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Dietary and Metabolic Manipulations of the Carcinogenic Process: Role of Nucleotide Pool Imbalances in Carcinogenesis

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Ezio Laconi

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Shanthi Vasudevan

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Ayumi Denda

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Sudhasri Rajagopal

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Srinivasan Rajalakshmi

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Dittakavi S. R. Sarma

Department of Pathology, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8

Perturbations in DNA and/or membranes are considered to be important for the carcinogenic process. A search for nutritional and metabolic means of disturbing the homeostasis of DNA and membranes revealed that nucleotide pools of fer an exciting possibility. An imbalance in nucleotide pools can exert a two-pronged attack on both DNA and membranes. When given to rats, orotic acid, a precursor of pyrimidine nucleotides, results in an imbalance in nucleotide pools (an increase in uridine nucleotides and a decrease in inosine/adenine nucleotides), alterations in both DNA and membranes, and promotion of carcinogenesis in the liver initiated by chemical carcinogens. Agents such as adenine and allopurinol, which inhibit the metabolism of orotic acid and thereby decrease the formation of uridine nucleotides, and galactosamine, which traps uridine nucleotides, inhibited the promotional effects of orotic acid in the liver. These results suggested that orotic acid needs to be metabolized to uridine nucleotides and the creation of a subsequent imbalance in nucleotide pools is important for the promotional effects of orotic acid. To determine whether the creation of a nucleotide pool imbalance is a more general mechanism of tumor-promotion, two lines of approach were investigated. One was to determine the effect of orotic acid on promotion of carcinogenesis in other organs, and the second approach was to determine how to induce nucleotide pool imbalances by means other than orotic acid administration. It is interesting to note that orotic acid promotes carcinogenesis in duodenum initiated by azoxymethane. Regarding the second approach, it became apparent that several metabolic disturbances result in increased orotic acid synthesis and alterations in nucleotide pools. For example, increased administration of amino acids, ammonia, certain disturbances in urea cycle enzymes and/or metabolites, and certain types of liver dysfunction result in increased synthesis of orotic acid. Similarly, folic acid deficiency also results in increased levels of deoxyuridine nucleotide levels.

Toxicologic Pathology, Vol. 15, No. 2, 190-193 (1987)
DOI: 10.1177/019262338701500210


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