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Vinnytsia National Pirogov Memorial Medical University Department of Children Infectious Diseases “Approved” at sub-faculty meeting “__”_____2012, protocol №_____ Head of Department prof. _______I.I. Nezgoda STUDY GUIDE FOR INDEPENDENT WORK OF STUDENTS Topic: “Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types”. Course V English-speaking Students’ Medical Faculty Composed by assistant O.V. Bodnariuk Vinnitsa 2012 I. The theme urgency Toxoplasma infection is ubiquitous in animals and is one of the most common latent infections of humans throughout the world. The incidence varies considerably among people and animals in different geographic areas. Human cytomegalovirus (CMV) is a member of the Herpesviridae family with wide distribution. Most CMV infections are inapparent, but the virus can cause a variety of clinical illnesses that range in severity from mild to fatal. CMV is the most common congenital infection, which occasionally causes the syndrome of cytomegalic inclusion disease (hepatosplenomegaly, jaundice, petechia, purpura, and microcephaly). Herpes simplex virus 1 and 2 (HSV-1 and HSV-2) are two species of the herpes virus family, Herpesviridae, which cause infections in humans.[1] Eight members of herpes virus infect humans to cause a variety of illnesses including cold sores, chickenpox or varicella, shingles or herpes zoster (VZV), cytomegalovirus (CMV), and various cancers, and can cause brain inflammation (encephalitis). All viruses in the herpes family produce life-long infections. II. Startup aims of the study. To teach students major methods of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types and their treatment. Student should have knowledge: 1. Etiology and properties of the cause and causing factors of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 2. Epidemiology (source of infection, ways of transmission, age-old receptivity and morbidity) theirs. 3. Pathogenesis of disease, pathomorphologic changes in the skin and staggered organs. 4. Classification of clinical forms of herpetic infection. 5. Clinic of typical form of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types 6. Complications of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 7. Methods of laboratory research of these infection. 8. Principles of therapy of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 9. Measures of prophylaxis of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. A student should be able: 1. To follow the basic rules of work with a patient sick with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types 2. To take anamnesis with the estimation of epidemiology information (taking into account seasonality, origin of febricities, polymorphism of clinical signs of illness). 3. To examine a patient and reveal the basic clinical signs of illness. 4. To represent information of anamnesis and objective inspection in a hospital chart and formulate the preliminary diagnosis. 5. To write a plan of examination. 6. 7. 8. 9. To define a clinical diagnosis (form of disease, type, severity, course of disease). To prescribe the treatment taking into account age, severity of illness. To write out a prescription. To organize disease measures in the hearth of infection (to find out the source of infection, fill an urgent report in SES, to set a quarantine, to define the circle of contact persons). 10. To write epicrisis with the estimation of development of illness, results of inspection, efficiency of treatment, prognosis, by recommendations for a subsequent supervision or treatment depending on the form of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 11. Perform diagnostic options in patient with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 12. Make differential diagnosis. 13. Interpret data of laboratory studies. 14. Causes of complications of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in children . 15. Indications for hospitalization of children with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types.. 16. Principles of treatment of children with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 17. Discharge from hospital and attendance the children’s institutions by children with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. III. Educational aims of the study - forming the deontological presentations, skills of conduct with the patients; - to develop deontological presentations, be able to carry out deontology approach to the patient; - to develop the presentations of influence of ecological and socio-economic factors on the state of health; - to develop sense of responsibility for a time illness and loyalty of professional actions; - to acquire the skills of psychological contact establishment and creation of trusting relations between the doctor and the patient and his parents; - the development of responsibility sense for time illness and completeness of patient’s investigation. IV. The questions for self-check: 1. Indexes of morbidity from Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in Ukraine. 2. Sources of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 3. The ways of transmission of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in children. 4. Prophylactic measures in the hearth of infection. 5. Conditions necessary for development of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in children. 6. Duration of incubation period of the Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in children. 7. Clinical forms of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in children. 8. Clinical diagnostics of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types 9. What clinical forms of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types occur in children of early age? 10. Laboratory methods of inspection of the patients with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 11. What complications occur in children more frequently? 12. Causes of complications of Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types in children. 13. Indications for hospitalization of children with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 14. Principles of treatment of children with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. 15. Discharge from hospital and attendance the children’s institutions by children with Toxoplasmosis, Cytomegalovirus infection, Herpes simplex I, II types. V. The contents of a theme Toxoplasma gondii, an obligate intracellular protozoan, is acquired perorally, transplacentally, or, rarely, parenterally in laboratory accidents; by transfusion; or from a transplanted organ. In the immunologically normal child, the acute acquired infection may be asymptomatic, cause lymphadenopathy, or damage almost any organ. Once acquired, the latent encysted organism persists for the lifetime of the host. In the immunocompromised infant or child, either initial acquisition or recrudescence of latent organisms often causes signs or symptoms related to the central nervous system (CNS). Infection acquired congenitally, if untreated, almost always causes signs or symptoms in the perinatal period or later in life. The most frequent of these signs are due to chorioretinitis and CNS lesions. However, other manifestations, such as intrauterine growth retardation, fever, lymphadenopathy, rash, hearing loss, pneumonitis, hepatitis, and thrombocytopenia, also occur. Congenital toxoplasmosis in infants with human immunodeficiency virus (HIV) infection may be fulminant. ETIOLOGY. T. gondii is a coccidian protozoan. Its tachyzoites are oval or crescent-like, multiply only in living cells, and measure 2-4 × 4-7 mum. Tissue cysts, which are 10-100 mum in diameter, may contain thousands of parasites and remain in tissues, especially the CNS and skeletal and heart muscle, for the life of the host. Toxoplasma can multiply in all tissues of mammals and birds, and its disease spectrum is expressed with remarkable similarity in different host species. Newly infected cats and other Felidae excrete infectious Toxoplasma oocysts in their feces. Toxoplasma are acquired by susceptible cats by ingestion of infected meat containing encysted brandyzoites or by ingestion of oocysts excreted by other recently infected cats. The parasites then multiply through schizogonic and gametogonic cycles in the distal ileal epithelium of the cat intestine. Oocysts containing two sporocysts are excreted, and under proper conditions of temperature and moisture, each sporocyst matures into four sporozoites. For about 2 wk the cat excretes 105 -107 oocysts/day, which, in a suitable environment, may retain their viability for a year or more. Oocysts sporulate 1-5 days after excretion and are then infectious. Oocysts are killed by drying, boiling, and exposure to some strong chemicals, but not to bleach. Oocysts have been isolated from soil and sand frequented by cats, and outbreaks associated with contaminated water have been reported. Oocysts and tissue cysts are the sources of animal and human infections (Fig. 280-1) . EPIDEMIOLOGY. Toxoplasma infection is ubiquitous in animals and is one of the most common latent infections of humans throughout the world. The incidence varies considerably among people and animals in different geographic areas. In many areas of the world, approximately 5.35% of pork, 9-60% of lamb, and 0-9% of beef contain T. gondii organisms. Significant antibody titers have been detected in 50-80% of residents of some localities and in < 5% in others. A higher prevalence of infection usually occurs in warmer, more humid climates. Human infection is usually acquired by the oral route via undercooked or raw meat that contains cysts or by ingestion of oocysts. Freezing meat to -20°C or heating it to 66°C renders the cysts noninfectious. Outbreaks of acute acquired infection have occurred in families who have consumed the same infected food. Except for transplacental infection from mother to fetus and, rarely, by organ transplantation or transfusion, Toxoplasma are not transmitted from person to person. Seronegative transplant recipients who receive an organ (e.g., heart or kidney) from seropositive donors have experienced life-threatening illness requiring therapy. Seropositive recipients may have increased serologic titers without associated disease. Congenital Toxoplasmosis. Transmission to the fetus usually occurs when the infection is acquired by an immunologically normal mother during gestation. Congenital transmission from immunologically normal women infected prior to pregnancy is extremely rare. Immunocompromised women who are chronically infected have transmitted the infection to their fetuses. The incidence of congenital infection in the United States ranges from 1/1,000 to 1/8,000 live births. The incidence of newly acquired infection in a population of pregnant women depends on the risk of becoming infected in that specific geographic area and the proportion of the population that has not been previously infected. PATHOGENESIS. T. gondii is usually acquired by children and adults from ingesting food that contains cysts or that is contaminated with oocysts usually from acutely infected cats. Oocysts also may be transported to food by flies and cockroaches. When the organism is ingested, bradyzoites are released from cysts or sporozoites from oocysts, and the organisms then enter gastrointestinal cells. They multiply, rupture cells, and infect contiguous cells. They are transported via the lymphatics