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The TRIM5α B-Box 2 Domain Promotes Cooperative Binding to the Retroviral Capsid by Mediating Higher-Order Self-Association▿

机译:TRIM5αB-Box 2域通过介导高阶自缔合促进与逆转录病毒衣壳的协同结合

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摘要

The retroviral restriction factor, TRIM5α, blocks infection of a spectrum of retroviruses soon after virus entry into the cell. TRIM5α consists of RING, B-box 2, coiled-coil, and B30.2(SPRY) domains. The B-box 2 domain is essential for retrovirus restriction by TRIM5α, but its specific function is unknown. We show here that the B-box 2 domain mediates higher-order self-association of TRIM5αrh oligomers. This self-association increases the efficiency of TRIM5α binding to the retroviral capsid, thus potentiating restriction of retroviral infection. The contribution of the B-box 2 domain to cooperative TRIM5α association with the retroviral capsid explains the conditional nature of the restriction phenotype exhibited by some B-box 2 TRIM5α mutants; the potentiation of capsid binding that results from B-box 2-mediated self-association is essential for restriction when B30.2(SPRY) domain-mediated interactions with the retroviral capsid are weak. Thus, B-box 2-dependent higher-order self-association and B30.2(SPRY)-dependent capsid binding represent complementary mechanisms whereby sufficiently dense arrays of capsid-bound TRIM5α proteins can be achieved.
机译:逆转录病毒限制因子TRIM5α在病毒进入细胞后立即阻止了一系列逆转录病毒的感染。 TRIM5α由RING,B-box 2,螺旋线圈和B30.2(SPRY)域组成。 B-box 2结构域对于TRIM5α限制逆转录病毒必不可少,但其具体功能尚不清楚。我们在这里显示B框2域介导TRIM5αrh低聚物的高阶自缔合。这种自缔合增加了TRIM5α结合逆转录病毒衣壳的效率,从而增强了逆转录病毒感染的限制。 B-box 2结构域对与逆转录病毒衣壳协同TRIM5α缔合的贡献解释了某些B-box 2TRIM5α突变体表现出的限制性表型的条件性质。当B30.2(SPRY)域介导的与逆转录病毒衣壳的相互作用较弱时,由B-box 2介导的自缔合引起的衣壳结合的增强对于限制至关重要。因此,B框2依赖的高阶自缔合和B30.2(SPRY)依赖的衣壳结合代表了互补的机制,从而可以实现足够密集的衣壳结合TRIM5α蛋白阵列。

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  • 作者

    Li, Xing; Sodroski, Joseph;

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  • 年度 2008
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  • 原文格式 PDF
  • 正文语种 en
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