Low toxicity cancer chemotherapy by suicide inactivation of DNA polymerase alpha holoenzyme: first results with new thiazolidinyl- and perhydrothiazinyl-ethyl-N-mustard-phosphamide esters.

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H J Hohorst, L Bielicki, K Müller, G Voelcker

Author Information

H J Hohorst: Gustav-Embden-Zentrum of Biological Chemistry, University of Frankfurt/Main, Federal Republic of Germany.

PMID: 3384844 DOI: 10.1007/BF00405840

Thiazolidinyl- and perhydrothiazinyl-ethyl-N-mustard-phosphamide esters were designed to act as highly specific suicide inactivators of DNA polymerase alpha holoenzymes. Acute and subacute toxicity of these drugs in mice was very small. By daily i.p. injection, on day 0-4 mice were cured of P 388 lymphatic leukaemia with no depression of blood leucocytes. The findings suggest that suicide inactivators of DNA polymerase alpha holoenzyme may be promising drugs for low toxicity cancer chemotherapy.

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Animals

Antineoplastic Agents

DNA Polymerase II

Kinetics

Leukemia P388

Leukemia, Experimental

Mice

Nitrogen Mustard Compounds

Thiazines

Thiazoles

Thiazolidines

Antineoplastic Agents

Nitrogen Mustard Compounds

Thiazines

Thiazoles

Thiazolidines

NSC 612567

NSC 613060

DNA Polymerase II

Journal Article Research Support, Non-U.S. Gov't

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