and disseminated hematogenously throughout the body. Tachyzoites proliferate, producing necrotic focuses surrounded by a cellular reaction. With the development of a normal immune response (humoral and cell-mediated), tachyzoites disappear from tissues. In immunodeficient individuals and some apparently immunologically normal patients, the acute infection progresses and may cause potentially lethal involvement such as pneumonitis, myocarditis, or necrotizing encephalitis. In acute acquired lymphadenopathic toxoplasmosis, characteristic lymph node changes include reactive follicular hyperplasia with irregular clusters of epithelioid histiocytes that encroach on and blur the margins of germinal centers. Focal distention of sinuses with monocytoid cells also occurs. Cysts form as early as 7 days after infection and remain for the life span of the host. During latent infection they produce little or no inflammatory response but cause recrudescent disease in immunocompromised patients or chorioretinitis in older children who acquired the infection congenitally. Congenital Toxoplasmosis. When a mother acquires the infection during gestation, the organism may disseminate hematogenously to the placenta. When this occurs, infection may be transmitted to the fetus transplacentally or during vaginal delivery. Of untreated maternal infections acquired in the first trimester, approximately 17% of fetuses are infected, usually with severe disease. Of untreated maternal infection acquired in the third trimester, approximately 65% of fetuses are infected, usually with disease that is mild or inapparent at birth. These different rates of transmission and outcomes are most likely related to placental blood flow, the virulence and amount of T. gondii acquired, and the immunologic ability of the mother to restrict parasitemia. Examination of the placenta of infected newborns may reveal chronic inflammation and cysts. Tachyzoites can be seen with Wright or Giemsa stains but are best demonstrated with the immunoperoxidase technique. The tissue cyst stains well with periodic acid-Schiff (PAS) and silver stains as well as with the immunoperoxidase technique. Gross or microscopic areas of necrosis may be present in many tissues, especially the central nervous system, choroid and retina, heart, lungs, skeletal muscle, liver, and spleen. Areas of calcification occur in the brain. Almost all congenitally infected individuals manifest signs or symptoms of infection, such as chorioretinitis, by adolescence if they are not treated in the newborn period. Some severely involved infants with congenital infection appear to have Toxoplasma antigen-specific anergy of their lymphocytes, which may be important in the pathogenesis of their disease. The predilection to predominant involvement of the CNS and eye in congenital infection has not been fully explained. Immunity. There are profound and prolonged alterations of T-lymphocyte populations during acute acquired T. gondii infections, but they have not correlated with outcome. Lymphocytosis, increased CD8+ count, and decreased CD4+ :CD8+ ratio are commonly present. Depletion of CD4+ cells in patients with acquired immunodeficiency syndrome (AIDS) may contribute to the severe manifestations of toxoplasmosis seen in these patients. CLINICAL MANIFESTATIONS. The manifestations of primary infection with T. gondii are highly variable and influenced primarily by host immunocompetence. Reactivation of previously asymptomatic congenital toxoplasmosis is usually manifest as ocular toxoplasmosis. Acquired Toxoplasmosis. Immunologically normal children who acquire the infection postnatally may have no clinically recognizable disease. When clinical manifestations are apparent, they may include almost any combination of fever, stiff neck, myalgia, arthralgia, maculopapular rash that spares the palms and soles, localized or generalized lymphadenopathy, hepatomegaly, hepatitis, reactive lymphocytosis, meningitis, brain abscess, encephalitis, confusion, malaise, pneumonia, polymyositis, pericarditis, pericardial effusion, and myocarditis. Chorioretinitis, usually unilateral, occurs in approximately 1% of cases. Symptoms may be present for a few days only or may persist many months. The most common manifestation is enlargement of one or a few lymph nodes in the cervical region. Cases of Toxoplasma lymphadenopathy rarely resemble infectious mononucleosis (due to Epstein-Barr virus or cytomegalovirus), Hodgkin disease, or other lymphadenopathies (Chapter 496) . In the pectoral area in older girls and women, the nodes may be confused with breast neoplasms. Mediastinal, mesenteric, and retroperitoneal lymph nodes may be involved. Involvement of intra-abdominal lymph nodes may be associated with fever and mimic appendicitis. Nodes may be tender but do not suppurate. Lymphadenopathy may appear and disappear for as long as 1 to 2 yr. Most patients with malaise and lymphadenopathy recover spontaneously without antimicrobial therapy. Significant organ involvement in immunologically normal individuals is uncommon, but some individuals have suffered significant morbidity. Ocular Toxoplasmosis. In the United States and Western Europe, T. gondii has been estimated to cause 35% of cases of chorioretinitis (Fig. 280-2) . In Brazil, retinal lesions with the appearance of toxoplasmic chorioretinitis have occurred in multiple members of the same family. Retinal lesions are present in 30% of those who are seropositive for T. gondii infection in Brazil. Manifestations include blurred vision, photophobia, epiphora, and, with macular involvement, loss of central vision. Findings due to congenital ocular toxoplasmosis also include strabismus, microophthalmia, microcornea, cataract, anisometropia, and nystagmus. Episodic recurrences are common, but precipitating factors have not been defined. Immunocompromised Persons. Congenital T. gondii infection in infants with AIDS is usually a fulminant, rapidly fatal disorder, involving brain and other organs such as the lung and heart. Disseminated T. gondii infections also occur in older children who are immunocompromised by AIDS, by malignancies and cytotoxic therapy or corticosteroids, or by immunosuppressive drugs given for organ transplantation. Immunocompromised individuals experience the clinical forms of Toxoplasma infection that occur in immunologically normal individuals. Signs and symptoms that are referable to the CNS are the most frequent manifestations of severe disease (occurring in 50% of patients), although other organs also may be involved, including the heart, gastrointestinal tract, and testes. Bone marrow transplant recipients present a special problem because active infection in these patients is difficult to diagnose. Specific antibody level may not increase in serum or may be absent. In most instances, active infection occurs in a child with prior evidence of latent infection. Individuals who have antibodies to T. gondii and HIV infection are at significant risk of development of toxoplasmic encephalitis, which may be the presenting manifestation of AIDS. In patients with AIDS, toxoplasmic encephalitis is fatal if not treated. Typical findings of CNS toxoplasmosis in patients with AIDS include fever, headache, altered mental status, psychosis, cognitive impairment, seizures and focal neurologic defects, including hemiparesis, aphasia, ataxia, visual field loss, cranial nerve palsies, and dysmetric or movement disorders. Uncommon findings of CNS involvement include meningismus, panhypopituitarism, and the syndrome of inappropriate antidiuretic hormone. In adult patients with AIDS, toxoplasmic retinal lesions are often large with diffuse necrosis and contain many organisms but little inflammatory cellular infiltrate. Toxoplasmic encephalitis and congenital toxoplasmosis are a particular problem in immunocompromised individuals from areas where the incidence of latent infection is high. Approximately 25-50% of patients with AIDS and Toxoplasma antibodies ultimately experience toxoplasmic encephalitis in the absence of prophylaxis with trimethoprim-sulfamethoxazole and treatment of HIV infection with protease inhibitors. The reason only a subpopulation of latently infected individuals experiences toxoplasmic encephalitis is unknown. A diagnosis of presumptive toxoplasmic encephalitis in patients with AIDS should prompt a therapeutic trial of medications effective against T. gondii. Clear clinical improvement within 7-14 days and improvement in findings of neuroradiological studies within 3 wk after therapy is initiated make the presumptive diagnosis almost certain. Congenital Toxoplasmosis. The signs and symptoms associated with acute acquired T. gondii infection in the pregnant woman are the same as those seen in the immunologically normal child, most commonly lymphadenopathy. Congenital infection also may be transmitted by an asymptomatic immunosuppressed woman (e.g., those treated with corticosteroids and those with HIV infection). GENETICS. In monozygotic twins the clinical pattern of involvement is most often similar, whereas in dizygotic twins manifestations often differ. In dizygotic twins severe manifestations in one twin have led to a diagnosis of subclinical disease in the other twin. Also, congenital infection has occurred in only one twin of a pair of dizygotic twins. The major histocompatibility complex (MHC) class II gene DQ3 appears to be more frequent in patients seropositive for T. gondii infection with AIDS and toxoplasmic encephalitis than in patients seropositive for T. gondii infection with AIDS who do not have toxoplasmic encephalitis, and in children with congenital toxoplasmosis and hydrocephalus as compared with those without hydrocephalus. SPECTRUM AND FREQUENCY OF SIGNS AND SYMPTOMS. Congenital infection may present as a mild or severe neonatal disease, with onset during the 1st month of life, or with sequelae or relapse of a previously undiagnosed infection at any time during infancy or later in life. A wide variety of manifestations of congenital infection occur in the perinatal period. These range from relatively mild signs, such as small size for gestational age, prematurity, peripheral retinal scars, persistent jaundice, mild thrombocytopenia, and cerebrospinal fluid pleocytosis, to the classic triad of signs consisting of chorioretinitis, hydrocephalus, and cerebral calcifications. Infection may result in erythroblastosis, hydrops fetalis, and perinatal death. More than half of congenitally infected infants are considered normal in the perinatal period, but almost all such children will have ocular involvement later in life. Neurologic signs in neonates, which include convulsions, setting-sun sign, and an increase in head circumference due to hydrocephalus, may be associated with substantial cerebral damage. However, such signs also may occur in association with encephalitis without extensive destruction or with relatively mild inflammation adjacent to and obstructing the aqueduct of Sylvius. If such infants are treated promptly, signs and symptoms may resolve, and they may develop normally. The spectrum and frequency of manifestations that develop in the perinatal period in infants with congenital Toxoplasma infection are presented in Table 280-1 . Infection in most of these 210 infants was initially suspected because their mothers were identified by a serologic screening program that detected pregnant women with acute acquired T. gondii infection. Twenty-one infants (10%) had severe congenital