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HIV-1蛋白酶的共翻译折叠与成熟

Cotranslational folding and maturation of HIV-1 protease.

作者信息

Westerfield Justin, Nicolaus Felix, Swanstrom Ronald, von Heijne Gunnar

机构信息

Department of Biochemistry and Biophysics, Stockholm University, SE-106 91 Stockholm, Sweden.

Department of Biochemistry and Biophysics, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, USA.

出版信息

bioRxiv. 2025 Aug 27:2025.08.27.672612. doi: 10.1101/2025.08.27.672612.

Abstract

HIV-1 particle assembly depends critically on multiple proteolytic cleavages of viral polyproteins by the viral protease, PR. PR is translated as part of the Gag-Pro-Pol polyprotein, which undergoes autoproteolysis to liberate active, dimeric PR during virus particle maturation. Gag-Pro-Pol is produced via an infrequent -1 frameshifting event in ribosomes translating full length genomic RNA as Gag mRNA. Here, we study the cotranslational folding and autoproteolytic processing of frameshifted transframe-protease-reverse transcriptase (TF-PR-RT) constructs by translation. We demonstrate partial cotranslational folding of ribosome-bound PR at its conserved α-helix near the C terminus. Unexpectedly, we find that the initial dimerization of TF-PR-RT involves ribosome-bound nascent chains that are then not further cleaved. Moreover, only ribosome-bound nascent chains are substrates for PR-catalyzed processing. These observations are consistent with a model for virion assembly in which dimerization of a subset of Pro-Pol precursors leads to cleavage of PR monomers that then carry out the bulk of the proteolytic processing needed for virion maturation and infectivity.

摘要

HIV-1病毒颗粒的组装关键取决于病毒蛋白酶(PR)对病毒多聚蛋白的多次蛋白水解切割。PR作为Gag-Pro-Pol多聚蛋白的一部分被翻译,在病毒颗粒成熟过程中,该多聚蛋白会发生自蛋白水解,从而释放出有活性的二聚体PR。Gag-Pro-Pol是在核糖体将全长基因组RNA作为Gag mRNA进行翻译时,通过罕见的-1移码事件产生的。在此,我们通过翻译研究移码后的跨框蛋白酶-逆转录酶(TF-PR-RT)构建体的共翻译折叠和自蛋白水解加工过程。我们证明了核糖体结合的PR在其C末端附近保守的α螺旋处发生部分共翻译折叠。出乎意料的是,我们发现TF-PR-RT的初始二聚化涉及核糖体结合的新生链,这些新生链随后不再进一步切割。此外,只有核糖体结合的新生链是PR催化加工的底物。这些观察结果与病毒体组装模型一致,在该模型中,一部分Pro-Pol前体的二聚化导致PR单体的切割,然后这些单体进行病毒体成熟和感染性所需的大部分蛋白水解加工。

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