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人类胚胎星形胶质细胞HIV-1感染的病毒学和分子参数

Virological and molecular parameters of HIV-1 infection of human embryonic astrocytes.

作者信息

Di Rienzo A M, Aloisi F, Santarcangelo A C, Palladino C, Olivetta E, Genovese D, Verani P, Levi G

机构信息

Laboratory of Virology, Istituto Superiore di Sanità, Rome, Italy.

出版信息

Arch Virol. 1998;143(8):1599-615. doi: 10.1007/s007050050401.

DOI:10.1007/s007050050401
PMID:9739337
Abstract

Two different strains of HIV-1, the lymphotropic HIV-IIIB and the monocytotropic HIV-Ba-L, were able to infect tertiary cultures of astrocytes established from the human embryonic brain. The infection did not require contact with infected cells, as astrocytes were exposed to infectious cell-free supernatants. Except for an early transient peak of p24 consistently observed after infection with HIV-Ba-L, the infection of astrocytes appeared to be nonproductive. However, viral production was always observed when infected astrocytes were cocultured with permissive cells (CEM-SS or monocytes). To exclude the possibility that undetectable levels of virus are chronically produced by astrocytes, we exposed permissive cells to p24 negative supernatants taken from infected cultures. In such conditions permissive cells were never infected. Infection of astrocytes by HIV-1 was further supported by the finding that provirus persisted in these cells. Indeed, by a nested PCR, we detected HIV-1 DNA even one month after infection. Moreover, at the transcriptional level we observed expression of the multiply spliced RNA (tat and nef primers). Noteworthy, this pattern of HIV-1 expression did not change appreciably when astrocytes were pretreated and cultivated in the presence of IL-1 beta. Altogether, our data support the concept that astrocytes may play a role in the spread of HIV-1 infection within the brain and in the pathogenesis of neuro-AIDS.

摘要

两种不同的HIV-1毒株,嗜淋巴细胞的HIV-IIIB和嗜单核细胞的HIV-Ba-L,能够感染从人胚胎脑建立的星形胶质细胞第三代培养物。这种感染不需要与感染细胞接触,因为星形胶质细胞暴露于无细胞感染性上清液中。除了在感染HIV-Ba-L后始终观察到的早期短暂的p24峰值外,星形胶质细胞的感染似乎是非生产性的。然而,当感染的星形胶质细胞与允许性细胞(CEM-SS或单核细胞)共培养时,总是能观察到病毒产生。为了排除星形胶质细胞长期产生无法检测水平病毒的可能性,我们将允许性细胞暴露于从感染培养物中获取的p24阴性上清液中。在这种情况下,允许性细胞从未被感染。HIV-1对星形胶质细胞的感染进一步得到了前病毒在这些细胞中持续存在这一发现的支持。事实上,通过巢式PCR,我们甚至在感染后一个月检测到了HIV-1 DNA。此外,在转录水平上,我们观察到了多重剪接RNA(tat和nef引物)的表达。值得注意的是,当星形胶质细胞在IL-1β存在下进行预处理和培养时,这种HIV-1表达模式没有明显变化。总之,我们的数据支持星形胶质细胞可能在HIV-1感染在脑内的传播以及神经艾滋病发病机制中起作用这一概念。

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