toxoplasmosis with CNS involvement, eye lesions, and general systemic manifestations. Seventy-one (34%) had mild involvement with normal clinical examination results other than retinal scars or isolated intracranial calcifications. One hundred and sixteen (55%) had no detectable manifestations; this may reflect the difficulties associated with funduscopic examination of the peripheral retina in infants and young children. These figures represent an underestimation of the relative frequency of severe congenital infection for the following reasons: The most severe cases, including most of those individuals who died, were not referred; therapeutic abortion was often performed when acute acquired infection of the mother was diagnosed early during pregnancy; in utero spiramycin therapy may have diminished the severity of infection; and only 13 infants had CT brain scans and 23% did not have a cerebrospinal fluid examination. Routine newborn examinations often yield normal findings for congenitally infected infants, but more careful evaluations may reveal significant abnormalities: Specifically, of 28 infants who were detected by a universal state mandated serologic screening program for T. gondii-specific immunoglobulin M (IgM), 26 had normal findings of routine newborn examinations and 14 had significant abnormalities detected with more careful evaluation. These abnormalities included retinal scars (7 infants), active chorioretinitis (3 infants), and CNS abnormalities (8 infants). The clinical spectrum and natural history of untreated congenital toxoplasmosis, which is clinically apparent in the first year of life, are presented in Table 280-2 . More than 80% of these children had IQ of less than 70, and many had convulsions and severely impaired vision. SKIN. Cutaneous manifestations in infants with congenital toxoplasmosis include rashes, petechiae, ecchymoses, or large hemorrhages secondary to thrombocytopenia. Rashes may be fine punctate, diffuse maculopapular, lenticular, deep blue-red, sharply defined macular, and diffuse blue papules. Macular rashes involving the entire body, including the palms and soles; exfoliative dermatitis; and cutaneous calcifications have been described. Jaundice due to hepatic involvement with T. gondii and/or hemolysis, cyanosis due to interstitial pneumonitis from congenital infection, and edema secondary to myocarditis or nephrotic syndrome may be present. Jaundice and conjugated hyperbilirubinemia may persist for months. SYSTEMIC SIGNS. From 25% to more than 50% of infants with clinically apparent disease at birth are born prematurely. Low Apgar scores also are common. Intrauterine growth retardation and instability of temperature regulation may occur. Other systemic manifestations include lymphadenopathy, hepatosplenomegaly, myocarditis, pneumonitis, nephrotic syndrome, vomiting, diarrhea, and feeding problems. Bands of metaphyseal lucency and irregularity of the line of provisional calcification at the epiphyseal plate may occur without periosteal reaction in the ribs, femurs, and vertebrae. Congenital toxoplasmosis may be confused with isosensitization causing erythroblastosis fetalis; the Coombs test result is usually negative with congenital T. gondii infection. ENDOCRINE ABNORMALITIES. Endocrine abnormalities may occur secondary to hypothalamic or pituitary involvement or endorgan involvement. The following have been reported: myxedema, persistent hypernatremia with vasopressin-sensitive diabetes insipidus without polyuria or polydipsia, sexual precocity, and partial anterior hypopituitarism. CENTRAL NERVOUS SYSTEM. Neurologic manifestations of congenital toxoplasmosis vary from massive acute encephalopathy to subtle neurologic syndromes. Toxoplasmosis should be considered as a cause of any undiagnosed neurologic disease in children < 1 yr of age, especially if retinal lesions are present. Hydrocephalus may be the sole clinical neurologic manifestation of congenital toxoplasmosis and may either be compensated or require shunt placement. Hydrocephalus may present in the perinatal period, progress after the perinatal period, or, less commonly, present later in life. Patterns of seizures are protean and have included focal motor seizures, petit and grand mal seizures, muscular twitching, opisthotonus, and hypsarrhythmia (which may resolve with corticotropin [ACTH] therapy). Spinal or bulbar involvement may be manifested by paralysis of the extremities, difficulty in swallowing, and respiratory distress. Microcephaly usually reflects severe brain damage, but some children with microcephaly due to congenital toxoplasmosis who have been treated appear to function normally in the early years of life. Untreated congenital toxoplasmosis that is symptomatic in the first year of life can cause substantial diminution in cognitive function and developmental delays. Intellectual impairment also occurs in some children with subclinical infection despite treatment with pyrimethamine and sulfonamides for 1 mo. Seizures and focal motor defects may become apparent after the newborn period, even when infection is subclinical at birth. Cerebrospinal fluid (CSF) abnormalities occur in at least one third of infants with congenital toxoplasmosis. Local production of T. gondii-specific antibodies may be demonstrated in CSF fluid of congenitally infected individuals (see later under Diagnosis). CT scan of the brain with contrast enhancement is useful to detect calcifications, determine ventricular size, image active inflammatory lesions and demonstrate porencephalic cystic structures (Fig. 280-3) . Calcifications occur throughout the brain, but there appears to be a special propensity for development of such lesions in the caudate nucleus (i.e., especially basal ganglia area), choroid plexus, and subependyma. Ultrasonography may be useful for following ventricular size in congenitally infected babies. Magnetic resonance imaging (MRI), CT with contrast enhancement, and radionucleotide brain scans may be useful for detecting active inflammatory lesions. EYES. Almost all untreated congenitally infected individuals will develop chorioretinal lesions by adulthood, and about 50% will have severe visual impairment. T. gondii causes a focal necrotizing retinitis in congenitally infected individuals (see Fig. 280-2) . Retinal detachment may occur. Any part of the retina may be involved, either unilaterally or bilaterally, including the maculae. The optic nerve may be involved, and toxoplasmic lesions that involve projections of the visual pathways in the brain or the visual cortex also may lead to visual impairment. In association with retinal lesions and vitritis, the anterior uvea may be intensely inflamed, leading to erythema of the external eye. Other ocular findings include cells and protein in the anterior chamber, large keratic precipitates, posterior synechiae, nodules on the iris, and neovascular formation on the surface of the iris, sometimes with an associated increase in intraocular pressure and development of glaucoma. The extraocular musculature may also be involved directly. Other manifestations include strabismus, nystagmus, visual impairment, and micro-ophthalmia. The differential diagnosis of lesions resembling those of ocular toxoplasmosis includes congenital colobomatous defect and other inflammatory lesions due to cytomegalovirus, Treponema pallidum, Mycobacterium tuberculosis, or vasculitis. Ocular toxoplasmosis is a recurrent and progressive disease that requires multiple courses of therapy. Couvreur et al. report limited data that suggest that occurrence of lesions in the early years of life may be prevented by instituting antimicrobial treatment (with pyrimethamine and sulfonamides in alternate months with spiramycin) during the first year of life. Brzin et al. have noted that treatment of the infected fetus in utero followed by treatment in the first year of life with pyrimethamine, sulfadiazine and leukovorin reduces the incidence and the severity of the retinal disease. EARS. Sensorineural hearing loss, both mild and severe, may occur. It is not known whether this is a static or progressive disorder. Treatment in the first year of life is associated with diminished occurrence of this sequela. CONCOMITANT INFECTIONS. Congenital toxoplasmosis in infants with HIV infection usually presents as a severe and fulminant illness with substantial CNS involvement but also may be more indolent in its presentation with focal neurologic deficits or systemic manifestations such as pneumonitis. DIAGNOSIS. Diagnosis of acute Toxoplasma infection can be established by isolation of T. gondii from blood or body fluids and also by demonstration of tachyzoites in sections or preparations of tissues and body fluids, cysts in the placenta or tissues of a fetus or newborn, and characteristic lymph node histologic features. Serologic tests also are very useful for diagnosis. Culture. Organisms are isolated by inoculation of body fluids, leukocytes, or tissue specimens into mice or tissue cultures. Body fluids should be processed and inoculated immediately, but T. gondii has been isolated from tissues and blood that have been stored at 4°C overnight. Freezing or treatment of specimens with formalin kills T. gondii. Six to 10 days after inoculation into mice, or earlier if mice die, peritoneal fluids should be examined for tachyzoites. If they survive for 6 wk and there is antibody in sera of the inoculated mouse, definitive diagnosis is made by visualization of Toxoplasma cysts in mouse brain. If cysts are not seen, subinoculations of mouse tissue into other mice are performed. Microscopic examination of tissue culture inoculated with T. gondii shows necrotic, heavily infected cells with numerous extracellular tachyzoites. Isolation of T. gondii from blood or body fluids reflects acute infection. Except in the fetus or neonate it is usually not possible to distinguish acute from past infection by isolation of T. gondii from tissues such as skeletal muscle, lung, brain, or eye obtained by biopsy or at autopsy. Diagnosis of acute infection can be made by demonstration of tachyzoites in biopsy tissue sections, bone marrow aspirate, or body fluids such as CSF or amniotic fluid. Immunofluorescent antibody and immunoperoxidase staining techniques may be necessary because it is often difficult to see the tachyzoite with ordinary stains. Tissue cysts are diagnostic of infection but do not differentiate between acute and chronic infection; the presence of many cysts suggests recent acute infection. Cysts in the placenta or tissues of the newborn infant establish the diagnosis of congenital infection. Characteristic histologic features strongly suggest the diagnosis of toxoplasmic lymphadenitis. Serologic Testing. Multiple serologic tests may be necessary to confirm the diagnosis of congenital or acutely acquired Toxoplasma infection. Each laboratory that reports serologic test results must have established values for their tests that diagnose infection in specific clinical settings, provide interpretation of their results, and assure appropriate quality control before therapy is based on serologic test results. Serologic test results used as the basis for therapy should be confirmed in a reference laboratory. The Sabin-Feldman dye test is sensitive and specific. It measures primarily IgG antibodies. Results should be expressed in international units (IU/mL), based on international standard reference sera available from the World Health Organization. The IgG indirect