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作为DNA初免、NYVAC和包膜蛋白加强免疫方案的传播奠基者型、HIV-1 M组共识型和三价嵌合包膜疫苗在恒河猴中的免疫原性比较。

Comparison of Immunogenicity in Rhesus Macaques of Transmitted-Founder, HIV-1 Group M Consensus, and Trivalent Mosaic Envelope Vaccines Formulated as a DNA Prime, NYVAC, and Envelope Protein Boost.

作者信息

Hulot Sandrine L, Korber Bette, Giorgi Elena E, Vandergrift Nathan, Saunders Kevin O, Balachandran Harikrishnan, Mach Linh V, Lifton Michelle A, Pantaleo Giuseppe, Tartaglia Jim, Phogat Sanjay, Jacobs Bertram, Kibler Karen, Perdiguero Beatriz, Gomez Carmen E, Esteban Mariano, Rosati Margherita, Felber Barbara K, Pavlakis George N, Parks Robert, Lloyd Krissey, Sutherland Laura, Scearce Richard, Letvin Norman L, Seaman Michael S, Alam S Munir, Montefiori David, Liao Hua-Xin, Haynes Barton F, Santra Sampa

机构信息

Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts, USA.

Los Alamos National Laboratory, Los Alamos, New Mexico, USA.

出版信息

J Virol. 2015 Jun;89(12):6462-80. doi: 10.1128/JVI.00383-15. Epub 2015 Apr 8.

Abstract

UNLABELLED

An effective human immunodeficiency virus type 1 (HIV-1) vaccine must induce protective antibody responses, as well as CD4(+) and CD8(+) T cell responses, that can be effective despite extraordinary diversity of HIV-1. The consensus and mosaic immunogens are complete but artificial proteins, computationally designed to elicit immune responses with improved cross-reactive breadth, to attempt to overcome the challenge of global HIV diversity. In this study, we have compared the immunogenicity of a transmitted-founder (T/F) B clade Env (B.1059), a global group M consensus Env (Con-S), and a global trivalent mosaic Env protein in rhesus macaques. These antigens were delivered using a DNA prime-recombinant NYVAC (rNYVAC) vector and Env protein boost vaccination strategy. While Con-S Env was a single sequence, mosaic immunogens were a set of three Envs optimized to include the most common forms of potential T cell epitopes. Both Con-S and mosaic sequences retained common amino acids encompassed by both antibody and T cell epitopes and were central to globally circulating strains. Mosaics and Con-S Envs expressed as full-length proteins bound well to a number of neutralizing antibodies with discontinuous epitopes. Also, both consensus and mosaic immunogens induced significantly higher gamma interferon (IFN-γ) enzyme-linked immunosorbent spot assay (ELISpot) responses than B.1059 immunogen. Immunization with these proteins, particularly Con-S, also induced significantly higher neutralizing antibodies to viruses than B.1059 Env, primarily to tier 1 viruses. Both Con-S and mosaics stimulated more potent CD8-T cell responses against heterologous Envs than did B.1059. Both antibody and cellular data from this study strengthen the concept of using in silico-designed centralized immunogens for global HIV-1 vaccine development strategies.

IMPORTANCE

There is an increasing appreciation for the importance of vaccine-induced anti-Env antibody responses for preventing HIV-1 acquisition. This nonhuman primate study demonstrates that in silico-designed global HIV-1 immunogens, designed for a human clinical trial, are capable of eliciting not only T lymphocyte responses but also potent anti-Env antibody responses.

摘要

未标记

一种有效的1型人类免疫缺陷病毒(HIV-1)疫苗必须诱导保护性抗体反应以及CD4(+)和CD8(+) T细胞反应,尽管HIV-1具有极大的多样性,这些反应仍需有效。共有序列和镶嵌免疫原是完整的但却是人工蛋白质,通过计算机设计以引发具有改善的交叉反应广度的免疫反应,试图克服全球HIV多样性的挑战。在本研究中,我们比较了恒河猴中传播奠基者(T/F)B亚型Env(B.1059)、全球M组共有序列Env(Con-S)和全球三价镶嵌Env蛋白的免疫原性。这些抗原采用DNA初免-重组NYVAC(rNYVAC)载体和Env蛋白加强免疫策略进行递送。虽然Con-S Env是单个序列,但镶嵌免疫原是一组三个Env,经过优化以包含潜在T细胞表位的最常见形式。Con-S和镶嵌序列都保留了抗体和T细胞表位所包含的共同氨基酸,并且对于全球流行毒株至关重要。作为全长蛋白表达的镶嵌和Con-S Env与许多具有不连续表位的中和抗体结合良好。此外,共有序列和镶嵌免疫原诱导的γ干扰素(IFN-γ)酶联免疫斑点试验(ELISpot)反应均显著高于B.1059免疫原。用这些蛋白免疫,特别是Con-S,还诱导出比B.1059 Env更高的针对病毒的中和抗体,主要针对1级病毒。Con-S和镶嵌序列刺激的针对异源Env的CD8-T细胞反应比B.1059更强。本研究的抗体和细胞数据均强化了在全球HIV-1疫苗开发策略中使用计算机设计的集中免疫原的概念。

重要性

人们越来越认识到疫苗诱导的抗Env抗体反应对于预防HIV-1感染的重要性。这项非人灵长类动物研究表明,为人类临床试验设计的计算机设计的全球HIV-1免疫原不仅能够引发T淋巴细胞反应,还能引发强效的抗Env抗体反应。

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