“Let my liver rather heat with wine” - a review of hepatic fibrosis pathophysiology and emerging therapeutics

IF 2.6 Q2 GASTROENTEROLOGY & HEPATOLOGY

Hepatic Medicine : Evidence and Research Pub Date : 2019-09-01 DOI:10.2147/HMER.S213397

C. G. Moscoso, C. Steer

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引用次数: 4

Abstract

Abstract Cirrhosis is characterized by extensive hepatic fibrosis, and it is the 14th leading cause of death worldwide. Numerous contributing conditions have been implicated in its development, including infectious etiologies, medication overdose or adverse effects, ingestible toxins, autoimmunity, hemochromatosis, Wilson’s disease and primary biliary cholangitis to list a few. It is associated with portal hypertension and its stigmata (varices, ascites, hepatic encephalopathy, combined coagulopathy and thrombophilia), and it is a major risk factor for hepatocellular carcinoma. Currently, orthotopic liver transplantation has been the only curative modality to treat cirrhosis, and the scarcity of donors results in many people waiting years for a transplant. Identification of novel targets for pharmacologic therapy through elucidation of key mechanistic components to induce fibrosis reversal is the subject of intense research. Development of robust models of hepatic fibrosis to faithfully characterize the interplay between activated hepatic stellate cells (the principal fibrogenic contributor to fibrosis initiation and perpetuation), hepatocytes and extracellular matrix components has the potential to identify critical components and mechanisms that can be exploited for targeted treatment. In this review, we will highlight key cellular pathways involved in the pathophysiology of fibrosis from extracellular ligands, effectors and receptors, to nuclear receptors, epigenetic mechanisms, energy homeostasis and cytokines. Further, molecular pathways of hepatic stellate cell deactivation are discussed, including apoptosis, senescence and reversal or transdifferentiation to an inactivated state resembling quiescence. Lastly, clinical evidence of fibrosis reversal induced by biologics and small molecules is summarized, current compounds under clinical trials are described and efforts for treatment of hepatic fibrosis with mesenchymal stem cells are highlighted. An enhanced understanding of the rich tapestry of cellular processes identified in the initiation, perpetuation and resolution of hepatic fibrosis, driven principally through phenotypic switching of hepatic stellate cells, should lead to a breakthrough in potential therapeutic modalities.

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“让我的肝更热与酒”-回顾肝纤维化病理生理和新兴疗法

摘要肝硬化以广泛的肝纤维化为特征，是全球第14大死亡原因。它的发展涉及许多促成因素，包括感染病因、药物过量或不良反应、可摄入毒素、自身免疫、血色素沉着症、Wilson病和原发性胆汁性胆管炎等。它与门静脉高压及其症状（静脉曲张、腹水、肝性脑病、合并凝血障碍和血栓形成倾向）有关，是肝细胞癌的主要危险因素。目前，原位肝移植已成为治疗肝硬化的唯一治疗方式，而供体的稀缺导致许多人等待移植数年。通过阐明诱导纤维化逆转的关键机制成分来鉴定药物治疗的新靶点是深入研究的主题。开发强大的肝纤维化模型，忠实地表征活化的肝星状细胞（纤维化开始和持续的主要纤维化因子）、肝细胞和细胞外基质成分之间的相互作用，有可能确定可用于靶向治疗的关键成分和机制。在这篇综述中，我们将重点介绍参与纤维化病理生理学的关键细胞途径，从细胞外配体、效应物和受体，到核受体、表观遗传学机制、能量稳态和细胞因子。此外，还讨论了肝星状细胞失活的分子途径，包括凋亡、衰老和逆转或转分化为类似静止的失活状态。最后，总结了生物制剂和小分子诱导的肝纤维化逆转的临床证据，描述了目前正在进行临床试验的化合物，并强调了间充质干细胞治疗肝纤维化的努力。对主要通过肝星状细胞表型转换驱动的肝纤维化的起始、持续和解决过程中发现的丰富的细胞过程的理解，应该会导致潜在治疗模式的突破。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Hepatic Medicine : Evidence and Research GASTROENTEROLOGY & HEPATOLOGY-

自引率

0.00%

发文量

审稿时长

16 weeks

期刊介绍： Hepatic Medicine: Evidence and Research is an international, peer-reviewed, open access, online journal. Publishing original research, reports, editorials, reviews and commentaries on all aspects of adult and pediatric hepatology in the clinic and laboratory including the following topics: Pathology, pathophysiology of hepatic disease Investigation and treatment of hepatic disease Pharmacology of drugs used for the treatment of hepatic disease Although the main focus of the journal is to publish research and clinical results in humans; preclinical, animal and in vitro studies will be published where they will shed light on disease processes and potential new therapies. Issues of patient safety and quality of care will also be considered. As of 1st April 2019, Hepatic Medicine: Evidence and Research will no longer consider meta-analyses for publication.