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1型人类免疫缺陷病毒与痘苗病毒在人离体淋巴组织中的相互作用

Interactions between human immunodeficiency virus type 1 and vaccinia virus in human lymphoid tissue ex vivo.

作者信息

Vanpouille Christophe, Biancotto Angélique, Lisco Andrea, Brichacek Beda

机构信息

Laboratory of Molecular and Cellular Biophysics, National Institute of Child Health and Human Development, Bethesda, MD 20892, USA.

出版信息

J Virol. 2007 Nov;81(22):12458-64. doi: 10.1128/JVI.00326-07. Epub 2007 Sep 5.

Abstract

Vaccinia virus (VACV) has been attracting attention recently not only as a vector for various vaccines but also as an immunization tool against smallpox because of its potential use as a bioterrorism agent. It has become evident that in spite of a long history of studies of VACV, its tissue pathogenesis remains to be fully understood. Here, we investigated the pathogenesis of VACV and its interactions with human immunodeficiency virus type 1 (HIV-1) in the context of human lymphoid tissues. We found that ex vivo-cultured tonsillar tissue supports productive infection by the New York City Board of Health strain, the VACV strain of the Dryvax vaccine. VACV readily infected both T and non-T (B) lymphocytes and depleted cells of both of these subsets equally over a 12-day period postinfection. Among T lymphocytes, CD8(+) cells are preferentially depleted in accordance with their preferential infection: the probability that a CD8(+) T cell will be productively infected is almost six times higher than for a CD4(+) T cell. T cells expressing CCR5 and the activation markers CD25, CD38, and HLA-DR are other major targets for infection by VACV in lymphoid tissue. As a consequence, VACV predominantly inhibits the replication of the R5(SF162) phenotype of HIV-1 in coinfected tissues, as R5-tropic HIV-1 requires activated CCR5(+) CD4(+) cells for productive infection. Human lymphoid tissue infected ex vivo by VACV can be used to investigate interactions of VACV with other viruses, in particular HIV-1, and to evaluate various VACV vectors for the purpose of recombinant vaccine development.

摘要

痘苗病毒(VACV)近来不仅作为多种疫苗的载体受到关注,还因其有可能被用作生物恐怖主义制剂而成为预防天花的免疫工具。尽管对VACV已有很长时间的研究,但很明显其组织发病机制仍有待充分了解。在此,我们在人类淋巴组织背景下研究了VACV的发病机制及其与人免疫缺陷病毒1型(HIV-1)的相互作用。我们发现,体外培养的扁桃体组织支持纽约市卫生局毒株(Dryvax疫苗的VACV毒株)的有效感染。VACV很容易感染T淋巴细胞和非T(B)淋巴细胞,并在感染后12天内同等程度地消耗这两个亚群的细胞。在T淋巴细胞中,CD8(+)细胞根据其优先感染而优先被消耗:CD8(+) T细胞被有效感染的概率几乎比CD4(+) T细胞高六倍。表达CCR5以及激活标志物CD25、CD38和HLA-DR的T细胞是VACV在淋巴组织中感染的其他主要靶点。因此,VACV在共感染组织中主要抑制HIV-1的R5(SF162)表型的复制,因为R5嗜性HIV-1需要活化的CCR5(+) CD4(+)细胞进行有效感染。体外被VACV感染的人类淋巴组织可用于研究VACV与其他病毒,特别是HIV-1的相互作用,并评估各种VACV载体以用于重组疫苗开发。

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