Survey
* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project
Download A Phase II study for LCH resistant patient with 2 CDA
Document related concepts
Transcript
LCH-S-2005 An International Phase II Study evaluating the combination of Cladribine (2 CdA) + Cytarabine Cytosinearabinoside in refractory Multisystem Langerhans Cell Histiocytosis (LCH) The Langerhans Cell histiocytosis Salvage Therapy Working Group Histiocyte Society Date: December 2005 Salvage therapy S 2005 December 2005 Composition of the Working group ..............................................................................................................................3 Background ...................................................................................................................................................................6 Study objective............................................................................................................................................................10 Eligibility criteria ........................................................................................................................................................11 Inclusion criteria:.....................................................................................................................................................11 Exclusion criteria:....................................................................................................................................................11 Endpoints.....................................................................................................................................................................13 Major endpoint: .......................................................................................................................................................13 Secondary endpoints: ..............................................................................................................................................13 Treatment ....................................................................................................................................................................14 Combination chemotherapy: Initial 2 courses (figure 1).........................................................................................14 Decision rules after 2 courses (figure 2): ................................................................................................................14 Maintenance therapy (figure 3) ...............................................................................................................................15 Part 1: ..................................................................................................................................................................15 Part 2: ..................................................................................................................................................................15 Part 3: ..................................................................................................................................................................16 Oral 6-mercapto purine and oral Methotrexate: How to adapt the therapy in case of side effects......................16 Supportive care guidelines ..........................................................................................................................................20 Protocol deviation as a consequence of side effects....................................................................................................22 Pre-treatment evaluation..............................................................................................................................................23 Evaluation and response criteria..................................................................................................................................23 Follow-up and long term outcome ..............................................................................................................................25 Drug Information.........................................................................................................................................................26 Cladribine (2-Cda) (Leustatin)............................................................................................................................26 Cytarabine (Ara-C) (Cytosar-U) .........................................................................................................................27 Expected toxicity.........................................................................................................................................................29 Drug combination....................................................................................................................................................29 Cladribine(2-CDA) (Leustatin)...........................................................................................................................29 Cytarabine (Ara-C) (Cytosar-U) .........................................................................................................................30 Toxicity reporting........................................................................................................................................................31 Statistical considerations .............................................................................................................................................32 Appendix .....................................................................................................................................................................34 Appendix 1 : Risk organs definition........................................................................................................................35 Appendix 2 : WHO toxicity criteria ........................................................................................................................36 Appendix 3: Data monitoring Time table...............................................................................................................42 Appendix 4: Informed consent ................................................................................................................................43 Appendix 5 : LCH 2005 S Inclusion sheet (2 pages) ..............................................................................................44 Appendix 6 : LCH 2005 S Toxicity report sheet in case of severe adverse event OR DEATH ............................46 References ...................................................................................................................................................................47 Page 2 of 48 Salvage therapy S 2005 December 2005 Composition of the Working group Name City Country M Arico Palermo, Italy R Arceci Baltimore, USA F Bernard Montpellier, France J Braier Buenos Aires, Argentina J Donadieu –Chair Paris, France M Egeler Leiden, Netherlands N Grois Vienna, Austria J-I Henter – Co Chair Stockholm, Scandinavia K Mc Clain Houston, Texas M Minkov Vienna, Austria J Pritchard Edinburgh, UK C Rodriguez – Galindo Memphis, USA K Stine Little Rock, USA Takamato Kyoto, Japan S Van Gool Leuven, Belgia S Weitzman Toronto, Canada K Windebank Newcastle, UK J Whitlock Nashville, USA Composition of the Working group /details: Study Chairman Jean Donadieu Hospital Trousseau Hematologie-Oncologie 26 Rue Du D Netter Paris, F-75012 France P + 33 - 1- 44736062 F + 33 – 1 - 44736573 e-mail: [email protected] Maurizio Arico U.O. Onco-Ematologia Pediatrica Ospedale dei Bambini "G. Di Cristina" Via Benedettini 1 90134 Palermo Tel. +39-091-6666131 Fax +39-091-6666001 e-mail: [email protected] Bob Arceci, Johns Hopkins Oncology Center Bunting-Blaustein Cancer Research Building 1650 Orleans Street 2M51 Baltimore, MD 21231 United States of America P +1 – 410 - 5027519 F +1 – 410 - 9558897 e-mail: [email protected] Frédéric Bernard Pédiatrie 3, Hémato-Immuno-Oncologie Pédiatrie Hôpital Arnaud de Villeneuve Av. du Doyen Giraud 34000 MONTPELLIER Phone. 