慢性可卡因使用、B细胞紊乱和艾滋病病毒感染者接受抑制性抗逆转录病毒治疗后免疫恢复迟钝之间的联系

NeuroImmune pharmacology and therapeutics Pub Date : 2023-03-25 Epub Date: 2023-03-27 DOI:10.1515/nipt-2022-0019
Da Cheng, Zhenwu Luo, Sylvia Fitting, William Stoops, Sonya L Heath, Lishomwa C Ndhlovu, Wei Jiang
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引用次数: 0

摘要

背景:我们最近发现,抗CD4自身抗体有助于在接受抗逆转录病毒疗法(ART)的HIV+患者中钝化CD4+T细胞的重建。可卡因的使用在艾滋病毒携带者中很常见,并与疾病进展加速有关。然而,可卡因引起的免疫紊乱的潜在机制仍然不清楚。方法:我们评估了HIV+慢性可卡因使用者和非抑制性抗逆转录病毒疗法使用者以及未感染对照组的抗CD4 IgG和微生物易位标志物的血浆水平,以及B细胞基因表达谱和活化。评估血浆纯化的抗CD4 IgG的抗体依赖性细胞毒性(ADCC)。结果:与非使用者相比,HIV+可卡因使用者的血浆抗CD4 IgG、脂多糖(LPS)和可溶性CD14(sCD14)水平增加。在可卡因使用者中观察到了相反的相关性,但在非毒品使用者中没有观察到。来自HIV+可卡因使用者的抗CD4 IgG通过体外ADCC介导CD4+T细胞死亡。HIV+可卡因使用者的B细胞与非使用者相比,表现出与微生物易位相关的激活信号通路和激活(循环和TLR4表达)。结论:这项研究提高了我们对可卡因相关B细胞扰动和免疫衰竭的理解,并使我们对自身反应性B细胞作为新的治疗靶点有了新的认识。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The link between chronic cocaine use, B cell perturbations, and blunted immune recovery in HIV-infected individuals on suppressive ART.

The link between chronic cocaine use, B cell perturbations, and blunted immune recovery in HIV-infected individuals on suppressive ART.

The link between chronic cocaine use, B cell perturbations, and blunted immune recovery in HIV-infected individuals on suppressive ART.

The link between chronic cocaine use, B cell perturbations, and blunted immune recovery in HIV-infected individuals on suppressive ART.

Background: We recently reveal that anti-CD4 autoantibodies contribute to blunted CD4+ T cell reconstitution in HIV+ individuals on antiretroviral therapy (ART). Cocaine use is common among HIV+ individuals and is associated with accelerated disease progression. However, the mechanisms underlying cocaine-induced immune perturbations remain obscure.

Methods: We evaluated plasma levels of anti-CD4 IgG and markers of microbial translocation, as well as B-cell gene expression profiles and activation in HIV+ chronic cocaine users and non-users on suppressive ART, as well as uninfected controls. Plasma purified anti-CD4 IgGs were assessed for antibody-dependent cytotoxicity (ADCC).

Results: HIV+ cocaine users had increased plasma levels of anti-CD4 IgGs, lipopolysaccharide (LPS), and soluble CD14 (sCD14) versus non-users. An inverse correlation was observed in cocaine users, but not non-drug users. Anti-CD4 IgGs from HIV+ cocaine users mediated CD4+ T cell death through ADCC in vitro. B cells from HIV+ cocaine users exhibited activation signaling pathways and activation (cycling and TLR4 expression) related to microbial translocation versus non-users.

Conclusions: This study improves our understanding of cocaine associated B cell perturbations and immune failure and the new appreciation for autoreactive B cells as novel therapeutic targets.

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