IL-2 and TCR stimulation induce expression and secretion of IL-32β by human T cells

IL-2 和 TCR 刺激诱导人 T 细胞表达和分泌 IL-32β

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作者:Franziska Christine Sanna,Iva Benešová,Philip Pervan,Adriana Krenz,Alexander Wurzel,Robert Lohmayer,Jasmin Mühlbauer,Amélie Wöllner,Nina Köhl,Ayse Nur Menevse,Slava Stamova,Valentina Volpin,Philipp Beckhove,Maria Xydia

Abstract

IL-32 expression is important for pathogen clearance but detrimental in chronic inflammation, autoimmunity, and cancer. T cells are major IL-32 producers in these diseases and key mediators of pathogen and tumor elimination but also autoimmune destruction. However, their contribution to IL-32 biology during immune responses is hardly understood due to several isoforms with divergent inflammatory properties. Here, we identified IL-32β as the predominant isoform in various T cell subsets of healthy individuals and breast cancer patients with the highest levels detected in intratumoral regulatory T cells. We show that IL-32β is induced by IL-2 but IL-32β release requires T Cell Receptor rather than IL2R stimulation. Using inhibitors of protein secretion pathways and serial (ultra)centrifugation of T cell supernatants, we demonstrate that T cells actively secrete IL-32β unconventionally, as a free protein and, to a minor degree, through exosomes. Thus, our data identify activated T cells as major IL-32β secretors in health and cancer.

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