33 467336603, Fax.33 467540035 e-mail: [email protected] Jorge Braier Pediatric Hemato / Oncology Hospital Garrahan Combate de los Pozos, 1881 Buenos Aires 1245 Argentina P: 54 1 43084300 F 54 11 43085325 e-mail: [email protected] Page 3 of 48 Salvage therapy S 2005 December 2005 Maarten Egeler, Leiden University Medical Center Department of Pediatrics - IHOBA, Rm J6-222 PO Box 9600 2300 RC LEIDEN The Netherlands Telephone: 31 71 526-4131/2824 Telefax: 31 71 524-8198 e-mail: [email protected] Nicole Grois St. Anna Children's Hospital Kinderspitalgasse 6 A-1090 Vienna, Austria Tel: +43-1-40170-476 Fax: +43-1-40170-430 e-mail: [email protected] Jan-Inge Henter, Co Chair Childhood Cancer Research Unit Karolinska Hospital, Q6:05 SE-171 76 Stockholm, Sweden Phone: +46 - 8 5177 2870 or 8- 5177 7098 Telefax: +46 - 8 5177 3184 e-mail: [email protected] Ken Mc Clain Texas Children’s Clinical care center 6701 Fanin Street Suite 1410 Houston TX 77030 USA P: 1 832 822 4208 F : 1 832-825-1503 e-mail: [email protected] Milen Minkov St. Anna Children's Hospital Kinderspitalgasse 6 A-1090 Vienna, Austria Tel: +43-1-40170-476 Fax: +43-1-40170-430 e-mail: [email protected] Jon Pritchard Royal Hospital for sick Children 9 Sciennes Road Department of Oncology & Haematology Edinburgh EH91LF SCOTLAND Phone 44 131 5360000 Fax: 44 131 5360001 e-mail: : [email protected] Carlos Rodriguez-Galindo, MD Department of Hematology-Oncology St Jude Children's Research Hospital Tel (901) 495-2203 e-mail: [email protected] Kimo Stine Pediatric Hemato/ Oncology Arkansas children’s Hospital 800 Marshall St. Little Rock AR 72202 USA e-mail: Tel 1 501 364 1494 Fax 1 501 364 3634 e-mail: [email protected] Stefaan Van Gool, Pediatric Hemato-oncology and Neuro-oncology University Hospital Gasthuisberg Laboratory of Experimental Immunology Herestraat 49 B-3000 Leuven Belgium Tel: + 32-16-332211 Fax: +32-16-343842 e-mail: [email protected] Sheila Weitzman The Hospital for Sick Children 555 University avenue Toronto, Ontario, Canada Tel 416 813 5872 Fax: 416 813 5327 e-mail: [email protected] Jim Whitlock Pediatric Hematology/ Oncology Vanderbilt University Medical Center 2220 Pierce Avenue, 397 PRB Nashville, TN 37232-6310 USA Tel 1 615 936 1762 Fax : 1 615 936 1767 e-mail: : [email protected] Kevin Windebank Senior Lecturer in Child Health, & Consultant Paediatric Oncologist Sir James Spence Institute Royal Victoria Infirmary Newcastle upon Tyne NE1 4LP. UK P 44 191 202 3026 FAX +44 191 202 3060 e-mail: [email protected] Page 4 of 48 Salvage therapy S 2005 December 2005 The coordinator of the study at the country level is the member of the working group who is responsible for the ethic committee for his country (EU) or for his center (north America). Statistician: Mrs Anne AUPERIN Département d’épidémiologie et Biostatistique Institut Gustave Roussy Rue Camille Desmoulins Villejuif 94800 France e mail : [email protected] Drug Safety Monitoring Board David Webb, UK Stephan Ladisch USA MG Valsecchi Italia Page 5 of 48 Salvage therapy S 2005 December 2005 Background The clinical presentation and outcome of treatment for Langerhans CHcell histiocytosis (LCH) are is very variable, ranging from an isolated spontaneously remitting bone lesion to a multi-system disease with life-threatening organ dysfunction. Dysfunction Involvement of the lungs or of the hematopoetic system and/or involvement of the spleen, the liver or the digestive tract, are features which may be associated with a poor outcome (1-6). Since the early 1990’s, international cooperative approaches to this rare disease have been organized under the aegis of the Histiocyte Society, an international association of researchers dedicated to clinical and fundamental research into the histiocytic disorders. The successive trials have helped to standardize the initial investigations and have led to the randomized therapy now being tested in the third prospective therapeutic trial for newly diagnosed patients (LCH III). The trials have also allowed confirmation of many different prognostic factors, as well as a better understanding of the natural history of the disease. In patients with multisystem LCH (more than one organ involved, at the time of diagnosis or during the course of the disease), a poor response to the initial standard chemotherapy with vinblastine and corticosteroids prednisolone has been shown to be the most important single prognostic factor, defining a group of patients with a less than 30% survival rate at 2 years from diagnosis, as detailed in Table 1 (1;3;5;7). Table 1: Review of the outcome of patients with poor response to therapy References Study Drugs received in the first 6 weeks Criteria definition failure (3;7) DAL HX83 Vinblastine VP16 and corticosteroid Vinblastine VP16 and corticosteroid Vinblastine or VP16 and corticosteroid Mainly vinblastine and corticosteroid AD Worse (7) DAL 90 HX (1) LCH I (5) French survey for of Number of resistant patients Survival rate % 9 11% AD Worse 25 40% Progression of the disease 13 0% AD Worse Page 6 of 48 Salvage therapy S 2005 December 2005 The progression pattern of the disease is unpredictable, however. The disease usually retains some sensitivity to treatment but with only partial control followed by secondary progression. Many of these patients suffer profound and refractory pancytopenia and usually die from sepsis or bleeding. In this setting, the serum albumin level is also profoundly decreased, related to digestive tract leak and/or to lack of production due to liver dysfunction. Both nutritional status and an enhanced catabolic state contribute to the progressive deterioration. The clinical presentation of this group of patients differs from those patients with lung involvement as the sole ‘risk’ organ dysfunction. The outcome in these patients can also be dramatically compromised as lung destruction can be fatally aggravated by an undercurrent intercurrent infection or a mechanical complication such as pneumothorax. These latter situations remain distinct from the multivisceral involvement previously described, however, and the impact of chemotherapy is uncertain (8). Over the last 15 years, several new drugs and or procedures have been reported as being useful in the treatment of patients with LCH. A new therapeutic approach is often reported as a promising single case report but unfortunately, further evaluation in a larger group of patients proves it to be disappointing. This is especially true for high risk patients with haematological dysfunction and failure to respond to standard therapy, who represent the majority of early deaths in LCH (2;4-6). Examples of this are agents such as cyclosporine A, interferon alpha and 2-Chlorodeoxyadenosine (2-CdA) when used as monotherapy (9-18). Despite promising case reports and small series, stem cell transplantation (SCT) has, as yet, not been clearly demonstrated to be an effective salvage procedure in this group of patients. There are many limitations to successful SCT in this setting, including the difficulty of finding an appropriate donor in a short period of time and the toxicity of the conditioning regimen. The preliminary results of a small survey of 7 patients transplanted with a low-intensity conditioning regimen, suggests that this approach may be more promising (20), but this needs to be tested prospectively. New strategies for the treatment of patients with refractory LCH are therefore much needed. One promising strategy is a combination of 2-CdA and cytosine cytarabine-arabinoside (ara-C). To date, only one pilot study using 2-CdA and Ara-C has been reported (21), which suggests that patients with multivisceral LCH Page 7 of 48 Salvage therapy S 2005 December 2005 and failure of standard therapy may have a favorable response to this therapeutic stratagem. The main limitation of the study is the small numbers of patients enrolled, but it is noteworthy that 7 of 10 refractory patients have achieved sustained complete remission (CR), some with responses evident only after several months of follow-up (21).This is, a result that is significantly different from the reported historical outcome for this group of patients. There is in addition, a good pharmacological rationale for the combination of 2-Cda and ara-C. 2-CdA is a deoxyadenosine analogue phosphorylated by the enzyme deoxycytidine kinase (dCK), leading to the formation of 2-CdA mono-, di- and triphosphate (2-CdAMP, 2-CdADP, and 2-CdATP). These nucleotides are resistant to deoxyadenosine aminase, and their accumulation results in inhibition of DNA synthesis and cell death. 