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首页> 外文期刊>Journal of Medicinal Chemistry >Synthesis and Identification of [1,2,4]Thiadiazole Derivatives as a New Series of Potent and Orally Active Dual Agonists of Peroxisome Proliferator-Activated Receptors a and delta
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Synthesis and Identification of [1,2,4]Thiadiazole Derivatives as a New Series of Potent and Orally Active Dual Agonists of Peroxisome Proliferator-Activated Receptors a and delta

机译:合成和鉴定[1,2,4]噻二唑衍生物作为过氧化物酶体增殖物激活的受体α和δ的新的有效和口服活性双重激动剂。

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摘要

Cardiovascular disease is the most common cause of morbidity and mortality in developed nations. To effectively target dyslipidemia to reduce the risk of cardiovascular disease, it may be beneficial to activate the peroxisome proliferator-activated receptors (PPARs) PPAR alpha and PPAR delta simultaneously through a single molecule. Replacement of the methylthiazole of 5 (the PPAR delta selective agonist) with [1,2,4]thiadiazole gave compound 13, which unexpectedly displayed submicromolar potency as a partial agonist at PPARa in addition to the high potency at PPAR delta. Optimization of 13 led to the identification of 24 as a potent and selective PPAR alpha/delta dual agonist. Compound 24 and its close analogs represent a new series of PPAR alpha/delta dual agonists. The high potency, significant gene induction, excellent PK profiles, and good in vivo efficacies in three animal models may render compound 24 as a valuable pharmacological tool in elucidating the complex roles of PPAR alpha/delta dual agonists and as a potential treatment of the metabolic syndrome.
机译:在发达国家,心血管疾病是发病率和死亡率的最常见原因。为了有效地靶向血脂异常以降低发生心血管疾病的风险,通过单个分子同时激活过氧化物酶体增殖物激活受体(PPAR),PPARα和PPAR delta可能是有益的。用[1,2,4]噻二唑代替5的甲基噻唑(PPARδ选择性激动剂),得到的化合物13除了在PPARδ上具有高效力外,还出乎意料地显示出亚微摩尔效价,作为PPARa上的部分激动剂。 13的优化导致24被鉴定为有效和选择性的PPARα/δ双激动剂。化合物24及其紧密类似物代表一系列新的PPARα/δ双激动剂。在三种动物模型中的高效力,显着的基因诱导,出色的PK分布和良好的体内功效可能使化合物24成为阐明PPARα/δ双激动剂的复杂作用的有价值的药理工具,并作为代谢的潜在治疗方法综合症。

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