Inflammatory Network of Liver Fibrosis and How It Can Be Targeted Therapeutically

Immuno Pub Date : 2023-11-28 DOI:10.3390/immuno3040023
Kirstin O. Lowe, Constantin E. Tanase, Susan Maghami, Leanne E. Fisher, Amir Ghaemmaghami
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Abstract

Liver fibrosis is a complex, dynamic process associated with a broad spectrum of chronic liver diseases and acute liver failure, characterised by the dysregulated intrahepatic production of extracellular matrix proteins replacing functional liver cells with scar tissue. Fibrosis progresses due to an interrelated cycle of hepatocellular injury, triggering a persistent wound-healing response. The accumulation of scar tissue and chronic inflammation can eventually lead to cirrhosis and hepatocellular carcinoma. Currently, no therapies exist to directly treat or reverse liver fibrosis; hence, it remains a substantial global disease burden. A better understanding of the intricate inflammatory network that drives the initiation and maintenance of liver fibrosis to enable the rationale design of new intervention strategies is required. This review clarifies the most current understanding of the hepatic fibrosis cellular network with a focus on the role of regulatory T cells, and a possible trajectory for T cell immunotherapy in fibrosis treatment. Despite good progress in elucidating the role of the immune system in liver fibrosis, future work to better define the function of different immune cells and their mediators at different fibrotic stages is needed, which will enhance the development of new therapies.
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肝纤维化的炎症网络及其治疗靶点
肝纤维化是一个复杂的动态过程,与多种慢性肝病和急性肝功能衰竭有关,其特点是肝内细胞外基质蛋白生成失调,瘢痕组织取代了功能性肝细胞。纤维化的发展是由于肝细胞损伤的相互关联的循环,引发了持续的伤口愈合反应。瘢痕组织的积累和慢性炎症最终会导致肝硬化和肝细胞癌。目前,还没有直接治疗或逆转肝纤维化的疗法;因此,肝纤维化仍然是全球疾病的沉重负担。我们需要更好地了解促使肝纤维化发生和维持的复杂炎症网络,以便合理地设计新的干预策略。本综述阐明了目前对肝纤维化细胞网络的最新认识,重点是调节性T细胞的作用,以及T细胞免疫疗法在肝纤维化治疗中的可能发展轨迹。尽管在阐明免疫系统在肝纤维化中的作用方面取得了良好进展,但未来的工作还需要更好地界定不同免疫细胞及其介质在不同纤维化阶段的功能,这将促进新疗法的开发。
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