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Functional Replacement of the RING, B-Box 2, and Coiled-Coil Domains of Tripartite Motif 5α (TRIM5α) by Heterologous TRIM Domains

机译:三元基序5α(TRIM5α)的RING,B-Box 2和卷曲螺旋结构域被异源TRIM域功能性取代

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摘要

Tripartite motif 5α (TRIM5α) restricts some retroviruses, including human immunodeficiency virus type 1 (HIV-1), from infecting the cells of particular species. TRIM5α is a member of the TRIM family of proteins, which contain RING, B-box, coiled-coil (CC), and, in some cases, B30.2(SPRY) domains. Here we investigated the abilities of domains from TRIM proteins (TRIM6, TRIM34, and TRIM21) that do not restrict HIV-1 infection to substitute for the domains of rhesus monkey TRIM5α (TRIM5αrh). The RING, B-box 2, and CC domains of the paralogous TRIM6 and TRIM34 proteins functionally replaced the corresponding TRIM5αrh domains, allowing HIV-1 restriction. By contrast, similar chimeras containing the components of TRIM21, a slightly more distant relative of TRIM5, did not restrict HIV-1 infection. The TRIM21 B-box 2 domain and its flanking linker regions contributed to the functional defectiveness of these chimeras. All of the chimeric proteins formed trimers. All of the chimeras that restricted HIV-1 infection bound the assembled HIV-1 capsid complexes. These results indicate that heterologous RING, B-box 2, and CC domains from related TRIM proteins can functionally substitute for TRIM5αrh domains.
机译:三方基序5α(TRIM5α)限制了某些逆转录病毒(包括1型人类免疫缺陷病毒(HIV-1))感染特定物种的细胞。 TRIM5α是TRIM蛋白质家族的成员,该蛋白质包含RING,B-box,卷曲螺旋(CC),在某些情况下还包含B30.2(SPRY)域。在这里,我们研究了TRIM蛋白的结构域(TRIM6,TRIM34和TRIM21)的功能,这些结构域不限制HIV-1感染来代替恒河猴TRIM5α的结构域(TRIM5αrh)。同源的TRIM6和TRIM34蛋白的RING,B-box 2和CC结构域在功能上取代了相应的TRIM5αrh结构域,从而允许HIV-1限制。相比之下,包含TRIM21(TRIM5的亲戚稍远一点)的成分的类似嵌合体并没有限制HIV-1的感染。 TRIM21 B-box 2域及其侧翼接头区域有助于这些嵌合体的功能缺陷。所有嵌合蛋白形成三聚体。限制HIV-1感染的所有嵌合体都与组装的HIV-1衣壳复合物结合。这些结果表明,来自相关TRIM蛋白的异源RING,B-box 2和CC结构域可以在功能上替代TRIM5αrh结构域。

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