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首页> 外文期刊>Arzneimittel-Forschung: =Drug Research >Amino derivatives of phenyl alkyl thiophene as inhibitors of bone resorption. Structure-activity relationship.
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Amino derivatives of phenyl alkyl thiophene as inhibitors of bone resorption. Structure-activity relationship.

机译:苯基烷基噻吩的氨基衍生物可作为骨吸收的抑制剂。构效关系。

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Metabolism of arachidonic acid through the 5-lipoxygenase (LO) pathway generates compounds that stimulate osteoclastic bone resorption; since LO metabolites might play a role in bone loss due to excessive resorption it was tried to develop a series of antiresorptive agents starting from an already known LO inhibitor. Of the 35 compounds synthesized, 11 strongly inhibited (10 mumol/l) retinoic acid-induced bone resorption in cultured mouse calvariae; they were also tested for their effect on LO activity using rat peritoneal neutrophils, but no correlation could be drawn between inhibition of LO and bone resorption. Other pathways, still to be identified, must therefore be targeted by these compounds even though LO inhibition might contribute to their effects on bone. Two compounds selected for further studies were found active on parathyroid hormone-induced osteolysis, while they had no effect on basal resorption; they must, therefore, act at some key point in the process of activation of osteoclastic resorption. This series of compounds may represent a new way for the treatment of bone loss due to excessive resorption.
机译:通过5-脂氧合酶(LO)途径的花生四烯酸代谢产生刺激破骨细胞骨吸收的化合物。由于LO代谢物可能由于过度吸收而在骨质流失中起作用,因此尝试从已知的LO抑制剂开始开发一系列抗吸收剂。在合成的35种化合物中,有11种在培养的小鼠颅盖中强烈抑制(10μmol/ l)维甲酸诱导的骨吸收。还使用大鼠腹膜中性粒细胞测试了它们对LO活性的影响,但在LO抑制与骨吸收之间没有相关性。因此,即使LO抑制可能有助于它们对骨骼的影响,这些化合物也必须靶向其他尚待确定的途径。发现选择用于进一步研究的两种化合物对甲状旁腺激素诱导的骨溶解有效,而对基础吸收没有影响。因此,它们必须在破骨细胞吸收激活过程中的某些关键时刻起作用。这一系列的化合物可能代表了一种治疗由于过度吸收而引起的骨丢失的新方法。

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