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CRF07_BC与中国患者中HIV疾病进展缓慢有关。

CRF07_BC is associated with slow HIV disease progression in Chinese patients.

作者信息

Ye Jingrong, Chen Jing, Wang Juan, Wang Yuncong, Xing Hui, Yu Fengting, Liu Lifeng, Han Yang, Huang Huihuang, Feng Yi, Ruan Yuhua, Zheng Minna, Lu Xinli, Guo Xiaoli, Yang Hong, Guo Qi, Lin Yi, Wu Jianjun, Wu Shouli, Tang Yilong, Sun Xiaoguang, Zou Xiaobai, Yu Guolong, Li Jianjun, Zhou Quanhua, Su Ling, Zhang Lincai, Gao Zhan, Xin Ruolei, He Shufang, Xu Conghui, Hao Mingqiang, Hao Yinxiao, Ren Xianlong, Li Jie, Bai Lishi, Jiang Tianjun, Zhang Tong, Shao Yiming, Lu Hongyan

机构信息

Institute for HIV/AIDS and STD Prevention and Control, Beijing Center for Disease Prevention and Control (CDC) and Beijing Research Center for Preventive Medicine, No.16, Hepingli Middle Street; Dong Chen District, Beijing, China.

Division of Virology and Immunology, State Key Laboratory for Infectious Disease and Prevention and Control and National Center for AIDS/STD Prevention and Control (NCAIDS), China CDC, No.155 Changbai Road, Changping District, Beijing, China.

出版信息

Sci Rep. 2022 Mar 8;12(1):3773. doi: 10.1038/s41598-022-07518-4.

Abstract

HIV subtypes convey important epidemiological information and possibly influence the rate of disease progression. In this study, HIV disease progression in patients infected with CRF01_AE, CRF07_BC, and subtype B was compared in the largest HIV molecular epidemiology study ever done in China. A national data set of HIV pol sequences was assembled by pooling sequences from public databases and the Beijing HIV laboratory network. Logistic regression was used to assess factors associated with the risk of AIDS at diagnosis ([AIDSAD], defined as a CD4 count < 200 cells/µL) in patients with HIV subtype B, CRF01_AE, and CRF07_BC. Of the 20,663 sequences, 9,156 (44.3%) were CRF01_AE. CRF07_BC was responsible for 28.3% of infections, followed by B (13.9%). In multivariable analysis, the risk of AIDSAD differed significantly according to HIV subtype (OR for CRF07_BC vs. B: 0.46, 95% CI 0.39─0.53), age (OR for ≥ 65 years vs. < 18 years: 4.3 95% CI 1.81─11.8), and transmission risk groups (OR for men who have sex with men vs. heterosexuals: 0.67 95% CI 0.6─0.75). These findings suggest that HIV diversity in China is constantly evolving and gaining in complexity. CRF07_BC is less pathogenic than subtype B, while CRF01_AE is as pathogenic as B.

摘要

HIV亚型传递着重要的流行病学信息,并可能影响疾病进展速度。在本研究中,在中国有史以来规模最大的HIV分子流行病学研究中,对感染CRF01_AE、CRF07_BC和B亚型的患者的HIV疾病进展情况进行了比较。通过汇集来自公共数据库和北京HIV实验室网络的序列,构建了一个全国性的HIV pol序列数据集。采用逻辑回归分析评估HIV B亚型、CRF01_AE和CRF07_BC患者诊断时患艾滋病的风险([AIDSAD],定义为CD4细胞计数<200个/微升)的相关因素。在20663条序列中,9156条(44.3%)为CRF01_AE。CRF07_BC导致了28.3%的感染,其次是B亚型(13.9%)。在多变量分析中,根据HIV亚型,患AIDSAD的风险有显著差异(CRF07_BC与B亚型相比的OR:0.46,95%CI 0.39─0.53),年龄(≥65岁与<18岁相比的OR:4.3,95%CI 1.81─11.8),以及传播风险组(男男性行为者与异性恋者相比的OR:0.67,95%CI 0.6─0.75)。这些发现表明,中国的HIV多样性在不断演变且日益复杂。CRF07_BC的致病性低于B亚型,而CRF01_AE的致病性与B亚型相当。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dd9/8904811/7e64f68d8ed3/41598_2022_7518_Fig1_HTML.jpg

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