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1型原发性人类免疫缺陷病毒分离株糖蛋白120 V2区长度变异与生物学表型及共受体使用情况的关系

Length variation of glycoprotein 120 V2 region in relation to biological phenotypes and coreceptor usage of primary HIV type 1 isolates.

作者信息

Jansson M, Backström E, Scarlatti G, Björndal A, Matsuda S, Rossi P, Albert J, Wigzell H

机构信息

Microbiology and Tumor Biology Center, Karolinska Institute, 171 77 Stockholm, Sweden.

出版信息

AIDS Res Hum Retroviruses. 2001 Oct 10;17(15):1405-14. doi: 10.1089/088922201753197079.

Abstract

Conflicting data have been published concerning the correlation between the length of the second variable region (V2) in the HIV-1 envelope and the biological phenotype of the virus. Here the V2 region length of primary HIV-1 isolates was compared with biological phenotype and coreceptor usage. The V2 region variation was determined by DNA fragment length analysis, virus biological phenotype by the MT-2 cell assay, and coreceptor usage by infection of U87.CD4 cells expressing CCR3, CCR5, or CXCR4. Ninety-three primary virus isolates from 40 patients were analyzed. This panel of viruses included sequential isolates obtained from patients who progressed to AIDS with or without a virus phenotypic switch. We found that NSI MT-2-negative isolates had significantly shorter V2 regions than SI MT-2-positive isolates. However, when V2 region lengths of viruses were analyzed in more detail, we observed that NSI isolates obtained from patients shortly before the phenotypic switch had V2 region lengths similar to those of SI isolates. V2 regions of NSI isolates obtained from patients who progressed to AIDS without a virus phenotypic switch had, in contrast, shorter V2 region than isolates obtained just before virus phenotypic switch. Coreceptor analysis revealed that CCR5-using (R5) isolates generally had shorter V2 regions than virus isolates with the ability to enter CXCR4-expressing cells. Moreover, no significant difference in V2 region length was observed between monotropic SI isolates, that is, X4 isolates, and multitropic SI isolates, that is, R3R5X4 or R5X4 isolates. Thus, we conclude that R5 NSI isolates obtained from patients with stable virus phenotype through the whole disease course display shorter V2 regions than isolates obtained from patients at switch of virus phenotype, suggesting that V2 region length may influence virus coreceptor usage.

摘要

关于人类免疫缺陷病毒1型(HIV-1)包膜中第二个可变区(V2)的长度与病毒生物学表型之间的相关性,已发表了相互矛盾的数据。在此,我们将原发性HIV-1分离株的V2区长度与生物学表型及共受体使用情况进行了比较。通过DNA片段长度分析确定V2区变异,通过MT-2细胞试验确定病毒生物学表型,通过感染表达CCR3、CCR5或CXCR4的U87.CD4细胞确定共受体使用情况。对来自40名患者的93株原发性病毒分离株进行了分析。这组病毒包括从进展为艾滋病的患者中获得的连续分离株,这些患者伴有或不伴有病毒表型转换。我们发现,非细胞病变性(NSI)MT-2阴性分离株的V2区明显短于细胞病变性(SI)MT-2阳性分离株。然而,当更详细地分析病毒的V2区长度时,我们观察到,在表型转换前不久从患者中获得的NSI分离株的V2区长度与SI分离株相似。相比之下,在没有病毒表型转换的情况下进展为艾滋病的患者中获得的NSI分离株的V2区比在病毒表型转换前刚获得的分离株的V2区短。共受体分析显示,使用CCR5的(R5)分离株的V2区通常比具有进入表达CXCR4细胞能力的病毒分离株短。此外,在单向性SI分离株(即X4分离株)和多向性SI分离株(即R3R5X4或R5X4分离株)之间,未观察到V2区长度有显著差异。因此,我们得出结论,在整个病程中具有稳定病毒表型的患者中获得的R5 NSI分离株的V2区比在病毒表型转换时从患者中获得的分离株短,这表明V2区长度可能影响病毒共受体的使用。

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