A genetic disorder reveals a hematopoietic stem cell regulatory network co-opted in leukemia

Author:

Voit Richard A.ORCID,Tao Liming,Yu FulongORCID,Cato Liam D.,Cohen Blake,Fleming Travis J.,Antoszewski MateuszORCID,Liao Xiaotian,Fiorini Claudia,Nandakumar Satish K.,Wahlster Lara,Teichert Kristian,Regev Aviv,Sankaran Vijay G.ORCID

Abstract

AbstractThe molecular regulation of human hematopoietic stem cell (HSC) maintenance is therapeutically important, but limitations in experimental systems and interspecies variation have constrained our knowledge of this process. Here, we have studied a rare genetic disorder due to MECOM haploinsufficiency, characterized by an early-onset absence of HSCs in vivo. By generating a faithful model of this disorder in primary human HSCs and coupling functional studies with integrative single-cell genomic analyses, we uncover a key transcriptional network involving hundreds of genes that is required for HSC maintenance. Through our analyses, we nominate cooperating transcriptional regulators and identify how MECOM prevents the CTCF-dependent genome reorganization that occurs as HSCs differentiate. We show that this transcriptional network is co-opted in high-risk leukemias, thereby enabling these cancers to acquire stem cell properties. Collectively, we illuminate a regulatory network necessary for HSC self-renewal through the study of a rare experiment of nature.

Funder

U.S. Department of Health & Human Services | National Institutes of Health

New York Stem Cell Foundation

Edward P. Evans Foundation

Klarman Family Foundation

Howard Hughes Medical Institute

Publisher

Springer Science and Business Media LLC

Subject

Immunology,Immunology and Allergy

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