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


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.

SUBMITTER: Mocavini I 

PROVIDER: S-EPMC6447846 | biostudies-literature | 2019 Apr

REPOSITORIES: biostudies-literature

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

Mocavini Ivano I   Pippa Simone S   Licursi Valerio V   Paci Paola P   Trisciuoglio Daniela D   Mannironi Cecilia C   Presutti Carlo C   Negri Rodolfo R  

Cancer science 20190318 4


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)  ...[more]

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