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HIV-1 Genetic Diversity and Its Impact on Baseline CD4+T Cells and Viral Loads among Recently Infected Men Who Have Sex with Men in Shanghai China

机译:中国上海最近感染男性的男性HIV-1遗传多样性及其对基线CD4 + T细胞和病毒载量的影响

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摘要

The HIV-1 epidemic among men who have sex with men (MSM) has been spreading throughout China. Shanghai, a central gathering place for MSM, is facing a continuously increasing incidence of HIV-1 infection. In order to better understand the dynamics of HIV-1 diversity and its influence on patient’s immune status at baseline on diagnosis, 1265 newly HIV-1-infected MSM collected from January 2009 to December 2013 in Shanghai were retrospectively analyzed for genetic subtyping, CD4+T cell counts, and viral loads. HIV-1 phylogenetic analysis revealed a broad viral diversity including CRF01_AE (62.13%), CRF07_BC (24.51%), subtype B (8.06%), CRF55_01B (3.24%), CER67_01B (0.95%), CRF68_01B (0.4%), CRF08_BC (0.08%) and CRF59_01B (0.08%). Twenty-four unique recombination forms (URFs) (1.98%) were identified as well. Bayesian inference analysis indicated that the introduction of CRF01_AE strain (1997) was earlier than CRF07_BC strain (2001) into MSM population in Shanghai based on the time of the most recent common ancestor (tMRCA). Three epidemic clusters and five sub-clusters were found in CRF01_AE. Significantly lower CD4+T cell count was found in individuals infected with CRF01_AE than in those infected with CRF07_BC infection (P<0.01), whereas viral load was significantly higher those infected with CRF01_AE than with CRF07_BC (P<0.01). In addition, the patients with >45 years of age were found to have lower CD4+T cell counts and higher viral loads than the patients with <25 years of age (P<0.05). This study reveals the presence of HIV-1 subtype diversity in Shanghai and its remarkable influence on clinical outcome. A real-time surveillance of HIV-1 viral diversity and phylodynamics of epidemic cluster, patient’s baseline CD4+T cell count and viral load would be of great value to monitoring of disease progression, intervention for transmission, improvement of antiretroviral therapy strategy and design of vaccines.
机译:与男性发生性关系的男性中的HIV-1流行病已在整个中国蔓延。上海是MSM的聚集地,面临着不断增长的HIV-1感染率。为了更好地了解HIV-1多样性的动态及其对患者基线免疫状态的影响,以进行诊断,回顾性分析了2009年1月至2013年12月在上海收集的1265例HIV-1感染的MSM的基因亚型,CD4 + T细胞计数和病毒载量。 HIV-1的系统发育分析显示,病毒具有广泛的多样性,包括CRF01_AE(62.13%),CRF07_BC(24.51%),B亚型(8.06%),CRF55_01B(3.24%),CER67_01B(0.95%),CRF68_01B(0.4%),CRF08_BC( 0.08%)和CRF59_01B(0.08%)。还鉴定出二十四种独特的重组形式(URF)(1.98%)。贝叶斯推断分析表明,根据最近祖先的时间,在上海MSM人群中引入CRF01_AE菌株(1997年)的时间要早​​于CRF07_BC菌株(2001年)的时间。在CRF01_AE中发现了三个流行病集群和五个子集群。 CRF01_AE感染者的CD4 + T细胞计数明显低于CRF07_BC感染者(P <0.01),而CRF01_AE感染者的病毒载量明显高于CRF07_BC(P <0.01)。此外,发现> 45岁的患者比<25岁的患者具有更低的CD4 + T细胞计数和更高的病毒载量(P <0.05)。这项研究揭示了上海存在HIV-1亚型多样性及其对临床结果的显着影响。实时监测HIV-1病毒多样性和流行群的系统动力学,患者的基线CD4 + T细胞计数和病毒载量,对于监测疾病进展,传播干预,改善抗逆转录病毒治疗策略和设计抗病毒药物具有重要价值。疫苗。

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