2-CdA thus has an antiproliferative effect on histiocytes and lymphocytes (14). Ara-C Cytosine Arabinoside (Ara-C), a cytostatic drug also phosphorylated by dCK, has been used successfully, together with vincristine and prednisolone, as first line treatment of children with disseminated LCH and organ dysfunction (22). In other studies, both in vitro and in vivo, pretreatment with 2-CdA resulted in increased accumulation of Ara-CTP (the active form of Ara-C) in circulating blasts from relapsed adults with refractory acute myelogenous leukemia (AML) (23). Kornblau et al. also studied the effect of combination 2-CdA and Ara-C in adults patients with AML(24). Ara-C was administered at a dose of 1 g/m² 2iv over 2 hours at hour 0, 48, 72, 96 and 120, and 2-CdA at 12 mg/m²/2/day x 5 days beginning at hour 24. Non-hematopoetic toxicity was generally tolerable. All patients had a WBC nadir of <0.1 x 109 by day 7, one patient died before day 14 and one patient showed no recovery of platelets beyond 75 days. In general the myelotoxicity was hard to evaluate in these aleukemic patients because of confounding factors related to the disease itself. Evaluation of response is an important issue in the management of patients with LCH, especially those with multi-organ dysfunction. A recently developed scoring system (25) has been tested in the evaluation of response to stem cell transplantation (19) and to the 2-CdA and Ara-C combination (21). This scoring system takes into account clinical criteria (including fever, spleen and liver size, oxygen requirement, the number of weekly transfusions and /or the number of albumin infusions), and a limited number of laboratory parameters (complete blood Page 8 of 48 Salvage therapy S 2005 December 2005 count, albumin level, liver function tests), as well as imaging studies. Further validation of this scoring system however, will require a prospective, multiinstitutional evaluation and for this present study the established LCH III evaluation system will be utilized. Page 9 of 48 Salvage therapy S 2005 December 2005 Study objective To assess the efficacy of the combination of 2-Cda and Ara-C in LCH patients who fail to respond to front-line chemotherapy AND who have risk organ involvement. Page 10 of 48 Salvage therapy S 2005 December 2005 Eligibility criteria Inclusion criteria: All the 5 following criteria must be present: a A biopsy-proven definitive diagnosis of LCH AND Risk organ involvement (Appendix 1) AND Failure of initial therapy defined by disease progression in one or more risk organs except solely lung(excluding isolated lung involvement), after at least 6 weekly doses of vinblastine and 28 days of corticosteroid prednisolone at a minimum dose of 40 mg/m2², with or without the addition of a third drug. The patient will be eligible for inclusion in LCH-S-2005 even if he/she has not been registered or treated “according to” the LCH-III protocol, however as long as a similar initial treatment approach is required before inclusion on LCH-S-2005.has been used. If drugs other than vinblastine and corticosteroid prednisolone have been given in the two months prior to the inclusion in this study, the coordinator of the study has to validate the inclusion in writing. Patients who initially respond but then reactivate with reactivation in a risk organ(s), except solely lung excluding isolated lung disease, resistant in one or more risk organs after at least 6 weekly doses of vinblastine and 28 days of corticosteroid prednisolone at a minimum dose of 40 mg/m², 2, may also be enrolled in the study. AND Informed consent. All patients or their legal guardians (if the patient is below the legal age of consent), must sign a research ethics board approved consent form indicating their awareness of the investigational nature and the risks of this study. When appropriate, younger patients will be included in all discussions in order to obtain verbal assent. Exclusion criteria: The presence of any of the following criteria will exclude the patient from study: Page 11 of 48 Salvage therapy S 2005 December 2005 Isolated sclerosing cholangitis, with an inadequate liver function, as defined by biological biochemical liver abnormalities and typical imaging, without evidence of active LCH as the only evidence of risk organ involvement Isolated lung involvement at any age as well as systemic disease with lung disease as the only risk organ involvement Inadequate renal function as defined by serum creatinine > 3x normal for age. Pregnancy or breast-feeding. There is no age limit, but it is important to consider that the 2-Cda Ara-C association has only been evaluated in young children with LCH until now. Before inclusion of adult, a contact with the study coordinator is recommended. Page 12 of 48 Salvage therapy S 2005 December 2005 Endpoints Major endpoint: The major endpoint is the response rate after two courses of therapy, evaluated at 9-10 weeks from the initiation of the first course therapy. The response is considered as favorable if the status of the patient is Active Disease Better or Non Active Disease. Any early death, whatever the cause, is considered as an unfavorable response. Secondary endpoints: The number of courses and the time period taken to obtain Non Active Disease. The time period taken to obtain haematological recovery after each course of induction therapy. Red cell, neutrophil and platelet recovery will all be analyzed separately. The type of subsequent and/or maintenance therapy utilized. The early and late toxicity. The early and late morbidity The early and late mortality. Page 13 of 48 Salvage therapy S 2005 December 2005 Treatment Combination chemotherapy: Initial 2 courses (figure 1) Cytosine ArabinosideCytarabine (Ara-C) 500 mg/m2/dose in 250 ml/m2 twice a day for 5 days, as a 2 hour iv infusion, at hours 1, 13, 25, 37, 49, 61, 73, 85, 97 and 109 . Total Ara-C dose will be 1000mg /m2/day. Ara-C is started on the first day of the course. Children who are <10 kg body weight do not require dose reduction (21) except in the first month of life, when the dose of Ara-C will be 33mg/kg/day and 16.5 mg/kg per dose. 2-chlorodeoxyadenosine (2-CdA) 9 mg/m2/day as a 2 hour iv infusion given daily for 5 days. 2-CdA is started on the second day of the course and is given at hours 23,47,71,95 & 119. The infusion of 2-CdA have should not to be given at the same time as Ara-C. For children <10 Kg body weight, the dose of 2-CdA will be 0.3mg/Kg/day (21). The second course is started in the fifth week after the initiation of therapy whatever the hematological values. Dexamethasone eye drops 0.1% or saline eye drops (investigator choice) to both eyes three times daily for 6 days will be administered with the Ara-C. Eye drops could be administrated for more than 6 days according to local policy. G-CSF Administration of G-CSF 5 micrograms/kg/dose, subcutaneously or intravenously, given daily until neutrophil recovery occurs, is not contraindicated and is provided following local policy. Its use, however, should be clearly recorded. The use of GM-CSF and the use of Peg G-CSF are contraindicated. Decision rules after 2 courses (figure 2): The response will be evaluated at week 5-6 after the second cycle (i.e. week 9-10 Page 14 of 48 Salvage therapy S 2005 December 2005 from the start of the first cycle unless delayed). The interval between the first and second cycles is usually 4 weeks, but can be extended in cases of infectious or metabolic complications. The evaluation after the second cycle must be done during the fifth week after the start of the 2 nd course. There are three possibilities: A) Disease progression in risk organs Stem cell transplantation is recommended (see protocol of the Histiocyte Society) B) Improvement of the disease status in risk organs, but active disease still present: The therapy should be repeated for 1 course of 2 Cda-AraC starting between 28 and 35 days after the course n°2 followed by 2 courses of 2 CdA at 5mg/m²/day for 5 days, at 3 weekly intervals. For children <10 Kg body weight, the dose of 2-CdA will be 0.15 mg/Kg/day. At the end of this period, if the status of the patient is No Active Disease (NAD), maintenance therapy should be started. However, if at the end of this period, the disease is still active, the treating physician is required to contact the national study coordinator, for discussion of further therapy. C) No disease activity: Start maintenance therapy Maintenance therapy (figure 3) Part 1: Two courses of 2- CdA at 5mg/m2/ day for 3 days, given IV as a