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直击艾滋病病毒的要害:艾滋病病毒疫苗设计的另一种方法。

Hitting HIV where it hurts: an alternative approach to HIV vaccine design.

作者信息

Altfeld Marcus, Allen Todd M

机构信息

Partners AIDS Research Center, Infectious Disease Unit, Massachusetts General Hospital and Division of AIDS, Harvard Medical School, Boston, MA 02129, USA.

出版信息

Trends Immunol. 2006 Nov;27(11):504-10. doi: 10.1016/j.it.2006.09.007. Epub 2006 Sep 25.

Abstract

The ability of HIV-1 to mutate represents a major challenge to current vaccine approaches. However, some individuals achieving control of HIV during natural infection seem unique in their dominant targeting by cellular immune responses of conserved regions of HIV that, if mutated, exact a substantial impact on viral replicative capacity, or fitness. Notably, the partial suppression of HIV in treated individuals harboring viruses with drug-resistant mutations has also been linked to impaired viral fitness. The convergence of these observations suggests that vaccines designed to focus immune responses narrowly against regions of HIV susceptible to highly deleterious mutations might prove effective in controlling viral replication to levels that slow disease progression and reduce transmission. Therefore, it will be crucial to identify these "Achilles heels" of HIV that might represent uniquely susceptible targets, and test whether vaccine constructs enabling specific targeting of CD8(+) T-cell responses against such regions would enable the control of HIV and SIV.

摘要

HIV-1的变异能力对当前的疫苗研发方法构成了重大挑战。然而,一些在自然感染期间实现HIV控制的个体,其细胞免疫反应对HIV保守区域的主要靶向作用似乎很独特,这些保守区域一旦发生突变,就会对病毒复制能力或适应性产生重大影响。值得注意的是,在携带耐药突变病毒的接受治疗个体中,HIV的部分抑制也与病毒适应性受损有关。这些观察结果的趋同表明,设计用于将免疫反应精准聚焦于HIV易发生高度有害突变区域的疫苗,可能在将病毒复制控制到减缓疾病进展和减少传播的水平方面被证明是有效的。因此,识别这些可能代表独特易感靶点的HIV“阿喀琉斯之踵”,并测试能够使CD8(+) T细胞反应特异性靶向这些区域的疫苗构建体是否能够控制HIV和SIV,将至关重要。

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