Organ–Organ Crosstalk and Alcoholic Liver Disease

Poole, Lauren G.; Dolin, Christine E.; Arteel, Gavin E.

doi:10.3390/biom7030062

Cited by 37 publications

(25 citation statements)

References 105 publications

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“…79 Endocrine adiponectin-FGF15/19 axis controls adipose and gut to liver communication arm of an adipose-intestine-liver partnership in response to alcohol challenges. However, other organs such as muscle, bone, spleen and brain may be within this communication axis regulated by the adiponectin-FGF15/19 axis and ethanol.…”

Section: Discussionmentioning

confidence: 99%

Endocrine Adiponectin‐FGF15/19 Axis in Ethanol-Induced Inflammation and Alcoholic Liver Injury

et al. 2018

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Alcoholic liver disease (ALD) is the most prevalent form of liver diseases, encompassing a spectrum of progressive pathological changes from steatosis to steatohepatitis to fibrosis/cirrhosis and hepatocellular carcinoma. Alcoholic steatosis/steatohepatitis is the initial stage of ALD and a major risk factor for advanced liver injuries. Adiponectin is a hormone secreted from adipocytes. Fibroblast growth factor (FGF) 15 (human homolog, FGF19) is an ileum-derived hormone. Adipocyte-derived adiponectin and gut-derived FGF15/19 regulate each other, share common signaling cascades and exert similar beneficial functions. Emerging evidence has revealed that dysregulated adiponecitn-FGF15/19 axis and impaired hepatic adiponectin-FGF15/19 signaling are associated with alcoholic liver damage in rodents and humans. More importantly, endocrine adiponectin-FGF15/19 signaling confers protection against ethanol-induced liver damage via fine-tuning the adipose-intestine-liver crosstalk, leading to limited hepatic inflammatory responses, and ameliorated alcoholic liver injury. This review is focused on the recently discovered endocrine adiponectin-FGF15/19 axis that is emerging as an essential adipose-gut-liver coordinator involved in the development and progression of alcoholic steatohepatitis.

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Section: Discussionmentioning

confidence: 99%

Endocrine Adiponectin‐FGF15/19 Axis in Ethanol-Induced Inflammation and Alcoholic Liver Injury

et al. 2018

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“…[38][39][40][41][42] No matter the etiology, chronic liver diseases share a well-documented, common natural history, which ranges initially from simple steatosis, to inflammation and necrosis (steatohepatitis), to fibrosis and cirrhosis. [43][44][45][46] Fibrosis may improve with removal of insult, but reversal of severe stages of fibrosis/cirrhosis is more limited. 47 Cirrhosis is often considered an end-stage liver disease and requires liver transplant.…”

Section: Inflammation As a Therapeutic Target For Chronic Liver Diseasementioning

confidence: 99%

“…[63][64][65] We recently demonstrated that the hepatic matrisome changes robustly to acute injury (e.g., acute lipopolysaccharide), even under conditions in which the ECM appears histologically unchanged. 45 These subhistologic transitional changes to the matrisome appear to resolve after acute injury 66,67 (►Fig. 1); with chronic injury, the transitional matrisome is replaced by collagenous scarring in the liver, which is again in-line with subcutaneous wound healing.…”

Section: Before Fibrosismentioning

confidence: 99%

The Matrisome, Inflammation, and Liver Disease

Dolin

Arteel

2020

Semin Liver Dis

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Chronic fatty liver disease is common worldwide. This disease is a spectrum of disease states, ranging from simple steatosis (fat accumulation) to inflammation, and eventually to fibrosis and cirrhosis if untreated. The fibrotic stage of chronic liver disease is primarily characterized by robust accumulation of extracellular matrix (ECM) proteins (collagens) that ultimately impairs the function of the organ. The role of the ECM in early stages of chronic liver disease is less well-understood, but recent research has demonstrated that several changes in the hepatic ECM in prefibrotic liver disease are not only present but may also contribute to disease progression. The purpose of this review is to summarize the established and proposed changes to the hepatic ECM that may contribute to inflammation during earlier stages of disease development, and to discuss potential mechanisms by which these changes may mediate the progression of the disease.

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“…This can be explained through the well-known classic example of hepatic encephalopathy during decompensation of chronic liver disease and alcoholic liver disease. 29 This crosstalk is linked through gut-related pathological changes such as increased permeability, altered microbiome of the gut, leading to "gut dysbiosis." 30 The brain essentially requires glucose for its metabolism which is generated in high amounts by the liver.…”

Section: Liver and Brain Crosstalkmentioning

confidence: 99%

Brain Crosstalk with Other Organs in ICU Patient

Saran

Gurjar

2019

Journal of Neuroanaesthesiology and Critical Care

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Crosstalk between various organs exists in the human body. This can be part of physiological reflexes such as cardiac reflexes that protect the organs during stressful stimuli or can be part of pathological conditions where an insult to an organ releases cytokines that cause distant effects on other organs. In critically ill patients, these crosstalks are independent of pre-existing common risk factors or the presence of new risk exposure during the treatment. Crosstalk can manifest in series or parallel. The human brain, being a control center of the human body, does crosstalk with almost every organ in the body. In this narrative review, crosstalk of the brain with various organs and systems such as the heart, lungs, liver, kidneys, gut, muscle, bone, skin, adipose tissue, and immune system is being discussed along with clinical manifestations and management. Future research might help to target these pathological processes in preventing progression of single-organ dysfunction to multi-organ failures in critically ill patients.

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Organ–Organ Crosstalk and Alcoholic Liver Disease

Cited by 37 publications

References 105 publications

Endocrine Adiponectin‐FGF15/19 Axis in Ethanol-Induced Inflammation and Alcoholic Liver Injury

Endocrine Adiponectin‐FGF15/19 Axis in Ethanol-Induced Inflammation and Alcoholic Liver Injury

The Matrisome, Inflammation, and Liver Disease

Brain Crosstalk with Other Organs in ICU Patient

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