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  • JARID1B expression and its function in DNA damage repair are tightly regulated by miRNAs in breast cancer.

JARID1B expression and its function in DNA damage repair are tightly regulated by miRNAs in breast cancer.

Cancer science (2018-12-28)
Ivano Mocavini, Simone Pippa, Valerio Licursi, Paola Paci, Daniela Trisciuoglio, Cecilia Mannironi, Carlo Presutti, Rodolfo Negri
ABSTRACT

JARID1B/KDM5B histone demethylase's mRNA is markedly overexpressed in breast cancer tissues and cell lines and the protein has been shown to have a prominent role in cancer cell proliferation and DNA repair. However, the mechanism of its post-transcriptional regulation in cancer cells remains elusive. We performed a computational analysis of transcriptomic data from a set of 103 breast cancer patients, which, along with JARID1B upregulation, showed a strong downregulation of 2 microRNAs (miRNAs), mir-381 and mir-486, potentially targeting its mRNA. We showed that both miRNAs can target JARID1B 3'UTR and reduce luciferase's activity in a complementarity-driven repression assay. Moreover, MCF7 breast cancer cells overexpressing JARID1B showed a strong protein reduction when transfected with mir-486. This protein's decrease is accompanied by accumulation of DNA damage, enhanced radiosensitivity and increase of BRCA1 mRNA, 3 features previously correlated with JARID1B silencing. These results enlighten an important role of a miRNA's circuit in regulating JARID1B's activity and suggest new perspectives for epigenetic therapies.

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Anti-Actin antibody produced in rabbit, affinity isolated antibody, buffered aqueous solution