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Severe Aplastic Anemia following Parvovirus B19-Associated Acute Hepatitis

机译:细小病毒B19相关的急性肝炎后的严重再生障碍性贫血

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摘要

Human parvovirus (HPV) B19 is linked to a variety of clinical manifestations, such as erythema infectiosum, nonimmune hydrops fetalis, and transient aplastic anemia. Although a few cases have shown HPVB19 infection as a possible causative agent for hepatitis-associated aplastic anemia (HAAA) in immunocompetent patients, most reported cases of HAAA following transient hepatitis did not have delayed remission. Here we report a rare case of severe aplastic anemia following acute hepatitis with prolonged jaundice due to HPVB19 infection in a previously healthy young male. Clinical laboratory examination assessed marked liver injury and jaundice as well as peripheral pancytopenia, and bone marrow biopsy revealed severe hypoplasia and fatty replacement. HPVB19 infection was diagnosed by enzyme immunoassay with high titer of anti-HPVB19 immunoglobulin M antibodies. Immunosuppressive therapy was initiated 2 months after the onset of acute hepatitis when liver injury and jaundice were improved. Cyclosporine provided partial remission after 2 months of medication without bone marrow transplantation. Our case suggests that HPVB19 should be considered as a hepatotropic virus and a cause of acquired aplastic anemia, including HAAA.
机译:人细小病毒(HPV)B19与多种临床表现有关,例如感染性红斑,胎儿非免疫性积水和短暂再生障碍性贫血。尽管少数病例显示HPVB19感染是免疫功能正常的肝炎相关性再生障碍性贫血(HAAA)的可能病因,但大多数报道的短暂性肝炎后HAAA病例并没有延迟缓解。在这里,我们报道了在先前健康的年轻男性中,由于HPVB19感染而导致急性黄疸延长并导致黄疸延长的严重再生障碍性贫血的罕见病例。临床实验室检查评估了明显的肝损伤和黄疸以及周围的全血细胞减少症,骨髓活检显示严重的发育不全和脂肪替代。通过高滴度抗HPVB19免疫球蛋白M抗体的酶免疫分析法诊断出HPVB19感染。急性肝炎发作2个月后开始免疫抑制治疗,当肝损伤和黄疸得到改善时。服药2个月后,环孢素可部分缓解,无需骨髓移植。我们的案例表明,HPVB19应该被视为是一种肝炎病毒,并且是包括HAAA在内的获得性再生障碍性贫血的病因。

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