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甲状腺激素类似物:2013 年我们处于什么位置?

Thyroid hormone analogues: where do we stand in 2013?

机构信息

Center for Genomic Medicine, Houston Methodist Research Institute , Houston, Texas.

出版信息

Thyroid. 2013 Nov;23(11):1333-44. doi: 10.1089/thy.2012.0458. Epub 2013 Oct 16.

Abstract

Thyroid hormones (THs) are important in the development and maintenance of lipid and energy homeostasis. THs act through two closely related TH receptors (TRs α and β), which are conditional transcription factors. Recently, TH analogues or thyromimetics with varying degrees of TR subtype and liver uptake selectivity have been developed. These compounds exert beneficial effects of TH excess states without many undesirable TR-dependent side effects. Several selective TR modulators (STRMs) showed exceptionally promising results in lowering serum cholesterol in preclinical animal models and human clinical studies. Moreover, some first generation STRMs elicit other potentially beneficial effects on obesity, glucose metabolism, and nonalcoholic fatty liver disease (NAFLD). While it was initially thought that STRMs would be an effective long-term therapy to combat elevated cholesterol, possibly in conjunction with another cholesterol-lowering therapy, the statins, three major first generation STRMs failed to progress beyond early phase III human trials. The aim of this review is to discuss how STRMs work, their actions in preclinical animal models and human clinical trials, why they did not progress beyond clinical trials as cholesterol-lowering therapeutics, whether selective TR modulation continues to hold promise for dyslipidemias, and whether members of this drug class could be applied to the treatment of other aspects of metabolic syndrome and human genetic disease.

摘要

甲状腺激素 (THs) 在脂质和能量稳态的发育和维持中很重要。THs 通过两种密切相关的 TH 受体 (TRα 和 TRβ) 发挥作用,这两种受体是条件转录因子。最近,已经开发出具有不同程度 TR 亚型和肝脏摄取选择性的 TH 类似物或甲状腺刺激剂。这些化合物在没有许多不良的 TR 依赖性副作用的情况下发挥 TH 过度状态的有益作用。几种选择性 TR 调节剂 (STRMs) 在降低临床前动物模型和人类临床研究中的血清胆固醇方面显示出非常有前景的结果。此外,一些第一代 STRMs 对肥胖、葡萄糖代谢和非酒精性脂肪性肝病 (NAFLD) 产生其他潜在的有益影响。虽然最初认为 STRMs 将是一种有效的长期治疗方法,以对抗升高的胆固醇,可能与另一种降胆固醇治疗方法,他汀类药物联合使用,但三种主要的第一代 STRMs 未能在人类 III 期临床试验后期取得进展。本文的目的是讨论 STRMs 的作用机制,它们在临床前动物模型和人类临床试验中的作用,为什么它们不能作为降胆固醇治疗药物在临床试验之外取得进展,选择性 TR 调节是否仍然对血脂异常有希望,以及这类药物是否可以应用于代谢综合征和人类遗传疾病的其他方面的治疗。

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