fluorescent-antibody (IgG-IFA) test measures the same antibodies as the dye test, and the titers tend to be parallel. These antibodies usually appear 1-2 wk after infection, reach high titers ( 1:1,000) after 6-8 wk, and then decline over months to years. Low titers (1:4 to 1:64) usually persist for life. Antibody titer does not correlate with severity of illness. Approximately half of the commercially available IFA kits for T. gondii have been found to be improperly standardized and may yield significant numbers of false-positive and false-negative results. An agglutination test (Bio-Merieux, Lyon, France) that is available commercially in Europe uses formalin-preserved whole parasites to detect IgM antibodies. This test is accurate, simple to perform, and inexpensive. The IgM indirect fluorescent antibody (IgM-IFA) test is useful for the diagnosis of acute infection with T. gondii in the older child because IgM antibodies appear earlier (often by 5 days after infection) and disappear sooner than IgG antibodies. In most instances, antibodies detected by the test rise rapidly (to levels of 1:50 to <1:1,000) and fall to low titers (1:10 or 1:20) or disappear after weeks or months. However, some patients continue to have positive results at low titers for as long as several years. The IgM-IFA test detects Toxoplasma-specific IgM in only approximately 25% of congenitally infected infants at birth. IgM antibodies also are often not present in sera of immunodeficient patients with acute toxoplasmosis or in most patients with active toxoplasmosis present only in the eye. The IgM-IFA test may yield false-positive results as a result of rheumatoid factor. The double-sandwich enzyme-linked immunosorbent assay (ELISA) is more sensitive and specific than the IgM-IFA test for detection of Toxoplasma IgM antibodies. In the older child, a level of IgM antibodies against Toxoplasma in serum of 2.0 or greater (value of one reference laboratory; each laboratory must establish its own values) indicates that Toxoplasma infection has most likely been acquired recently. IgM-ELISA detects approximately 75% of infants with congenital infection. IgMELISA avoids both the false-positive results due to rheumatoid factor and false-negative results due to high levels of passively transferred maternal IgG antibody in fetal serum, as occurs in the IgM-IFA test. Results obtained with commercial kits must be interpreted with caution since false-positive reactions are not infrequent. Care must also be taken to determine whether the kits have been standardized for diagnosis of infection in specific clinical settings (e.g., in the newborn infant). The IgA ELISA is a more sensitive test than the IgM ELISA for detection of congenital infection in the fetus and newborn as well as for detection of acute infection in some pregnant women. The immunosorbent agglutination assay (ISAGA) combines trapping of a patient's IgM to a solid surface and use of formalin-fixed organisms or antigen-coated latex particles. It is read as an agglutination test. There are no false-positive results due to rheumatoid factor or antinuclear antibodies. IgM antibodies to Toxoplasma are detected by the IgM-IFA test for a shorter time than they are by the IgM-ELISA. The IgM ISAGA is more sensitive than the IgM ELISA and may detect specific IgM antibodies before and for longer periods than the IgM ELISA. At present, IgM ISAGA is the best test for diagnosis of congenital infection in the newborn. The IgE ELISA and IgE ISAGA are also useful in establishing the diagnosis of congenital toxoplasmosis or acute acquired T. gondii infection. The differential agglutination test (HS/SC) compares antibody titers obtained with formalin-fixed tachyzoites (HS antigen) with titers obtained using acetone- or methanol-fixed tachyzoites (AC antigen) to differentiate recent and remote infections in adults and older children. This method may be particularly useful in differentiating remote infection in pregnant women, since levels of IgM and IgA antibodies detectable by ELISA or ISAGA may remain elevated for prolonged periods (e.g., months to years in adults and older children). The indirect hemagglutination (IHA) test measures different T. gondii antibodies from those measured in the IFA and dye tests. They may persist for years. However, the IHA test should not be used in infants with suspected congenital infection or in screening for infection acquired during pregnancy because it may be negative for too long a period early during infection. A relatively higher level of Toxoplasma antibody in the aqueous humor or in cerebrospinal fluid demonstrates local production of antibody during active ocular or CNS toxoplasmosis. This comparison is calculated as follows:Significant correlation coefficients [C] are 8 or more (eye), 4 or more (CNS for congenital infection), and over 1 (CNS for patients with AIDS). If the serum dye test titer is 300 IU/mL or more, most often it is not possible to demonstrate significant local antibody production using this formula with either the dye test or the IgM-IFA test titer. IgM antibody may be present in CSF. Toxoplasma antigen has been detected during acute Toxoplasma infection but not in sera of uninfected or chronically infected individuals. Antigen was present in the serum, amniotic fluid, and cerebrospinal fluid in the few infants tested with congenital infections. Comparative Western immunoblot tests of sera from a mother and baby may detect congenital infection. Infection is suspected when the mother's serum and her baby's serum contain antibodies that react with different Toxoplasma antigens. Enzyme-linked immunofiltration assay (ELIFA), using micropore membranes, permits simultaneous study of antibody specificity by immunoprecipitation and characterization of antibody isotypes by immunofiltration with enzyme-labeled antibodies. This method may be capable of detecting 85% of cases of congenital infection in the first few days of life. It is still being evaluated. Polymerase chain reaction (PCR) is used to amplify the DNA of T. gondii, which then can be detected by using a DNA probe. Detection of a repetitive T. gondii gene, the B1 gene, in amniotic fluid is the procedure of choice for establishing the diagnosis of congenital Toxoplasma infection in the fetus. The sensitivity and specificity of this test using amniotic fluid obtained at 18 weeks gestation are approximately 95%. PCR of vitreous fluid has been used to diagnose ocular toxoplasmosis. Lymphocyte blastogenesis to Toxoplasma antigens has been used to diagnose congenital toxoplasmosis if a question persists concerning the diagnosis and other test results are negative. However, a negative result does not exclude the diagnosis, as many infected infants do not respond to T. gondii antigens in the newborn period. Acquired Toxoplasmosis. Recent infection is diagnosed by seroconversion from a negative to a positive IgG antibody titer (in the absence of transfer of antibody by transfusion); a serial two-tube rise in Toxoplasma-specific IgG titer when sera are obtained 3 wk apart and tested in parallel; or the presence of Toxoplasma-specific IgM antibody. Ocular Toxoplasmosis. IgG antibody titers of 1:4 to 1:64 are usual in older children with active toxoplasmic chorioretinitis. When the retinal lesions are characteristic and serologic tests findings are positive, the diagnosis is likely. PCR of vitreous fluid has been used to diagnose ocular toxoplasmosis but is infrequently performed because of the risks associated with obtaining vitreous fluid. Immunocompromised Persons. IgG antibody titers may be low, and Toxoplasma-specific IgM is often absent in immunocompromised individuals with toxoplasmosis. Demonstration of Toxoplasma antigens or DNA in serum, blood, and CSF may identify disseminated Toxoplasma infection in immunocompromised persons. Resolution of CNS lesions during a therapeutic trial of pyrimethamine and sulfadiazine has been useful in patients with AIDS. Brain biopsy has been used to establish the diagnosis of toxoplasmic encephalitis when there is no response to this therapeutic trial or to exclude other likely diagnoses. Congenital Toxoplasmosis. Fetal ultrasound examination, performed every 2 wk during gestation, and PCR analysis of amniotic fluid are used for prenatal diagnosis. T. gondii may also be isolated from the placenta. Serologic tests are the most useful in establishing a diagnosis of congenital toxoplasmosis. Either persistent or rising titers in the dye or IFA test or a positive IgM ELISA or ISAGA result is diagnostic of congenital toxoplasmosis. The half-life of IgM is 3-5 days, so if there is a placental leak, the level of IgM antibodies in the infant's serum falls significantly within 1-2 wk. Passively transferred maternal IgG antibodies may require many months to a year to disappear from the infant's serum, depending on the magnitude of the original titer. Synthesis of Toxoplasma antibody is usually demonstrable by the third month of life if the infant is untreated. If the infant is treated, synthesis may be delayed until the ninth month of life, and, infrequently, it may not occur at all. When an infant begins to synthesize antibody, infection may be documented serologically even without demonstration of IgM antibodies by a rise in the ratio of specific serum antibody titer to the total IgG, whereas the ratio will fall if the specific antibody has been passively transferred from the mother. At birth, when a diagnosis of congenital toxoplasmosis is suspected, the following diagnostic studies should be performed: general, ophthalmologic, and neurologic examinations; head CT scan; attempt to isolate T. gondii from the placenta and the infant's white blood cells from umbilical cord blood and buffy coat; measurement of serum Toxoplasma-specific IgG, IgM, IgA, and IgE antibodies and the total amount of IgM and IgG in serum; lumbar puncture including analysis of CSF for cells, glucose, protein, Toxoplasma-specific IgG and IgM antibodies, and total amount of IgG; and evaluations of CSF for T. gondii by PCR and inoculation into mice. The presence of Toxoplasma-specific IgM in CSF that is not contaminated with blood, or local antibody production of Toxoplasma-specific IgG antibody demonstrated in CSF establishes the diagnosis of congenital Toxoplasma infection. Many manifestations of congenital toxoplasmosis occur in other perinatal diseases, especially disease caused by cytomegalovirus. Neither cerebral calcification nor chorioretinitis is pathognomonic. Fewer than 50% of children < 5 yr of age with chorioretinitis satisfy the serologic criteria for congenital toxoplasmosis; the causes of most of the other cases are unknown. The clinical picture in the newborn infant may also be compatible with sepsis, aseptic meningitis, syphilis, or hemolytic disease. TREATMENT. Pyrimethamine plus sulfadiazine or trisulfapyrimidines act synergistically against Toxoplasma. Combined therapy is indicated to treat many of the forms of toxoplasmosis. However, use of pyrimethamine is contraindicated during the first trimester of pregnancy. Spiramycin should be used to prevent transmission of infection to the fetus of acutely infected pregnant women and to treat congenital toxoplasmosis. Pyrimethamine inhibits the enzyme dihydrofolate reductase (DHFR), and thus the synthesis of folic acid, and therefore produces a dose-related, reversible, and usually gradual depression of the bone marrow, resulting in thrombocytopenia, leukopenia, and anemia. Neutropenia is the most