T Brian H McMurry
Index: DNA Repair (Amst.) 6(8) , 1161-9, (2007)
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The DNA repair protein, O(6)-alkylguanine-DNA alkyltransferase (MGMT) can confer resistance to the cancer chemotherapeutic effects of the class of DNA damaging drugs generally referred to as the O(6)-alkylating agents. Inactivation of MGMT is thus a practical approach to improving the efficacy of such agents. An account is given of the collaboration between groups at Trinity College, Dublin and the Paterson Institute, Manchester which led to the development of the MGMT inactivating drug, Patrin (PaTrin-2, Lomeguatrib). The development of a simpler method of synthesis of O(6)-arylmethylguanines opened up the way to make a series of O(6)-heteroalkylmethyl analogues of the archetypal MGMT pseudosubstrate, O(6)-methylguanine. Of these, the furfuryl and thenyl compounds were the most active against recombinant Human MGMT in an in vitro assay. The 4-bromothenyl derivative was chosen for clinical trial as the most active compound. The MGMT active site tolerates O(6)-substituted guanines where the side chain can be quite large, but does not tolerate those with an aromatic or heteroaromatic ring with an 'ortho' substituent.
Structure | Name/CAS No. | Molecular Formula | Articles |
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Lomeguatrib
CAS:192441-08-0 |
C10H8BrN5OS |
Effect of lomeguatrib-temozolomide combination on MGMT promo...
2013-06-01 [Tumour Biol. 34(3) , 1935-47, (2013)] |
Randomized trial of the combination of lomeguatrib and temoz...
2007-06-20 [J. Clin. Oncol. 25(18) , 2540-5, (2007)] |
[Analysis of the relevant factors of mechanism for telozolom...
2011-10-01 [Zhonghua Zhong Liu Za Zhi 33(10) , 794-6, (2011)] |
Inhibition of DNA repair with MGMT pseudosubstrates: phase I...
2011-09-06 [Br. J. Cancer 105(6) , 773-7, (2011)] |
Novel role of triazenes in haematological malignancies: pilo...
2007-08-01 [DNA Repair (Amst.) 6(8) , 1179-86, (2007)] |
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