Mechanisms of Liver Injury. II. Mechanisms of Neutrophil-induced Liver Cell Injury During Hepatic Ischemia-reperfusion and Other Acute Inflammatory Conditions

Overview

Journal Am J Physiol Gastrointest Liver Physiol

Publisher American Physiological Society

Specialties Gastroenterology
Physiology

Date 2006 May 12

PMID 16687579

Citations 194

Authors

Hartmut Jaeschke

Affiliations

Soon will be listed here.

Abstract

Polymorphonuclear leukocytes (neutrophils) are a vital part of the innate immune response to microbial infections and tissue trauma, e.g., ischemia-reperfusion injury, in many organs including the liver. However, an excessive inflammatory response can lead to a dramatic aggravation of the existing injury. To design interventions, which selectively target the detrimental effects of neutrophils, a detailed understanding of the pathophysiology is critical. Systemic or local exposure to proinflammatory mediators causes activation and priming of neutrophils for reactive oxygen formation and recruits them into the vascular beds of the liver without causing tissue injury. However, generation of a chemotactic signal from the parenchyma will trigger extravasation and an attack on target cells (e.g., hepatocytes). Adhesion to the target induces degranulation with release of proteases and formation of reactive oxygen species including hydrogen peroxide and hypochlorous acid, which can diffuse into hepatocytes and induce an intracellular oxidant stress and mitochondrial dysfunction. Various neutrophil-derived proteases are involved in transmigration and cell toxicity but can also promote the inflammatory response by processing of proinflammatory mediators. In addition, necrotic cells release mediators, e.g., high-mobility group box-1, which further promotes neutrophilic hepatitis and tissue damage. On the basis of these evolving insights into the mechanisms of neutrophil-mediated liver damage, the most selective strategies appear not to interfere with the cytotoxic potential of neutrophils, but rather strengthen the target cells' defense mechanisms including enhancement of the intracellular antioxidant defense systems, activation of cell survival pathways, or initiation of cell cycle activation and regeneration.

Citing Articles

Intestine-derived fibroblast growth factor 19 alleviates lipopolysaccharide-induced liver injury by regulating bile acid homeostasis and directly improving oxidative stress.

Tang X, Ning J, Zhao Y, Feng S, Shao L, Liu T J Intensive Med. 2025; 5(1):79-88.

PMID: 39872844 PMC: 11763227. DOI: 10.1016/j.jointm.2024.06.003.

Ferroptosis and Intrinsic Drug-induced Liver Injury by Acetaminophen and Other Drugs: A Critical Evaluation and Historical Perspective.

Jaeschke H, Ramachandran A J Clin Transl Hepatol. 2024; 12(12):1057-1066.

PMID: 39649034 PMC: 11622198. DOI: 10.14218/JCTH.2024.00324.

Exploring the effects of hypoxia and reoxygenation time on hepatocyte apoptosis and inflammation.

Xu X, Zhou T, Tulahong A, Ruze R, Shao Y PLoS One. 2024; 19(11):e0310535.

PMID: 39570857 PMC: 11581257. DOI: 10.1371/journal.pone.0310535.

Loss of β-catenin reveals a role for glutathione in regulating oxidative stress during cholestatic liver disease.

Balogun O, Shao D, Carson M, King T, Kosar K, Zhang R Hepatol Commun. 2024; 8(7.

PMID: 38967587 PMC: 11227358. DOI: 10.1097/HC9.0000000000000485.

Mesangial cell-derived CircRNAs in chronic glomerulonephritis: RNA sequencing and bioinformatics analysis.

Fan J, Li X Ren Fail. 2024; 46(2):2371059.

PMID: 38946402 PMC: 467094. DOI: 10.1080/0886022X.2024.2371059.