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1型人类免疫缺陷病毒感染长期存活者的gag和pol序列特征分析

Characterization of gag and pol sequences from long-term survivors of human immunodeficiency virus type 1 infection.

作者信息

Huang Y, Zhang L, Ho D D

机构信息

Aaron Diamond AIDS Research Center, New York, New York, USA.

出版信息

Virology. 1998 Jan 5;240(1):36-49. doi: 10.1006/viro.1997.8913.

Abstract

We previously identified a group of 10 long-term survivors (LTS) of human immunodeficiency virus type 1 (HIV-1) infection. Extensive biological analysis revealed that some of these individuals do well, at least in part, because they possess weakened or attenuated viruses. Also, previously, to determine the genotype associated with the attenuated phenotype in vivo, we characterized nef, vif, vpr, vpu, env, and LTR in our cohort of LTS. In this study, we analyzed gag and pol genes derived from eight individuals in our cohort. For each subject multiple full-length gag and pol clones were obtained for analysis. In most cases, the sequences derived from the LTS had an intact open reading frame. At the protein level, there were no discernible differences between the sequences derived from LTS and those derived from patients with AIDS. Thus, no common defect in gag and pol was found in our cohort. One individual (subject SF), however, had only Gag-defective proviral sequences (10 of 10) in his peripheral blood mononuclear cells. Furthermore, longitudinal studies of the samples collected from SF over a 2-year period showed that all p17 gag clones sequenced (24 of 24) were defective due to G-to-A hypermutations. This viral defect in Gag may provide the molecular basis for this individual's extremely low viral load and long-term asymptomatic state. These results, together with previous findings in our LTS cohort, reinforce the notion that it is unlikely that a single common viral genetic determinant accounts for the lack of disease progression in all cases. Multiple host and viral factors undoubtedly contribute to the well-being of LTS of HIV-1 infection.

摘要

我们之前鉴定出一组10名人类免疫缺陷病毒1型(HIV-1)感染的长期存活者(LTS)。广泛的生物学分析表明,其中一些个体情况良好,至少部分原因是他们携带弱化或减毒的病毒。此外,之前为了确定体内与减毒表型相关的基因型,我们对我们的LTS队列中的nef、vif、vpr、vpu、env和LTR进行了特征分析。在本研究中,我们分析了队列中8名个体的gag和pol基因。对于每个受试者,获得了多个全长gag和pol克隆用于分析。在大多数情况下,LTS来源的序列具有完整开放阅读框。在蛋白质水平上,LTS来源的序列与艾滋病患者来源的序列之间没有明显差异。因此,在我们的队列中未发现gag和pol存在共同缺陷。然而,一名个体(SF受试者)外周血单个核细胞中只有Gag缺陷的前病毒序列(10个中有10个)。此外,对从SF在2年期间收集的样本进行的纵向研究表明,所有测序的p17 gag克隆(24个中有24个)由于G到A的超突变而存在缺陷。Gag中的这种病毒缺陷可能为该个体极低的病毒载量和长期无症状状态提供分子基础。这些结果与我们LTS队列中的先前发现一起,强化了这样一种观念,即单一常见的病毒遗传决定因素不太可能在所有情况下都导致疾病进展的缺乏。多种宿主和病毒因素无疑对HIV-1感染的LTS的健康状况有贡献。

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