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首页> 外文期刊>Current topics in medicinal chemistry >PPAR modulators and PPAR pan agonists for metabolic diseases: the next generation of drugs targeting peroxisome proliferator-activated receptors?
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PPAR modulators and PPAR pan agonists for metabolic diseases: the next generation of drugs targeting peroxisome proliferator-activated receptors?

机译:用于代谢疾病的PPAR调节剂和PPAR泛激动剂:靶向过氧化物酶体增殖物激活受体的下一代药物?

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摘要

The Peroxisome Proliferator-Activated Receptors-PPAR alpha, PPAR gamma, and PPAR delta--are members of the nuclear receptor gene family that have emerged as therapeutic targets for the development of drugs to treat human metabolic diseases. The discovery of high affinity, subtype-selective agonists for each of the three PPAR subtypes has allowed elucidation of the pharmacology of these receptors and development of first-generation therapeutic agents for the treatment of diabetes and dyslipidemia. However, despite proven therapeutic benefits of selective PPAR agonists, safety concerns and dose-limiting side effects have been observed, and a number of late-stage development failures have been reported. Scientists have continued to explore ligand-based activation of PPARs in hopes of developing safer and more effective drugs. This review highlights recent efforts on two newer approaches, the simultaneous activation of all three PPAR receptors with a single ligand (PPAR pan agonists) and the selective modulation of a single PPAR receptor in a cell or tissue specific manner (selective PPAR modulator or SPPARM) in order to induce a subset of target genes and affect a restricted number of metabolic pathways.
机译:过氧化物酶体增殖物激活受体-PPARα,PPARγ和PPARδ是核受体基因家族的成员,它们已成为开发治疗人类代谢性疾病药物的治疗靶标。对三种PPAR亚型中的每一种的高亲和力,亚型选择性激动剂的发现,已经阐明了这些受体的药理学,并开发了用于治疗糖尿病和血脂异常的第一代治疗剂。然而,尽管选择性PPAR激动剂具有公认的治疗益处,但已观察到安全性问题和剂量限制的副作用,并且已报道了许多后期发育失败的情况。科学家们继续探索基于配体的PPAR激活,以期开发出更安全,更有效的药物。这篇综述重点介绍了最近在两种更新方法上的努力:用单个配体同时激活所有三个PPAR受体(PPAR泛激动剂)和以细胞或组织特异性方式(选择性PPAR调节剂或SPPARM)选择性调节单个PPAR受体为了诱导靶基因的子集并影响有限数量的代谢途径。

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