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Delineating antibody recognition against Zika virus during natural infection

寨卡病毒 病毒学 抗体 登革热病毒 登革热 黄病毒 中和抗体 免疫学 病毒 生物 抗体反应 医学
作者
Lei Yu,Ruoke Wang,Fei Gao,Shelley D. Minteer,Jianying Liu,Jing Wang,Wenxin Hong,Lingzhai Zhao,Yingfen Wen,Chibiao Yin,Hua Wang,Qi Zhang,Yangyang Li,Panpan Zhou,Rudian Zhang,Yang Liu,Xiaoping Tang,Yongjun Guan,Chuan Qin,Long Qing Chen,Xuanling Shi,Xia Jin,Gong Cheng,Fu-Chun Zhang,Linqi Zhang
出处
期刊:JCI insight [American Society for Clinical Investigation]
卷期号:2 (12) 被引量:56
标识
DOI:10.1172/jci.insight.93042
摘要

Zika virus (ZIKV) is an emerging mosquito-transmitted flavivirus that shares a considerable degree of homology with dengue virus (DENV). Here, we examined longitudinal antibody response against ZIKV during natural infection in 2 convalescent individuals. By decomposing the antibody recognition into DI/DII and DIII of the E glycoprotein, we showed their development in humans followed a spatiotemporal hierarchy. Plasma binding to DI/DII appeared to peak and wane during early infection with extensive cross-reactivity with DI/DII of DENV. Binding to DIII, however, peaked early but persisted months into the infection without detectable cross-reactivity with DIII of DENV. A clear trend of increase in DIII-specific neutralizing activity was observed over the course of infection. mAbs isolated during early infection are largely DI/DII specific, weakly neutralizing, and highly cross-reactive with DENV, while those from later infection are more diverse in recognition, potently neutralizing, and ZIKV specific. The most potent neutralizing mAb targeting the DIII provided 100% protection in mice from lethal ZIKV infection and could therefore serve as a promising candidate for antibody-based therapy and prevention. The dynamic features unveiled here will assist us to better understand the pathogenesis of ZIKV infection and inform rational design of vaccines.

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