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dc.creatorKydonaki EKen
dc.creatorFreitas Len
dc.creatorFonseca BMen
dc.creatorReguengo Hen
dc.creatorRaposo Simón Cen
dc.creatorBastos ARen
dc.creatorFernandes EMen
dc.creatorCanadas RFen
dc.creatorOliveira JMen
dc.creatorCorrelo VMen
dc.creatorReis RLen
dc.creatorVliora Men
dc.creatorGkiata Pen
dc.creatorKoutedakis Yen
dc.creatorNtina Gen
dc.creatorPinto Ren
dc.creatorCarrillo AEen
dc.creatorMarques Fen
dc.creatorAmorim T.en
dc.date.accessioned2022-03-16T12:33:13Z
dc.date.available2022-03-16T12:33:13Z
dc.date.issued2021
dc.identifier10.3390/nu13092981
dc.identifier.issn2072-6643
dc.identifier.urihttp://hdl.handle.net/11615/58431
dc.description.abstractOsteoporosis is characterized by bone loss. The present study aims to investigate the effects of bovine colostrum (BC) on bone metabolism using ovariectomized (OVX) and orchidectomized (ORX) rat models. Twenty-seven-week-old Wistar Han rats were randomly assigned as: (1) placebo control, (2) BC supplementation dose 1 (BC1: 0.5 g/day/OVX, 1 g/day/ORX), (3) BC supplementation dose 2 (BC2: 1 g/day/OVX, 1.5 g/day/ORX) and (4) BC supplementation dose 3 (BC3: 1.5 g/day/OVX, 2 g/day/ORX). Bone microarchitecture, strength, gene expression of VEGFA, FGF2, RANKL, RANK and OPG, and bone resorption/formation markers were assessed after four months of BC supplementation. Compared to the placebo, OVX rats in the BC1 group exhibited significantly higher cortical bone mineral content and trabecular bone mineral content (p < 0.01), while OVX rats in the BC3 group showed significantly higher trabecular bone mineral content (p < 0.05). ORX rats receiving BC dose 2 demonstrated significantly higher levels of trabecular bone mineral content (p < 0.05). Serum osteocalcin in the ORX was pointedly higher in all BC supplementation groups than the placebo (BC1: p < 0.05; BC2, BC3: p < 0.001). Higher doses of BC induced significantly higher relative mRNA expression of OPG, VEGFA, FGF2 and RANKL (p < 0.05). BC supplementation improves bone metabolism of OVX and ORX rats, which might be associated with the activation of the VEGFA, FGF2 and RANKL/RANK/OPG pathways.en
dc.sourceNutrientsen
dc.subjectbovine colostrumen
dc.subjectboneen
dc.subjectosteoporosisen
dc.subjectsupplementationen
dc.titleBovine Colostrum Supplementation Improves Bone Metabolism in an Osteoporosis-Induced Animal Modelen
dc.typejournalArticleen


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