In vitro protease cleavage and computer simulations reveal the HIV-1 capsid maturation pathway

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作者
Jiying Ning
Gonca Erdemci-Tandogan
Ernest L. Yufenyuy
Jef Wagner
Benjamin A. Himes
Gongpu Zhao
Christopher Aiken
Roya Zandi
Peijun Zhang
机构
[1] University of Pittsburgh School of Medicine,Department of Structural Biology
[2] Pittsburgh Center for HIV Protein Interactions,Department of Physics and Astronomy
[3] University of Pittsburgh School of Medicine,Department of Pathology
[4] University of California,Division of Structural Biology
[5] Microbiology and Immunology,undefined
[6] Vanderbilt University Medical Center,undefined
[7] University of Oxford,undefined
[8] The Henry Wellcome Building for Genomic Medicine,undefined
[9] Electron Bio-Imaging Centre,undefined
[10] Diamond Light Sources,undefined
[11] Harwell Science and Innovation Campus,undefined
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摘要
HIV-1 virions assemble as immature particles containing Gag polyproteins that are processed by the viral protease into individual components, resulting in the formation of mature infectious particles. There are two competing models for the process of forming the mature HIV-1 core: the disassembly and de novo reassembly model and the non-diffusional displacive model. To study the maturation pathway, we simulate HIV-1 maturation in vitro by digesting immature particles and assembled virus-like particles with recombinant HIV-1 protease and monitor the process with biochemical assays and cryoEM structural analysis in parallel. Processing of Gag in vitro is accurate and efficient and results in both soluble capsid protein and conical or tubular capsid assemblies, seemingly converted from immature Gag particles. Computer simulations further reveal probable assembly pathways of HIV-1 capsid formation. Combining the experimental data and computer simulations, our results suggest a sequential combination of both displacive and disassembly/reassembly processes for HIV-1 maturation.
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