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甲状腺激素类似物的心脏特异性作用。

Cardiac specific effects of thyroid hormone analogues.

机构信息

Department of Medicine, North Shore University Hospital and Feinstein Institute for Medical Research, Manhasset, New York, USA.

出版信息

Horm Metab Res. 2011 Oct;43(11):737-42. doi: 10.1055/s-0031-1291177. Epub 2011 Oct 18.

DOI:10.1055/s-0031-1291177
PMID:22009366
Abstract

There is significant interest in development of thyroid hormone analogues to harness specific properties as therapeutic agents for a variety of clinical indications including obesity, hypercholesterolemia, heart failure, and thyrotoxicosis. To date, most analogues have been designed to target liver specific effects, which can promote weight loss and lipid lowering through either tissue specific uptake or thyroid hormone receptor (TR) β isoform selectivity at the same time minimizing the unwanted cardiac and bone effects. We have developed a molecular biomarker assay to study the induction of the transcription of the cardiac specific α-myosin heavy chain (MHC) gene as a more sensitive and specific measure of thyroid hormone action on cardiac myocytes. We tested 5 TRβ and 1 TRα selective agonists as well as 2 putative TR antagonists in our α-MHC hnRNA assay. Using reverse transcription and polymerase chain reaction, we measured the induction of the α-MHC primary transcript in response to administration of drug. The TRα and only 2 of the TRβ agonists were highly active, when compared to the effect of T3, at the level of the cardiac myocyte. In addition, our data suggests that the reason that the antagonist NH-3 is not able to block the T3-mediated induction of α-MHC is that it does not get transported into the cardiac myocyte. Our data suggest that this assay will be useful in preclinical studies of the potential cardiac specific effects of thyroid hormone analogues and that predictions of function based on structure are not necessarily accurate or complete.

摘要

人们对甲状腺激素类似物的开发非常感兴趣,希望将其作为治疗各种临床病症的特效药物,这些病症包括肥胖症、高胆固醇血症、心力衰竭和甲状腺毒症等。迄今为止,大多数类似物的设计旨在针对肝脏的特异性作用,通过组织特异性摄取或甲状腺激素受体(TR)β同工型选择性,同时最大程度地减少不必要的心脏和骨骼效应,从而促进体重减轻和降低血脂。我们开发了一种分子生物标志物测定法,用于研究心脏特异性α-肌球蛋白重链(MHC)基因转录的诱导,作为更敏感和特异的甲状腺激素对心肌细胞作用的衡量指标。我们在α-MHC hnRNA 测定法中测试了 5 种 TRβ和 1 种 TRα选择性激动剂以及 2 种假定的 TR 拮抗剂。我们使用逆转录和聚合酶链反应,测量了药物给药后α-MHC 初级转录物的诱导。与 T3 的作用相比,TRα和仅有的 2 种 TRβ激动剂在心肌细胞水平上具有很高的活性。此外,我们的数据表明,拮抗剂 NH-3 不能阻断 T3 介导的α-MHC 诱导的原因是它不能被转运到心肌细胞中。我们的数据表明,该测定法将有助于甲状腺激素类似物潜在心脏特异性作用的临床前研究,并且基于结构的功能预测不一定准确或完整。

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Cardiac specific effects of thyroid hormone analogues.甲状腺激素类似物的心脏特异性作用。
Horm Metab Res. 2011 Oct;43(11):737-42. doi: 10.1055/s-0031-1291177. Epub 2011 Oct 18.
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Curr Chem Genom Transl Med. 2014 Mar 7;8:36-46. doi: 10.2174/2213988501408010036. eCollection 2014.
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Thyroid hormone analogues for the treatment of metabolic disorders: new potential for unmet clinical needs?甲状腺激素类似物治疗代谢紊乱:新的潜在未满足的临床需求?
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