythematosus. Skin Pharmacol Physiol 2005;18:230-3. 42. Dam C, Bygum A. Subacute cutaneous lupus erythematosus induced or exacerbated by proton pump inhibitors. Acta Derm Venereol 2008;88:87-9. 43. Marzano AV, Ramoni S, Del Papa N, Barbareschi M, Alessi E. Leflunomide-induced subacute cutaneous lupus erythematosus with erythema multiforme-like lesions. Lupus 2008;17:329-31. 44. DeBandt M, Sibilia J, Le Loet X, Prouzeau S, Fautrel B, Marcelli C et al. Systemic lupus erythematosus induced by anti tumor necrosis factor alpha therapy: a French national survey. Arthritis Res Ther 2005;7:R545-51. 45. Bentley DD, Graves JE, Smith DI, Hefferman MP. Efalizumabinduced subacute cutaneous lupus erythematosus. J Am Acad Dermato 2006;54:S242-3. 46. Spillane AP, Xia Y, Sniezek PJ. Drug-induce lupus erythematosus in a patient treated with adalimumab. J Am Acad Dermatol 2007;56:S114-6. 47. Chen JK, Chen TS, Lim P, Iqbal M. Drug-induced subacute cutaneous lupus erythematosus associated with doxorubicin. J Am Acad Dermatol 2012;67:273-5. 48. Marzano AV, Borghi A, Meroni PL, Crosti C, Cugno M. Immunemediated inflammatory reactions and tumors as skin side effects of inflammatory bowel disease therapy. Autoimmunity 2014 [E-pub ahead of print]. 49. Wilkerson E, Hazey MA, Bahrami S, Callen JP. Golimumab-exacerbated subacute cutaneous lupus erythematosus. Arch Dermatol 2012;148:1186-90. Vol. 149 - No. 3 MARZANO 50. Lowe G, Henderson CL, Grau RH, Hansen CB, Sontheimer RD. A systematic review of drug-induced subacute cutaneous lupus erythematosus. Br J Dermatol 2011;164:465-72. 51. Marzano AV, Lazzari R, Polloni I, Crosti C, Fabbri P, Cugno M. Drug-induced subacute cutaneous lupus erythematosus: evidence for differences from its idiopathic counterpart. Br J Dermatol 2011;165:335-41. 52. Tan EM, Cohen AS, Fries JF, Masi AT, McShane DJ, Rothfield NF et al. The 1982 revised criteria for the classification of systemic lupus erythematosus. Arthritis Rheum 1982;25:1271-7. 53. Hillesheim PB, Bahrami S, Jeffy BG, Callen JP. Tissue eosinophilia. Not an indicator of drug-induced subacute cutaneous lupus erythematosus. Arch Dermatol 2012;148:190-3. 54. Sontheimer RD, Henderson CL, Grau RH. Drug-induced subacute cutaneous lupus erythematosus: a paradigm for bedside-to-bench patient-oriented translational clinical investigation. Arch Dermatol Res 2009;301:65-70. 55. Callen JP. Drug-induced cutaneous lupus erythematosus, a distinct syndrome that is frequently unrecognized. J Am Acad Dermatol 2001;45:315–6. 56. Marzano AV, Borghi A, Mercogliano M, Facchetti M, Caputo R. Nitrendipine-induced subacute cutaneous lupus erythematosus. Eur J Dermatol 2003;13:213-6. 57.Yoshimasu T, Hiroi A, Uede K, Furukawa F. Discoid lupus erythematosus (DLE)-like lesion induced by uracil. Eur J Dermatol 2001;11:54-7. 58. Vezzoli P, Violetti SA, Serini SM, Muratori S, Berti E, Crosti C. Cutaneous lupus erythematosus induced by adalimumab. J Dermatol 2011;38:283-4. 59. Aguayo-Leiva I, Vano-Galvan S, Carrillo-Gijon R, Jaén-Olasolo P. Lupus tumidus induced by bortezomib not requiring discontinuation of the drug. J Eur Acad Dermatol Venereol 201;24:13634. 60. Schneider SW, Staender S, Schlüter B, Luger TA, Bonsmann G. Infliximab-induced lupus erythematosus tumidus in a patient with rheumatoid arthritis. Arch Dermatol. 2006;142:115-6. 61. Schepis C, Lentini M, Siragusa M, Batolo D. ACE-inhibitorinduced drug eruption resembling lymphocytic infiltration (of Jessner-Kanof) and Lupus erythematosus tumidus. Dermatology 2004;208:354-5. 62. Böckle BC, Baltaci M, Weyrer W, Sepp NT. Bortezomib-induced lupus erythematosus tumidus. Oncologist 2009;14:637-9. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 309 G ITAL DERMATOL VENEREOL 2014;149:311-6 Inflammatory/infectious cutaneous side effects of biological drugs in patients with psoriasis: a general review with personal data F. RONGIOLETTI 1, 2, M. BURLANDO 1, 2, A. PARODI 1, 2 In recent years, the use of biologic drugs has greatly changed the therapy of psoriasis and psoriatic arthritis, but they have some adverse effects. In particular, skin lesions induced by anti-tumor necrosis factor (TNF) and anti-interleukin (IL) 12/23 drug (ustekinumab) have been reported with an increased incidence, highlighting the importance of the skin as a major target of the side effects of these drugs. There is a wide spectrum of skin lesions of different morphology and etiology that includes skin lesions directly related to drug administration, the development of cutaneous immune-mediated conditions and cutaneous infections. The aim of this review is to revisit the literature data on inflammatory/infectious skin adverse effects of biologics both anti-TNF-α inhibitors and anti-IL 12/23 antagonists and to report and update our personal data on inflammatory/infectious side effects in patients with psoriasis/psoriatic arthritis treated with biologics. Key words: Biological products - Drug-related side effects and adverse reactions - Psoriasis. T he advent of biological drugs such as anti-tumor necrosis factor (TNF)-a and anti-interleukin (IL) 12/23 inhibitors in recent years has provided an important armamentarium in the treatment of various dermatologic diseases, especially psoriasis.1 However, even if well tolerated, increasing use of these medications in clinical practice has led to the recognition of a variety of dermatologic adverse drug reactions. There is a wide spectrum of skin lesions of different morphology and etiology induced by biologics that includes skin lesions directly related to drug administration, the development of cutaneous Corresponding author: F. Rongioletti, MD, Clinica Dermatologica, Viale Benedetto XV 7, Genoa, Italy. E-mail: [email protected] Vol. 149 - No. 3 1IRCCS, San Martino‑IST University Hospital Genoa, Italy 2Section of Dermatology DISSAL University of Genoa, Genoa, Italy immune-mediated conditions and cutaneous infections (Table I). This paper is divided into two parts. The first is a general review of all the inflammatory/infectious dermatologic side effects related to biological drugs including both anti-TNF-a and anti CD 12/23 inhibitors. The second part deals with our personal experience with the inflammatory/infectious skin adverse reactions observed in treating psoriatic patients at the Section of Dermatology, University of Genoa, Italy by both anti-TNF-a blockers (infliximab, etanercept, adalimumab, golimumab) and IL-12/23 antagonist (ustekinumab). Overview of cutaneous adverse events related to TNF-α inhibitors The main inflammatory skin adverse reactions reported during therapy with anti-TNF-a inhibitors are “toxic/allergic” reactions and immune-mediated skin diseases, “autoimmune” skin diseases including interface dermatitis (lichenoid reactions, erythema multiforme, lupus and lupus-like disease), cutaneous vasculitis, bullous diseases, granulomatous dermatitis, eczematous reactions (atopic-like dermatitis), alopecia and psoriasiform dermatitis, which represents GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 311 RONGIOLETTI INFLAMMATORY SIDE EFFECTS OF BIOLOGICS IN PATIENTS WITH PSORIASIS Table I.—Main cutaneous adverse events associated to treat‑ ment with TNF-alpha antagonists. 1.Skin lesions related to the administration of treatment –– Toxic/allergic reactions –– Acute infusion reactions –– Delayed exanthematous rash –– Injection site reactions 2.Immune-mediated diseases –– New onset psoriasis and exacerbation of prior psoriasis –– Eczematous reactions (atopic-like dermatitis) –– Lupus-like syndromes and cutaneous lupus –– Vasculitis –– Lichenoid reaction –– Erythema multiforme, Stevens-Johnson syndrome –– Alopecia areata/psoriasiform alopecia –– Granulomatous reactions (sarcoid-like) –– Bullous diseases –– Miscellanea 3.Cutaneous infections –– Bacterial infections: cellulitis, folliculitis –– Viral infections: herpes zoster, herpes simplex –– Fungal infections: candidiasis, pityriasis versicolor a paradoxical side effect.2, 3 Each cutaneous eruption improved or resolved with switching to a different TNF-a inhibitor, discontinuation of the anti-TNF-a agent, and/or topical or systemic steroids. The mechanism for such diverse cutaneous eruptions among this class of medications remains poorly understood. The spectrum of cutaneous injections is quite variable, depending on the type of TNF-a blocker used and include bacteriae, viral, fungal and protozoan infection. Skin lesions related to the administration of treat‑ ment Toxic/allergic reactions The most frequent side effects of TNF-α inhibitor drugs are: i) acute infusion reactions and delayed exanthematous rash with infliximab; and ii) injection site reactions (ISRs) to subcutaneously administered etanercept, adalimumab and golimumab. Infusion reactions to infliximab occurs in 16% of treated patients compared with 6% of placebo. The acute reaction occurs during or within 24 hours while the delayed reaction occurs from 24 hours to 14 days after administration. The risk is also linked to the presence of human antichimeric antibodies but may be lessened by concomitant use of methotrexate, azathioprine. Most of these reactions are mild or 312 moderate with hypertension, pruritus, sudden flush, vomiting, tachycardia or bradycardia, shivers and fever. Only few reactions are severe and are characterized by urticaria, Quincke’s edema, tickling throat, dyspnea, and hypotension. In the former, reducing the infusion rate to 60-80 mL/h (20-30 drops/min) led to disappearance of symptoms while in the latter the infusion should be immediately stopped giving appropriate drugs (steroids, adrenaline).4 Patients treated with TNF-α inhibitors such as etanercept, adalimumab and golimumab can develop ISRs around the sites of injections. The mechanism resides mainly in type IV delayed type reaction with recruitment of CD8+ cytotoxic lymphoid cells (TH1lymphocyte- reaction). Well syndrome-like reaction with dermal infiltrate of eosinophils and recall ISRs have also been reported. Recall ISRs are reaction at sites where anti-TNF-a was previously injected after the last injection. Biopsy specimens from recall ISRs demonstrates that the dermal infiltrate was predominantly composed of CD4+ T lymphocytes. Clinically, these reactions consist of erythema, edema, pruritus, pain, indurated plaque and occur within the first 2 months, usually 1 to 2 days after the last injection and heals within a few days. Discontinuation of therapy is usually not necessary.5, 6 Long-term studies are necessary to determine the durability of response and the real risk of ISRs with golimumab and certolizumab pegol.7 Immune-mediated disorders The use of anti-TNF-α is associated with a growing number of autoimmune or immune-mediated diseases which include psoriasiform reactions, interface dermatitis (lichenoid reactions, lupus and lupus-like syndrome, erythema multiforme/StevensJohnson syndrome), cutaneous vasculitis, granulomatous dermatitis, eczematous reactions, alopecia and bullous diseases.8 Psoriasiform reactions (new onset psoriasis and exacerbation of prior psoriasis) The development of psoriasis or the exacerbation of a pre-existent psoriasis is a paradoxal phenomenon that have been described in patients treated with TNF-a inhibitors such as infliximab, etanercept, adalimumab.9-12 The incidence of induced psoriasis is estimated at 2.3-5%. In a study of the Mayo GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 INFLAMMATORY SIDE EFFECTS OF BIOLOGICS IN PATIENTS WITH PSORIASIS RONGIOLETTI Clinic dealing with patients seen from 1998 to 2010, 56 patients (73% females, mean age 48 y) presented with a psoriasiform reaction. They were affected by Crohn’s disease in 39% of cases and rheumatoid arthritis in 25%. New-onset or worsening psoriasis occurred after a mean treatment duration of 17.1 months with infliximab in 54% of cases, adalimumab in 34% and etanercept in 12%. The clinical presentation included: plaque psoriasis (N.=27), palmoplantar pustulosis (N.=25), scalp psoriasis (N.=12), generalized pustular psoriasis (N.=7), erythrodermic psoriasis (N.=2), and inverse psoriasis (N.=2). Several patients were treated with more than a single TFN-a inhibitor.12 As for the treatment, stopping TNF blocking therapy should be decided on individual basis. In cases of mild or non-acute reactions, topical corticosteroids and phototherapy ± acitretin seem to be effective. For more severe or acute systemic reactions, addition of cyclosporine or methotrexate should be evaluated. We have to consider that switching to a different TNF inhibitor may well worsen the lesions as this paradoxical response appears to be a class effect. The underlying pathogenesis of induction of psoriasis or psoriasiform reactions by TNF-a inhibitors remain elusive but the disruption of balance between TNF/INF-a (YANG & YIN theory) is one of the most reputed hypothesis. In fact, TNF influences expression of many other cytokines including INF-a which is produced by plasmacytoid dendritic cells, involved in early lesions of psoriasis. The blockade of TNF-α receptors by the drugs results in deregulated overproduction of INF-α which could be responsible of the paradox of worsening or inducing psoriasiform reactions.13 antibodies to double-stranded DNA (dsDNA).14-16 Antihistone antibodies are present in 17-57%. The positivity of anti dsDNA seems not to be related to clinical manifestations. As for pathogenesis, the accumulation of nuclear debris (nucleosomes) from apoptotic cells could promote autoantibody production; however, inhibition of cytotoxic T cells by anti-TNF-α therapy reduce the elimination of autoantibody-producing B cells with a shift to TH1 to TH2 response. Another paradoxical phenomenon is the disappearance of subacute cutaneous lupus erythematosus by the use of etanercept in several cases. Anti-TNF-α is rarely associated with dermatomyositis that usually causes inflammatory rash and muscle weakness; these symptoms may persist after discontinuation of anti-TNF-α but respond to corticosteroid and immunosuppressive treatments.17 Lichenoid reactions with an interface pattern have been reported and considered as a relevant classeffect.18 Five cases of erythema multiforme, 2 of StevensJohnson syndrome and 1 overlap during anti-tumor necrosis factor treatment for plaque psoriasis have been described.19 The Stevens-Johnson syndrome, when associated with adalimumab administration can show severe mucositis, peripheral rash, desquamation, and concomitant fever; these manifestations are characterized by high morbidity and mortality and can respond to intravenous hydrocortisone.20 This is another paradoxical phenomenon as resolution of toxic epidermal necrolysis with anti-TNFa treatment is found in the literature.21 Lupus erythematosus and interface disorders Leukocytoclastic vasculitis is the most frequent type of vasculitis, and purpura is the most frequent cutaneous lesion associated with anti-TNF-a agents; vasculitis, moreover, can be associated also with an extracutaneous implication in one-quarter of patients, especially renal involvement.22 Infliximab and etanercept are more involved than adalimumab. The anti-TNF-α and especially infliximab induce the development of systemic lupus erythematosus (SLE) and can also worsen a pre-existent discoid lupus erythematosus. The disease develops within a few months of starting therapy but also after 4 years. Infliximab is implicated in 37% of cases, etanercept in 33% and adalimubab in 25%. Women in their fifth decade of life are more involved. Forty-five per cent of cases have “limited cutaneous lupus” (subacute) while more than 50% develop SLE characterized by maculopapular and butterfly rash, alopecia, photosensitivity, hypocomplementemia, fever, renal disease and high prevalence of antinuclear antibodies and Vol. 149 - No. 3 Vasculitis Granulomatous dermatitis Granulomatous dermatitis has also been associated with anti-TNF-a inhibitors, especially etanercept and mostly considered as cases of sarcoid-like granulomatosis or complete sarcoidosis with pulmonary and cutaneous involvement.23 This is intriguing GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 313 RONGIOLETTI INFLAMMATORY SIDE EFFECTS OF BIOLOGICS IN PATIENTS WITH PSORIASIS because TNF-α antibody drugs have also been used successfully to treat sarcoidosis. The incidence is estimated in ~1/2800. Dermatological patients may present with nodular lesions, tattoo inflammation and erythema nodosum. The mean delay between induction therapy and the development of the disease is 12 months. It seems that anti TNF treatment enhances the level of triggering infectious antigens and/or modifies the cytokine environment. Anecdotal cases of interstitial granulomatous dermatitis associated with the use of TNF-a inhibitors have been described.24 Paradoxically, also in this setting, additional casesof interstitial granulomatous dermatitis have been successfully treated with etanercept.25 Eczematous reactions Eczematous reactions have been diagnosed as dyshidrotic, contact, nummular, atopic, papular, and nonspecific eczema. Histopathology showed a spongiotic dermatitis and rarely a mild psoriasiform dermatitis with additional keratinocyte necrosis. Discontinuation of therapy led to remission and recurrence occurred when the biological drug was restarted. Treatment consisted mostly of topical steroids.26 Alopecia Non cicatricial alopecia, usually presenting as alopecia areata-like reaction occurring 2-24 months after starting therapy with anti-TNF have been described as a significant association. This adverse drug reaction appears to be a class effect as all TNF-a inhibitors including also certolizumab have been considered as culprit.27 Anti-TNF-a may induce also psoriasiform eruptions with severe scalp involvement and alopecia. Histopathology revealed epidermal psoriasiform changes and dermal infiltrate with plasma cells and eosinophils.28 Remission of alopecia areata was observed after stopping therapy as well as with continued treatment with biological drugs. Topical steroids seems to improve alopecia. However, psoriasiform alopecia may evolve into a cicatricial form. Bullous diseases Anecdotal cases of autoimmune bullous diseases such pemphigoid and pemphigus have been described with anti TNF-a inhibitors 29 as well as cases of multiple lesions of focal cutaneous mucinosis,30 314 pseudolymphomatous reactions,31 morphea,32 vitiligo 33 and neutrophilic dermatoses (neutrophilic eccrine hidradenitis-like and Sweet’s-like syndrome).34 Cutaneous infections A review of the German register for use of biologics in rheumatoid arthritis found a cutaneous infection rate of 7.2% with TNF blockade therapy. The spectrum of cutaneous infectious is quite variable, depending on the type of TNF-α blocker used and include bacterial, viral, fungal and protozoan infections. Thus, in a prospective study in patients affected by rheumatoid arthritis that analyzed the incidence and type of skin side effects associated with anti-TNF, the most frequent were cutaneous infections.35 The most frequently associated skin condition is bacterial cellulitis, erysipelas and abscess formation occurring in less than 0.1% to 7% of patients with TNF inhibition followed by infection with herpes simplex and herpes zoster seen in 0.8% to less than 5% of TNFinhibited patients. Cutaneous fungal infections are found from 1% to 6.9% of patients. Skin infections are also the second most common infection seen in patients receiving anti-TNF therapy accounting for 21% of all infections, only preceded by the respiratory tract infections. Since TNF-α is a proinflammatory cytokine that plays an important role in innate immunity and protection against bacterial, viral and parasitic diseases, it is likely that its inhibition may increase the risk of infection, especially at the levels of skin and soft tissues compared with other areas.16 Additional skin infections that has been linked to anti TNF-a includes folliculitis, pytiriasis versicolor, and granulomatous infectious diseases (tuberculosis, histoplasmosis, leshmaniasis and nontuberculous mycobacteria).36 In relation to the type of anti-TNF drugs related to the development of infection, infliximab has been shown to be associated with higher incidence of skin infection than other drugs.37 Overview of cutaneous adverse events related to il-12/23 antagonist (ustekinumab) Ustekinumab is a human monoclonal antibody that binds to the shared p40 subunit of IL-12 and IL-23. Since the drug is on the market for less time than anti-TNF-a inhibitors, data on its side effects are less evident. However, it has been implicated in GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 INFLAMMATORY SIDE EFFECTS OF BIOLOGICS IN PATIENTS WITH PSORIASIS similar skin reaction as anti-TNF-a such as injection site erythema that seems the most frequent side effect, psoriasiform eruptions including pustular and arthritic flares, alopecia areata, autoimmune bullous diseases such as linear IgA dermatitis, eczematous drug reactions, pseudolymphomatous reactions.38-43 RONGIOLETTI Ustekinumab (9 patients) No inflammatory/infectious skin adverse reaction has been observed. One patient with only cutaneous psoriasis developed a severe arthritis. Conclusions Personal experience We have treated 109 psoriatic patients with biologics at the DISSAL, Section of Dermatology, University of Genoa from 2006 to 2013. Forty-six patients have been treated with etanercept, 33 with adalimumab, 16 with infliximab, 9 with ustekinumab and 4 with golimumab. Side effects have been divided into serious (leading to ceasing the therapy) and slight reactions (therapy has been maintained and patients have been accurately monitored). Etanercept (46 patients) We observed seven skin adverse reaction: two serious side effect characterized by one case of recurrent flares of erysipela (3 times in 3 months) and one of purpuric vasculitis and five slight effects including: 1 injection-site reaction, 1 lichenoid reaction, 1 urticaria, 1 cheilitis and 1 alopecia areata. References Infliximab (16 patients) We observed seven infusion reactions with two serious side effects characterized by 2 hypotension, seizures, angioedema; one of the 2 patients showed a subsequent worsening of his psoriasis with the development of a generalized pustular erythrodermic psoriasis. In addition we saw 4 slight infusion reactions. Adalimubab (34 patients) Four slight side effects including 1 injection side reaction, 1 pyodermitis vegetans, 1 alopecia and 1 urticaria have been observed. Golimumab (4 patients) One patient developed a pyoderma gangrenosum of the right flank that resolved after treatment with cyclosporine Vol. 149 - No. 3 As the use of biologics (anti-TNF and anti IL12/23) continues to increase, diagnosis and management of skin adverse reactions will become an important challenge. The overall rates of inflammatory adverse events is more or less similar between the different TNF-a inhibitors. The main difference are referred more to the rates of specific events. Infusion reactions with infliximab and injection site reactions with etanercept and adalimubab are the most common side effects. Although an increased incidence of infections with the use of TNF-a inhibitors has been reported, we could not confirm these data. Curiously, IL12/23 inhibitor ustekinumab is associated with similar skin side effects than TNF-a inhibitors. Discontinuation of the anti-TNF-α treatment should be evaluated on individual basis. A greater number of patients treated with longer courses of therapy, coupled with careful observations and reporting, will better define risks and benefits of biologic agents. 1. Menter A, Gottlieb A, Feldman SR, Van Voorhees AS et al. Guidelines of care for the management of psoriasis and psoriatic arthritis: Section 1. Overview of psoriasis and guidelines of care for the treatment of psoriasis with biologics. J Am Acad Dermatol 2008;58:82650. 2. Moustou AE, et al. Cutaneous side effects of anti-tumor necrosis factor biologic therapy: a clinical review. J Am Acad Dermatol 2009;61:486-504. 3. Nagy G, Lukács K, Sziray A, Fazekas K, Florián A, Tamási L, Károlyi Z. Adverse events during biological therapy - focusing on dermatological side-effects. Orv Hetil 2011;152:212-20. 4. Lequerrè T, Vittecoq O, Klemmer N, Goeb V, Pouplin S, Menard JF et al. Management of infusion reaction to infliximab in patients with rheumatoid arthritis orspondyloarthritis: experience from an immunotherapy unit of rheumatology. J Rheumatol 2006;33:1307-14. 5. Paltiel M, Gober LM, Deng A, Mikdashi J, Alexeeva I, Saini SS et al. Immediate type I hypersensitivity response implicated in worsening injection site reactions to adalimumab. Arch Dermatol 2008;144:1190-4. 6. Benucci M, Manfredi M, Demoly P, Campi P. Injection site reactions to TNF-a blocking agents with positive skin tests. Allergy 2008;63:138-9. 7. Zidi I, Bartegi A, Ben AN. Dermatologic adverse events: golimumab, friend or foe? Pharmazie 2011;66:5-10. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 315 RONGIOLETTI INFLAMMATORY SIDE EFFECTS OF BIOLOGICS IN PATIENTS WITH PSORIASIS 8. Borchers AT, Leibushor N, Cheema GS, Naguwa SM, Gershwin ME. Immune-mediated adverse effects of biologicals used in the treatment of rheumatic diseases. Autoimmun 2011;37:273-88. 101. 9. de Gannes GC, Ghoreishi M, Pope J, Russell A, Bell D, Adams S et al. Psoriasis and pustular dermatitis triggered by TNF-{a} inhibitors in patients with rheumatologic conditions. Arch Dermatol 2007;143:223-31. 10. Wollina U, Hansel G, Koch A, Schönlebe J, Köstler E, Haroske G. Tumor necrosis factor-a inhibitor-induced psoriasis or psoriasiform exanthemata: first 120 cases from the literature including a series of six new patients. Am J Clin Dermatol 2008;9:1-14. 11. Joyau C, Veyrac G, Dixneuf V, Jolliet P. Anti-tumour necrosis factor a therapy and increased risk of de novo psoriasis: is it really a paradoxical side effect? Clin Exp Rheumatol 2012;30:700-6. 12. Shmidt E, Wetter DA, Ferguson SB, Pittelkow MR. Psoriasis and palmoplantar pustulosis associated with tumor necrosis factor-α inhibitors: The Mayo Clinic experience, 1998 to 2010. J Am Acad Dermato 2012;67:e179-85. 13. Palucka AK, Blanck JP, Bennett L, Pascual V, Banchereau J. Crossregulation of TNF and IFN-a in autoimmune diseases. Proc Natl Acad Sci USA 2005;1:3372-7. 14. De Bandt M, Sibilia J, Le Loët X, Prouzeau S, Fautrel B, Marcelli C et al. Systemic lupus erythematosus induced by anti-tumor necrosis factor a therapy: a French national survey. Arthritis Res 2005;7:545-51. 15. Costa MF, Said NR, Zimmermann B. Drug-induced lupus due to anti-tumor necrosis factor a agents. Semin Arthritis Rheum 2008;37:381-7. 16. Levine D, Switlyk SA, Gottlieb A. Cutaneous lupus erythematosus and anti-TNF-a therapy: a case report with review of the literature. J Drugs Dermatol 2010;9:1283-7. 17. Klein R, Rosenbach M, Kim EJ, Kim B, Werth VP, Dunham J. Tumor necrosis factor inhibitor-associated dermatomyositis. Arch Dermatol 2010;146:780-4. 18. Garcovich S, Burlando M, Rongioletti F, Garcovich A, Parodi A, Amerio P. Cutaneous drug eruption with an interface dermatitis pattern due to anti-tumour necrosis factor-a agents: a relevant classeffect. Acta Derm Venereol 2010;90:311-2. 19. Ahdout J, Haley JC, Chiu MW. Erythema multiforme during antitumor necrosis factor treatment for plaque psoriasis. Am Acad Dermatol 2010;62:874-9. 20. Mounach A, Rezqi A, Nouijai A, Ghozlani I, Achemlal L, Maghraoui AE et al. Stevens-Johnson syndrome complicating adalimumab therapy in rheumatoid arthritis disease. Rheumatoll Int 2013;33:1351-3. 21. Hunger RE, Hunziker T, Buettiker U, Braathen LR, Yawalkar N. Rapid resolution of toxic epidermal necrolysis with anti-TNF-a treatment. Allergy Clin Immunol 2005;116:923-4. 22. Ramos-Casals M, Brito-Zerón P, Muñoz S, Soria N, Galiana D, Bertolaccini L et al. Autoimmune diseases induced by TNFtargeted therapies: analysis of 233 cases. Medicine (Baltimore) 2007;86:242-51. 23. Skoie IM, Wildhagen K, Omdal R. Development of sarcoidosis following etanercept treatment: a report of three cases. Int 2012;32:1049-53. 24. Deng A, Harvey V, Sina B, Strobel D, Badros A, Junkins-Hopkins JM et al. Interstitial granulomatous dermatitis associated with the use of tumor necrosis factor a inhibitors. Arch Dermatol 2006;142:198-202. 25. Ahmed ZS, Joad S, Singh M, Bandagi SS. Interstitial granuloma- 316 tous dermatitis successfully treated with etanercept. Am J Case Rep 2014;15:94-6. 26. Bonnet N, Guis S, Koeppel MC, Roudier J, Grimaud JC, Jean-Pastor MJ, Berbis P. Cutaneous events during anti-TNF a therapy: a prospective observational study of 41 cases. Ann Dermatol Venereol 2010;137:12-20. 27. Bene J, Moulis G, Auffret M. Alopecia induced by tumour necrosis factor-a antagonists: description of 52 cases and disproportionality analysis in a nationwide pharmacovigilance database. Rheumatology (Oxford) 2014 [Epub ahead of print]. 28. Doyle LA, Sperling LC, Baksh S, Psoriatic alopecia/alopecia areata-like reactions secondary to anti-tumor necrosis factor-α therapy: a novel cause of noncicatricial alopecia. Am J Dermatopathol 2011;33:161-6. 29. Boussemart L, Jacobelli S, Batteux F, Goulvestre C, Grange P, Carlotti A et al. Autoimmune bullous skin diseases occurring under anti-tumor necrosis factor therapy: two case reports. Dermatology 2010;221:201-5. 30. Duparc A, Gosset P, Lasek A, Modiano P. [Multiple lesions of focal cutaneous mucinosis: a side-effect of anti-TNF a therapy?]. Ann Dermatol Venereol 2010;137:140-2. 31. Guis S, Schiano de Colella JM, Bonnet N, Andrac-Meyer L, Balandraud N, Mattei JP et al. Cutaneous pseudolymphoma associated with a TNF-a inhibitor treatment: etanercept. J Dermatol 2008;18:474-6. 32. Stewart FA, Gavino AC, Elewski BE. New side effect of TNF-a inhibitors: morphea. Skinmed 2013;11:59-60. 33. Maruthappu T, Leandro M, Morris SD. Deterioration of vitiligo and new onset of halo naevi observed in two patients receiving adalimumab. Dermatol Ther 2013;26:370-2. 34. Hryluk EB, Linskey KR, Duncan LM, Nazarian RM. Broad range of adverse cutaneous eruptions in patients on TNF-a antagonists. J Cutan Pathol 2012;39:481-92. 35. Gottlieb AB, Kerbleski JF. Cutaneous infections Dermatological complications and safety of anti-TNF treatments. Gut 2009;58:10339. 36. Laquer V, Ta T, Nguyen T, Tan B. Mycobacterium porferae infection in a psoriasis patient on anti-TNF-α therapy. Dermatol Online J 2013;19:196-209. 37. Hernández MV, Meineri M, Sanmartí R. Skin lesions and treatment with tumor necrosis factor a antagonists. Reumatol Clin 2013;09:53-61. 38. Stamell EF, Kutner A, Viola K, Cohen SR. Ustekinumab associated with flares of psoriatic arthritis. JAMA Dermatol 2013;149:1410-3. 39. Wenk KS, Claros JM, Ehrlich A. Flare of pustular psoriasis after initiating ustekinumab therapy.J Dermatolog Treat 2012;23:212-4. 40. Verros C, Rallis E, Crowe M. Alopecia areata during ustekinumab administration: Co-existence or an adverse reaction? Dermatol Online J 2012;18:14. 41. Becker JG, Mundi JP, Newlove T, Mones J, Shupack J. Development of linear IgA bullous dermatosis in a patient with psoriasis taking ustekinumab. J Am Acad Dermatol 2012;67:e150-1. 42. Jung J, Levin EC, Jarrett R, Lu D, Mann C. Lymphomatoid drug reaction to ustekinumab. Arch Dermatol 2011;147:992. 43. Pernet C, Guillot B, Bessis D. Eczematous drug eruption after ustekinumab treatment. Arch Dermatol 2012;148:959-6. