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首页> 外文期刊>Vaccine >Recombinant influenza virus expressing HIV-1 p24 capsid protein induces mucosal HIV-specific CD8 T-cell responses
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Recombinant influenza virus expressing HIV-1 p24 capsid protein induces mucosal HIV-specific CD8 T-cell responses

机译:表达HIV-1 p24衣壳蛋白的重组流感病毒诱导粘膜HIV特异性CD8 T细胞反应

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摘要

Influenza viruses are promising mucosal vaccine vectors for HIV but their use has been limited by difficulties in engineering the expression of large amounts of foreign protein. We developed recombinant influenza viruses incorporating the HIV-1 p24 gag capsid into the NS-segment of PR8 (H1N1) and X31 (H3N2) influenza viruses with the use of multiple 2A ribosomal skip sequences. Despite the insertion of a sizable HIV-1 gene into the influenza genome, recombinant viruses were readily rescued to high titers. Intracellular expression of p24 capsid was confirmed by in vitro infection assays. The recombinant influenza viruses were subsequently tested as mucosal vaccines in BALB/c mice. Recombinant viruses were attenuated and safe in immunized mice. Systemic and mucosal HIV-specific CD8 T-cell responses were elicited in mice that were immunized via intranasal route with a prime-boost regimen. Isolated HIV-specific CD8 T-cells displayed polyfunctional cytokine and degranulation profiles. Mice boosted via intravaginal route induced recall responses from the distal lung mucosa and developed heightened HIV specific CD8 T-cell responses in the vaginal mucosa. These findings demonstrate the potential utility of recombinant influenza viruses as vaccines for mucosal immunity against HIV-1 infection. (C) 2016 Elsevier Ltd. All rights reserved.
机译:流感病毒是用于HIV的有希望的粘膜疫苗载体,但由于难以工程化大量外源蛋白的表达而受到限制。我们使用多个2A核糖体跳跃序列,开发了将HIV-1 p24 gag衣壳整合到PR8(H1N1)和X31(H3N2)流感病毒的NS段的重组流感病毒。尽管在流感基因组中插入了相当大的HIV-1基因,但重组病毒还是很容易挽救到高滴度的。通过体外感染测定证实了p24衣壳的细胞内表达。随后在BALB / c小鼠中测试重组流感病毒作为粘膜疫苗。重组病毒在免疫小鼠中减毒且安全。在通过初免-加强疗法通过鼻内途径免疫的小鼠中引发了全身性和粘膜性HIV特异性CD8 T细胞应答。分离的HIV特异性CD8 T细胞显示出多功能的细胞因子和脱颗粒特征。通过阴道内途径增强的小鼠诱发了远端肺粘膜的召回反应,并在阴道粘膜中产生了更高的HIV特异性CD8 T细胞应答。这些发现证明重组流感病毒作为针对HIV-1感染的粘膜免疫疫苗的潜在用途。 (C)2016 Elsevier Ltd.保留所有权利。

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