Gene/Protein
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Target Concepts:
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Query: UMLS:C0476089 (
endometrial cancer
)
11,379
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Although
endometrial cancer
is the most common cancer of the female reproductive tract, we have little understanding of what controls
endometrial cancer
beyond the transcriptional effects of steroid hormones such as estrogen. As a result, we have limited therapeutic options for the ~62,000 women diagnosed with
endometrial cancer
each year in the United States. Here, in an attempt to identify new prognostic and therapeutic targets, we focused on a new area for this cancer-alternative mRNA splicing-and investigated whether splicing factor, SF3B1, plays an important role in
endometrial cancer
pathogenesis. Using a tissue microarray, we found that human endometrial tumors expressed more SF3B1 protein than non-cancerous tissues. Furthermore, SF3B1 knockdown reduced in vitro proliferation, migration, and invasion of the
endometrial cancer
cell lines Ishikawa and AN3CA. Similarly, the SF3B1 inhibitor, Pladienolide-B (PLAD-B), reduced the Ishikawa and AN3CA cell proliferation and invasion in vitro. Moreover, PLAD-B reduced tumor growth in an orthotopic
endometrial cancer
mouse model. Using RNA-Seq approach, we identified ~2000 differentially expressed genes (DEGs) with SF3B1 knockdown in
endometrial cancer
cells. Additionally, alternative splicing (AS) events analysis revealed that SF3B1 depletion led to alteration in multiple categories of AS events including alternative exon skipping (ES), transcript start site usage (TSS), and transcript termination site (TTS) usage. Subsequently, bioinformatics analysis showed
KSR2
as a potential candidate for SF3B1-mediated functions in
endometrial cancer
. Specifically, loss of SF3B1 led to decrease in
KSR2
expression, owing to reduced maturation of
KSR2
pre-mRNA to a mature RNA. Importantly, we found rescuing the
KSR2
expression with SF3B1 knockdown partially restored the cell growth of
endometrial cancer
cells. Taken together, our data suggest that SF3B1 plays a crucial oncogenic role in the tumorigenesis of
endometrial cancer
and hence may support the development of SF3B1 inhibitors to treat this disease.
...
PMID:Splicing factor SF3B1 promotes endometrial cancer progression via regulating KSR2 RNA maturation. 3304 78