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 G ITAL DERMATOL VENEREOL 2014;149:317-27 Tyrosine kinase inhibitors: muco-cutaneous side effects at the microscope V. GRASSO 1, C. VASSALLO 1, G. CROCI 2, V. BRAZZELLI 1 In the past recent years, treatments that target receptors with kinase activity, involved in the transmission of neoplastic proliferation signals, had revolutionized cancer therapy. Imatinib mesylate has been the first of this novel family of drugs approved for the treatment of hematologic malignancies. Afterwards, other second-generation kinase inhibitors, such as dasatinib and nilotinib, have been introduced to circumvent resistance to imatinib. These target therapies have a better tolerability profile than standard chemotherapy, but their range of activity is not simply directed at tumor cells, and a wide spectrum of systemic side effects is now recognized. In particular, muco-cutaneous side effects represent the most frequent non-hematological adverse events. Due to the need of a prompt recognition of these toxicities, diagnosis is usually made on clinical grounds, and an accurate histological characterization is generally lacking. The aim of this paper was to focus on the histopathological findings of cutaneous reactions related to tyrosine kinase inhibitors use. We propose a differentiation between specific and non-specific cutaneous side effects, through an analysis of the possible etiopathogenetic mechanisms of actions of the drug, clinical aspects and major histological features. A review of the literature has been integrated by our personal experience, highlighting the importance of clinico-histological correlation, necessary to make a proper diagnosis. Key words: Chemotherapy - Cancer - Regional perfusion Skin diseases - Exanthema. C ancer chemotherapy has been one of the major medical advances in the last few decades, and the field of targeted therapies, small molecule drugs directed against cancer-specific signalling pathways, Corresponding author: V. Brazzelli, Department of Clinical-Surgical, Diagnostic and Pediatric Sciences, Institute of Dermatology, Fondazione IRCCS Policlinico San Matteo, 27100 Pavia, Italy. E-mail: [email protected] Vol. 149 - No. 3 1Department of Clinical-Surgical, Diagnostic and Pediatric Sciences Institute of Dermatology, University of Pavia and Foundation IRCCS Policlinico San Matteo Pavia, Italy 2Department of Human Pathology, University of Pavia and Foundation IRCCS Policlinico San Matteo Pavia, Italy marked a turning point in terms of therapeutic responses and allowed to increase the selectivity of drug action and limit systemic side-effects. Tyrosine kinase inhibitors (TKIs) block the ATPbinding site and autophosphorylation of the tyrosine residues of several proto-oncogenes. This mechanism finally inhibits the activation of intracellular signal-transduction pathways in tumour cells, responsible for deregulation of key cell functions such as proliferation and differentiation.1-5 The first-generation TKI was imatinib mesylate (Gleevec®, STI571), approved for the treatment of chronic myeloid leukemia (CML) and gastrointestinal stromal tumours (GISTs).6 The development of polyclonal resistance to imatinib gave birth to a second generation of multikinase inhibitors, dasatinib (Sprycel®, BMS-354825) and nilotinib (Tasigna®, AMN107).7-14 Today, these drugs can be used up front in newly diagnosed patients and the registration of new TKIs is proceeding remarkably fast.5, 15 The availability of highly potent TKIs has really broadened the treatment armamentarium in cancer therapy and frequent updates are mandatory for the physicians treating oncologic patients and for those GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 317 GRASSO Tyrosine kinase inhibitors dealing with systemic adverse events related to their employ. During the last years, growing attention has been paid to tolerance and toxicity profiles of these new drugs. In particular, cutaneous reactions are one of the most commonly reported adverse events associated with TKIs administration, being mostly mild to moderate in severity and often transient and self-limiting, even if severe life-threatening reactions have been described.16-18 The heterogeneity of reactions to TKIs proves that these drugs exert different effects on the skin, but much remains to be elucidated about their pathophysiology. Considering our personal experience and the most relevant papers in the literature, we can support the concept of differentiation between specific mucocutaneous side effects, since a drug-related pathogenetic mechanism of action or peculiar clinical and histopathological findings may be recognised, and non-specific adverse events, whose clinico-histological features and biological activity of the drug are unlikely to be related. Despite the high incidence of cutaneous side effects reported in several clinical trials, an accurate diagnostic investigation and categorization has never been carried out, because diagnosis is often made on clinical grounds alone. Nevertheless, a cutaneous biopsy and histopathological examination are necessary to make a precise diagnosis and offer a dermatological in-depth analysis in terms of biological activity of the drug, pathogenesis of a particular side effect and need for therapy. In this paper, we review the most frequent specific and non-specific muco-cutaneous side effects associated to the use of first- and second-generation TKIs, focusing on the histologic findings and highlighting the importance of the integration of both clinical and histopathologic data to make a proper diagnosis. Specific muco-cutaneous side effects Hypopigmentation and hyperpigmentation Many case reports evidenced the occurrence of pigmentary changes during TKIs treatment.19-21 Clinically, they appear with localized hypopigmented patches (Figure 1), or with diffuse depigmentation of the skin. Hair depigmentation may present as well. 318 Figure 1.—Clinical findings of vitiligo-like hypopigmented patches with irregular and undefined borders on the back, in a 44year-old female patient with CML treated with imatinib. Other similar lesions were present on the legs and arms, and appeared two months after the beginning of the therapy. In the center of the hypochromic patch, a small scar corresponding to the skin biopsy is evident. In a study conducted by Arora et al., depigmentation appeared in 41% of 118 patients treated with imatinib, and the median time of onset was four weeks.22 We reported the development of vitiligo-like lesions and generalized lightening of the skin in a pediatric patient treated with imatinib, assessing the skin colour changes by means of a colorimetric measurement over a period of four months.23 We also described the case of another pediatric patient treated with dasatinib, who developed achromic patches on his neck and the dorsal surfaces of his hands, and GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Tyrosine kinase inhibitors GRASSO Photoinduced dermatoses Figure 2.—Histopathological features of vitiligo-like hypopigmentation, showing irregular epidermal hyperplasia, with absence of melanocytes in the basal layer. Scanty perivascular inflammatory infiltrates are detectable in the superficial dermis. The reduction of melanocytes has been confirmed by S100 staining (Hematoxylin&Eosin, x20). complete depigmentation of his hair, eyelashes and eyebrows.24 The cases described emphasize the role of the c-kit pathway in melanocyte biology. TKIs-induced skin depigmentation is thought to be caused by blockade of c-kit signalling, which may occur via direct inhibition of c-kit mediated gene activation.25-28 The link between the c-kit receptor and melanogenic genes probably occurs through the microphtalmia transcription factor (MITF), which is crucial for melanocyte development.29 A clue to histological diagnosis includes a reduction or complete absence of melanocytes in association with a partial or total loss of epidermal pigmentation. Superficial perivascular and perifollicular lymphocytic infiltrates are generally absent (Figure 2). Paradoxically, the same drug can induce darkening of the skin and hyperpigmentation, though less frequently. Etienne et al. reported hair repigmentation in 9 of 133 patients and Valeyrie et al. in 8 of 54 patients treated with imatinib.19, 30 How the same drug can induce two opposite cutaneous adverse events remains unclear, and further studies on TKIs effects on the c-kit-transduced signal and regulation of MITF will help to explain the complex molecular mechanisms involved in melanocyte differentiation. Vol. 149 - No. 3 Photosensitization and photoinduced dermatoses most likely represent specific TKIs-related cutaneous adverse reactions. Rousselot and colleagues described 8 cases of photosensitization in patients receiving imatinib therapy. Sunburn intensity varied from painless to painful erythema, limited to exposed skin.31 The photosensitivity risk related to genetic polymorphisms of human ATP-binding cassette (ABC) transporter ABCG and its inhibition by drugs have been studied in vitro. Imatinib can inhibit the ATPbinding cassette subfamily G member 2 (ABCG2)mediated porphyrin transport inducing a significant enhancement of the cellular photosensitivity through the disruption of porphyrin homeostasis. It can be hypothesized that certain genetic polymorphisms and/or inhibition of ABCG2 by imatinib can increase the potential risk of drug-induced phototoxicity.32, 33 Like imatinib, both nilotinib and dasatinib decreased ABCG2 surface expression, supporting the hypothesis that all three TKIs are substrates of ABC transporters and that, at higher concentrations, TKIs overcome transporter function.34 At the same time, skin protection against ultraviolet rays is altered because of the impaired melanogenesis induced by TKIs via an inhibition of c-kit activity. We studied two patients who presented with photoinduced erythematous eruption limited to photoexposed areas during imatinib treatment (Figure 3).35 In both cases, histopathological examination revealed Figure 3.—Clinical presentation of photoinduced rash in sun-exposed area in a 52-year-old female patient with CML and receiving imatinib. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 319 GRASSO Tyrosine kinase inhibitors Figure 5.—Tense bullae, erosions and crusts on erythematous background after four months of imatinib therapy in a 45-yearold male patient affected by CML. Other similar lesions were evident in photo-exposed areas of both forearms, highly suggestive of pseudoporphyria. Figure 4.—Histopathological features of photoinduced dermatitis, showing interface dermatitis with scattered necrotic keratinocytes, focal exocytosis, perivascular inflammatory infiltrates in the superficial dermis and vasodilation of capillaries and venules (Hematoxylin&Eosin, x10). interface dermatitis, scattered necrotic keratinocytes, focal exocytosis, perivascular inflammatory infiltrates in the superficial dermis composed by lymphocytes and scattered eosinophils, and mild dermal elastosis. Vasodilation of superficial capillaries and venules was evident between collagen bundles (Figure 4). The appearance of such a cutaneous side effect may be attributed to the biological activity of the drug. Pseudoporphyria Imatinib has been also reported to induce pseudoporphyria. In a case report, the patient developed tense, sometimes hemorrhagic blisters without surrounding erythema on the dorsa of the hands and ankles. Histology of a biopsy taken from a blister showed a subepidermal bulla, along with dermal 320 edema and a scant lymphohistiocytic perivascular infiltrate with sporadic eosinophils. Type IV collagen was found to be localized to the floor of the blister. A subsequent biopsy of peribullous skin showed slightly thickened upper vessel walls with some amorphous eosinophilic material; moreover, a duplication of the basal membrane with type IV collagen stain was seen, without PAS positivity.36, 37 We studied a patient with a history of skin fragility aggravated by photoexposition, appeared during imatinib therapy. On clinical examination, widespread erosions and crusted lesions on erythematous background located on the dorsal surface of both hands and forearms were evident (Figure 5). Porphyrin metabolism abnormalities were not detected. Histologic features were characterized by a subepidermal blister with dermal papillae protruding in the lumen, scant dermal inflammatory infiltrates (Figure 6), and the presence of diastase-resistant, PAS positive material deposited around capillary vessels with thickened walls (Figure 7), all features consistent with a diagnosis of porphyria cutanea tarda or pseudoporphyria. Recently, Pérez and colleagues described a patient treated with imatinib who developed multiple tense hemorrhagic blisters, erosions, crusts, and scars on both hands. The histological examination revealed GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Tyrosine kinase inhibitors GRASSO Figure 6.—Histological findings of imatinib-induced pseudoporphyria, characterized by cell-poor, subepidermal blister with dermal papillae protruding in the lumen, scant inflammatory infiltrates and dermal elastosis. Thickened vessel walls are evident in the superficial dermis (Hematoxylin&Eosin, x10). Figure 7.—High power view of superficial vessels showing diastase-resistant, PAS positive, homogeneous material deposited around thickened walls (Periodic acid-Schiff, x40). subepidermal vesicles and positive PAS staining of the blood vessel walls.38 As described in true photoinduced dermatoses, similar pathophysiologic mechanisms may be proposed for TKIs-related pseudoporphyria. In particular, the enhanced cellular photosensitivity induced by the alteration of intracellular porphyrin levels may be responsible for the development of this peculiar cutaneous side effect. Pityriasiform eruptions A series of three male patients on imatinib who developed an erythematous macular eruption on the trunk and arms has been reported by some of us.39 The lesions presented a peripheral collarette of desquamation and a vaguely parallel distribution to Langer’s skin lines, suggesting a clinical diagnosis of pityriasis rosea-like drug eruption (Figure 8). Other authors reported similar clinical features as a side effect of imatinib therapy.40, 41 We suggest that this kind of eruption represent a specific drug-related side effect since many histological hallmarks can be recognised. In all specimens, Vol. 149 - No. 3 Figure 8.—Pityriasis rosea-like eruption in a 50-year-old male patient with CML after one month of imatinib treatment. Widespread, monomorphous, slightly pruritic, erythematous patches with a collarette of scales are evident. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 321 GRASSO Tyrosine kinase inhibitors Figure 9.—Histological findings of pytirasis rosea-like eruption include orthokeratotic hyperkeratosis, interface dermatitis with scattered necrotic keratinocytes, focal exocytosis and lymphocytic inflammatory infiltrates in the dermis. A remarkable vasodilation of blood capillaries, venules and lympathic vessels with elongated shapes is detectable (Hematoxylin&Eosin, x10). histological findings included interface dermatitis with scattered necrotic keratinocytes and focal exocytosis, superficial and mid-dermal lymphocytic inflammatory infiltrates with perivascular and periadnexal accentuation (Figure 9). A constant peculiar finding that can be considered a clue for the diagnosis of TKIs-related pityriasiform eruptions, is the presence of a remarkable dilation of lymphatic vessels and blood capillaries. Some of these vessels are telangiectases, and notable perivascular infiltrates without signs of vasculitis may be seen (Figure 10). These histopathological findings may be correlated to the specific drug’s inhibition of growth factors, like platelet-derived growth factor receptor (PDGF-R), a growth factor involved in interstitial fluid homeostasis. This inhibition may lead to an increase in dermal interstitial fluid pressure, through a dysregulation of the tension between endothelial cells and the extracellular matrix. Pasmatzi et al. described a case of disseminated erythematous and pityriasiform plaques with similar histopathological features.42 Psoriasiform eruptions Valeyrie et al. reported a psoriasiform rash localized on the scalp, trunk and arm in 4 of 54 imatinib- 322 Figure 10.—Typical histopathological features of pityriasis rosealike eruption, with interface dermatitis, focal vacuolar changes at the dermo-epidermal junction, superficial lymphocytic inflammatory infiltrates with perivascular accentuation. Dilated superficial vessels with bizarre, elongated shapes and no signs of vasculitis are evident (Hematoxylin&Eosin, x10). treated patients.19 In other reports, the eruption can present with psoriasiform palmoplantar hyperkeratosis.43 Imatinib has been related to psoriasis induction in some patients with CML.44-46 A case of psoriasis vulgaris developing during nilotinib treatment has been recently described.47 Histological examination showed pathological features of psoriasis, including epidermal hyperkeratosis and acanthosis with parakeratosis, and perivascular lymphocytic infiltration in the superficial dermis. The mechanisms underlying psoriasiform eruptions are still unclear. An interference with cytokine production and T cell proliferation induced by the drug could be hypothesized. In particular, TKIs inhibit the function of CD4+ CD25+ regulatory T cells (Treg) and block intracellular signalling of effector T cells, so it is possible that the balance of these effects GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Tyrosine kinase inhibitors GRASSO leads to the development or exacerbation of pre-existing psoriasis.48, 49 Superficial edema Superficial edema is another common cutaneous reactions associated with TKIs, with an incidence of 55.9% reported in the IRIS study.50 It mainly affects the face, especially the periorbital area, but it can also affect the legs. The incidence of peripheral edema varies from 5% to 18% for dasatinib.51, 52 The diagnosis of this cutaneous adverse event is generally made on the basis of clinical aspects, and histological examinations are poorly described. Common histological findings include superficial edema with ectasis of lymphatic and blood vessels, without alteration of endothelial cells, without inflammatory cells. The specific chronic inhibition of PDGF-R and other growth factors may impair pericyte function and lead to weakening of the vessel wall. The same process of vasodilation is found in other TKIs specific side effects, suggesting that this represents a major histological feature and a clue to diagnosis. Non-specific muco-cutaneous side effects Erythematous maculopapular rashes The occurrence of erythematous maculopapular rashes is frequently reported in clinical trials and case series. These rashes are usually labelled as “non-specific” and initially manifest as erythematous macules and papules or erythema alone; they can mimick morbilliform eruptions and may eventually become purpuric or progress to erythroderma. The lesions are generally located on the trunk and proximal segments of arms and tend to be mild and self-limiting. The lower extremities, intertriginous areas, and face are less frequently involved.17, 19 The incidence of erythematous skin rashes associated to imatinib was 33.9% in the IRIS study, 17% in the DASISION study, 22% in the ENESTnd study, and ranging from 19% to 66.7% in the most relevant case series.19, 50, 53-55 Maculopapular eruptions and exfoliative rashes are also the most frequent dasatinib-related cutaneous side effect.51, 52 As concerns Vol. 149 - No. 3 nilotinib, skin rashes are reported with an incidence ranging from 2-20% to 41-47%.12, 54 According to a meta-analysis conducted by Drucker et al., the incidence of all-grade skin rash with nilotinib was 34.3%, higher than with dasatinib, whose incidence was 23.3%.56 Histologically, hyperkeratosis with parakeratosis is generally observed, together with focal spongiosis, discrete lymphocytic exocytosis and necrotic keratinocytes. The papillary dermis shows a variable degree of edema and lympho-histiocytic perivascular infiltrate, with eosinophils and few neutrophils. An irregularity of the dermoepidermal junction with scattered melanophages may also be detected. These findings are consistent with a drug eruption, but not specific for a TKIs-induced skin rash.57, 58 Sometimes, clinical findings are more suggestive for a specific skin rash induced by TKIs, such as the presence of erythematous follicular papules and perifollicular lesions, including lesions resembling keratosis pilaris. The pathogenetic mechanism of rash has thus far not been studied and remains elusive. It may be hypothesized a direct inhibitory effect against other kinases, which are active in the skin. Nevertheless, their inhibition has a putative role in rash development that needs further study. Muco-cutaneous lichenoid eruptions The clinical appearance of muco-cutaneous lichenoid eruptions induced by TKIs can be heterogeneous. The eruption may be mild to extensive, generally characterized by dark purple, pruriginous, lichen planus-like papular lesions. Cases of widespread eruptions with papules and plaques have been described.59-64 Mucosal lesions are less frequent and may be characterized by white plaques with a reticulated pattern, grey-violaceous plaques or reddish macules and erosions.65-67 We studied two cases of oral lichenoid reactions during imatinib therapy. One patient presented white lesions on the oral mucosa and the tongue, characterized by fixed radiating striae.35 The other patient showed white striae on the oral mucosa only (Figure 11). A mucosal biopsy showed acanthosis with mild parakeratosis of the epithelium, vacuolar degeneration of the basal layer, lymphocytic perivascular infiltration of upper dermis and capillary vasodilation (Figure 12). Despite the absence of histological clues, a mild vasodilation is detectable. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 323 GRASSO Tyrosine kinase inhibitors Figure 11.—Clinical findings of lichenoid drug eruption of the oral mucosa characterized by asymptomatic, white fixed striae, in a 55-year-old male patient after three months of imatinib therapy for CML. Kuraishi et al. reviewed fourteen patients with cutaneous lichenoid eruptions due to imatinib, highlighting the fact that these eruptions are clearly doserelated.68 It is proposed that these lesions may be closely correlated with the drug-induced altered expression of epidermal markers and changes in epidermal homeostasis, but the exact pathogenetic mechanism remains unclear. Neutrophilic dermatoses The appearance of neutrophilic dermatoses has been sparsely reported in the literature. Sometimes, the adverse cutaneous reactions have been classified under precise diagnoses; otherwise, they have been simply described as pustular eruptions because of the lack of consistent clinical and histological criteria.69 Ayirookuzhi et al. described a patient who developed an abrupt onset of tender and painful erythematous plaques and nodules on the dorsal aspects of both hands and forearms, preceded by the use of imatinib. The histological examination showed neutrophilic dermatosis with epidermal sparing and intradermal abscess formation involving both the superficial and deep dermis, consistent with Sweet syndrome.70 Two patients with imatinib-induced acute generalized exanthematous pustulosis have been described.71, 72 Both patients exhibited an acute generalized pustular eruption with multiple painful pruritic pustules on an erythematous and edematous 324 Figure 12.—Histopathological features of oral lichenoid drug eruption include acanthosis with mild parakeratosis, focal vacuolar degeneration of the basal layer, lymphocytic perivascular infiltration in the lamina propria and mild capillary vasodilation (Hematoxylin&Eosin, x10). background, beginning in the face and later spreading to the trunk and extremities. The histological examination showed intraepidermal pustules with parakeratosis, interstitial cellular infiltration of neutrophils, exocytosis of abundant eosinophils and apoptotic neutrophils, without signs of vasculitis. A case of neutrophilic eccrine hidradenitis during imatinib treatment has also been reported.73 The patient developed a progressive, erythematous, papular rash most prominent over the medial thighs and volar wrists and also involving the palmoplantar surfaces. A skin biopsy demonstrated necrosis and squamous metaplasia of the eccrine glands and ducts associated with an infiltrate of lymphocytes and neutrophils. Considering the uncommon and heterogeneous presentation of these eruptions, they may not be considered drug-specific and no pathogenetic mechanism has been proposed. Furthermore, the appearance of neutrophilic dermatoses can ben related to the primary hematological disease. Panniculitides Ugurel et al. described a patient treated with imatinib and presenting with recurrent skin lesions characterized by erythematous, swollen and deeply indurated nodules on the upper and lower limbs.74 Biopsy of lesional skin showed a mild, nonspecific mononuclear perivascular infiltrate throughout the GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Tyrosine kinase inhibitors GRASSO dermis. In the subcutaneous tissue, numerous macrophages, neutrophils and lymphocytes were present between the adipocytes throughout the fatty tissue lobules and closely to small blood vessels, without septal involvement. Focal necrotic adipocytes were also detected. The clinical and histopathological data were consistent with a diagnosis of imatinib-induced panniculitis. Even dasatinib can induce similar cutaneous reactions. Two patients presenting with painful subcutaneous nodules with overlying erythema on the lower limbs have been described.75 The histological examination revealed a lobular panniculitis, with massive infiltration by polymorphonuclear leukocytes, without signs of vasculitis. No precise pathogenetic mechanism has been suggested and their uncommon occurrence may justify their categorization as non-specific drug-related adverse events. Other rare cutaneous side effects Clark and colleagues reported a case of mycosis fungoides-like reaction in a patient treated with imatinib.76 On clinical examination, the patient showed a diffuse skin eruption characterized by slightly erythematous and pruritic macules which extended in a centripetal way. A skin biopsy revealed the presence of a mild superficial and mid-perivascular cellular infiltrate consisting of epidermotropic, large, hyperchromatic lymphocytes with focal vacuolar changes of basal keratinocytes and scattered eosinophils. The immunohistochemical studies showed 80% of cells expressing CD3 with approximately equal numbers of CD4+ and CD8+ lymphocytes, supporting the diagnosis of a mycosis fungoides-like reactive infiltrate. In another report, a patient developing a facial eruption characterized by symmetrical, slightly erythematous and indurated plaques after the initiation of imatinib treatment has been described.77 The histological examination showed reticular degeneration of the pilosebaceous follicles with the formation of cystic spaces associated with presence of mucin, and perifollicular infiltrates of mononuclear cells and eosinophils, with slight atypia of some lymphocytes. Immunohistochemistry showed that most of the infiltrating cells were CD3+ and CD4+, CD20- and CD68-, confirming the diagnosis of follicular mucinosis. Plana and colleagues reported a case of pityria- Vol. 149 - No. 3 sis rubra pilaris-like reaction induced by imatinib, characterized by large orange-red plaques with areas of uninvolved skin between them, marked follicular hyperkeratosis and waxy keratoderma on the palms and soles.78 On histological examination, irregular hyperkeratosis with alternating vertical and orthoparakeratosis was seen, and hair follicles with keratinous plugs were also a distinctive feature. Battistella and colleagues reported a case of handfoot syndrome in a patient receiving imatinib.79 Clinically, the patient experienced painful palmoplantar erythema with edema, spreading over the lateral aspects of the feet and dorsal surfaces of the fingers and toes. A skin biopsy showed upper epidermal necrosis and many necrotic keratinocytes of the underlying layers, a moderate inflammatory lymphocytic infiltrate in the papillary dermis and some slight interface dermatitis. Conclusions We analyzed the most frequent muco-cutaneous side effects associated with the employ of first- and second-generation TKIs, with a focus on the histological findings and the need for integration between the clinical and histopathological data in order to make a proper diagnosis. The tolerability profile of first- and second-generation TKIs is overall comparable, but even low-grade side effects affect quality of life and adherence to therapy. In particular, muco-cutaneous side effects represent the most common non-hematological adverse reactions and their great heterogeneity mirrors the different targets of TKIs. The incidence of many cutaneous reactions appears to be related to the cumulative dosage, which further supports a specific pharmacological effect of the drug rather than immunologic or allergic mechanisms. Here, a distinction between specific and non-specific muco-cutaneous adverse events is proposed, considering the pathological mechanisms of action of the drug, the clinical aspects and histological features. Many of these specific cutaneous toxicities may be regarded as potential indicators of responsiveness to therapy, or even direct markers of treatment outcome, because they indicate biological activity. Furthermore, the increasingly specificity of new molecules will emphasize the need for a more accurate categorization of these peculiar cutaneous reactions, GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 325 GRASSO Tyrosine kinase inhibitors considering that specific effects of the drug in the skin are reflected in a broad spectrum of clinico-histological findings. Dermatologists play a central role in recognizing and treating these side effects, and the adaptation of the treatment to the clinical conditions. The timely reporting of severe complication is recommended. References 1. Schlessinger J. Cell signalling by receptor tyrosine kinases. Cell 2000;103:211-225. 2. Krause DS, Van Etten RA. Tyrosine kinases as targets for cancer therapy. N Eng J Med 2005;353:172-187. 3. Arora A, Scholar EM. Role of tyrosine kinase inhibitors in cancer therapy. J Pharmacol Exp Ther 2005;315:971-9. 4. Cross SS. The molecular pathology of new anti-cancer agents. Current Diagnostic Pathology 2005;11:329-39. 5. Baccarani M, Deininger MW, Rosti G, Hochhaus A, Soverini S, Apperley JF et al. European LeukemiaNet raccomendations for the management of chronic myeloid leukemia: 2013. Blood 2013;122:872-4. 6. Guilhot F. Indications for imatinib mesylate therapy and clinical management. Oncologist 2004;9:271-81. 7. Weisberg E, Manley P, Mestan J, Cowan-Jacob S, Ray A, Griffin JD. (AMN107) Nilotinib: a novel and selective inhibitor of BCRABL. Br J Cancer 2006;94:1765-9. 