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标题: 抗肝纖維化藥物的療效和安全性 [打印本页]

作者: StephenW    时间: 2020-11-27 19:50     标题: 抗肝纖維化藥物的療效和安全性

Efficacy and safety of anti-hepatic fibrosis drugs
Konstantinos Damiris  1 , Zaid H Tafesh  2 , Nikolaos Pyrsopoulos  3
Affiliations
Affiliations

    1
    Department of Medicine, Rutgers-New Jersey Medical School, Newark, NJ 07103, United States.
    2
    Medicine-Gastroenterology and Hepatology, Rutgers-New Jersey Medical School, Newark, NJ 07103, United States.
    3
    Medicine-Gastroenterology and Hepatology, Rutgers-New Jersey Medical School, Newark, NJ 07103, United States. [email protected].

    PMID: 33244194 PMCID: PMC7656211 DOI: 10.3748/wjg.v26.i41.6304

Abstract

Recent progress in our understanding of the pathways linked to progression from hepatic insult to cirrhosis has led to numerous novel therapies being investigated as potential cures and inhibitors of hepatic fibrogenesis. Liver cirrhosis is the final result of prolonged fibrosis, which is an intimate balance between fibrogenesis and fibrinolysis. A number of these complex mechanisms are shared across the various etiologies of liver disease. Thankfully, investigation has yielded some promising results in regard to reversal of fibrosis, particularly the indirect benefits associated with antiviral therapy for the treatment of hepatitis B and C and the farnesoid receptor agonist for the treatment of primary biliary cholangitis and metabolic associated fatty liver disease. A majority of current clinical research is focused on targeting metabolic associated fatty liver disease and its progression to metabolic steatohepatitis and ultimately cirrhosis, with some hope of potential standardized therapeutics in the near future. With our ever-evolving understanding of the underlying pathophysiology, these therapeutics focus on either controlling the primary disease (the initial trigger of fibrogenesis), interrupting receptor ligand interactions and other intracellular communications, inhibiting fibrogenesis, or even promoting resolution of fibrosis. It is imperative to thoroughly test these potential therapies with the rigorous standards of clinical therapeutic trials in order to ensure the highest standards of patient safety. In this article we will briefly review the key pathophysiological pathways that lead to liver fibrosis and present current clinical and experimental evidence that has shown reversibility of liver fibrosis and cirrhosis, while commenting on therapeutic safety.

Keywords: Antifibrotic; Cirrhosis; Clinical trial; Fibrosis; Liver; Pharmacotherapy; Safety.

©The Author(s) 2020. Published by Baishideng Publishing Group Inc. All rights reserved.
作者: StephenW    时间: 2020-11-27 19:51

抗肝纖維化藥物的療效和安全性
Konstantinos Damiris 1,Zaid H Tafesh 2,Nikolaos Pyrsopoulos 3
隸屬關係
隸屬關係

    1個
    羅格斯-新澤西醫學院的醫學系,紐瓦克,新澤西州07103,美國。
    2
    美國新澤西州紐瓦克市羅格斯-新澤西醫學院的醫學-胃腸病學和肝病學。
    3
    美國新澤西州紐瓦克市羅格斯-新澤西醫學院的醫學-胃腸病學和肝病學。 [email protected]

    PMID:33244194 PMCID:PMC7656211 DOI:10.3748 / wjg.v26.i41.6304

抽象

在我們對與從肝損傷到肝硬化發展相關的途徑的理解中的最新進展,導致人們研究了許多新療法,將其作為肝纖維化的潛在治療方法和抑製劑。肝硬化是長時間纖維化的最終結果,這是纖維形成與纖維蛋白溶解之間的密切平衡。這些複雜的機制中有許多是在肝病的各種病因中共享的。值得慶幸的是,有關纖維化逆轉的研究已經取得了一些令人鼓舞的結果,特別是與抗病毒治療乙型和丙型肝炎相關的間接益處以及法尼類受體激動劑用於治療原發性膽源性膽管炎和代謝性脂肪肝疾病。當前的大多數臨床研究都集中在針對代謝相關性脂肪肝疾病及其進展為代謝性脂肪性肝炎並最終發展為肝硬化,並希望在不久的將來有潛在的標準化療法。隨著我們對基本病理生理學的不斷發展的了解,這些療法的重點是控制原發疾病(纖維生成的最初觸發),中斷受體配體相互作用和其他細胞內通訊,抑制纖維生成,甚至促進纖維化的解決。必須以嚴格的臨床治療試驗標準對這些潛在療法進行全面測試,以確保達到最高的患者安全標準。在本文中,我們將簡要回顧導致肝纖維化的關鍵病理生理途徑,並提供當前的臨床和實驗證據,這些證據顯示出肝纖維化和肝硬化的可逆性,同時對治療安全性做出了評論。

關鍵字:抗纖維化;肝硬化;臨床試驗;纖維化;肝;藥物治療;安全。

©The 2020作者。百世登出版集團有限公司出版。保留所有權利。
作者: StephenW    时间: 2020-11-27 19:52

https://www.wjgnet.com/1007-9327/full/v26/i41/6304.htm




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