| Literature DB >> 30413363 |
Nicholas A Spidale1, Katelyn Sylvia1, Kavitha Narayan1, Bing Miu1, Michela Frascoli1, Heather J Melichar2, Wu Zhihao3, Jan Kisielow4, Amy Palin5, Thomas Serwold6, Paul Love5, Michihiro Kobayashi7, Momoko Yoshimoto7, Nitya Jain8, Joonsoo Kang9.
Abstract
Lineage-committed αβ and γδ T cells are thought to originate from common intrathymic multipotent progenitors following instructive T cell receptor (TCR) signals. A subset of lymph node and mucosal Vγ2+ γδ T cells is programmed intrathymically to produce IL-17 (Tγδ17 cells), however the role of the γδTCR in development of these cells remains controversial. Here we generated reporter mice for the Tγδ17 lineage-defining transcription factor SOX13 and identified fetal-origin, intrathymic Sox13+ progenitors. In organ culture developmental assays, Tγδ17 cells derived primarily from Sox13+ progenitors, and not from other known lymphoid progenitors. Single cell transcriptome assays of the progenitors found in TCR-deficient mice demonstrated that Tγδ17 lineage programming was independent of γδTCR. Instead, generation of the lineage committed progenitors and Tγδ17 cells was controlled by TCF1 and SOX13. Thus, T lymphocyte lineage fate can be prewired cell-intrinsically and is not necessarily specified by clonal antigen receptor signals.Entities:
Keywords: IL-17; SOX13; T cell receptor; T cells; development; thymus; transcription factor
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Year: 2018 PMID: 30413363 PMCID: PMC6249057 DOI: 10.1016/j.immuni.2018.09.010
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745