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

AI Article Synopsis

  • Naïve CD4 T cells require different signals during activation to elicit a proper immune response, and this study focused on their behavior after stimulation for 14 days.
  • The findings revealed that activated CD4 T cells showed increased glucose needs and developed a pathogenic Th17 profile, indicating a potential flexibility towards a Th17/1 phenotype, while regulatory T cells did not appear functional.
  • The study also highlighted the role of the vasoactive intestinal peptide (VIP) system, which was found to modulate gene expressions related to Th17 stabilization and plasticity, underlining VIP's importance in T cell responses in various conditions.

Article 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.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8878027PMC
http://dx.doi.org/10.3390/ijms23042346DOI Listing

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