交叉反应抗体增强了人类感染登革热病毒的能力。
Cross-reacting antibodies enhance dengue virus infection in humans.
机构信息
Department of Medicine, Imperial College London, London W12 0NN, UK.
出版信息
Science. 2010 May 7;328(5979):745-8. doi: 10.1126/science.1185181.
Abstract
Dengue virus co-circulates as four serotypes, and sequential infections with more than one serotype are common. One hypothesis for the increased severity seen in secondary infections is antibody-dependent enhancement (ADE) leading to increased replication in Fc receptor-bearing cells. In this study, we have generated a panel of human monoclonal antibodies to dengue virus. Antibodies to the structural precursor-membrane protein (prM) form a major component of the response. These antibodies are highly cross-reactive among the dengue virus serotypes and, even at high concentrations, do not neutralize infection but potently promote ADE. We propose that the partial cleavage of prM from the viral surface reduces the density of antigen available for viral neutralization, leaving dengue viruses susceptible to ADE by antibody to prM, a finding that has implications for future vaccine design.
摘要
登革热病毒共有 4 种血清型循环传播,且多种血清型的连续感染较为常见。对于二次感染时病情加重的一种假说认为是抗体依赖性增强(ADE)导致 Fc 受体细胞内的病毒复制增加。在本研究中,我们制备了一组抗登革热病毒的人源单克隆抗体。针对结构前体-膜蛋白(prM)的抗体构成了主要的反应成分。这些抗体在登革热病毒血清型之间具有高度的交叉反应性,即使在高浓度下,也不能中和感染,但能强烈促进 ADE。我们提出,prM 从病毒表面的部分裂解降低了可用于中和病毒的抗原密度,使登革热病毒容易受到针对 prM 的抗体的 ADE 影响,这一发现对未来的疫苗设计具有重要意义。
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