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用于HIV-1蛋白组装体结构分析的动态核极化增强魔角旋转核磁共振光谱法

Dynamic Nuclear Polarization Enhanced MAS NMR Spectroscopy for Structural Analysis of HIV-1 Protein Assemblies.

作者信息

Gupta Rupal, Lu Manman, Hou Guangjin, Caporini Marc A, Rosay Melanie, Maas Werner, Struppe Jochem, Suiter Christopher, Ahn Jinwoo, Byeon In-Ja L, Franks W Trent, Orwick-Rydmark Marcella, Bertarello Andrea, Oschkinat Hartmut, Lesage Anne, Pintacuda Guido, Gronenborn Angela M, Polenova Tatyana

机构信息

Department of Chemistry and Biochemistry, University of Delaware , Newark, Delaware 19716, United States.

Bruker Biospin Corporation , 15 Fortune Drive, Billerica, Massachusetts United States.

出版信息

J Phys Chem B. 2016 Jan 21;120(2):329-39. doi: 10.1021/acs.jpcb.5b12134. Epub 2016 Jan 12.

Abstract

Mature infectious HIV-1 virions contain conical capsids composed of CA protein, generated by the proteolytic cleavage cascade of the Gag polyprotein, termed maturation. The mechanism of capsid core formation through the maturation process remains poorly understood. We present DNP-enhanced MAS NMR studies of tubular assemblies of CA and Gag CA-SP1 maturation intermediate and report 20-64-fold sensitivity enhancements due to DNP at 14.1 T. These sensitivity enhancements enabled direct observation of spacer peptide 1 (SP1) resonances in CA-SP1 by dipolar-based correlation experiments, unequivocally indicating that the SP1 peptide is unstructured in assembled CA-SP1 at cryogenic temperatures, corroborating our earlier results. Furthermore, the dependence of DNP enhancements and spectral resolution on magnetic field strength (9.4-18.8 T) and temperature (109-180 K) was investigated. Our results suggest that DNP-based measurements could potentially provide residue-specific dynamics information by allowing for the extraction of the temperature dependence of the anisotropic tensorial or relaxation parameters. With DNP, we were able to detect multiple well-resolved isoleucine side-chain conformers; unique intermolecular correlations across two CA molecules; and functionally relevant conformationally disordered states such as the 14-residue SP1 peptide, none of which are visible at ambient temperatures. The detection of isolated conformers and intermolecular correlations can provide crucial constraints for structure determination of these assemblies. Overall, our results establish DNP-based MAS NMR spectroscopy as an excellent tool for the characterization of HIV-1 assemblies.

摘要

成熟的传染性HIV-1病毒粒子含有由CA蛋白组成的锥形衣壳,该衣壳由Gag多蛋白的蛋白水解切割级联反应产生,这一过程称为成熟。衣壳核心通过成熟过程形成的机制仍知之甚少。我们展示了对CA和Gag CA-SP1成熟中间体管状组装体的动态核极化增强的魔角旋转核磁共振(DNP-enhanced MAS NMR)研究,并报告了在14.1 T磁场下由于DNP导致的灵敏度提高了20至64倍。这些灵敏度的提高使得通过基于偶极的相关实验能够直接观察到CA-SP1中的间隔肽1(SP1)共振,明确表明在低温下组装的CA-SP1中SP1肽是无结构的,这证实了我们早期的结果。此外,还研究了DNP增强和光谱分辨率对磁场强度(9.4 - 18.8 T)和温度(109 - 180 K)的依赖性。我们的结果表明,基于DNP的测量有可能通过提取各向异性张量或弛豫参数的温度依赖性来提供残基特异性的动力学信息。利用DNP,我们能够检测到多个分辨率良好的异亮氨酸侧链构象异构体;两个CA分子之间独特的分子间相关性;以及功能相关的构象无序状态,如14个残基的SP1肽,这些在室温下均不可见。孤立构象异构体和分子间相关性的检测可为这些组装体的结构测定提供关键限制。总体而言,我们的结果确立了基于DNP的MAS NMR光谱学作为表征HIV-1组装体的优秀工具。

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