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吡非尼酮对心脏病和糖尿病改变的功能及结构影响。

Functional and structural impact of pirfenidone on the alterations of cardiac disease and diabetes mellitus.

作者信息

Avila Guillermo, Osornio-Garduño Diana Stephanie, Ríos-Pérez Erick Benjamín, Ramos-Mondragón Roberto

机构信息

Department of Biochemistry, Cinvestav-IPN, AP 14-740, México City, DF 07000, Mexico.

Department of Biochemistry, Cinvestav-IPN, AP 14-740, México City, DF 07000, Mexico.

出版信息

Cell Calcium. 2014 Nov;56(5):428-35. doi: 10.1016/j.ceca.2014.07.008. Epub 2014 Jul 23.

Abstract

A synthetic compound, termed pirfenidone (PFD), is considered promising for the treatment of cardiac disease. It leads to beneficial effects in animal models of diabetes mellitus (DM); as well as in heart attack, atrial fibrillation, muscular dystrophy, and diabetic cardiomyopathy (DC). The latter is a result of alterations linked to metabolic syndrome as they promote cardiac hypertrophy, fibrosis and contractile dysfunction. Although reduced level of fibrosis and stiffness represent an essential step in the mechanism of PFD action, a wide range of functional effects might also contribute to the therapeutic benefits. For example, PFD stimulates L-type voltage-gated Ca(2+) channels (LTCCs), which are pivotal for a process known as excitation-contraction coupling (ECC). Recent evidence suggests that these two types of actions - namely structural and functional - aid in treating both cardiac disease and DM. This view is supported by the fact that in DC, for example, systolic dysfunction arises from both cardiac stiffness linked to fibrosis and down-regulation of ECC. Thus, not surprisingly, clinical trials have been conducted with PFD in the settings of DM, for treating not only cardiac but also renal disease. This review presents all these concepts, along with the possible mechanisms and pathophysiological consequences.

摘要

一种名为吡非尼酮(PFD)的合成化合物被认为在心脏病治疗方面颇具前景。它在糖尿病(DM)动物模型以及心脏病发作、心房颤动、肌肉萎缩症和糖尿病性心肌病(DC)中均产生有益效果。后者是与代谢综合征相关的改变所致,因为这些改变会促进心脏肥大、纤维化和收缩功能障碍。尽管纤维化程度降低和僵硬程度减轻是PFD作用机制中的关键步骤,但广泛的功能效应可能也有助于其治疗益处。例如,PFD可刺激L型电压门控钙通道(LTCCs),而这些通道对于一个称为兴奋 - 收缩偶联(ECC)的过程至关重要。最近的证据表明,这两种作用——即结构作用和功能作用——有助于治疗心脏病和DM。例如,在DC中,收缩功能障碍源于与纤维化相关的心脏僵硬以及ECC的下调,这一事实支持了这一观点。因此,毫不奇怪,已经在DM背景下开展了使用PFD的临床试验,用于治疗不仅是心脏病,还有肾病。本综述介绍了所有这些概念,以及可能的机制和病理生理后果。

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