1. LncRNA-OIS1 regulates DPP4 activation to modulate senescence induced by RAS
- Author
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Ran Elkon, Eric Pintó Barberà, Dannys Jorge Martínez-Herrera, Reuven Agami, Maite Huarte, Alejandro Pineiro Ugalde, Ruiqi Han, Naama Messika-Gold, Li Li, Rui Lopes, Pieter C van Breugel, Gozde Korkmaz, Elzo de Wit, Jarno Drost, Ricardo J Soares, Hans Teunissen, Annita Louloupi, Boye Schnack Nielsen, Kim Holmstrøm, Fabricio Loayza-Puch, and Molecular Genetics
- Subjects
0301 basic medicine ,Senescence ,Dipeptidyl Peptidase 4 ,Gene Expression ,Biology ,medicine.disease_cause ,03 medical and health sciences ,RNA interference ,Neoplasms ,Gene expression ,Genetics ,medicine ,RNA and RNA-protein complexes ,Gene silencing ,Humans ,Cellular Senescence ,Gene knockdown ,Genome ,Oncogene ,Cell biology ,030104 developmental biology ,Genes, ras ,HEK293 Cells ,Ectopic expression ,RNA, Long Noncoding ,Carcinogenesis - Abstract
Oncogene-induced senescence (OIS), provoked in response to oncogenic activation, is considered an important tumor suppressor mechanism. Long non-coding RNAs (lncRNAs) are transcripts longer than 200 nt without a protein-coding capacity. Functional studies showed that deregulated lncRNA expression promote tumorigenesis and metastasis and that lncRNAs may exhibit tumor-suppressive and oncogenic function. Here, we first identified lncRNAs that were differentially expressed between senescent and non-senescent human fibroblast cells. Using RNA interference, we performed a loss-function screen targeting the differentially expressed lncRNAs, and identified lncRNA-OIS1 (lncRNA#32, AC008063.3 or ENSG00000233397) as a lncRNA required for OIS. Knockdown of lncRNA-OIS1 triggered bypass of senescence, higher proliferation rate, lower abundance of the cell-cycle inhibitor CDKN1A and high expression of cell-cycle-associated genes. Subcellular inspection of lncRNA-OIS1 indicated nuclear and cytosolic localization in both normal culture conditions as well as following oncogene induction. Interestingly, silencing lncRNA-OIS1 diminished the senescent-associated induction of a nearby gene (Dipeptidyl Peptidase 4, DPP4) with established role in tumor suppression. Intriguingly, similar to lncRNA-OIS1, silencing DPP4 caused senescence bypass, and ectopic expression of DPP4 in lncRNA-OIS1 knockdown cells restored the senescent phenotype. Thus, our data indicate that lncRNA-OIS1 links oncogenic induction and senescence with the activation of the tumor suppressor DPP4.
- Published
- 2017