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自身整合屏障蛋白是1型人类免疫缺陷病毒整合的宿主因子。

The barrier-to-autointegration protein is a host factor for HIV type 1 integration.

作者信息

Chen H, Engelman A

机构信息

Department of Cancer Immunology and AIDS, Dana-Farber Cancer Institute, and Department of Pathology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Dec 22;95(26):15270-4. doi: 10.1073/pnas.95.26.15270.

Abstract

In vivo, retroviral integration is mediated by a large nucleoprotein complex, termed the preintegration complex (PIC). PICs isolated from infected cells display in vitro integration activity. Here, we analyze the roles of different host cell factors in the structure and function of HIV type 1 (HIV-1) PICs. PICs purified by size exclusion after treatment with high salt lost their integration activity, and adding back an extract from uninfected cells restored this activity. In parallel, the native protein-DNA intasome structure detected at the ends of HIV-1 by Mu-mediated PCR footprinting was abolished by high salt and restored by the crude cell extract. Various purified proteins previously implicated in retroviral PIC function then were analyzed for their effects on the structure and function of salt-treated HIV-1 PICs. Whereas relatively low amounts (5-20 nM) of human barrier-to-autointegration factor (BAF) protein restored integration activity, substantially more (5-10 microM) human host factor HMG I(Y) was required. Similarly high levels (3-8 microM) of bovine RNase A, a DNA-binding protein used as a nonspecific control, also restored activity. Mu-mediated PCR footprinting revealed that of these three purified proteins, only BAF restored the native structure of the HIV-1 protein-DNA intasome. We suggest that BAF is a natural host cofactor for HIV-1 integration.

摘要

在体内,逆转录病毒整合由一种大型核蛋白复合物介导,称为前整合复合物(PIC)。从感染细胞中分离出的PIC在体外具有整合活性。在此,我们分析了不同宿主细胞因子在1型人类免疫缺陷病毒(HIV-1)PIC的结构和功能中的作用。用高盐处理后通过尺寸排阻法纯化的PIC失去了其整合活性,而添加未感染细胞的提取物可恢复该活性。同时,通过Mu介导的PCR足迹法在HIV-1末端检测到的天然蛋白质-DNA整合酶结构被高盐破坏,并通过粗细胞提取物恢复。然后分析了先前与逆转录病毒PIC功能有关的各种纯化蛋白质对经盐处理的HIV-1 PIC的结构和功能的影响。虽然相对少量(5-20 nM)的人类自身整合屏障因子(BAF)蛋白可恢复整合活性,但需要更多(5-10 microM)的人类宿主因子HMG I(Y)。同样,作为非特异性对照的DNA结合蛋白牛RNase A的高水平(3-8 microM)也能恢复活性。Mu介导的PCR足迹法显示,在这三种纯化蛋白中,只有BAF能恢复HIV-1蛋白质-DNA整合酶的天然结构。我们认为BAF是HIV-1整合的天然宿主辅助因子。

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