The pharmacokinetics of dietary fucoxanthin, one of the xanthophylls in brown sea algae, is little understood. In the present study, mice were orally administered fucoxanthin, and the distribution and accumulation of fucoxanthin and its metabolites fucoxanthinol and amarouciaxanthin A were measured in the plasma, erythrocytes, liver, lung, kidney, heart, spleen and adipose tissue. In a single oral administration of 160 nmol fucoxanthin, fucoxanthinol and amarouciaxanthin A were detectable in all specimens tested in the present study, but fucoxanthin was not. The time at maximum concentration (T max ) of these metabolites in adipose tissue was 24 h, while the T max in the others was 4 h. The area under the curve to infinity (AUC 1 ) of fucoxanthinol in the liver was the highest value (4680 nmol/g £ h) among the tissues tested in the present study, while the AUC 1 of amarouciaxanthin A in adipose tissue was the highest value (4630 nmol/g £ h). In daily oral administration of 160 nmol fucoxanthin for 1 week, fucoxanthin was also detectable in the tissues even at a low concentration. The amount of fucoxanthinol was 123 nmol/g in the heart and 85·2 nmol/g in the liver. Amarouciaxanthin A in the adipose tissue was distributed at a concentration of 97·5 nmol/g. These results demonstrate that dietary fucoxanthin accumulates in the heart and liver as fucoxanthinol and in adipose tissue as amarouciaxanthin A.
Fucoxanthin: Fucoxanthinol: Amarouciaxanthin A: MiceBrown algae are a traditional foodstuff of East Asians, and an epidemiological study (1) has shown that the consumption of brown sea algae is associated with a low risk of breast cancer. Brown alga powders or extracts have been reported to suppress chemical-induced carcinogenesis in animals (2 -5) . Fucoxanthin is one of the xanthophylls found in brown algae such as kombu (Laminaria japonica), hijiki (Sargassum fusiforme) and wakame (Undaria pinnatifida) (6) . The oral administration of fucoxanthin prevented carcinogenesis in several animal models (7,8) . Recent studies with cancer cell lines have suggested that the suppressive effect is due to the inhibitory effect of fucoxanthin on cell proliferation through the induction of apoptosis (9,10) and cell cycle arrest (11) . In addition to these activities, the compound also has anti-inflammatory and anti-obesity activities (12,13) . Interestingly, a recent study showed that dietary fucoxanthin stimulates the expression of uncoupling protein 1 in the mitochondria of white adipose tissue and facilitates the consumption of fats in rats (14) . Thus, fucoxanthin has various physiological activities and contributes to the beneficial effects of brown algae.Many studies (15 -20) have reported the metabolism of hydrocarbon carotenoids such as a-carotene and b-carotene; these carotenoids are absorbed in the small intestine and then converted to vitamin A. However, information on the metabolism of non-provitamin A-type carotenoids is insufficient to explain their bioavailability and safety, although some xanthophylls such as a...
