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人细小病毒B19

Human parvovirus B19.

作者信息

Heegaard Erik D, Brown Kevin E

机构信息

Department of Clinical Microbiology, University State Hospital, Rigshospitalet, Copenhagen, Denmark.

出版信息

Clin Microbiol Rev. 2002 Jul;15(3):485-505. doi: 10.1128/CMR.15.3.485-505.2002.

DOI:10.1128/CMR.15.3.485-505.2002
PMID:12097253
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC118081/
Abstract

Parvovirus B19 (B19) was discovered in 1974 and is the only member of the family Parvoviridae known to be pathogenic in humans. Despite the inability to propagate the virus in cell cultures, much has been learned about the pathophysiology of this virus, including the identification of the cellular receptor (P antigen), and the control of the virus by the immune system. B19 is widespread, and manifestations of infection vary with the immunologic and hematologic status of the host. In healthy immunocompetent individuals B19 is the cause of erythema infectiosum and, particularly in adults, acute symmetric polyarthropathy. Due to the tropism of B19 to erythroid progenitor cells, infection in individuals with an underlying hemolytic disorder causes transient aplastic crisis. In the immunocompromised host persistent B19 infection is manifested as pure red cell aplasia and chronic anemia. Likewise, the immature immune response of the fetus may render it susceptible to infection, leading to fetal death in utero, hydrops fetalis, or development of congenital anemia. B19 has also been suggested as the causative agent in a variety of clinical syndromes, but given the common nature, causality is often difficult to infer. Diagnosis is primarily based on detection of specific antibodies by enzyme-linked immunosorbent assay or detection of viral DNA by dot blot hybridization or PCR. Treatment of persistent infection with immunoglobulin reduces the viral load and results in a marked resolution of anemia. Vaccine phase I trials show promising results.

摘要

细小病毒B19(B19)于1974年被发现,是已知对人类致病的细小病毒科的唯一成员。尽管无法在细胞培养物中繁殖该病毒,但人们对这种病毒的病理生理学已经有了很多了解,包括细胞受体(P抗原)的鉴定以及免疫系统对病毒的控制。B19广泛传播,感染的表现因宿主的免疫和血液学状态而异。在健康的免疫功能正常个体中B19是传染性红斑的病因,特别是在成年人中,是急性对称性多关节炎的病因。由于B19对红系祖细胞的嗜性,潜在溶血性疾病个体的感染会导致短暂性再生障碍危象。在免疫功能低下的宿主中,持续性B19感染表现为纯红细胞再生障碍和慢性贫血。同样,胎儿不成熟的免疫反应可能使其易受感染,导致宫内胎儿死亡、胎儿水肿或先天性贫血的发生。B19也被认为是多种临床综合征的病原体,但鉴于其普遍性,因果关系往往难以推断。诊断主要基于通过酶联免疫吸附测定检测特异性抗体,或通过斑点杂交或PCR检测病毒DNA。用免疫球蛋白治疗持续性感染可降低病毒载量并显著缓解贫血。疫苗I期试验显示出有希望的结果。

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Identification and characterization of a second novel human erythrovirus variant, A6.第二种新型人类红细胞病毒变体A6的鉴定与特征分析。
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