Activated oncogenes restrict cell proliferation and transformation by triggering a DNA damage-dependent senescence checkpoint in response to DNA hyper-replication. Here, we show that loss of the p16(INK) (4a) cyclin-dependent kinase inhibitor and melanoma tumour suppressor facilitates a DNA damage response after a hyper-replicative phase in human melanocytes. Unlike cells expressing activated oncogenes, however, melanocytes depleted for p16(INK) (4a) display enhanced proliferation and an extended replicative lifespan in the presence of replication-associated DNA damage. Analysis of human benign naevi confirmed that DNA damage and loss of p16(INK) (4a) expression co-segregate closely. Thus, we propose that loss of p16(INK) (4a) facilitates tumourigenesis by promoting the proliferation of genetically unstable cells.
Otávia L. Caballero, Daniel Cohen, Qing Liu, Manel Esteller, Julie Bonacum, Peter White, James Engles, Robert Yochem, James G. Herman, William H. Westra, Christoph Lengauer, David Sidransky, Jin Jen
Andrea Piunti, Alessandra Rossi, Aurora Cerutti, Mareike Albert, Sriganesh Jammula, Andrea Scelfo, Laura Cedrone, Giulia Fragola, Linda Olsson, Haruhiko Koseki, Giuseppe Testa, Stefano Casola, Kristian Helin, Fabrizio d’Adda di Fagagna, Diego Pasini
Camilla Cristalli, Maria Cristina Manara, Sérgio Valente, Evelin Pellegrini, Alberto Bavelloni, Alessandra De Feo, William L. Blalock, Elisabetta Di Bello, David Piñeyro, Angelika Merkel, Manel Esteller, Òscar M. Tirado, Antonello Mai, Katia Scotlandi
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