Discovery of Coumarin-Dihydropyridine Hybrids as Bone Anabolic Agents

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dc.contributor.author Sashidhara, K V
dc.contributor.author Kumar, Manoj
dc.contributor.author Khedgikar, Vikram
dc.contributor.author Kushwaha, Priyanka
dc.contributor.author Modukuri, R K
dc.contributor.author Kumar, Abdhesh
dc.contributor.author Gautam, Jyoti
dc.contributor.author Singh, Divya
dc.contributor.author Sridhar, Balasubramaniam
dc.contributor.author Trivedi, Ritu
dc.date.accessioned 2013-03-07T10:29:42Z
dc.date.available 2013-03-07T10:29:42Z
dc.date.issued 2012
dc.identifier.citation Journal of Medicinal Chemistry. 2013, 56(1), 109-22 en
dc.identifier.uri http://hdl.handle.net/123456789/1023
dc.description.abstract The concept of molecular hybridization led us to discover a novel series of coumarin-dihydropyridine hybrids that have potent osteoblastic bone formation in vitro and that prevent ovariectomy-induced bone loss in vivo. In this context, among all the compounds screened for alkaline phosphatase activity, four compounds 10, 14, 18, and 22 showed significant activity at pM concentrations. A series of other in vitro data strongly suggested compound 18 as most promising bone anabolic agent, which was further evaluated for in vivo studies. From these studies compound 18 proved useful, which at low oral dose of 1 mg/kg/day body weight, increased bone mass density and volume, expression of osteogenic genes (RUNX2, BMP-2 and ColI), bone formation rate (BFR), mineral apposition rate (MAR), improved the trabecular microarchitecture and decreased bone turn over markers in an ovariectomized rodent model for postmenopausal osteoporosis. en
dc.format.extent 4383343 bytes
dc.format.mimetype application/pdf
dc.language.iso en en
dc.relation.ispartofseries CSIR-CDRI Communication No. 8367 en
dc.subject Coumarin-Dihydropyridine Hybrids en
dc.subject Osteoblastic bone en
dc.subject RUNX2 en
dc.subject BMP-2 en
dc.subject ColI en
dc.subject BFR en
dc.subject MAR en
dc.title Discovery of Coumarin-Dihydropyridine Hybrids as Bone Anabolic Agents en
dc.type Article en


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