趋化因子系统在肝纤维化中的作用:综述。

Digestive medicine research Pub Date : 2022-06-01 Epub Date: 2022-06-30 DOI:10.21037/dmr-21-87
Kyle L Poulsen, Christina K Cajigas-Du Ross, Jarod K Chaney, Laura E Nagy
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引用次数: 6

摘要

背景与目的:肝纤维化是一种具有异常伤口愈合反应特征的疾病。纤维化通常是慢性肝病的终末期,如酒精相关肝病(ALD)、代谢相关肝病、病毒性肝炎和肝脏自身免疫性疾病。先天免疫通过产生促炎介质、白细胞浸润和组织损伤等多种机制参与许多疾病的进展。趋化因子及其受体协调组织中免疫细胞的积累和激活,并与多种肝脏疾病相关;然而,对它们在肝纤维化中的潜在作用知之甚少。这是一篇关于趋化因子生物学与肝纤维化关系的当前知识的叙述性综述,并对未来可能探索的潜在治疗机会进行了深入研究。方法:对PubMed检索1993 - 2021年间发表的关于趋化因子生物学、慢性肝病和肝纤维化的相关英文研究和文本进行全面的文献回顾。该综述的撰写和构建详细介绍了有趣的趋化因子生物学,趋化因子与组织损伤和解决的关系,并确定了纤维化治疗的发现领域。关键内容和发现:趋化因子与许多慢性肝脏疾病有关,无论病因如何。如果没有适当的治疗,这些疾病大多会发展为纤维化。趋化因子对肝脏疾病和纤维化的作用是多种多样的,包括调节肝脏炎症的典型作用,以及通过激活肝星状细胞(hsc)直接促进纤维化。有限的临床证据表明,针对某些肝脏疾病的趋化因子可能为肝纤维化患者提供治疗益处。结论:在几乎所有疾病中,配体和受体的趋化因子系统是一个复杂的炎症信号网络。趋化因子和细胞靶标的特定来源为慢性肝脏疾病和已建立的纤维化提供了独特的病理生理后果。虽然大多数趋化因子是促炎的,并有助于组织损伤,但其他趋化因子可能有助于解决已建立的纤维化。迄今为止,针对趋化因子系统和肝脏疾病和/或纤维化的靶向治疗方法很少,进一步的研究可以确定可行的治疗方案,以改善终末期肝病患者的预后。
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Role of the chemokine system in liver fibrosis: a narrative review.

Background and objective: Liver fibrosis is a disease with characteristics of an aberrant wound healing response. Fibrosis is commonly the end-stage for chronic liver diseases like alcohol-associated liver disease (ALD), metabolic-associated liver disease, viral hepatitis, and hepatic autoimmune disease. Innate immunity contributes to the progression of many diseases through multiple mechanisms including production of pro-inflammatory mediators, leukocyte infiltration and tissue injury. Chemokines and their receptors orchestrate accumulation and activation of immune cells in tissues and are associated with multiple liver diseases; however, much less is known about their potential roles in liver fibrosis. This is a narrative review of current knowledge of the relationship of chemokine biology to liver fibrosis with insights into potential future therapeutic opportunities that can be explored in the future.

Methods: A comprehensive literature review was performed searching PubMed for relevant English studies and texts regarding chemokine biology, chronic liver disease and liver fibrosis published between 1993 and 2021. The review was written and constructed to detail the intriguing chemokine biology, the relation of chemokines to tissue injury and resolution, and identify areas of discovery for fibrosis treatment.

Key content and findings: Chemokines are implicated in many chronic liver diseases, regardless of etiology. Most of these diseases will progress to fibrosis without appropriate treatment. The contributions of chemokines to liver disease and fibrosis are diverse and include canonical roles of modulating hepatic inflammation as well as directly contributing to fibrosis via activation of hepatic stellate cells (HSCs). Limited clinical evidence suggests that targeting chemokines in certain liver diseases might provide a therapeutic benefit to patients with hepatic fibrosis.

Conclusions: The chemokine system of ligands and receptors is a complex network of inflammatory signals in nearly all diseases. The specific sources of chemokines and cellular targets lend unique pathophysiological consequences to chronic liver diseases and established fibrosis. Although most chemokines are pro-inflammatory and contribute to tissue injury, others likely aid in the resolution of established fibrosis. To date, very few targeted therapies exist for the chemokine system and liver disease and/or fibrosis, and further study could identify viable treatment options to improve outcomes in patients with end-stage liver disease.

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