Cell cycle inhibitor, p19INK4d, promotes cell survival and decreases chromosomal aberrations after genotoxic insult due to enhanced DNA repair

MARÍA E. SCASSA; MARIELA C. MARAZITA; JULIETA M. CERUTI; ABEL L. CARCAGNO; PABLO F. SIRKIN; MARCELA GONZÁLEZ-CID; OMAR P. PIGNATARO; EDUARDO T. CÁNEPA

MUTATION RESEARCH-DNA REPAIR

ELSEVIER

Lugar: Amsterdam, The Netherlands; Año: 2006

0921-8777

Genome integrity and cell proliferation and survival are regulated by an intricate network of pathways that includes cell cycle checkpoints, DNA repair and recombination, and programmed cell death. It makes sense that there should be a coordinated regulation of these different processes, but the components of such mechanisms remain unknown. In this report, we demonstrate that p19INK4d expression enhances cell survival under genotoxic conditions. By using p19INK4d -proficient clones, we demonstrated that p19INK4d expression correlates with the cellular resistance to UV treatment with increased DNA repair activity against UV-induced lesions. On the contrary, p19INK4d -deficient cells show reduced ability to repair DNA damage and increased sensitivity to genotoxic insult when compared with their p19INK4d -proficient counterparts. Consistent with these findings, our studies also show that p19INK4d overexpressing cells present not only a minor accumulation of UV-induced chromosomal aberrations but a lower frequency of spontaneous chromosome abnormalities than p19INK4d -deficient cells. Lastly, we suggest that p19INK4d effects are dissociated from its role as CDK4/6 inhibitor. The results presented herein support a crucial role for p19INK4d in regulating genomic stability and overall cell viability under conditions of genotoxic stress. We propose that p19INK4d would belong to a protein network that would integrate DNA repair, apoptotic and checkpoint mechanisms in order to maintain the genomic integrity.