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首页> 外文期刊>Medical Microbiology and Immunology >High polymorphism rates in well-known T cell epitopes restricted by protective HLA alleles during HIV infection are associated with rapid disease progression in early-infected MSM in China
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High polymorphism rates in well-known T cell epitopes restricted by protective HLA alleles during HIV infection are associated with rapid disease progression in early-infected MSM in China

机译:在HIV感染期间受保护性HLA等位基因限制的众所周知的T细胞表位中的高多态性率与中国早期感染MSM的快速疾病进展相关

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摘要

T cell epitopes restricted by several protective HLA alleles, such as B*57, B*5801, B*27, B*51 and B*13, have been very well defined over the past two decades. We investigated 32 well-known T cell epitopes restricted by protective HLA molecules among 54 Chinese men who have sex with men (MSM) at the early stage of HIV-1 infection. Subjects in our cohort carrying protective HLA types did not exhibit slow CD4 T cell count decline (P=0.489) or low viral load set points (P=0.500). Variations occurred in 96.88% (31/32) of the known wild-type epitopes (rate 1.85-100%), and the variation rates of the strains of two CRF01_AE lineages were significantly higher than those of non-CRF01_AE strains (76.82% vs. 48.96%, P=0.004; 71.27% vs. 8.96%, P=0.025). Subjects infected with CRF01_AE exhibited relatively rapid disease progression (P=0.035). Therefore, the lack of wild-type protective T cell epitopes restricted by classic protective HLA alleles in CRF01_AE HIV-1 strains may be one of the reasons why rapid disease progression is observed in Chinese MSM with HIV-1 infection.
机译:T细胞表位受几种保护性HLA等位基因限制,例如B * 57,B * 5801,B * 27,B * 51和B * 13,在过去的二十年中已经很好地定义。我们调查了32名众所周知的T细胞表位,在HIV-1感染早期与男性(MSM)发生性关系的54名中国男性中受保护性HLA分子受限制。携带保护性HLA类型的队列中的受试者未表现出缓慢的CD4 T细胞计数下降(P = 0.489)或低病毒载荷设定点(P = 0.500)。已知野生型表位(速率1.85-100%)的96.88%(31/32)发生的变化,并且两种CRF01_AE谱系的菌株的变异率明显高于非CRF01_AE菌株(76.82%VS 。48.96%,p = 0.004; 71.27%与8.96%,p = 0.025)。感染CRF01_AE的受试者表现出相对快速的疾病进展(P = 0.035)。因此,CRF01_AE HIV-1菌株中经典保护性HLA等位基因限制的野生型保护性T细胞表位可能是患有HIV-1感染的中国MSM在中国MSM中观察到快速疾病进展的原因之一。

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