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Bone-Specific Metabolism of Dietary Polyphenols in Resorptive Bone Diseases.

Molecular nutrition & food research (2020-06-09)
Andrew G Kunihiro, Paula B Luis, Jennifer B Frye, Wade Chew, H H Chow, Claus Schneider, Janet L Funk
RÉSUMÉ

Curcumin prevents bone loss in resorptive bone diseases and inhibits osteoclast formation, a key process driving bone loss. Curcumin circulates as an inactive glucuronide that can be deconjugated in situ by bone's high β-glucuronidase (GUSB) content, forming the active aglycone. Because curcumin is a common remedy for musculoskeletal disease, effects of microenvironmental changes consequent to skeletal development or disease on bone curcumin metabolism are explored. Across sexual/skeletal development or between sexes in C57BL/6 mice ingesting curcumin (500 mg kg-1 ), bone curcumin metabolism and GUSB enzyme activity are unchanged, except for >twofold higher (p < 0.05) bone curcumin-glucuronide substrate levels in immature (4-6-week-old) mice. In ovariectomized (OVX) or bone metastasis-bearing female mice, bone substrate levels are also >twofold higher. Aglycone curcumin levels tend to increase proportional to substrate such that the majority of glucuronide distributing to bone is deconjugated, including OVX mice where GUSB decreases by 24% (p < 0.01). GUSB also catalyzes deconjugation of resveratrol and quercetin glucuronides by bone, and a requirement for the aglycones for anti-osteoclastogenic bioactivity, analogous to curcumin, is confirmed. Dietary polyphenols circulating as glucuronides may require in situ deconjugation for bone-protective effects, a process influenced by bone microenvironmental changes.

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Description du produit

Sigma-Aldrich
4-Méthylumbelliféryl-β-D-glucuronide hydrate, ≥98% (HPLC), BioReagent, for identification of transformed plants
Sigma-Aldrich
D-Saccharic acid 1,4-lactone monohydrate, ≥98.0% (HPLC)