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p53 polymorphism influences response in cancer chemotherapy via modulation of p73-dependent apoptosis
Authors:Bergamaschi Daniele  Gasco Milena  Hiller Louise  Sullivan Alexandra  Syed Nelofer  Trigiante Giuseppe  Yulug Isik  Merlano Marco  Numico Gianmauro  Comino Alberto  Attard Marlene  Reelfs Olivier  Gusterson Barry  Bell Alexandra K  Heath Victoria  Tavassoli Mahvash  Farrell Paul J  Smith Paul  Lu Xin  Crook Tim
Affiliation:Ludwig Institute for Cancer Research, Imperial College Faculty of Medicine, St. Mary's Campus, London, England.
Abstract:Intact p73 function is shown to be an important determinant of cellular sensitivity to anticancer agents. Inhibition of p73 function by dominant-negative proteins or by mutant p53 abrogates apoptosis and cytotoxicity induced by these agents. A polymorphism encoding either arginine (72R) or proline (72P) at codon 72 of p53 influences inhibition of p73 by a range of p53 mutants identified in squamous cancers. Clinical response following cisplatin-based chemo-radiotherapy for advanced head and neck cancer is influenced by this polymorphism, cancers expressing 72R mutants having lower response rates than those expressing 72P mutants. Polymorphism in p53 may influence individual responsiveness to cancer therapy.
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