HIV Pathogenesis Programme, The Doris Duke Medical Research Institute, University of KwaZulu-Natal, Durban, South Africa.
Department of Virus Immunology, Leibniz Institute of Virology, Hamburg, Germany.
J Infect Dis. 2024 Mar 14;229(3):753-762. doi: 10.1093/infdis/jiad432.
Immune dysfunction often persists in people living with human immunodeficiency virus (HIV) who are on antiretroviral therapy (ART), clinically manifesting as HIV-1-associated comorbid conditions. Early ART initiation may reduce incidence of HIV-1-associated immune dysfunction and comorbid conditions. Immunometabolism is a critical determinant of functional immunity. We investigated the effect of HIV-1 infection and timing of ART initiation on CD4+ T cell metabolism and function.
Longitudinal blood samples from people living with HIV who initiated ART during hyperacute HIV-1 infection (HHI; before peak viremia) or chronic HIV-1 infection (CHI) were assessed for the metabolic and immune functions of CD4+ T cells. Metabolite uptake and mitochondrial mass were measured using fluorescent analogues and MitoTracker Green accumulation, respectively, and were correlated with CD4+ T cell effector functions.
Initiation of ART during HHI prevented dysregulation of glucose uptake by CD4+ T cells, but glucose uptake was reduced before and after ART initiation in CHI. Glucose uptake positively correlated with interleukin-2 and tumor necrosis factor-α production by CD4+ T cells. CHI was associated with elevated mitochondrial mass in effector memory CD4+ T cells that persisted after ART and correlated with PD-1 expression.
ART initiation in HHI largely prevented metabolic impairment of CD4+ T cells. ART initiation in CHI was associated with persistently dysregulated immunometabolism of CD4+ T cells, which was associated with impaired cellular functions and exhaustion.
接受抗逆转录病毒疗法(ART)的艾滋病毒(HIV)感染者常存在免疫功能障碍,临床上表现为与 HIV-1 相关的合并症。早期开始 ART 可能会降低 HIV-1 相关免疫功能障碍和合并症的发生率。免疫代谢是功能性免疫的关键决定因素。我们研究了 HIV-1 感染和开始 ART 的时机对 CD4+T 细胞代谢和功能的影响。
对在超急性 HIV-1 感染(HHI;在病毒血症高峰之前)或慢性 HIV-1 感染(CHI)期间开始接受 ART 的 HIV 感染者的纵向血液样本进行了评估,以研究 CD4+T 细胞的代谢和免疫功能。使用荧光类似物测量了代谢物摄取,并用 MitoTracker Green 积累测量了线粒体质量,并用 CD4+T 细胞效应功能进行了相关分析。
HHI 期间开始 ART 可防止 CD4+T 细胞葡萄糖摄取失调,但 CHI 中在开始 ART 之前和之后葡萄糖摄取减少。葡萄糖摄取与 CD4+T 细胞产生白细胞介素-2 和肿瘤坏死因子-α呈正相关。CHI 与效应记忆 CD4+T 细胞中线粒体质量升高有关,这种升高在 ART 后仍然存在,并与 PD-1 表达相关。
HHI 期间开始 ART 可在很大程度上防止 CD4+T 细胞代谢受损。CHI 期间开始 ART 与 CD4+T 细胞免疫代谢持续失调有关,这与细胞功能受损和衰竭有关。
