Dose-Responsive Alteration in Hepatic Lipid Peroxidation and Retinol Metabolism with Increasing Dietary beta-Carotene in Iron Deficient Rats

Author:

Ikeda Ryouko1,Uehara Mariko1,Takasaki Misao1,Chiba Hiroshige1,Masuyama Ritsuko1,Furusho Tadasu2,Suzuki Kazuharu1

Affiliation:

1. Department of Nutritional Science, Faculty of Applied Bio-Science, Tokyo University of Agriculture, Sakuragaoka 1-1-1, Setagaya-Ku, Tokyo 156-8502, Japan

2. Department of Nutrition, Junior College of Tokyo University of Agriculture, Sakuragaoka 1-1-1, Setagaya-Ku, Tokyo 156-8502, Japan

Abstract

Phosphatidylcholine hydroperoxide (PCOOH) levels are increased in the iron-deficient rat liver. We investigated the antioxidative effect of dietary beta-carotene and altered retinol metabolism in iron-deficient rats. Experiment 1: Male Wistar-strain rats were divided into six groups and fed a control diet, an iron-deficient diet, and iron-deficient diets with four different levels of dietary beta-carotene. The PCOOH concentration in the iron-deficient rat liver was decreased by supplementation with dietary beta-carotene. However, the beta-carotene dose response was not related to antioxidative potency. Hepatic and plasma beta-carotene concentrations were increased by iron deficiency. The hepatic retinol concentration was increased while the plasma retinol concentration was decreased in iron-deficient rats. Experiment 2: Male Wistar-strain rats were divided into two groups, with one group receiving a control diet with beta-carotene and the other an iron-deficient diet with beta-carotene. Intestinal iron was decreased and intestinal beta-carotene was unchanged in iron-deficient rats. The intestinal beta-carotene conversion ratio and beta-carotene cleavage enzyme activity were decreased in iron-deficient rats. Dietary beta-carotene played the role of an antioxidant in hepatic lipid peroxidation in the iron-deficient state, but there was no dose dependency. Moreover, intestinal beta-carotene cleavage and hepatic retinol release appear to be altered in iron-deficient rats.

Publisher

Hogrefe Publishing Group

Subject

Nutrition and Dietetics,General Medicine,Endocrinology, Diabetes and Metabolism,Medicine (miscellaneous)

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