Alternatively spliced CSF3R isoforms in SRSF2 P95H mutated myeloid neoplasms

小基因 选择性拼接 RNA剪接 外显子 生物 髓样 癌症研究 祖细胞 基因亚型 外显子剪接增强剂 遗传学 分子生物学 基因 干细胞 核糖核酸
作者
Borwyn A. Wang,Hrishikesh Mehta,Srinivasa R. Penumutchu,Blanton S. Tolbert,Chonghui Cheng,Marek Kimmel,Torsten Haferlach,Jaroslaw P. Maciejewski,Seth J. Corey
出处
期刊:Leukemia [Springer Nature]
卷期号:36 (10): 2499-2508 被引量:4
标识
DOI:10.1038/s41375-022-01672-4
摘要

Alternatively spliced colony stimulating factor 3 receptor (CSF3R) isoforms Class III and Class IV are observed in myelodysplastic syndromes (MDS), but their roles in disease remain unclear. We report that the MDS-associated splicing factor SRSF2 affects the expression of Class III and Class IV isoforms and perturbs granulopoiesis. Add-back of the Class IV isoform in Csf3r-null mouse progenitor cells increased granulocyte progenitors with impaired neutrophil differentiation, while add-back of the Class III produced dysmorphic neutrophils in fewer numbers. These CSF3R isoforms were elevated in patients with myeloid neoplasms harboring SRSF2 mutations. Using in vitro splicing assays, we confirmed increased Class III and Class IV transcripts when SRSF2 P95 mutations were co-expressed with the CSF3R minigene in K562 cells. Since SRSF2 regulates splicing partly by recognizing exonic splicing enhancer (ESE) sequences on pre-mRNA, deletion of either ESE motifs within CSF3R exon 17 decreased Class IV transcript levels without affecting Class III. CD34+ cells expressing SRSF2 P95H showed impaired neutrophil differentiation in response to G-CSF and was accompanied by increased levels of Class IV. Our findings suggest that SRSF2 P95H promotes Class IV splicing by binding to key ESE sequences in CSF3R exon 17, and that SRSF2, when mutated, contributes to dysgranulopoiesis.
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