病理性增殖:HIV 感染者 CD4 T 细胞恢复不良的潜在机制。
Pathological proliferation: a potential mechanism for poor CD4 T cell recovery in people living with HIV.
机构信息
Center for Infectious Diseases, Beijing Youan Hospital, Capital Medical University, Beijing, China.
Beijing Institute of Sexually Transmitted Disease Prevention and Control, Beijing, China.
出版信息
Front Cell Infect Microbiol. 2024 Mar 27;14:1344778. doi: 10.3389/fcimb.2024.1344778. eCollection 2024.
BACKGROUND
People living with HIV (PLWH) fail to achieve normalization of CD4 T cell counts and function, especially in immunological non-responders (INRs). The frequencies of Ki67CD4 T cells were inversely associated with CD4 T cell counts in HIV infected patients. Early ART did not normalize CD4 T cell proliferation. However, the features of the abnormal proliferation CD4 T cell in INRs are far from known.
METHOD
PLWH were divided into INRs (n= 16) and immunological responders (IRs, n= 53) groups. Mass cytometry was applied to peripheral blood T cells to profile the immune cells and liquid chip technique was used to measure plasma levels of cytokines and chemokines. Correlation analyses were conducted to evaluate associations between the degree of CD4 T cell proliferation and immune function.
RESULTS
The percentage of Ki67 CD4 T cells were significant higher in INRs, and we defined these cells with significant higher level of Ki67, as over-proliferating cells. No significant difference of markers' expression (HLA-DR, CD38, CD57, PD-1, PD-L1, CD107a, perforin) was found between INRs and IRs. Compared with naïve CD4 T cells in INRs, Ki67 CD4 T cells exhibited lower levels of CD57 and CD38. Whereas Ki67 T cells exhibited higher levels of CD38 and CD57 and activation compared with differentiated mature central memory CD4 T cells and effector memory CD4 T cells. Ki67 cells did not show higher levels of senescence and activation compared to certain Ki67 CD4 central memory T cells in IRs. Furthermore, Ki67 CD4 Tcm cells exhibited positive correlations with pro-inflammatory cytokines.
CONCLUSION
We proposed and validated the hypothesis of "pathological proliferation" in INRs: excessive proliferation of CD4 T cells in INRs may be accompanied by aberrant activation, senescence and loss of immune function. Eventually, such over-proliferating but poor-quality cells in INRs result in incomplete recovery of both CD4 T cell counts and function. An intervention that enhancing the proliferative capacity or functional ability or both of CD4 T cell in INRs might therefore be beneficial.
背景
人类免疫缺陷病毒(HIV)感染者(PLWH)无法实现 CD4 T 细胞计数和功能的正常化,尤其是在免疫无应答者(INRs)中。Ki67CD4 T 细胞的频率与 HIV 感染患者的 CD4 T 细胞计数呈负相关。早期抗逆转录病毒治疗(ART)并不能使 CD4 T 细胞增殖正常化。然而,INRs 中异常增殖的 CD4 T 细胞的特征尚不清楚。
方法
将 PLWH 分为免疫无应答者(INRs,n=16)和免疫应答者(IRs,n=53)组。采用液质联用技术检测血浆细胞因子和趋化因子水平,用质谱流式细胞术分析外周血 T 细胞免疫表型。进行相关性分析以评估 CD4 T 细胞增殖程度与免疫功能之间的关系。
结果
INRs 中 Ki67 CD4 T 细胞的比例显著升高,我们将这些细胞定义为过度增殖细胞,这些细胞具有更高水平的 Ki67。INRs 和 IRs 之间的标志物表达(HLA-DR、CD38、CD57、PD-1、PD-L1、CD107a、穿孔素)无显著差异。与 INRs 中的幼稚 CD4 T 细胞相比,Ki67 CD4 T 细胞的 CD57 和 CD38 表达水平较低。而 Ki67 T 细胞与分化成熟的中央记忆 CD4 T 细胞和效应记忆 CD4 T 细胞相比,具有更高的 CD38 和 CD57 表达水平和激活状态。与 IRs 中某些 Ki67 CD4 中央记忆 T 细胞相比,Ki67 细胞的衰老和激活水平并没有更高。此外,Ki67 CD4 Tcm 细胞与促炎细胞因子呈正相关。
结论
我们提出并验证了 INRs 中“病理性增殖”的假设:INRs 中 CD4 T 细胞的过度增殖可能伴随着异常激活、衰老和免疫功能丧失。最终,INRs 中这种过度增殖但质量较差的细胞导致 CD4 T 细胞计数和功能的不完全恢复。因此,增强 INRs 中 CD4 T 细胞的增殖能力或功能能力或两者兼而有之的干预措施可能是有益的。
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