内脏利什曼病患者 CD4+T 细胞中白细胞介素-7 信号的改变。
Altered IL-7 signaling in CD4+ T cells from patients with visceral leishmaniasis.
机构信息
Department of Medicine, Institute of Medical Sciences, Banaras Hindu University, Varanasi Uttar Pradesh India.
School of Medicine & Health Sciences, The George Washington University, Washington, Washington, United States of America.
出版信息
PLoS Negl Trop Dis. 2024 Feb 26;18(2):e0011960. doi: 10.1371/journal.pntd.0011960. eCollection 2024 Feb.
BACKGROUND
CD4+ T cells play a central role in control of L. donovani infection, through IFN-γ production required for activation of macrophages and killing of intracellular parasites. Impaired control of parasites can in part be explained by hampered CD4+ T cells effector functions in visceral leishmaniasis (VL) patients. In a recent studies that defined transcriptional signatures for CD4+ T cells from active VL patients, we found that expression of the IL-7 receptor alpha chain (IL-7Rα; CD127) was downregulated, compared to CD4+ T cells from endemic controls (ECs). Since IL-7 signaling is critical for the survival and homeostatic maintenance of CD4+ T cells, we investigated this signaling pathway in VL patients, relative to ECs.
METHODS
CD4+ T cells were enriched from peripheral blood collected from VL patients and EC subjects and expression of IL7 and IL7RA mRNA was measured by real time qPCR. IL-7 signaling potential and surface expression of CD127 and CD132 on CD4+ T cell was analyzed by multicolor flow cytometry. Plasma levels of soluble IL-7 and sIL-7Rα were measured by ELISA.
RESULT
Transcriptional profiling data sets generated previously from our group showed lower IL7RA mRNA expression in VL CD4+ T cells as compared to EC. A significant reduction was, however not seen when assessing IL7RA mRNA by RT-qPCR. Yet, the levels of soluble IL-7Rα (sIL-7Rα) were reduced in plasma of VL patients compared to ECs. Furthermore, the levels of soluble IL-7 were higher in plasma from VL patients compared to ECs. Interestingly, expression of the IL-7Rα protein was higher on VL patient CD4+ T cells as compared to EC, with activated CD38+ CD4+ T cells showing higher surface expression of IL-7Rα compared to CD38- CD4+ T cells in VL patients. CD4+ T cells from VL patients had higher signaling potential baseline and after stimulation with recombinant human IL-7 (rhIL-7) compared to EC, as measured by phosphorylation of STAT5 (pSTAT5). Interestingly, it was the CD38 negative cells that had the highest level of pSTAT5 in VL patient CD4+ T cells after IL-7 stimulation. Thus, despite unaltered or potentially lowered IL7RA mRNA expression by CD4+ T cells from VL patients, the surface expression of the IL-7Rα was higher compared to EC and increased pSTAT5 was seen following exposure to rhIL-7. Accordingly, IL-7 signaling appears to be functional and even enhanced in VL CD4+ T cells and cannot explain the impaired effector function of VL CD4+ T cells. The enhanced plasma IL-7 may serve as part of homeostatic feedback mechanism regulating IL7RA expression in CD4+ T cells.
背景
CD4+T 细胞通过 IFN-γ 的产生在控制利什曼原虫感染中发挥核心作用,IFN-γ的产生对于激活巨噬细胞和杀死细胞内寄生虫是必需的。在利什曼原虫病(VL)患者中,寄生虫的控制受损部分可以用 CD4+T 细胞效应功能受损来解释。在最近的研究中,我们定义了活跃的 VL 患者的 CD4+T 细胞的转录特征,与地方流行对照(EC)相比,我们发现白细胞介素 7 受体α链(IL-7Rα;CD127)的表达下调。由于 IL-7 信号对于 CD4+T 细胞的存活和体内平衡维持至关重要,因此我们研究了 VL 患者相对于 EC 的这种信号通路。
方法
从 VL 患者和 EC 受试者的外周血中富集 CD4+T 细胞,并通过实时 qPCR 测量 IL7 和 IL7RA mRNA 的表达。通过多色流式细胞术分析 CD4+T 细胞上的 IL-7 信号潜能和 CD127 和 CD132 的表面表达。通过 ELISA 测量血浆中可溶性 IL-7 和 sIL-7Rα 的水平。
结果
我们之前的研究小组生成的转录谱数据集显示,VL CD4+T 细胞中的 IL7RA mRNA 表达水平低于 EC。然而,通过 RT-qPCR 评估时,并未观察到明显的降低。然而,VL 患者血浆中的可溶性 IL-7Rα(sIL-7Rα)水平低于 EC。此外,VL 患者血浆中的可溶性 IL-7 水平高于 EC。有趣的是,与 EC 相比,VL 患者的 CD4+T 细胞上表达的 IL-7Rα 蛋白更高,激活的 CD38+CD4+T 细胞与 VL 患者的 CD38-CD4+T 细胞相比,IL-7Rα 的表面表达更高。与 EC 相比,VL 患者的 CD4+T 细胞具有更高的基线信号潜能,并且在用重组人 IL-7(rhIL-7)刺激后,通过磷酸化 STAT5(pSTAT5)来测量。有趣的是,在 VL 患者的 CD4+T 细胞中,经过 IL-7 刺激后,CD38 阴性细胞具有最高水平的 pSTAT5。因此,尽管 VL 患者的 CD4+T 细胞中 IL7RA mRNA 的表达不变或可能降低,但与 EC 相比,IL-7Rα 的表面表达更高,并且在暴露于 rhIL-7 后观察到增加的 pSTAT5。因此,IL-7 信号似乎在 VL CD4+T 细胞中是功能性的,甚至增强,并且不能解释 VL CD4+T 细胞的效应功能受损。增强的血浆 IL-7 可能是调节 CD4+T 细胞中 IL7RA 表达的体内平衡反馈机制的一部分。
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