common side effect in treated infants. All patients treated with pyrimethamine should have platelet and white blood cell counts twice weekly. Seizures may occur with overdosage of pyrimethamine. Folinic acid (calcium leukovorin) should always be administered concomitantly with pyrimethamine to prevent suppression of the bone marrow. Potential toxic effects of sulfonamides (e.g., crystalluria, hematuria, and rash) should be monitored. Hypersensitivity reactions occur, especially in patients with AIDS. Acquired Toxoplasmosis. Patients with lymphadenopathy do not need specific treatment unless they have severe and persistent symptoms or evidence of damage to vital organs. If such signs and symptoms occur, treatment with pyrimethamine, sulfadiazine, and leukovorin should be initiated. Patients who appear to be immunologically normal but have severe and persistent symptoms or damage to vital organs (e.g., chorioretinitis, myocarditis) need specific therapy until these specific symptoms resolve, followed by therapy for an additional 2 wk. This therapy usually lasts for at least 4-6 wk; the optimal duration of therapy is unknown. A loading dose of pyrimethamine for older children is 2 mg/kg/24 hr (maximum 50 mg), given for the first 2 days of treatment. The maintenance dose is 1 mg/kg/24 hr(maximum: 25 mg/24 hr). Folinic acid is administered orally at a dosage of 5-20 mg three times/wk (or even daily depending on the white blood cell count). Sulfadiazine or trisulfapyrimidine is administered to children >1 yr of age with a loading dose of 75 mg/kg/24 hr followed by 50 mg/kg/24 hr. Ocular Toxoplasmosis. Patients with ocular toxoplasmosis are usually treated with pyrimethamine, sulfadiazine, and leukovorin for approximately 1 wk after the lesion develops a quiescent appearance (i.e., sharp borders and associated inflammatory cells in the vitreous resolve), which usually occurs in 2-4 wk. Within 7-10 days the borders of the retinal lesions sharpen, and visual acuity usually returns to that noted before development of the acute lesion. Systemic corticosteroids have been administered concomitantly with antimicrobial treatment when lesions involve the macula, optic nerve head, or papillomacular bundle. Photocoagulation has been used to treat active lesions and prevent spread (i.e., most new lesions appear contiguous to old ones). Occasionally vitrectomy and removal of the lens are needed to restore visual acuity. Immunocompromised Persons. Serologic evidence of acute infection in an immunocompromised patient, regardless of whether signs and symptoms of infection are present or tachyzoites are present in tissue, are indications for therapy similar to that described for immunocompetent children with symptoms of organ injury. It is important to establish the diagnosis as rapidly as possible and institute treatment early. In immunocompromised patients other than those with AIDS, therapy should be continued for at least 4-6 wk beyond complete resolution of all signs and symptoms of active disease. Careful follow-up observation of these patients is imperative because relapse may occur, requiring prompt reinstitution of therapy. Relapse is frequent in patients with AIDS, and suppressive therapy with pyrimethamine and sulfonamides should be continued for life. Therapy usually induces a beneficial response clinically, but it does not eradicate cysts from the CNS and perhaps not from other tissues either. Prophylactic treatment with trimethroprim-sulfamethoxazole for Pneumocystis carinii pneumonia appears to reduce the incidence of toxoplasmosis in patients with AIDS. Treatment of Congenital Toxoplasmosis. All infected newborns should be treated, whether or not they have clinical manifestations of the infection. In infants with congenital infection, treatment may be effective in interrupting acute disease that damages vital organs. Infants should be treated for 1 yr with oral pyrimethamine (1-2 mg/kg/24 hr for 2 days, then 1 mg/kg/24 hr for 2 mo or 6 mo, then 1 mg/kg/24 hr Monday, Wednesday, and Friday), sulfadiazine or triple sulfonamides (100 mg/kg/24 hr loading dose, then 100 mg/kg/24 hr divided in 2 doses) and calcium leukovorin (5-10 mg/kg/24 hr Monday, Wednesday, and Friday). In the U.S. National Collaborative Study, the relative efficacy in reducing sequelae of infection and the safety of treatment, with 2 versus 6 months of the higher dosage of pyrimethamine are being compared. Pyrimethamine, available only in tablet form, may be crushed and administered in a suspension with juice or food. The effectiveness of these regimens has not been proved, but they are considered reasonable empirical recommendations. Information concerning the U.S. National Colloborative Study evaluating these regimens can be obtained from Dr. Rima McLeod by calling (773)-834-4152. Prednisone (1 mg/kg/24 hr orally in divided doses) has been utilized in addition when active chorioretinitis involves the macula or the CSF protein is 1,000 mg/dL at birth, but its efficacy also is not established. Treatment of Pregnant Women with T. gondii Infection. The immunologically normal pregnant woman who acquired T. gondii before conception does not need treatment to prevent congenital infection of her fetus. Although data are not available to allow for a definitive time interval, if infection occurs in the 6 mo prior to conception, it is reasonable to evaluate the fetus and treat to prevent congenital infection in the fetus in the same manner as described for the acutely infected pregnant patient. Treatment of a pregnant woman who acquires infection at any time during pregnancy reduces the chance of congenital infection in her infant by approximately 60%. The medications used are spiramycin and pyrimethamine in combination with sulfadiazine or triple sulfonamides. Spiramycin is available in the United States through the FDA (telephone 302-443-7580). Because pyrimethamine is potentially teratogenic, spiramycin is administered in the 1st trimester. The dose of spiramycin is 1 g each 8 hr given without food; lower doses are less effective. Toxicity is infrequent. Adverse reactions include paresthesias, rash, nausea, vomiting, and diarrhea. Treatment during the remainder of pregnancy with pyrimethamine and a sulfonamide should be continued at dosages similar to those recommended for therapy of the symptomatic immunocompetent patient with acquired toxoplasmosis. Treatment of the mother of an infected fetus with pyrimethamine and a sulfonamide reduces infection in the placenta and the severity of disease in the newborn. The approach in France to congenital toxoplasmosis includes systematic serologic screening of all women of childbearing age and again intrapartum. Mothers with acute infection are treated with spiramycin, which decreases the transmission from 60% to 23%. Ultrasound and amniocentesis for PCR after 18 wk gestation are used for fetal diagnosis; they have 97% sensitivity and 100% specificity. Fetal infection is treated with pyrimethamine and sulfadiazine, or by termination of pregnancy. This strategy has excellent outcome with normal development of children. Only 19% have subtle findings of congenital infection, including intracranial calcifications (13%) and chorioretinal scars (6%), although 39% have chorioretinal scars detected at follow-up observation during later childhood. Chronically infected pregnant women who have been immunocompromised by cytotoxic drugs or corticosteroid therapy have transmitted T. gondii to their fetuses. Such women should be treated with spiramycin throughout gestation. The best approach to prevention of congenital toxoplasmosis in the fetus of a pregnant woman with HIV infection and inactive T. gondii infection is unknown. If the pregnancy is not terminated, the mother should be treated with spiramycin during the first 17 wk of gestation and then with pyrimethamine and sulfadiazine until term. In a study of adult patients with AIDS, a dose of 75 mg pyrimethamine/24 hr and high dosages of intravenously administered clindamycin (1,200 mg every 6 hr intravenously) appeared equal in efficacy to sulfonamides and pyrimethamine. Other currently experimental agents include the macrolides roxithromycin and azithromycin. PROGNOSIS. Early institution of specific treatment for congenitally infected infants usually cures the manifestations of toxoplasmosis such as active chorioretinitis, meningitis, encephalitis, hepatitis, splenomegaly, and thrombocytopenia. Hydrocephalus due to aqueductal obstruction may develop or become worse during therapy. Such treatment also may reduce the incidence of some sequelae, such as diminished cognitive or abnormal motor function. Without therapy, chorioretinitis often recurs. Children with extensive involvement at birth may function normally later in life or have mild to severe impairment of vision, hearing, cognitive function, and other neurologic functions. Delays in diagnosis and therapy, perinatal hypoglycemia, hypoxia, hypotension, repeated shunt infections, and severe visual impairment are associated with a poorer prognosis. The prognosis is guarded but is not necessarily poor for infected babies. Treatment with pyrimethamine and sulfadiazine does not eradicate the encysted parasite. No protective vaccine is available. PREVENTION. Methods of prevention are outlined in Figure 280-1 . Counseling women about these methods of preventing transmission of T. gondii during pregnancy can substantially reduce acquisition of infection during gestation. Women who do not have specific antibody to T. gondii prior to pregnancy should only eat well cooked meat during pregnancy and avoid contact with oocysts excreted by cats. Cats that are kept in-doors, maintained on prepared diets, and not fed fresh, uncooked meat should not contact encysted T. gondii or shed oocysts. Serologic screening, ultrasound monitoring, and treatment of pregnant women during gestation can also reduce the incidence and manifestations of congenital toxoplasmosis. Human cytomegalovirus (CMV) is a member of the Herpesviridae family with wide distribution. Most CMV infections are inapparent, but the virus can cause a variety of clinical illnesses that range in severity from mild to fatal. CMV is the most common congenital infection, which occasionally causes the syndrome of cytomegalic inclusion disease (hepatosplenomegaly, jaundice, petechia, purpura, and microcephaly). In immunocompetent adults, the infection is occasionally characterized by a mononucleosis-like syndrome. In immunosuppressed individuals, including recipients of transplants and patients with AIDS, CMV pneumonitis, retinitis, and gastrointestinal disease are common and can be fatal. Primary infection occurs in a seronegative, susceptible host. Recurrent infection represents reactivation of latent infection or reinfection in a seropositive immune host. Disease may result from primary or recurrent CMV infection, but the former is a more common cause of severe disease. ETIOLOGY. CMV is the largest of the herpesviruses, with a genome of 240 kb and a virus diameter of 200 nm. It contains double-stranded DNA in a 64-nm core enclosed by an icosahedral capsid composed of 162 capsomers. The core is assembled in the nucleus of the host cells. The capsid is surrounded by a poorly defined amorphous tegument, which is itself surrounded by a loosely applied, lipid-containing envelope. The envelope is acquired during the budding process through the nuclear membrane into a cytoplasmic vacuole, which contains the protein components of the envelope. Mature