In Vivo DNA Re-replication Elicits Lethal Tissue Dysplasias

• Main Authors: Sergio Muñoz, Sabela Búa, Sara Rodríguez-Acebes, Diego Megías, Sagrario Ortega, Alba de Martino, Juan Méndez
• Format: Article
• Language: English
• Published: Elsevier 2017-05-01
• Series: Cell Reports
• Online Access: http://www.sciencedirect.com/science/article/pii/S2211124717305260

Summary: Mammalian DNA replication origins are “licensed” by the loading of DNA helicases, a reaction that is mediated by CDC6 and CDT1 proteins. After initiation of DNA synthesis, CDC6 and CDT1 are inhibited to prevent origin reactivation and DNA overreplication before cell division. CDC6 and CDT1 are highly expressed in many types of cancer cells, but the impact of their deregulated expression had not been investigated in vivo. Here, we have generated mice strains that allow the conditional overexpression of both proteins. Adult mice were unharmed by the individual overexpression of either CDC6 or CDT1, but their combined deregulation led to DNA re-replication in progenitor cells and lethal tissue dysplasias. This study offers mechanistic insights into the necessary cooperation between CDC6 and CDT1 for facilitation of origin reactivation and describes the physiological consequences of DNA overreplication. : Muñoz et al. investigate the effects of deregulated DNA replication in vivo. The combined overexpression of CDC6 and CDT1, two key proteins that activate replication origins, resulted in aberrant origin reactivation, DNA overreplication, and lethal dysplasia in the intestine and other tissues. Keywords: CDC6, CDT1, DNA replication, replication origin, tissue dysplasia