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人 CD4+CD45RA+T 细胞体外激活后的行为:血管活性肠肽的调节作用。

Human CD4CD45RA T Cells Behavior after In Vitro Activation: Modulatory Role of Vasoactive Intestinal Peptide.

机构信息

Departamento de Biología Celular, Facultad de Biología y Facultad de Medicina, Universidad Complutense de Madrid, 28040 Madrid, Spain.

出版信息

Int J Mol Sci. 2022 Feb 20;23(4):2346. doi: 10.3390/ijms23042346.

DOI:10.3390/ijms23042346
PMID:35216459
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8878027/
Abstract

Naїve CD4 T cells, which suffer different polarizing signals during T cell receptor activation, are responsible for an adequate immune response. In this study, we aimed to evaluate the behavior of human CD4CD45RA T cells after in vitro activation by anti-CD3/CD28 bead stimulation for 14 days. We also wanted to check the role of the VIP system during this process. The metabolic biomarker Glut1 was increased, pointing to an increase in glucose requirement whereas Hif-1α expression was higher in resting than in activated cells. Expression of Th1 markers increased at the beginning of activation, whereas Th17-associated biomarkers augmented after that, showing a pathogenic Th17 profile with a possible plasticity to Th17/1. Foxp3 mRNA expression augmented from day 4, but no parallel increases were observed in IL-10, IL-2, or TGFβ mRNA expression, meaning that these potential differentiated Treg could not be functional. Both VIP receptors were located on the plasma membrane, and expression of VPAC receptor increased significantly with respect to the VPAC receptor from day 4 of CD4CD45RA T activation, pointing to a shift in VPAC receptors. VIP decreased IFNγ and IL-23R expression during the activation, suggesting a feasible modulation of Th17/1 plasticity and Th17 stabilization through both VPAC receptors. These novel results show that, without polarizing conditions, CD4CD45RA T cells differentiate mainly to a pathogenic Th17 subset and an unpaired Treg subset after several days of activation. Moreover, they confirm the important immunomodulatory role of VIP, also on naїve Th cells, stressing the importance of this neuropeptide on lymphocyte responses in different pathological or non-pathological situations.

摘要

幼稚 CD4 T 细胞在 T 细胞受体激活时受到不同的极化信号影响,负责产生适当的免疫反应。在这项研究中,我们旨在评估人类 CD4CD45RA T 细胞在体外经抗-CD3/CD28 珠刺激 14 天后的行为。我们还想检查 VIP 系统在此过程中的作用。代谢生物标志物 Glut1 增加,表明葡萄糖需求增加,而静息细胞中的 Hif-1α 表达高于激活细胞。Th1 标志物的表达在激活开始时增加,而 Th17 相关生物标志物在之后增加,显示出具有潜在可塑性的致病性 Th17 表型,可能向 Th17/1 转化。Foxp3 mRNA 的表达从第 4 天开始增加,但在 IL-10、IL-2 或 TGFβ mRNA 的表达中没有观察到平行增加,这意味着这些潜在分化的 Treg 可能没有功能。两种 VIP 受体都位于质膜上,并且从 CD4CD45RA T 激活的第 4 天起,VPAC 受体的表达显著增加,表明 VPAC 受体发生了转变。VIP 在激活过程中降低了 IFNγ 和 IL-23R 的表达,这表明通过两种 VPAC 受体对 Th17/1 可塑性和 Th17 稳定进行了可行的调节。这些新结果表明,在没有极化条件的情况下,CD4CD45RA T 细胞在激活数天后主要分化为致病性 Th17 亚群和未配对的 Treg 亚群。此外,它们证实了 VIP 的重要免疫调节作用,也作用于幼稚 Th 细胞,强调了这种神经肽在不同病理或非病理情况下淋巴细胞反应中的重要性。

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