O6-Methylguanine-DNA methyltransferase inactivation and chemotherapy

doi:10.1093/bmb/ldm036

British Medical Bulletin Advance Access originally published online on February 1, 2008
British Medical Bulletin 2008 85(1):17-33; doi:10.1093/bmb/ldm036

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O⁶-Methylguanine-DNA methyltransferase inactivation and chemotherapy

Barbara Verbeek, Thomas D. Southgate, David E. Gilham and Geoffrey P. Margison^*

Paterson Institute for Cancer Research, University of Manchester, Manchester, UK

^* Correspondence to: Geoffrey P. Margison, Cancer Research UK Carcinogenesis Group, Paterson Institute for Cancer Research, University of Manchester, Wilmslow Road, Manchester M20 4BX, UK. E-mail: gmargison{at}picr.man.ac.uk

Introduction: Alkylating agents are frequently used in the chemotherapy ofmany types of cancer. This group of drugs mediates cell deathby damaging DNA and therefore, understandably, cellular DNArepair mechanisms can influence both their antitumour efficacyand their dose-limiting toxicities.

Sources of data: This review focuses on the mechanism of action of the DNA repairprotein, O⁶-methylguanine-DNA methyltransferase (MGMT) and itsexploitation in cancer therapy and reviews the current literature.

Areas of agreement: MGMT can provide resistance to alkylating agents by DNA damagereversal. Inhibition of tumour MGMT by pseudosubstrates to overcometumour resistance is under clinical evaluation. In addition,MGMT overexpression in haematopoietic stem cells has been shownin animal models to protect normal cells against the myelosuppressiveeffects of chemotherapy: this strategy has also entered clinicaltrials.

Areas of controversy: MGMT inhibitors enhance the myelotoxic effect of O⁶-alkylatingdrugs and therefore reduce the maximum-tolerated dose of theseagents. Retroviral vectors used for chemoprotective gene therapyare associated with insertional mutagenesis and leukaemia development.

Growing points: The results of ongoing preclinical and clinical research involvingvarious aspects of MGMT modulation should provide new prospectsfor the treatment of glioma, melanoma and other cancer types.

Areas timely for developing research: Tissue- and tumour-specific approaches to the modulation ofMGMT together with other DNA repair functions and in combinationwith immuno- or radiotherapy are promising strategies to improvealkylating agent therapy.

Keywords: AGT • chemotherapy • DNA repair • drug resistance • Lomeguatrib • myeloprotective gene therapy • glioma • MGMT/O⁶-methylguanine-DNA methyltransferase • O⁶-benzylguanine • O⁶-(4-bromothenyl)guanine

Accepted for publication December 14, 2007.

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