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HIV-1 反义蛋白 ASP 是细胞膜表面的跨膜蛋白和病毒包膜的整合蛋白。

The HIV-1 Antisense Protein ASP Is a Transmembrane Protein of the Cell Surface and an Integral Protein of the Viral Envelope.

机构信息

Institute of Human Virology, University of Maryland School of Medicine, Baltimore, Maryland, USA.

Institute of Human Virology, University of Maryland School of Medicine, Baltimore, Maryland, USA

出版信息

J Virol. 2019 Oct 15;93(21). doi: 10.1128/JVI.00574-19. Print 2019 Nov 1.

Abstract

The negative strand of HIV-1 encodes a highly hydrophobic antisense protein (ASP) with no known homologs. The presence of humoral and cellular immune responses to ASP in HIV-1 patients indicates that ASP is expressed , but its role in HIV-1 replication remains unknown. We investigated ASP expression in multiple chronically infected myeloid and lymphoid cell lines using an anti-ASP monoclonal antibody (324.6) in combination with flow cytometry and microscopy approaches. At baseline and in the absence of stimuli, ASP shows polarized subnuclear distribution, preferentially in areas with low content of suppressive epigenetic marks. However, following treatment with phorbol 12-myristate 13-acetate (PMA), ASP translocates to the cytoplasm and is detectable on the cell surface, even in the absence of membrane permeabilization, indicating that 324.6 recognizes an ASP epitope that is exposed extracellularly. Further, surface staining with 324.6 and anti-gp120 antibodies showed that ASP and gp120 colocalize, suggesting that ASP might become incorporated in the membranes of budding virions. Indeed, fluorescence correlation spectroscopy studies showed binding of 324.6 to cell-free HIV-1 particles. Moreover, 324.6 was able to capture and retain HIV-1 virions with efficiency similar to that of the anti-gp120 antibody VRC01. Our studies indicate that ASP is an integral protein of the plasma membranes of chronically infected cells stimulated with PMA, and upon viral budding, ASP becomes a structural protein of the HIV-1 envelope. These results may provide leads to investigate the possible role of ASP in the virus replication cycle and suggest that ASP may represent a new therapeutic or vaccine target. The HIV-1 genome contains a gene expressed in the opposite, or antisense, direction to all other genes. The protein product of this antisense gene, called ASP, is poorly characterized, and its role in viral replication remains unknown. We provide evidence that the antisense protein, ASP, of HIV-1 is found within the cell nucleus in unstimulated cells. In addition, we show that after PMA treatment, ASP exits the nucleus and localizes on the cell membrane. Moreover, we demonstrate that ASP is present on the surfaces of viral particles. Altogether, our studies identify ASP as a new structural component of HIV-1 and show that ASP is an accessory protein that promotes viral replication. The presence of ASP on the surfaces of both infected cells and viral particles might be exploited therapeutically.

摘要

HIV-1 的负链编码一种高度疏水的反义蛋白(ASP),没有已知的同源物。在 HIV-1 患者中,针对 ASP 的体液和细胞免疫反应的存在表明 ASP 得到了表达,但它在 HIV-1 复制中的作用仍不清楚。我们使用抗 ASP 单克隆抗体(324.6)结合流式细胞术和显微镜方法,研究了多个慢性感染的髓样和淋巴样细胞系中的 ASP 表达。在基线和无刺激的情况下,ASP 表现出偏亚核分布,优先分布在抑制性表观遗传标记含量低的区域。然而,在用佛波醇 12-肉豆蔻酸 13-乙酸酯(PMA)处理后,ASP 易位到细胞质中,并且即使在没有细胞膜通透性的情况下,也可以在细胞表面检测到,这表明 324.6 识别的 ASP 表位是暴露在细胞外的。此外,用 324.6 和抗 gp120 抗体进行表面染色表明,ASP 和 gp120 共定位,提示 ASP 可能被整合到出芽病毒粒子的膜中。事实上,荧光相关光谱研究表明,324.6 与无细胞 HIV-1 颗粒结合。此外,324.6 能够以类似于抗 gp120 抗体 VRC01 的效率捕获和保留 HIV-1 病毒粒子。我们的研究表明,ASP 是 PMA 刺激的慢性感染细胞的质膜的固有蛋白,并且在病毒出芽时,ASP 成为 HIV-1 包膜的结构蛋白。这些结果可能为研究 ASP 在病毒复制周期中的可能作用提供线索,并表明 ASP 可能代表新的治疗或疫苗靶点。HIV-1 基因组包含一个以与所有其他基因相反的方向(即反义方向)表达的基因。这个反义基因的蛋白产物称为 ASP,其特征描述较差,其在病毒复制中的作用仍不清楚。我们提供的证据表明,HIV-1 的反义蛋白 ASP 存在于未刺激细胞的细胞核内。此外,我们表明,在用 PMA 处理后,ASP 离开细胞核并定位于细胞膜上。此外,我们证明 ASP 存在于病毒粒子的表面。总之,我们的研究将 ASP 鉴定为 HIV-1 的一种新的结构成分,并表明 ASP 是一种促进病毒复制的辅助蛋白。在感染细胞和病毒粒子的表面都存在 ASP,这可能具有治疗潜力。

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