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

O. Lowe, Kirstin; E. Tanase, Constantin; Maghami, Susan; E. Fisher, Leanne; M. Ghaemmaghami, Amir

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Authors

Kirstin O. Lowe

Constantin E. Tanase

Susan Maghami

Leanne E. Fisher



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.

Citation

O. Lowe, K., E. Tanase, C., Maghami, S., E. Fisher, L., & M. Ghaemmaghami, A. (2023). Inflammatory Network of Liver Fibrosis and How It Can Be Targeted Therapeutically. Immuno, 3(4), 375-408. https://doi.org/10.3390/immuno3040023

Journal Article Type Review
Acceptance Date Nov 22, 2023
Online Publication Date Nov 28, 2023
Publication Date Nov 28, 2023
Deposit Date Jun 27, 2024
Publicly Available Date Jun 27, 2024
Journal Immuno
Electronic ISSN 2673-5601
Publisher MDPI
Peer Reviewed Peer Reviewed
Volume 3
Issue 4
Pages 375-408
DOI https://doi.org/10.3390/immuno3040023
Public URL https://nottingham-repository.worktribe.com/output/27871782
Publisher URL https://www.mdpi.com/2673-5601/3/4/23

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