two hour infusion. The second course is started at day 21 after the start of the first course provided the counts have recovered to ANC >750 /mm3 and platelets > 75,000/mm3. For children <10 Kg body weight, the dose of 2-CdA will be 0.15 mg/Kg/day. Part 2: Beginning at day 21 from the start of the 2nd course of 2-CdA for a 6 months duration Vinblastine 6mg/m² IV every two weeks combined with Corticosteroids prednisolone 40 mg/m²/day per os, divided into 3 doses per day, for 5 days Page 15 of 48 Salvage therapy S 2005 December 2005 every two weeks (therefore 12 pulses of vinblastine would be injected given during a 6 months period) 6 MP Mercaptopurine (6MP) at a dose of 50 mg/m² per os daily Methotrexate (MTX) at a dose of 20 mg/m² per os once weekly Part 3: Beginning at day 14 from the start of the last pulse vinblastine for a 12 months duration: 6 MP at a dose of 50 mg/m² per os daily Methotrexate MTX at a dose of 20 mg/m² per os once weekly Oral 6-mercapto purine and oral Methotrexate: How to adapt the therapy in case of side effects If neutrophil count falls below 500/µl treatment will be held until recovery above these levels and then resumed as tolerated. If neutrophil count falls below 500/µl on > 2 occasions during continuation, decrease dose of 6-MP or MTX by 25% on alternation basis upon resumption of therapy. Begin by reducing the 6-MP dose. Transaminase values of 20N mandate holding therapy until the level returns to <10N. Persistence of values > 20 N for > 2 weeks requires an evaluation including: bilirubin, alkaline phosphatase, coagulation tests, albumin, total protein and hepatitis serologies. A liver biopsy as well a MRI evaluation, a cholangiography should be considered before additional therapy is given, to help to distinguish hepatic toxicity from LCH involvement or sclerosing cholangitis. Should therapy be withheld for myelosuppresion or elevated transaminase, resume therapy at the correct chronologically. Page 16 of 48 Course 1 Course 2 Evaluation period * * * * * 2 CDA: 9m g/m ² IV 2 hours Ara-C 500 m g/m ² tw ice a day /IV 2 hours /day Days * ** ** ** ** ** 1 2 3 4 5 * * * * ** ** ** ** ** 6 Figure 1 : Induction courses: 2 CdA and Ara-C 7 8 9 10 11 12 13 14 26 27 28 29 30 31 32 33 34 35 36 37 38 39 40 41 42 59 60 61 62 63 64 65 66 67 68 69 70 71 72 73 74 Salvage therapy S 2005 December 2005 Figure 2 : Overall shape of the protocol and decision rules after the 2 initial courses Non active disease AD better AD Intermediate 2 -Cda 9 mg/m² Ara-C course 1 2 -Cda 9mg/m² Ara-C course 2 Duration 28 days Duration 28 days Evaluation 1 Maintenance Therapy 2 -Cda 9 mg/m² Ara-C course 3 Duration 28 days W orse Non active disease 2 -Cda 5 mg/m² 2 -Cda 5 mg/m² 5 days 5 days Duration 21 days HSCT Page 18 of 48 Duration 21 days Maintenance Therapy Evaluation 2 AD better AD Intermediate AD W orse Please Contact Coordinator Salvage therapy S 2005 December 2005 Figure 3 : Maintenance therapy Maintenance therapy Duration 21 days Duration 21 days 2 -Cda 5 mg/m² 2 -Cda 5 mg/m² 3 days 3 days Duration 6 months Duration 1 year VLB and 5 days steroid every 2 two weeks: 12 courses AND 6 MP daily + MTX per os once a week Page 19 of 48 6 MP daily + MTX per os once a week Salvage therapy S 2005 December 2005 Supportive care guidelines The clinical condition of patients eligible for this study is usually extremely poor. The team who is going to administer this protocol should be experienced in the management of patients receiving very intensive chemotherapy protocols, such as those given in AML therapy. Therapies such as parenteral nutritional support, antibiotic and antifungal therapy, prophylactic therapy for aspergillosis and pneumocystis pneumoniae, immunoglobulin infusion, transfusion support including albumin infusion, are usually a vital necessity necessary in this subset of patients. By definition, pancytopenia does not constitute a contraindication to the initial treatment, but any documented infection must be controlled before starting the therapy. Antibiotics : Wide spectrum antibiotic and antifungal therapy is recommended to treat febrile neutropenia according to local policy. Prophylactic therapy for prevention of fungal disease, particularly aspergillosis infection, is highly recommended, according to local policy. Pneumocystis carinii prophylaxis Oral sulphamethoxazole/trimethoprim 3mg/kg/day of the trimethoprim, divided into 2 doses/day, on 3 consecutive days per week, should be given throughout the study period and for 12 weeks thereafter Fluids and parenteral nutrition: the insertion of a double lumen central catheter or infusion port, prior to therapy start, is encouraged *During the chemotherapy courses, twice maintenance fluids i.e 3L/m2/24 hours iv (or 200 ml/Kg for children under 10 Kg body weight) should be given except during high volume chemotherapy infusions. Urine output should be maintained at least 60% of input, measured 4 hourly. If the urine output is insufficient, furosemide 0.5 mg/Kg (maximum 20 mg/dose), should be given Blood count, renal and liver function studies and electrolytes are to be measured daily until the results are stable, or more frequently if clinically indicated Parenteral nutritional support is encouraged Page 20 of 48 Salvage therapy S 2005 December 2005 An albumin infusion is recommended for hypoalbuminemia until the albumin level remain stable above 30g/L (ie 3.0g/dl) Intra venous immunoglobulin support is recommended Blood Products: All cellular blood products have to be irradiated. Antiemetic therapy Could Should be provided following local policy as example: •Ondansetron (Zofran) 5 mg/m2 po/iv prechemotherapy and 8 hourly p.r.n. (or an alternative antiemetic) •Dexamethasone 0.5 mg/Kg/dose (maximum of 8 mg/ dose) given 12 hourly po may be added for severe nausea and vomiting or a febrile reaction G-CSF Administration of G-CSF 5 micrograms/Kg/dose, subcutaneously or intravenously, given daily until neutrophil recovery occurs, is not contraindicated and may be provided following local policy. The use of G-CSF must be recorded. The use of GM-CSF and the use of Peg G-CSF are contraindicated. Page 21 of 48 Salvage therapy S 2005 December 2005 Protocol deviation as a consequence of side effects. The treating physician always has the responsibility to adjust therapy according to the precise clinical condition of the patient. As this protocol is aimed at a group of patients in a life threatening situation, with numerous potential complications, decisions to delay therapy or decrease doses are not recommended, except to manage an acute infection, or a metabolic complication. Any significant deviation from the protocol (delay more than 2 weeks or administration of less than 80% of recommended dose) has to be reported to the national study coordinator. Page 22 of 48 Salvage therapy S 2005 December 2005 Pre-treatment evaluation A complete history, physical examination, including neurologic examination. Height, weight and body surface area should be recorded. Documentation of measurable disease, as well as signs and symptoms is required. Evaluation of all measurable disease by appropriate radiological or ultrasound means Haematology - complete blood count, platelet count, differential, PT and /or INR, PTT. (transfusion requirement should be documented) Chemistry - SGPT, SGOT, bilirubin, total protein, albumin, electrolytes, creatinine, calcium, phosphate, uric acid, ferritin and ESR. In case of lung X-ray abnormalities, a CT scan must be performed. Lung function must be evaluated according to local policy. HLA typing of the patient is recommended before the first course and family typing should be done as soon as possible. Evaluation and response criteria To evaluate the disease activity in Langerhans cell histiocytosis a multi-step approach is required, starting with a clinical examination and few simple, biological tests and imaging. Page 23 of 48 Salvage therapy S 2005 December 2005 The following information is supposed to be collected at each evaluation. Variables Fever Spleen size Liver size Skin area of the skin involvement Clinical data Pain related to the disease Nb of RBC transfusion in the week previous evaluation Nb of Platelets transfusion in the week previous evaluation Nb of albumin perfusion in the week previous evaluation Oxygen requirement Complete Blood Count ESR Biochemistry Liver enzyme Hematology Gamma GT and bilirubin Albumin Creatinin Calcium & atePhosphor Coagulation