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细小病毒 B19 的摄取是一个高度选择性的过程,由 VP1u 控制,这是病毒嗜性的一个新决定因素。

Parvovirus B19 uptake is a highly selective process controlled by VP1u, a novel determinant of viral tropism.

机构信息

Department of Chemistry and Biochemistry, University of Bern, Bern, Switzerland.

出版信息

J Virol. 2013 Dec;87(24):13161-7. doi: 10.1128/JVI.02548-13. Epub 2013 Sep 25.

Abstract

The VP1 unique region (VP1u) of human parvovirus B19 (B19V) is the immunodominant part of the viral capsid. Originally inaccessible, the VP1u becomes exposed upon primary attachment to the globoside receptor. To study the function of the exposed VP1u in B19V uptake, we expressed this region as a recombinant protein. Here, we report that purified recombinant VP1u binds and is internalized in UT7/Epo cells. By means of truncations and specific antibodies, we identified the most N-terminal amino acid residues of VP1u as the essential region for binding and internalization. Furthermore, the recombinant VP1u was able to block B19V uptake, suggesting that the protein and the virus undertake the same internalization pathway. Assays with different erythroid and nonerythroid cell lines showed that the N-terminal VP1u binding was restricted to a few cell lines of the erythroid lineage, which were also the only cells that allowed B19V internalization and infection. These results together indicate that the N-terminal region of VP1u is responsible for the internalization of the virus and that the interacting receptor is restricted to B19V-susceptible cells. The highly selective uptake mechanism represents a novel determinant of the tropism and pathogenesis of B19V.

摘要

人细小病毒 B19(B19V)的 VP1 独特区(VP1u)是病毒衣壳的免疫优势部分。最初不可接近,VP1u 在初次附着于神经节苷脂受体时暴露。为了研究暴露的 VP1u 在 B19V 摄取中的功能,我们将该区域表达为重组蛋白。在这里,我们报告纯化的重组 VP1u 结合并内化在 UT7/Epo 细胞中。通过截断和特异性抗体,我们确定 VP1u 的最 N 端氨基酸残基是结合和内化所必需的区域。此外,重组 VP1u 能够阻断 B19V 的摄取,表明该蛋白和病毒采用相同的内化途径。用不同的红细胞和非红细胞系细胞进行的测定表明,N 端 VP1u 结合仅限于少数红细胞系细胞系,这些细胞系也是允许 B19V 内化和感染的唯一细胞系。这些结果共同表明,VP1u 的 N 端区域负责病毒的内化,并且相互作用的受体仅限于 B19V 易感细胞。高度选择性的摄取机制代表了 B19V 嗜性和发病机制的新决定因素。

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