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通过抗体与V3环结合对1型艾滋病毒进行血清分型:与病毒基因型的关系。世界卫生组织艾滋病毒分离与鉴定网络。

Serotyping HIV type 1 by antibody binding to the V3 loop: relationship to viral genotype. WHO Network for HIV Isolation and Characterization.

作者信息

Cheingsong-Popov R, Lister S, Callow D, Kaleebu P, Beddows S, Weber J

机构信息

Department of Genito-Urinary Medicine and Communicable Diseases, St. Mary's Hospital Medical School, London, U.K.

出版信息

AIDS Res Hum Retroviruses. 1994 Nov;10(11):1379-86. doi: 10.1089/aid.1994.10.1379.

DOI:10.1089/aid.1994.10.1379
PMID:7888191
Abstract

We have investigated whether peptides representing the HIV-1 principal neutralization domain (V3) can be used as antigens in antibody-binding assays to predict the genotypes of the subjects' virus. Serum samples collected from HIV-1-infected subjects from the four WHO-sponsored vaccine evaluation sites (Uganda, Rwanda, Thailand, and Brazil) were characterized by antibody binding to a panel of synthetic V3 peptides that were derived from the consensus sequences of the V3 region of the HIV-1 subgroups according to the env phylogenetic analysis (A-E). An indirect V3 peptide-binding assay was used for primary screening, and a V3 peptide antigen-limiting ELISA was then used as a secondary assay to discriminate cross-reactivity if the screening assay was equivocal. In general, V3 peptide serology could predict HIV-1 genotypes. In sera for which the genotype of the virus was known, peptide assays could predict the correct genotype in approximately 90% of cases for genotypes A, B, C, and E; Ugandan sera of genotype D were more broadly reactive. There was considerable serological cross-reactivity between some HIV-1 genotypes, in particular between A and C, and, to a lesser extent, B and D subtypes. Owing to polymorphism at the crown of the V3 loop, an additional B peptide (B') was required to type Brazilian B genotype sera. These simple assays may help facilitate the determination and distribution of HIV-1 genotypes circulating in populations.

摘要

我们研究了代表HIV-1主要中和结构域(V3)的肽段是否可用作抗体结合试验中的抗原,以预测受试者病毒的基因型。从世界卫生组织赞助的四个疫苗评估地点(乌干达、卢旺达、泰国和巴西)的HIV-1感染受试者收集的血清样本,通过与一组合成V3肽段的抗体结合来表征,这些肽段是根据env系统发育分析(A-E)从HIV-1亚组V3区域的共有序列推导而来的。采用间接V3肽段结合试验进行初步筛选,如果筛选试验结果不明确,则使用V3肽段抗原限量ELISA作为二次试验来区分交叉反应性。一般来说,V3肽段血清学可以预测HIV-1基因型。在已知病毒基因型的血清中,肽段试验对A、B、C和E基因型的预测准确率约为90%;乌干达D基因型血清的反应性更广泛。一些HIV-1基因型之间存在相当程度的血清学交叉反应,特别是A和C之间,以及程度较轻的B和D亚型之间。由于V3环顶部的多态性,需要额外的B肽段(B')来鉴定巴西B基因型血清。这些简单的试验可能有助于促进对人群中循环的HIV-1基因型的确定和分布。

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