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由HIV-1保守区域组装而成并以mRNA形式递送的四价免疫原显示出强大的临床前T细胞免疫原性和广度。

Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth.

作者信息

Moyo Nathifa, Wee Edmund G, Korber Bette, Bahl Kapil, Falcone Samantha, Himansu Sunny, Wong Adrianne L, Dey Antu K, Feinberg Mark, Hanke Tomáš

机构信息

The Jenner Institute, University of Oxford, Oxford OX3 7DQ, UK.

Los Alamo National Laboratory, Theoretical Biology and Biophysics, Los Alamos, NM 87545, USA.

出版信息

Vaccines (Basel). 2020 Jul 6;8(3):360. doi: 10.3390/vaccines8030360.

Abstract

A vaccine will likely be one of the key tools for ending the HIV-1/AIDS epidemic by preventing HIV-1 spread within uninfected populations and achieving a cure for people living with HIV-1. The currently prevailing view of the vaccine field is to introduce protective antibodies, nevertheless, a vaccine to be effective may need to harness protective T cells. We postulated that focusing a T-cell response on the most vulnerable regions of the HIV-1 proteome while maximizing a perfect match between the vaccine and circulating viruses will control HIV-1 replication. We currently use a combination of replication-deficient simian (chimpanzee) adenovirus and poxvirus modified vaccinia virus Ankara to deliver bivalent conserved-mosaic immunogens to human volunteers. Here, we exploit the mRNA platform by designing tetravalent immunogens designated as HIVconsvM, and demonstrate that mRNA formulated in lipid nanoparticles induces potent, broad and polyfunctional T-cell responses in a pre-clinical model. These results support optimization and further development of this vaccine strategy in experimental medicine trials in humans.

摘要

疫苗可能是终结HIV-1/艾滋病流行的关键工具之一,可预防HIV-1在未感染人群中传播,并实现对HIV-1感染者的治愈。目前疫苗领域的主流观点是引入保护性抗体,然而,一种有效的疫苗可能需要利用保护性T细胞。我们推测,将T细胞反应聚焦于HIV-1蛋白质组中最脆弱的区域,同时使疫苗与循环病毒之间的匹配度最大化,将能够控制HIV-1复制。我们目前使用复制缺陷型猿猴(黑猩猩)腺病毒和痘病毒安卡拉痘苗病毒的组合,向人类志愿者递送二价保守镶嵌免疫原。在此,我们通过设计名为HIVconsvM的四价免疫原利用mRNA平台,并证明脂质纳米颗粒中配制的mRNA在临床前模型中可诱导强效、广泛和多功能的T细胞反应。这些结果支持在人体实验医学试验中优化和进一步开发这种疫苗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/30c2/7563622/288694d4700d/vaccines-08-00360-g001a.jpg

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