Dietary retinoic acid supplementation stimulates intestinal tumour formation and growth in multiple intestinal neoplasia (Min)/+ mice

doi:10.1093/carcin/bgg176

Carcinogenesis Advance Access originally published online on September 26, 2003

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Carcinogenesis, Vol. 25, No. 1, 149-153, January 2004
© Oxford University Press; all rights reserved

CARCINOGENESIS

Dietary retinoic acid supplementation stimulates intestinal tumour formation and growth in multiple intestinal neoplasia (Min)/+ mice

Linda Møllersen, Jan Erik Paulsen, Hege Benedikte Ølstørn, Helle Katrine Knutsen and Jan Alexander¹

Department of Food Toxicology, Norwegian Institute of Public Health, Oslo, Norway

Chemopreventive activity by retinoic acid (RA) has been demonstratedpreviously in rat colon. The spontaneous tumourigenesis in theMin/+ mouse, which harbours a germline mutation in the tumoursuppressor gene adenomatous polyposis coli (Apc), is characterizedby inactivation of Apc, nuclear accumulation of ß-cateninand the enhanced expression of specific genes activated by Tcell factor (TCF)/ß-catenin signalling. Recently itwas reported that ß-catenin interacts with retinoicacid receptor in a retinoid-dependent manner, reducing ß-catenin/TCFregulated transcription. Our hypothesis was therefore that dietarysupplementation with all-trans RA may inhibit the Apc-driventumourigenesis in Min/+ mice. Surprisingly, in two differentexperiments the results showed that dietary RA significantlystimulated both the formation and growth of small intestinaltumours. In the first experiment Min/+ mice were exposed to50 mg 2-amino-1-methyl-6-phenylimidazo[4,5-b]pyridine/kg bodyweightat day 3–6 after birth and then treated with 50 mg/kgdietary RA in 1–3 weeks from the age of 2 weeks. In thesecond experiment the mice were not treated with carcinogen,and the diet was supplemented with 5 or 10 mg/kg RA from theage of 4 weeks until termination of the experiment at 11 weeks.Immunohistochemical studies revealed no differences in ß-catenin,cyclin D1 or proliferating cell nuclear antigen staining followingRA treatment. There was no intestinal toxicity in mice fed 10mg/kg RA, indicating that the increased tumourigenesis in Min/+mice is a specific effect of all-trans RA.

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