๐”– Bobbio Scriptorium
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Experimental colonic carcinogenesis after gastric surgery

โœ Scribed by Mr P. W. J. Houghton; R. J. Owen; P. J. Henly; N. J. McC. Mortensen; M. J. Hill; R. C. N. Williamson


Publisher
John Wiley and Sons
Year
1990
Tongue
English
Weight
469 KB
Volume
77
Category
Article
ISSN
0007-1323

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โœฆ Synopsis


Experimental colonic carcinogenesis after gastric surgery

Peptic ulcer surgery may predispose to the subsequent development of colorectal cancer. This experimental study has investigated the efects of gastric operations on colonic cell proliferation, bile acid excretion and carcinogenesis. Male Sprague-Dawley rats (n = 105) underwent sham operation, Pblya partial gastrectomy or vagotomy and pyloroplasty. The carcinogen azoxymethane was administered weekly for 6 weeks thereafter (total dose 60 mg kg-I). When the animals were killed 24 weeks after operation, colons were examined for mucosal mass, crypt cell production rate ( C C P R ) and tumour yield; faeces were assayed for contents of neutral steroids and bile acids (both total and individual). Morphometric indices and mucosal D N A content were similar in all three groups. Pblya gastrectomy reduced: ( I ) C C P R throughout the colon (by 42-65 per cent, P<0-002); ( 2) the number of rats with colorectal tumours (26 per cent versus 63 per cent, P < 0.05); (3) faecal levels of neutral steroids and bile acids, notably hyodeoxycholic acid ( P < 0-01). Although vagotomy and pyloroplasty increased caecal CCPR, there were no consistent differences in faecal steroids and no alteration in tumour yield after the operation. These results fail to support clinical studies suggesting that gastric surgery predisposes to colonic carcinogenesis. Indeed, Pblya partial gastrectomy exerts a protective effect, probably by inhibiting colonic cell proliferation.


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