首页> 美国卫生研究院文献>Journal of Virology >Quantitative analysis of serum neutralization of human immunodeficiency virus type 1 from subtypes A B C D E F and I: lack of direct correlation between neutralization serotypes and genetic subtypes and evidence for prevalent serum-dependent infectivity enhancement.
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Quantitative analysis of serum neutralization of human immunodeficiency virus type 1 from subtypes A B C D E F and I: lack of direct correlation between neutralization serotypes and genetic subtypes and evidence for prevalent serum-dependent infectivity enhancement.

机译:定量分析ABCDEF和I亚型的1型人类免疫缺陷病毒的血清中和作用:中和血清型和遗传亚型之间缺乏直接相关性并且没有普遍存在的血清依赖性感染力增强证据。

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摘要

Human immunodeficiency virus type 1 (HIV-1) M group strains have been assigned to date to nine distinct genetic subtypes, designated A through I, according to phylogenetic analyses of nucleotide sequences of their env or gag genes. Whether there is any relationship between phylogenetic subtypes and the neutralization serotypes is not clear, yet defining the nature of any such relationship by mathematical means would be of major importance for the development of globally effective HIV-1 vaccines. We have therefore developed a quantitative method to analyze serum neutralization of HIV-1 isolates and to identify HIV-1 neutralization serotypes. This method involves calculations of the neutralization index, N(i), a newly defined parameter derived from plots generated from in vitro neutralization assays, calculations of pairwise serum-virus vector distances, and cluster analyses. We have applied this approach to analyze three independent neutralization matrices involving primary HIV-1 strains and sera from genetic subtypes A, B, C, D, E, F, and I. Detailed serum and HIV-1 isolate cluster analyses have shown that in general, the identified neutralization serotypes do not directly correlate with HIV-1 genetic subtypes. These results suggest that neutralization serotypes do not during natural HIV-1 infection are not governed by antibodies directed against simple epitopes within gp120 monomers. A significant proportion (28%) of 1,213 combinations of sera and HIV-1 isolates caused serum-dependent infectivity enhancement [negative N(i) values] rather than neutralization. We also noted that negative N(i) values tended to correlate better with certain HIV-1 isolates rather than with HIV-1-positive sera. Syncytium-inducing variants of HIV-1 were slightly more likely than non-syncytium-inducing variants to undergo serum-dependent infectivity enhancement, although the latter variants could clearly be susceptible to enhancement.
机译:根据人类env或gag基因核苷酸序列的系统发育分析,迄今为止,人类免疫缺陷病毒1型(HIV-1)M组菌株已被划分为9种不同的遗传亚型,命名为A至I。系统发育亚型和中和血清型之间是否存在任何关系尚不清楚,但通过数学方法确定任何此类关系的性质对于开发全球有效的HIV-1疫苗至关重要。因此,我们开发了一种定量方法来分析HIV-1分离株的血清中和并鉴定HIV-1中和血清型。该方法涉及中和指数N(i)的计算,这是一个新定义的参数,该参数源自通过体外中和测定生成的图,成对的血清-病毒载体距离计算和聚类分析。我们已经采用这种方法来分析涉及基因型A,B,C,D,E,F和I的主要HIV-1菌株和血清的三个独立的中和基质。详细的血清和HIV-1分离物聚类分析表明,通常,鉴定出的中和血清型与HIV-1遗传亚型不直接相关。这些结果表明,中和血清型在自然HIV-1感染期间不会受到针对gp120单体内简单表位的抗体的控制。 1,213份血清和HIV-1分离株组合中有很大一部分(28%)导致血清依赖性感染力增强[N(i)值为负],而不是中和。我们还注意到,负N(i)值倾向于与某些HIV-1分离株更好地相关,而不是与HIV-1阳性血清相关。 HIV-1的合胞体诱导变异体比非合体诱导变异体发生血清依赖性感染力增强的可能性稍高,尽管后者显然很容易被增强。

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