viruses exit the cells by reverse pinocytosis. Serologic tests do not define specific serotypes. In contrast, restriction endonuclease analysis of CMV DNA shows that, although all known human strains are genetically homologous, none are identical unless they were obtained from epidemiologically related cases. EPIDEMIOLOGY. Seroepidemiologic surveys demonstrate CMV infection in every population examined worldwide. The prevalence of infection, which increases with age, is higher in developing countries and among lower socioeconomic strata of the more developed nations. Transmission sources of CMV include saliva, breast milk, cervical and vaginal secretions, urine, semen, stools, and blood. The spread of CMV requires very close or intimate contact because it is very labile. Transmission occurs by direct person-to-person contact, but indirect transmission is possible via contaminated fomites. The incidence of congenital infection ranges from 0.2-2.4% of all live births, with the higher rates in populations with a lower standard of living. The fetus may become infected as a consequence of primary and recurrent maternal infection. The risk for fetal infection is greatest with maternal primary CMV infection (40%) and much less likely with recurrent infection (< 1%). In the United States, from 14% of pregnant women acquire primary CMV infection, with as many as 8,000 newborns with neurodevelopmental sequelae associated with congenital CMV infection. Perinatal transmission is common, reaching 10-60% by 6 mo of age. The most important sources of virus are genital tract secretions at delivery and breast milk. Infected infants excrete virus for years in saliva and urine. After the 1st year of life, the prevalence of infection is dependent on group activities, with childcare centers contributing to the rapid spread of CMV in childhood. Infection rates of 50-80% during childhood are common. For children who are not exposed to other toddlers, the rate of infection increases very slowly throughout the first decade of life. A second peak occurs in adolescence as a result of sexual transmission. Seronegative child-care workers and parents of young children shedding CMV have a 1020% annual risk of acquiring CMV, which contrasts with 1-3% per year for the general population. Health care providers are not at increased risk for acquiring CMV infection from patients. Nosocomial infection is a hazard of transfusion of blood and blood products. In a population with a 50% prevalence of CMV infection, the risk has been estimated at 2.7% per unit of whole blood. Leukocyte transfusions pose a much greater risk. Infection is usually asymptomatic, but even in well children and adults there is a risk of disease if the recipient is seronegative and receives multiple units. Immunocompromised patients and seronegative premature infants have a much higher (10-30%) risk of disease. CMV infection is transmitted in transplanted organs (e.g., kidney, heart, and bone marrow). After transplantation, many patients excrete CMV as a result of infection acquired from the donor organ or from reactivation of latent infection caused by immunosuppression. Seronegative recipients of organs from seropositive donors are at greatest risk for severe disease. PATHOGENESIS. Cytomegalic cells are strikingly enlarged epithelial or mesenchymal cells with large intranuclear inclusions and smaller intracytoplasmic inclusions, and are pathognomonic for CMV infection. The virus induces focal mononuclear cell infiltrates, which may be present with or without cytomegalic cells. The virus may induce focal necrosis in the brain and liver, which may be extensive and accompanied by granulomatous change with calcifications. The lung, liver, kidney, gastrointestinal tract, and salivary and other exocrine glands are the most commonly affected organs, although the virus has been found in most cell types. The extent of abnormal organ function and the quantity of virus that can be recovered from infected organs are not related to the number of cytomegalic inclusion-bearing cells, which may be few or absent in each organ section examined. CLINICAL MANIFESTATIONS. The signs and symptoms of CMV infection vary with age, route of transmission, and immunocompetence of the patient. The infection is subclinical in most patients. In young children, primary CMV infection occasionally causes pneumonitis, hepatomegaly, hepatitis, and petechial rashes. In older children, adolescents, and adults, CMV may cause mononucleosis-like syndrome characterized by fatigue, malaise, myalgia, headache, fever, hepatosplenomegaly, abnormal liver function test results, and atypical lymphocytosis. The course of CMV mononucleosis is generally mild, lasting 2-3 wk. An occasional patient may present with persistent fever, overt hepatitis, or morbilliform rash, or a combination. Recurrent infections are asymptomatic in the immunocompetent host. Immunocompromised Hosts. In immunocompromised individuals, the risk of CMV disease is increased with both primary and recurrent infections (Chapter 179) . Illness with a primary infection includes pneumonitis (most common), hepatitis, chorioretinitis, gastrointestinal disease, or fever with leukopenia as isolated entities or as manifestations of generalized disease, which is often fatal. The risk is greatest in bone marrow transplant recipients and in patients with AIDS. Pneumonia, retinitis, and involvement of the central nervous system and gastrointestinal tract are usually severe and progressive. Submucosal ulcerations can occur anywhere in the gastrointestinal tract. Hemorrhage and perforation are known complications, as are pancreatitis and cholecystitis. Congenital Infection. The condition of symptomatic congenital CMV infection was originally called cytomegalic inclusion disease. Only 5% of all congenitally infected infants have severe cytomegalic inclusion disease, another 5% have mild involvement, and 90% are born with subclinical but chronic CMV infection. The most characteristic signs and symptoms include intrauterine growth retardation, prematurity, hepatosplenomegaly and jaundice, thrombocytopenia and purpura, and microcephaly and intracranial calcifications. Other neurologic problems include chorioretinitis, sensorineural hearing loss, and mild increases in cerebrospinal fluid protein. Symptomatic newborns are usually easy to identify. Most symptomatic congenital infections and those resulting in sequelae are caused by primary rather than recurrent infections in pregnant women. Asymptomatic congenital CMV infection is likely a leading cause of sensorineural hearing loss in young children, occurring in approximately 7% of infected infants. Perinatal Infection. Infections resulting from exposure to CMV in the maternal genital tract at delivery or in breast milk occur despite the presence of maternally derived, passively acquired antibody. Approximately 612% of seropositive mothers transmit CMV to their infants by contaminated cervical-vaginal secretions and 50% by breast milk. The majority of infants remain asymptomatic and do not exhibit sequelae. Occasionally, perinatally acquired CMV infection is associated with pneumonitis. Premature and ill fullterm infants may have neurologic sequelae and psychomotor retardation. However, the risk of hearing loss, chorioretinitis, and microcephaly does not appear to be increased. Seronegative premature infants with birth weights of <1,500 g with transfusion-acquired CMV infection have a 40% risk of experiencing hepatosplenomegaly, pneumonitis, gray pallor, jaundice, petechiae, thrombocytopenia, atypical lymphocytosis, and hemolytic anemia. DIAGNOSIS. Active CMV infection is best demonstrated by virus isolation from urine, saliva, bronchoalveolar washings, breast milk, cervical secretions, buffy coat, and tissues obtained by biopsy. Rapid (24 hr) identification is now routine with the centrifugation-enhanced rapid culture system based on the detection of CMV early antigens using monoclonal antibodies. Several methods are used for rapid detection of CMV antigens, and polymerase chain reaction (PCR) and DNA hybridization techniques are also available for rapid diagnosis. The presence of viral shedding and active infection does not distinguish between primary and recurrent infections. A primary infection is confirmed by seroconversion or the simultaneous detection of immunoglobulin (Ig) M as well as IgG antibodies. Rising IgG antibody titers may be caused by primary and recurrent infection and must be interpreted carefully. Sensitive and specific serologic tests to measure IgG antibodies are available in diagnostic laboratories. Complement fixation, neutralization, anticomplement immunofluorescence, and indirect immunofluorescence assays are preferable to define increases in antibody titers because they are quantitative. In contrast, radioimmunoassay (RIA) and enzyme-linked immunosorbent assay (ELISA) are less reliable for demonstrating significant changes in titers because most laboratories establish binding ratio (RIA) and absorbance units (ELISA) at a fixed serum dilution to compare the quantities of antibodies present in two sera. A simple increase in antibody titers in initially seropositive patients must be interpreted with caution because these are occasionally seen years after primary infection. IgG antibodies persist for life. IgM antibodies can be demonstrated transiently (4-16 wk) during the acute phase of symptomatic as well as asymptomatic primary infection in adults. RIA, ELISA, and an IgM capture RIA have acceptable specificity and sensitivity to detect primary infections. IgM antibodies are rarely found with these assays (0.2-1%) in patients with recurrent infection. A recurrent infection is defined by the reappearance of viral excretion in a patient known to have been seropositive in the past. The distinction between reactivation of endogenous virus and reinfection with a different strain of CMV requires restriction enzyme analysis of viral DNA to demonstrate polymorphisms between viral isolates. In immunocompromised patients, excretion of CMV, increases in IgG titers, and even the presence of IgM antibodies are common, making the distinction between primary and recurrent infections more difficult. Demonstrating viremia by buffy coat culture or detection of CMV DNA implies active disease and worse prognosis regardless of whether the type of infection is primary, recurrent, or uncertain. Congenital Infection. The definitive method for diagnosis of congenital CMV infection is virus isolation or demonstration of specific DNA sequences by PCR. This must be performed at or shortly after birth. Urine and saliva are the best specimens for culture. Infants with congenital CMV infection may excrete CMV in high titers in the urine for several months. An IgG antibody test is of little diagnostic value because a positive result also reflects maternal antibodies, although a negative result excludes the diagnosis of congenital CMV infection. Demonstration of stable or rising titers in serial specimens during the first year of life does not help because acquired infection in the first few months of life is common. In general, IgM tests lack sensitivity and specificity and are unreliable for diagnosis of congenital CMV infection. Congenital toxoplasmosis and syphilis must also be considered. CMV infection can be diagnosed in utero by isolation of the virus from the amniotic fluid. A negative culture does not exclude fetal infection because the interval between maternal infection and