8. Piccaluga PP, Paolini S, Martinelli G. Tyrosine kinase inhibitors for the treatment of Philadelphia chromosome-positive adult acute lymphoblastic leukemia. Cancer 2007;110:1178-86. 9. Talpaz M, Shah NP, Kantarjian HM, Donato N, Nicoll J, Paquette R et al. Dasatinib in imatinib-resistant Philadelphia chromosomepositive leukemias. N Eng J Med 2006;354:2531-41. 10. McCormack PL, Keam SJ. Dasatinib: a review of its use in the treatment of chronic myeloid leukaemia and Philadelphia chromosomepositive acute lymphoblastic leukaemia. Drugs 2011;71:1771-95. 11. Deininger MW. Nilotinib. Clin Cancer Res 2008; 14:4027-31. 12. Kantarjian HM, Giles F, Wunderle L, Bhalla K, O’Brien S, Wassmann B et al. Nilotinib in imatinib-resistant CML and Philadelphia chromosome-positive ALL. N Eng J Med 2006;354:2542-51. 13. Kantarjian HM, Giles F, Gattermann N, Bhalla K, Alimena G, Palandri F et al. Nilotinib (formerly AMN107), a highly selective BCR-ABL tyrosine kinase inhibitor, is effective in patients with Philadelphia chromosome-positive chronic myelogenous leukemia in chronic phase following imatinib resistance and intolerance. Blood 2007;110:3540-6. 14. Signorovitch J, Ayyagari R, Reichmann WM, Wu EQ, Chen L. Major molecular response during the first year of dasatinib, imatinib or nilotinib treatment for newly diagnosed chronic myeloid leukemia: a network meta-analysis. Cancer Treat Rev 2014;40:285-92. 15. O’Brien S, Berman E, Borghaei H, Deangelo DJ, Devetten MP, Devine S et al. NCCN clinical practice guideline in oncology: chronic myelogenous leukemia. J Natl Compr Canc Netw 2009;7:984-1023. 16. Brazzelli V, Grasso V, Borroni G. Imatinib, dasatinib and nilotinib: a review of adverse cutaneous reactions with emphasis on our clinical experience: J Eur Acad Dermatol Venereol 2013;27:1471-80. 17. Amitay-Laish I, Stemmer SM, Lacouture ME. Adverse cutaneous reactions secondary to tyrosine kinase inhibitors including imatinib mesylate, nilotinib, and dasatinib. Dermatol Ther 2011;24:386-95. 18. Faye E, Bondon-Guitton E, Olivier-Abbal P, Montastruc JL; French Network of Regional Pharmacovigilance Centers. Spontaneous reporting of serious cutaneous reactions with protein kinase inhibitors. Eur J Clin Pharmacol 2013;69:1819-26. 326 19. Valeyrie L, Bastuji-Garin S, Revuz J, Bachot N, Wechsler J, Berthaud P et al. Adverse cutaneous reactions to imatinib (STI-571) in Philadelphia chromosome positive leukemias: a prospective study of 54 patients. J Am Acad Dermatol 2003;48:201-6. 20. Basso FG, Boer CC, Corrėa ME, Torrezan M, Cintra ML, De Magalhães MH et al. Skin and oral lesions associated to imatinib mesylate therapy. Support Care Cancer 2009;17:465-8. 21. Tsao AS, Kantarjian HM, Cortes J, O’Brien S, Talpaz M. Imatinib mesylate causes hypopigmentation in the skin. Cancer 2003;98:2483-7. 22. Arora B, Kumar L, Sharma A, Wadhwa J, Kochupillai V. Pigmentary changes in chronic myeloid leukemia patients treated with imatinib mesylate. Ann Oncol 2004;15:358-9. 23. Brazzelli V, Roveda E, Prestinari F, Barbagallo T, Bellani E, Trevisan V et al. Vitiligo-like lesions and diffuse lightening of the skin in a pediatric patient treated with imatinib mesylate: a non-invasive colorimetric assessment. Pediatr Dermatol 2006;23:175-8. 24. Brazzelli V, Grasso V, Barbaccia V, Manna G, Rivetti N, Zecca M et al. Hair depigmentation and vitiligo-like lesions in a leukaemic pediatric patients during chemotherapy with dasatinib. Acta Derm Venereol 2012;92:218-9. 25.Yoshida H, Kunisada T, Grimm T, Nishimura EK, Nishioka E, Nishikawa SI. Review: melanocyte migration and survival controlled by SCF/c-kit expression. J Investig Dermatol Symp Proc 2001;6:1-5. 26. Botchkareva NV, Khlgatian M, Longley BJ, Botchkarev VA, Gilchrest BA. SCF/c-kit signalling is required for cyclic regeneration of the air pigmentation unit. FASEB J 2001;15:645-58. 27. Wehrle-Haller B. The role of Kit-ligand in melanocyte development and epidermal homeostasis. Pigment Cell Res 2003;16:287-96. 28. Cario-Andre M, Ardilouze L, Pain C, Gauthier Y, Mahon FX, Taieb A. Imatinib mesylate inhibits melanogenesis in vitro. Br J Dermatol 2006;155:493-4. 29.Hemesath TJ, Price ER, Takemoto C Badalian T, Fisher DE. MAP kinase links the transcription factor microphtalmia to c-Kit signalling in melanocytes. Nature 1998;391:298-301. 30. Etienne G, Cony-Makhoul P, Mahon FX. Imatinib mesylate and gray hair. N Eng J Med 2002;347:446. 31. Rousselot P, Larghero J, Raffoux E, Calvo F, Tulliez M, Giraudier S et al. Photosensitization in chronic myelogenous leukemia patients treated with imatinib mesylate. Br J Haematol 2003;120:1091-2. 32. Tamura A, Onishi Y, An R, Koshiba S, Wakabayashi K, Hoshijima K et al. In vitro evaluation of photosensitivity risk related to genetic polymorphisms of human ABC transporter ABCG2 and inhibition by drugs. Drug Metab Pharmacokinet 2007;22:428-40. 33. Tamura A, An R, Hagiya Y, Hoshijima K, Yoshida T, Mikuriya K et al. Drug-induced phototoxicity evoked by inhibition of human ABC transporter ABCG2: development of in vitro high-speed screening systems. Expert Opin Drug Metab Toxicol 2008;4:255-72. 34. Dohse M, Scharenberg C, Shukla S, Robey RW, Volkmann T, Deeken JF et al. Comparison of ATP-binding cassette transporter interactions with the tyrosine kinase inhibitors imatinib, nilotinib and dasatinib. Drug Metab Dispos 2010;38:1371-80. 35. Brazzelli V, Muzio F, Manna G, Moggio E, Vassallo C, Orlandi E et al. Photoinduced dermatitis and oral lichenoid reaction in a chronic myeloid leukemia patient treated with imatinib mesylate. Photodermatol Photoimmnuol Photomed 2012;28:2-5. 36. Timmer-de Mik L, Kardaun SH, Kramer MH, Hayes DP, Bousema MT. Imatinib-induced pseudoporphyria. Clin Exp Dermatol 2009;34:705-7. 37. Berghoff AT, English JC 3rd. Imatinib mesylate-induced pseudoporphyria. J Am Acad Dermatol 2010;63:14-6. 38. Pérez NO, Esturo SV, Vialdomiu Edel A, Moreno AJ, Valls AT. Pseudoporphyria induced by imatinib mesylate. Int J Dermatol 2014;53:143-4. 39. Brazzelli V, Prestinari F, Roveda E, Barbagallo T, Bellani E, Vassallo C et al. Pityriasis rosea-like eruption during treatment with GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Tyrosine kinase inhibitors GRASSO imatinib mesylate: description of three cases. J Am Acad Dermatol 2005;53:S240-3. 40. Cho AY, Kim DH, Im M, Lee Y, Seo YJ, Lee JH. Pityriasis rosealike drug eruption induced by imatinib mesylate. Ann Dermatol 2011;23:S360-3. 41. Konstantopoulos K, Papadogianni A, Dimopoulou M, Kourelis C, Meletis J. Pityriasis rosea associated with imatinib (STI571, Gleevec). Dermatology 2002;205:172-3. 42. Pasmatzi E, Monastirli A, Matsouka P, Tsambaos D. Disseminated erythematous and pityriasiform plaques caused by imatinib mesylate. Acta Derm Venereol 2003;83:391-2. 43. Deguchi N, Kawamura T, Shimizu A, Kitamura R, Yanagi M, Shibagaki N et al. Imatinib mesylate causes palmo-plantar hyperkeratosis and nail dystrophy in three patients with chronic myeloid leukemia. Br J Dermatol 2006;154:1216-8. 44. Woo SM, Huh CH, Park KC, Youn SW. Exacerbation of psoriasis in chronic myelogenous leukemia patient treated with imatinib. J Dermatol 2007;34:724-6. 45. Dickens E, Lewis F, Bienz N. Imatinib: a designer drug, another cutaneous complication. Clin Exp Dermatol 2009;34:603-4. 46. Atalay F, Kizilkiliç E, Ada RS. Imatinib-induced psoriasis. Turk J Haematol 2013;30:216-8. 47. Nagai T, Karakawa M, Komine M, Muroi K, Ohtsuki M, Ozawa K. Development of psoriasis in a patient with chronic myelogenous leukemia during nilotinib treatment. Eur J Haematol 2013;91:270-2. 48. Tachil J. T-regulatory cell response in psoriasis and changes with imatinib therapy. Clin Exp Dermatol 2009;34:e1022. 49. Larmonier N, Janikashvili N, LaCasse CJ, Larmonier CB, Cantrell J, Situ E et al. Imatinib mesylate inhibits CD4+ CD25+ regulatory T cell activity and enhances active immunotherapy against BCRABL-tumors. J Immunol 2008;181:6955-63. 50. O’Brien SG, Guilhot F, Larson RA, Gathmann I, Baccarani M, Cervantes F et al. Imatinib compared with interferon and low-dose cytarabine for newly diagnosed chronic-phase chronic myeloid leukemia. N Engl J Med 2003;348:994-1004. 51. Shah NP, Kim DW, Kantarjian HM. Dasatinib 50 mg or 70 mg BID compared to 100 mg or 140 mg QD in patients with CML in chronic phase (CP) who are resistant or intolerant to imatinib: one-year results of CA180034. J Clin Oncol [ASCO Annual Meeting Proceeding Part I (June 20 Supplement)] 20007;25:Abstract 7004. 52.Hochhaus A, Kantarjian HM, Baccarani M, Lipton JH, Apperley F, Druker BJ et al. Dasatinib induces notable hematologic and cytogenetic responses in chronic-phase chronic myeloid leukemia after failure of imatinib therapy. Blood 2007;109:2303-9. 53. Kantarjian HM, Shah NP, Cortes JE, Baccarani M, Agarwal MB, Undurraga MS et al. Dasatinib or imatinib in newly diagnosed chronic-phase chronic myeloid leukemia: 2-year follow-up from a randomized phase 3 trial (DASISION). Blood 2012;119:1123-9. 54. Kantarjian HM, Hochhaus A, Saglio G, De Souza C, Flinn IW, Stenke L et al. Nilotinib versus imatinib for the treatment of patients with newly diagnosed chronic phase, Philadelphia chromosome-positive, chronic myeloid leukaemia: 24-month minimum follow-up of the phase 3 randomised ENESTnd trial. Lancet Oncol 2011;12:841-51. 55. Druker BJ, Talpaz M, Resta DJ, Peng B, Buchdunger E, Ford JM et al. Efficacy and safety of a specific inhibitor of the BCRABL tyrosine kinase in chronic myeloid leukemia. N Eng J Med 2001;344:1031-7. 56. Drucker AM, Wu S, Busam KJ, Berman E, Amitay-Laish I, Lacouture ME. Rash with the multitargeted kinase inhibitors nilotinib and dasatinib: meta-analysis and clinical characterization. Eur J Haematol 2013;90:142-50. 57. Oztas P, Erbasi S, Lenk N, Polat M, Han O, Artuz F et al. Imatinibinduced erythrodermia in a patient with chronic myeloid leukemia. Acta Derm Venereol 2006;86:174-5. 58. Sanghavi SA, Dongre AM, Khopkar US. Imatinib mesylate induced erythroderma. Indian J Dermatolo Venereol Leprol 2012;78:408. Vol. 149 - No. 3 59. Lim D, Muir J. Lichenoid eruption to STI 571. Am J Hematol 2002;70:179. 60. Prabhash K, Doval DC. Lichenoid eruption due to imatinib. Indian J Dermatolo Venereol Leprol 2005;71:287-8. 61. Chan CY, Browning J, Smith-Zagone MJ, Martinelli PT, Hsu S. Cutaneous lichenoid dermatitis associated with imatinib mesylate. Dermatol Online J 2007;13:29. 62. Sendagorta E, Herranz P, Feito M, Ramirez P, Feltes R, Floristán U et al. Lichenoid drug eruption related to imatinib: report of a new case and review of the literature. Clin Exp Dermatol 2009;34:e3156. 63. Ghosh SK. Generalized lichenoid drug eruption associated with imatinib mesylate therapy. Indian J Dermatol 2013;58:388-92. 64. Lee JH, Chung JY, Jung MY, Kim CR, Park JH, Lee JH et al. Lichenoid drug eruption after low-dose imatinib mesylate treatment. Ann Dermatol 2013;25:500-2. 65. Pascual JC, Matarredona J, Miralles J, Conesa V, Borras-Blasco J. Oral and cutaneous lichenoid eruption secondary to imatinib: report of two cases. Int J Dermatol 2006;45:1471-3. 66. Wahiduzzaman M, Pubalan M. Oral and cutaneous lichenoid reaction with nail changes secondary to imatinib: report of a case and review literature. Dermatol Online J 2008;14:14. 67. Gómes-Fernández C, Sendagorta-Cudós E, Casado Verrier B, Feito Rodríguez M, Suárez Aguado J et al. Oral lichenoid eruption associated with imatinib treatment. Eur J Dermatol 2010;20:127-8. 68. Kuraishi N, Nagai Y, Hasegawa M, Ishikawa O. Lichenoid drug eruption with palmoplantar hyperkeratosis due to imatinib mesylate: a case report and review of the literature. Acta Derm Venereol 2010;90:73-6. 69. Gambillara E, Laffitte E, Widmer N, Decosterd LA, Duchosal MA, Kovacsovics T et al. Severe pustular eruption associated with imatinib and voriconazole in a patient with chronic myeloid leukemia. Dermatology 2005;211:363-5. 70. Ayirookuzhi SJ, Ma L, Ramshesh P, Mills G. Imatinib-induced Sweet syndrome in a patient with chronic myeloid leukemia. Arch Dermatol 2005;141:368-70. 71. Schwarz M, Kreuzer KA, Baskaynak G, Dörken B, Le Coutre P. Imatinib-induced acute generalized exanthematous pustulosis (AGEP) in two patients with chronic myeloid leukemia. Eur J Haematol 2002;69:254-6. 72. Brouard MC, Prins C, Mach-Pascual S, Saurat JH. Acute generalized exanthematous pustulosis associated with STI571 in a patient with chronic myeloid leukemia. Dermatology 2001;203:57-59. 73. Dib EG, Ifthikharuddin JJ, Scott GA, Partilo SR. Neutrophilic eccrine hidradenitis induced by imatinib mesylate (Gleevec) therapy. Leuk Res 2005;29:233-4. 74. Ugurel S, Lahaye T, Hildenbrand R, Glorer E, Reiter A, Hochhaus A et al. Panniculitis in a patient with chronic myelogenous leukaemia treated with imatinib. Br J Dermatol 2003;149:678-9. 75. Assouline S, Laneuville P, Gambacorti-Passerini C. Panniculitis during dasatinib therapy for imatinib-resistant chronic myelogenous leukemia. N Eng J Med 2006;354:2623-4. 76. Clark SH, Duvic M, Prieto VG. Mycosis fungoides-like reaction in a patient treated with Gleevec. J Cutan Pathol 2003;30:279-81. 77.Yanagi T, Sawamura D, Shimizu H. Follicular mucinosis associated with imatinib (STI571). Br J Dermatol 2004;151:1276-8. 78. Plana A, Carrascosa JM, Vilavella M, Ferrandiz C. Pityriasis rubra pilaris-like reaction induced by imatinib. Clin Exp Dermatol 2013;38:520-2. 79. Battistella M, Frémont G, Vignon-Pennamen MD, Gornet JM, Dubertret L, Viguier M. Imatinib-induced hand-foot syndrome in a patient with metastatic gastrointestinal stromal tumor. Arch Dermatol 2008;144:1400-2. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 327 G ITAL DERMATOL VENEREOL 2014;149:329-33 Thalidomide-induced granuloma annulare C. FERRELI 1, L ATZORI 1, F. MANUNZA 1, M. PAU 2, A. CADDORI 3 Granuloma annulare (GA) is an acquired, usually self-limiting, asymptomatic granulomatous skin disease with well recognized clinical and histological features that occurs in children and adults generally before the age of 30. Five clinical types are described including the localized, generalized, subcutaneous, perforating, and patch forms. The possible role of immune dysregulation has been pointed out in the pathogenesis of GA, as it has been reported in association with several diseases and conditions like diabetes, thyroid diseases, malignancies, tuberculosis, human immunodeficiency, Epstein Barr and hepatitis C virus infection. Drug-induced GA is a rare presentation, that can appear similar or identical to idiopathic GA. We present a 75-yearold Caucasian man with a violaceous ring-like firm, papular eruption, localized on the dorsal aspect of both hands, with histological features of GA, which subsequently resolved with the discontinuation of thalidomide he had started 1 month earlier for the treatment of a multiple myeloma. The lesions appeared with renewed intensity after resuming a therapy cycle. Jones’s algorithm for the diagnosis of adverse drug reactions (ADR) showed a certain association, thus the final diagnosis of thalidomide-induced GA was made. Key words: Granuloma annulare - Thalidomide - Drug-related side effects and adverse reactions. D rug induced GA is a rare entity, firstly described by Rothwell in 1980 induced by gold therapy.1 Since then, besides gold,2 it has been described in association with a number of medications, among them allopurinol,3-5 diclofenac,6 calcium channel blockers,7 antidepressants,8 anticonvulsants,9, 10 interferon.11 More recently, case reports came out Corresponding author: C. Ferreli, M. Aresu Department of Medical Science, University of Cagliari, Via Ospedale 54, 09124 Cagliari, Italy. E-mail: [email protected] Vol. 149 - No. 3 1Unit of Dermatology M. Aresu Department of Medical Science University of Cagliari, Cagliari, Italy 2Unit of Dermatology, AOU Cagliari, Cagliari, Italy 3Unit of Internal Medicine, SS. Trinità Hospital ASL 8, Cagliari, Italy in the literature about the association between antitumor necrosis factor alpha (TNF-alpha) drugs and the occurrence of GA.12-17 The paradox of this last observation is that TNF inhibitors can be used for the treatment of refractory GA.18 Case report A 75-year-old Caucasian male was admitted to our hospital because of the recent onset of erythematous ringlike firm papular lesions, mostly in annular configuration with clear centre and slightly elevated borders, localized on the dorsal aspect of both hands. The eruption occurred 15 days after the start of thalidomide therapy, at the starting dosage of 100 mg/day, then increased to 150 mg/day, for multiple myeloma. Dermatologic examination revealed asymptomatic multiple erythematous papules and annular plaques localized on lateral and dorsal aspect of both hands and fingers (Figure 1). No rash was present elsewhere. The mucous membranes, hair and nails were normal. Laboratory examination of complete blood count, serum chemistries, liver and kidney function tests showed normal results, as well as rheumatoid factor, anti doublestranded DNA, antinuclear antibodies, CRP, pANCA and cANCA. The patient was otherwise healthy, no arthralgias, or autoimmunity disorders were present. The past GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 329 FERRELI THALIDOMIDE INDUCED GRANULOMA ANNULARE Figure 1.—Papular eruption on the dorsal aspect of both hands and fingers. Figure 2.—Resolution of the rash after drug withdrawal. Figure 3.—Palisading infiltrate of histiocytes surrounding areas of collagen degeneration with a dense perivascular lymphocytic infiltrate (H&E 10X). Figure 4.—Palisading granulomas around degenerated collagen (H&E 40X). 330 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 THALIDOMIDE INDUCED GRANULOMA ANNULARE FERRELI association (certain), and the diagnosis of drug-induced GA was made. Discussion Figure 5.—Mucin deposition in areas of interstitial histiocytic infiltrate (Alcian blue 40X). medical history was remarkable for multiple myeloma related pathological fractures on D12, L2-L5 and duodenal bulb disease. Histopathological examination of a biopsy taken from the dorsum of the hand showed a palisading infiltrate of histiocytes, surrounding areas of necrobiotic collagen fibres and a dense perivascular lymphocytic infiltrate with few eosinophils, without vasculitis (Figures 3, 4). There was also a prominent interstitial histiocytic infiltrate and mucin deposition (Figure 5), with no evidence of interface dermatitis. Neither lymphoid atypia nor giant histiocytes were observed. Thalidomide administration was suspected to have induced the lesions as its discontinuation produced a dramatic improvement within one month (Figure 2). A rechallenge with thalidomide 100 mg/day associated with prednisone 25 mg/bid three months later resulted in the recurrence of lesions within two weeks. Thalidomide was definitely stopped with complete and persistent resolution of the rash. Jones’s algorithm for the diagnosis of adverse drug reactions 19 confirmed the highly probable Vol. 149 - No. 3 GA is a relatively common idiopathic disorder occurring in all races and ages more frequently affecting women under 30 years of age. Five clinical variants are described, localized, generalized, subcutaneous, perforating, and patch forms, with often overlapping clinical features. The proposed pathogenetic mechanisms are many: they range from IFN-gamma producing lymphocytes in the setting of a Th1 inflammatory reaction,20 to type IV delayed hypersensitivity,21 lymphocytes mediated monocytes’ activation 22 and elastic fibers degeneration.23 Several etiologic factors have been suggested, such as viral infections (HSV, EBV, HBV, HCV and HIV), insect bites and trauma,24 TB testing and sunlight 25 and neoplastic disorders,26 although they are still unproven.27 Drug induced GA has been described after exposure to a number of drugs and, more recently, anti TNF-alpha drugs have been added to the list.12-17 TNF-alpha is a cytokine that plays an important role in the normal host defence 28 but, when overproduced, it is implicated in the pathogenesis of several inflammatory conditions and autoimmune disorders by inducing and maintaining inflammation through lymphocytes’ activation and cytokine production.29 Thalidomide has re-emerged as a novel antineoplastic agent with antiangiogenic activities and it has been shown to down regulate the production of TNF-alpha, both in vivo and in vitro, suggesting its immunomodulatory role.30 In our patient thalidomide was administered for the treatment of multiple myeloma and the temporal relationship among the development of the dermatosis, its resolution upon drug discontinuation and its recurrence upon rechallenge of this drug, confirmed the iatrogenic nature of the rash. The chance that idiopathic GA had occurred in association with multiple myeloma is unlikely as our patient did not have clinical evidence of GA prior to thalidomide treatment. Moreover, to the best of our knowledge, GA has never been reported in patients affected with multiple myeloma. Besides, there are several potentially drug induced entities that clinically resemble GA that should be regarded in the GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 331 FERRELI THALIDOMIDE INDUCED GRANULOMA ANNULARE differential diagnosis, such as interstitial granulomatous dermatitis (IGD),31 palisaded neutrophilic and granulomatous dermatitis (PNGD),32 interstitial granulomatous drug reaction (IGDR),33 and a GA in the setting of systemic disease.34 In the case reported herein histologic features supporting the diagnosis of GA included collagen necrobiosis, interstitial histiocytosis and abundant mucin deposition, in the absence of interface dermatitis and lymphoid atypia, features generally found in IGDR. The occurrence of drug induced GA following anti-TNF-alpha treatment has been primarily described in patients with collagen vascular diseases, mainly rheumatoid arthritis, after administration of new “biologic” anti-TNF-alpha agents,35 but it has not yet been described in association with thalidomide therapy. Conversely, thalidomide, an old anti-TNF-alpha inhibitor, and its derivative lenalidomide, have been reported to induce IGDR 29, 36 suggesting that there is a spectrum of drug induced granulomatous reactions with often subtle clinical findings and variable histopathologic pictures. The pathogenesis of the granulomatous reaction developing in the course of TNF-alpha inhibitors could be related to some specific hystiocyte and/or lymphocyte activity regulated by this cytokine and the immunologic burden in genetically predisposed individuals. Further reports might unravel the question and convey new insights on this unusual cutaneous adverse drug reaction. Conclusions The occurrence of GA during the administration of TNF-alpha inhibitors has been described mainly in patient affected by rheumatoid arthritis, and has encouraged the hypothesis that this drugs can promote a disease specific reaction. Our case occurred in absence of rheumatoid arthritis, therefore suggesting that the drug is primarily responsible for the cutaneous reaction due to a kind of immunologic suppression induced by this class of drugs. References 1. Rothwell R. S, Schloss E H. Granuloma Annulare and Gold Therapy Arch Dermatol 1980;116:863 2. Martin N, Belinchón I, Fuente C, Vélez A, Sánchez-Yus E. Granuloma annulare and gold therapy. Arch Dermatol 1990;126:1370-1. 332 3. Singh SK, Manchanda K, Bhayana AA, Verma A. Allopurinol induced granuloma annulare in a patient of lepromatous leprosy. J Pharmacol Pharmacother 2013;4:152-4. 4. Becker D, Enk A, Bräuninger W, Knop J. Granuloma anulare disseminatum as a rare side effect of allopurinol. Hautarzt 1995;46:343-5. 5. Goihman-Yahr M Disseminated granuloma annulare and intranasal calcitonin. Int J Dermatol 1993;32:150. 6. Le Corre Y, Léonard F, Fertin C, Kalis B. Granuloma-annulare type photosensitivity disorder caused by diclofenac. Ann Dermatol Venereol 1992;119:932-3. 7. Lim AC, Hart K, Murrell D. A granuloma annulare-like eruption associated with the use of amlodipine. Australas J Dermatol 2002;43:24-7. 8. Álvarez-Pérez A, Gómez-Bernal S, Gutiérrez-González E, Rodríguez-Granados MT, Toribio J. Granuloma annulare photoinduced by paroxetine. Photodermatol Photoimmunol Photomed 2012;28:47-9. 9. Lagier L, Dunoyer E, Estève E. Topiramate: a new inductor of granuloma annulare? 2011;138:141-3. 10. Cassone G, Tumiati B. Granuloma annulare as a possible new adverse effect of topiramate. Int J Dermatol 2014;53:259-61. 11. Kluger N, Moguelet P, Chaslin-Ferbus D, Khosrotherani K, Aractingi S. Generalized Interstitial Granuloma Annulare Induced by Pegylated Interferon-Alpha. Dermatology 2006;213:248–249 12. Ratnarathorn M, Raychaudhuri S P, Naguwa S Disseminated granuloma annulare: a cutaneous adverse effect of anti-tnf agents Indian J Dermatol 2011;56:752-754. 13. Werchau S, Enk A, Hartmann M. Generalized interstitial granuloma annulare response to adalimumab. Int J Dermatol 2010;49:45760 14. Voulgari PV, Markatseli TE, Exarchou SA, Zioga A, Drosos AA. Granuloma annulare induced by anti-tumour necrosis factor therapy. Ann Rheum Dis 2008;67:567-70. 15. Viguier M, Richette P, Bachelez H, Wendling D, Aubin F Paradoxical cutaneous manifestations during anti-TNF-alpha therapy. Ann Dermatol Venereol 2010;137:64-71. 16. Devos SA, van den Bossche N, De Vos M, Naeyaert JM. Adverse skin reactions to anti-TNF-alpha monoclonal antibody therapy. Dermatology 2003;206:388-90. 17. Lebas D, Staumont-Sallé D, Solau-Gervais E, Flipo RM, Delaporte E. Cutaneous manifestations during treatment with TNF-alpha blockers: 11 cases. Ann Dermatol Venereol 2007;134:337-42. 18. Kozic H, Webster GF. Treatment of widespread granuloma annulare with adalimumab: a case report. J Clin Aesthet Dermatol 2011;4:42-3. 19. Jones JK. Criteria for journal reports of suspected drug reactions. Clin Pharm 1982;1:554-5. 20. Fayyazi A, Schweyer S, Eichmeyer B, Herms J, Hemmerlein B, Radzun HJ et al. Expression of IFNgamma, coexpression of TNFalpha and matrix metalloproteinases and apoptosis of T lymphocytes and macrophages in granuloma annulare. Arch Dermatol Res 2000;292:384-90. 21. Buechner SA, Winkelmann RK, Banks PM. Identification of T-cell subpopulations in granuloma annulare. Arch Dermatol 1983;119:125-8. 22. Umbert P, Winkelmann RK. Histologic, ultrastructural and histochemical studies of granuloma annulare. Arch Dermatol 1977;113:1681-6. 23. Hanna WM, Moreno-Merlo F, Andrighetti L. Granuloma annulare: an elastic tissue disease? Case report and literature review. Ultrastruct Pathol 1999;23:33-8. 24. Smith MD, Downie JB, DiCostanzo D. Granuloma annulare. Int J Dermatol 1997;36:326-33. 25. Stewart LR, George S Hamacher K L, Hsu S. Granuloma annulare of the palms. Dermatol Online J 2011;17:5. 26. Hawryluk EB, Izikson L. English JC 3rd. Non-infectious granulo- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 THALIDOMIDE INDUCED GRANULOMA ANNULARE matous diseases of the skin and their associated systemic diseases: an evidence-based update to important clinical questions. Am J Clin Dermatol 2010;11:171-81. 27. Dahl MV Granuloma annulare: long-term follow-up. Arch Dermatol 2007;143:946-7. 28. Saripalli YV, Gaspari AA. Focus on: biologics that affect therapeutic agents in dermatology. J Drugs Dermatol 2005;4:233-45. 29. Deng A, Harvey V, Sina B, Strobel D, Badros A, Junkins-Hopkins JM et al. Interstitial granulomatous dermatitis associated with the use of tumor necrosis factor alpha inhibitors. Arch Dermatol 2006;142:198-202. 30. Klausner JD, Freedman VH, Kaplan G. Thalidomide as an AntiTNF-a Inhibitor: Implications for Clinical Use Clin Immunol and Immunopathol 1996;81:219-23. 31. Tomasini C, Pippione M. Interstitial granulomatous dermatitis with plaques. J Am Acad Dermatol 2002;46:892-9. 32. Gordon K, Miteva M, Torchia D, Romanelli P. Allopurinol-induced palisaded neutrophilic and granulomatous dermatitis. Cutan Ocul Toxicol 2012;31:338-40. Vol. 149 - No. 3 FERRELI 33. Hernández N, Peñate Y, Borrego L. Generalized erythematousviolaceous plaques in a patient with a history of dyslipidemia. Interstitial granulomatous drug reaction (IGDR). Int J Dermatol 2013;52:393-4. 34. Thornsberry LA, English JC 3rd. Etiology, diagnosis, and therapeutic management of granuloma annulare: an update. Am J Clin Dermatol 2013;14:279-90. 35. Wendling D, Prati C. Paradoxical effects of anti-TNF-α agents in inflammatory diseases. Expert Rev Clin Immunol 2014;10:15969. 36. Yazganoğlu KD, Tambay E, Mete O, Ozkaya E. Interstitial granulomatous drug reaction due to thalidomide. J Eur Acad Dermatol Venereol 2009;23:490-3. Presented at the 88th SIDeMaST National Congress. