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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Differentiation of skeletal osteogenic progenitor cells to osteoblasts with 3,4-diarylbenzopyran based amide derivatives: Novel osteogenic agents
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Differentiation of skeletal osteogenic progenitor cells to osteoblasts with 3,4-diarylbenzopyran based amide derivatives: Novel osteogenic agents

机译:基于3,4-二芳基苯并吡喃的酰胺衍生物将骨骼成骨祖细胞分化为成骨细胞:新型成骨剂

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摘要

A series of 3,4-diarylbenzopyran based amide derivatives was synthesized and evaluated for osteogenic activity in in vitro and in vivo models of osteoporosis. Compounds 17a, 21b-c and 22a-b showed significant osteogenic activity in osteoblast differentiation assay. Among the synthesized compounds, 22b was identified as lead molecule which showed significant osteogenic activity at 1 pM concentration in osteoblast differentiation assay and at 1 mg kg(-1) body weight dose in estrogen deficient balb/c mice model. In vitro bone mineralization and expression of osteogenic marker genes viz BMP-2, RUNX-2, OCN, and collagen type 1 further confirmed the osteogenic potential of 22b. Gene expression study for estrogen receptor a and 13 (ER-alpha and ER-beta) in mouse calvarial osteoblasts (MCOs) unveiled that possibly 22b exerted osteogenic efficacy via activation of Estrogen receptor-beta preferentially. In vivo pharmacokinetic, estrogenicity and acute toxicity studies of 22b showed that it had good bioavailability and was devoid of uterine estrogenicity at 1 mg kg(-1) and inherent toxicity up to 1000 mg kg(-1) body weight dose respectively. 2016 Elsevier Masson SAS. All rights reserved.
机译:合成了一系列基于3,4-二芳基苯并吡喃的酰胺衍生物,并在骨质疏松症的体外和体内模型中评估了其成骨活性。在成骨细胞分化测定中,化合物17a,21b-c和22a-b显示出显着的成骨活性。在合成的化合物中,22b被鉴定为铅分子,在成骨细胞分化试验中浓度为1 pM时,在雌激素缺乏的balb / c小鼠模型中,剂量为1 mg kg(-1)时,显示出显着的成骨活性。 BMP-2,RUNX-2,OCN和1型胶原的体外骨矿化和成骨标记基因的表达进一步证实了22b的成骨潜力。小鼠颅骨成骨细胞(MCO)中雌激素受体a和13(ER-alpha和ER-beta)的基因表达研究表明,可能22b通过优先激活雌激素受体β发挥成骨功效。 22b的体内药代动力学,雌激素和急性毒性研究表明,它具有良好的生物利用度,分别在1 mg kg(-1)和最高1000 mg kg(-1)体重剂量时没有子宫雌激素性。 2016 Elsevier Masson SAS。版权所有。

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