相关研究结果于2016年4月5日在线发表在Immunity期刊上,而且将作为封面文章发表,论文标题为“Key gp120 Glycans Pose Roadblocks to the Rapid Development of VRC01-Class Antibodies in an HIV-1-Infected Chinese Donor”。
作者: ipsvirus 时间: 2016-12-12 20:28 Key gp120 Glycans Pose Roadblocks to the Rapid Development of VRC01-Class Antibodies in an HIV-1-Infected Chinese Donor
Leopold Kong13, Bin Ju13, Yajing Chen13, Linling He13, Li Ren13, Jiandong Liu13, Kunxue Hong, Bin Su, Zheng Wang, Gabriel Ozorowski, Xiaolin Ji, Yuanzi Hua, Yanli Chen, Marc C. Deller, Yanling Hao, Yi Feng, Fernando Garces, Richard Wilson, Kaifan Dai, Sijy O’Dell, Krisha McKee, John R. Mascola, Andrew B. Ward, Richard T. Wyatt, Yuxing Li14, Ian A. Wilson14, Jiang Zhu14, Yiming Shao1
VRC01-class antibodies neutralize diverse HIV-1 strains by targeting the conserved CD4-binding site. Despite extensive investigations, crucial events in the early stage of VRC01 development remain elusive. We demonstrated how VRC01-class antibodies emerged in a Chinese donor by antigen-specific single B cell sorting, structural and functional studies, and longitudinal antibody and virus repertoire analyses. A monoclonal antibody DRVIA7 with modest neutralizing breadth was isolated that displayed a subset of VRC01 signatures. X-ray and EM structures revealed a VRC01-like angle of approach, but less favorable interactions between the DRVIA7 light-chain CDR1 and the N terminus with N276 and V5 glycans of gp120. Although the DRVIA7 lineage was unable to acquire broad neutralization, longitudinal analysis revealed a repertoire-encoded VRC01 light-chain CDR3 signature and VRC01-like neutralizing heavy-chain precursors that rapidly matured within 2 years. Thus, light chain accommodation of the glycan shield should be taken into account in vaccine design targeting this conserved site of vulnerability.