实时成像揭示了Env和Gag在HIV-1 T细胞病毒学突触上的顺序运输。

IF 2.7 3区 医学 Q3 VIROLOGY
Lili Wang, Sudeh Izadmehr, Edwin Kamau, Xiang-Peng Kong, Benjamin K Chen
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引用次数: 21

摘要

背景:在被感染和未感染的T细胞之间形成的称为病毒学突触(VS)的细胞粘附增强了HIV感染。VS是由细胞表面上的Env和CD4之间的相互作用引发的,并导致病毒组装聚集到细胞-细胞接触部位。然而,Env对VS的招募及其与Gag招募的关系并没有很好的定义。结果:为了研究HIV-1 Env通过VS的运输,我们构建了一个携带绿色荧光蛋白-Env融合蛋白的HIV分子克隆,称为HIV Env- isfgfp -∆V1V2。Env- isfgfp -∆V1V2融合蛋白本身不产生病毒颗粒,但可以通过与全长HIV构建体共转染而获救,并产生包装荧光Env的病毒颗粒。这些获救的荧光Env可以参与VS的形成,并可用于直接成像cd4依赖性Env从供体到靶细胞的跨VS转移。荧光标记的Gag和Env的运动到VS和转移到靶细胞也可以通过实时成像跟踪。延时实时成像显示,在细胞粘附后不久,在细胞-细胞接触部位有有限的Env积累,随后Gag重新分布到接触区域。结论:Env和Env以协调的时间序列被募集到VS中,随后通过突触一起转移到靶细胞。观察到,在VS形成过程中,Env积累比Gag再分布到接触区域要早。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Sequential trafficking of Env and Gag to HIV-1 T cell virological synapses revealed by live imaging.

Background: HIV infection is enhanced by cell adhesions that form between infected and uninfected T cells called virological synapses (VS). VS are initiated by an interaction between Env and CD4 on cell surfaces and result in the recruitment of virus assembly to the site of cell-cell contact. However, the recruitment of Env to the VS and its relationship to Gag recruitment is not well defined.

Results: To study the trafficking of HIV-1 Env through the VS, we constructed a molecular clone of HIV carrying a green fluorescent protein-Env fusion protein called, HIV Env-isfGFP-∆V1V2. The Env-isfGFP-∆V1V2 fusion protein does not produce virus particles on its own, but can be rescued by cotransfection with full-length HIV constructs and produce virus particles that package the fluorescent Env. These rescued fluorescent Env can participate in VS formation and can be used to directly image CD4-dependent Env transfer across VS from donor to target cells. The movements of fluorescently tagged Gag and Env to the VS and transfer into target cells can be also tracked through live imaging. Time lapse live imaging reveals evidence of limited Env accumulation at the site of cell-cell contact shortly after cell adhesion, followed by Gag re-distribution to contact area. Both Gag and Env can be recruited to form button-like spots characteristic of VS.

Conclusions: Env and Gag are recruited to the VS in a coordinated temporal sequence and subsequently transfer together across the synapse into the target cell. Env accumulations, when observed, are earlier than Gag re-distribution to the contact area during formation of VS.

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来源期刊
Retrovirology
Retrovirology 医学-病毒学
CiteScore
5.80
自引率
3.00%
发文量
24
审稿时长
>0 weeks
期刊介绍: Retrovirology is an open access, online journal that publishes stringently peer-reviewed, high-impact articles on host-pathogen interactions, fundamental mechanisms of replication, immune defenses, animal models, and clinical science relating to retroviruses. Retroviruses are pleiotropically found in animals. Well-described examples include avian, murine and primate retroviruses. Two human retroviruses are especially important pathogens. These are the human immunodeficiency virus, HIV, and the human T-cell leukemia virus, HTLV. HIV causes AIDS while HTLV-1 is the etiological agent for adult T-cell leukemia and HTLV-1-associated myelopathy/tropical spastic paraparesis. Retrovirology aims to cover comprehensively all aspects of human and animal retrovirus research.
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