Lysine-specific demethylase 1 regulates hematopoietic stem cell expansion and myeloid cell differentiation.

赖氨酸特异性去甲基化酶 1 调节造血干细胞扩增和髓系细胞分化

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作者:Staehle Hans Felix, Koellerer Christoph, Staehle Anne Marie, Schulze Jana, Eble Philipp, Müller Anja, Zell Franziska, Müller Judith M, Perner Florian, Attia Aya, Mallm Jan-Philipp, Pozdnyakova Olga, Rippe Karsten, Brors Benedikt, Feuerbach Lars, Imbusch Charles D, Metzger Eric, Schüle Roland, Pahl Heike L, Jutzi Jonas S
The lysine-specific demethylase 1 (LSD1) regulates hematopoietic stem cell differentiation and has been identified as a therapeutic target in hematological disorders. LSD1 demethylates mono and dimethylated histones 3 at lysine 4 and 9. In addition, it acts as a scaffold for the formation of chromatin-modifying complexes that regulates the transcription of myeloid-lineage-specific genes in complex with GFI1, a transcriptional repressor. While both enzymatic and non-enzymatic functions of LSD1 have been well defined, the relative importance of these two functions in hematopoiesis remains incompletely understood. Here, we investigated the contribution of enzymatic and non-enzymatic functions of LSD1 to myelopoiesis. We show that myeloid differentiation is independent of the enzymatic functions of LSD1 but requires the non-enzymatic, scaffolding function, which directs GFI1 binding to target sequences. In the absence of the LSD1 protein, GFI1 DNA binding is diminished, and myeloid cell differentiation arrests at an immature, myelomonocytic-like cell stage, which overexpresses Prtn3. We provide functional data implicating Prtn3 as an effector of the stem cell expansion and myeloid maturation block caused by the loss of LSD1.

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