| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2093311 | Stem Cell Reports | 2016 | 15 Pages |
•GATA-2 rescues +9.5−/− AGM hematopoietic activity•GATA-2 upregulates Gpr65, which encodes a negative regulator of hematopoiesis•GPR65 suppresses hematopoiesis by repressing Gata2 expression•GPR65 represses Gata2 expression by increasing H4K20me1, restricting Scl/TAL1 occupancy
SummaryHematopoietic stem cells (HSCs) originate from hemogenic endothelium within the aorta-gonad-mesonephros (AGM) region of the mammalian embryo. The relationship between genetic circuits controlling stem cell genesis and multi-potency is not understood. A Gata2 cis element (+9.5) enhances Gata2 expression in the AGM and induces the endothelial to HSC transition. We demonstrated that GATA-2 rescued hematopoiesis in +9.5−/− AGMs. As G-protein-coupled receptors (GPCRs) are the most common targets for FDA-approved drugs, we analyzed the GPCR gene ensemble to identify GATA-2-regulated GPCRs. Of the 20 GATA-2-activated GPCR genes, four were GATA-1-activated, and only Gpr65 expression resembled Gata2. Contrasting with the paradigm in which GATA-2-activated genes promote hematopoietic stem and progenitor cell genesis/function, our mouse and zebrafish studies indicated that GPR65 suppressed hematopoiesis. GPR65 established repressive chromatin at the +9.5 site, restricted occupancy by the activator Scl/TAL1, and repressed Gata2 transcription. Thus, a Gata2 cis element creates a GATA-2-GPCR circuit that limits positive regulators that promote hematopoiesis.
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