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dc.contributor.authorZiaee, M
dc.contributor.authorSamini, M
dc.contributor.authorBolourtchian, M
dc.contributor.authorGhaffarzadeh, M
dc.contributor.authorAhmadi, M
dc.contributor.authorEgbal, MA
dc.contributor.authorKhorrami, A
dc.contributor.authorAndalib, S
dc.contributor.authorMaleki-Dizaji, N
dc.contributor.authorGarjani, A
dc.date.accessioned2018-08-26T08:05:27Z
dc.date.available2018-08-26T08:05:27Z
dc.date.issued2012
dc.identifier.urihttp://dspace.tbzmed.ac.ir:8080/xmlui/handle/123456789/49825
dc.description.abstractFibrates, as hypolipidemic drugs known as agonists of peroxisome proliferator-activated receptors, diminish inflammatory responses. Studies have shown that incorporation of a silicon atom into a drug structure improves its pharmacological potency, modifies its selectivity toward a given target, or changes its metabolic rate, in addition to increasing the lipophilicity of the compounds. A siliconized analog of clofibrate, ethyl-2-methyl-2-(4-(trimethylsily)phenoxy) propionate was synthesized, whereby the chlorine atom in the phenoxy ring was replaced by a trimethylsilyl group. The anti-inflammatory effects of the siliconized analog (silafibrate) were evaluated in an air-pouch model of inflammation and compared with those of clofibrate. Oral administration of both drugs produced a significant anti-inflammatory action by reducing carrageenan induced pouch leukocyte recruitment, exudates production, and granulated tissue weight. The silicon isostere of clofibrate has improved anti-inflammatory properties.
dc.language.isoEnglish
dc.relation.ispartofIRANIAN JOURNAL OF PHARMACEUTICAL RESEARCH
dc.subjectClofibrate
dc.subjectSilicon
dc.subjectSiliconized analog
dc.subjectAnti-inflammatory
dc.titleSynthesis of a Novel Siliconized Analog of Clofibrate (Silafibrate) and Comparison of their Anti-inflammatory Activities
dc.typeArticle
dc.citation.volume11
dc.citation.issue1
dc.citation.spage91
dc.citation.epage95
dc.citation.indexWeb of science
dc.identifier.DOI10.22037/IJPR.2011.1045


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