首页> 美国卫生研究院文献>The Journal of Clinical Investigation >IL-7 is a potent and proviral strain–specific inducer of latent HIV-1 cellular reservoirs of infected individuals on virally suppressive HAART
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IL-7 is a potent and proviral strain–specific inducer of latent HIV-1 cellular reservoirs of infected individuals on virally suppressive HAART

机译:IL-7是病毒抑制性HAART上感染个体的潜在HIV-1细胞储库的强效和前病毒株特异性诱导剂

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摘要

The persistence of HIV-1 in virally suppressed infected individuals on highly active antiretroviral therapy (HAART) remains a major therapeutic problem. The use of cytokines has been envisioned as an additional therapeutic strategy to stimulate latent proviruses in these individuals. Immune activation therapy using IL-2 has shown some promise. In the present study, we found that IL-7 was significantly more effective at enhancing HIV-1 proviral reactivation than either IL-2 alone or IL-2 combined with phytohemagglutinin (PHA) in CD8-depleted PBMCs. IL-7 also showed a positive trend for inducing proviral reactivation from resting CD4+ T lymphocytes from HIV-1–infected patients on suppressive HAART. Moreover, the phylogenetic analyses of viral envelope gp120 genes from induced viruses indicated that distinct proviral quasispecies had been activated by IL-7, as compared with those activated by the PHA/IL-2 treatment. These studies thus demonstrate that different activators of proviral latency may perturb and potentially deplete only selected, specific portions of the proviral archive in virally suppressed individuals. The known immunomodulatory effects of IL-7 could be combined with its ability to stimulate HIV-1 replication from resting CD4+ T lymphocytes, in addition to other moieties, to potentially deplete HIV-1 reservoirs and lead to the rational design of immune-antiretroviral approaches.
机译:HIV-1在高活性抗逆转录病毒疗法(HAART)上被病毒抑制的感染者的持久性仍然是一个主要的治疗问题。已经设想使用细胞因子作为刺激这些个体中潜伏的原病毒的另一种治疗策略。使用IL-2的免疫激活疗法已显示出一定的前景。在本研究中,我们发现,在CD8缺失的PBMC中,IL-7在增强HIV-1前病毒再激活方面比单独使用IL-2或将IL-2结合植物血凝素(PHA)更为有效。 IL-7在抑制性HAART上,还可以诱导HIV-1感染患者的静息CD4 + T淋巴细胞诱导原病毒的再激活。此外,对来自诱导病毒的病毒包膜gp120基因的系统进化分析表明,与PHA / IL-2处理激活的准种相比,IL-7激活了不同的准病毒准种。因此,这些研究表明,在病毒抑制的个体中,不同的前病毒潜伏期激活剂可能会干扰并可能耗尽仅选定的特定部分的前病毒档案。 IL-7的已知免疫调节作用与其刺激HIV-1从静止的CD4 + T淋巴细胞(除了其他部分)复制的能力相结合,还可能耗尽HIV-1的储库并导致免疫抗逆转录病毒方法的合理设计。

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