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Chemically-defined generation of human hemogenic endothelium and definitive hematopoietic progenitor cells
來源: | 作者:Yun Chang 1, Ramizah Syahirah 2, Stephanie N Oprescu 3, Xuepeng Wang 4, Juhyung Jung 1, Scott H Cooper 4, Sandra Torregrosa-Allen 5, Bennett D Elzey 6, Alan Y Hsu 7, Lauren N Randolph 8, Yufei Sun 9, Shihuan Kuang 3, Hal E Broxmeyer 4, Qing Deng 10, Xiaoj | 發(fā)布時間: 2022-05-31 | 220 次瀏覽 | 分享到:

Human hematopoietic stem cells (HSCs), which arise from aorta-gonad-mesonephros (AGM), are widely used to treat blood diseases and cancers. However, a technique for their robust generation in vitro is still missing. Here we show temporal manipulation of Wnt signaling is sufficient and essential to induce AGM-like hematopoiesis from human pluripotent stem cells. TGFβ inhibition at the stage of aorta-like SOX17+CD235a- hemogenic endothelium yielded AGM-like hematopoietic progenitors, which closely resembled primary cord blood HSCs at the transcriptional level and contained diverse lineage-primed progenitor populations via single cell RNA-sequencing analysis. Notably, the resulting definitive cells presented lymphoid and myeloid potential in vitro; and could home to a definitive hematopoietic site in zebrafish and rescue bloodless zebrafish after transplantation. Engraftment and multilineage repopulating activities were also observed in mouse recipients. Together, our work provided a chemically-defined and feeder-free culture platform for scalable generation of AGM-like hematopoietic progenitor cells, leading to enhanced production of functional blood and immune cells for various therapeutic applications.

Keywords: Chemically defined; Hematopoietic stem and progenitor cells; RNA sequencing; Stem cell differentiation; Transplantation; Wnt signaling.


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