fetal infection is unknown. Although isolation of CMV by this means documents fetal infection, it does not indicate whether the newborn will have a symptomatic or an asymptomatic infection. TREATMENT. Ganciclovir combined with immune globulin, either standard intravenous immunoglobulin (IVIG) or hyperimmune CMV IVIG, has been used to treat life-threatening CMV infections in immunocompromised hosts (e.g., bone marrow, heart, and kidney transplant recipients and patients with AIDS). Two published regimens are ganciclovir (7.5 mg/kg/24 hr intravenously divided every 8 hr for 14 days) with CMV IVIG (400 mg/kg on days 1, 2, and 7, and 200 mg/kg on day 14); and ganciclovir (7.5 mg/kg/24 hr intravenously divided every 8 hr for 20 days with IVIG 500 mg/kg every other day for 10 doses). CMV retinitis and gastrointestinal disease appear to be clinically responsive to therapy but, like viral excretion, often recur on cessation. Toxicity with ganciclovir is frequent and often severe, including neutropenia, thrombocytopenia, liver dysfunction, reduction in spermatogenesis, and gastrointestinal and renal abnormalities. Foscarnet is an alternative antiviral agent, although there is limited information of its use in children. Congenital Infection. A phase II study with ganciclovir (12 mg/kg 24 hr for a total of 6 wk) showed hearing improvement or stabilization in 5 of 30 infants, suggesting efficacy. A randomized study of symptomatic congenital CMV infection is in progress. PROGNOSIS. Patients with CMV mononucleosis usually recover fully, although some have a protracted symptomatic illness. Most immunocompromised patients also recover uneventfully, but many experience severe pneumonitis, with a high fatality rate if hypoxemia develops. CMV infection and disease may be terminal events in individuals with increased susceptibility to infections such as patients with AIDS. Congenital Disease. The prognosis for normal development with symptomatic cytomegalic inclusion disease is poor; more than 90% of these children demonstrate central nervous system and hearing defects in later years. In infants with subclinical infection, the outlook is much better. The primary concern is the subsequent development of sensorineural hearing loss (5-10%), chorioretinitis (3-5%), and other less frequent manifestations such as developmental abnormalities, microcephaly, and neurologic deficits. PREVENTION. The use of CMV-free blood products, especially for premature newborns, and, whenever possible, the use of organs from CMV-free donors for transplantation represent important measures to prevent CMV infection and disease in patients at high risk. Pregnant women who are CMV seropositive are at low risk of delivering a symptomatic newborn. If possible, pregnant women should have a CMV serologic test, especially if they care for young children who are potential CMV excreters. Those who are CMV seronegative should be counseled regarding good handwashing and other hygienic measures and avoidance of contact with oral secretions of others. Passive Immunoprophylaxis. The use of IVIG or CMV IVIG for prophylaxis of infection in solid organ and bone marrow transplant recipients reduces the risk of symptomatic disease but does not prevent infection. The efficacy of prophylaxis is more striking when the hazard of primary CMV infection is greatest, such as in bone marrow transplantation. There is no consensus for a uniform prophylaxis regimen for CMV infection. Recommended regimens include either IVIG (1,000 mg/kg) or CMV IVIG (500 mg/kg) given as a single intravenous dose beginning within 72 hr of transplantation and once weekly thereafter until day 90-120 after transplantation. Active Immunization. The beneficial role of immunity is substantial, as illustrated by the fact that most severe disease follows primary infection, especially in congenital infection, transfusion-acquired infection, and infection in transplant recipients. Candidates for a CMV vaccine include seronegative women of childbearing age and seronegative transplant recipients. Live, attenuated vaccines such as the Towne strain prototype are immunogenic, but immunity wanes quickly. Vaccine virus does not seem to be transmissible. The vaccine does not protect renal transplant recipients from CMV infection, but appears to reduce the virulence of primary infection. In a study of vaccine efficacy in normal adult women, the Towne strain vaccine did not provide protection against naturally acquired infection. Other types of vaccines, such as subunit and recombinant vaccines, are being evaluated in early clinical trials. Herpes simplex virus 1 and 2 (HSV-1 and HSV-2) They are also called Human Herpes Virus 1 and 2 (HHV-1 and HHV-2) and are neurotropic and neuroinvasive viruses; they enter and hide in the human nervous system, accounting for their durability in the human body. HSV-1 is commonly associated with herpes outbreaks of the face known as cold sores or fever blisters, whereas HSV-2 is more often associated with genital herpes. An infection by a herpes simplex virus is marked by watery blisters in the skin or mucous membranes of the mouth, lips or genitals. Lesions heal with a scab characteristic of herpetic disease. However, the infection is persistent and symptoms may recur periodically as outbreaks of sores near the site of original infection. After the initial, or primary, infection, HSV becomes latent in the cell bodies of nerves in the area. Some infected people experience sporadic episodes of viral reactivation, followed by transportation of the virus via the nerve's axon to the skin, where virus replication and shedding occurs. Herpes is contagious if the carrier is producing and shedding the virus. This is especially likely during an outbreak but possible at other times. There is no cure yet, but there are treatments which reduce the likelihood of viral shedding. Transmission HSV is transmitted during close contact with an infected person who is shedding virus from the skin, in saliva or in secretions from the genitals. This horizontal transmission of the virus is more likely to occur when sores are present, although viral shedding, and therefore transmission, does occur in the absence of visible sores. In addition, vertical transmission of HSV may occur between mother and child during childbirth, which can be fatal to the infant. The immature immune system of the child is unable to defend against the virus and even if treated, the infection can result in inflammation of the brain (encephalitis) that may cause brain damage. Transmission occurs when the infant passes through the birth canal, but the risk of infection is reduced if there are no symptoms or exposed blisters during delivery. The first outbreak after exposure to HSV is commonly more severe than future outbreaks, as the body has not had a chance to produce antibodies; this first outbreak carries a low (~1%) risk of developing aseptic meningitis. Disorders HSV infection causes several distinct medical disorders. Common infection of the skin or mucosa may affect the face and mouth (orofacial herpes), genitalia (genital herpes), or hands (herpes whitlow). More serious disorders occur when the virus infects and damages the eye (herpes keratitis), or invades the central nervous system, damaging the brain (herpes encephalitis). Patients with immature or suppressed immune systems, such as newborns, transplant recipients, or AIDS patients are prone to severe complications from HSV infections. HSV infection has also been associated with bipolar disorder, schizophrenia and Alzheimer's disease, although this is often dependent on the genetics of the infected person . In all cases HSV is never removed from the body by the immune system. Following a primary infection, the virus enters the nerves at the site of primary infection, migrates to the cell body of the neuron, and becomes latent in the ganglion. As a result of primary infection, the body produces antibodies to the particular type of HSV involved, preventing a subsequent infection of that type at a different site. In HSV-1 infected individuals, seroconversion after an oral infection will prevent additional HSV-1 infections such as whitlow, genital herpes, and keratitis. Prior HSV-1 seroconversion seems to ameliorate the symptoms of a later HSV-2 infection, however HSV-2 can still be contracted. Most indications are that an HSV-2 infection contracted prior to HSV-1 seroconversion will immunize that person against HSV-1 infection. This is not necessarily good, as prior HSV-1 infection has the tendency to ameliorate the effects of symptomatic HSV-2 reoccurrences. Orofacial infection Herpes affects the face and mouth. Infection occurs when the virus comes into contact with oral mucosa or abraded skin. Infection by the type 1 strain of herpes simplex virus (HSV-1) is the most common cause of orofacial herpes, though cases of oral infection by the type 2 strain are increasing. Herpes infections are largely asymptomatic; when symptoms appear they will typically resolve within two weeks. The main symptom of oral infection is acute herpetic gingivostomatitis (inflammation of the mucosa of the cheek and gums), which occurs within 5– 10 days of infection. Other symptoms may also develop, including painful ulcers—sometimes confused with canker sores—fever, and sore throat. Primary HSV infection in adolescents frequently manifests as severe pharyngitis with lesions developing on the cheek and gums. Some individuals develop difficulty in swallowing (dysphagia) and swollen lymph nodes (lymphadenopathy). Primary HSV infections in adults often results in pharyngitis similar to that observed in glandular fever (infectious mononucleosis), but gingivostomatitis is less likely. Recurrent oral infection is more common with HSV-1 infections than with HSV-2. Prodromal symptoms often precede a recurrence. Symptoms typically begin with tingling (itching) and reddening of the skin around the infected site. Eventually, fluid-filled blisters form on the lip (labial) tissue and the area between the lip and skin (vermilion border). The recurrent infection is thus often called herpes simplex labialis. Rare reinfections occur inside the mouth (intraoral HSV stomatitis) affecting the gums, alveolar ridge, hard palate, and the back of the tongue, possibly accompanied by herpes labialis. Genital infection Following the classification HSV into two distinct categories of HSV-1 and HSV-2 in the 60s, it was established that "HSV-2 was below the waist, HSV-1 was above the waist". Although genital herpes is largely believed to be caused by HSV-2, genital HSV-1 infections are increasing and now exceed 50% in certain populations, and that rule of thumb no longer applies. HSV is believed to be asymptomatic in the majority of cases, thus aiding contagion and hindering containment. When symptomatic, the typical manifestation of a primary HSV-1 or HSV-2 genital infection is clusters of inflamed papules and vesicles on the outer surface of the genitals resembling cold sores. These usually appear 4–7 days after sexual exposure to HSV for the first time.Genital HSV-1 infection recurs at rate of about one sixth of that of genital HSV-2. Neonatal HSV infection is a rare but serious condition, usually caused by vertical transmission of HSV from mother to newborn. The majority of cases (85%) occur during birth when the baby comes in contact with infected genital secretions in the birth canal, an estimated 5% are infected in utero, and approximately 10% of cases are acquired postnatally. Detection