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Drug Metabolism and Disposition 2010-Nov

Isolation and identification of phase 1 metabolites of curcumol in rats.

Rakstu tulkošanu var veikt tikai reģistrēti lietotāji
Ielogoties Reģistrēties
Saite tiek saglabāta starpliktuvē
Yan Lou
Hui Zhang
Hao He
Kaifeng Peng
Ning Kang
Xingchuan Wei
Xuegai Li
Lixia Chen
Xinsheng Yao
Feng Qiu

Atslēgvārdi

Abstrakts

Curcumol is one of the major components of the essential oil of Curcuma wenyujin with the structure of a guaiane-type sesquiterpenoid hemiketal. It exhibits clear antitumor, antihepatic fibrosis, antioxidant, and antimicrobial activities. In this article, the metabolism of curcumol in rats was investigated by characterizing metabolites excreted into urine. Sixteen phase 1 metabolites of curcumol were isolated from the urine of rats after an oral dose of 40 mg/kg, and their structures were elucidated on the basis of spectroscopic data. The metabolites were characterized as 2α-hydroxycurcumol (M-1), (11αH)-3α-hydroxy-9-en-8,13-epoxycurcumol (M-2), (11αH)-14-hydroxy-9-en-8,13-epoxycurcumol (M-3), (11βH)-14-hydroxy-9-en-8,12-epoxycurcumol (M-4), 10α,14-dihydroxy-(1αH,7βH)-guai-4-en-3,8-dione (M-5), 10β,14-dihydroxy-(1αH,7βH)-guai-4-en-3,8-dione (M-6), 10β-hydroxy-(1αH,7βH,11αH)-guai-8(13),8(14)-diepoxy-4-en-3-one (M-7), 10β-hydroxy-(1αH,7βH,11βH)-guai-8(12),8(14)-diepoxy-4-en-3-one (M-8), 10α-hydroxy-(1αH,7βH,11αH)-guai-8(13), 8(14)-diepoxy-4-en-3-one (M-9), 10α-hydroxy-(1αH,7βH,11βH)-guai-8(12),8(14)-diepoxy-4-en-3-one (M-10), 10α,14,15-trihydroxy-(1αH,7βH)-guai-4-en-3,8-dione (M-11), 10β-hydroxy-(1αH,7βH)-guai-4-en-3,8-dioxo-13-oic acid (M-12), (1αH,7βH)-guai-4,10(14)-dien-3, 8-dioxo-13-oic acid (M-13), 5β,10β-dihydroxy-(1αH,7βH,11αH)-guai-8(13),8(14)-diepoxide (M-14), 10β,14-dihydroxycurcumol (M-15), and 5β,10β,14-trihydroxy-(1αH,7βH)-guai-8-one (M-16). All were newly identified compounds, among which M-3 and M-4, M-5 and M-6, and M-7, M-8, M-9, and M-10 are three groups of epimers. On the basis of the metabolite profile, the possible metabolic pathways of curcumol in rats are proposed. This is the first study of the metabolites of guaiane-type sesquiterpene in animals.

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