Dual‐Specificity Phosphatase 26 Protects Against Nonalcoholic Fatty Liver Disease in Mice Through Transforming Growth Factor Beta–Activated Kinase 1 Suppression

Ye, Ping; Liu, Jijun; Wu-ping, XU; Liu, Denghai; Ding, Xiangchao; Shen, Le; Zhang, Hao; Chen, Shanshan; Chen, Manhua; Xia, Jiahong

doi:10.1002/hep.30485

Cited by 45 publications

(41 citation statements)

References 45 publications

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“…4C) ( Fig. 3g) andaltered the expression of DUSP1 71 (Fig. 3g), in further support of the stress response induced by ethanol in the liver chip.…”

Section: Ethanol-induced Steatosis In the Liver-chipsupporting

confidence: 71%

Modeling alcoholic liver disease in a human Liver-Chip

Nawroth

et al. 2020

Preprint

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Fatty liver disease (FLD), is a major public health burden that affects up to 30% of people in Western countries and leads to progressive liver injury, comorbidities, and increased mortality. Key risk factors for developing FLD are obesity and alcohol consumption, both of which are growing in prevalence worldwide. There is an urgent need for human-relevant preclinical models to improve our understanding of FLD progression to steatohepatitis and for the development of sensitive noninvasive diagnostics and therapies. Alcohol-induced liver disease (ALD) represents an ideal case for modeling FDL as ethanol exposure is a comparatively simpler trigger for experimental induction of the pathology, as opposed to the complexity of modeling the diet- and life-style induced FLD. Further, despite their different root causes several common characteristics in disease progression and deterioration of liver function in the two disease entities, highlighting the potential of an ALD microphysiological model for broad application in translational research. Here, we leverage our recently reported human Liver-Chip for toxicity applications, to expand the capabilities of the platform for broad application in translational research. We report the first in vitro modeling of ALD that uses human relevant blood alcohol concentrations (BAC) and affords multimodal profiling of clinically relevant endpoints. Our ALD Liver-Chip recapitulates established FLD markers in response to ethanol in a concentration-dependent manner, including lipid accumulation and oxidative stress. Importantly, we show that the ALD Liver-Chip supports the study of secondary insults, as patients with advanced ALD often show high blood endotoxin levels due to alcohol-associated increased intestinal permeability and barrier dysfunction. Moreover, owing to new developments in the design, the ALD Liver-Chip enables the measurement of structural changes of the bile canaliculi (BC) network as a novel in vitro quantitative readout of alcoholic liver toxicity. In summary, we report the development of a human ALD Liver-Chip as a new platform for modeling the progression of alcohol-induced liver injury with direct translation to clinical research.

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“…4C) ( Fig. 3g) andaltered the expression of DUSP1 71 (Fig. 3g), in further support of the stress response induced by ethanol in the liver chip.…”

Section: Ethanol-induced Steatosis In the Liver-chipsupporting

confidence: 71%

Modeling alcoholic liver disease in a human Liver-Chip

Nawroth

et al. 2020

Preprint

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“…A more recent study showed that DUSP12, which plays an important role in brown adipocyte differentiation, physically binds to ASK1, promotes its dephosphorylation, and inhibits its action on p38α/β in order to reducelipogenesis and to suppress lipid accumulation in livers of high-fat fed mice [167]. Similar to DUSP12, DUSP14, DUSP26 and MKP-5 suppress the development of hepatic steatosis by inhibiting p38s [167][168][169][170]. Both DUSP14 and DUSP26 directly bind and dephosphorylate TAK1 kinase, which results in the inhibition of TAK1 and its downstream targets JNKs and p38s [168,169].…”

