Thymic iNKT single cell analyses unmask the common developmental program of mouse innate T cells

胸腺 iNKT 单细胞分析揭示了小鼠固有 T 细胞的共同发育程序

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作者:S Harsha Krovi ,Jingjing Zhang ,Mary Jessamine Michaels-Foster ,Tonya Brunetti ,Liyen Loh ,James Scott-Browne ,Laurent Gapin

Abstract

Most T lymphocytes leave the thymus as naïve cells with limited functionality. However, unique populations of innate-like T cells differentiate into functionally distinct effector subsets during their development in the thymus. Here, we profiled >10,000 differentiating thymic invariant natural killer T (iNKT) cells using single-cell RNA sequencing to produce a comprehensive transcriptional landscape that highlights their maturation, function, and fate decisions at homeostasis. Our results reveal transcriptional profiles that are broadly shared between iNKT and mucosal-associated invariant T (MAIT) cells, illustrating a common core developmental program. We further unmask a mutual requirement for Hivep3, a zinc finger transcription factor and adapter protein. Hivep3 is expressed in early precursors and regulates the post-selection proliferative burst, differentiation and functions of iNKT cells. Altogether, our results highlight the common requirements for the development of innate-like T cells with a focus on how Hivep3 impacts the maturation of these lymphocytes.

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