and prevention is difficult because transmission is asymptomatic in 60% - 98% of cases. Neonatal HSV rates in the U.S. are estimated to be between 1 in 3,000 and 1 in 20,000 live births. Approximately 22% of pregnant women have had previous exposure to HSV-2, and an additional 2% acquire the virus during pregnancy, mirroring the HSV-2 infection rate in the general population.The risk of transmission to the newborn is 30-57% in cases where the mother acquired a primary infection in the third trimester of pregnancy. Risk of transmission by a mother with existing antibodies for both HSV-1 and HSV-2 has a much lower (1-3%) transmission rate. This in part is due to the transfer of significant titer of protective maternal antibodies to the fetus from about the seventh month of pregnancy. However, shedding of HSV1 from both primary genital infection and reactivations is associated with higher transmission from mother to infant. Neonatal herpes manifests itself in three forms: skin, eyes, and mouth herpes (SEM) sometimes referred to as "localized", disseminated herpes (DIS), and central nervous system herpes(CNS). SEM herpes is characterized by external lesions but no internal organ involvement. Lesions are likely to appear on trauma sites such as the attachment site of fetal scalp electrodes, forceps or vacuum extractors that are used during delivery, in the margin of the eyes, the nasopharynx, and in areas associated with trauma or surgery (including circumcision). DIS herpes affects internal organs, particularly the liver. CNS herpes is an infection of the nervous system and the brain that can lead to encephalitis. Infants with CNS herpes present with seizures, tremors, lethargy, and irritability, they feed poorly, have unstable temperatures, and their fontanelle (soft spot of the skull) may bulge. CNS herpes is associated with highest morbidity, and DIS herpes has a higher mortality rate. These categories are not mutually exclusive and there is often overlap of two or more types. SEM herpes has the best prognosis of the three, however, if left untreated it may progress to disseminated or CNS herpes with its attendant increases in mortality and morbidity. Death from neonatal HSV disease in the U.S. is currently decreasing; The current death rate is about 25%, down from as high as 85% in untreated cases just a few decades ago. Other complications from neonatal herpes include prematurity with approximately 50% of cases having a gestation of 38 weeks or less, and a concurrent sepsis in approximately one quarter of cases that further clouds speedy diagnosis. Reductions in morbidity and mortality are due to the use of antiviral treatments such as vidarabine and acyclovir. However, morbidity and mortality still remain high due to diagnosis of DIS and CNS herpes coming too late for effective antiviral administration; early diagnosis is difficult in the 20-40% of infected neonates that have no visible lesions. Harrison's Principles of Internal Medicine, recommends that pregnant women with active genital herpes lesions at the time of labor be delivered by caesarean section. Women whose herpes is not active can be managed with acyclovir. The current practice is to deliver women with primary or first episode non primary infection via caesarean section, and those with recurrrent infection vaginally, even in the presence of lesions because of the low risk (1-3%) of vertical transmission associated with recurrent herpes. Viral meningitis HSV-2 is the most common cause of Mollaret's meningitis, a type of recurrent viral meningitis. This condition was first described in 1944 by French neurologist Pierre Mollaret. Recurrences usually last a few days or a few weeks, and resolve without treatment. They may recur weekly or monthly for approximately 5 years following primary infection. Diagnosis Primary orofacial herpes is readily identified by clinical examination of persons with no previous history of lesions and contact with an individual with known HSV-1 infection. The appearance and distribution of sores in these individuals typically presents as multiple, round, superficial oral ulcers, accompanied by acute gingivitis. Adults with non-typical presentation are more difficult to diagnose. Prodromal symptoms that occur before the appearance of herpetic lesions help differentiate HSV symptoms from the similar symptoms of other disorders, such as allergic stomatitis. When lesions do not appear inside the mouth primary orofacial herpes is sometimes mistaken for impetigo, a bacterial infection. Common mouth ulcers (aphthous ulcer) also resemble intraoral herpes, but do not present a vesicular stage. Genital herpes can be more difficult to diagnose than oral herpes since most HSV-2infected persons have no classical symptoms.Further confusing diagnosis, several other conditions resemble genital herpes, including lichen planus, atopic dermatitis, and urethritis.Laboratory testing is often used to confirm a diagnosis of genital herpes. Laboratory tests include: culture of the virus, direct fluorescent antibody (DFA) studies to detect virus, skin biopsy, and polymerase chain reaction (PCR) to test for presence of viral DNA. Although these procedures produce highly sensitive and specific diagnoses, their high costs and time constraints discourage their regular use in clinical practice. Serological tests for antibodies to HSV are rarely useful to diagnosis and not routinely used in clinical practice, but are important in epidemiological studies. Serologic assays cannot differentiate between antibodies generated in response to a genital versus an oral HSV infection, and as such cannot confirm the site of infection. Absence of antibody to HSV-2 does not exclude genital infection because of the increasing incidence of genital infections caused by HSV-1. Antiviral medication Antiviral medications used against herpes viruses work by interfering with viral replication, effectively slowing the replication rate of the virus and providing a greater opportunity for the immune response to intervene. All drugs in this class depend on the activity of the viral enzyme thymidine kinase to convert the drug sequentially from its prodrug form to monophosphate (with one phosphate group), diphosphate (with two phosphate groups), and finally to the triphosphate (with three phosphate groups) form which interferes with viral DNA replication. The antiviral medication acyclovir There are several prescription antiviral medications for controlling herpes simplex outbreaks, including aciclovir (Zovirax), valaciclovir (Valtrex), famciclovir (Famvir), and penciclovir. Aciclovir was the original, and prototypical, member of this drug class; it is now available in generic brands at a greatly reduced cost. Valaciclovir and famciclovir—prodrugs of aciclovir and penciclovir, respectively—have improved solubility in water and better bioavailability when taken orally. Aciclovir is the recommended antiviral for suppressive therapy for use during the last months of pregnancy to prevent transmission of herpes simplex to the neonate in cases of maternal recurrent herpes.. The use of valaciclovir and famciclovir, while potentially improving treatment compliance and efficacy, are still undergoing safety evaluation in this context. Several studies with mice provide evidence that treatment with famciclovir soon after initial infection can help lower the incidence of future outbreaks, by reducing the amount of latent virus in the neural ganglia. A review of human subjects treated with famciclovir during their first herpes episode supports these findings, with only 4.2 percent of famciclovir-treated patients experiencing a recurrence within one to six months after the first outbreak, compared to 19 percent of acyclovir-treated patients. Despite these promising results, early famciclovir treatment for herpes has yet to find mainstream adoption. However, the potential effect on latency drops to zero a few months post-infection. Antiviral medications are also available as topical creams for treating recurrent outbreaks on the lips, although their effectiveness is disputed. Penciclovir cream has a 7-17 hour longer cellular half-life than aciclovir cream, increasing its effectiveness relative to aciclovir when topically applied. ]Tromantadine is available as a gel that inhibits the entry and spread of the virus by altering the surface composition of skin cells and inhibiting release of viral genetic material. Zilactin is a topical analgesic barrier treatment, which forms a "shield" at the area of application to prevent a sore from increasing in size, and decrease viral spreading during the healing process. Other drugs Cimetidine, a common component of heartburn medication, has been shown to lessen the severity of herpes zoster outbreaks in several different instances. This is an off-label use of the drug. It and probenecid have been shown to reduce the renal clearance of acyclovir. These compounds also reduce the rate, but not the extent, at which valaciclovir is converted into aciclovir. Another treatment is the use of petroleum jelly. Healing of cold sores is sped by barring water or saliva from reaching the sore. Vaccines Zostavax is a live vaccine developed by Merck & Co. (September, 2008) which has been shown to reduce the incidence of herpes zoster VI. Control materials for the preliminary and final stages of the lesson Tests and tasks 1. A 9-year-old boy has been ill for 2 days. Now he has fever up to 37,5°С, maculae, papules, vesicles on his skin, skin of the head. Vesicles are round, situated on an unindurated base, surrounded by erythematous corona. What is your diagnosis? A. Smallpox B. Scarlet fever C. Herpetic infection D. Streptodermia E. Varicella 2. A 7-year-old girl was in contact with a patient with herpes zoster. Fever up to 39,3°С, polymorphic rash (maculae, papules, crusts, vesicles) on her skin and mucous membranes of oral cavity have occurred at the 7th day of illness. What is your diagnosis? A. Smallpox B. Herpes simplex C. Herpes zoster D. Varicella E. Streptoderma 3. A 4-year-old girl has severe form of varicella. What medication should not be administered(choose one answer)? A. Acyclovir B. Specific immunoglobulin C. Recombinant interferon D. Inductor of endogenous interferon E. Steroid hormones 4. An 8-year-old boy is not ill with varicella. He had been in touch with the child, who had varicellas. He can fall ill within: A. 28 days B. 17 days C. 21 days D. 14 days E. 11-21 days 5. A 9 -year-old boy has fever, polymorphic rash - maculae, papules, vesicles and crusts on his face, skin of the head, trunk, limb and extremities. Severe headache, vomiting, ataxia, slow down and discoordination of motion have occured on the 10th day of illness. What the complication occurred? A. Encephalitis B. Serous meningitis C. Neyrotoxycosis D. Encephalitis reaction E. Meningo- encephalitis Correct answers for tests N Answers 1 E 2 D 3 A 4 E 5 A VII. Literature № Author(s) 1. Mikhailova A.M., Minkov I.P., Savchuk A.I. Publishing house Year of edition, vol., issue Number of pages Odessa 2003 236 Name of source City, (textbook, manual, monograph, etc.) Infection diseases in children. 2. Jonathan Cohan Infectious disease. Harcourt Publisher s limited 2004 2nd edition 2136 3. David C Dale Infectious diseases The clinician guide to Diagnosis, Treatment and Prevention. WebMD Corporati on 2004 edition 310 4. Duker Krugman's Infectious Diseases of Children. Mosby 11th edition 1574 5. Fleisher Textbook of Pediatric Emergency Medicine. 4th edition
