Hepatic macrophages in liver homeostasis and diseases-diversity, plasticity and therapeutic opportunities

Wen, Yankai; Lambrecht, Joeri; Ju, Cynthia; Tacke, Frank

doi:10.1038/s41423-020-00558-8

Cited by 342 publications

(341 citation statements)

References 240 publications

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“…Innate immune cells (mainly neutrophils, monocytes and macrophages) are primed to detect tissue damaging or infectious insults, and therefore are key orchestrators of inflammatory responses. During progression of CLD these cells initiate and drive both liver and systemic inflammation by recognising/responding to damage-associated molecular patterns (DAMPs) released from injured/activated liver cells and/or pathogen-associated molecular patterns (PAMPs) (16). Fibrosis occurs following chronic liver injury from an insult (toxic, metabolic, or infectious) which can perpetuate inflammation.…”

Section: Systemic Inflammation and Immune Dysfunction In Cirrhosismentioning

confidence: 99%

“…Circulating monocytes, a key component of the mononuclear phagocyte immune system, play pivotal roles in defence against infections and contribute to the systemic inflammation in chronic liver failure. In addition, they augment the local macrophage pool via their recruitment to inflammatory sites after a sterile/tissue-damaging or infectious insult to the liver (10,16,25). Human monocytes are divided into three major subsets: classical (CD14 + CD16 − ), intermediate (CD14 + CD16 + ) and nonclassical (CD14 dim CD16 + ).…”

Section: Monocyte Dysfunction In Chronic Liver Failurementioning

confidence: 99%

“…Macrophages are the most abundant hepatic immune cells with pivotal roles: from maintaining liver homeostasis and immune tolerance in the face of continuous exposure to harmless gutderived antigens from food and commensal microbes or their products, to rapidly identifying pathogens and orchestrating immune responses for their elimination (16). In addition, they are functionally important for clearing cellular debris and metabolic waste, and regulating iron and cholesterol homeostasis (16). During steady state, the predominant macrophage population comprises resident Kupffer cells (KCs) which are capable of self-renewal and have a specific transcriptional program defined by their unique niche (44)(45)(46).…”

Section: A Liver Macrophages In Steady Statementioning

confidence: 99%

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Macrophages in Chronic Liver Failure: Diversity, Plasticity and Therapeutic Targeting

Singanayagam

Triantafyllou

2021

Front. Immunol.

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Chronic liver injury results in immune-driven progressive fibrosis, with risk of cirrhosis development and impact on morbidity and mortality. Persistent liver cell damage and death causes immune cell activation and inflammation. Patients with advanced cirrhosis additionally experience pathological bacterial translocation, exposure to microbial products and chronic engagement of the immune system. Bacterial infections have a high incidence in cirrhosis, with spontaneous bacterial peritonitis being the most common, while the subsequent systemic inflammation, organ failure and immune dysregulation increase the mortality risk. Tissue-resident and recruited macrophages play a central part in the development of inflammation and fibrosis progression. In the liver, adipose tissue, peritoneum and intestines, diverse macrophage populations exhibit great phenotypic and functional plasticity determined by their ontogeny, epigenetic programming and local microenvironment. These changes can, at different times, promote or ameliorate disease states and therefore represent potential targets for macrophage-directed therapies. In this review, we discuss the evidence for macrophage phenotypic and functional alterations in tissue compartments during the development and progression of chronic liver failure in different aetiologies and highlight the potential of macrophage modulation as a therapeutic strategy for liver disease.

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Section: Systemic Inflammation and Immune Dysfunction In Cirrhosismentioning

confidence: 99%

Section: Monocyte Dysfunction In Chronic Liver Failurementioning

confidence: 99%

Section: A Liver Macrophages In Steady Statementioning

confidence: 99%

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Macrophages in Chronic Liver Failure: Diversity, Plasticity and Therapeutic Targeting

Singanayagam

Triantafyllou

2021

Front. Immunol.

