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Single-cell RNA sequencing identifies shared differentiation paths of mouse thymic innate T cells.

Minji LeeEunmin LeeSeong Kyu HanYoon Ha ChoiDong-Il KwonHyobeen ChoiKwanghwan LeeEun Seo ParkMin-Seok RhaDong Jin JooEui-Cheol ShinSanguk KimJong Kyoung KimYou Jeong Lee
Published in: Nature communications (2020)
Invariant natural killer T (iNKT), mucosal-associated invariant T (MAIT), and γδ T cells are innate T cells that acquire memory phenotype in the thymus and share similar biological characteristics. However, how their effector differentiation is developmentally regulated is still unclear. Here, we identify analogous effector subsets of these three innate T cell types in the thymus that share transcriptional profiles. Using single-cell RNA sequencing, we show that iNKT, MAIT and γδ T cells mature via shared, branched differentiation rather than linear maturation or TCR-mediated instruction. Simultaneous TCR clonotyping analysis reveals that thymic maturation of all three types is accompanied by clonal selection and expansion. Analyses of mice deficient of TBET, GATA3 or RORγt and additional in vivo experiments corroborate the predicted differentiation paths, while human innate T cells from liver samples display similar features. Collectively, our data indicate that innate T cells share effector differentiation processes in the thymus.
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