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2022 年肝脏纤维化:未满足的需求和未来蓝图。

Hepatic fibrosis 2022: Unmet needs and a blueprint for the future.

机构信息

Division of Liver DiseasesIcahn School of Medicine at Mount SinaiNew YorkNew YorkUSA.

Institute for Liver and Digestive HealthUniversity College LondonLondonUK.

出版信息

Hepatology. 2022 Feb;75(2):473-488. doi: 10.1002/hep.32285. Epub 2022 Jan 11.


DOI:10.1002/hep.32285
PMID:34923653
Abstract

Steady progress over four decades toward understanding the pathogenesis and clinical consequences of hepatic fibrosis has led to the expectation of effective antifibrotic drugs, yet none has been approved. Thus, an assessment of the field is timely, to clarify priorities and accelerate progress. Here, we highlight the successes to date but, more importantly, identify gaps and unmet needs, both experimentally and clinically. These include the need to better define cell-cell interactions and etiology-specific elements of fibrogenesis and their link to disease-specific drivers of portal hypertension. Success in treating viral hepatitis has revealed the remarkable capacity of the liver to degrade scar in reversing fibrosis, yet we know little of the mechanisms underlying this response. Thus, there is an exigent need to clarify the cellular and molecular mechanisms of fibrosis regression in order for therapeutics to mimic the liver's endogenous capacity. Better refined and more predictive in vitro and animal models will hasten drug development. From a clinical perspective, current diagnostics are improving but not always biologically plausible or sufficiently accurate to supplant biopsy. More urgently, digital pathology methods that leverage machine learning and artificial intelligence must be validated in order to capture more prognostic information from liver biopsies and better quantify the response to therapies. For more refined treatment of NASH, orthogonal approaches that integrate genetic, clinical, and pathological data sets may yield treatments for specific subphenotypes of the disease. Collectively, these and other advances will strengthen and streamline clinical trials and better link histologic responses to clinical outcomes.

摘要

在过去的四十年中,人们在理解肝纤维化的发病机制和临床后果方面取得了稳步进展,这使得人们期待能有一种有效的抗纤维化药物,但目前还没有一种药物获得批准。因此,对该领域进行评估是及时的,可以明确优先事项并加速进展。在这里,我们重点介绍了迄今为止的成功,但更重要的是,确定了实验和临床方面的差距和未满足的需求。这些需求包括需要更好地定义细胞-细胞相互作用和纤维化发生的病因特异性因素,以及它们与门脉高压疾病特异性驱动因素的联系。在治疗病毒性肝炎方面取得的成功揭示了肝脏在逆转纤维化方面降解疤痕的惊人能力,但我们对这种反应的机制知之甚少。因此,迫切需要阐明纤维化消退的细胞和分子机制,以便治疗方法能够模仿肝脏的内源性能力。更好的、更精确的、更具预测性的体外和动物模型将加速药物开发。从临床角度来看,目前的诊断方法正在不断改进,但在生物学上并不总是合理的,也不够准确,无法替代活检。更迫切的是,必须验证数字病理学方法,这些方法利用机器学习和人工智能,以便从肝活检中获取更多的预后信息,并更好地量化对治疗的反应。为了更精细地治疗 NASH,可以整合遗传、临床和病理数据集的正交方法可能会为疾病的特定亚表型提供治疗方法。总的来说,这些和其他进展将加强和简化临床试验,并更好地将组织学反应与临床结果联系起来。

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本文引用的文献

[1]
Repositioning of a novel GABA-B receptor agonist, AZD3355 (Lesogaberan), for the treatment of non-alcoholic steatohepatitis.

Sci Rep. 2021-10-21

[2]
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Sci Transl Med. 2021-10-20

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Cirrhosis regression is associated with improved clinical outcomes in patients with nonalcoholic steatohepatitis.

Hepatology. 2022-5

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Cell. 2021-9-2

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Artif Intell Rev. 2022

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Diet-Induced Models of Non-Alcoholic Fatty Liver Disease: Food for Thought on Sugar, Fat, and Cholesterol.

Cells. 2021-7-16

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A Machine Learning Approach to Liver Histological Evaluation Predicts Clinically Significant Portal Hypertension in NASH Cirrhosis.

Hepatology. 2021-12

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Liver-fibrosis-activated transcriptional networks govern hepatocyte reprogramming and intra-hepatic communication.

Cell Metab. 2021-8-3

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Microscopic examination of spatial transcriptome using Seq-Scope.

Cell. 2021-6-24

[10]
Integrating Spatial Transcriptomics and Single-Cell RNA-seq Reveals the Gene Expression Profling of the Human Embryonic Liver.

Front Cell Dev Biol. 2021-5-20

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