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HIV-1 envelope glycoprotein signatures that correlate with the development of cross-reactive neutralizing activity

机译:与交叉反应中和活性的发展相关的HIV-1包膜糖蛋白标记

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Background Current HIV-1 envelope glycoprotein (Env) vaccines are unable to induce cross-reactive neutralizing antibodies. However, such antibodies are elicited in 10-30% of HIV-1 infected individuals, but it is unknown why these antibodies are induced in some individuals and not in others. We hypothesized that the Envs of early HIV-1 variants in individuals who develop cross-reactive neutralizing activity (CrNA) might have unique characteristics that support the induction of CrNA. Results We retrospectively generated and analyzed env sequences of early HIV-1 clonal variants from 31 individuals with diverse levels of CrNA 2–4 years post-seroconversion. These sequences revealed a number of Env signatures that coincided with CrNA development. These included a statistically shorter variable region 1 and a lower probability of glycosylation as implied by a high ratio of NXS versus NXT glycosylation motifs. Furthermore, lower probability of glycosylation at position 332, which is involved in the epitopes of many broadly reactive neutralizing antibodies, was associated with the induction of CrNA. Finally, Sequence Harmony identified a number of amino acid changes associated with the development of CrNA. These residues mapped to various Env subdomains, but in particular to the first and fourth variable region as well as the underlying α2 helix of the third constant region. Conclusions These findings imply that the development of CrNA might depend on specific characteristics of early Env. Env signatures that correlate with the induction of CrNA might be relevant for the design of effective HIV-1 vaccines.
机译:背景技术当前的HIV-1包膜糖蛋白(Env)疫苗无法诱导交叉反应的中和抗体。但是,这种抗体是在10%至30%的HIV-1感染个体中引起的,但未知为什么这些抗体是在某些个体而不是其他个体中被诱导的。我们假设开发交叉反应中和活性(CrNA)的个体中早期HIV-1变体的Envs可能具有支持CrNA诱导的独特特征。结果我们回顾性分析了血清转化后2-4年CrNA水平不同的31名个体的早期HIV-1克隆变异体的env序列。这些序列揭示了许多与CrNA发育相吻合的Env特征。这些包括统计学上较短的可变区1和较低的糖基化概率,这是由NXS与NXT糖基化基序的比例高所暗示的。此外,参与许多广泛反应的中和抗体的表位的332位糖基化的可能性较低,与CrNA的诱导有关。最后,Sequence Harmony确定了许多与CrNA发生有关的氨基酸变化。这些残基映射到各种Env子域,但特别映射到第一和第四可变区以及第三恒定区的下面的α2螺旋。结论这些发现暗示CrNA的发展可能取决于早期Env的特定特征。与CrNA诱导相关的Env标记可能与有效HIV-1疫苗的设计有关。

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