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人类免疫缺陷病毒衣壳蛋白的N端延伸将体外组装表型从管状颗粒转变为球形颗粒。

N-Terminal extension of human immunodeficiency virus capsid protein converts the in vitro assembly phenotype from tubular to spherical particles.

作者信息

Gross I, Hohenberg H, Huckhagel C, Kräusslich H G

机构信息

Heinrich-Pette-Institut, D-20251 Hamburg, Germany.

出版信息

J Virol. 1998 Jun;72(6):4798-810. doi: 10.1128/JVI.72.6.4798-4810.1998.

DOI:10.1128/JVI.72.6.4798-4810.1998
PMID:9573245
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC110021/
Abstract

Expression of retroviral Gag polyproteins is sufficient for morphogenesis of virus-like particles with a spherical immature protein shell. Proteolytic cleavage of Gag into the matrix (MA), capsid (CA), nucleocapsid (NC), and p6 domains (in the case of human immunodeficiency virus [HIV]) leads to condensation to the mature cone-shaped core. We have analyzed the formation of spherical or cylindrical particles on in vitro assembly of purified HIV proteins or inside Escherichia coli cells. CA protein alone yielded cylindrical particles, while all N-terminal extensions of CA abolished cylinder formation. Spherical particles with heterogeneous diameters or amorphous protein aggregates were observed instead. Extending CA by 5 amino acids was sufficient to convert the assembly phenotype to spherical particles. Sequences C-terminal of CA were not required for sphere formation. Proteolytic cleavage of N-terminally extended CA proteins prior to in vitro assembly led to the formation of cylindrical particles, while proteolysis of in vitro assembly products caused disruption of spheres but not formation of cylinders. In vitro assembly of CA and extended CA proteins in the presence of cyclophilin A (CypA) at a CA-to-CypA molar ratio of 10:1 yielded significantly longer cylinders and heterogeneous spheres, while higher concentrations of CypA completely disrupted particle formation. We conclude that the spherical shape of immature HIV particles is determined by the presence of an N-terminal extension on the CA domain and that core condensation during virion maturation requires the liberation of the N terminus of CA.

摘要

逆转录病毒Gag多聚蛋白的表达足以形成具有球形未成熟蛋白壳的病毒样颗粒。将Gag蛋白水解切割成基质(MA)、衣壳(CA)、核衣壳(NC)和p6结构域(对于人类免疫缺陷病毒[HIV]而言)会导致凝聚形成成熟的锥形核心。我们分析了纯化的HIV蛋白在体外组装时或在大肠杆菌细胞内形成球形或圆柱形颗粒的情况。单独的CA蛋白产生圆柱形颗粒,而CA的所有N端延伸都消除了圆柱的形成。取而代之的是观察到具有不同直径的球形颗粒或无定形蛋白聚集体。将CA延伸5个氨基酸就足以将组装表型转变为球形颗粒。CA的C端序列对于球体形成不是必需的。在体外组装之前对N端延伸的CA蛋白进行蛋白水解切割会导致形成圆柱形颗粒,而对体外组装产物进行蛋白水解则会导致球体破坏但不会形成圆柱体。在亲环蛋白A(CypA)存在的情况下,以CA与CypA摩尔比为10:1对CA和延伸的CA蛋白进行体外组装,会产生明显更长的圆柱体和异质球体,而更高浓度的CypA会完全破坏颗粒形成。我们得出结论,未成熟HIV颗粒的球形形状是由CA结构域上存在N端延伸决定的,并且病毒体成熟过程中的核心凝聚需要CA的N端被释放。

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本文引用的文献

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Sequential steps in human immunodeficiency virus particle maturation revealed by alterations of individual Gag polyprotein cleavage sites.通过单个Gag多聚蛋白切割位点的改变揭示的人类免疫缺陷病毒颗粒成熟的连续步骤。
J Virol. 1998 Apr;72(4):2846-54. doi: 10.1128/JVI.72.4.2846-2854.1998.
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Proteolytic refolding of the HIV-1 capsid protein amino-terminus facilitates viral core assembly.HIV-1衣壳蛋白氨基末端的蛋白水解重折叠促进病毒核心组装。
EMBO J. 1998 Mar 16;17(6):1555-68. doi: 10.1093/emboj/17.6.1555.
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Structure of the carboxyl-terminal dimerization domain of the HIV-1 capsid protein.人类免疫缺陷病毒1型衣壳蛋白羧基末端二聚化结构域的结构
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Crystal structure of human cyclophilin A bound to the amino-terminal domain of HIV-1 capsid.与HIV-1衣壳氨基末端结构域结合的人亲环素A的晶体结构。
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Human immunodeficiency virus type 1 capsid formation in reticulocyte lysates.1型人类免疫缺陷病毒衣壳在网织红细胞裂解物中的形成。
J Virol. 1996 Nov;70(11):8187-94. doi: 10.1128/JVI.70.11.8187-8194.1996.
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