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从炎症到纤维化——心肌组织重塑的分子和细胞机制及差异化治疗机会展望

From Inflammation to Fibrosis-Molecular and Cellular Mechanisms of Myocardial Tissue Remodelling and Perspectives on Differential Treatment Opportunities.

作者信息

Suthahar Navin, Meijers Wouter C, Silljé Herman H W, de Boer Rudolf A

机构信息

Department of Cardiology, University Medical Center Groningen, University of Groningen, PO Box 30.001, 9700 RB, Groningen, The Netherlands.

出版信息

Curr Heart Fail Rep. 2017 Aug;14(4):235-250. doi: 10.1007/s11897-017-0343-y.

Abstract

PURPOSE OF REVIEW

In this review, we highlight the most important cellular and molecular mechanisms that contribute to cardiac inflammation and fibrosis. We also discuss the interplay between inflammation and fibrosis in various precursors of heart failure (HF) and how such mechanisms can contribute to myocardial tissue remodelling and development of HF.

RECENT FINDINGS

Recently, many research articles attempt to elucidate different aspects of the interplay between inflammation and fibrosis. Cardiac inflammation and fibrosis are major pathophysiological mechanisms operating in the failing heart, regardless of HF aetiology. Currently, novel therapeutic options are available or are being developed to treat HF and these are discussed in this review. A progressive disease needs an aggressive management; however, existing therapies against HF are insufficient. There is a dynamic interplay between inflammation and fibrosis in various precursors of HF such as myocardial infarction (MI), myocarditis and hypertension, and also in HF itself. There is an urgent need to identify novel therapeutic targets and develop advanced therapeutic strategies to combat the syndrome of HF. Understanding and describing the elements of the inflammatory and fibrotic pathways are essential, and specific drugs that target these pathways need to be evaluated.

摘要

综述目的

在本综述中,我们重点介绍了导致心脏炎症和纤维化的最重要细胞和分子机制。我们还讨论了炎症与纤维化在各种心力衰竭(HF)前驱疾病中的相互作用,以及这些机制如何导致心肌组织重塑和HF的发展。

最新发现

最近,许多研究文章试图阐明炎症与纤维化相互作用的不同方面。无论HF的病因如何,心脏炎症和纤维化都是衰竭心脏中的主要病理生理机制。目前,有新的治疗选择可供使用或正在开发用于治疗HF,本综述将对此进行讨论。一种进行性疾病需要积极的管理;然而,现有的HF治疗方法并不充分。在HF的各种前驱疾病如心肌梗死(MI)、心肌炎和高血压中,以及在HF本身中,炎症和纤维化之间存在动态相互作用。迫切需要确定新的治疗靶点并制定先进的治疗策略来对抗HF综合征。了解和描述炎症和纤维化途径的要素至关重要,需要评估针对这些途径的特定药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/062e/5527069/279ac0cea149/11897_2017_343_Fig1_HTML.jpg

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