Macrophage Phenotype in Liver Injury and Repair

Sun, Ying‐Yin; Li, Xiaofeng; Meng, Xiao‐Ming; Huang, Cheng; Zhang, Lei; Li, Jun

doi:10.1111/sji.12468

Cited by 95 publications

(73 citation statements)

References 90 publications

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“…HCs and KCs also play an important role in liver fibrosis. Damaged HCs or activated KCs can secrete TGF‐β1, one of the strongest pro‐fibrosis factors, and accelerate the activation of HSCs (Jiang et al, ; Sun et al, ). It was shown that NOX1, NOX2, NOX4 were expressed in HCs and HSCs, whereas only NOX2 was expressed in KCs.…”

Section: Discussionmentioning

confidence: 99%

Ursolic acid ameliorates CCl4‐induced liver fibrosis through the NOXs/ROS pathway

Gan

Zhang

Huang

et al. 2018

Journal Cellular Physiology

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Liver fibrosis is a reversible wound‐healing response that occurs after liver injury. NADPH oxidases (NOXs) and reactive oxygen species (ROS) which are expressed in hepatocytes (HCs), hepatic stellate cells (HSCs), and Kupffer cells (KCs) play an important role in the development of hepatic fibrosis. In in vitro studies, we had shown that ursolic acid (UA) could reverse liver fibrosis by inhibiting the activation of NOX‐mediated fibrotic signaling networks in HSCs. In this study, we verified that UA could alleviate CCl4‐induced liver fibrosis by reducing the expression of NOXs/ROS in HCs, HSCs, KCs. Meanwhile, the phagocytic index α and clearance index K which represent phagocytosis of KCs were unchanged. Together, all our data demonstrated that UA induced the proliferation of HCs, promoted apoptosis in HSCs, and prevented activation of KCs in vivo by reducing the expression of NOXs/ROS in HCs, HSCs, KCs. Besides, UA had no effect on the host defense function.

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Section: Discussionmentioning

confidence: 99%

Ursolic acid ameliorates CCl4‐induced liver fibrosis through the NOXs/ROS pathway

Gan

Zhang

Huang

et al. 2018

Journal Cellular Physiology

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“…We then tested whether HO-1 deletion would affect macrophage polarization in vivo in a model of warm liver IRI, where macrophage phenotypes play a critical role in the degree of tissue damage and repair (10). Groups of mHO-1-KO and control mice were subjected to partial (75%) warm hepatic IRI for 90 minutes.…”

Section: Mho-1-ko Mice Exhibit Full Deletion Of Ho-1 In Macrophagesmentioning

confidence: 99%

“…Classically activated macrophages (M1) are proinflammatory, while alternatively activated macrophages (M2) harbor an antiinflammatory phenotype, often after upregulation of HO-1 (8,9). Increasing evidence supports the importance of M1/M2 polarization in tissue injury and repair in liver (10), heart (11), and kidney (12). In addition, it has been reported that resolvin D1 (13) and microRNA-155 deficiency (14) ameliorate liver IRI by inducing M2 polarization.…”

Section: Introductionmentioning

confidence: 99%

Myeloid HO-1 modulates macrophage polarization and protects against ischemia-reperfusion injury

Zhang¹,

Nakamura

Kageyama

et al. 2018

JCI Insight

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“…28,29 Diverse macrophage populations, based on their transcriptional profile and functions, have been observed in liver. 1,30,31 For example, restorative macrophages present after CCl 4induced liver injury have antifibrotic properties 25 and different gene signatures than restorative macrophages present after acetaminophen (APAP)-induced liver injury. [32][33][34] Several studies have also addressed the time course of hepatic macrophage changes in response to liver injury.…”

Section: Diverse Functions Of Hepatic Macrophages More Than M1 and Mmentioning

confidence: 99%

Regulation of Hepatic Inflammation via Macrophage Cell Death

Weinman

2018

Semin Liver Dis

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Macrophages are innate immune cells with diverse functions including clearing infectious agents, inducing inflammation and fibrosis, resolving fibrosis, and restoring tissue integrity. Liver macrophages consist of both resident Kupffer cells and infiltrating macrophages. They have heterogeneous highly plastic phenotypes, and they change their phenotypes rapidly in response to a diverse array of signals present in the injured or recovering liver. Cell death by apoptosis, necroptosis, or pyroptosis is a common response of liver macrophages to infectious and toxic insults. At the same time, the uptake of apoptotic and other dead cells, efferocytosis, is mediated by a series of dead cell receptors including MerTK, TIM4, and Stablin-1. These generate a critical signal that determines macrophage phenotype evolution. This review discusses the processes that lead to macrophage apoptosis and efferocytosis, and how these alter the course of liver diseases.

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Macrophage Phenotype in Liver Injury and Repair

Cited by 95 publications

References 90 publications

Ursolic acid ameliorates CCl4‐induced liver fibrosis through the NOXs/ROS pathway

Ursolic acid ameliorates CCl4‐induced liver fibrosis through the NOXs/ROS pathway

Myeloid HO-1 modulates macrophage polarization and protects against ischemia-reperfusion injury

Regulation of Hepatic Inflammation via Macrophage Cell Death

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