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 333 ORIGINAL ARTICLES G ITAL DERMATOL VENEREOL 2014;149:335-40 Topical lactoferrin can improve stable psoriatic plaque R. SARACENO 1, T. GRAMICCIA 1, S. CHIMENTI 1, P. VALENTI 1, M. PIETROPAOLI 2, L. BIANCHI 1 Aim. Lactoferrin (LF), a non-haem iron binding glycoprotein, shares antimicrobial properties with innate immune system components influencing proinflammatory release of cytokines involved in psoriatic plaque development. The objective of the study was to verify if LF could provide a therapeutic application in psoriasis. Methods. An open-label, two arms, 4-week trial was designed on 30 subjects affected by mild to moderate plaque psoriasis. All patients received oral bovine LF 100 mg. Fifteen patients (group A) were topically treated with 10% LF ointment, 15 patients (group B) with 20% LF ointment. All patients applied only ointment vehicle on contra lateral target lesion as intra-patient side to side control. Efficacy was assessed by Target Lesion Score. Results. Twenty-two patients completed the study. Improvement in elevation, redness and scaling was observed on LF treated psoriatic target lesions comparing to the controlateral controls (P<0.05). There was no additional efficacy for 20% versus 10% topical applications. Oral drug alone did not exert any improvement on the control plaques receiving topical placebo. Conclusion. Our clinical results suggest that LF could be included as a possible safe topical therapeutic option in the treatment of psoriatic plaque. Key words: Lactoferrin - Immune system - Interleukin-6 - Psoriasis. P soriasis is a chronic inflammatory skin disease affecting 1% to 3% of the Italian population.1 It ranges in severity from mild to severe, and patients experience significant deterioration in quality of life.2-4 Topical therapies represent the first line treatment for patients with mild to moderate stable Corresponding author: R. Saraceno, MD, Department of Dermatology, Policlinico Tor Vergata, viale Oxford 81, 00133 Rome, Italy. E-mail: [email protected] Vol. 149 - No. 3 1Department of Dermatology Tor Vergata University, Rome, Italy 2Biotechnology Society, Rome, Italy and localized plaque psoriasis affecting less than 10% of the body’s surface.5 Interactions among keratinocytes and components of innate and acquired immune system are considered main steps in the pathogenesis of psoriasis.6 Innate immune cells produce key cytokines (tumour necrosis factor-α [TNF-α], interferon-α [IFN-α], interferon-γ [IFN-γ], interleukin-1β [IL-1β], and interleukin-6 [IL-6]) that activate myeloid dendritic cells.7 Activated myeloid dendritic cells lead to T cell differentiation, keratinocytes activation and production of antimicrobial peptides (i.e., cathelicidin, psoriasin and β-defensins).8 Lactoferrin (LF), a non haem iron binding glycoprotein belonging to transferrin family, has been reported to possess both antibacterial and immune modulatory properties.9 LF is the second most abundant protein in human milk and is found in most exocrine secretions including tears, nasal secretions, saliva, intestinal mucus and genital secretions.10, 11 Moreover, LF is a key element in the host defense system involved in several physiological functions including a direct antimicrobial role by limiting the proliferation and adhesion of microbes and/or by killing them.12 These properties are mainly related to the ability to sequester iron in biological fluids or to destabilize the membranes of microorganisms.13 In addition to the antimicrobial properties, both in vitro and in vivo studies, suggest that LF may have a direct effect on regulation of cytokine production including TNF-α, GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 335 SARACENO Topical lactoferrin and psorias IFN-γ, IL-6 and IL-1β.14, 15 TNF-α and IL-6 play an important pathogenetic role in psoriasis.7 The role of TNF-α is clinically validated by the effect of antiTNF-α targeted therapies. IL-6 is raised in psoriasis and the pleiotropic effects include stimulation of epidermal keratinocyte hyperplasia as well as promoting the differentiation of IL-17-producing T lymphocytes.15 According to these findings, we designed a clinical and investigative study in order to evaluate the therapeutic properties of bovine LF (bLF) topically applied and the possible additional effect of low doses of bLF orally administered in patients affected by mild to moderate stable plaque-type psoriasis. Materials and methods A four-week, prospective, bilateral-paired controlled study of bLF in subjects with mild to moderate psoriasis showing stable localized symmetrical lesions was disegned. Patients were randomized (1:1) according to the CONSORT criteria.16 The study protocol and consent form were approved by the local health authority and all subjects provided written informed consent prior to study enrollment. Inclusion criteria were: 1) clinical diagnosis of stable and symmetrical plaque psoriasis for at least one month and involving <10% body surface area; 2) age 18 years or above; 3) psoriasis area and severity index (PASI) 17 score ≤10. Paired target lesions were considered when in similar anatomic locations and with equal baseline severity score for erythema, scaling and infiltration. Subjects who were pregnant or nursing were not included in the study. Patients were also ineligible if they had used topical agents within 4 weeks from the enrollment or received systemic antipsoriatic drugs within 8 weeks from the entry date. Symmetrical lesions localized on the knees or elbows with similar TLS (±1) were selected by a dermatologist not directly involved in the study using photos and masked as to the date of when the photos were taken. Patients were treated for 4 weeks according to the mean duration of most of the psoriatic topical treatments, as follows: 1) bLF ointment on the target lesion; 2) only ointment vehicle on a contra lateral target lesion as intra-patient side to side control. Thirty out-patients (15 women and 15 men, mean age 49.2, range 1867 years) with stable bilateral symmetrical psoriasis were enrolled in this study. Fifteen patients were included in group A and 15 in group B. Only psoriatic 336 target lesions were treated with bLF 10% ointment BID (group A) or bLF 20% ointment OD (group B). bLF ointment was provided by Giellepi Chemicals S.p.a. (Seregno, Milan, Italy). The ointment composition was 10 or 20% of bLF in a mixture of liquid paraffin and polyethylene, as hydrophobic gel base vehicle. Oral bLF, 100 mg (Lattoglobina® 100 mg capsules, Grünenthal-Formenti, Achen, Germany), was fasting administered BID in both groups. Because of the preliminary design of the study, oral placebo treated groups with and without drug or placebo ointment were not included. Visits were scheduled at baseline, at week 2 and at week 4. The follow-up period was 4 weeks. Evaluation was performed by PASI score (for the inclusion criteria) and by assessing erythema, scaling, and infiltration according TLS, using a four point scale for each parameter (0=none; 1=mild; 2=moderate, 3=severe). The clinical evaluation was assessed by a blinded independent dermatologist. VAS from 0 to 10 was also proposed to assess patient pruritic symptoms. Safety was evaluated by recording any adverse event occurring during the study period. Routine bloods tests, serum ferritin, iron and transferrin levels were performed at baseline, at week 4 and at the end of the study. Biochemical assay Plasma concentrations of TNF-α and IL-6 were determined in duplicate using a high sensitivity commercial sandwich enzyme-linked immunosorbent assay (ELISA) kit (Mabtech, Italy). All assay procedures were performed as described by the manufacturer. The lower limit of cytokine’s detection was 0.02 pg/mL for IL-6, and 0.06 pg/mL for TNF-α. Statistical analysis The minimal level of significance of the differences was fixed at P≤0.05 for all the procedures. The statistical analysis was carried out by using SPSS11.01 Software. The study was designed to reach a power of 0.80 with a type 1 error of 0.05, using the “POWER and PRECISION 3.2” program, SPSS. Results A total of 22 (12 women and 10 men, mean age 51.6, range 18-67 years) out of 30 patients with bi- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Topical lactoferrin and psorias SARACENO Table I.—Baseline characteristics of the study population. Group A Total number of patients Male/Female Mean age (range) Mean age of onset (years)±SD Psoriatic arthritis Mean PASI T0 (range) Mean TLS T0 (range) Group B 15 7/8 49.5 (18-67) 35.0±13 1/15 3.1 (1.2-6.8) 4.9 (2-6) A 15 5/10 49.0 (18-66) 31.8±15 2/15 3.4 (1.2-7.4) 5.0 (3-6) B Figure 1.—Group A: Clinical response of the target lesion (A) after 4 weeks (B) of treatment with bLF 10% applied BID. lateral symmetrical psoriasis completed the study. Ten patients were counted in group A (4 women and 6 men) and 12 patients in group B (8 women and 4 men). Eight patients discontinued the study due to lack of efficacy (2 patients of group A and 1 patient of group B), worsening of the treated lesion (1 patient of group B) and lack of compliance (4 patients of group B). Lesions were localized on knees and elbows. The study population was homogeneous for demographics and disease features (Table I). Over the treatment period, both bLF 10% and bLF 20% ointments improved the target lesions: reduction of plaques’ elevation, redness and scaling were noted after 4 weeks of treatment, slightly more evident in group B patients (Figures 1, 2). The mean TLS improved by 23.5% at week 2 and by 37.3% at week 4 in group A, and by 25.8% at week 2 and by 35.5% at week 4 in group B (Figure 3). These changes were statistically significant (P<0.05 Wilcoxon two sample test). In both groups, over the 4-week treatment period, a substantial improvement Vol. 149 - No. 3 of itch from baseline to week 4 (VAS score: from 5.8 to 3.2) was noticed in the target bLF treated lesions, compared to the control lesions (VAS score at week 4 was 5.1). At 4 week of follow-up, these results were not maintained. Adverse events were observed in 3 subjects in group B and these included burning sensation at the site of drug application (these subjects did not withdraw from the study). No serious adverse events were reported during the study and the follow-up period. No significant changes in routine laboratory values were observed in any of the patients. In group A, serum TNF-α and IL-6 mean levels at week 0 and week 4 showed no significant variations (Table II). Discussion LF is a member of the transferrin family of nonhaem iron binding proteins with several physiological functions including protection against microbial GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 337 SARACENO Topical lactoferrin and psorias A B Figure 2.—Group B: Clinical response of the target lesion (A) after 4 weeks (B) of treatment with bLf 20% applied OD. static effect related to the high iron binding affinity of the protein that deprives iron-requiring bacteria of this essential growth nutrient.18-20 The second antibacterial property of LF is due to a direct bactericidal effect against gram negative and gram positive bacteria that cannot be attributed to simple iron deprivation.12 Moreover, in vitro and in vivo studies suggest that LF plays an anti-inflammatory effect by inhibiting the production of several cytokines including TNF-α,13 IL-6 14 and by influencing dendritic cells,21 that are key mediators of the inflammatory response in psoriasis.7 Psoriasis is a chronic inflammatory disorder mediated by elements of the innate and adaptive immune systems.7 Innate immunity is non-specific and protects the body against the constant risks of pathogens.8 Thus the epidermis constitutes a major barrier to the environment and provide the first line of defense against invading microbes. Even though our study was conducted in a small series of cases, we could observe a clinical effect of bLF ointment in the local treatment of stable localized psoriatic plaques. Both the concentrations proposed achieved similar improvement. In contrast, the clinical com- Figure 3.—The chart shows the efficacy of lactoferrin on the target lesion score (TLS) in both groups of treatment. In contrast the same PASI at baseline and at week 4 highlights that no changes in the controlateral side were induced by lactoferrin orally administered. *Changes statistically significant (P<0.05 Wilcoxon two sample tests). infection, regulation of myelopoiesis and systemic immune responses.9-12 The antibacterial functions of LF have been substantiated by both in vitro 13 and in vivo 14 evidences. The first mechanism is a bacterio- Table II.—Serum IL-6 and TNF-α levels at baseline and 4 weeks after therapy. Serum cytokines IL-6 (pg/mL) TNF-α (pg/mL) T0 2.112 (±3.820) 25.233 (±6.425) T4 3.446 (±8.758) 23.073 (±3.283) These parameters were detected in order to evaluate the immunomodulatory effects of bovine lactoferrin orally administered on the release of two key cytokines in psoriasis. A slight increase in IL-6 and a slight decrease in TNF-α serum concentrations were observed at the end of treatment (T4). Both variations were not statistically significant. 338 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Topical lactoferrin and psorias parable contralateral plaques who only received the systemic oral bLF or those treated with placebo ointment vehicle, did not show any clinical improvement suggesting that oral bLF at the dosage proposed did not reach the skin or was too low or ineffective or administrated for a too short period of time. The antimicrobial effects of bLF and the aforementioned opposite results, suggest that the topical application of bLF locally may modulate the expression and functions of epidermal barrier components such as corneocytes and specialized cells of epidermis namely Langerhans’ cells. According with this hypothesis, it has been demonstrated that the topical administration of the iron-binding protein, human LF, inhibits Langerhans’ cells migration and TNF-α release.13, 21 By these experiments, LF appeared as a potent inhibitor of Langerhans’ cells migration and TNF-α production. These properties could explain and justify its role in treating chronic skin inflammation such as psoriasis in which TNF-α is an important mediator. Furthermore, since LF exists as a constituent of normal skin, raises the possibility that in psoriasis LF could be reduced and that LF may act as endogenous regulator of skin immune functions influencing local cytokines production. We were not able to correlate the slight variations detected in the serum levels of TNF-α and IL-6 in our patients at the end of the protocol with the anti-inflammatory effect mediated by the oral Lf in other subjects.22 Moreover, patients reported a significant reduction in pruritic symptoms in both sides. This effect could be mediated by the aforementioned cytokines or through more specific pathways (i.e., substance P, histamine). One of the key mechanism of innate immune responses are the existence of receptors to recognize pathogens and the production of factors that kill pathogens such as the antimicrobial peptides (AMPs).23 AMPs are emerging as participants in the defense system of the epithelial barriers and they represent a primary system for protection in response to microbial invasion. AMPs dysfunction emerges as a central factor in the pathogenesis of several cutaneous diseases including psoriasis.24 Evidence of this comes from the observation that psoriatic keratinocytes are a rich source of AMPs, including LL-37, β-defensins, and S100A7.25 It has been recently demonstrated that the aforementioned AMPs bind self-DNA and self-RNA to form structures that gain access to endosomal Toll-like receptors, leading to an aberrant activation of plasmacytoid dendritic cells Vol. 149 - No. 3 SARACENO (pDCs) to produce IFN-γ.26 pDC-derived IFN-γ may initiate the autoimmune-inflammatory cascade in psoriasis, a process characterized by the activation of myeloid DCs and their maturation into DCs that stimulate pathogenic autoimmune T cells.26 According with the antimicrobial properties of both Lf and AMPs, LF may compete with AMPs, down-regulate their expressions and the development of autoimmunity. This mechanism could further explain the antiinflammatory effects of LF in psoriasis. Limitations of the study Main limitations are represented by the small size samples of the cases enrolled, the absence of a control group not taking oral bLF, the short period of the study, and the low doses of oral LF. The study design did not include a control group only treated with topical LF because previous studies showed that only high doses (800 mg to 5 g) of oral LF are effective in the treatment of psoriasis.27, 28 For this reason we administered low doses of oral LF in order to evaluate a possible synergistic effect with topical LF ointment. Since oral LF did not show synergistic or positive effects, the absence of a control group could not be considered a major limitation. Finally, since several topical and available treatments are effective in the short period, we decided to evaluate the efficacy of a new formulation in a 4-week period.29 Further investigations could evaluate possible synergistic effect of topical bLF associated with corticosteroid as most of the therapeutic experiences either as fixed combination 30 or as separate daily application.31 The clinical results observed in our study suggest that LF could become a new therapeutic option in the treatment of mild and localized psoriasis. LF was well tolerated and transient site burning reported from three patients occurs during the first few days and resolves within 1 week of therapy. According with these results and to the limited adverse events observed, the once daily application (20% formulation) could be considered more suitable for psoriatic patients and possibly increase compliance to the treatment. References 1. Saraceno R, Mannheimer R, Chimenti S. Regional Distribution of psoriasis in Italy. J Eur Acad Dermatol Venereol 2008;22:324-9. 2. Krueger GG, Feldman SR, Camisa C, Duvic M, Elder JT, Gottlieb AB et al. Two considerations for patients with psoriasis and their GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 339 SARACENO Topical lactoferrin and psorias clinicians: what defines mild, moderate, and severe psoriasis? What constitutes a clinically significant improvement when treating psoriasis? J Am Acad Dermatol 2000;43:281-5. 3. Al-Suwaidan SN, Feldman SR. Clearance is not a realistic expectation of psoriasis treatment. J Am Acad Dermatol 2000;42:796-802. 4. Linder D, Sampogna F, Torreggiani A, Balato N, Bianchi L, Cassano N et al. Psodisk, a new visual method for assessing the burden of psoriasis on patients. J Eur Acad Dermatol Venereol 2012;26:11635. 5. Lebwohl M, Ali S. Treatment of psoriasis. Part 1. Topical therapy and phototherapy. J Am Acad Dermatol 2001;45:487-98; 499-502. 6. Chiricozzi A, Zhang S, Dattola A, Gabellini M, Chimenti S, Nistico SP. Role of Th17 in the pathogenesis of cutaneous inflammatory diseases. J Biol Regul Homeost Agents 2012;26:313-8. 7. Nestle FO, Kaplan DH, Barker J. Psoriasis. N Engl J Med 2009;361:496-509. 8. Schauber J, Gallo RL. Antimicrobial peptides and the skin immune defense system. J Allergy Clin Immunol 2009;124:R13-8. 9. Legrand D, Pierce A, Elass E, Carpentier M, Mariller C, Mazurier J. Lactoferrin structure and functions. Adv Exp Med Biol 2008;606:163-94. 10. Rodríguez-Franco DA, Vázquez-Moreno L, Ramos-Clamont Montfort G. Antimicrobial mechanisms and potential clinical application of lactoferrin. Rev Latinoam Microbiol 2005;47:102-11. 11. Valenti P, Antonini G. Lactoferrin: an important host defence against microbial and viral attack. Cell Mol Life Sci 2005;62:2576-87. 12. Ward PP, Conneely OM. Lactoferrin: role in iron homeostasis and host defense against microbial infection. Biometals 2004;17:203-8. 13. Machnicki M, Zimecki M, Zagulski T. Lactoferrin regulates the release of tumour necrosis factor alpha and interleukin 6 in vivo. Int J Exp Pathol 1993;74:433-9. 14. Crouch SP, Slater KJ, Fletcher J. Regulation of cytokine release from mononuclear cells by the iron-binding protein lactoferrin. Blood 1992;80:235-40. 15. Kimura A, Naka T, Kishimoto T. IL-6-dependent and -independent pathways in the development of interleukin 17-producing T helper cells. Proc Natl Acad Sci USA 2007;104:12099-104. 16. Schultz KF, Altman DG, Moher D. The CONSORT Group. CONSORT 2010 Statement: Updated Guidelines for Reporting ParallelGroup Randomized Trials. Trials 2010;11:32. 17. Fredriksson T, Pettersson U. Severe psoriasis – oral therapy with a new retinoid. Dermatologica 1978;157:238-44. 18. Bullen JJ, Rogers HJ, Leigh L. Iron-binding proteins in milk and resistance to Escherichia coli infection in infants. Br Med J 1972;1:69. 19. Bullen JJ, Rogers HJ, Griffiths E. Role of iron in bacterial infection. Curr Top Microbiol Immunol 1978;80:1. 340 20. Reiter B. Review of nonspecific antimicrobial factors in colostrum. Ann Rech Vet 1978;9:205. 21. Cumberbatch M, Bhushan M, Dearman RJ, Kimber I, Griffiths CE. IL-1beta-induced Langerhans’ cell migration and TNF-alpha production in human skin: regulation by lactoferrin. Clin Exp Immunol 2003;132:352-9. 22. Paesano R, Pietropaoli M, Gessani S, Valenti P. The influence of lactoferrin, orally administered, on systemic iron homeostasis in pregnant women suffering of iron deficiency and iron deficiency anaemia. Biochimie 2009;91:44-51. 23. Gilliet M, Lande R. Antimicrobial peptides and self-DNA in autoimmune skin inflammation. Curr Opin Immunol 2008;20:401-7. 24. Büchau AS, Gallo RL. Innate immunity and antimicrobial defense systems in psoriasis. Clin Dermatol 2007;25:616-24. 25. Lande R, Gregorio J, Facchinetti V, Chatterjee B, Wang YH, Homey B et al. Plasmacytoid dendritic cells sense self-DNA coupled with antimicrobial peptide. Nature 2007;449:564-9. 26. Nestle FO, Conrad C, Tun-Kyi A, Homey B, Gombert M, Boyman O et al. Plasmacytoid predendritic cells initiate psoriasis through interferon-alpha production. J Exp Med 2005;202:135-43. 27. Drouin R, Moroni O, Cantin K, Juneau C. A double-blind, placebocontrolled, randomized trial of XP-828L (800 mg) on the quality of life and clinical symptoms of patients with mild-to-moderate psoriasis. Altern Med Rev 2008;13:145-52. 28. Poulin Y, Bissonnette R, Juneau C, Cantin K, Drouin R, Poubelle PE. XP-828l in the treatment of mild to moderate psoriasis: randomized, double-blind, placebo-controlled study. J Cutan Med Surg 2006;10:241-8. 29. Kamili QU, Menter A. Topical treatment of psoriasis. Curr Probl Dermatol 2009;38:37-58. 30. Girolomoni G, Vena GA, Ayala F, Cannavò SP, De Pità O, Chimenti S et al. Consensus on the use of the fixed combination calcipotriol/ betamethasone dipropionate in the treatment of plaque psoriasis. G Ital Dermatol Venereol 2012;147:609-24. 31. Calzavara-Pinton P, Rossi MT, Sala R, Venturini M. The separate daily application of tacalcitol 4 µg/g ointment and budesonide 0.25 mg/g cream is more effective than the single daily application of a two compound ointment containing calcipotriol 50 µg/g and betamethasone dipropionate 0.5 mg/g. G Ital Dermatol Venereol 2011;146:295-9. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. Received on October 30, 2013. Accepted for publication on November 20, 2013. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 G ITAL DERMATOL VENEREOL 2014;149:341-6 Clinically and/or histologically pigmented poromas in Caucasian patients R. BETTI 1, C. BOMBONATO 1, A. CERRI 1, L. MONEGHINI 2, P. ABRAMO 1, S. MENNI 1 Aim. Pigmented poromas are rarely reported and considered to be more common in non-white people and on non-acral sites. Objective of the present study was to report our cases of pigmented poromas with particular attention to the presence of clinical and/or microscopic evidence of pigmentation, their characteristics and the diagnostic pitfall with other pathologies. Methods. All the histologically confirmed poromas observed from January 1994 to July 2012 were considered. Clinicepidemiological data were collected. The presence of clinical pigmentation was recorded as well as the presence of melanin pigmentation or melanocytes in the histologic specimens. Results. One hundred and one patients with poromas were collected. All the patients were Caucasians. All the lesions were solitary. Only three patients had a clinically visible pigmented poromas. In eight cases the presence of melanin and melanocytes did not produce a clinically visible pigmentation. All the poromas with pigmentation did not occur on palmo-plantar surfaces. Conclusion. Pigmented poromas may be observed even in Caucasian patients and their clinical aspect mimic basal cell carcinoma and/or melanoma. The presence of pigment visible at the histology may not be observed in the clinical expression. The absence of pigmentation on palmo-plantar location is confirmed in all the reported cases. Key words: 1Dermatologic Clinic, Department of Health Sciences University of Milan, San Paolo Hospital, Milan, Italy 2Department of Health Sciences, Division of Pathology University of Milan, San Paolo Hospital, Milan, Italy patients.2 They are usually non-pigmented even if the pigmented variant can be occasionally found.3-12 This variant seems to be more frequent in non-white people and on non-acral sites 12 although recently a pigmented palmar case has been reported.13 This study describes three additional cases of clinically pigmented poromas (PP) in white patients and briefly discusses their frequency, their characteristics, the diagnostic pitfall with other pathologies, the problem of the supposed pigmentation mechanism and other cases in which the presence of melanin and/or melanocytes in the histologic specimens did not involve an evident clinical pigmentation. Materials and methods Poroma - Pigmentation - Foot. Subject populations P oromas are benign adnexal tumors derived from cells of the outer layer of acrosyringium and the sweat duct ridge.1 They often appear as flesh-colored to reddish solitary nodules, papules or plaques, frequently present on the palmo-plantar area of aged Corresponding author: R. Betti, Department of Health Sciences, Division of Dermatology, University of Milan, San Paolo Hospital, via di Rudinì 8, 20142 Milan, Italy. E-mail: [email protected] Vol. 149 - No. 3 All the cases of histologically confirmed poromas observed in our institution from January 1994 to July 2012 were collected. Clinic-epidemiological data recorded were age at diagnosis, gender, location, size, symptoms, color, preoperative diagnosis. Pathological diagnosis according to the four accepted poromas subtypes was made: these are classically based on the difference of their tumor cells location.2 Classic poromas (EP) exhibit a lobular growth pattern and GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 341 BETTI Pigmented poromas A B C D Figure 1.—Patient 1. A) A 1 cm in diameter uniformly brownish nodular lesion over the left retroauricular region of a 67-year-old white man; B) anastomosing cords of small monomorphous polygonal, epithelial poroid cells extending from the epidermis onto the subjacent dermis with sporadic cystic spaces delimitated by cuticolar cells (HE x2.5); diffuse areas with melanin pigmented poroid cells were present (HE x10); C) the presence of intracellular melanin in the poroid cells is diffuse; D) MART-1 immunohistochemical stain show the presence of dendritic melanocytes dispersed throughout the lesion (MART-1 x40). broad connection to the overlying epidermis, Hidroacanthomas simplex (HS) are essentially located within the epidermis, whereas dermal duct tumors (DDT) are intradermal neoplasms mostly composed of small lobular aggregations of cells, with little or no connection to the epidermis. Poroid hidroadenoma (PH) were described by Abenoza and Ackerman as dermal neoplasms consisting of single or few large aggregations of “poroid” and “cuticular” cells, with cystic areas.2 The presence of clinical pigmentation was recorded as well as the presence of melanin pigmentation or melanocytes in the histologic specimens. 342 Results A total of 101 patients with poromas participated into the study. Among them, 33 were EPs, 6 HSs, 3PHs. No DDTs were observed. Microscopic and/or clinical presence of pigmentation was observed in eleven cases. The clinical data of pigmented poromas are summarized in Table I. Only three patients had a clinically visible pigmentation. In the other eight patients the presence of melanin deposition in the poroid cells (five patients) and melanocytes (three patients) or GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Pigmented poromas BETTI A B C D Figure 2.—Patient 2. Flesh to brownish dome shaped nodule 12x10 mm in diameter on the back of a 69-year-old Caucasian man (A). The pigmentation is uniform but more visible in the emilateral portion of the nodule. The majority of tumor cells consisted of small, dark, homogeneous poroid cells and cuticular cells. Melanin filled poroid cells and dispersed MART-1 dendritic melanocytes were also seen (B) (HE, original magnification x40). Patient 3. Irregularly pigmented nodular lesion on the inner surface of right subauricular region of a 64-year-old white man (C). Anastomosing cords and lobules of small monomorphous cuboidal epithelial cells extending from the epidermis into the subjacent dermis. At the basal level, in a scattered manner, an increased number of melanin poroid cells and basal melanocytes were visible (D) (HE, original magnification x10). both (five patients) slight scattered in the dermis do not produce a clinically visible pigmentation. Poromas on the feet (Table I, patients 4, 8, 11) were never located on the soles but on the dorsal surface. The presurgical clinical diagnosis of the three pigmented poromas was: Patient 1 (Figure 1): suspected melanoma; Patient 2 (Figures 2A, B): suspected basal cell carcinoma or possibly melanoma; Patient 3 (Figures 2C, D): basal cell carcinoma. Vol. 149 - No. 3 Case reports Patient 1.—A 67-year-old white man had a 1-cm brownish nodule with smooth surface of 8-months duration on his left retro auricular region (Figure 1A). On palpation, a firm and freely movable lesion was felt. Hematoxylin and eosin-stained sections after an excisional biopsy revealed a dermal nodule composed of anastomosing cords of small monomorphic polygonal, epithelial poroid cells extending from the epidermis to the subjacent dermis with sporadic cystic spaces delimitated by cuticular cells (Figure 1B). Areas with diffuse intracellular presence of melanin GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 343 BETTI Pigmented poromas Table I.—Patients with histologic and/or clinically evident pigmented poromas. Patient Age Sex Site Clinical pigmentation Histologic Diagnosis 1 2 3 4 5 6 7 8 9 10 11 67 64 69 58 55 83 72 68 43 51 69 M M M M F M F M F M M Retroauricular Subauricular Back Foot Face Buttock Hand (finger) Foot Trunk Armpit Foot + (Figure 1) + (Figure 2C) + (Figure 2A) - Poroma Poroma Poroma Poroma Poroma Poroma Poroma Poroma Hidroacanthoma simplex Poroma Poroma All the samples showed the presence of pigmentation at the histology. in the pigmented poroid cells were present (Figure 1C). MART-1 immunohistochemical stain showed the presence of dendritic melanocytes dispersed throughout the neoplasia (Figure 1D). Patient 2.—A 69-year-old white man presented with a 14-months history of a dome shaped nodular lesion on his back. The nodule showed a uniform pigmentation mainly located in its emilateral portion. The nodule felt elastic hard and presented flesh to brownish, well circumscribed, 12x10 mm in diameter (Figure 2A). On histological examination the majority of tumor cells consisted of small, dark, homogeneous poroid and cuticular cells. The poroid cells were melanin filled and dispersed MART-1 dendritic melanocytes were observed (Figure 2B). Patient 3.