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Gain-of-Sensitivity Mutations in a Trim5-Resistant Primary Isolate of Pathogenic SIV Identify Two Independent Conserved Determinants of Trim5α Specificity

机译：致病性SIV的抗Trim5的主要分离株中的灵敏度增益突变可确定Trim5α特异性的两个独立的保守决定簇。

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Retroviral capsid recognition by Trim5 blocks productive infection. Rhesus macaques harbor three functionally distinct Trim5 alleles: Trim5α^Q, Trim5α^TFP and Trim5^CypA. Despite the high degree of amino acid identity between Trim5α^Q and Trim5α^TFP alleles, the Q/TFP polymorphism results in the differential restriction of some primate lentiviruses, suggesting these alleles differ in how they engage these capsids. Simian immunodeficiency virus of rhesus macaques (SIVmac) evolved to resist all three alleles. Thus, SIVmac provides a unique opportunity to study a virus in the context of the Trim5 repertoire that drove its evolution in vivo. We exploited the evolved rhesus Trim5α resistance of this capsid to identify gain-of-sensitivity mutations that distinguish targets between the Trim5α^Q and Trim5α^TFP alleles. While both alleles recognize the capsid surface, Trim5α^Q and Trim5α^TFP alleles differed in their ability to restrict a panel of capsid chimeras and single amino acid substitutions. When mapped onto the structure of the SIVmac239 capsid N-terminal domain, single amino acid substitutions affecting both alleles mapped to the β-hairpin. Given that none of the substitutions affected Trim5α^Q alone, and the fact that the β-hairpin is conserved among retroviral capsids, we propose that the β-hairpin is a molecular pattern widely exploited by Trim5α proteins. Mutations specifically affecting rhesus Trim5α^TFP (without affecting Trim5α^Q) surround a site of conservation unique to primate lentiviruses, overlapping the CPSF6 binding site. We believe targeting this site is an evolutionary innovation driven specifically by the emergence of primate lentiviruses in Africa during the last 12 million years. This modularity in targeting may be a general feature of Trim5 evolution, permitting different regions of the PRYSPRY domain to evolve independent interactions with capsid.

机译：Trim5识别逆转录病毒衣壳可阻止生产性感染。猕猴具有三个功能上不同的Trim5等位基因：Trim5α^{Q ，Trim5α^{TFP 和Trim5 ^{CypA 。尽管Trim5α^{Q 和Trim5α^{TFP 等位基因之间具有高度的氨基酸同一性，但Q / TFP多态性导致某些灵长类慢病毒的差异性限制，表明这些等位基因在他们如何参与这些衣壳。猕猴猿猴免疫缺陷病毒（SIVmac）进化为抵抗所有三个等位基因。因此，SIVmac提供了一个独特的机会来研究Trim5谱系中的一种病毒，从而推动了它在体内的进化。我们利用该衣壳的恒河猴Trim5α抗性来鉴定敏感性增益突变，以区分Trim5α^{Q 和Trim5α^{TFP 等位基因之间的靶标。虽然两个等位基因都识别衣壳表面，但Trim5α^{Q 和Trim5α^{TFP 等位基因在限制一组衣壳嵌合体和单个氨基酸取代方面的能力有所不同。当被映射到SIVmac239衣壳N末端结构域的结构上时，单个氨基酸取代影响映射到β-发夹的两个等位基因。考虑到所有取代都不会单独影响Trim5α^{Q ，并且在逆转录病毒衣壳中β-发夹是保守的，因此我们认为β-发夹是Trim5α蛋白广泛利用的分子模式。特异影响恒河猴Trim5α^{TFP 的突变（不影响Trim5α^{Q ）围绕灵长类慢病毒特有的保守位点，与CPSF6结合位点重叠。我们认为，以该站点为目标是一项进化创新，特别是由过去1200万年来非洲灵长类慢病毒的出现推动。这种针对性的模块化可能是Trim5进化的一般特征，允许PRYSPRY域的不同区域进化与衣壳的独立相互作用。}}}}}}}}}}}}

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期刊名称 PLoS Pathogens
作者
Kevin R. McCarthy; Aaron G. Schmidt; Andrea Kirmaier; Allison L. Wyand; Ruchi M. Newman; Welkin E. Johnson;
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年(卷),期 2013(9),5
年度 2013
页码 e1003352
总页数 15
原文格式 PDF
正文语种
中图分类微生物学;寄生动物、寄生虫学;医学寄生虫学;人体病毒学（致病病毒）;病毒（滤过性病毒）;
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1. Gain-of-Sensitivity Mutations in a Trim5-Resistant Primary Isolate of Pathogenic SIV Identify Two Independent Conserved Determinants of Trim5α Specificity [J] . Kevin R. McCarthy, Aaron G. Schmidt, Andrea Kirmaier, PLoS Pathogens . 2013,第5期

机译：致病性SIV的抗Trim5的主要分离株中的灵敏度增益突变可识别Trim5α特异性的两个独立的保守决定簇。
2. Chaperonin GroEL: a novel phylogenetically conserved protein with strong immunoreactivity of Avian Pathogenic Escherichia coli isolates from duck identified by immunoproteomics. [J] . Bao YinLi, Zhai ZhiPeng, Wang ShaoHui, Vaccine . 2013,第28期

机译：伴侣蛋白GroEL：一种新型的系统保守蛋白，具有免疫组学特性，可从禽类中分离出具有强免疫反应活性的禽病原大肠杆菌。
3. Phosphotyrosine signaling analysis of site-specific mutations on EGFRvIII identifies determinants governing glioblastoma cell growth [J] . Paul H. Huang, Emily R. Miraldi, Alexander M. Xu, Molecular BioSystems . 2010,第7期

机译：EGFRvIII上位点特异性突变的磷酸酪氨酸信号转导分析可确定决定胶质母细胞瘤细胞生长的决定因素
4. IDENTIFY CANCER DRIVER GENES THROUGH SHARED MENDELIAN DISEASE PATHOGENIC VARIANTS AND CANCER SOMATIC MUTATIONS [C] . MENG MA, CHANGCHANG WANG, BENJAMIN S. GLICKSBERG, Pacific Symposium on Biocomputing . 2017

机译：通过共享孟德尔疾病致病性变异和癌细胞突变来识别癌症司机基因
5. Effect of antigenic site mutations on the binding specificity of an anti-hemagglutinin antibody to H3N2 influenza virus isolates. [D] . Hagembe, Juliana Liambaya. 2009

机译：抗原位点突变对抗血凝素抗体与H3N2流感病毒分离株结合特异性的影响。
6. Virus Adaptation Following Experimental Infection of Chickens with a Domestic Duck Low Pathogenic Avian Influenza Isolate from the 2017 USA H7N9 Outbreak Identifies Polymorphic Mutations in Multiple Gene Segments [O] . Klaudia Chrzastek, Karen Segovia, Mia Torchetti, 2021

机译：来自2017年美国H7N9爆发的国内鸭低病原禽流感孤立鸡的鸡的实验感染病毒适应鉴定了多个基因段中的多态突变
7. Gain-of-sensitivity mutations in a Trim5-resistant primary isolate of pathogenic SIV identify two independent conserved determinants of Trim5α specificity. [O] . Kevin R McCarthy, Aaron G Schmidt, Andrea Kirmaier, 2013

机译：致病性sIV的Trim5抗性初级分离株中的增敏性突变鉴定Trim5α特异性的两个独立的保守决定簇。

Gain-of-Sensitivity Mutations in a Trim5-Resistant Primary Isolate of Pathogenic SIV Identify Two Independent Conserved Determinants of Trim5α Specificity

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