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Dynamic interplay between viral adaptation and immune recognition during HIV-1 infection

机译:HIV-1感染期间病毒适应与免疫识别之间的动态相互作用

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摘要

Untreated human immunodeficiency virus (HIV) infections usually lead to death from AIDS, although the rate of the disease progression varies widely among individuals. The cytotoxic T lymphocyte (CTL) response, which is restricted by highly polymorphic MHC class I alleles, plays a central role in controlling HIV replication. It is now recognized that the antiviral efficacy of CTLs at the single cell level is dependent on their antigen specificity and is important in determining the quality of host response to viruses so that the individual will remain asymptomatic. However, because of the extreme mutational plasticity of HIV, HIV-specific CTL responses are continuously and dynamically changing. In order to rationally design an effective vaccine, the questions as to what constitutes an effective antiviral CTL response and what characterizes a potent antigenic peptide to induce such responses are becoming highlighted as needing to be answered.
机译:未经治疗的人类免疫缺陷病毒(HIV)感染通常会导致艾滋病死亡,尽管个体之间疾病进展的速度差异很大。受高度多态性的MHC I类等位基因限制的细胞毒性T淋巴细胞(CTL)反应在控制HIV复制中起着核心作用。现在已经认识到,CTL在单细胞水平上的抗病毒效力取决于其抗原特异性,并且在确定宿主对病毒的反应质量方面很重要,因此该个体将保持无症状。但是,由于HIV的极端突变可塑性,特定于HIV的CTL反应不断且动态变化。为了合理地设计有效的疫苗,关于哪些成分构成有效的抗病毒CTL应答以及表征有效抗原肽以诱导此类应答的特征的问题已成为需要回答的问题。

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