| Literature DB >> 33890574 |
Carter J Barger1, Linda Chee2, Mustafa Albahrani2, Catalina Munoz-Trujillo2, Lidia Boghean2, Connor Branick2, Kunle Odunsi3, Ronny Drapkin4, Lee Zou5, Adam R Karpf6.
Abstract
The ass="Gene">FOXM1 transcription factor is an oncoprotein and a top biomarker of poor prognosis in <ass="Chemical">span class="Species">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 (RS) 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 (HR), and poly-ADP ribosylase (PARP) 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.Entities:
Keywords: cancer biology; chromosomes; gene expression; human
Year: 2021 PMID: 33890574 DOI: 10.7554/eLife.55070
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140