The role of alkalizing and neutral potassium salts in urinary bladder carcinogenesis in rats

Abstract

Using an initiation-promotion rat model, we have previously shown that the alkalizing salt KHCO₃ is a strong and the neutral salt KCl a weak promoter of urinary bladder carcinogenesis. We have now studied the effects of these salts on rat urinary bladder epithelium without prior exposure to a bladder tumour initiator. In four studies ranging in duration from 4 to 130 weeks, (equimolar) amounts of K⁺ were administered in the diet to male and female rats (85 rats/sex/ group) as KHCO3 or KCl. Comparable increases in urinary volume and potassium levels were found with both KHCO₃ and KCl, but only KHCO₃ induced an elevated urinary pH. The feeding of KHCO₃ resulted in simple epithelial hyper-plasia and, after prolonged administration, in papillary/ nodular hyperplasia, papillomas and transitional cell carcinomas of the urinary bladder. With KCl, only a slight increase in proliferative urothelial lesions was found; one male showed papillary hyperplasia and one female exhibited nodular hyperplasia and a papilloma. Our results allow the conclusion that KHCO₃, a strong promoter of bladder carcinogenesis, is capable of inducing urinary bladder cancer in rats without prior application of an initiator, whereas KCl, a weak tumour promoter, induced only a few (pre)neoplastic lesions.