| Literature DB >> 17499351 |
Jiri Neuzil1, Lan-Feng Dong, Lalitha Ramanathapuram, Tobias Hahn, Miroslava Chladova, Xiu-Fang Wang, Renata Zobalova, Lubomir Prochazka, Mikhal Gold, Ruth Freeman, Jaroslav Turanek, Emmanuel T Akporiaye, Jeffrey C Dyason, Stephen J Ralph.
Abstract
Mitochondria have recently emerged as new and promising targets for cancer prevention and therapy. One of the reasons for this is that mitochondria are instrumental to many types of cell death and often lie downstream from the initial actions of anti-cancer drugs. Unlike the tumour suppressor gene encoding p53 that is notoriously prone to inactivating mutations but whose function is essential for induction of apoptosis by DNA-targeting agents (such as doxorubicin or 5-fluorouracil), mitochondria present targets that are not so compromised by genetic mutation and whose targeting overcomes problems with mutations of upstream targets such as p53. We have recently proposed a novel class of anti-cancer agents, mitocans that exert their anti-cancer activity by destabilising mitochondria, promoting the selective induction of apoptotic death in tumour cells. In this communication, we review recent findings on mitocans and propose a common basis for their mode of action in inducing apoptosis of cancer cells. We use as an example the analogues of vitamin E that are proving to be cancer cell-specific and may soon be developed into efficient anti-cancer drugs.Entities:
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Year: 2007 PMID: 17499351 DOI: 10.1016/j.mam.2007.02.003
Source DB: PubMed Journal: Mol Aspects Med ISSN: 0098-2997