SRSF2 regulates alternative splicing to drive hepatocellular carcinoma development

C Luo, Y Cheng, Y Liu, L Chen, L Liu, N Wei, Z Xie… - Cancer research, 2017 - AACR
C Luo, Y Cheng, Y Liu, L Chen, L Liu, N Wei, Z Xie, W Wu, Y Feng
Cancer research, 2017AACR
Aberrant RNA splicing is recognized to contribute to cancer pathogenesis, but the
underlying mechanisms remain mainly obscure. Here, we report that the splicing factor
SRSF2 is upregulated frequently in human hepatocellular carcinoma (HCC), where this
event is associated with poor prognosis in patients. RNA-seq and other molecular analyses
were used to identify SRSF2-regulated alternative splicing events. SRSF2 binding within an
alternative exon was associated with its inclusion in the RNA, whereas SRSF2 binding in a …
Abstract
Aberrant RNA splicing is recognized to contribute to cancer pathogenesis, but the underlying mechanisms remain mainly obscure. Here, we report that the splicing factor SRSF2 is upregulated frequently in human hepatocellular carcinoma (HCC), where this event is associated with poor prognosis in patients. RNA-seq and other molecular analyses were used to identify SRSF2-regulated alternative splicing events. SRSF2 binding within an alternative exon was associated with its inclusion in the RNA, whereas SRSF2 binding in a flanking constitutive exon was associated with exclusion of the alternative exon. Notably, cancer-associated splice variants upregulated by SRSF2 in clinical specimens of HCC were found to be crucial for pathogenesis and progression in hepatoma cells, where SRSF2 expression increased cell proliferation and tumorigenic potential by controlling expression of these variants. Our findings identify SRSF2 as a key regulator of RNA splicing dysregulation in cancer, with possible clinical implications as a candidate prognostic factor in patients with HCC. Cancer Res; 77(5); 1168–78. ©2017 AACR.
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