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评估未感染HIV-1个体对候选HIV-1疫苗的细胞毒性T细胞反应。

Evaluation of cytotoxic T cell responses to candidate HIV-1 vaccines in HIV-1-uninfected individuals.

作者信息

McElrath M J, Corey L, Greenberg P D

机构信息

Department of Medicine, University of Washington School of Medicine, Seattle 98195.

出版信息

AIDS Res Hum Retroviruses. 1994;10 Suppl 2:S69-72.

PMID:7865336
Abstract

The ability to induce a strong, HIV-1-specific CD8+ CTL response is assumed to be an important component of a protective HIV-1 vaccine. Identification of CTL responses in seronegative vaccines requires in vitro stimulation of CTL precursors with cells that have processed HIV-1 gene products via the endogenous intracellular pathway for presentation in association with MHC class I molecules. We have developed a method to detect CTL responses to HIV epitopes and HIV-infected cells that can be applied to recipients of HIV vaccines regardless of immunization with a particular recombinant virus or prior immunological status. Primed CTL precursors from PBMCs are stimulated for two 1-week cycles with autologous monocyte-derived macrophages infected with HIV-1Ba-L. The effector CTLs generated in culture are then tested in a standard chromium release assay for lysis, using autologous target cells, including EBV-transformed lymphoblastoid cell lines (LCLs) expressing individual HIV-1 proteins following infection with a recombinant vaccinia virus, or LCLs transduced with the CD4 gene and infected with isolates of HIV. Using this methodology we have examined CTL responses induced by candidate HIV vaccines in HIV-1-uninfected individuals participating in phase I/II AVEG trials. Our findings indicate that this approach makes it possible to overcome some of the previous technical difficulties involved in the analysis of CTL responses in immunocompetent vaccine recipients and thereby facilitates the identification of potentially effective candidate HIV-1 vaccines.

摘要

诱导强烈的、HIV-1特异性CD8+CTL反应的能力被认为是HIV-1保护性疫苗的一个重要组成部分。在血清阴性疫苗中鉴定CTL反应需要用通过内源性细胞内途径处理过HIV-1基因产物以与MHC I类分子结合呈递的细胞对CTL前体进行体外刺激。我们已经开发出一种检测针对HIV表位和HIV感染细胞的CTL反应的方法,该方法可应用于HIV疫苗接种者,无论其是否用特定重组病毒免疫或既往免疫状态如何。来自外周血单核细胞(PBMC)的致敏CTL前体用感染了HIV-1Ba-L的自体单核细胞衍生巨噬细胞刺激两个1周周期。然后在标准的铬释放试验中使用自体靶细胞检测培养中产生的效应CTL的裂解作用,所述自体靶细胞包括感染重组痘苗病毒后表达单个HIV-1蛋白的EB病毒转化的淋巴母细胞系(LCL),或转导了CD4基因并感染HIV分离株的LCL。使用这种方法,我们检测了参与I/II期AVEG试验的未感染HIV-1个体中候选HIV疫苗诱导的CTL反应。我们的研究结果表明,这种方法能够克服先前在免疫功能正常的疫苗接种者中分析CTL反应所涉及的一些技术难题,从而有助于鉴定潜在有效的候选HIV-1疫苗。

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