| Literature DB >> 31956895 |
Linde De Troyer1,2, Peihua Zhao1,2, Tibor Pastor1,2, Maria Francesca Baietti1,2, Jasmine Barra1,2, Roberto Vendramin1,2, Ruveyda Dok2, Benoit Lechat1,2, Paul Najm1,2, Delphi Van Haver3,4,5, Francis Impens3,4,5, Eleonora Leucci2, Anna A Sablina1,2.
Abstract
Dysregulated splicing is a common event in cancer even in the absence of mutations in the core splicing machinery. The aberrant long non-coding transcriptome constitutes an uncharacterized level of regulation of post-transcriptional events in cancer. Here, we found that the stress-induced long non-coding RNA (lncRNA), LINC02657 or LASTR (lncRNA associated with SART3 regulation of splicing), is upregulated in hypoxic breast cancer and is essential for the growth of LASTR-positive triple-negative breast tumors. LASTR is upregulated in several types of epithelial cancers due to the activation of the stress-induced JNK/c-JUN pathway. Using a mass-spectrometry based approach, we identified the RNA-splicing factor SART3 as a LASTR-interacting partner. We found that LASTR promotes splicing efficiency by controlling SART3 association with the U4 and U6 small nuclear ribonucleoproteins (snRNP) during spliceosome recycling. Intron retention induced by LASTR depletion downregulates expression of essential genes, ultimately decreasing the fitness of cancer cells.Entities:
Year: 2020 PMID: 31956895 DOI: 10.1093/nar/gkz1237
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971