Conversion of adult endothelium to immunocompetent haematopoietic stem cells

被引:0
|
作者
Raphael Lis
Charles C. Karrasch
Michael G. Poulos
Balvir Kunar
David Redmond
Jose G. Barcia Duran
Chaitanya R. Badwe
William Schachterle
Michael Ginsberg
Jenny Xiang
Arash Rafii Tabrizi
Koji Shido
Zev Rosenwaks
Olivier Elemento
Nancy A. Speck
Jason M. Butler
Joseph M. Scandura
Shahin Rafii
机构
[1] Ansary Stem Cell Institute,Division of Regenerative Medicine, Department of Medicine
[2] Weill Cornell Medicine,Department of Surgery, Department of Medicine
[3] Ronald O. Perelman and Claudia Cohen Center for Reproductive Medicine and Infertility,Department of Obstetrics and Gynecology
[4] Weill Cornell Medicine,Institute for Regenerative Medicine and Department of Cell and Developmental Biology
[5] Weill Cornell Medicine,Department of Medicine
[6] Institute for Computational Biomedicine & Institute for Precision Medicine,undefined
[7] Weill Cornell Medicine,undefined
[8] Angiocrine Bioscience,undefined
[9] Genomics Resources Core Facility,undefined
[10] Weill Cornell Medicine,undefined
[11] Stem Cell and Microenvironment Laboratory,undefined
[12] Weill Cornell Medicine in Qatar,undefined
[13] Education City,undefined
[14] Qatar Foundation,undefined
[15] Abramson Family Cancer Research Institute,undefined
[16] University of Pennsylvania,undefined
[17] Hematology-Oncology,undefined
[18] Weill Cornell Medicine and the New York Presbyterian Hospital,undefined
来源
Nature | 2017年 / 545卷
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摘要
Developmental pathways that orchestrate the fleeting transition of endothelial cells into haematopoietic stem cells remain undefined. Here we demonstrate a tractable approach for fully reprogramming adult mouse endothelial cells to haematopoietic stem cells (rEC-HSCs) through transient expression of the transcription-factor-encoding genes Fosb, Gfi1, Runx1, and Spi1 (collectively denoted hereafter as FGRS) and vascular-niche-derived angiocrine factors. The induction phase (days 0–8) of conversion is initiated by expression of FGRS in mature endothelial cells, which results in endogenous Runx1 expression. During the specification phase (days 8–20), RUNX1+ FGRS-transduced endothelial cells commit to a haematopoietic fate, yielding rEC-HSCs that no longer require FGRS expression. The vascular niche drives a robust self-renewal and expansion phase of rEC-HSCs (days 20–28). rEC-HSCs have a transcriptome and long-term self-renewal capacity similar to those of adult haematopoietic stem cells, and can be used for clonal engraftment and serial primary and secondary multi-lineage reconstitution, including antigen-dependent adaptive immune function. Inhibition of TGFβ and CXCR7 or activation of BMP and CXCR4 signalling enhanced generation of rEC-HSCs. Pluripotency-independent conversion of endothelial cells into autologous authentic engraftable haematopoietic stem cells could aid treatment of haematological disorders.
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页码:439 / 445
页数:6
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