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Co-regulation and function of FOXM1/RHNO1 bidirectional genes in cancer
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The FOXM1 transcription factor is an oncoprotein and a top biomarker of poor prognosis in human cancer. Overexpression and activation of FOXM1 is frequent in high-grade serous carcinoma (HGSC), the most common and lethal form of human ovarian cancer, and is linked to copy number gains at chromosome 12p13.33. We show that
FOXM1
is co-amplified and co-expressed with
RHNO1
, a gene involved in the ATR-Chk1 signaling pathway that functions in the DNA replication stress response. We demonstrate that
FOXM1
and
RHNO1
are head-to-head (i.e., bidirectional) genes (BDG) regulated by a bidirectional promoter (BDP) (named F/R-BDP). FOXM1 and RHNO1 each promote oncogenic phenotypes in HGSC cells, including clonogenic growth, DNA homologous recombination repair, and poly-ADP ribosylase inhibitor resistance. FOXM1 and RHNO1 are one of the first examples of oncogenic BDG, and therapeutic targeting of FOXM1/RHNO1 BDG is a potential therapeutic approach for ovarian and other cancers.
eLife Sciences Publications, Ltd
Title: Co-regulation and function of FOXM1/RHNO1 bidirectional genes in cancer
Description:
The FOXM1 transcription factor is an oncoprotein and a top biomarker of poor prognosis in human cancer.
Overexpression and activation of FOXM1 is frequent in high-grade serous carcinoma (HGSC), the most common and lethal form of human ovarian cancer, and is linked to copy number gains at chromosome 12p13.
33.
We show that
FOXM1
is co-amplified and co-expressed with
RHNO1
, a gene involved in the ATR-Chk1 signaling pathway that functions in the DNA replication stress response.
We demonstrate that
FOXM1
and
RHNO1
are head-to-head (i.
e.
, bidirectional) genes (BDG) regulated by a bidirectional promoter (BDP) (named F/R-BDP).
FOXM1 and RHNO1 each promote oncogenic phenotypes in HGSC cells, including clonogenic growth, DNA homologous recombination repair, and poly-ADP ribosylase inhibitor resistance.
FOXM1 and RHNO1 are one of the first examples of oncogenic BDG, and therapeutic targeting of FOXM1/RHNO1 BDG is a potential therapeutic approach for ovarian and other cancers.
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