首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Severe genital herpes infections in HIV-infected individuals with impaired herpes simplex virus-specific CD8+ cytotoxic T lymphocyte responses
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Severe genital herpes infections in HIV-infected individuals with impaired herpes simplex virus-specific CD8+ cytotoxic T lymphocyte responses

机译:单纯疱疹病毒特异性CD8 +细胞毒性T淋巴细胞受损的HIV感染者中的严重生殖器疱疹感染

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摘要

The specific mechanisms underlying the varied susceptibility of HIV-infected (HIV+) individuals to opportunistic infections (OI) are still incompletely understood. One hypothesis is that quantitative differences in specific T cell responses to a colonizing organism determine the development of an AIDS-defining OI. We evaluated this hypothesis for herpes simplex virus (HSV) infection, a common OI in HIV+ patients. Using limiting dilution analyses, the frequency of HSV-specific CD8+ cytotoxic T lymphocyte precursors (pCTL) and proliferative precursors were quantitated in peripheral blood mononuclear cells from 20 patients coinfected with HIV and HSV-2. The frequency of HSV-specific CD8+ pCTL in HSV+HIV+ individuals was significantly lower than in HSV+HIV− individuals (1 in 77,000 vs. 1 in 6,000, P = .0005) and was not different than in HSV-HIV− individuals (1 in 100,000, P = .24). HIV+ patients who suffered more severe genital herpes recurrences had significantly lower HSV-specific CD8+ pCTL frequencies than those patients with mild recurrences (1 in 170,000 vs. 1 in 26,000, P = .03). In contrast, no significant difference was seen in proliferative precursor frequencies between those patients with mild vs. severe genital herpes (1 in 3,800 vs. 1 in 6,600, P > .5). Quantitative differences in pCTL frequency to HSV appear to be the most important host factor influencing the frequency and severity of HSV reactivation in HIV+ patients. Studies to reconstitute such immunity, especially in people with acyclovir-resistant HSV, appear warranted.
机译:仍未完全了解HIV感染者(HIV +)对机会感染(OI)易感性不同的具体机制。一种假设是,对定殖生物体的特定T细胞反应的定量差异决定了定义AIDS的OI的发展。我们评估了单纯疱疹病毒(HSV)感染这一假设,这是HIV +患者常见的OI。使用有限稀释法分析,对20名感染了HIV和HSV-2的患者外周血单个核细胞中HSV特异性CD8 + 细胞毒性T淋巴细胞前体(pCTL)和增殖前体的频率进行了定量。 HSV + HIV +个体中HSV特异性CD8 + pCTL的频率显着低于HSV + HIV-个体(77,000中的1比6,000中的1,P = .0005),并且没有差异高于HSV-HIV−个体(100,000分之一,P = 0.24)。患有较严重生殖器疱疹复发的HIV +患者的HSV特异性CD8 + pCTL频率显着低于那些轻度复发的患者(170,000中的1对26,000中的1,P = .03)。相反,轻度和重度生殖器疱疹患者之间的增殖前体频率没有显着差异(3,800中的1对6,600中的1,P> .5)。 pCTL频率与HSV的定量差异似乎是影响HIV +患者中HSV重新激活的频率和严重程度的最重要宿主因素。重建这种免疫力的研究,尤其是在对阿昔洛韦具有抗药性的HSV人群中,显得很有必要。

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