testscreen T cell lymphocyte subsets / phenotype Ig G A M Ferritin imaging Tumoral size in case of soft tissue tumor Lung CT (only at baseline and at week 9) Once the information collected; a synthesis of the situation of the patient is done using the previously published recommendation and the disease for each organ (specially the risk organs) has to be categorized in Active or Non Active Disease as follows: Page 24 of 48 Salvage therapy S 2005 December 2005 NON ACTIVE DISEASE (NAD) no evidence of disease resolution of all signs or symptoms Regression disease regression of signs or symptoms, no new lesions persistence of signs of symptoms, no new lesions progression of signs or symptoms and/or appearance of new lesions stable disease ACTIVE DISEASE (AD) progressive disease Then the response is considered by comparison of the actual situation with the immediately previous situation. There are three categories of response: complete resolution NAD BETTER regression Mixed new lesions in one site, regression in another site Stable unchanged INTERMEDIATE WORSE Progression For this protocol, the timing of the evaluation are as follows: 1. In the week before starting the therapy, 2. At the end of the fourth week (from start of the first course 3. At the end of the fifth week (from start of the second course) 4. 6 months after therapy start 5. 12 months after therapy start Follow-up and long term outcome A 5 yr follow up of the patients is recommended in all cases, even if the patient is withdrawn of from the study for a 5 year period. Once the study period (1 year) is ended, the follow up has to be organized according to standard recommendation in this disease. Page 25 of 48 Salvage therapy S 2005 December 2005 Drug Information Cladribine (2-Cda) (Leustatin) Source and Pharmacology: Cladribine is a synthetic purine nucleoside analogue. It must be activated by deoxycytidine kinase to its triphosphorylated form. It is then incorporated into DNA and results in DNA strand breakage and inhibition of DNA synthesis. The introduction of DNA strand breaks results in a depletion of nicotinamide adenine dinucleotide and ATP and disruption of cellular metabolism. Formulation and Stability: Cladribine is supplied in a 10 ml or 20 ml glass vial as a sterile, isotonic, preservative-free solution containing 10 mg (1 mg/ml) cladribine. The intact vials should be stored under refrigeration and protected from light. Freezing does not adversely affect the solution. For further dilution, 5% dextrose containing solutions are NOT recommended due to cladribine degradation. When diluted in 0.9% NaCl, solutions should be stored under refrigeration for no more than 8 hours prior to administration. Seven day infusions may be prepared by diluting the entire 7-day dose in 100ml of bacteriostatic 0.9% NaCl (containing 0.9% benzyl alcohol) and passing the diluent and drug through a sterile 0.22 micron filter as it is being prepared. When prepared in this fashion, acceptable chemical and physical stability has been demonstrated for at least 7 days. Supplier: Commercially available Toxicity: The dose limiting toxicity of cladribine is bone marrow suppression, which may be enhanced by combination with Ara-C. Immunosuppression and increased risk of opportunistic infections may also be seen. Nausea and vomiting are usually mild. Page 26 of 48 Salvage therapy S 2005 December 2005 Anorexia, diarrhea, headache, fever and chills and rash, pain, swelling and tenderness at the injection site are fairly common. Rarely, elevation in liver function tests and renal dysfunction have been reported. Delayed neurotoxicity, characterized by progressive, irreversible motor weakness of the upper and lower extremities has been reported with high doses (4-9 times the currently recommended doses). Cumulative thrombocytopenia requiring prolonged need for platelet transfusions occurs occasionally after multiple courses. The issue of second malignancy including EBV-induced lymphoproliferative disease has yet to be clarified. A limitation of fertility is a potential side effect, not already documented in human. Dosage and Route of administration: 9 mg/m2/d or 5 mg/m²/d i.v. in 250ml/m2 N/S as a 2-hours infusion daily for 3-5 days as per the protocol Cytarabine (Ara-C) (Cytosar-U) Source and Pharmacology: Cytarabine is a deoxycytidine analogue. It must be triphosphorylated to its active form, ARA-CTP, by deoxycytidine kinase and other nucleotide kinases. Ara-CTP inhibits DNA polymerase. In addition, ara-CTP is incorporated into DNA as a false base, causing inhibition of DNA synthesis. It is cell cycle, S phase specific. Cytarabine does penetrate the blood brain barrier. It is converted to its inactive form, uracil arabinoside, by pyrimidine nucleoside deaminase. Approximately 80% of the dose is recovered in the urine, mostly as uracil arabinoside (ara-U). Formulation and Stability: Cytarabine is available in multi-dose vials containing 100, 500, 1000 and 2000mg of lyophilized drug. Intact vials can be stored at room temperature. Reconstitute with sterile water or bacteriostatic water to a recommended Page 27 of 48 Salvage therapy S 2005 December 2005 concentration of 20mg/ml up to a 100mg/ml, except for IT administration. Reconstituted solution stable for 8 days at room temperature or refrigerated (concentration dependent). Supplier: Commercially available Toxicity: Myelosuppression is the dose limiting adverse effect, with leukopenia and thrombocytopenia being predominant. Other adverse effects reported commonly include nausea and vomiting (may be severe at high doses), diarrhea, mucositis, anorexia, alopecia, skin rash and liver dysfunction. A flu-like syndrome characterized by fever, muscle and bone aches is common. Less common side effects include allergic reactions and cellulitis at the injection site. High doses of cytarabine can cause conjunctivitis, hepatitis, and a group of CNS symptoms including somnolence, peripheral neuropathy, ataxia and personality changes. CNS symptoms are usually reversible and are more common in patients who have received previous cranial irradiation. In addition, a syndrome of sudden respiratory distress progressing to pulmonary edema has occurred. Dosage and Route of Administration: 500 mg/m2/dose i.v. over 2 hours, every 12 hours for 10 doses. Page 28 of 48 Salvage therapy S 2005 December 2005 Expected toxicity Drug combination The most severe life –threatening toxicity resulting from a combination of the 2 drugs is likely to be fever associated with neutropenia and sepsis Cladribine(2-CDA) (Leustatin) * Transient myelosuppression commonly requiring blood product support. Infections are common and appear to be associated with the degree of neutropenia. * Cumulative myelotoxicity especially prolonged thrombocytopenia can occur after multiple cycles. Thrombocytopenia lasting up to 6 months has been observed * Fever is common but does not appear to be a direct side effect of the drug and appears to correspond to periods of maximal cell lysis in patients with LCH or periods of neutropenia * Immunosuppression with monocytopenia and T-cell depletion occurs which may last for years. Significant opportunistic infections are uncommon except in the leukemic population. * 2-CdA does not appear to increase the incidence of second malignancies. However prolonged EBV infection and EBV–induced lympho proliferative disease have been rarely reported after high cumulative doses. * Severe irreversible neurotoxicity and nephrotoxicity has been observed and appears to be dose-related, occurring at doses of 0.4-0.5 mg/kg (16-20 mg/m²) day for 7-14 days in combination with Cyclophosphamide and Total Body Irradiation. Page 29 of 48 Salvage therapy S 2005 December 2005 * The neurotoxicity seen in adults with AML when the dose reached 19-21mg/m2 was an axonal peripheral polyneuropathy affecting lower limbs more than upper, and proximal muscles more than distal. At the doses suggested in this protocol, these toxicities appear to be rare, although neurotoxicity at lower doses in patients with pre-existing neurologic conditions have been described. *Mild nausea,abdominal pain, diarrhoea, fatigue, headache, skin rash and elevations of liver enzymes may occur. •Pulmonary toxicity and cardiotoxicity are not usually seen at these doses. •Sterility has been observed in animal models but is not documented in human. No significant drug interactions have been reported to date. Cytarabine (Ara-C) (Cytosar-U) * myelosuppression, nausea and vomiting, gastrointestinal mucosal damage including stomatitis, alopecia * a syndrome of fever, skin rash, conjunctivitis, malaise, myalgia and chest pain has been reported in children on standard doses. Steroid eye-drops are recommended when high dose Ara-C is given * neurotoxicity--mainly cerebellar dysfunction, primarily associated with high dose Ara-C, other complications predisposing conditions include renal and liver toxicty. Ara-C should be discontinued immediately if nystagmus or ataxia occur. Page 30 of 48 Salvage therapy S 2005 December 2005 Toxicity reporting Toxicity should be reported using standard WHO criteria / Appendix 2; using a specific sheet / Appendix 6. Any unexpected toxicity (WHO grade 4) must be reported to national study coordinator within 48 hours, as must any death, whatever the cause of death. Fever, prolonged and severe pancytopenia are considered as EXPECTED events during the two initial courses of 2-Cda and Ara-C and as UNEXPECTED during the maintenance therapy. The referring physician of the patient is responsible for the reporting of all unexpected severe toxicities to the study coordinator who is the national coordinator in EU, or the coordinator of the study in each center in north America. The study coordinator must inform the chairman of the study within 48 hours and the chairman must inform data monitoring safety committee of any unexpected event within 48 hours. The data safety monitoring committee in turn must provide advice regarding the interpretation of the unexpected event within a week and must make a recommendation about the continuation of the study, according to the arrest rules. The study coordinator will then inform the study committee. Once the advice of the committee has been received, a final decision is taken, which will then be transmitted to each national authority that has approved this clinical trial. Page 31 of 48 Salvage therapy S 2005 December 2005 Statistical considerations Langerhans cell histiocytosis is a rare disease. From published surveys of LCH patients, it is apparent that the inclusion criteria used here restrict this study to a very limited subset of the patients, likely representing less than 5% of all newly diagnosed LCH. There will likely be no more than 12 patients a year eligible for study, if all the participating countries include all their eligible patients. Two important considerations have been taken into account when restricting the inclusion criteria. First, this group of patients has an extremely poor outcome with standard approaches, compared to other LCH patients, who have an excellent short-term outcome. Secondly, the expected toxicities of the drug combination being evaluated in this study are significantly greater than the complications seen with standard first line therapy in LCH. So the restrictive inclusion criteria are used here to protect better prognosis LCH patients from an unduly toxic approach. The limited expected enrollment does not allow for a randomized trial. A phase II, open labeled trial design has therefore been chosen. The short term response rate, as for most phase II studies, will be used as the major end point of the study, based on the standard criteria for response in risk organs used in the previous LCH clinical trials (Non Active Disease/ Active Disease better or stable or worse). With regards to literature (1, 3, 5, 7), the best response rate of historical controls in this group of patient is about 25%. So, a response rate of less than 25% is unacceptable and that a response rate of 50% is achievable with this protocol. A Simon two-stage phase II study is designed with an unacceptable response rate of 25% and a promising response rate of 50%. 13 patients will be included in the first stage. If 3 responses are observed, the study will be stopped and the treatment declared ineffective. If 4 responses are observed, 17 additional patients will be included. At the end of the study (after the inclusion of 30 patients), the treatment will be declared promising if 11 responses are observed and ineffective if 10 responses are observed. Page 32 of 48 Salvage therapy S 2005 December 2005 The error rate (accepting a poor treatment) will be 0.09 and the error rate (rejecting a promising treatment) will be 0.08. Summary of the trial Type: Phase II open labeled study Major end point: Response rate at week 9-10 after therapy initiation. Good response is defined by Non Active disease or Active disease Better. Poor response is defined by Active disease Worse or Intermediate or Early death, whatever the cause of death Plan: Simon Plan/ Two steps Number of patients: Total 30 (13 at step 1 and 17 at step 2) Step 1: No. of patients 13: Arrest Rule: Step 1 (Interim analysis): If there are less than 4 responses, the treatment is considered as non effective. The trial is stopped Step 2: No. of patients: 17 Step 2: If there are less than 11 responses amongst the total number of patients (n=30) the treatment is considered as non effective. Otherwise, the treatment is considered as effective. The error rate (accepting a poor strategy) will be 9% and the error rate (rejecting a promising strategy) will be 8%. Page 33 of 48 Salvage therapy S 2005 December 2005 Appendix Page 34 of 48 Salvage therapy S 2005 December 2005 Appendix 1 : Risk organs definition Hematopoetic involvement: Anemia Leukocytopenia Thrombocytopenia haemoglobin <10 g/dl, infants < 9 g/dl leukocytes < 4,0 x109/l, <4000/mm3 platelets < 100 x 109/l <100,000/mm3 with or without bone marrow involvement. Bone marrow involvement is defined as the demonstration of CD1a positive cells on bone marrow smears. The clinical significance of CD1a positivity in the bone marrow remains to be proven. Spleen involvement: enlargement > 2 cm below costal margin (proven by sonography) Liver involvement: enlargement >3 cm below costal margin (proven by sonography) and/or total protein < 5,5 g/dl, albumin < 2,5 g/dl (not due to protein losing enteropathy) ascites edema hyperbilirubinemia with total bilirubin > 1,5 g/dl Lung involvement: typical changes on high resolution computed tomography (HR-CT) and/or histopathological diagnosis Page 35 of 48 Salvage therapy S 2005 December 2005 Appendix 2 : WHO toxicity criteria PARAMETER GRADE 1 GRADE 2 GRADE 3 GRADE 4 Hemoglobin > 3 mo.- < 2 y.o. 9.0-9.9 7.0-8.9 <7.0 Cardiac Failure 2ndary to anemia Hemoglobin > = 2 y.o. 10-10.9 7.0-9.9 <7.0 Cardiac Failure 2ndary to anemia Abs Neutrophil Ct 750-1200 400-749 250-399 <250 50,000-75,000 25,000-49,999 <25,000 or bleeding HEMATOLOGY Platelets PT 1.1-1.25xN 1.26-1.5xN 1.51-3.0xN >3xN PTT 1.1-1.66xN 1.67-2.33xN 2.34-3.0xN >3xN Bilirubin 1.1-1.9xN 2.0-2.9xN 3.0-7.5xN >7.5xN AST (SGOT) 1.1-4.9xN 5.0-9.9xN 10.0-15.0xN >15.0xN ALT (SGPT) 1.1-4.9xN 5.0-9.9xN 10.0-15.0xN >15.0xN GGT 1.1-4.9xN 5.0-9.9xN 10.0-15.0xN >15.0xN Pancreatic Amylase 1.1-1.4xN 1.5-1.9xN 2.0-3.0xN >3.0xN Total Amylase + Lipase* 1.1-1.4xN 1.5-2.4xN 2.5-5.0xN >5.0xN Uric Acid 7.5-9.9 10-12.4 12.5-15.0 >15.0 or Gout CPK See Neuromuscular Toxicity Abdominal Pain Mild ModerateNo Rx Needed ModerateRx Needed SevereHospital and Rx Diarrhea Soft stools Liquid stools Liquid Stools and Mild Dehydration Bloody stools Dehydration requiring IV therapy or Hypotensive Shock Constipation Mild Moderate Severe Distention and Vomiting Nausea Mild ModerateDecreased po intake SevereLittle po intake Unable to ingest food or fluid for >24 hours Vomiting <1 episode/day 1-3 episodes/day duration >3d GASTROINTESTINAL or >3 episodes/day duration >7d Page 36 of 48 or Intractable Vomiting PARAMETER GRADE 1 GRADE 2 GRADE 3 GRADE 4 RENAL AND ELECTROLYTES CREATININE 2 Month-2 Years 0.6-0.8 0.9-1.1 1.2-1.5 >1.5 2 Years-Adolescent 0.7-1.0 1.1-1.6 1.7-2.0 >2.0 Adolescents 1.0-1.7 1.8-2.4 2.5-3.5 >3.5 Creatinine Clearance 60-75 50-59 2 cc/min/1.73 m 35-49 2 cc/min/1.73 m <35 2 2 cc/min/1.73 m cc/min/1.73 m ELECTROLYTES High Sodium 145-149 150-155 >155 or mental status changes Low Sodium 130-135 129-124 <124 or mental status changes High Potassium 5.0-5.9 6.0-6.4 6.5-7.0 >7.0 or Cardiac arrhythmias Low Potassium 3.0-3.5 2.5-2.9 2.0-2.4 <2.0 High Calcium 10.5-11.2 11.3-11.9 12.0-12.9 >=13.0 Low Calcium 7.8-8.4 7.0-7.7 6.0-6.9 <6.0 Low Magnesium 1.2-1.4 0.9-1.1 0.6-0.8 <0.6 or Cardiac arrhythmias Hypoglycemia 55-65 40-54 30-39 <30 or Mental status changes Hyperglycemia 116-159 160-249 250-400 >400 or Ketoacidosis Proteinuria