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1型人类免疫缺陷病毒A和D亚型的嗜神经性:分子进化、重组及共受体使用情况

Human immunodeficiency virus type 1 clade A and D neurotropism: molecular evolution, recombination, and coreceptor use.

作者信息

Zhang K, Hawken M, Rana F, Welte F J, Gartner S, Goldsmith M A, Power C

机构信息

Department of Clinical Neuroscience, University of Calgary, 3330 Hospital Drive NW, Calgary, Alberta, T2N 4N1, Canada.

出版信息

Virology. 2001 Apr 25;283(1):19-30. doi: 10.1006/viro.2001.0876.

Abstract

Human immunodeficiency virus type 1 (HIV-1) non-B clade viral infections of the brain have not been studied to date. Among nine AIDS patients from Nairobi, Kenya, infected with HIV-1 A (N = 5) or D (N = 4) clade strains, brain-derived HIV-1 env sequences displayed greater evolutionary distance than B clade brain-derived viruses (P < 0.001). Similarly, molecular diversity between matched brain and spleen env clones was clade-dependent and concentrated in the hypervariable V4 region (P < 0.001), with phylogenetic clustering of sequences derived from the same organ. Brain-derived A and D clade sequences displayed significantly lower ratios of nonsynonymous/synonymous substitution rates (d(N)/d(S)) compared to matched spleen-derived clones and brain-derived B clade viruses. Interclade recombination events were infrequently observed among the present env sequences. A chimeric virus containing the C2V3 region from an A clade brain-derived sequence preferentially used CD4 and CCR5 for infection. These findings demonstrate that differences in molecular diversity in brain-derived sequences were dependent on the individual clade and domain within the env gene, but both B and non-B clade brain-derived viruses exhibit a preference for CCR5 as a coreceptor.

摘要

1型人类免疫缺陷病毒(HIV-1)非B亚型病毒对大脑的感染迄今尚未得到研究。在肯尼亚内罗毕的9名感染HIV-1 A亚型(N = 5)或D亚型(N = 4)毒株的艾滋病患者中,源自大脑的HIV-1 env序列显示出比B亚型源自大脑的病毒更大的进化距离(P < 0.001)。同样,匹配的大脑和脾脏env克隆之间的分子多样性取决于亚型,且集中在高变V4区域(P < 0.001),来自同一器官的序列存在系统发育聚类。与匹配的脾脏来源克隆和大脑来源的B亚型病毒相比,大脑来源的A和D亚型序列显示出明显更低的非同义/同义替换率(d(N)/d(S))比值。在目前的env序列中很少观察到亚型间重组事件。一种含有来自A亚型大脑来源序列的C2V3区域的嵌合病毒优先利用CD4和CCR5进行感染。这些发现表明,大脑来源序列中分子多样性的差异取决于env基因内的个体亚型和结构域,但B亚型和非B亚型大脑来源的病毒均表现出对CCR5作为共受体的偏好。

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