—A 64-year-old white man presented with a 1-year history of enlarging, soft, irregularly pigmented nodular lesion on the inner surface of his right subauricular region. On physical examination, a 12 mm in size, nontender lesion, with both pigmented and non-pigmented areas clearly distinct in location, was observed (Figure 2C). Microscopic examination revealed anastomosing cords and lobules of small monomorphic cuboidal epithelial cells extending from the epidermis to the subjacent dermis. At the basal level, an increased number of melanocytes and melanin filled basal cells was visible in a scattered manner (Figure 2D), moreover a slight number of melanin pigmented poroid cells in the epidermis was also present. Discussion Pigmented poromas are rare, a general total of 50 cases including ours 4-16 being reported in literature. Their anatomical locations were determined as follows: head and neck 17 cases (including ours), trunk including buttocks 13 cases (including ours), arms 19 cases. All the described cases do not include lesions 344 on palms and soles, so certainly PPs have a predilection for non acral sites, in contrast with the more prevalent non pigmented variant.3, 4 Although most of the literature reports affected Japanese, oriental or non-white patients, some reports (including ours) certainly have interested white patients.10, 16 In a few reports patient race is not specified.12, 15 All the reports describe PPs as rare. However, Battistella et al. analyzed the clinical characteristics of 266 patients with poromas and reported a 17% of pigmented cases,1 questioning the real rarity of pigmented poromas. In absence of any further specification, probably some confusion exists when one considering the clinical expression of pigmentation and the histologic presence of melanin and/or melanocytes within the tumoral lobules. In our clinical records of 101 poromas, eleven cases showed the histologic presence of pigmentation within the tumoral lobules (Table I), but only three patients showed the clinical expression of pigmentation (Figures 1, 2). Another report 4 documented three clinically pigmented cases out of 25 patients and seven cases with the microscopic presence of melanin deposits. The report of Moore et al. does not clearly indicate the clinical presence of pigmentation 14 although the authors tend to equalize the histologic presence of pigment with the clinical expression in five patients. Anyway, Minagawa and Koga stressed the fact that PPs contain variable amounts of melanin 11 and this causes the tumors to vary in color. The poroma variations based on the amounts of melanin within the lesion and the different histopathological features 2 may cause problems in differential diagnosis with a variety of benign and malignant conditions above all basal cell carcinoma, seborrheic keratosis and melanoma.5, 10, 11 Dermatoscopy may be GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Pigmented poromas BETTI useful in narrowing the diagnosis.11 The absence of pigment network, the presence of branched streaks or aggregated pigment globules, varying dark-brown and blue-grey colors in variable sized ovoid nests, blue-gray dots and arborizing vessels, but not maple leaf-like structures and spoke-wheel areas share common features with basal cell carcinoma. Atypical pigment network, dots or globules, streaks, irregular and polymorphous blood vessels, regression structures and a blue-white veil share features with melanomas. For these reasons a precautionary narrow- margin excision or excisional surgery is recommended.5, 10 It has been hypothesized that melanocytes colonization of a poroma may be an indicator of malignant transformation to porocarcinoma.6 Moreover, it has been observed that porocarcinoma develops from or is associated with a pre-existing poroma in nearly half of the cases.17, 18 However, porocarcinoma arising in pre-existing pigmented poroma is extremely rare and this finding is at best speculative and has not been validated by larger studies.12 We have not observed the presence of malignant transformation in our 101 poromas, nor we have had the opportunity to observe the suggested transformation of long-standing poromas.19 About the mechanism/s of pigmentation of the tumoral lobules several hypothesis have been proposed to explain this phenomenon present in a range of skin tumors including poromas. Endothelin-1 (ET1), a peptide known to trigger melanocyte activation and to act as a potent mitogen and melanogen for melanocytes has been implicated to participate in the pigmentation process in seborrheic keratosis, actinic keratosis and basal cell carcinomas.20 Hu et al. indicated the possibility that the up-regulation of Endothelin-1 (ET-1) or other melanocytic-stimulating factors may be associated with the colonization (migration and proliferation) of melanocytes from the adjacent epidermis to the poroma at non acral sites only.3 In order to explain the lack of pigmentation at acral sites, the same authors hypothesized that certain characteristics of acral (palmo-plantar) skin inhibit melanocytic colonization. Ueo et al. proposed that for intraepidermal lesion (i.e., hidroacanthoma simplex) the melanin may be transferred to the tumor directly from adjacent normal basal melanocytes.18 Another possibility 21 may be the activation by the tumor of melanocytes persistently present within the eccrine acrosyringium, but even this hypothesis is inconsistent with the lack of reports of palmo-plantar PPs. The lack of response of vitiligo palmo-plantar lesions to Vol. 149 - No. 3 UVB therapy suggest that melanocytes poorly colonize these areas.3 The sum of findings seem to indicate that other factors may play a role in the melanocytic colonization of poromas. These factors may depend on signals derived from the tumors lobules as well as from the surrounding dermal stroma. Further studies are obviously necessary to elucidate this mechanism. Based on these referred literature reports about the pigmentation mechanisms, to discuss the different features of pigmentation seen in our cases may be only speculative. We have different conditions. The diffuse, uniform clinical pigmentation present in patient 1 and the uniformly diffused but emilaterally localized in patient 2 can reflect the uniform presence of melanin filled poroid cells and dendritic mrlanocytes scattered throughout the dermis. The scattered slight pigmentation of the third case can reflect the slight scattered presence of pigment in the basal layer. The absence of clinically relevant or evident pigmentation despite the histological presence of melanocytes, melanin or melanophages in the tumor may be explained by the low density of pigment and the different depth of the tumor lobules interested by the pigmentation. As suggested, differences in the density of melanocytes in the surrounding epidermis may be partially explain the lack of pigment.3 In summary our cases suggest that PPs may be observed in white patients and their clinical aspect mimicks basal cell carcinoma and/or melanoma. Moreover, the presence of histological pigment may not to produce a clinical pigmented expression. The absence of pigmentation on palmo-plantar location is confirmed in all our reported cases and no malignant transformation was observed. References 1. Battistella M, Langbein L, Peltre Band Cribier B. From hidroacanthoma simplex to poroid hidroadenoma: clinicopathologic and immunohistochemic study of poroid neoplasms and reappraisal of their histogenesis. Am J Dermatopathol 2010;32:459-68. 2. Abenoza P, Ackerman AB. Neoplasms with eccrine differentiation. In: Abenoza P, Ackerman AB, editors. Ackerman’s histologic diagnosis of neoplastic skin diseases. Philadelphia: Lea and Febiger eds; 1990. p. 113-85. 3. Hu SC, Chen GS, Wu CS, Chai CY, Chen WT, Lan CC. Pigmented eccrine poromas: expression of melanocyte stimulating cytokines by tumour cells does not always result in melanocyte colonization. J Eur Acad Dermatol Venereol 2008;22:303-10. 4. Chen CC, Chang YT, Liu HN. Clinical and histological characteristics of poroid neoplasms: a study of 25 cases in Taiwan. Int J Dermatol 2006;45:722-7. 5. Nicolino R, Zalaudek I, Ferrara G, Annese P, Giorgio CM, Mo- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 345 BETTI Pigmented poromas scarella E et al. Dermoscopy of eccrine poroma. Dermatology 2007;215:160-3. 6. Wang SH, Tsai TF. Congenital polypoid pigmented eccrine poroma of a young woman. J Eur Acad Dermatol Venereol 2008;22:366-8. 7. Chiu HH, Chen PH, Wu CS, Chen GS, Chen GS, Tsai KB, Wen CH et al. Origin of poroid hidradenoma and pigmentation mechanism of eccrine poroma: critical analysis of an unique presentation. J Eur Acad Dermatol Venereol 2009;23:597-59. 8. Allende I, Gardeazabal J, Acebo E, Díaz-Pérez JL. Pigmented eccrine poroma. Actas Dermosifiliogr 2008;99:496. 9. Ishida M, Hotta M, Kushima R, Okabe H. A case of porocarcinoma arising in pigmented hidroacanthoma simplex with multiple lymph node, liver and bone metastases. J Cutan Pathol 2011;38:227-31. 10. Smith EV, Madan V, Joshi A, May K, Motley RJ. A pigmented lesion on the foot. Clin Exp Dermatol 2012;37:84-6. 11. Minagawa A, Koga I. Dermoscopy of pigmented poroma. Dermatology 2010;221:78-83. 12. Phelps A, Murphy MJ. Pigmented classic poroma: a tumor with a predilection for nonacral sites?. J Cutan Pathol 2010;37:1121-2. 13. Nishikawa Y, Kaneko T, Takiyoshi N, Aizu T, Nakajima K, Matsuzaki Y et al. Dermoscopy of eccrine poroma with calcification. J Dermatol Case Rep 2009;28:38-40. 14. Elloumi-Jellouli A, Marrrak H, Ben Ammar S, Ben Ayed M, Mokhtar I. Porome eccrine pigmentè. Ann Dermatol Venereol 2004;131:1023. 15. Moore TO, Orman HL, Orman SK, Helm KF. Poromas of the head and neck. J Am Acad Dermatol 2001;44:48-52. 346 16. Zina AM, Bundino S, Pippione MG. Pigmented hidroacanthoma simplex with porocarcinoma. Light and electron microscopic study of a case. J Cutan Pathol 1982;9:104-12. 17. Nakanishi Y, Matsuno Y, Shimoda T, Wada T, Yamazaki N, Yamamoto A et al. Eccrine porocarcinoma with melanocyte colonization. Br J Dermatol 1998;138:519-21. 18. Ueo T, Kashima K, Daa T, Kondoh Y, Yanagi T, Yokoyama S. Porocarcinoma arising in pigmented hidroacanthoma simplex. Am J Dermatopathol 2005;27:500-3. 19. Manaka I, Kadono S, Kawashima M, Kobayashi T, Imokawa G. The mechanism of hyperpigmentation in seborrheic keratosis involves the high expression of endothelin-converting enzyme-1a and TNF-a, which stimulate secretion of endothelin-1. Br J Dermatol 2001;145:895-903. 20. Vural P, Erzengin D, Canbaz M, Selcuki D. Nitric oxide and endothelin-1,2 in actinic keratosis and basal cell carcinoma: changes in nitric oxide/endothelin ratio. Int J Dermatol 2001;40:704-8. 21. Robson A, Greene J, Ansari N, Kim B. Eccrine porocarcinoma (malignant eccrine poroma): a clinicopathologic study of 69 cases. Am J Surg Pathol 2001;25:710-20. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. Received on September 6, 2013. Accepted for publication on October 15, 2013. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 G ITAL DERMATOL VENEREOL 2014;149:347-53 In vivo and in vitro evaluation of topical formulations containing physiological lipid mixture for replacement of skin barrier function C. BARBA 1, J. L. PARRA 1, L. CODERCH 1, A. SEMENZATO Aim. The aim of the study was to describe a new in vivo and in vitro approach of the efficacy evaluation of cosmetic emollients to better understand the link between the formulation and the activity of cosmetic products. Methods. Two long term in vivo studies were carried out on nine healthy Caucasian volunteers mean age 40±12 years to evaluate the protecting and repairing effects of the two different barrier repair cosmetic formulations. The application of the formulations was repeated once a day during 7 days and biophysical parameters (TEWL and Skin Hydration) were measured before and after Sodium laureth sulphate exposure The in vitro study was carried out by freeze substitution transmission electron microscopy (FSTEM) on stratum corneum samples obtained by sections of fresh skin from young pigs, depleted with a solvent mixture and treated with the two products Results. The in vivo results demonstrated that daily product application provided a reinforcement of the skin barrier with protecting and repairing effects from chemical injuries the extent of which was dependent on the formulation features (product A>product B) The role of the technical form on the lipid availability was confirmed by the in vitro evaluation tests. Conclusion. The results point out that a daily application of physiological lipid mixture containing emulsion can protect healthy skin and promote the reparing effect on unpaired barrier skin, reducing TEWL and maintaining hydration of the stratum corneum. The efficacy degree is higher when the cosmetic form promotes the availability of active ingredients increasing the product performance. Key words: Emollients - Cosmetics - Ceramides - Dermatitis, Atopic. C osmetic emollients are widely used for the management of atopic dermatitis since many years, as adjuvant of pharmacological therapies.1 Corresponding author: A. Semenzato, Department of Pharmaceutical and Pharmacological Sciences, Via F. Marzolo 5, 35131 Padua, Italy. E-mail: [email protected] Vol. 149 - No. 3 1IQAC-CSIC, 2 Barcelona, Spain 2Department of Pharmaceutical and Pharmacological Sciences University of Padua, Padua, Italy According to the “bricks and mortar model” proposed in nineties by P.M. Elias,2, 3 the stratum corneum, the first line of defense within the epidermal barrier,4 is a multicellular vertically stacked layer of cells embedded within a hydrophobic extracellular matrix, predominantly composed of 50% ceramides, 20-25% cholesterol, and 10-20% free fatty acids.5 This peculiar structure provides fundamental roles in maintaining protection from the environment as well as preventing water loss.6 A significant decrease in all three key lipids, especially ceramides, has been well established in atopic skin, characterized by an increased TEWL and enhanced barrier permeability, because the lipid imbalance and the inadequate amounts of ceramides contribute to defective formation of the corneocyte lipid envelope and lipid mortar.7, 8 The topical application of ointments or creams, containing high lipid concentrations, can provide positive effects to dry skin and impaired epidermal barrier by means of occlusive effects, as a consequence of lipids deposition on the external skin surface.1, 8 Cosmetic emollients available on the market are numerous and very different in composition and in the functional effects they can deliver. Most of them, the so called traditional emollients, contain GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 347 BARBA IN VIVO AND IN VITRO EVALUATION OF TOPICAL FORMULATIONS CONTAINING PHYSIOLOGICAL LIPID MIXTURE high concentrations of highly hydrophobic mineral oils which can create an occlusive film on the skin surface that powerfully decreases the water loss through epidermis and improves the dryness symptoms. These products are normally characterized by a lower compliance by the patients, since they are not easy to spread and leave an oily feeling on the skin surface. Apolar lipids, even though they are very effective in reducing water loss on the short time, are not able to repair the functional deficiency of atopic skin, in terms of lipid synthesis, in particular as regards the diminished amount of ceramides.5, 9 The most innovative formulations on the market focus their activity on the so called “physiologic lipid replacement therapy”. They contain epidermal lipid mixtures (ceramide/cholesterol/fatty acid) as active ingredients to restore normal balance of the epidermal barrier.10, 11 In contrast to traditional emollients that form an external occlusive barrier due to the presence of petrolatum or other mineral oils, physiological lipid-based topical emulsions are supposed to permeate the stratum corneum and stimulate the endogenous lipid synthesis, particularly of ceramides, leading, in a long period, to an increase of the total amount of epidermal “mortar”. Because of this peculiar mechanism of action these cosmetic emollients are usually called barrier repair topical emulsions.12, 13 The maximal efficacy can be reached using all the three components (ceramides, cholesterol, fatty acids) in a proper physiological ratios.8 The helpfulness of cosmetic emollients in the management of pathological skin is commonly evaluated in vivo using non-invasive biophysical techniques (transepidermal water loss [TEWL] and skin hydration, in terms of water-holding capacity of stratum corneum), before and after treatment.14-16 These in vivo tests allow to quantify the clinical effects of emollients. However, they are not able to discriminate the effects of the different ingredients (i.e., active molecules and vehicle components). The purpose of this study is to describe a new approach to the efficacy evaluation of cosmetic emollients carried out both in vivo and in vitro to better understand the link between formulation and efficacy of products, in the perspective to provide to dermatologists some key elements in the product choice within the wide market offer. 348 Materials and methods We studied two oil in water emulsions, named Product A and Product B, containing hydrocarbons and triglycerides as oily phase and a physiological lipid mixture (ceramide, cholesterol, fatty acid) as barrier repair ingredients. The two products are different in that: —— Product A is a cream based on a non-ionic emulsifier that possesses high affinity and compatibility with skin that contains an amount of ceramide 3 times greater than Product B and an amount of occlusive lipids 1.5 times greater than Product B. —— Product B is a gel-emulsion based on a polymeric emulsifier, belonging to the acrylates family. In vivo studies Subjects Nine healthy Caucasian volunteers (all females) phototype III–IV, mean age 40±12 years (range 2957 years), participated in the studies. The subjects were advised to avoid topical drugs or moisturisers on the tested areas for 48h before the experiments. To obtain reliable measurements, the volunteers were acclimatised for 15 min in a conditioned room (22.5°C, 50% RH) before the experiments. Biophysical measurements TEWL, which indicates the barrier function of skin, was measured using a Tewameter TM 210 (Courage and Khazaka). Skin hydration was determined using a Corneometer CM 85 (Courage & Khazaka), which measures skin capacitance in arbitrary units (AU). All parameters were recorded in accordance with established guidelines.17, 18 Protection study A long-term study was performed to test the protective effect of the two cosmetic emollients applied to normal skin, followed by SLS exposure. Baseline measurements of TEWL and skin capacitance were obtained in three marked zones of the right volar forearm before topical application: two areas for topical treatment (Product A and B) and one untreated area (control). Samples were randomly applied (20 µL) onto the marked areas of 4 cm2 using a micropipette GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 IN VIVO AND IN VITRO EVALUATION OF TOPICAL FORMULATIONS CONTAINING PHYSIOLOGICAL LIPID MIXTURE Microman® M25 (Gilson, France). After 24 h (day 1) both parameters, TEWL and skin capacitance, were evaluated and then 20 µL of solutions were applied again. The application of the two products was repeated once a day during 7 days with a total of 7 applications, and parameters were measured on days 1, 4, 7 and 9. Next, the three areas were exposed to 2% sodium laureth sulphate (SLS) aqueous solution for 2 h (see below) and the resultant irritant reaction was assessed 2 h 30 min by measuring TEWL and skin capacitance. Statistical analysis SLS Exposure.—Twenty-five µL of an aqueous solution of 2% SLS were applied on a filter paper placed in each of several aluminium chambers (d=8 mm, Finn Chambers, Epitest Oy, Finland). The chambers were fixed to the skin for 2h with adhesive tape. Upon removal of the patch, the skin was gently rinsed with water and allowed to dry. Sample preparation Repairing study A long-term study was done to test the reparative effect of the two cosmetic emollients on disturbed skin. Baseline measurements of TEWL and skin capacitance were obtained in three marked areas of the left volar forearm before topical application: two areas for topical treatment (Product A and B) and one untreated area (control). Next, the three areas were exposed to 0.5% SLS aqueous solution for 24 h (see below) and the resultant irritant reaction was assessed 24 h after SLS exposure by measuring TEWL and skin capacitance (day 1). Then Product A and Product B were randomly applied (20 µL) onto the marked areas of 4 cm2 using micropipette Microman® M25 (Gilson, France). After 24 h (day 2) parameters, TEWL and skin capacitance were evaluated. The application of the two products was repeated once a day during 7 days with a total of 7 applications, and TEWL and skin capacitance were measured on days 1, 2, 4, 7 and 10. SLS Exposure.—Twenty-five µL of an aqueous solution 0.5% SLS were applied on a filter paper placed in each of several aluminium chambers (d=8 mm, Finn Chambers, Epitest Oy, Finland). The chambers were fixed to the skin for 24 hours with adhesive tape. Upon removal of the patch, the skin was gently rinsed with water and allowed to dry. Vol. 149 - No. 3 BARBA The mean values and standard deviations (SD) were calculated. Dixon’s test was used for detecting outliers, which were excluded from the data. Oneway analysis of variance, with the Kruskal–Wallis test, was used to determine significant differences between the values obtained from the different treatments (significance level accepted: P<0.05). In vitro studies Sections of fresh skin from young pigs, weighing 20-30 kg, were placed in water at 70°C for 3-4 min and the epidermis was scraped off in sheets. To isolate stratum corneum (SC), the epidermal sheets were incubated for 2 h at 37ºC with the epidermal side in contact with a solution of 0.5% Trypsin in PBS at pH 7.4. Trypsin is used to remove adherent cells from epidermis. After the 2h, the Trypsin was removed by several washes of the SC with Milli-Q water.19 SC samples were then treated with chloroform/methanol (2:1) during 2 h, obtaining lipid depleted SC (Ld SC). SC treatments Lipid depleted SC samples were treated with 100mg of Product A or Product B, incubated at 25°C for 48 h, then removed, immediately washed with water, for 15 minutes, at constant agitation and stored at dryness. Freeze-substitution transmission microscopy experiments electron The SC samples were fixed in 5% glutaraldehyde in 0.1M sodium cacodylate buffer, pH 7.3, and postfixed in 0.25% RuO4 in 0.1 M sodium cacodylate, pH 6.8, with 0.25% potassium ferrocyanide (K4Fe(CN)6). After 1h the RuO4 solution was replaced by fresh RuO4 in order to establish an optimal fixation. After rising in buffer, the SC samples were cryofixed, by rapid freezing on a liquid nitrogen cooled metal mirror (Cryo-vacublock, Leica) at -196°C prior to freezesubstitution, as described elsewhere.20, 21 Finally the samples were transferred to a mold containing Lowicryl, and were incubated for 8 h at -50°C under GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 349 BARBA IN VIVO AND IN VITRO EVALUATION OF TOPICAL FORMULATIONS CONTAINING PHYSIOLOGICAL LIPID MIXTURE Figure 1.—Variation of TEWL and skin capacitance after sample application. Changes were evaluated vs. both basal and placebo values (*P<0.05). UVA-radiation, to allow polymerization. Ultrathin sections were cut (Ultracut UCT, Leica), transferred to Formvar-coated grids and examined in a Hitachi 600 transmission electron microscope. Results In vivo studies Figure 1 displays the variation of the two parameters (skin TEWL and the skin capacitance) after sample application during the treatment period. Changes were evaluated vs. both the basal and the control values. TEWL values were slightly decreased on day 4 and 7, but the baseline levels were re-established on day 9. Skin capacitance values showed a statistically significant increase after topical application of both the formulations, at all the control times. Figure 2 shows the effects induced by SLS on the biophysical parameters of the skin areas treated with the two products and untreated (control). At 2 h 30 min an increase of TEWL values of all the treated areas was found, but the skin areas previously treated for one week with Product A and B show statistically significant lower values than the control area. In Figure 3 the reparative effect of the two products on disturbed skin is shown. Both the emulsions induced a higher repairing effect of the barrier function and promoted a repairing of the skin hydration, being the Product A the most effective one. In vitro studies Figure 2.—Variation of TEWL at different intervals following SLS exposure. Changes evaluated vs. basal values (*P<0.05). 350 In Figure 4, the freeze-substitution transmission electron microscopy (FSTEM) micrographs of SC before and after lipid depletion are shown. The in vitro protocol used allows a good visualization of lipid bilayers in the untreated stratum corneum sample (Figure 4A) and a clear absence of lipid bilayers in the SC sample extracted with solvents (Figure 4B). In Figure 5 the effects of Product A and B appli- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 IN VIVO AND IN VITRO EVALUATION OF TOPICAL FORMULATIONS CONTAINING PHYSIOLOGICAL LIPID MIXTURE BARBA Figure 3.—Variation of TEWL and skin capacitance on the reparation study. Changes were evaluated vs. both basal and placebo values (*P<0.05). A B Figure 4.—FSTEM micrographs for SC untreated (A), lipid extracted (B). A B Figure 5.—FSTEM micrographs for lipid extracted SC treated with product A (on the left) and product B (on the right). Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 351 BARBA IN VIVO AND IN VITRO EVALUATION OF TOPICAL FORMULATIONS CONTAINING PHYSIOLOGICAL LIPID MIXTURE cation on lipid depleted SC samples are shown The FSTEM micrographs point out the different ability to permeate the stratum corneum and fill up the intercellular spaces of the two products. A partial bilayer reconstitution has been found on the lipid depleted SC samples treated with the Product A, but not in those on which Product B was applied. Discussion The objects of this study were two commercial products, specifically formulated for a physiologic lipid replacement therapy. In a clinical perspective the two products would have been classified as comparable or similar. As a matter of fact, both are water in oil systems, easy to spread, with a good skin feeling, containing a physiological lipid mixture (ceramide, cholesterol, fatty acid) together with some apolar lipids (hydrocarbons and triglycerides) as active ingredients. However, the two products, seen in a technological formulation perspective, show some significant differences, that could justify a different skin performance. The first difference is the topical delivery vehicle used: Product A is an cream based on a non-ionic emulsifier that possesses high affinity and compatibility with skin, whereas Product B is a gel-emulsion based on a polymeric emulsifier, belonging to the acrylates family. The second difference is the amount of the active ingredients in each formulation: Product A contains an amount of ceramides three times greater than Product B and an amount of lipids 1.5 times greater than Product B. The in vivo/in vitro testing protocol used in this study, point out some peculiar skin behaviour of the two products, strictly related to their formulation compositions. The in vivo results carried out on normal skin, showed an increase of skin hydration (Product A>Product B), but no marked effects on TEWL after products application. As expected, the barrier function of normal skin, measured by TEWL values, was slightly modified by the application of the two emollients, since both the formulations did not present a marked occlusive character. However, skin hydration is statistically significant increased, being the Product A more markedly effective, suggesting that both 352 Product A and B moisturized the stratum corneum with a non-occlusive mechanism. A one week treatment with product A and B promoted a reinforcement of the skin barrier, that was demonstrated by a lower increase of the TEWL values in respect to untreated skin, after SLS (Product A>Product B) This protective effect on normal skin can be related to the lipid barrier replacement mechanism of the active ingredients. The ability of the two formulations on repairing the damaged skin was confirmed by the in vivo study carried out on pre-treated skin. The two products induced a high repairing effect of the barrier function, both in terms of TEWL values and skin water-holding capacity (Product A> Product B) A reinforcement of the skin barrier due to the application of these ceramide containing formulations, led to a protecting effect from chemical injuries. Once again, the protective effect was more pronounced for the cream (Product A), than for the gelemulsion (Product B). This is not surprising considering the formulation differences between of the two emulsions. As a matter of fact, the non-ionic emulsifier system used in Product A supported and promoted the bioavailability of the active ingredients, in a more effective way, than the acrylate polymers used in Product B. The influence of the formulation on the bioavailability of lipids was confirmed by the in vitro evaluation tests. Only Product A, formulated with a nonionic emulsifier, with high skin affinity, was effective in the stratum corneum permeation and able to fill up the intercellular spaces. This was not so for the gel emulsion based on acrylate polymers (Product B). Conclusions To maintain skin hydration and reinforce its barrier function, with a daily regular moisturizer use, is an essential part of the atopic dermatitis and dry skin management and every day dermatologists are requested to select for their patients the appropriate product among a broad market offer. The classification commonly used in: traditional emollients (i.e., with a relevant external occlusive effects), and innovative formulations based on the barrier repair activity of the ceramide dominant physiological lipid-based mixtures seems inadequate, from a technological point of view, to justify and explain the different clinical effects. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 IN VIVO AND IN VITRO EVALUATION OF TOPICAL FORMULATIONS CONTAINING PHYSIOLOGICAL LIPID MIXTURE The performance of cosmetic emollients and their mechanism of interaction with healthy and impaired skin can be very different depending on their composition, not only as regards the active ingredients but also the technical form. A daily application of the two products, that are both physiological lipid mixture containing emulsions, can moisturize normal skin and promote the repairing effect on unpaired barrier skin reducing TEWL and maintaining hydration of the stratum corneum. The extent of this effect is higher when the cosmetic form of the product promotes the bioavailability of active ingredients leading to a more effective skin performance on dry and atopic skin. A better understanding of the most advantageous product compositions can be obtained using in vivo/in vitro methodologies. References 1. Mack Correa MC, Nebus J. Management of patients with atopic dermatitis: the role of emollient therapy. Dermatol Res Practice 2012:836931. 2. Elias PM. Lipids and the epidermal permeability barrier. Arch Dermatol Res 1981;270:95-117. 3. Elias PM, Menon GK. Structural and lipid biochemical correlates of the epidermal permeability barrier. Adv Lipid Res 1991;24:1-26. 4. Elias PM. Stratum corneum defensive functions: an integrated view. J Invest Dermatol 2005;25:183-200. 5. Sugarman JL. The epidermal barrier in atopic dermatitis. Semin Cutan Med Surg 2008;27:108-14. 6. Elias PM, Wakefield JS. Therapeutic implications of a barrierbased pathogenesis of atopic dermatitis. Clin Rev Allergy Immunol 2011;41:282-95. 7. Danby S, Cork MJ. A new understanding of atopic dermatitis: the role of epidermal barrier dysfunction and subclinical inflammation. J Clin Dermatol 2010;1:33-46. 8. Sajiæ D, Asiniwasis R, Skotnicki-Grant S. A look at epidermal barrier function in atopic dermatitis: physiologic lipid replacement and the role of ceramides. Skin therapy letter 2012;17:6-9. Vol. 149 - No. 3 BARBA 9. Anderson PC, Dinulos JG. Are the new moisturizers more effective? Curr Opin Pediatr 2009;21:486-90. 10. Mao-Qiang M, Brown BE, Wu-Pong S, Feingold KR, Elias PM. Exogenous nonphysiologic vs physiologic lipids. Divergent mechanisms for correction of permeability barrier dysfunction. Arch Dermatol 1995;131:809-16. 11. Man MQ M, Feingold KR, Thornfeldt CR, Elias PM, Optimization of physiological lipid mixtures for barrier repair, J Invest Dermatol 1996;106:1096-101 12. Sugarman JL, Parish LC. Efficacy of a lipid-based barrier repair formulation in moderate-to-severe pediatric atopic dermatitis. J Drugs Dermatol 2009;8:1106-11. 13. Draelos ZD. The effect of ceramide-containing skin care products on eczema resolution duration. Cutis 2008;81:87-91. 14. Coderch L, Fonollosa J, De Pera M, De la Maza A, Parra JL. Efficacy of stratum corneum lipid supplementation on human skin. Contact Dermatitis 2002;47:139-46. 