Tr-1+ <150 mg/day 2+ 150-499 mg/day 3+ 500-1000 mg/day 4+, or nephrotic syndrome >1000 mg/day Hematuria Microscopic <25 cells/hpf Microscopic >=25 cells/hpf Gross Obstruction or Transfusion requirement Comments Calcium values are corrected for albumin concentration. CrCl values do not apply to infants <2 months old. Salvage therapy S 2005 December 2005 OTHER SYMPTOM GRADE 1 GRADE 2 GRADE 3 GRADE 4 Allergy Pruritis without Rash Pruritic Rash Mild Urticaria Severe Urticaria Anaphylaxis, Angioedema 38.5-40 >40 Sustained Fever: >40, >5 days Diffuse maculopapular rash, dry desquamation Vesiculation, ulcers Exfoliative dermatitis, Stevens-Johnson or Erythema multiforme, Moist desquamation Painful, difficulty swallowing, but able to eat and drink Painful: unable to swallow solids Painful: requires IV fluids Drug (Rectal) Fever Cutaneous Stomatitis Mild discomfort Page 38 of 48 Salvage therapy S 2005 December 2005 CENTRAL NERVOUS SYSTEM SYMPTOM GRADE 1 GRADE 2 GRADE 3 GRADE 4 Seizures None 1 Uncomplicated Sz +/- Temp Elevation 1 Sz/Month for >=2 Consecutive Months Or 3 Sz over 6 Months; No Temp Elevation >1 Sz/Month; No Temp Elevation; No Decrease in Sz Frequency Despite dose reduction Headache <=1/Month <2 Hrs duration Mild >1/Month >2 Hrs Duration Moderate to Severe Responds to non-narcotic analgesia or prophylaxis >2/Month >2 Hrs Duration Moderate to Severe Responds to narcotic analgesia, or does not respond to prophylaxis >4/Month; >2 Hrs Duration; Moderate to Severe; Non-Responsive to narcotic Analgesia; or persistently Recurrent despite prophylaxis No decrease in frequency or Severity despite dose reduction Mental Status And Behavior Changes which do not Affect Function Changes requiring pharmacologic or other therapy; or mild lethargy, sedation or somnolence which resolves with rest Changes not improved by drugs or other therapies; or onset of confusion, memory impairment, lethargy, sedation, or somnolence which does not respond to rest Onset of delirium, obtundation, coma, or psychosis, or Grade 3 toxicity which does not respond to dose reduction Behavior refers to the development of attention deficits with or without hyperactivity, depression, mania, agitation, sleep disorders, phobias, obsessive-compulsive behaviors, or anxiety. Mental status refers to the level of consciousness, memory function, language and analytical operations, and non-dominant hemisphere functioning. Alternative explanations should be sought. Balance Posture & None None Ataxia, dizziness, vertigo, tremor, impaired postural balance Onset of movement disorder; or Grade 3 toxicity which does not respond to dosage adjustment "Ataxia" can be mistakenly diagnosed in the face of central weakness or peripheral neuropathy, which should not be considered a drug toxicity of this category. Movement disorders refer to tardive or other dyskinesias, dystonias, chorea, or ballismus. Alternative explanations should be sought. Page 39 of 48 Salvage therapy S 2005 December 2005 SYMPTOM GRADE 1 GRADE 2 GRADE 3 GRADE 4 Visual None Blurriness, diplopia, or horizontal nystagmus of < 1 hour duration, with spontaneous resolution > = 1 episode of Grade 2 symptoms per week, or an episode of Grade 2 Sx lasting 1 hour with spontaneous resolution by 4 hours or vertical nystagmus Decrease in visual acuity, visual field deficit, or oculogyric crisis, or Grade 3 Sx which persist after dose reduction Myelopathy None None None Myelopathic/spinal cord symptoms, such as: Pyramidal tract weakness and disinhibition, sensory level, loss of proprioception, bladder/bowel dysfunction Persistent or progressive paresthesias, burning sensation in feet, or mild dysesthesia; no weakness; mild to moderate deep tendon reflex changes; no sensory loss Onset of significant weakness, decrease or loss of DTRs, sensory loss in "stocking glove" distribution, radicular sensory loss, multiple cranial nerve involvement; bladder or bowel dysfunction, fasciculations, respiratory embarrassment from chest wall weakness. Grade 3 symptoms which do not resolve with dose reduction PERIPHERAL NERVOUS SYSTEM Neuropathy/ Lower Motor Neuronopathy None Mild transient Paresthesia only Infectious agents other than HIV can precipitate a neuropathy and should be considered, especially CMV. Neuropathies which do not resolve after dose reduction or discontinuation should be pursued for alternative infectious or non-infectious etiologies, since drugrelated neuropathies will usually resolve after dose reduction or drug discontinuation. It should be borne in mind that many subjects will worsen for up to one month after drug discontinuation prior to improvement ("coasting"). Abnormalities should be confirmed by nerve conduction studies (NCS) +/-electromyographic studies (EMG). Myopathy or Neuromuscular Junction Impairment Normal or mild (<2 x N) CPK elevation Mild proximal weakness and/or atrophy not affecting gross motor function. Mild myalgias, +/mild CPK elevation (<2 x N) Proximal muscle weakness and/or atrophy affecting motor function +/- CPK elevation; or severe myalgias with CPK >2 x N; Consider confirmatory EMG and/or muscle bx Onset of myasthenia-like symptoms (fatiguable weakness with external, variable ophthalmoplegia and/or ptosis), or neuromuscular junction blockade (acute paralysis) symptoms (confirm with EMG); or Grade 3 symptoms which do not resolve on dose adjustment; confirm with muscle bx HIV can produce a myopathy, and should be differentiated. Drug-induced myopathy can be accompanied by normal CPK levels. On occasion, neuropathic or central weakness can mimic myopathic weakness. Page 40 of 48 Salvage therapy S 2005 December 2005 SYMPTOM GRADE 1 GRADE 2 GRADE 3 GRADE 4 Clinical symptoms not otherwise specified in this table No therapy; monitor condition May require intervention monitoring minimal and Requires medical care and possible hospitalization Requires active medical intervention, hospitalization, or hospice care Laboratory values not otherwise specified in this table Abnormal, but requiring no immediate intervention; follow Sufficiently abnormal to require evaluation as to causality and perhaps mild therapeutic intervention, but not of sufficient severity to warrant immediate changes in study drug Sufficiently severe to require evaluation and treatment, including at least temporary suspension of study drug Life-threatening severity. Requires immediate evaluation, treatment, and usually hospitalization. Study drug must be stopped immediately and should not be restarted until the abnormality is clearly felt to be caused by some other mechanism that study drug. Page 41 of 48 Appendix 3: Data monitoring Time table Each evaluation must be communicated to the coordinator of the study in a timely fashion. The following variables will be used to define the inclusion criteria and will be used in the evaluation of the disease status during the follow up of the patients: Clinical data Biochemistry Hematology imaging Variables Week -1 End Course 1 End Course 2 Week 26 Week 52 Fever Spleen size Liver size Skin area Pain related to the disease Nb of RBC transfusion Nb of Platelets transfusion Nb of albumin perfusion Oxygen requirement ESR Complete Blood Count Liver enzyme Gamma GT or bilirubin Albumin Creatinin Calcium Phosphor Coagulation test T cell lymphocyte phenotype Ig G A M Ferritin Tumoral size in case of soft tissue tumor Lung CT (only at baseline and at week 9) + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + + Salvage therapy S 2005 December 2005 Appendix 4: Informed consent Informed consent : Must be written in the language of the patient / guardians Page 43 of 48 Salvage therapy S 2005 December 2005 Appendix 5 : LCH 2005 S Inclusion sheet (2 pages) To be faxed or mailed to Dr J Donadieu Service d’hémato oncologie Pédiatrique Hopital Trousseau 26 avenue du Dr Netter 75012 Paris FRANCE FAX : 33 1 44 73 65 73 by mail : [email protected] Patient initial : Inclusion date: Informed consent : Date of signature: Referring physician : name and address including e mail: Reference pathologist: name: Signature of the referring physician: Page 44 of 48 Salvage therapy S 2005 December 2005 LCH 2005 S Inclusion sheet (page 2) Patient Initial !___!___!