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用人III型嗜T淋巴细胞病毒/淋巴结病相关病毒(HTLV-III/LAV)对人单核细胞进行体外感染。

In vitro infection of human monocytes with human T lymphotropic virus type III/lymphadenopathy-associated virus (HTLV-III/LAV).

作者信息

Nicholson J K, Cross G D, Callaway C S, McDougal J S

出版信息

J Immunol. 1986 Jul 1;137(1):323-9.

PMID:3011909
Abstract

We explored the possibility that normal human monocytes can be infected with the retrovirus human T lymphotropic virus type III/lymphadenopathy-associated virus (HTLV-III/LAV). The T4 antigen, believed to be the receptor for HTLV-III/LAV binding to CD4 cells, is found on monocytes at low levels. Anti-T4A, which recognizes an epitope on the T4 molecule, inhibits viral binding to monocytes, and virus inhibits anti-T4A binding, although inhibition in both cases is not total. Virus particles were detected in HTLV-III/LAV-pulsed monocytes by electron microscopy as early as 10 min and for up to 3 days after inoculation, although budding virus was not observed. Monocytes were exposed to virus, were washed, and were cultured. Monocyte cultures were monitored by conventional assays for virus replication: immunofluorescence detection of cytoplasmic virus, supernatant reverse transcriptase activity, and supernatant virus antigen. These assays were either negative or at the lower limits of positivity. However, the amount of infectious virus was shown to increase over time in monocyte cultures by harvesting monocytes or their culture supernatants and titrating them into assay cultures containing stimulated T cells. Virus recovery from monocytes and virus recovery from T cells differed both quantitatively and qualitatively. Recovery from T cells and T cell supernatants peaked at 3 to 6 days and declined thereafter. Recovery from monocytes and monocyte supernatants increased over time in culture and never attained the levels of T cell cultures. Taken together, these studies indicate that HTLV-III/LAV binds to monocytes via the T4 molecule and enters the cells. Infectious virus is retained and increases with time in infected monocyte cultures. Both viral binding and infection are at low levels compared with levels in T cells. Unlike the usual infection of T cells characterized by high level virus replication with cell depletion, the infection appears to be persistent in monocytes.

摘要

我们探究了正常人单核细胞能否被逆转录病毒人类嗜T淋巴细胞病毒III型/淋巴结病相关病毒(HTLV-III/LAV)感染的可能性。T4抗原被认为是HTLV-III/LAV与CD4细胞结合的受体,在单核细胞上低水平表达。识别T4分子上一个表位的抗T4A可抑制病毒与单核细胞的结合,且病毒可抑制抗T4A的结合,不过在这两种情况下抑制都不完全。通过电子显微镜最早在接种后10分钟就能在HTLV-III/LAV脉冲处理的单核细胞中检测到病毒颗粒,且在接种后长达3天内都能检测到,尽管未观察到出芽病毒。将单核细胞暴露于病毒,洗涤后进行培养。通过常规检测方法监测单核细胞培养物中的病毒复制:检测细胞质病毒的免疫荧光、上清液逆转录酶活性以及上清液病毒抗原。这些检测结果要么为阴性,要么处于阳性下限。然而,通过收获单核细胞或其培养上清液并将其滴定到含有活化T细胞的检测培养物中,结果显示单核细胞培养物中感染性病毒的量会随时间增加。从单核细胞中回收病毒与从T细胞中回收病毒在数量和质量上均有所不同。从T细胞和T细胞上清液中回收病毒的量在3至6天达到峰值,之后下降。从单核细胞和单核细胞上清液中回收病毒的量在培养过程中随时间增加,且从未达到T细胞培养物中的水平。综上所述,这些研究表明HTLV-III/LAV通过T4分子与单核细胞结合并进入细胞。感染性病毒在受感染的单核细胞培养物中持续存在并随时间增加。与T细胞中的水平相比,病毒结合和感染水平均较低。与以高水平病毒复制和细胞耗竭为特征的T细胞通常感染情况不同,这种感染在单核细胞中似乎是持续性的。

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