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“…This recruitment of pro-inflammatory cells, which significantly changes the immune cell composition of the liver during NAFLD, may occur via various chemoattractant-axes, including the CCL2/CCR2, CCL1/CCR8, CXCR6/CXCL16, and CCL25/CCR9-pathways, with the chemoattractants being secreted by activated Kupffer cells, liver sinusoidal endothelial cells, and hepatic stellate cells. Besides the enhanced recruitment, also an enhanced polarization of macrophages toward a pro-inflammatory (“M1-like”) phenotype can be observed, potentially caused by stimulating cytokines such as TNF and IFN-γ ( 30 , 32 ).…”

Section: Inflammatory Processes During Nashmentioning

confidence: 99%

“…Many experimental studies revealed that the “sterile” inflammation observed during NAFLD leads to a perpetuation of liver disease. Indeed, studies depleting certain types of immune cells ( 36 , 37 ), or blocking the polarization and recruitment of inflammatory cells, have led to significant alleviation of fibrosis in various mouse models and early-stage clinical trials ( 32 ). However, it should not be forgotten that the inflammatory response is also crucial for healing and tissue repair, often observed during the early stages of liver injury ( 38 ).…”

Section: Inflammatory Processes During Nashmentioning

confidence: 99%

Controversies and Opportunities in the Use of Inflammatory Markers for Diagnosis or Risk Prediction in Fatty Liver Disease

Lambrecht

Tacke

2021

Front. Immunol.

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In the Western society, non-alcoholic fatty liver disease (NAFLD), characterized by the excessive accumulation of fat in the liver, represents the most common cause of chronic liver disease. If left untreated, approximately 15%–20% of patients with NAFLD will progress to non-alcoholic steatohepatitis (NASH), in which lobular inflammation, hepatocyte ballooning and fibrogenesis further contribute to a distorted liver architecture and function. NASH initiation has significant effects on liver-related mortality, as even the presence of early stage fibrosis increases the chances of adverse patient outcome. Therefore, adequate diagnostic tools for NASH are needed, to ensure that relevant therapeutic actions can be taken as soon as necessary. To date, the diagnostic gold standard remains the invasive liver biopsy, which is associated with several drawbacks such as high financial costs, procedural risks, and inter/intra-observer variability in histology analysis. As liver inflammation is a major hallmark of disease progression, inflammation-related circulating markers may represent an interesting source of non-invasive biomarkers for NAFLD/NASH. Examples for such markers include cytokines, chemokines or shed receptors from immune cells, circulating exosomes related to inflammation, and changing proportions of peripheral blood mononuclear cell (PBMC) subtypes. This review aims at documenting and critically discussing the utility of such novel inflammatory markers for NAFLD/NASH-diagnosis, patient stratification and risk prediction.

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Fatty Liver/Adipose Tissue Dual‐Targeting Nanoparticles with Heme Oxygenase‐1 Inducer for Amelioration of Obesity, Obesity‐Induced Type 2 Diabetes, and Steatohepatitis

Hong

Kim

2022

Advanced Science

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Persistent uptake of high‐calorie diets induces the storage of excessive lipid in visceral adipose tissue. Lipids secreted from obese adipose tissue are accumulated in peripheral tissues such as the liver, pancreas, and muscle, and impair insulin sensitivity causing type 2 diabetes mellitus (T2DM). Furthermore, the accumulation of inflammatory cytokines and lipids in the liver induces apoptosis and fibrogenesis, and ultimately causes nonalcoholic steatohepatitis (NASH). To modulate obese tissue environments, it is challenged to selectively deliver inducers of heme oxygenase‐1 (HO‐1) to adipose tissue with the aid of a prohibitin targeting drug delivery system. Prohibitin binding peptide (PBP), an oligopeptide targeting prohibitin rich in adipose tissue, is conjugated on the surface of Hemin‐ or CoPP‐loaded poly(lactide‐co‐glycolide) nanoparticles (PBP‐NPs). PBP‐NPs efficiently differentiate lipid storing white adipocytes into energy‐generating brown adipocytes in T2DM and NASH models. In addition, PBP‐NPs are found to target prohibitin overexpressed fatty liver in the NASH model and inhibit hepatic uptake of circulating lipids. Furthermore, PBP‐NPs switch phenotypes of inflammatory macrophages in damaged organs and lower inflammation. Taken together, dual‐targeted induction of HO‐1 in fatty adipose and liver tissues is proven to be a promising therapeutic strategy to ameliorate obesity, insulin resistance, and steatohepatitis by lowering lipids and cytokines.

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Hepatic macrophages in liver homeostasis and diseases-diversity, plasticity and therapeutic opportunities

Cited by 342 publications

References 240 publications

Macrophages in Chronic Liver Failure: Diversity, Plasticity and Therapeutic Targeting

Macrophages in Chronic Liver Failure: Diversity, Plasticity and Therapeutic Targeting

Controversies and Opportunities in the Use of Inflammatory Markers for Diagnosis or Risk Prediction in Fatty Liver Disease

Fatty Liver/Adipose Tissue Dual‐Targeting Nanoparticles with Heme Oxygenase‐1 Inducer for Amelioration of Obesity, Obesity‐Induced Type 2 Diabetes, and Steatohepatitis

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