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High prevalence of neutralizing activity against multiple unrelated human immunodeficiency virus type 1 (HIV-1) subtype B variants in sera from HIV-1 subtype B-infected individuals: evidence for subtype-specific rather than strain-specific neutralizing activity

机译:来自HIV-1亚型B感染个体的血清中针对多种不相关的人类免疫缺陷病毒1型(HIV-1)B亚型变体的中和活性普遍存在:有亚型特异性而非菌株特异性中和活性的证据

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摘要

It is assumed that an effective human immunodeficiency virus type 1 (HIV-1) vaccine should be capable of eliciting neutralizing antibodies. However, even the best antibodies known to date lack neutralizing ability against a significant proportion of primary HIV-1 variants and, despite great efforts, still no immunogen is available that can elicit humoral immunity which is protective against infection or disease progression. We tested sera from 35 participants in the Amsterdam Cohort Studies on HIV-1 infection, who were all infected with HIV-1 subtype B and therapy-naive at the time of sampling, for neutralizing activity against a panel of 23 tier 2-3 HIV-1 variants, with a minimum of five HIV-1 variants per subtype (A, B, C and D). Strong cross-clade neutralizing activity was detected in sera from seven individuals. Strikingly, sera from 22 of 35 individuals (63%) neutralized three or more of the six tier 2-3 HIV-1 subtype B viruses in the panel. There was a strong correlation between neutralization titre and breadth in serum. Indeed, the IC50 of sera with strong cross-clade neutralizing activity was significantly higher than the IC50 of sera with cross-subtype B activity, which, in turn, had a higher IC50 than sera with the lowest neutralization breadth. These results imply that humoral immunity, at least in HIV-1 subtype B-infected individuals, is often subtype-specific rather than strain-specific and that the breadth of neutralization is correlated with the titre of neutralizing activity in serum. Considering the difficulties in designing a vaccine that is capable of eliciting cross-clade neutralizing activity, subtype-specific vaccines may be explored as an interesting alternative
机译:假定有效的1型人类免疫缺陷病毒(HIV-1)疫苗应能够引发中和抗体。然而,即使迄今为止已知的最好的抗体也缺乏针对显着比例的主要HIV-1变体的中和能力,尽管付出了很大的努力,但仍然没有可用的免疫原来引发体液免疫,从而可以防止感染或疾病进展。我们测试了来自阿姆斯特丹队列研究的35名HIV-1感染者的血清,这些血清在采样时均感染了HIV-1 B型亚型且在治疗时未接受过治疗,其血清中和了针对23种2-3层HIV的活性-1个变体,每个亚型(A,B,C和D)至少具有五个HIV-1变体。在来自七个个体的血清中检测到强的跨层中和活性。令人惊讶的是,来自35个人中的22个人(63%)的血清中和了六种2-3级HIV-1 B型亚型病毒中的三种或更多种。血清中和滴度和广度之间有很强的相关性。实际上,具有强大的跨包中和活性的血清的IC50显着高于具有交叉亚型B活性的血清的IC50,这又比具有最低中和宽度的血清的IC50高。这些结果表明,至少在HIV-1亚型B感染个体中,体液免疫通常是亚型特异性的,而不是菌株特异性的,并且中和的广度与血清中和活性的效价有关。考虑到在设计能够引发跨包中和活性的疫苗方面的困难,可以探索亚型特异性疫苗作为有趣的替代方法

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