Garrison Keith E, Jones R Brad, Meiklejohn Duncan A, Anwar Naveed, Ndhlovu Lishomwa C, Chapman Joan M, Erickson Ann L, Agrawal Ashish, Spotts Gerald, Hecht Frederick M, Rakoff-Nahoum Seth, Lenz Jack, Ostrowski Mario A, Nixon Douglas F
Division of Experimental Medicine, Department of Medicine, University of California San Francisco, San Francisco, California, United States of America.
PLoS Pathog. 2007 Nov;3(11):e165. doi: 10.1371/journal.ppat.0030165.
Human endogenous retroviruses (HERVs) are remnants of ancient infectious agents that have integrated into the human genome. Under normal circumstances, HERVs are functionally defective or controlled by host factors. In HIV-1-infected individuals, intracellular defense mechanisms are compromised. We hypothesized that HIV-1 infection would remove or alter controls on HERV activity. Expression of HERV could potentially stimulate a T cell response to HERV antigens, and in regions of HIV-1/HERV similarity, these T cells could be cross-reactive. We determined that the levels of HERV production in HIV-1-positive individuals exceed those of HIV-1-negative controls. To investigate the impact of HERV activity on specific immunity, we examined T cell responses to HERV peptides in 29 HIV-1-positive and 13 HIV-1-negative study participants. We report T cell responses to peptides derived from regions of HERV detected by ELISPOT analysis in the HIV-1-positive study participants. We show an inverse correlation between anti-HERV T cell responses and HIV-1 plasma viral load. In HIV-1-positive individuals, we demonstrate that HERV-specific T cells are capable of killing cells presenting their cognate peptide. These data indicate that HIV-1 infection leads to HERV expression and stimulation of a HERV-specific CD8+ T cell response. HERV-specific CD8+ T cells have characteristics consistent with an important role in the response to HIV-1 infection: a phenotype similar to that of T cells responding to an effectively controlled virus (cytomegalovirus), an inverse correlation with HIV-1 plasma viral load, and the ability to lyse cells presenting their target peptide. These characteristics suggest that elicitation of anti-HERV-specific immune responses is a novel approach to immunotherapeutic vaccination. As endogenous retroviral sequences are fixed in the human genome, they provide a stable target, and HERV-specific T cells could recognize a cell infected by any HIV-1 viral variant. HERV-specific immunity is an important new avenue for investigation in HIV-1 pathogenesis and vaccine design.
人类内源性逆转录病毒(HERVs)是已整合到人类基因组中的古代感染因子的残余物。在正常情况下,HERVs功能有缺陷或受宿主因素控制。在感染HIV-1的个体中,细胞内防御机制受损。我们假设HIV-1感染会消除或改变对HERV活性的控制。HERV的表达可能会刺激T细胞对HERV抗原产生反应,并且在HIV-1/HERV相似的区域,这些T细胞可能会发生交叉反应。我们确定HIV-1阳性个体中HERV的产生水平超过HIV-1阴性对照。为了研究HERV活性对特异性免疫的影响,我们检测了29名HIV-1阳性和13名HIV-1阴性研究参与者对HERV肽的T细胞反应。我们报告了通过ELISPOT分析在HIV-1阳性研究参与者中检测到的对源自HERV区域的肽的T细胞反应。我们显示抗HERV T细胞反应与HIV-1血浆病毒载量呈负相关。在HIV-1阳性个体中,我们证明HERV特异性T细胞能够杀死呈递其同源肽的细胞。这些数据表明HIV-1感染导致HERV表达并刺激HERV特异性CD8 + T细胞反应。HERV特异性CD8 + T细胞具有与在对HIV-1感染的反应中起重要作用一致的特征:一种类似于对有效控制的病毒(巨细胞病毒)作出反应的T细胞的表型,与HIV-1血浆病毒载量呈负相关,以及裂解呈递其靶肽的细胞的能力。这些特征表明引发抗HERV特异性免疫反应是免疫治疗性疫苗接种的一种新方法。由于内源性逆转录病毒序列固定在人类基因组中,它们提供了一个稳定的靶点,并且HERV特异性T细胞可以识别被任何HIV-1病毒变体感染的细胞。HERV特异性免疫是HIV-1发病机制和疫苗设计研究的一个重要新途径。
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