15. Coderch L, López O, de la Maza A, Parra JL. Ceramides and skin function. Am J Clin Dermatol 2003;4:107-9. 16. Ramírez R, Martí M, Barba C, Méndez S, Parra JL, Coderch L. Skin efficacy of liposomes composed of internal wool lipids rich in ceramides. Int J Cosmet Sci 2010;61:235-45. 17. Rogier V, EEMCO Group. EEMCO guidance for the assessment of transepidermal water loss in cosmetic sciences Skin Pharmacol Appl Skin Physiol 2001;14:117-28. 18. Berardesca E. EEMCO Group. EEMCO Guidance for the assessment of stratum corneum hydration: electrical methods. Skin Res Technol 197;3:126-32. 19. López O, Cócera M, Wertz PW, López-Iglesias C, de la Maza A. New arrangement of proteins and lipids in the stratum corneum cornified envelope. Biophys Biochem Acta 2007;1768:521-9. 20. Van den Bergh BAI, Bouwstra JA, Junginger HE, Wertz PW. Elasticity of vesicles affects hairless mouse skin structure and permeability. J Controlled Rel 1999;62:367-79. 21. Lopez O, Cocera M, Coderch L, Parra JL, de la Maza A. Reconstitution of liposomes inside the intercellular lipid domain of the stratum corneum. Langmuir 2002;18:7002-8. Funding.—This work was partly funded by Unifarco S.p.A. The authors wish to thank Carmen López-Iglesias for her expert assistance with the FSTEM study performed in the Scientific and Technological CenterUniversity of Barcelona (CCIT-UB). Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. Received on July 19, 2013. Accepted for publication on September 24, 2013. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 353 G ITAL DERMATOL VENEREOL 2014;149:355-61 Psychopathology and eating disorders in patients with psoriasis M. L. CROSTA 1, G. CALDAROLA 2, S. FRAIETTA 1, A. CRABA 1 C. BENEDETTI 2, V. COCO 2, L. JANIRI 1, L. RINALDI 1, C. DE SIMONE 2 Aim. Psoriasis is a multifactorial chronic inflammatory skin disease that often occurs in patients who are overweight or obese. In literature the connections between obesity and eating disorders are well known, but few studies have investigated the link between eating disorders and psoriasis. We hypothesized that Eating Disorders (ED) can be considered a psychogenic cofactors, which contribute to the development of obesity and metabolic syndrome in psoriatic patients, who are frequently prone to psychiatric comorbidity. Methods. From January to April 2011 we enrolled 100 consecutive psoriatic outpatients and a control group of 100 selected non-psoriatic outpatients, matched by age, gender, and BMI to the study group. The assessment battery was composed by the Psoriasis Area Severity Index (PASI) score, the Eating Disorder Inventory (EDI) and the Symptom Checklist-90 Revised (SCL-90-R®). Results. Our data showed that most of EDI and SCL-90R subscales was mostly altered in psoriatic population compared to patients without psoriasis. Moreover, we noticed in patients with psoriasis an association between the progressive weight increase and an impairment on most of EDI subscales. Conclusion. Psoriasis is associated with psychopathological traits, which are frequently found in EDs. Since obesity makes psoriasis less susceptible to therapy and weight loss improves drug response, dermatologists should be alert to suspect the presence of this condition. Key words: Psoriasis - Eating disorders – Psychopathology Obesity. P soriasis is a multifactorial chronic inflammatory skin disease. This condition is known to be associated with serious comorbidities, and, among them, has been shown that the most frequent is PsoCorresponding author: G. Caldarola, Department of Dermatology, Sacro Cuore Catholic University, L.go F. Vito 8, 00168 Rome, Italy. E-mail: [email protected] Vol. 149 - No. 3 1Institute of Psychiatry Catholic University of the Sacred Heart, Rome, Italy 2Institute of Dermatology Catholic University of the Sacred Heart, Rome, Italy riatic Arthritis.1 Furthermore, prevalence of obesity, metabolic syndrome and cardiovascular disease have been found to be higher among patients with psoriasis compared with the general population.2-7 It is known from the literature, that psoriasis often occurs in patients who are overweight or obese.8, 9 There are also many studies showing the relation between obesity and eating disorders (ED).10-12 EDs are conditions defined by abnormal eating habits, which may involve either insufficient or excessive food intake. Anorexia nervosa and Bulimia nervosa are the most common specific form. Other types include binge eating disorder (BED) and ED not otherwise specified. BED, as defined by the diagnostic and statistical manual of mental disorders, fourth edition (DSM-IV TR), is characterized by recurrent episodes of binge eating (e.g., eating an unusually large amount of food accompanied by a sense of lack of control) in the absence of significant compensatory behaviours (e.g., self-induced vomiting, excessive exercise).12 Moreover, it is associated with significant medical complications related to obesity, psychiatric comorbidity and reduced quality of life.13, 14 BED can be considered among the psychopathological cofactors that may contribute to the development of obesity and metabolic syndrome in pa- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 355 CROSTA EATING DISORDERS IN PSORIASIS tients with psoriasis, which are also prone to several psychiatric comorbidities, including depression and anxiety.15-23 From this evidence, few studies have investigated the relation between EDs and psoriasis, showing in particular the possible influence of BED on obesity and metabolic syndrome related to psoriasis.24, 25 The purpose of our research was to evaluate the presence of a disturbance of eating behavior and psychopathological traits in patients suffering from psoriasis, in comparison with a population not affected and correlate data with the severity of the skin disorder and the Body Mass Index (BMI). Materials and methods This was an observational study carried out at the Department of Dermatology of the Catholic University of Sacred Heart in collaboration with the Institute of Psychiatry. One hundred consecutive and unselected patients affected by psoriasis were enrolled into the study from January to April 2011. During the same period, we selected a group of 100 non-psoriatic patients attending the videodermoscopy outpatient clinic of the same Department. We matched the two groups by age, gender and BMI. In fact, major confounding factors are gender and age, as eating disorders are significantly more common among women and younger age groups. Moreover, we matched the two groups by BMI to avoid the influence of obesity on EDs. Patients with and without psoriasis had to be at least 18 year old and they had to fill in two psychiatric questionnaire: Eating Disorder Inventory (EDI) and Symptom Checklist 90 Revised (SCL-90-R®). All patients were evaluated in different clinical aspects, which included gender, weight, height and morbidity (diabetes, hypertension, dyslipidemia, metabolic syndrome, cardiovascular diseases, liver disease, cancer). BMI was calculated as weight and height ratio (kg/m2). On BMI basis, the two populations were divided into 3 groups: normal weight (BMI<25 kg/ m2), overweight (BMI 25-29.9 kg/m2) and obese (BMI≥30 kg/m2). Moreover we collected data about psoriasis type and severity, duration of disease, and current treatments. We evaluated the severity of psoriasis using PASI (Psoriasis Area Severity Index).26 356 To determine the PASI score, a score is assigned from 0 to 4 to the psoriatic lesions on the basis of erythema, infiltration and desquamation. Four anatomic regions (head, trunk, arms and legs) are evaluated separately and a score from 0 to 6 is assigned to each region, depending on the surface rate involved. Scores are multiplied by a coefficient and then added together. Total score ranges from 0 (absence of disease) to 72 (high severity psoriasis). Using the PASI score we divided our population into 3 groups: remission (PASI 0), mild disease (0<PASI<10), moderate-severe disease (PASI>10). EDs were analysed using EDI. The EDI 27, 28 is a widely used self-report measure of EDs, developed by Garner et al. in 1983 to measure symptoms of anorexia nervosa, bulimia and BED, although it does not allow a specific diagnosis. It is made up of 64 items grouped into 8 subscales. Three of them measure attitudes and behaviours related to eating, weight and body imaging: drive for thinness (DT), bulimia (B) and body dissatisfaction (BD). The other 5 subscales explore general clinically relevant psychological traits: ineffectiveness (IN), perfectionism (PE), interpersonal distrust (ID), interoceptive awareness (IA) and maturity fears (MF). The SCL-90-R 29 is used as a screening measure of general psychiatric symptomatology. It is a self-report format made up of 90 items validated by Derogatis et al. in 1977. It includes dimensions measuring somatization (SOM), obsessive-compulsive (OC), depression (DEP), anxiety (ANX), phobic anxiety (PHOB), hostility (HOS), interpersonal sensitivity (IS), paranoid ideation (PAR), psychoticism (PSY), and sleep disease (SLEEP). We have used the suggested cut-off scores (psychopathological traits >1). We also calculated a Global Severity Index (GSI). It represents the sum of the scores divided by the number of items and it is designed to measure overall psychological distress; the cut-off score for the GSI used in this study is 0.57, as indicated by the existing literature:30, 31 scores equal to or above 0.57 are considered to be indicative of “dysfunctional” subjects, who have a high probability of psychiatric disorders. Statistical analysis Data collection and statistical analyses were performed by an independent investigator. Categorical variables were described as numbers and percent- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 EATING DISORDERS IN PSORIASIS CROSTA ages; continuous variables were described as mean ± standard deviation (SD) or median ± range. Categorical variables were analysed using multivariable analysis or chi square tests. To compare continuous variables we used the Pearson correlation and the ANalysis Of VAriance (ANOVA) in a model that included an independent predictor on univariate analyses. P values inferior to 0.05 were considered statistically significant. When multiple T test were performed, Bonferroni style correction was used. Statistical analyses were performed using the statistical software IBM-SPSS version 19.0. Results A total of 200 subjects were enrolled in the study: 100 patients with psoriasis and 100 without it. The demographic and clinical characteristics were similar in the two study groups (Table I). It is worthy of note that 65% of the patients with psoriasis had a BMI higher than 25: 46% of them were overweight (BMI 25-30) and 19% were obese (BMI≥30). Table II reports the results of the EDI questionnaire at multivariable analysis by psoriasis with BMI, age and gender. The cut-offs vary in the different subscales. In the table we reported, the number of patients with above threshold scores at each subscale and the mean score for the two sample groups. There were no significant differences between the psoriasis group and the group without psoriasis in the EDI subscales, except for the BD (P=0.03) and ID (P=0.006) subscales. showing more pathological scores in patients with psoriasis. Table III shows, instead, the results of the SCL90-R questionnaire at multivariable analysis by psoriasis with BMI, age and gender, which indirectly assesses the presence of psychopathological traits. A score ≥1 was considered pathological. Interestingly, the SCL-90-R questionnaire was globally more impaired in patients with psoriasis than in patients not affected, as indicated by higher score on the GSI. In addition, this difference was statistically significant in 4 of 10 subscales (PAR, ANX, DEP and SOM). On the basis of the BMI, we divided patients with psoriasis into 3 groups: 35 patients with BMI<25 (35%), 46 patients with BMI 25-30 (46%), 19 patients with BMI≥30 (19%). Table IV summarizes EDI results in the 3 different BMI classes of psoriatic patients. The ANOVA analyses showed significant differences in some EDI subscales as B (P=0.007), BD (P=0.001) and IA (P=0.064) in the obese group compared to the other two groups. Moreover, there was a strong trend towards significance in some other SCL-90-R subscales (ANX (P=0.08), HOS (P=0.08), PAR (P=0.09), SI (P=0.09). Table I.—Baseline clinical characteristics. Subjects (%) Age (mean±SD) (range) Gender: male/female BMI (mean±SD) Morbidity Diabetes (%) Hypertension (%) Dyslipidemia (%) Liver diseases (%) Metabolic syndrome (%) Cardiovascular disesase (%) Cancer PASI (mean±SD). Disease duration (mean±SD) Psoriatic Arthritis (%) Treatment Topic (%) Sistemic (%) Biological (%) With psoriasis Without psoriasis P 100 (50%) 47.7±12.9 20-73 51/49 27.2±4.3 100 (50%) 50.8±15.2 19-80 61/39 27.8±4.4 0.12 0.16 0.34 14 26 7 2 12 2 0 4±5.6 13.8±12.7 44 18 25 6 0 14 3 0 - 0.44 0.87 0.77 0.48 0.67 0.65 0 - 19 17 55 - - BMI: Body Mass Index; PASI: Psoriasis Area Severity Index Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 357 CROSTA EATING DISORDERS IN PSORIASIS Table II.—EDI subscales at multivariable analysis. Subscale DT (n.v.<14.5) Number of patients (%) mean±SD B (n.v.<7.5) Number of patients (%) mean±SD BD (n.v.<15.8) Number of patients (%) mean±SD IN (n.v.<15.8) Number of patients (%) mean±SD P (n.v.<9) Number of patients (%) mean±SD ID (n.v.<8) Number of patients (%) mean±SD IA (n.v. <13.8) Number of patients (%) mean±SD MF (n.v.<9.5) Number of patients (%) mean±SD Number of patients with at least one altered subscale (%) With psoriasis Without psoriasis P 4 (4%) 3.76±4.3 6 (6%) 2.96±4.71 0.56 2 (2%) 0.72±2.42 2 (2%) 0.78±1.81 0.17 8 (8%) 7.47±5.49 13 (13%) 7.19±6.31 0.03 4 (4%) 3.44±3.99 0 (0%) 2.68±3.09 0.08 5 (5%) 2.64±2.86 8 (8%) 2.82±3.19 0.85 22 (22%) 4.42±3.66 4 (4%) 2.95±2.68 0.006 4 (4%) 2.76±3.46 1 (1%) 1.78±2.73 0.07 17 (17%) 5.7±4.54 43 (43%) 14 (14%) 5.06±3.78 31 (31%) 0.64 0.08 DT: drive for thinness; B: bulimia; BD: body dissatisfaction; IN: ineffectiveness; P: perfectionism; ID: interpersonal distrust; IA: interoceptive awareness; MF: maturity fears. The Pearson correlation was used to highlight the association between the progressive increase in weight and the worsening of the EDI scores: the increase in BMI led to an increase in the scores of five EDI subscales. In particular, BMI had a significant association with DT (P=0.01), B (P<0.001), BD (P=0.006), IN (P=0.014) and IA (P=0.001), in the psoriasis group, but no correlation was observed between the increasing in BMI and the SCL-90-R scores Conversely, the Pearson correlation showed an association between the increase in BMI and only two EDI subscales in the control group: BD (P=0.02) and ID (P=0.008); but there was an important correlation between the increase in BMI and several SCL-90-R subscales: SOM (P=0.017), OC (P=0.004), ANX (P=0.05), HOS (P=0.04), PAR (P=0.009), PSY (P=0.047), SLEEP (P=0.013). Moreover, for a better understanding of the psychological traits in the psoriasis group, we divided the population into 3 sub-groups on the basis of PASI score: 30 patients (30%) with disease remission (PASI 0), 56 patients (56%) with low-grade disease (0<PASI<10) and 14 patients (14%) with moderate-to-severe skin disease (PASI>10). 358 There was no significant association between disease severity and psychopathological traits, probably due to the non-homogeneous sample. Nevertheless, using the Pearson correlation, we observed a significantly worsening in the scores of two SCL-90-R subscales (HOS [P=0.026] and PHOB [P=0.034]) associated with an increase in the PASI score while there were no significant correlations between EDI subscales and PASI. We also investigated two other independent variables as “psoriasis duration” and “previous treatments”, but no correlation was found with psychological traits. Discussion Psoriasis is an autoimmune disease with a strong psychosomatic component whose onset and recurrence often follow trauma or stressful life events.32 If it is difficult to establish a cause-effect relationship between psychological factors and psoriasis, it is rather certain that the disease has a significant impact on the psychological state and quality of life.33-35 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 EATING DISORDERS IN PSORIASIS CROSTA Table III.—SCL-90-R subscales at multivariable analysis. Subscale SOM Number of patients (%) mean±SD OC Number of patients (%) mean±SD IS Number of patients (%) mean±SD DEP Number of patients (%) mean±SD ANX Number of patients (%) mean±SD HOS Number of patients (%) mean±SD PHOB Number of patients (%) mean±SD PAR Number of patients (%) mean±SD PSY Number of patients (%) mean±SD SLEEP Number of patients (%) mean±SD GSI Number of patients (%) mean±SD With psoriasis Without psoriasis P 39 (39%) 0.90±0.70 23 (23%) 0.67±0.56 <0.001 38 (38%) 0.89±0.69 32 (32%) 0.70±0.60 0.12 23 (23%) 0.71±0.66 19 (19%) 0.60±0.55 0.32 37 (37%) 0.91±0.73 25 (25%) 0.64±0.57 0.002 35 (35%) 0.78±0.66 15 (15%) 0.53±0.52 0.003 20 (20%) 0.67±0.62 20 (20%) 0.56±0.57 0.64 9 (9%) 0.27±0.45 6 (6%) 0.24±0.42 0.49 35 (35%) 0.89±0.77 22 (22%) 0.56±0.65 0.02 14 (14%) 0.43±0.49 8 (8%) 0.28±0.40 0.07 51 (51%) 1.07±1.06 36 (36%) 0.80±0.83 0.31 23 (23%) 0.75±0.56 14 (14%) 0.57±0.48 0.02 SOM: somatisation; OC: obsessive-compulsive; DEP: depression; ANX: anxiety; PHOB: phobic anxiety; HOS: hostility; IS interpersonal sensitivity; PAR: paranoid ideation; PSY: psychoticism; SLEEP: sleep disease; GSI: Global Severity Index. Table IV.—EDI results in the 3 BMI classes analysed by ANOVA. Subscale DT (n.v.<14.5) mean±SD B (n.v.<7.5) mean±SD BD (n.v.<15.8) mean±SD IN (n.v.<15.8) mean±SD P (n.v.<9) mean±SD ID (n.v.<8) mean±SD IA (n.v.<13.8) mean±SD MF (n.v.<9.5) mean±SD BMI<25 BMI 25-30 BMI>30 P 2.91±3.89 0.11±0.40 7±6.26 3.57±4.15 2.89±2.88 3.57±3.48 2.63±3.15 6.26±5.36 3.83±4.30 0.57±1.50 6.74±3.91 2.76±2.94 2.22±2.75 4.91±3.62 1.83±2.32 5.04±3.67 5.16±4.84 2.21±4.42 10.11±6.66 4.84±5.49 3.21±3.07 4.79±3.97 5.26±4.95 6.26±4.82 0.186 0.007 0.064 0.156 0.367 0.235 0.001 0.414 DT: drive for thinness, B: bulimia, BD: body dissatisfaction, IN: ineffectiveness, P: perfectionism, ID: interpersonal distrust, IA: interoceptive awareness, MF: maturity fears. Many psoriatic people have common psychopathological traits, among which are: the difficulty of experiencing and verbalizing their emotions (alexithymia); dysfunctional emotional responses, which includes the use of neurotic defenses (avoidance, de- Vol. 149 - No. 3 nial, repression, feeling isolations), and indications of a fear of intimate contact.36 The objective of this study was to assess concomitant ED and psychopathological traits in patients with psoriasis, trying to correlate data with different GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 359 CROSTA EATING DISORDERS IN PSORIASIS features of cutaneous disease (duration, severity) and BMI. This is the first prospective study evaluating the presence of these conditions in two groups of patients, with and without psoriasis. In fact, the previous studies about this argument are a cross-sectional, randomized, and controlled trial who evaluated it only in 100 psoriatic patients and a retrospective, observational study of medical claims data in pediatric population.24, 25 Our data showed a higher prevalence of psychopathological traits and symptoms indicating an eating disorder in patients with psoriasis compared to those without psoriasis. Regarding the EDI, BD and ID subscales showed a statistically significant alteration in patients with psoriasis. The first scale evaluates the belief that some parts of the body (especially those associated with typical changes of puberty) are too big or too fat. The fat body, grotesque and so distant from the standard, induces shame and discomfort feelings. ID represents a sense of alienation and reluctance to establish close relationships and can be considered a useful indicator of quality of life. These data disagree with the abovementioned retrospective study in the pediatric population, which missed in finding any association between the presence of psoriasis and EDI.23 Moreover, we found that psoriatic patients had a greater symptom severity of psychological distress as shown by General Severity Index (GSI) total score on the SCL-90-R. In addition they reported more somatization, depression, anxiety and paranoid ideation symptoms as showed on the relative subscales of SCL-90-R. These data are in accordance with literature. In particular, several studies reported the association between depression and psoriasis, with different opinions regarding the cause-effect relationship. In particular, recent studies define the major depressive disorder such as an inflammatory condition with elevated levels of pro-inflammatory cytokines,37 as well various autoimmune diseases, such as psoriasis. An interesting consideration that emerged from our study was the relationship between BMI and results of EDI in psoriatic people. In fact an association between the increasing weight and the worsening of EDI subscales was more frequent in the psoriasis group than in controls, through the Pearson correlation. With increasing BMI, the two groups showed an opposite trend in the two test scores. In particular, the 360 psoriatic group showed a worsening of eating disorder symptoms, assessed by the EDI subscales without deterioration of the psychopathological traits, detected by SCL-90-R. On the contrary, weight increase in the control group worsened the general psychological state. We may deduce that, in psoriatic patients, overweight/obesity is more frequently associated with an eating disorder than in general population. This hypothesis was also confirmed in our study by the comparison of patient and control obese subgroups, which showed, in patients with psoriasis, a higher prevalence of altered subscales in both questionnaires. However, these data have been not reported because referring to a very small sample of subjects. Moreover, this result is in accordance with a previous cross-sectional, randomized, and controlled trial, which evaluated the eating behaviors in 100 psoriatic patients, by the Eating Attitude Test, Beck Depression Inventory and Beck Anxiety Inventory, and a psychiatric interview. The authors found an higher prevalence of ED in patients with psoriasis and metabolic syndrome compared to the group of patients with psoriasis and without metabolic syndrome. Finally, our data indicates that there is not a correlation between the severity of somatic disease, assessed by PASI, and the patient psychological distress, indicated by GSI. It means that the impact of the psychological experience may not correlate with objective disease severity: in fact, even a mild-to-moderate involvement may have heavy psychological consequences. Limitations Because of some limitations, our study should be acknowledged as mainly hypothesis generating. First, our study population is relatively small. Second, patients were not evaluated by a psychiatrist, but they were only assessed by two self-rating scales. In fact, with these instruments, we may find the presence of symptoms related to an altered eating behavior. Then, further studies should include a psychiatric clinical interview in order to confirm a full diagnosis of BED according to the criteria of DSM-IV TR. Conclusions Our data show different associations between eating disorders and psoriasis, but they are not sufficient GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 EATING DISORDERS IN PSORIASIS to make a specific diagnosis. In patients with psoriasis, EDs seem to be associated with overweight/ obesity more frequently than in general population. This suggests the importance of suspecting by dermatologist the presence of an eating disorder in overweight/obese patients with psoriasis. When this comorbidity is found, a psychological approach to improve food control may help to lose weight and to increase response to therapy. References 1. Daudén E, Castañeda S, Suárez C, García-Campayo J, Blasco AJ, Aguilar MD et al. Integrated approach to comorbidity in patients with psoriasis. Working Group on Psoriasis-associated Comorbidities. Actas Dermosifiliogr 2012;1:1-64. 2. Sommer DM, Jenisch S, Suchan M, Christophers E, Weichenthal M. Increased prevalence of the metabolic syndrome in patients with moderate to severe psoriasis. Arch Dermatol Res 2006;298:3218. 3. Rahat SA, Gelfand JM. Psoriasis and metabolic disease: epidemiology and pathophysiology. Curr Opin Rheumatol 2008;20:416-22. 4. Christophers E. Comorbidities in psoriasis. Clin Dermatol 2007;25:529-34. 5. Gottlieb AB, Dann F. Comorbidities in patients with psoriasis. Am J Med 2009;122:1-9. 6. Armstrong AW, Harskamp CT, Armstrong EJ. The association between psoriasis and obesity: a systematic review and meta-analysis of observational studies. Nutr Diabetes 2012;2:e54. 7. Paller AS, Mercy K, Kwasny MJ, Choon SE, Cordoro KM, Girolomoni G et al. Association of pediatric psoriasis severity with excess and central adiposity: an international cross-sectional study. JAMA Dermatol 2013;149:166-76. 8. Sterry W, Strober BE, Menter A. Obesity in psoriasis: the metabolic, clinical and therapeutic implications. Report of an interdisciplinary conference and review. Br J Dermatol 2007;157:649-55. 9. Bremmer S, Van Voorhees AS, Hsu S, et al. Obesity and psoriasis: from the Medical Board of the National Psoriasis Foundation. J Am Acad Dermatol 2010;63:1058-69. 10. Stunkard AJ. Eating disorders and obesity. Psychiatr Clin North Am 2011;34:765-71. 11. Villarejo C, Fernández-Aranda F, et al. Lifetime obesity in patients with eating disorders: increasing prevalence, clinical and personality correlates. Eur Eat Disord Rev 2012;20:250-4. 12. American Psychiatric Association, Ed., Diagnostic and Statistical Manual of Mental Disorders. 5th edition, Washington, DC, USA; 2012. 13. Rieger E, Wilfley DE, Stein RI, Marino V, Crow SJ. A comparison of quality of life in obese individuals with and without binge eating disorder. Int J Eat Disord 2005;37:234-40. 14. Wilfley DE, Wilson GT, Agras WS. The clinical significance of binge eating disorder. Int J Eat Disord 2003;34:S96-S106. 15. Haves J, Koo J. Psoriasis: depression, anxiety, smoking and drinking habits. Dermatol Ther. 2010;23:174-80. 16. Kurd SK, Troxel AB, Crits-Christoph P. The risk of depression, anxiety and suicidality in patients with psoriasis: a population-based cohort study. Arch Dermatol 2010;146:891-5. Vol. 149 - No. 3 CROSTA 17. Russo PA, Ilchef R, Cooper AJ. Psychiatric morbidity in psoriasis: a review. Australas J Dermatol 2004;45:155-9. 18. Van Voorhees AS, Fried R. Depression and quality of life in psoriasis. Postgrad Med 2009;121:154-61. 19. Misery L. Depression and psoriasis. Ann Dermatol Venereol 2012;139:S53-7. 20. Kieć-Swierczyńska M, Dudek B, Krecisz B, SwierczyńskaMachura D, Dudek W, Garnczarek A et al. The role of psychological factors and psychiatric disorders in skin diseases. Med Pr. 2006; 57:551-5. 21. Parafianowicz K, Sicińska J, Moran A, Szumański J, Staniszewski K, Rudnicka L et al. Psychiatric comorbidities of psoriasis: pilot study Psychiatr Pol 2010;44:119-26. 22. Gupta MA, Gupta AK. Psychiatric and psychological co-morbidity in patients with dermatologic disorders: epidemiology and management. Am J Clin Dermatol 2003;4:833-42. 23. G Savron, R Montanaro, G Landi, G Bartolucci. Psychological aspects of patients with psoriasis and alopecia areata: a controlled study. Rivista di psichiatria 2001;36:135-45. 24. Altunay I, Demirci GT, Ates B, Kucukunal A, Aydın C, Karamustafalıoglu O et al. Do eating disorders accompany metabolic syndrome in psoriasis patients? Results of a preliminary study. Clin Cosmet Investig Dermatol 2011;4:139-43. 25. Kimball AB, Wu EQ, Guérin A, Yu AP, Tsaneva M, Gupta SR et al. Risks of developing psychiatric disorders in pediatric patients with psoriasis. J Am Acad Dermatol 2012;67:651-7.e1-2. 26. Fredriksson T, Pettersson U. Severe psoriasis--oral therapy with a new retinoid. Dermatologica 1978;157:238-44. 27. Garner DM, Olmsted MP, Polivy J. Development and validation of a multidimensional Eating Disorder Inventory for anorexia nervosa and bulimia. Int J Eating Dis 1983;2:15-34. 28. Milos G, Spindler A, Schnyder U. Psychiatric comorbidity and Eating Disorder Inventory (EDI) profiles in eating disorder patients. Can J Psychiatry 2004;49:179-80. 29. Derogatis LR. SCL-90-R, administration, scoring and procedures manual for the Revised version. Baltimore. Johns Hopkins University, School of Medicine; 1977. 30. Schauenburg H, Strack M. Die Symptom-Checklist-90-R zur darstellung von statistischen und klinisch signifikanten psychotherapieergebnissen. Psychother Psychosom Med Psychol 1998;48:257-64. 31. Schauenburg H, Strack M. Measuring psychotherapeutic change with the symptom checklist SCL-90-R. Psychother Psychosom 1999;68:199-206. 32. Rieder E, Tausk F. Psoriasis, a model of dermatologic psychosomatic disease: psychiatric implications and treatments. Int J Dermatol 2012;51:12-26. 33. Anzieu D. L’Io-pelle. Rome: Borla; 1987. 34. Anzieu D. L’epidermide nomade e la pelle psichica. Milan: Cortina; 1992. 35. Anzieu D. Il pensare. Dall’Io-pelle all’Io pensante, Borla, Roma 1996; 36. Anzieu D. Gli involucri psichici. Milan: Masson; 1997. 37. Elomaa AP, Niskanen L, Herzig KH, Viinamäki H, Hintikka J, Koivumaa-Honkanen H et al. Elevated levels of serum IL-5 are associated with an increased likelihood of major depressive disorder. BMC Psychiatry 2012;9:12:22. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. Received on May 8, 2013. Accepted for publication on September 20, 2013. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 361 CASE REPORTS G ITAL DERMATOL VENEREOL 2014;149:363-6 Periungual pyogenic granulomas due to topical tazarotene for nail psoriasis B. M. PIRACCINI, M. VENTURI, A. PATRIZI Tazarotene is a topically-applied, receptor-selective retinoid that has been shown to modulate several major pathogenic factors of psoriasis. Adverse effects are those of topical application of retinoids, the most common being mild to moderate burning, itching, stinging, and erythema, due to mild to moderate local skin irritation. While pyogenic granuloma–like lesions are a well recognized side effects of systemic retinoids, to our knowledge in the literature there is only one reported case of pyogenic granuloma (PG) following topical application of tazarotene for scalp psoriasis. In this paper we report 2 cases of periungual PGs following application of topical tazarotene and we present a review of the literature. Key words: Granuloma, pyogenic - Tazarotene - Nails - Psoriasis - Retinoids, adverse effects. T azarotene is a topically-applied, receptor-selective retinoid that has been shown to modulate several major pathogenic factors of psoriasis.1 Adverse effects are those of topical application of retinoids, the most common being mild to moderate burning, itching, stinging, and erythema, due to mild to moderate local skin irritation.2 While pyogenic granuloma-like lesions are a well recognized side effects of systemic retinoids,3-5 to our knowledge in the literature there is only one reported case of pyogenic granuloma (PG) following topical application of tazarotene for scalp psoriasis.3 In this paper we report 2 cases of periungual PGs following application of topical tazarotene and we present a review of the literature. Corresponding author: B. M. Piraccini, Division of Dermatology, Department of Experimental, Diagnostic and Specialty Medicine, University of Bologna, Via Massarenti 1, 40138 Bologna, Italy. E-mail: [email protected] Vol. 149 - No. 3 Division of Dermatology, Department of Experimental, Diagnostic and Specialty Medicine University of Bologna, Bologna, Italy Case series Case 1.