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CD4+ T 细胞亚群中 HIV-DNA 负荷的分布和降低幅度取决于抗逆转录病毒治疗的起始时机。

Distribution and reduction magnitude of HIV-DNA burden in CD4+ T cell subsets depend on art initiation timing.

机构信息

Virology Laboratory, Hôpitaux Universitaires de Strasbourg.

Strasbourg University, INSERM, UMR-S U1109, F-67000.

出版信息

AIDS. 2018 Apr 24;32(7):921-926. doi: 10.1097/QAD.0000000000001770.

Abstract

OBJECTIVE

The aim of our study was to analyze the dynamics of HIV-DNA levels in CD4 T-cell subsets in individuals starting successful dolutegravir-based regimens.

DESIGN

Twenty-seven individuals with acute infection (AI, n = 8) or chronic infection (CI, n = 5) and patients in virological success (VS, n = 10) or virological failure (VF, n = 4) on antiretroviral therapy (ART) who initiated a dolutegravir-based regimen were enrolled (NCT02557997).

METHODS

CD4 T-cells from baseline and week 48 of successful treatment were sorted into effector memory (TEM), transitional memory (TTM), central memory (TCM) and naïve (TN) cell groups for total HIV-DNA measurements by qPCR. Bayesian methods were used to estimate the posterior probability of a HIV-DNA decrease more than 0.25 log copies/10 cells at week 48.

RESULTS

All patients achieved HIV-RNA suppression at 48 weeks. At baseline and week 48, the highest contributions to the HIV-DNA-infected pool from CD4 T cells were observed in TTM cells in the AI group (62.4 and 60.2%, respectively), but in TCM cells for the CI, VS and VF groups (54.6 and 59.4%, 58.2 and 62.9%, 62.4 and 67.2%), respectively. HIV-DNA burden declined in all subsets after 48 weeks of treatment in the AI (probability (Pr) > 91%), CI (Pr > 52%) and VF (Pr > 52%) groups, but only in TEM cells in the VS group (Pr = 95%).

CONCLUSION

Our study showed that dolutegravir-based treatment reduced the HIV-DNA cellular burden in individuals from the AI, CI and VF groups, though the reduction levels differed between the patient subgroups. Early treated patients had the highest probability of HIV-DNA reduction. Interestingly, in the aviremic VS group, HIV-DNA reduction was limited to TEM cells.

摘要

目的

我们的研究旨在分析开始接受成功的多替拉韦为基础的治疗方案的个体中 CD4 T 细胞亚群中 HIV-DNA 水平的动态变化。

设计

共纳入了 27 名急性感染(AI,n=8)或慢性感染(CI,n=5)个体,以及正在接受抗病毒治疗(ART)的病毒学成功(VS,n=10)或病毒学失败(VF,n=4)的个体,他们均开始了多替拉韦为基础的治疗方案(NCT02557997)。

方法

从基线和成功治疗的第 48 周采集 CD4 T 细胞,并通过 qPCR 对总 HIV-DNA 进行检测,将细胞分为效应记忆(TEM)、过渡记忆(TTM)、中央记忆(TCM)和幼稚(TN)细胞群。采用贝叶斯方法来估计第 48 周 HIV-DNA 下降超过 0.25log 拷贝/10 细胞的后验概率。

结果

所有患者在第 48 周均实现了 HIV-RNA 抑制。在基线和第 48 周,AI 组中 TTM 细胞对 HIV-DNA 感染池的贡献最大(分别为 62.4%和 60.2%),而 CI、VS 和 VF 组中则是 TCM 细胞(分别为 54.6%和 59.4%、58.2%和 62.9%、62.4%和 67.2%)。在 AI(概率(Pr)>91%)、CI(Pr>52%)和 VF(Pr>52%)组中,所有亚群在 48 周的治疗后 HIV-DNA 负荷均下降,但 VS 组仅在 TEM 细胞中下降(Pr=95%)。

结论

我们的研究表明,多替拉韦为基础的治疗降低了 AI、CI 和 VF 组个体的 HIV-DNA 细胞负荷,但患者亚组之间的降低水平不同。早期治疗的患者 HIV-DNA 降低的可能性最高。有趣的是,在病毒学上无反应的 VS 组中,HIV-DNA 降低仅限于 TEM 细胞。

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