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驱动人类免疫缺陷病毒1型env基因进化的选择性限制的宿主特异性调节

Host-specific modulation of the selective constraints driving human immunodeficiency virus type 1 env gene evolution.

作者信息

Bagnarelli P, Mazzola F, Menzo S, Montroni M, Butini L, Clementi M

机构信息

Institute of Microbiology, University of Ancona, Ancona, Italy.

出版信息

J Virol. 1999 May;73(5):3764-77. doi: 10.1128/JVI.73.5.3764-3777.1999.

Abstract

To address the evolution of human immunodeficiency virus type 1 (HIV-1) within a single host, we analyzed the HIV-1 C2-V5 env regions of both cell-free genomic-RNA- and proviral-DNA-derived clones. Sequential samples were collected over a period of 3 years from six untreated subjects (three typical progressors [TPs] and three slow progressors [SPs], all with a comparable length of infection except one. The evolutionary analysis of the C2-V5 env sequences performed on 506 molecular clones (253 RNA- and 253 DNA-derived sequences) highlighted a series of differences between TPs and SPs. In particular, (i) clonal sequences from SPs (DNA and RNA) showed lower nucleotide similarity than those from TPs (P = 0. 0001), (ii) DNA clones from SPs showed higher intra- and intersample nucleotide divergence than those from TPs (P < 0.05), (iii) higher host-selective pressure was generally detectable in SPs (DNA and RNA sequences), and (iv) the increase in the genetic distance of DNA and RNA sequences over time was paralleled by an increase in both synonymous (Ks) and nonsynonymous (Ka) substitutions in TPs but only in nonsynonymous substitutions in SPs. Several individual peculiarities of the HIV-1 evolutionary dynamics emerged when the V3, V4, and V5 env regions of both TPs and SPs were evaluated separately. These peculiarities, probably reflecting host-specific features of selective constraints and their continuous modulation, are documented by the dynamics of Ka/Ks ratios of hypervariable env domains.

摘要

为了研究人类免疫缺陷病毒1型(HIV-1)在单一宿主内的进化情况,我们分析了源自无细胞基因组RNA和前病毒DNA的克隆的HIV-1 C2-V5 env区域。在3年时间里,从6名未接受治疗的受试者(3名典型进展者[TPs]和3名缓慢进展者[SPs],除1名外感染时间长度相当)采集了连续样本。对506个分子克隆(253个源自RNA的序列和253个源自DNA的序列)进行的C2-V5 env序列进化分析突出了TPs和SPs之间的一系列差异。具体而言,(i)SPs(DNA和RNA)的克隆序列显示出比TPs更低的核苷酸相似性(P = 0.0001),(ii)SPs的DNA克隆显示出比TPs更高的样本内和样本间核苷酸差异(P <0.05),(iii)在SPs(DNA和RNA序列)中通常可检测到更高的宿主选择压力,(iv)随着时间推移,DNA和RNA序列遗传距离的增加在TPs中与同义(Ks)和非同义(Ka)替换的增加平行,但在SPs中仅与非同义替换的增加平行。当分别评估TPs和SPs的V3、V4和V5 env区域时,出现了HIV-1进化动力学的几个个体特性。这些特性可能反映了选择性限制的宿主特异性特征及其持续调节,由高变env结构域的Ka/Ks比率动态记录。

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