—A 77-year-old woman presented with nail psoriasis involving all the nails of both hands. She had been treated with calcipotriol+betamethasone ointment once daily for six months with no benefit, so the patient was commenced on tazarotene 0.1% gel once daily. Three months after the beginning of this therapy, numerous periungual PG-like lesions appeared in the areas treated with the topical retinoid (Figure 1). The lesions had a diameter ranging from 0.5 to 1.5 cm and were very painful. The diagnosis of PGs was clinical. It was decided to stop the tazarotene and to start a topical treatment with clobetasol propionate ointment twice daily applied under occlusion in the evening. Two weeks later the lesions regressed. She was advised to continue her treatment regimen only with calcipotriol betamethasone ointment. Case 2.—A 39-year-old man presented with nail psoriasis, developed one year before in the hands. The patient was treated with tazarotene 0.1% gel once daily. Two months after the beginning of the topical retinoid, a PG appeared in the II digit of left hand (Figure 2). The lesion was mildly painful, had a diameter of no more than 0.5 cm, but with a tendency to enlarge. A skin biopsy was not performed because clinical features were already suggestive of PG. The patient was recommended to stop tazarotene. Two weeks later, the lesion was still present but was improving. PG healed over the next 4 weeks. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 363 PIRACCINI PERIUNGUAL PYOGENIC GRANULOMAS DUE TO TOPICAL TAZAROTENE FOR NAIL PSORIASIS Figure 1.—Numerous periungual PGs in the areas treated with tazarotene. Figure 2.—A PG appeared in the II digit of left hand treated with the topical retinoid. Discussion Nail PG is a relatively common acquired benign vascular tumour often seen as an emergency because 364 of its tendency to bleed.6 Nail PGs are due to different causes and, according to the pathogenesis, they have been classified by Piraccini et al.6 in PGs due to drugs, local mechanical trauma, peripheral nerve injury and inflammatory systemic diseases. Histopathology shows similar features in every type of PGs, irrespective of cause and location, but, when PG is single, especially if the nail bed is involved, histological examination is necessary to rule out malignant melanoma.6 Treatment must be chosen according to the etiology, but a first line approach involves the application of topical steroids and antibiotics or curettage.6 If PGs are due to drugs, topical medication or curettage may be effective, but, usually, a decrease in the dose or a suspension of the drug is required.6 The drugs that mostly induce periungual and subungual PGs are retinoids (systemic isotretinoin, systemic etretinate, systemic acitretin), antiretrovirals (indinavir, lamivudine), antineoplastic and immunosuppressive drugs (epidermal growth factor receptor inhibitors, capecitabine, cyclosporin, docetaxel, mitoxantrone).6 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 PERIUNGUAL PYOGENIC GRANULOMAS DUE TO TOPICAL TAZAROTENE FOR NAIL PSORIASIS In this paper we present 2 cases of PGs linked to topical tazarotene. An association between oral retinoids and the development of PG-like lesions is well known and substantiated by recurrence of the lesions with rechallenge of the suspected agent.3-6 On the other hand, cases of PGs after topical retinoids are only published as single case reports. The first case of PGs as a side effect of topical tretinoin for acne was published in 1979,7, 8 and 10 years later multiple PGs on a patient’s scalp treated with a combination of topical minoxidil and retinoic acid 5, 9 were reported. Another patient developed a PG-like reaction during treatment with oral isotretinoin for acne, and later PGs appeared on his chest after the use of topical tretinoin.4, 5 Therefore, the autohors 4 suggested that care should be taken if a topical retinoid is considered for maintenance therapy, because it can lead again to development of new PG-like lesions.4 In addition, care should be used to avoid application of tretinoin cream to open oozing skin, because of the possible onset of PG-like reaction.4 In the literature only one case of PG has been associated to topical tazarotene treatment during a controlled clinical trial of tazarotene 0.1% gel for scalp psoriasis.3 Tazarotene is a third-generation acetylenic, retinoid prodrug.1, 2 It focuses its activity on the predominant retinoic acid receptor (RAR) subtypes in the skin, RAR γ and RAR β, and has little or no interaction with other ubiquitous retinoid receptor types expressed elsewhere in the body.1 Adverse effects are typical of topical retinoids, the most common being mild to moderate local irritation with burning or itching and erythema.1, 2 Local irritation after tazarotene application for nail psoriasis (of the lateral folds or of the distal pulp) 11, 12 is usually manageable and transient and clearly dose-related.1, 2 Other side effects reported are peeling of the proximal nail fold,10, 11 desquamation 11 and paronychia.10, 11 The use of tazarotene for nail psoriasis was fist suggested by Scher et al.10 in 2001. Later, several papers have confirmed its efficacy on nail psoriasis and its good tolerability, even in children.11-14 Finally, in 2012, the therapeutic value and safety of tazarotene in a hydrophilic ointment formulation for the management of nail psoriasis have been proved in an open observational study.14 Our 2 patients with nail psoriasis improved after topical application of tazarotene gel, but they developed periungual PGs after 2 and 3 months of therapy. Vol. 149 - No. 3 PIRACCINI These are the first 2 cases of PGs due to tazarotene localized to the nail tissues, and this is also the first report of periungual PGs following tazarotene therapy for nail psoriasis. Although 2 cases do not permit to draw conclusions about the latency of onset of PGs after the beginning of cure, it is important to point out that our patients developed periungual PGs later than the other cases due to topical retinoids reported in the literature. The latency before onset of tazarotene-induced PG in the case presented by Dawkins et al.3 was 2 weeks, as was that of PGs in patients treated with a different topical retinoid (tretinoin cream).4, 7, 8 PGs due to systemic retinoids appear after about 3 months of treatment (ranging from 3 to 12 weeks),3, 6 so Teknetzis et al.8 suggested that PGs due to topical retinoids seem to develop earlier than those in the case of oral isotretinoin treatment. Consequently, it was suggested that caution in the topical use of these drugs may be warranted particularly during the first 2-3 weeks of treatment.8 Conclusions PGs in our patients occurred after 2 and 3 months of tazarotene application. So it is likely that Dermatologists will encounter similar side effects associated to topical retinoids also after a long period of treatment. Therefore they should continue a particular surveillance during the whole treatment time and not only in the first weeks. References 1. Marks R. Clinical safety of tazarotene in the treatment of plaque psoriasis. J Am Acad Dermatol 1997;37(2 Pt 3):S25-32. 2. Krueger GG, Drake LA, Elias PM, Lowe NJ, Guzzo C, Weinstein GD, et al. The safety and efficacy of tazarotene gel, a topical acetylenic retinoid, in the treatment of psoriasis. Arch Dermatol 1998;134:57-60. 3. Dawkins MA, Clark AR, Feldman SR. Pyogenic granuloma-like lesion associated with topical tazarotene therapy. J Am Acad Dermatol 2000;43:154-5. 4. MacKenzie-Wood AR, Wood G. Pyogenic granuloma-like lesions in a patient using topical tretinoin. Australas J Dermatol 1998;39:248-50. 5. Pierson JC, Owens NM. Pyogenic granuloma-like lesions associated with topical retinoid therapy. J Am Acad Dermatol.2001;45:967-8. 6. Piraccini BM, Bellavista S, Misciali C, Tosti A, De Berker D, Richert B. Periungual and subungual pyogenic granuloma. Br J Dermatol 2010;163:941-53. 7. Hegeborn M, Kirechner S. Multiple granulomata pyogenica bei acne vulgaris. Dermatologica 1979;158:93-8. 8. Teknetzis A, Ioannides VD, Vakali G, Lefaki I, Minas A. Pyogenic granulomas following topical application of tretinoin. J Eur Acad Dermatol Venereol 2004;18:337-9. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 365 PIRACCINI PERIUNGUAL PYOGENIC GRANULOMAS DUE TO TOPICAL TAZAROTENE FOR NAIL PSORIASIS 9. Baran R. Explosive eruption of pyogenic granuloma of the scalp due to topical combination therapy of minoxidil and retinoic acid. Dermatologica 1989;179:76-8. 10. Scher RK, Stiller M, Zhu YI. Tazaroteno 0 1% gel in the treatment of fingernail psoriasis: a double-blind, randomized, vehiclecontrolled study. Cutis. 2001;68:355-8. 11. Bianchi L, Soda R, Diluvio L, Chimenti S. Tazarotene 0.1% gel for psoriasis of the fingernails and toenails: an open, prospective study. Br J Dermatol. 2003;149:207-9. 12. Rigopoulos D, Gregoriou S, Katsambas A. Treatment of psoriatic nails with tazarotene cream 0.1% vs clobetasol propionate 0.05% cream: a double bind study. Acta Derm Venereol. 2007;87:167-8. 13. Diluvio L, Campione E, Paternò EJ, Mordenti C, El Hachem M, 366 Chimenti S. Childhood nail psoriasis: a useful treatment with tazarotene 0.05%. Pediatr Dermatol. 2007;24:332-3. 14. Fischer-Levancini C, Sánchez-Regaña M, Llambí F, Collgros H, Expósito-Serrano V, Umbert-Millet P. Nail psoriasis: treatment with tazarotene 0.1% hydrophilic ointment. Actas Dermosifiliogr 2012;103:725-8. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. Received on December 11, 2012. Accepted for publication on March 11, 2013. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 G ITAL DERMATOL VENEREOL 2014;149:367-70 Multiple skin ulcers due to Serratia marcescens in an immunocompetent patient M. CARLESIMO 1, A. PENNICA 2, M. MUSCIANESE 1, U. BOTTONI 3, C. ABRUZZESE 1, M. GIUBETTINI 1, G. PRANTEDA 4, G. PRANTEDA 1 Serratia marcescens is a species of gram negative bacillus, classified as a member of the Enterobacteriaceae, mainly involved in opportunistic infections, particulary in the hospital environment. Cutaneous infections have rarely reported in literature and are predominantly observed in elderly or in immunocompromised patients. The clinical manifestations of skin infections include granulomatous lesions, necrotizing fasciitis, nodules, cellulitis, ulcers, dermal abscesses. Infections caused by S. marcescens may be difficult to treat because of resistance to a variety of antibiotics, including ampicillin and first and second generation cephalosporins. Aminoglycosides have good activity against S. marcescens, but resistant strains have also been described. We report a very intriguing case of S. marcescens infection, in an immunocompetent 18-year-old man, causing multiple rounded ulcers of varying sizes, along with few pustular lesions that both clinically and histopathologically mimic a pyoderma gangrenosum (PG). This is a non infectious neutrophilic skin disorder, characterized by painful and rapidly progressing skin ulceration. According to our experience, we would strongly recommend to perform cultures of multiple skin ulcers resembling PG, even in young healthy patients, to ensure correct diagnosis and treatment, since resistant to conventional antibiotics bacteria such as S. marcescens may be the cause of these lesions, like in the case here reported. Key words: Pyoderma gangrenosum - Immunocompetence Serratia marcescens. S erratia marcescens was originally considered to be an innocuous saprophytic organism. Since the first reported S. marcescens infection in 1951,1 Corresponding author: G. Pranteda, MD, Operative Unit of Dermatology, NESMOS Department, Faculty of Medicine, La Sapienza University of Rome, Via di Grottarossa 1039, 00189 Rome, Italy. E-mail: [email protected] Vol. 149 - No. 3 1Operative Unit of Dermatology, NESMOS Department Faculty of Medicine and Psychology, “Sapienza” Sant’Andrea Hospital, Rome, Italy 2Operative Unit of Infective Diseases Faculty of Medicine and Psychology “Sapienza” Sant’Andrea Hospital, Rome, Italy 3Department of Health Sciences “Magna Graecia” University, Catanzaro, Italy 4Operative Unit of Dermatology Faculty of Medicine and Dentistry “Sapienza”, Umberto I Hospital, Rome, Italy similar cases have been reported with increasing frequency. S. marcescens is mainly involved in nosocomial infections, particularly urinary and lower respiratory tracts infections, as well as surgical wounds. Cutaneous infections are predominantly observed in immunocompromised patients or in patients affected by chronic debilitating disorders.2 We report a very rare case of multiple skin ulcers (MSU) caused by S. marcescens in an immunocompetent 18-year-old male. Case report A 18-year-old romanian student was admitted to our Department because of multiple rounded ulcers in absence of systemic symptoms. The current lesions began one year before as a small pustule and ruptured rapidly to form deep and painful ulcers. In Romania, he underwent a histological examination, which showed a diagnosis of pyoderma gangrenosum (PG), thus the patient underwent GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 367 CARLESIMO Skin ulcers due to S. marcescens in an immunocompetent patient Figure 1.—A) Multiple ulcerative lesions, some of which are fused together, on the right leg. These oozing and crusting ulcers were characterized by well-defined erythematous to violaceous borders. Pieces of necrotic epidermidis are attached on borders and in the center of lesions; B) close up of some fused lesions in which necrotic and crusting aspects are evident. prednisone (35 mg daily) and dapsone (75 mg daily for six days a week) for three months. Despite treatment was replaced with sulfamethoxazole-trimethoprim and minocyclin when relapses recurred, no healing was obtained. Worsening of lesions prompted admission to our Departement six months later. He was apyrexial and physical exhamination showed multiple painful and deep ulcers with well-defined erythematous to violaceous borders on the lower legs, the trunk and the upper limbs with an inguinal and axillary associated lymphadenopathy (Figure 1). Mucous membranes were not involved. His past medical hystory was unremarkable. Result of routine laboratory examinations were within normal range, except for a slight normochromic normocytic anemia (hemogobin: 11.6 g/dL) increased C-reactive protein (C-RP 6.36 mg/ dL) and erythrocyte sedimentation rate (ESR 67 mm/h) values. All the other laboratory tests were within normal ranges or negative. All instrumental investigations were normal. We performed a cultural and histological examination that showed chronic inflammatory infiltrates in the superficial dermis with acanthosis and pseudoepitheliomatous hyperplasia of epidermidis, focal abscessual areas surrounded by a zone of granulomatous inflammation, and features of leucocytoclastic vasculitis (Figure 2). The microbiology report indicated growth of the bacterium S. marcescens sensitive to ciprofloxacin, gentamicin and cefotaxime. Thus, the patient was treated with eradication therapy with intravenous ciprofloxacin (800 mg daily for five days), then oral ciprofloxacin (1000 mg daily for 30 days) with a significant improvement. At 3-month follow up, the ulcers had reduced in size and active healing and atrophic scar were present. The normalization of inflammatory markers was observed too. There was no evidence of recurrence during 12 months of follow-up however a long-term follow-up is recommended in order to detect an underlying immunodepression. 368 Discussion In the last decades S. marcescens has become of interest since its ability to cause serious infections. It is a facultative anaerobe with good survival abilities even in hostile conditions. Consequently, it can act as a nosocomial agent. It is often involved in urinary and lower respiratory tract infections, and surgical wounds infections. The incidence of cutaneous infections caused by S. marcescens is extremely low and in most such istances are observed in immunodepressed patients. Clinical manifestations include granulomatous lesions, fasciitis, nodules, cellulitis, ulcers and dermal abscesses.2 This case is intriguing since it is a case of S. marcescens infection, in an immunocompetent 18-yearold man, causing ulcerative lesions in which histopathological examination was consistent with PG-like lesion. In our case the patient presented lesions both clinically and histopathologically similar to PG, a non infectious neutrophilic skin disorder3. Nevertheless, a culture examination revealed an infection by S. marscences. Absence of underlying diseases commonly associated to PG (inflammatory bowel disease, polyarthritis, immune deficiency status and hematologic disorders), and healing of lesions after antibiotic therapy are both elements that support a non-secondary infection. Thus, in the case here reported, S. marcescens is the etiologic agent of these lesions. To the best of our knowledge this is one of the few reported cases of PG-like le- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 Skin ulcers due to S. marcescens in an immunocompetent patient CARLESIMO Figure 2.—A) Zoned acute and chronic inflammatory infiltrates in the superficial dermis with acanthosis and pseudoepitheliomatous hyperplasia of epidermidis (Haematoxylin and eosin, original magnification 30x); B) visible focal abscessual areas surrounded by a zone of granulomatous inflammation bordered by a rim of lymphocytes and plasma cells (Haematoxylin and eosin, original magnification 160x); C) features of leucocytoclastic vasculitis probable of secondary meaning (Haematoxylin and eosin, original magnification 400x). sions linked to S. marcescens infection in a young immunocompetent patient, who is probably genetically predisposed. In literature, cutaneous lesions similar to those in our patient have been linked to Helicobacter Cinaedi in a patient affected by a primary immunodeficiency.4 We strongly recommend the early consideration of infection by uncommon Vol. 149 - No. 3 bacteria such as S. marcescens also in immunocompetent young patients, since its recognition and treatment with a prolonged antibiotic therapy can lead to clinical improvement. Therefore it is always advisable to perform an easily obtainable cultural examination of MSU since this finding can modulate the therapy. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 369 CARLESIMO Skin ulcers due to S. marcescens in an immunocompetent patient References 1. Wheat, RP, Zuckerman, A, Rantz, LA. Infection due to Chromobacteria: report of eleven cases. Arch Intern Med 1951;88:461-6. 2. Marzano AV, Gasparini G, Caputo R. Cutaneous infection caused by Serratia marcescens. Cutis 2000;66:461-3. 3. Powell FC, Su WP, Perry HO. Pyoderma gangrenosum: classification and management. J Am Acad Dermatol 1996;34:395-409; 4. Dua J, Elliot E, Bright P, Grigoriadou S, Bull R, Millar M, Wijesu- 370 riya N, Longhurst HJ. Pyoderma gangrenosum-like ulcer caused by Helicobacter cinaedi in a patient with x-linked agammaglobulinaemia. Clin Exp Dermatol 2012;37:642-5 Presented at the 87th SIDeMaST Congress, 21-24 November 2012. Conflicts of interest.—The authors certify that there is no conflict of interest with any financial organization regarding the material discussed in the manuscript. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 CORRESPONDENCE A case of superimposed segmental giant melanocytic nevus TO THE EDITOR: Giant congenital melanocytic nevi (CMN) are congenital pigmented lesions affecting 1 in 20,000 live births, defined by surface diameter measuring 20 cm or more.1 Giant CMN show a high risk of developing malignant melanomas and are often associated with leptomeningeal melanocytosis.2 A full-term neonate was referred to our outpatient clinic for the evaluation of an extensive congenital skin pigmentation. Physical examination showed the presence of a main segmental nevus affecting the right lower limb associated with diffuse smaller round-to-oval nevi variable in diameter affecting scalp, face, trunk, and limbs (Figure 1). A diagnosis of superimposed segmental giant CMN was made on the basis of clinical findings and confirmed by histopathology. Magnetic resonance imaging (MRI) of the brain and spine was negative for melanosis or thickening of the leptomeninges. Several polygenic skin disorders, including psoriasis, atopic dermatitis, vitiligo, etc, are known to present in a pronounced segmental or linear arrangement often associated with a less severe non-segmental involvement.3 This pattern of clinical presentation has been defined as “superimposed segmental manifestation of a polygenic skin disorder”.3 In analogy to mendelian skin disorders, it may be explained by the concept of loss of heterozygosity (LOH),3, 4 i.e., a genetic mechanism by which a somatic cell becomes heterozygous if one allele is lost or homozygous if both alleles of the same gene or both chromosomal loci are lost.4 The etiology of giant CMN is still unknown, even if molecular studies, regarding both congenital and acquired melanocytic nevi, have recently identified common polygenic mutations involving loci of BRAF, N-ras, MC1R, and p53.5 In analogy to what mentioned above, our case can be considered a clear example of superimposed segmental manifestation of a polygenic skin disorder. Both giant CMN and smaller melanocytic nevi rise from a postzygotic mutational event, which happens earlier in giant CMN and later in nevi. In fact, while the main segmental nevus affecting the right lower limb would be the result of a LOH occurring in a precocious phase of a heterozygous embryo development, scattered smaller melanocytic nevi Figure 1.—A) Main segmental nevus affecting the right lower limb associated with diffuse smaller round-to-oval nevi; B) particular of the scalp. Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 371 CORRESPONDENCE would represent the result of the background heterozygous mutation probably occurring in a post-zygotic phase of the development of an otherwise healthy embryo. Recently, Happle has reviewed several historical cases of giant CMN associated with small disseminated nevi and has hypothesized that they could be categorized as “superimposed patchy manifestations of a polygenic disorder”, because the term “segmental” was not always appropriate to define the revised cases.5 Conversely, in our case, “segmental” is the best adequate adjective to describe the particular pattern of presentation of the giant CMN. To the best of our knowledge, excluding the historical cases revised by Happle,5 this is the first original case of giant CMN presenting as a superimposed segmental manifestation of a polygenic skin disorder, again confirming the geniality and the originality of the theory on ‘superimposed skin disorders’ proposed by Happle to explain these diseases. V. PICCOLO Department of Dermatology and Venereology, Second University of Naples, Naples, Italy [email protected] T. RUSSO Department of Dermatology and Venereology, Second University of Naples, Naples, Italy R. PICCIOCCHI Pediatric Dermatology Unit, A.O.R.N. Santobono-Pausillipon, Naples, Italy O. AMETRANO Pediatric Dermatology Unit, A.O.R.N. Santobono-Pausillipon, Naples, Italy E. MOSCARELLA Skin Cancer Unit, Arcispedale S. Maria Nuova, IRCCS Reggio Emilia, Italy G ITAL DERMATOL VENEREOL 2014;149:371-2 References 1. Kopf AW, Bart RS, Hennessey P. Congenital nevocytic nevi and malignant melanomas. J Am Acad Dermatol 1979;1:123-30. 2. Danarti R, König A, Happle R. Large congenital melanocytic nevi may reflect paradominant inheritance implying allelic loss. Eur J Dermatol 2003;13:430-2. 3. Happle R. Superimposed segmental manifestation of polygenic skin disorders. J Am Acad Dermatol 2007;57:690-9. 4. Happle R. Loss of heterozygosity in human skin. J Am Acad Dermatol 1999;41:143-61. 5. Happle R. Giant melanocytic nevus may be explained as a superimposed patchy manifestation of a polygenic trait. Dermatology 2010;221:30-3. Lymphangiomas arising on lymphedema: first step of malignant development TO THE EDITOR: A 45-year-old woman presented to our department with a crop of papular lesions that had appeared on her left limb over the last 2 months, at first on the thigh and then on the leg. The lesions were light brown, slightly prominent and translucid, smooth, rounded, with regular edges and painless. The same limb was markedly lymphedematous due to primary lymphedema precox, which had been diagnosed through lymphoscintigraphy about 6 years before. This investigation had disclosed, on the left, a failed flow of the radiocolloid, a congenital lack of iliac and lumbar-aortic lymph nodes as well as a great “dermal back flow”. The clinical diagnosis of lymphangioma arisen on lymphedema was suspected (Figure 1). A punch biopsy showed normal epidermis lying on a degenerated collagen tissue, vascular cavities coated by lymphatic endothelium and stuffed of lymphoid cells along with spots of amorphous material. No mitotic figures and cellular pleomorphism were seen (Figure 2). The structural pattern was compatible with the diagnosis of fibrolymphangioma. This case is of interest because it is a clear example of the three steps theory postulated by McConnel and Haslam 372 in 1956.1 They described 3 cases of angiosarcoma and 2 of lymphangiomatosis arisen on lymphedematous arms (due to radical mastectomy) and reviewed of the literature, thus finding cases where angiosarcomas had arisen in lymphedematous extremities also in the absence of any previous history of malignancies. On this basis, they recognized the long-standing lymphedema (rather than a malignant diathesis) as the main etiological factor and then, from the histological study, they drew the typical development of the lesions in three phases. The first stage is lymphedema accompanied by widespread degeneration of subcutaneous and dermal collagen and, to a lesser extent, degeneration of fatty tissue, as well as lymphocytic cuffing of small blood vessels, particularly those at the lower edge of the dermis. The second stage is that of premalignant angiomatosis, i.e., a multifocal proliferation of endothelial cells in the lower dermis and subcutaneous tissue, which in the larger and more superficial areas appear on the surface as bruises or vesicles. Many of these proliferating vessels seem to be arisen from lymphatics and often they form anastomosing plexus or cavernous spaces filled with lymphocytes. In our patient we GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 CORRESPONDENCE Figure 2.—Normal epidermis lying on a degenerated collagen tissue, lymph spaces and ectasic lymph vessels (Hematoxylin and eosin stain, 200X). Figure 1.—Multiples lymphangiomas on the markedly lympheodematous left limb. found a perfect matching of all these features, as described above. The third stage described by McConnell and Haslam is frankly malignant angiosarcoma; therefore, considering the high risk of the patient, we scheduled an intensive follow-up. Although the authors defined the relationship between edema and malignancy as obscure, to date, with the collection of new cases and the increased knowledge, we might recognize the cause of malignancy in the reduced antineoplastic immune surveillance due to the hampering of the regular lymph flow including the normal trafficking of immune cells. There is laboratory evidence confirming the presence of impaired lymphocytes and Langerhans cells trafficking in patients with obstructive lymphedema of the lower extremities, which makes the lymphedematous region an immunologically vulnerable site for the development of neoplasms.2, 3 In fact, the impossibility to scavenge potential neoplastic cells has a role in the growth of malignancies even more important of the degeneration of the connective tissue resulting from the severe lymphedema. This could explain also the unique but significant case of a squamous cell carcinoma (SCC) arisen within lymphangioma circumsciptum.4 SCC comes from a different precursor cell that should not be involved in the degeneration process caused by lymphostasis. In this light, we can add this case to the Vol. 149 - No. 3 expanding chapter of the immunocompromised district: a cutaneous site that has been damaged and immunologically “marked” by a variety of clinical events, such as chronic lymphedema, herpetic infections, vaccination, ionizing or UV radiation, thermal burns, or trauma.4 After the cause of event has disappeared, the affected district may either appear clinically normal or show cutaneous changes, but its immune behaviour is often compromised forever. An immunocompromised district becomes a site that is particularly susceptible to subsequent outbreaks of opportunistic infections, tumours and immunity-related disorders, often confined to the district itself. The reason for the anomaly of the local immune control may reside in locally hampered lymph drainage (as typically occurs in chronic lymphedema), or in locally altered neuromediator signalling (as it typically occurs in herpes zoster infection) or in the concomitant two condition (as it typically occurs in amputation stumps and radiation dermatitis).5 The case we present here fits this novel concept perfectly, since the appearance of premalignant lymphangioma affects the lymphedematous limb only. A. LO SCHIAVO Department of Dermatology, Second University of Naples, Naples, Italy G. BRANCACCIO Department of Dermatology, Second University of Naples, Naples, Italy [email protected] F. ROMANO Department of Dermatology, Second University of Naples, Naples, Italy GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 373 CORRESPONDENCE S. CACCAVALE Department of Dermatology, Second University of Naples, Naples, Italy G ITAL DERMATOL VENEREOL 2014;149:372-4 References 1. McConnell EM, Haslam P. Angiosarcoma in post-mastectomy lymphoedema; a report of 5 cases and a review of the literature. Br J Surg 1959;46:322-32. 2. Mallon E, Powell S, Mortimer P, Ryan TJ. Evidence for altered cellmediated immunity in postmastectomy lymphoedema. Br J Dermatol 1997;137:928-33. 3. Ruocco V, Schwartz RA, Ruocco E. Lymphedema: an immunologically vulnerable site for development of neoplasms. J Am Acad Dermatol 2002;47:124-7. 4. Wilson GR, Cox NH, McLean NR, Scott D. Squamous cell carcinoma arising within congenital lymphangioma circumscriptum. Br J Dermatol 1993;129:337-9. 