Section: The Role Of P38s In the Livermentioning

confidence: 99%

“…Similar to DUSP12, DUSP14, DUSP26 and MKP-5 suppress the development of hepatic steatosis by inhibiting p38s [167][168][169][170]. Both DUSP14 and DUSP26 directly bind and dephosphorylate TAK1 kinase, which results in the inhibition of TAK1 and its downstream targets JNKs and p38s [168,169]. MKP-5 prevents the development of hepatic steatosis by suppressing p38-ATF2 and p38-PPARγ signaling axis to reduce hepatic lipid accumulation [170].…”

Section: The Role Of P38s In the Livermentioning

confidence: 99%

Impact of Conventional and Atypical MAPKs on the Development of Metabolic Diseases

Kassouf

Sumara

2020

Biomolecules

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The family of mitogen-activated protein kinases (MAPKs) consists of fourteen members and has been implicated in regulation of virtually all cellular processes. MAPKs are divided into two groups, conventional and atypical MAPKs. Conventional MAPKs are further classified into four sub-families: extracellular signal-regulated kinases 1/2 (ERK1/2), c-Jun N-terminal kinase (JNK1, 2 and 3), p38 (α, β, γ, δ), and extracellular signal-regulated kinase 5 (ERK5). Four kinases, extracellular signal-regulated kinase 3, 4, and 7 (ERK3, 4 and 7) as well as Nemo-like kinase (NLK) build a group of atypical MAPKs, which are activated by different upstream mechanisms than conventional MAPKs. Early studies identified JNK1/2 and ERK1/2 as well as p38α as a central mediators of inflammation-evoked insulin resistance. These kinases have been also implicated in the development of obesity and diabetes. Recently, other members of conventional MAPKs emerged as important mediators of liver, skeletal muscle, adipose tissue, and pancreatic β-cell metabolism. Moreover, latest studies indicate that atypical members of MAPK family play a central role in the regulation of adipose tissue function. In this review, we summarize early studies on conventional MAPKs as well as recent findings implicating previously ignored members of the MAPK family. Finally, we discuss the therapeutic potential of drugs targeting specific members of the MAPK family.

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“…ASK1 is upregulated in NASH patients and correlates with the fibrosis stage. In animal models, inhibition of ASK1 as well as molecules upstream and downstream of the pathway improved NASH and hepatic lipid metabolism (36,37). Despite encouraging results from a small phase 2 study (38), selonsertib failed to improve NASH or fibrosis in the phase 3 STELLAR Study (https:// www.gilead.com/news-and-press/press-room/pressreleases/2019/4/gilead-announces-topline-data-fromphase-3-stellar3-study-of-selonsertib-in-bridging-fibrosis-f3-due-to-nonalcoholic-steatohepatitis-nash, accessed on 25 April 2019).…”

Section: Selonsertibmentioning

confidence: 99%

Emerging medical therapies for non-alcoholic fatty liver disease and for alcoholic hepatitis

Wong

Singal

2019

Transl. Gastroenterol. Hepatol

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Non-alcoholic fatty liver disease (NAFLD) and alcoholic liver disease (ALD) are currently the two most common liver diseases in the world. Alcoholic hepatitis (AH), a unique clinical syndrome among ALD patients has high short-term mortality. Apart from controlling the risk factor for individual respective disease, there are no Food and Drug Administration (FDA) approved medical therapies for these diseases. Over the last 5-10 years, the field has extensively grown with many new targets being studied in randomized clinical trials for these diseases, with many of these drugs being tested in both the conditions. In this chapter, we will describe the novel therapeutic agents and current status of ongoing clinical trials with these agents for the treatment of NAFLD and/or AH.

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Dual‐Specificity Phosphatase 26 Protects Against Nonalcoholic Fatty Liver Disease in Mice Through Transforming Growth Factor Beta–Activated Kinase 1 Suppression

Cited by 45 publications

References 45 publications

Modeling alcoholic liver disease in a human Liver-Chip

Modeling alcoholic liver disease in a human Liver-Chip

Impact of Conventional and Atypical MAPKs on the Development of Metabolic Diseases

Emerging medical therapies for non-alcoholic fatty liver disease and for alcoholic hepatitis

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