Single-Cell RNA-Seq Mapping of Human Thymopoiesis Reveals Lineage Specification Trajectories and a Commitment Spectrum in T Cell Development

人类胸腺造血的单细胞RNA测序图谱揭示了T细胞发育过程中的谱系分化轨迹和定向分化谱

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作者:Justin Le ,Jeong Eun Park ,Vi Luan Ha ,Annie Luong ,Sergio Branciamore ,Andrei S Rodin ,Grigoriy Gogoshin ,Fan Li ,Yong-Hwee Eddie Loh ,Virginia Camacho ,Sweta B Patel ,Robert S Welner ,Chintan Parekh

Abstract

The challenges in recapitulating in vivo human T cell development in laboratory models have posed a barrier to understanding human thymopoiesis. Here, we used single-cell RNA sequencing (sRNA-seq) to interrogate the rare CD34+ progenitor and the more differentiated CD34- fractions in the human postnatal thymus. CD34+ thymic progenitors were comprised of a spectrum of specification and commitment states characterized by multilineage priming followed by gradual T cell commitment. The earliest progenitors in the differentiation trajectory were CD7- and expressed a stem-cell-like transcriptional profile, but had also initiated T cell priming. Clustering analysis identified a CD34+ subpopulation primed for the plasmacytoid dendritic lineage, suggesting an intrathymic dendritic specification pathway. CD2 expression defined T cell commitment stages where loss of B cell potential preceded that of myeloid potential. These datasets delineate gene expression profiles spanning key differentiation events in human thymopoiesis and provide a resource for the further study of human T cell development.

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