Cell Type-Specific Regulation by a Heptad of Transcription Factors in Human Hematopoietic Stem and Progenitor Cells

Author:

Subramanian ShruthiORCID,Thoms Julie A.I.ORCID,Huang YizhouORCID,Cornejo Paola,Koch Forrest C.,Jacquelin Sebastien,Shen Sylvie,Song Emma,Joshi Swapna,Brownlee Chris,Woll Petter S.,Fajardo Diego ChaconORCID,Beck Dominik,Curtis David J.,Yehson Kenneth,Antonenas Vicki,Brien Tracey O’,Trickett Annette,Powell Jason A.,Lewis Ian D.,Pitson Stuart M.,Gandhi Maher K.,Lane Steven W.,Vafaee Fatemeh,Wong Emily S.,Göttgens BertholdORCID,Rokny Hamid Alinejad,Wong Jason W.HORCID,Pimanda John E.ORCID

Abstract

SummaryHematopoietic stem and progenitor cells (HSPCs) rely on a complex interplay of transcription factors (TFs) to regulate differentiation into mature blood cells. A heptad of TFs - FLI1, ERG, GATA2, RUNX1, TAL1, LYL1, LMO2 - bind regulatory elements in bulk CD34+ HSPCs. However, whether specific heptad-TF combinations have distinct roles in regulating hematopoietic differentiation remained unknown. We mapped genome-wide chromatin contacts and TF binding profiles in HSPC subsets (HSC, CMP, GMP, MEP) and found that heptad occupancy and enhancer-promoter interactions varied significantly across cell types and were associated with cell-type-specific gene expression. Distinct regulatory elements were enriched with specific heptad-TF combinations, including stem-cell-specific elements with ERG, and myeloid- and erythroid-specific elements with combinations of FLI1, RUNX1, GATA2, TAL1, LYL1, and LMO2. These findings suggest that specific heptad-TF combinations play critical roles in regulating hematopoietic differentiation and provide a valuable resource for development of targeted therapies to manipulate specific HSPC subsets.

Publisher

Cold Spring Harbor Laboratory

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