5. Ruocco V, Brunetti G, Puca RV, Ruocco E. The immunocompromised district: a unifying concept for lymphoedematous, herpes-infected and otherwise damaged sites. J Eur Acad Dermatol Venereol 2009;23:1364-73. A rare association between neurofibromatosis type 1 and vulvar sarcoma TO THE EDITOR: Neurofibromatosis type 1 (NF1) is a rare genetic disorder sporadic or genetically transmitted in autosomal dominant fashion with an estimated incidence of 1:3000-4000 live births. Clinical diagnostic criteria are well established, with patients needing two or more of the following: six or more café-au-lait spots, two neurofibromas or one plexiform neurofibroma, axillary or groin freckling, optic glioma, two Lisch nodules, bone dysplasia and first-degree relative with NF1. Susceptibility to neoplastic transformation is the main feature of the disease with a probability from 3 to 4 times greater than the general population to develop both benign and malignant tumors, supporting the classification of NF1 as a tumor predisposition syndrome. In addition to neurofibromas, optic pathway glioma, pheochromocytoma and leukemia, certain sarcomas are more frequent in NF1 patients than in the general population, most commonly malignant peripheral nerve sheath tumour (MPNST) and rhabdomyosarcoma.1 Sarcomas rarely involve the female genital tract; the uterus is primarily involved (90% of cases). The vulva is a rare site of presentation for primary malignant tumours; more commonly it is a site of metastasis or direct extension from tumours originating in other genital sites such as the cervix or endometrium, or from extragenital sites, including the rectum and bladder. Vulvar sarcomas are uncommon, comprising only approximately 2% of all vulvar malignancies.2 We report the first occurrence of a malignant, high grade, non differentiated vulvar sarcoma in a patient with NF1. A 44-year-old female with a previous diagnosis of NF1 was referred to our Department for the presence of a large vulvar mass, rapidly increasing in size over the last two years. Clinical examination revealed a large, nodular and exophytic mass, easily bleeding, painful, partially necrotic and 374 friable, involving the right side of the vulva (Figure 1). The surrounding skin appeared intensely erythematous and the inguinal lymph nodes were palpable bilaterally. Pelvic MRI revealed a large parenchymatous mass, (12×10×10 cm), localized in the median and paramedian vulva, with extra-vulvar development, showing inhomogeneous structure and containing cystic necrotic areas. The patient underwent a right hemivulvectomy. Histopathologic examination revealed a highly cellular, malignant tumor invading the skin and the subcutaneous tissue, composed of sheets of spindle-shaped cells provided with ovalar nuclei and weakly eosinophilic cytoplasm. In places the tumor cells were arranged in a herringbone pattern, though most part of the tumor showed no definite cell arrangement. A minor proportion of the tumor included small, rounded cell elements with abundant deeply eosinophilic cytoplasm and polar nuclei, reminiscent of rhabdomyosarcoma. Scarce fibrillary stroma was interspersed among the tumor cells. Extensive intratumoural necrosis and high mitotic index (30 mitoses/HPF) were observed (Figure 2). The tumor cells immunoreacted only with vimentin, showing no staining with a large panel of antibodies, including S-100 protein, cytokeratin 5/6 and 7, EMA, desmin, CD117, thrombomodulin, smooth muscle actin, myoglobin, neurofilaments, striated muscle actin, HMB45, Melan A, calretinin and CD34. Based on the morphologic and immunohistochemical results, a diagnosis of malignant, high grade non differentiated sarcoma, with fibrosarcoma-like areas was rendered. Postoperatively, the patient received adjuvant chemotherapy and she died three months later because of lung metastases’ presence. More than fifty histologic adult soft tissue sarcoma subtypes exist and they display a wide spectrum of clinical activities ranging from relatively slow-growing lesions to aggressive locally and regionally destructive lesions with potential for systemic metastasis. Furthermore, many of GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 CORRESPONDENCE Figure 2.—Histological appearance of the para-vulvar sarcoma in this NF1 patient. Tumour cells are arranged in a herringbone pattern, resembling a fibrosarcoma (Hematoxylin-eosin, 100x). Figure 1.—A large, nodular and exophytic mass, easily bleeding, painful, partially necrotic and friable, involving the right side of the vulva. these subtypes can occur at any age and in every part of the body.3 As to the vulva, Davos published a series of 16 vulvar sarcomas in non NF1 patients. Five were leiomyosarcoma; other sarcomas were malignant fibrous histiocytomas, one of which represented a dermatofibrosarcoma protuberans, and one each of fibrosarcoma, hemangiosarcoma, malignant hemangiopericytoma, epithelioid sarcoma, malignant schwannoma, malignant mesothelioma, and embrional rhabdomyosarcoma.2 The commonest site of origin was the labium majus (64%), followed by the posterior fourchette and by the deep vulvar tissues adjacent to Bartholin’s gland. In our case, the histological examination pointed to an undifferentiated pleomorphic sarcoma (UPS). This term is used for the classification of sarcomas that show no definable line of differentiation by histological, immunohistochemical, ultrastructural or molecular criteria. Overall 5-year survival of patients with UPS has been roughly 50%. Local surgical resection is the treatment of choice and negative margins are particularly important. The role of adjuvant chemotherapy and radiation is also unclear. The differential microscopical diagnosis in the present case was mainly with a MPNST, also referred to as malignant schwannoma, malignant neurilemmoma or neurofibrosarcoma, which resembles routine fibrosarcoma in its overall organization. However, comma-shaped Schwann Vol. 149 - No. 3 cells were not demonstrable by both light microscopy examination and using S-100 antibody. In addition, there was no evidence of nuclear palisading. Despite morphological hints of focal rhabdomyoblastic differentiation in the tumour, such those characteristically observed in Triton tumour, no immunoreactivity for striated muscle actin antibody was present. Nevertheless, MPNST cannot be entirely ruled out as this malignancy is known to be “one of the most difficult and elusive diagnoses in soft tissue diseases”. However, the occurrence of a MPNST in the vulvar area in extremely uncommon as the lesion is usually found in the lower extremities and head and neck region. Three cases of endocervical fibroblastic MPNST have recently been described in non-NF1 patients. However, these tumours differed from the present case in that they showed fibrocyte-like differentiation, as demonstrated ultrastructurally and by positive immunoreaction of tumour cells with both S-100 and CD 34.4 The association of non neurogenic sarcomas and NF1 is rarely described in literature. Zöller found two cases of leiomyosarcoma among 70 patients with NF1. Synovial sarcoma and gastrointestinal stromal tumour are also becoming increasingly recognized in association with NF1, and sporadic cases of malignant fibrous histiocytoma have been described in these patients.5 We describe a NF1 patient affected by a vulvar pleomorphic high grade undifferentiated sarcoma to underline the uncommon association and the presence of a rare sarcoma in an atypical setting such as the vulva. As NF1 patient may die at a young age after the onset an associated malignancy, it is important to examine routinely these patients in order to have an early diagnosis and treatment for a better outcome. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 375 CORRESPONDENCE E. MIRAGLIA Department of Dermatology, La Sapienza University of Rome, Policlinico Umberto I, Rome, Italy [email protected] I. PECORELLA Department of Experimental Medicine and Pathology, La Sapienza University of Rome, Policlinico Umberto I, Rome, Italy F. PERSECHINO Department of Dermatology, La Sapienza University of Rome, Policlinico Umberto I, Rome, Italy B. VISCONTI Department of Dermatology, La Sapienza University of Rome, Policlinico Umberto I, Rome, Italy S. CALVIERI Department of Dermatology, La Sapienza University of Rome, Policlinico Umberto I, Rome, Italy S. GIUSTINI Department of Dermatology, La Sapienza University of Rome, Policlinico Umberto I, Rome, Italy G ITAL DERMATOL VENEREOL 2014;149:374-6 References 1. de Oliveira MG, Pozatti Moure S, Sérgio Batista P, Moraes Chaves AC, Rados PV, Sant’Ana Filho M. NF1 diagnosis criteria and associated sarcomatous tumor review of the literature and case report. Oral Maxillofac Surg 2008;12:231-5. 2. Davos I, Abell MR. Soft tissue sarcomas of vulva. Gynecol Oncol 1976;4:70-86. 3. Dei Tos AP Classification of pleomorphic sarcomas: where are we now? Histopathology 2006;48:51-62. 4. Mills AM, Karamchandani JR, Vogel H, Longacre TA. Endocervical fibroblastic malignant peripheral nerve sheath tumor (neurofibrosarcoma): report of a novel entity possibly related to endocervical CD34 fibrocytes. Am J Surg Pathol 2011;35:404-12. 5. Zöller ME, Rembeck B, Oden A, Samuelsson M, Angervall L. Malignant an benign tumors in patients with neurofibromatosis type 1 in a defined Swedish population. Cancer 1997;79:2125-31. A clinical case of cutaneous silica granuloma TO THE EDITOR: Silica granuloma occurs as a consequence of the introduction in the skin of silicon dioxide, usually after injury. It was first described by Shattock in 1916 as a pseudotuberculoma silicoticum and later by Faulds in 1935 and Eden Ed Herbert in 1936.1-3 There is usually a long latency period from the moment of silicon penetration in the skin and the clinical appearance of the granuloma. This latency period varies from 1 year to more than 50 years, with an average interval of 10 years. Silica granulomas have a clinical appearance of single or multiple nodules along the scar line of a previous injury. The pathogenesis of silica granuloma is not clear. According to Rank et al. it is likely that silica granulomas represent a reaction due to immune mediated hypersensibility after a period of latency of many years after the injury in subjects with a predisposition.4 The histopathological picture reminds us of the sarcoidosis granuloma.2 The medium and deep dermis, sometimes even the hypodermis, are occupied by nodular infiltrates with a distinct peripheral boundary made up of epithelioid cells and some giant multinucleate cells type Langhans or external body type and few lymphocyte cells at the boundaries of the epithelioid nodules.2 The most typical finding is the presence in the cytoplasm of some giant cells of birefringent, brilliant, polygonal and elongated crystals, observable only under polarised light. Without these mineral inclusions it is not possible to distinguish a silica granuloma from a cutaneous sarcoidosis.2 The apparently low incidence of the silica granuloma is partly due to the 376 lack of routine exams under polarized light. Energy-dispersive X-ray analysis allows definitive diagnosis of silica granuloma. In this process a characteristic X-ray emission spectrum is evoked, it is recorded in graphic form, with characteristic peaks identifiable with an element’s atomic number.3 Some researchers have reported cases of systemic sarcoidosis associated with cutaneous manifestations where polarized crystals were evidently associated with the formation of the skin granuloma. As it is well known, Figure 1.—The lesion on the forehead before treatment. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 CORRESPONDENCE Figure 2.—Foreign-body granulomatous inflammation, sarcoid type. “Bare” granulomas adjacent to each other with no lymphocytes and plasma cells interposition can be observed. (Hematoxylin and eosin; magnification 2.5X). sarcoidosis has a particular tropism for scars and for areas previously exposed to injury. The foreign body could serve as a substrate stimulating the formation of the granuloma and in some cases of sarcoidosis. Surgical excision is the best treatment. Alternative treatments are intralesional injections of steroids with the risk of recurrence, once the treatment is suspended. Other systemic treatments with steroids, antibiotics and radiotherapy have been described. In some cases a spontaneous solution of the lesions is possible, so an observation period of 6-12 months is advis- able.5 The authors describe a case of silica granuloma in a 65-year-old patient after a latency period of 30 years and on a previous scar. A 65-year-old man presented to our facility with nodular lesions in the area of post-trauma scar lesions in the left frontal region (trauma occurred 30 years before). The patient had cranial trauma due to a car accident causing the breakage of the windscreen, which had in turn caused a cut injury in the left frontal region, that was surgically sutured. After about 30 years from the previous trauma and along the scar line, multiple painless nodules appeared. At the objective exam a linear scar about 10 cm long and parallel to the line of the left eyebrow and of a red-purple color standing out on the cutaneous level was observed. Multiple nodules distributed in an irregular manner could be felt at touch. They were along the line of the scar and of a painless fibrous thick consistency (Figure 1). A biopsy of a nodular lesion was performed and the histopathological exam showed an area of chronic, granulomatous tissue, with giant cells and no necrosis inflammation composed by multiple granulomas of epithelioid cells and giant multinucleate cells, surrounded by little inflammatory infiltration, as can be observed in sarcoid type granulomatous reactions. Rare fragments of foreign non-pigmented birefringent crystal material were present in some granulomas. The Ziehl-Nielsen coloration performed to search alchol-acid resistant bacilli was negative. The histopathological samples showed chronic granulomatous inflammation of the skin with sarcoid similar aspects, as can be observed in foreign bodies containing siliconates (Figures 2-4). Clinical and instrumental exams were performed in order to exclude a systemic sarcoidosis, and the results were negative. The diagnosis was silica granuloma and surgical revision of the scar was the treatment proposed. Figure 3.—Birefringent foreign body in the cytoplasm of a giant cell (Hematoxylin and eosin; magnification 20X). Vol. 149 - No. 3 GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 377 CORRESPONDENCE P. FINO Department of Plastic, Reconstructive and Esthetic Surgery, University of Rome “Sapienza”, Policlinico Umberto I, Rome, Italy [email protected] V. AMOROSI Department of Plastic, Reconstructive and Esthetic Surgery, University of Rome “Sapienza”, Policlinico Umberto I, Rome, Italy F. PIRO Department of Pathology, San Giovanni-Addolorata Hospital, Rome, Italy D. PEDACE Dermatology and Venereology, Free Practioner Figure 4.—The Ziehl-Nielsen stain was negative for alchol-acid resistent bacilli. Histologically, cutaneous silica granulomas are significant for their resemblance with cutaneous sarcoidosis. Furthermore, the non-specific clinical presentation makes the diagnosis more difficult and cutaneous silica granuloma might be a lesion that is often underdiagnosed. Thus, a thorough clinical history, histopathological examination and observation under polarized light microscopy are essential in achieving an accurate diagnosis and for implementing appropriate management. We suggest to any doctor and dermatologists who observe a lesion with the characteristics described above to consider this diagnostic hypothesis. Previous trauma information and silica exposure must be asked for in the clinical anamnesis. M. G. ONESTI Department of Plastic, Reconstructive and Esthetic Surgery, University of Rome “Sapienza”, Policlinico Umberto I, Rome, Italy S. CARELLA Department of Plastic, Reconstructive and Esthetic Surgery, University of Rome “Sapienza”, Policlinico Umberto I, Rome, Italy C. LATINI Department of Maxillofacial and Plastic, Reconstructive Surgery, San Giovanni-Addolorata Hospital, Rome, Italy G ITAL DERMATOL VENEREOL 2014;149:376-8 References 1. Shattock SG. Pseudotuberculoma silicoticum of the lip. Proc R Soc Med 1916;10:19-21. 2. Fernandez-Flores A, Montero MG. Does cutaneous silica granuloma develop mainly in predisposed patients? Eur J Dermatol 2006;16:321-2. 3. Bovenmyer DA, Landas SK, Bovenmyer JA. Spontaneous resolution of silica granuloma. J Am Acad Dermatol 1990;23:322-4. 4. Rank BK, Hicks JD, Lovie M. Pseudotuberculoma granulosum silicoticum. Br J Plast Surg 1972;25:42-8. 5. Fernandez-Flores A. Birefringent particles in granulomatous dermatitis, sarcoidal-type as well as in other non-granulomatous skin disorders in patients without sarcoidosis. Bratisl Lek Listy 2009;110:328-31. Merkel cell carcinoma of the lower limb TO THE EDITOR: A 83-year-old woman presented with a dome-shaped, deep, bluish- red nodule on her left thigh, measuring 2.0 cm in diameter (Figure 1). After informed consent and local anesthesia, the lesion was widely excised with a 3 cm border. Histopathological examination revealed a small cell undifferentiated carcinoma/Merkel’s cells carcinoma (MCC), infiltrating the dermis, the sub- 378 cutaneous tissue and the vascular spaces with aggregates of small round blue cells showing hyper-chromatic nuclei, scant cytoplasm and mitoses (Figures 2, 3). Immunohistochemistry was positive for both citokeratin 20 (CK-20) and chromogranin A, but negative for S100, CK-7 and common leukocyte antigens. Sentinel lymphnode biopsy (SLNB), physical examination and imaging studies, including total- GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 CORRESPONDENCE Figure 1.—Our patient showing a dome-shaped, deep, bluish-red nodule on her left thigh. body computer tomography (CT-SCAN), were negative, hence disease stage was I. The patient was treated with adjuvant external beam radiotherapy (EBRT) (6000 cGy) to the surgical area. A 7-year-follow-up did not show evidence of recurrence or metastasis. We have decided to examine retrospectively the presence of Merkel cell polyomavirus (MCV) in 2 formalin-fixed paraffin-embedded sections. Sections of 10 μm were obtained from formalin-fixed paraffin-embedded tissue biopsy specimens from the patient and were extracted with xylene to remove the paraffin, followed by two washes with absolute ethanol to remove the xylene. The presence of MCV was searched by primer-directed amplification with PCR. Specific primer pairs were designed to detect the viral large T protein (LT1 and LT3) and the viral capsid protein (VP1). For PCR amplification, a sensitive GoTaq® Flexi DNA polymerase system (Promega, Madison, WI, USA) was used with 0.5 μg 10 μL−1 genomic DNA, and 20 pmol of each primer. To demonstrate that the quality and quantity of the DNA samples isolated from the formalin-fixed paraffin-embedded tissue biopsies were acceptable, a 268-bp segment of the human β-globin gene was also amplified. Amplification products were separated by electrophoresis in 1.5% agarose gel stained with GelRed™ (Biotium Inc., Hayward, CA, USA). For the DNA sequence analysis, the PCR products were excised and purified with the Cycle-Pure mini kit (Omega Bio-Tek Inc., Norcross, GA, USA). The purified PCR products were Vol. 149 - No. 3 Figure 2.—Small cell undifferentiated Merkel’s cells carcinoma, infiltrating the dermis, the subcutaneous tissue and the vascular spaces (hematossilin-eosin 25X). Figure 3.—MCC showing vesicular, basophilic nuclei with prominent nucleoli and multiple mitoses (hematossilin-eosin 200X). GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 379 CORRESPONDENCE subjected to direct sequencing. In both sections, PCR was negative. MCC, first described by Toker as “trabecular carcinoma” of the skin in 1972 is a rare, highly malignant tumor of the skin which displays features of neuroendocrine differentiation. Often initially misdiagnosed due to its nondistinctive appearance, MCC usually occurs as a painless, dome-shaped, deep red nodule on sun-exposed skin with predominance in older patients. The acronym AEIOU has recently been proposed to describe the classical clinical characteristics of MCC: asymptomatic, expanding rapidly, immune suppression, older than 50 years of age, UV-exposed site on fair skin.1 The incidence of MCC has risen substantially over time, with an estimated three time increase annually between 1986 and 2001.1 The etiology of MCC is unknown. However, many patients with MCC have had a history of other synchronous or metachronous sunassociated skin cancers, implicating excessive sun exposure as a common risk factor for developing MCC. There may be an increased reciprocal risk of MCC with haematologic diseases and malignant melanoma, suggesting that MCC may share etiologic influences with other malignancies.1 Immunosuppressed patients are also at a higher risk for developing MCC.1 Although the MCV may explain the increased incidence of MCC in immunosuppressed patients, in our case, MCV research performed on formalin-fixed and paraffin-embedded tissue specimens with quantitative PCR was negative.2, 3 Frozen tissues from MCC patients seem to have higher percentages of PCR positivity.3 Patients with MCC should be rigorously staged. The primary site should be evaluated for satellite lesions and dermal seeding. To date, there seems to be no optimal imaging algorithm and fluorodeoxyglucose positron emission tomography (PET imaging), not performed in our case, has been reported useful.4 Although the contribution of sentinel lymphnode biopsy to accurate staging of patients with MCC is generally accepted, its potential significance in terms of predicting patient prognosis remains controversial. Depending on the stage of disease and patient’s health status, the primary treatment of MCC involves wide surgical excision with at least 2 to 3 cm margins. However, many clinicians believe that even in stage I MCC, surgery should be combined with adjuvant EBRT to the primary site and primary nodal chains because of a high loco-regional recurrence.5 Although most MCC cell lines are more radio-resistant than other small cell carcinomas, most clinical studies, as our case, demonstrated better local control rates with adjuvant EBRT after surgery.5 Combined EBRT and chemotherapy (doxorubicin in particular) have been suggested for patients with more advanced disease while, in disseminated diseases, the effect of EBRT is questionable and systemic chemotherapy induces considerable toxicity and treatment-related deaths. Recently, few studies have been published on the combination of chemotherapy with peptide receptor radionuclide therapy (PRRNT) in advanced stages of MCC. Male sex, tumor size, advanced clinical stage, small cell size, high mitotic index, diffuse pattern, as well as p53, have all been reported as poor prognostic factors, while better survival 380 was associated with limb localization, early stage disease, younger age and female sex.1 In our patient, age did not influence the prognosis. In conclusion, MCC is rare and almost always misdiagnosed during physical examination. Research has improved the accuracy of diagnosis of MCC through immunohistochemical staining, but the exact pathogenesis of MCC is still uncertain and the role of adjuvant radiation therapy continues to be debated. Although we know that only multi-institutional prospective clinical trials will explain the pathogenesis and define the exact role of radiation therapy of MCC, we reported our single case to underline that it is necessary to maintain a high index of suspicion for MCC in every skin lesion that presents as a solitary dome-shaped nodule, even in uncommon locations such as the thigh. M. DE PAOLA Section of Dermatology, Department of Clinical Medicine and Immunological Sciences, University of Siena, Santa Maria alle Scotte Hospital, Siena, Italy [email protected] S. POGGIALI Section of Dermatology, Department of Clinical Medicine and Immunological Sciences, University of Siena, Santa Maria alle Scotte Hospital, Siena, Italy C. MIRACCO Department of Human Pathology and Oncology, University of Siena, Santa Maria alle Scotte Hospital, Siena, Italy C. PISANI Section of Dermatology, Department of Clinical Medicine and Immunological Sciences, University of Siena, Santa Maria alle Scotte Hospital, Siena, Italy A. BATSIKOSTA Section of Dermatology, Department of Clinical Medicine and Immunological Sciences, University of Siena, Santa Maria alle Scotte Hospital, Siena, Italy R. BILENCHI Section of Dermatology, Department of Clinical Medicine and Immunological Sciences, University of Siena, Santa Maria alle Scotte Hospital, Siena, Italy G ITAL DERMATOL VENEREOL 2014;149:378-81 References 1. Heath M , Jaimes N, Lemos B, Mostaghimi A, Wang LC, Peñas PF et al. Clinical characteristics of Merkel cell carcinoma at diagnosis in 195 patients: the AEIOU features. J Am Acad Dermatol 2008;58:375-81. 2. Varga E, Kiss M, Szabó K, Kemény L Detection of Merkel cell polyomavirus DNA in Merkel cell carcinomas. Br J Dermatol 2009;161:930-2. 3. Touzé A, Gaitan J, Maruani A, Le Bidre E, Doussinaud A, Clavel C GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014 CORRESPONDENCE et al. Merkel cell polyomavirus strains in patients with Merkel cell carcinoma. Emerg Infect Dis 2009;15:960-2. 4. Iagaru A, Quon A, McDougall IR, Gambhir SS. Merkel cell carcinoma: is there a role for 2-deoxy-2-[f-18]fluoro-d-glucose-positron emission tomography/computed tomography? Mol Imaging Biol 2006;8:212-7. 5. Eng TY, Boersma MG, Fuller CD, Cavanaugh SX, Valenzuela F, Herman TS. Treatment of Merkel cell carcinoma. Am J Clin Oncol 2004;27:510-5. 6. Salavati A, Prasad V, Schneider CP, Herbst R, Baum RP. Peptide receptor radionuclide therapy of Merkel cell carcinoma using (177)lutetium-labeled somatostatin analogs in combination with radiosensitizing chemotherapy: a potential novel treatment based on molecular pathology. Ann Nucl Med 2012;26:365-9. Yellow urticaria in a patient with hepatic cirrhosis TO THE EDITOR: Most urticarial reactions were previously thought to occur as a result of immunological or inflammatory mechanisms. The lesions of urticaria are usually observed as erythematous plaques. However, we present the case of a 56-year-old man with acute urticaria that appeared yellow because of hyperbilirubinemia. A 56-year-old Japanese man was admitted to our hospital, presenting with clouding of consciousness and a high-grade continuous fever with chills. General physical examination revealed jaundice and a body temperature of 38.5 °C, with marked neck stiffness with a positive Kernig’s sign. His medical history included chronic hepatitis C and alcoholic cirrhosis, for which he had received treatment with lansoprazole, ursodeoxycholic acid, furosemide, and spironolactone for 5 years prior to presentation. He had also been undergoing endoscopic injection sclerotherapy for recurrent gastrointestinal bleeding. A cerebrospinal fluid (CSF) analysis revealed leukocytosis, a high protein concentration, and low glucose levels, with a decreased CSF-to-serum glucose ratio. Because cerebral meningitis was suspected, blood and cerebrospinal fluid samples were examined. The cultures of both these samples tested positive for hemolytic streptococcus. On the basis of a hemolytic streptococcus meningitis diagnosis, the patient intravenously received vancomycin and ampicillin. Approximately 24 h after receiving the antibiotics, he developed multiple well-defined, yellowish, edematous plaques that disseminated into the buttocks and anterior region of his knees (Figure 1). He was unable to describe any symptoms because he was comatose. Hematological examination revealed hyperbilirubinemia (direct bilirubin level, 5.2 mg/dL [reference range, 0-0.4 mg/dL]; total bilirubin level, 8.1 mg/dL [reference range, 0.3-1.2 mg/dL]), and thrombopenia (platelet count, 24,000/mm3). Liver enzyme levels were mildly elevated (aspartate aminotransferase level, 48 U/L [reference range, 13-33 U/L]). A half day later, the swelling subsided, but some of the yellowish macules persisted. On day 4, the patient died from progressive multiple-organ failure while comatose. Yellowish changes in skin color are usually evident in xanthoma, during ingestion of antimalarial drugs, in carotenemia, and in yellow urticaria.1, 2 The present patient’s dietary history ruled out food-induced skin discoloration. Although vancomycin and ampicillin were administered Vol. 149 - No. 3 before the appearance of the rash, there had been no report of yellowish skin eruptions by these drugs. Based on the clinical course of the eruption, we diagnosed the patient with yellow urticaria secondary to an elevated bilirubin level. We believe that the yellowish skin color was a consequence of the increased permeability of the blood vessels in the wheal and the deposition of excess bilirubin in the surrounding dermis. Previous reports have failed to show the existence of bilirubin in biopsy tissue by Gmelin staining.3 According to us a minimal bilirubin level must be present in a tissue section to be detected by Gmelin staining. In our previous report and that of Imanishi et al.,3 it is interesting to note that yellowish wheal had appeared after an increase in blood bilirubin levels within a few days. Bilirubin, a breakdown product of normal heme catabolism, A B Figure 1.—Yellowish edematous plaques located around the right knee (A) and on the buttocks (B). GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA 381 CORRESPONDENCE is now thought to be biologically active and hence may trigger urticarial reaction. Bilirubin has been shown to induce a dose-dependent decrease in transepithelial electrical resistance and an increase in paracellular permeability of the intestinal epithelium to fluorescent dextran.4 Moreover, increased intestinal permeability has been observed not only in vitro but in vivo as well.5 Given the severity of the infection, it might have been possible to easily increase vascular permeability. However, these results indicate that the elevation of serum bilirubin levels may have caused the increased permeability of blood vessels. Thus, we propose that hyperbilirubinemia may be a causative factor for urticaria, though further evidences are needed to support this hypothesis. T. CHIBA Department of Dermatology, Iizuka Hospital, Fukuoka, Japan [email protected] F. HAYASHI Department of Neurology, Iizuka Hospital, Fukuoka, Japan M. SHINMURA Department of Neurology, Iizuka Hospital, Fukuoka, Japan M. KIYOMATSU Department of Dermatology, Iizuka Hospital, Fukuoka, Japan 382 S. TATEMATSU Department of Dermatology, Iizuka Hospital, Fukuoka, Japan M. NAKAO Department of Dermatology, Iizuka Hospital, Fukuoka, Japan M. FURUE Department of Dermatology, Graduate School of Medical Sciences, Kyushu University, Fukuoka, Japan G ITAL DERMATOL VENEREOL 2014;149:381-2 References 1. Narváez-Moreno B, Pereyra-Rodríguez JJ. Yellow urticaria. N Engl J Med 20; 2; 367. 2. Patel SB, Mutasim DF. Yellow urticaria secondary to hyperbilirubinemia in a patient with end-stage liver disease. Cutis 20;; 0: 41-4. 3. Imanishi H, Tsuruta D, Kobayashi H, Ishii M. Yellow urticaria associated with hepatitis type-C liver cirrhosTh of Dermaogy 206;33: 823-4. 4. Raimondi F, Crivaro V, Capasso L, Maiuri L, Santoro P, Tuci M, et al. Unconjugated bilirubin modulates the intestinal epithelial barrier function in a human-derived in vitro model. Pediatric Research 206;60: 30-3. 5. Welsh FK, Ramsden CW, MacLennan K, Sheridan MB, Barclay GR, Guillu PJ, et al. Increased intestinal permeability and altered mucosal immunity in cholestatic jaundice. Annals of surgery 998;227:205-12. GIORNALE ITALIANO DI DERMATOLOGIA E VENEREOLOGIA June 2014
