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急性登革病毒感染期间人类记忆性抗体反应的保护能力

Protective Capacity of the Human Anamnestic Antibody Response during Acute Dengue Virus Infection.

作者信息

Xu Meihui, Züst Roland, Toh Ying Xiu, Pfaff Jennifer M, Kahle Kristen M, Davidson Edgar, Doranz Benjamin J, Velumani Sumathy, Tukijan Farhana, Wang Cheng-I, Fink Katja

机构信息

Singapore Immunology Network, Agency for Science Technology and Research, Singapore.

Integral Molecular, Philadelphia, Pennsylvania, USA.

出版信息

J Virol. 2016 Nov 28;90(24):11122-11131. doi: 10.1128/JVI.01096-16. Print 2016 Dec 15.

Abstract

Half of the world's population is exposed to the risk of dengue virus infection. Although a vaccine for dengue virus is now available in a few countries, its reported overall efficacy of about 60% is not ideal. Protective immune correlates following natural dengue virus infection remain undefined, which makes it difficult to predict the efficacy of new vaccines. In this study, we address the protective capacity of dengue virus-specific antibodies that are produced by plasmablasts a few days after natural secondary infection. Among a panel of 18 dengue virus-reactive human monoclonal antibodies, four groups of antibodies were identified based on their binding properties. While antibodies targeting the fusion loop of the glycoprotein of dengue virus dominated the antibody response, two smaller groups of antibodies bound to previously undescribed epitopes in domain II of the E protein. The latter, largely serotype-cross-reactive antibodies, demonstrated increased stability of binding at pH 5. These antibodies possessed weak to moderate neutralization capacity in vitro but were the most efficacious in promoting the survival of infected mice. Our data suggest that the cross-reactive anamnestic antibody response has a protective capacity despite moderate neutralization in vitro and a moderate decrease of viremia in vivo IMPORTANCE: Antibodies can protect from symptomatic dengue virus infection. However, it is not easy to assess which classes of antibodies provide protection because in vitro assays are not always predictive of in vivo protection. During a repeat infection, dengue virus-specific immune memory cells are reactivated and large amounts of antibodies are produced. By studying antibodies cloned from patients with heterologous secondary infection, we tested the protective value of the serotype-cross-reactive "recall" or "anamnestic" response. We found that results from in vitro neutralization assays did not always correlate with the ability of the antibodies to reduce viremia in a mouse model. In addition, a decrease of viremia in mice did not necessarily improve survival. The most protective antibodies were stable at pH 5, suggesting that antibody binding in the endosomes, after the antibody-virus complex is internalized, might be important to block virus spread in the organism.

摘要

全球一半人口面临登革热病毒感染风险。尽管目前少数国家已有登革热病毒疫苗,但报道的约60%的总体效力并不理想。自然感染登革热病毒后的保护性免疫相关因素仍不明确,这使得预测新疫苗的效力变得困难。在本研究中,我们探讨了自然二次感染后数天由浆母细胞产生的登革热病毒特异性抗体的保护能力。在一组18种登革热病毒反应性人单克隆抗体中,根据其结合特性鉴定出四组抗体。虽然靶向登革热病毒糖蛋白融合环的抗体在抗体反应中占主导地位,但有两组较小的抗体与E蛋白结构域II中以前未描述的表位结合。后者主要是血清型交叉反应性抗体,在pH 5时显示出增加的结合稳定性。这些抗体在体外具有弱至中等的中和能力,但在促进感染小鼠存活方面最为有效。我们的数据表明,尽管体外中和作用中等且体内病毒血症有适度降低,但交叉反应性记忆抗体反应仍具有保护能力。重要性:抗体可预防有症状的登革热病毒感染。然而,评估哪些类别的抗体提供保护并不容易,因为体外试验并不总是能预测体内保护作用。在重复感染期间,登革热病毒特异性免疫记忆细胞被重新激活并产生大量抗体。通过研究从异源二次感染患者克隆的抗体,我们测试了血清型交叉反应性“回忆”或“记忆”反应的保护价值。我们发现体外中和试验的结果并不总是与抗体在小鼠模型中降低病毒血症的能力相关。此外,小鼠体内病毒血症的降低并不一定能提高存活率。最具保护作用的抗体在pH 5时稳定,这表明抗体-病毒复合物内化后在内体中的抗体结合可能对阻止病毒在体内传播很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f199/5126370/ea4f77ab323d/zjv9991821900001.jpg

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