Novel Splice-switching Oligonucleotide Promotes BRCA1 Aberrant Splicing and Susceptibility to PARP Inhibitor Action

Overview

Journal Int J Cancer

Specialty Oncology

Date 2016 Dec 21

PMID 27997688

Citations 12

Authors

Lindsay D Smith

Flavia Leme de Calais

Michela Raponi

Massimiliano Mellone

Emanuele Buratti

Jeremy P Blaydes

Diana Baralle

Affiliations

Soon will be listed here.

Abstract

Tumors carrying hereditary mutations in BRCA1, which attenuate the BRCA1 DNA damage repair pathway, are more susceptible to dual treatment with PARP inhibitors and DNA damaging therapeutics. Conversely, breast cancer tumors with nonmutated functional BRCA1 are less sensitive to PARP inhibition. We describe a method that triggers susceptibility to PARP inhibition in BRCA1-functional tumor cells. BRCA1 exon 11 is a key for the function of BRCA1 in DNA damage repair. Analysis of the BRCA1 exon 11 splicing mechanism identified a key region within this exon which, when deleted, induced exon 11 skipping. An RNA splice-switching oligonucleotide (SSO) developed to target this region was shown to artificially stimulate skipping of exon 11 in endogenous BRCA1 pre-mRNA. SSO transfection rendered wild-type BRCA1 expressing cell lines more susceptible to PARP inhibitor treatment, as demonstrated by a reduction in cell survival at all SSO concentrations tested. Combined SSO and PARP inhibitor treatment increased γH2AX expression indicating that SSO-dependent skipping of BRCA1 exon 11 was able to promote DSBs and therefore synthetic lethality. In conclusion, this SSO provides a new potential therapeutic strategy for targeting BRCA1-functional breast cancer by enhancing the effect of PARP inhibitors.

Citing Articles

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Impacts and mechanisms of alternative mRNA splicing in cancer metabolism, immune response, and therapeutics.

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Zhao J, Chang L, Gu X, Liu J, Sun B, Wei X Cancer Sci. 2020; 111(8):3020-3031.

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