The hematopoietic homeostasis relies on the intricate regulation of hematopoietic stem cells during their proliferation and differentiation. Myeloid differentiation disorders can lead to chronic myeloid leukemia and acute myeloid leukemia. Previous studies have shown increased expression of MS4A3 in myeloid cells, suggesting that MS4A3 may play a critical role in hematopoietic myeloid differentiation. However, the underlying mechanism and its role in hematopoietic myeloid differentiation require further elucidation. In this study, using K562 cell lines with MS4A3 over-expression (oeMS4A3) and MS4A3 knockdown (shMS4A3), we demonstrated that the overexpression of MS4A3 resulted in an augmented skewing towards myeloid differentiation and cell cycle arrest at G0/G1. In addition, inhibition of ROS, TGF-β, and p38MAPK in oeMS4A3 K562 cells attenuated the skewing of myeloid differentiation. Furthermore, in vivo experiments revealed a slight myeloid differentiation suppression tendency in MS4A3 knockout mice. Taken together, we show that MS4A3 overexpression promote myeloid differentiation skewing through the activation of the ROS/p38MAPK/TGFβ pathway. This study underscored the role of MS4A3 in the hematopoietic myeloid differentiation.
Keywords: MS4A3; Myeloid skewing; ROS; TGF-β; p38MAPK.
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