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对源自艾滋病患者大脑和血液的全长人类免疫缺陷病毒1型env基因进行的遗传与功能分析。

Genetic and functional analysis of full-length human immunodeficiency virus type 1 env genes derived from brain and blood of patients with AIDS.

作者信息

Ohagen Asa, Devitt Amy, Kunstman Kevin J, Gorry Paul R, Rose Patrick P, Korber Bette, Taylor Joann, Levy Robert, Murphy Robert L, Wolinsky Steven M, Gabuzda Dana

机构信息

Department of Cancer Immunology and AIDS, Dana-Farber Cancer Institute, Boston, Massachusetts, USA.

出版信息

J Virol. 2003 Nov;77(22):12336-45. doi: 10.1128/jvi.77.22.12336-12345.2003.

Abstract

The genetic evolution of human immunodeficiency virus type 1 (HIV-1) in the brain is distinct from that in lymphoid tissues, indicating tissue-specific compartmentalization of the virus. Few primary HIV-1 envelope glycoproteins (Envs) from uncultured brain tissues have been biologically well characterized. In this study, we analyzed 37 full-length env genes from uncultured brain biopsy and blood samples from four patients with AIDS. Phylogenetic analysis of intrapatient sequence sets showed distinct clustering of brain relative to blood env sequences. However, no brain-specific signature sequence was identified. Furthermore, there was no significant difference in the number or positions of N-linked glycosylation sites between brain and blood env sequences. The patterns of coreceptor usage were heterogeneous, with no clear distinction between brain and blood env clones. Nine Envs used CCR5 as a coreceptor, one used CXCR4, and two used both CCR5 and CXCR4 in cell-to-cell fusion assays. Eight Envs could also use CCR3, CCR8, GPR15, STRL33, Apj, and/or GPR1, but these coreceptors did not play a major role in virus entry into microglia. Recognition of epitopes by the 2F5, T30, AG10H9, F105, 17b, and C11 monoclonal antibodies varied among env clones, reflecting genetic and conformational heterogeneity. Envs from two patients contained 28 to 32 N-glycosylation sites in gp120, compared to around 25 in lab strains and well-characterized primary isolates. These results suggest that HIV-1 Envs in brain cannot be distinguished from those in blood on the basis of coreceptor usage or the number or positions of N-glycosylation sites, indicating that other properties underlie neurotropism. The study also demonstrates characteristics of primary HIV-1 Envs from uncultured tissues and implies that Env variants that are glycosylated more extensively than lab strains and well-characterized primary isolates should be considered during development of vaccines and neutralizing antibodies.

摘要

1型人类免疫缺陷病毒(HIV-1)在大脑中的基因进化与在淋巴组织中的不同,这表明该病毒存在组织特异性分隔。来自未经培养的脑组织的原发性HIV-1包膜糖蛋白(Env)很少得到充分的生物学特性鉴定。在本研究中,我们分析了来自4例艾滋病患者未经培养的脑活检组织和血液样本中的37个全长env基因。对患者体内序列集进行的系统发育分析显示,相对于血液env序列,脑env序列有明显的聚类。然而,未鉴定出脑特异性特征序列。此外,脑env序列和血液env序列之间N-糖基化位点的数量或位置没有显著差异。共受体使用模式具有异质性,脑env克隆和血液env克隆之间没有明显区别。在细胞间融合试验中,9个Env使用CCR5作为共受体,1个使用CXCR4,2个同时使用CCR5和CXCR4。8个Env也可以使用CCR3、CCR8、GPR15、STRL33、Apj和/或GPR1,但这些共受体在病毒进入小胶质细胞过程中不发挥主要作用。2F5、T30、AG10H9、F105、17b和C11单克隆抗体对表位的识别在env克隆之间存在差异,反映了基因和构象的异质性。来自两名患者的Env在gp120中含有28至32个N-糖基化位点,而实验室菌株和特征明确的原发性分离株中约有25个。这些结果表明,不能根据共受体使用情况或N-糖基化位点的数量或位置来区分大脑中的HIV-1 Env和血液中的HIV-1 Env,这表明其他特性是神经嗜性的基础。该研究还展示了来自未经培养组织的原发性HIV-1 Env的特征,并意味着在疫苗和中和抗体的研发过程中,应考虑比实验室菌株和特征明确的原发性分离株糖基化程度更高的Env变体。

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