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HIV-specific CD8+ T cells and HIV eradication

机译:特定于HIV的CD8 + T细胞和消除HIV

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After the success of combination antiretroviral therapy (cART) to treat HIV infection, the next great frontier is to cure infected persons, a formidable challenge. HIV persists in a quiescent state in resting CD4~(+) T cells, where the replicative enzymes targeted by cART are not active. Although low levels of HIV transcripts are detectable in these resting cells, little to no viral protein is produced, rendering this reservoir difficult to detect by the host CD8~(+) T cell response. However, recent advances suggest that this state of latency might be pharmacologically reversed, resulting in viral protein expression without the adverse effects of massive cellular activation. Emerging data suggest that with this approach, infected cells will not die of viral cytopathic effects, but might be eliminated if HIV-specific CD8~(+) T cells can be effectively harnessed. Here, we address the antiviral properties of HIV-specific CD8~(+) T cells and how these cells might be harnessed to greater effect toward achieving viral eradication or a functional cure.
机译:在抗逆转录病毒疗法(cART)组合成功治疗艾滋病毒感染之后,下一个重要领域是治愈感染者,这是一个艰巨的挑战。 HIV在静止的CD4〜(+)T细胞中保持静止状态,而cART靶向的复制酶不活跃。尽管在这些静息细胞中可检测到低水平的HIV转录物,但几乎没有产生病毒蛋白,这使得宿主CD8〜(+)T细胞反应难以检测到该病毒库。但是,最近的进展表明,这种潜伏状态可能在药理学上被逆转,从而导致病毒蛋白表达而没有大规模细胞活化的不利影响。新兴数据表明,使用这种方法,感染的细胞不会死于病毒的细胞病变作用,但是,如果可以有效利用HIV特异性CD8〜(+)T细胞,则可以将其消除。在这里,我们讨论了HIV特异性CD8〜(+)T细胞的抗病毒特性,以及如何利用这些细胞对实现病毒根除或功能治愈产生更大的作用。

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