The distinct biological implications of Asxl1 mutation and its roles in leukemogenesis revealed by a knock-in mouse model

Springer Science and Business Media LLC - Tập 10 - Trang 1-15 - 2017
Yueh-Chwen Hsu1, Yu-Chiao Chiu2, Chien-Chin Lin1,3, Yuan-Yeh Kuo4, Hsin-An Hou5, Yi-Shiuan Tzeng4, Chein-Jun Kao3, Po-Han Chuang3, Mei-Hsuan Tseng5, Tzu-Hung Hsiao2, Wen-Chien Chou1,3,5, Hwei-Fang Tien5
1Graduate Institute of Clinical Medicine, National Taiwan University, Taipei, Taiwan
2Department of Medical Research, Taichung Veterans General Hospital, Taichung, Taiwan
3Department of Laboratory Medicine, National Taiwan University Hospital, Taipei, Taiwan
4Graduate Institute of Oncology, College of Medicine, National Taiwan University, Taipei, Taiwan
5Division of Hematology, Department of Internal Medicine, National Taiwan University Hospital, Taipei, Taiwan

Tóm tắt

Additional sex combs-like 1 (ASXL1) is frequently mutated in myeloid malignancies. Recent studies showed that hematopoietic-specific deletion of Asxl1 or overexpression of mutant ASXL1 resulted in myelodysplasia-like disease in mice. However, actual effects of a “physiological” dose of mutant ASXL1 remain unexplored. We established a knock-in mouse model bearing the most frequent Asxl1 mutation and studied its pathophysiological effects on mouse hematopoietic system. Heterozygotes (Asxl1 tm/+ ) marrow cells had higher in vitro proliferation capacities as shown by more colonies in cobblestone-area forming assays and by serial re-plating assays. On the other hand, donor hematopoietic cells from Asxl1 tm/+ mice declined faster in recipients during transplantation assays, suggesting compromised long-term in vivo repopulation abilities. There were no obvious blood diseases in mutant mice throughout their life-span, indicating Asxl1 mutation alone was not sufficient for leukemogenesis. However, this mutation facilitated engraftment of bone marrow cell overexpressing MN1. Analyses of global gene expression profiles of ASXL1-mutated versus wild-type human leukemia cells as well as heterozygote versus wild-type mouse marrow precursor cells, with or without MN1 overexpression, highlighted the association of in vivo Asxl1 mutation to the expression of hypoxia, multipotent progenitors, hematopoietic stem cells, KRAS, and MEK gene sets. ChIP-Seq analysis revealed global patterns of Asxl1 mutation-modulated H3K27 tri-methylation in hematopoietic precursors. We proposed the first Asxl1 mutation knock-in mouse model and showed mutated Asxl1 lowered the threshold of MN1-driven engraftment and exhibited distinct biological functions on physiological and malignant hematopoiesis, although it was insufficient to lead to blood malignancies.

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