___! Referring physician: Name: All the 5 following criteria must be present: a biopsy-proven definitive diagnosis of LCH AND Risk organ involvement (Appendix 1) AND Failure of initial therapy defined by disease progression in one or more risk organs except solely lung, after at least 6 weekly doses of vinblastine and 28 days of corticosteroid at a minimum dose of 40 mg/m², with or without the addition of a third drug. The patient will be eligible even if he/she has not been registered or treated “according to” the LCH-III protocol, however a similar initial treatment approach is required before inclusion on LCH-S-2005. If drugs other than vinblastine and corticosteroid have been given in the two months prior to the inclusion in this study, the coordinator of the study has to validate the inclusion in writing. Patients with reactivation in risk organ(s) except solely lung, resistant in one or more risk organs after at least 6 weekly doses of vinblastine and 28 days of corticosteroid at a minimum dose of 40 mg/m², may be enrolled in the study. AND Informed consent. All patients or their legal guardians (if the patient is below the legal age of consent), must sign a research ethics board approved consent form indicating their awareness of the investigational nature and the risks of this study. When appropriate, younger patients will be included in all discussions in order to obtain verbal assent. Exclusion criteria: The presence of any of the following criteria will exclude the patient from study: Isolated sclerosing cholangitis, with an inadequate liver function, as defined by biological liver abnormalities and typical imaging without evidence of active LCH as the only evidence of risk organ involvement Isolated lung involvement at any age as well as systemic disease with lung disease as the only risk organ involvement Inadequate renal function as defined by serum creatinine > 3x normal for age. Pregnancy or breast-feeding. Page 45 of 48 Salvage therapy S 2005 December 2005 Appendix 6 : LCH 2005 S Toxicity report sheet in case of severe adverse event OR DEATH Patient Initial !___!___!___! Name of the physician: Contact with referent physician: Description of event ...................................................................... Date of onset (DD / MM/YY) I__I__I I__I__I I__I__I Date of end (DD / MM/YY) I__I__I I__I__I I__I__I Did the event modify a preexisting condition Did the event result in death No Yes Progression Stable Regression Not applicable No Yes If death: Main cause If death: LCH status at the time of death No LCH activity LCH activity involving risk organs LCH activity but only in NON risk organs WHO grade 1 2 3 4 Frequency of the event Unique Temporary Permanent Not assessable Relation with the therapy NO DOUBTFUL PROBABLE NOT ASSESSABLE Symptomatic therapy: No Yes ......................................... Hospitalization or prolongation If yes duration No Yes Withdrawal of the therapy No Yes Temporary Other potential causes of adverse event ? If yes detailed : Outcome No Yes Total number of days...................................... ………………….................. Recovered Ongoing Other : .................................................................. Comments Page 46 of 48 Salvage therapy S 2005 December 2005 References 1. Gadner H, Grois N, Arico M, Broadbent V, Ceci A, Jakobson A et al. A randomized trial of treatment for multisystem langerhans'cell histiocytosis. Journal of Pediatrics 2001;138:728-34. 2. Berry DH, Gresik MV, Humphrey GB, Starling K, Vietti T, Boyett J et al. Natural history of histiocytosis X: a Pediatric Oncology Group Study. Med.Pediatr.Oncol. 1986;14:1-5. 3. Gadner H, Heitger A, Ritter J, Göbel U, Janka GE, Kühl J et al. Langerhanszell- Histiozytose im Kindesalter - Ergebnisse der DAL-HX 83 Studie. Klinishe Pädiat 1987;199:173-82. 4. Kilpatrick SE, Wenger DE, Gilchrist GS, Shives TC, Wollan PC, Unni KK. Langerhans' cell histiocytosis (Histiocytosis X) of bone; A clinicopathologic analysis of 263 pediatric and adult cases. Cancer 1995;76:2471-84. 5. The French Langerhans' Cell Histiocytosis Study Group. A multicentre retrospective survey of Langerhans' cell histiocytosis : 348 cases observed between 1983 and 1993. Arch Dis Child 1996;75:17-24. 6. Willis B, Ablin A, Weinberg V, Zoger S, Wara WM, Matthay KK. Disease course and late sequelae of Langerhans cell histiocytosis: 25-year experience at the University of California, San Francisco. J Clin Oncol 1996;14:2073-82. 7. Minkov M, Grois N, Heitger A, Potschger U, Westermeier T, Gadner H. Response to initial treatment of multisystem Langerhans cell histiocytosis: an important prognostic indicator. Med.Pediatr Oncol. 2002;39:581-5. 8. Braier J, Latella A, Balancini B, Castanos C, Rosso D, Chantada G et al. Outcome in children with pulmonary Langerhans cell Histiocytosis. Pediatr.Blood Cancer 2004;43:765-9. 9. Dimopoulos MA, Theodorakis M, Kostis E, Papadimitris C, Moulopoulos LA, Anastasiou-Nana M. Treatment of Langerhans cell histiocytosis with 2 chlorodeoxyadenosine. Leuk.Lymphoma 1997;25:187-9. 10. Frost JD, Wiersma SR. Progressive Langerhans cell histiocytosis in an infant with Klinefelter syndrome successfully treated with allogeneic bone marrow transplantation. J.Pediatr.Hematol.Oncol. 1996;18:396-400. 11. Grau J, Ribera JM, Tormo M, Indiano JM, Vercher J, Sandoval V et al. [Results of treatment with 2chlorodeoxyadenosine in refractory or relapsed Langerhans cell histiocytosis. Study of 9 patients]. Med.Clin.(Barc.) 2001;116:339-42. 12. Saven A, Figueroa ML, Piro LD, Rosenblatt JD. 2-Chlorodeoxyadenosine to treat refractory histiocytosis X. N.Engl.J.Med. 1993;329:734-5. 13. Saven A, Foon KA, Piro LD. 2-Chlorodeoxyadenosine-induced complete remissions in Langerhans-cell histiocytosis. Ann.Intern.Med. 1994;121:430-2. 14. Saven A, Piro LD. 2-Chlorodeoxyadenosine: a potent antimetabolite with major activity in the treatment of indolent lymphoproliferative disorders. Hematol Cell Ther 1996;38 Suppl 2:93-101. 15. Saven A, Burian C. Cladribine activity in adult langerhans-cell histiocytosis. Blood 1999;93:4125-30. 16. Stine KC, Saylors RL, Williams LL, Becton DL. 2-Chlorodeoxyadenosine (2-CDA) for the treatment of Page 47 of 48 Salvage therapy S 2005 December 2005 refractory or recurrent Langerhans cell histiocytosis (LCH) in pediatric patients. Med.Pediatr.Oncol. 1997;29:288-92. 17. Stine KC, Saylors RL, Saccente S, McClain KL, Becton DL. Efficacy of continuous infusion 2-CDA (cladribine) in pediatric patients with Langerhans cell histiocytosis. Pediatr.Blood Cancer 2004;43:814. 18. Weitzman S, Wayne AS, Arceci R, Lipton JM, Whitlock JA. Nucleoside analogues in the therapy of Langerhans cell histiocytosis: a survey of members of the histiocyte society and review of the literature. Med.Pediatr.Oncol. 1999;33:476-81. 19. Akkari V, Donadieu J, Piguet C, Bordigoni P, Michel G, Blanche S et al. Hematopoietic stem cell transplantation in patients with severe Langerhans cell histiocytosis and hematological dysfunction: Experience of the French Langerhans Cell Study Group. Bone Marrow Transplant. 2003;31:1097-103. 20. Steiner M, Matthes-Martin S, Peters C, Grois N, Minkov M, Attarbaschi A et al. Stem cell transplantation following reduced intensity conditionning regimen as therapeutic option for severe refractory langerhans cell histiocytosis. Histiocyte society XX meeting 2004;Abstract. 21. Bernard F, Thomas C, Bertrand Y, Munzer M, Landman-Parker J, Ouache M et al. Report of multicenter pilot study of 2-CdA and Ara-C combined chemotherapy in refractory Langerhans cell histiocytosis with hematological dysfunction. Eur J Cancer 2005;In press. 22. Egeler RM, de Kraker J, Voute PA. Cytosine-arabinoside, vincristine, and prednisolone in the treatment of children with disseminated Langerhans cell histiocytosis with organ dysfunction: experience at a single institution. Med.Pediatr.Oncol. 1993;21:265-70. 23. Crews KR, Gandhi V, Srivastava DK, Razzouk BI, Tong X, Behm FG et al. Interim comparison of a continuous infusion versus a short daily infusion of cytarabine given in combination with cladribine for pediatric acute myeloid leukemia. J.Clin.Oncol. 2002;20:4217-24. 24. Kornblau SM, Gandhi V, Andreef HM, Beran M, Kantarjian HM, Koller CA et al. Clinical and laboratory studies of 2-chlorodeoxyadenosine cytosine arabinoside for relapsed or refractory acute myelogenous leukemia in adults. Leukemia 1996;10:1563-9. 25. Donadieu J, Piguet C, Bernard F, Barkaoui M, Ouache M, Bertrand Y et al. A new clinical score for disease activity in Langerhans cell histiocytosis. Pediatr Blood Cancer 2004;43:1-7. 26. Simon R. Optimal two-stage designs for phase II clinical trials. Control Clin.Trials 1989;10:1-10. Page 48 of 48
