Your search keyword '"Du, Kuo"' showing total 9 results

1. Plasticity, heterogeneity, and multifunctionality of hepatic stellate cells in liver pathophysiology.

Author

Du K, Jun JH, Dutta RK, and Diehl AM

Subjects

Humans, Carcinogenesis, Homeostasis, RNA, Hepatic Stellate Cells, Liver

Abstract

HSCs, the resident pericytes of the liver, have consistently been at the forefront of liver research due to their crucial roles in various hepatic pathological processes. Prior literature often depicted HSCs in a binary framework, categorizing them as either quiescent or activated. However, recent advances in HSC research, particularly the advent of single-cell RNA-sequencing, have revolutionized our understanding of these cells. This sophisticated technique offers an unparalleled, high-resolution insight into HSC populations, uncovering a spectrum of diversity and functional heterogeneity across various physiological states of the liver, ranging from liver development to the liver aging process. The single-cell RNA-sequencing revelations have also highlighted the intrinsic plasticity of HSCs and underscored their complex roles in a myriad of pathophysiological processes, including liver injury, repair, and carcinogenesis. This review aims to integrate and clarify these recent discoveries, focusing on how the inherent plasticity of HSCs is central to their dynamic roles both in maintaining liver homeostasis and orchestrating responses to liver injury. Future research will clarify whether findings from rodent models can be translated to human livers and guide how these insights are harnessed to develop targeted therapeutic interventions., (Copyright © 2024 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Association for the Study of Liver Diseases.)

Published

2024

2. Increased Glutaminolysis Marks Active Scarring in Nonalcoholic Steatohepatitis Progression.

Author

Du K, Chitneni SK, Suzuki A, Wang Y, Henao R, Hyun J, Premont RT, Naggie S, Moylan CA, Bashir MR, Abdelmalek MF, and Diehl AM

Subjects

Adult, Amino Acid Transport System ASC analysis, Amino Acid Transport System ASC metabolism, Animals, Biomarkers analysis, Biomarkers metabolism, Cell Line, Cicatrix pathology, Disease Models, Animal, Disease Progression, Female, Glutaminase analysis, Glutaminase metabolism, Glutamine analysis, Glutamine metabolism, Hepatic Stellate Cells pathology, Humans, Liver cytology, Liver diagnostic imaging, Liver Cirrhosis pathology, Male, Metabolomics, Mice, Middle Aged, Minor Histocompatibility Antigens analysis, Minor Histocompatibility Antigens metabolism, Myofibroblasts pathology, Positron-Emission Tomography, Cicatrix diagnosis, Liver pathology, Liver Cirrhosis diagnosis, Non-alcoholic Fatty Liver Disease pathology

Abstract

Background & Aims: Nonalcoholic steatohepatitis (NASH) occurs in the context of aberrant metabolism. Glutaminolysis is required for metabolic reprograming of hepatic stellate cells (HSCs) and liver fibrogenesis in mice. However, it is unclear how changes in HSC glutamine metabolism contribute to net changes in hepatic glutaminolytic activity during fibrosis progression, or whether this could be used to track fibrogenic activity in NASH. We postulated that increased HSC glutaminolysis marks active scarring in NASH., Methods: Glutaminolysis was assessed in mouse NASH fibrosis models and in NASH patients. Serum and liver levels of glutamine and glutamate and hepatic expression of glutamine transporter/metabolic enzymes were correlated with each other and with fibrosis severity. Glutaminolysis was disrupted in HSCs to examine if this directly influenced fibrogenesis. 18 F-fluoroglutamine positron emission tomography was used to determine how liver glutamine assimilation tracked with hepatic fibrogenic activity in situ., Results: The serum glutamate/glutamine ratio increased and correlated with its hepatic ratio, myofibroblast content, and fibrosis severity. Healthy livers almost exclusively expressed liver-type glutaminase (Gls2); Gls2 protein localized in zone 1 hepatocytes, whereas glutamine synthase was restricted to zone 3 hepatocytes. In fibrotic livers, Gls2 levels reduced and glutamine synthase zonality was lost, but both Slc1a5 (glutamine transporter) and kidney-type Gls1 were up-regulated; Gls1 protein was restricted to stromal cells and accumulated in fibrotic septa. Hepatocytes did not compensate for decreased Gls2 by inducing Gls1. Limiting glutamine or directly inhibiting GLS1 inhibited growth and fibrogenic activity in cultured human HSCs. Compared with healthy livers, fibrotic livers were 18 F-fluoroglutamine-avid by positron emission tomography, suggesting that glutamine-addicted myofibroblasts drive increased hepatic utilization of glutamine as fibrosis progresses., Conclusions: Glutaminolysis is a potential diagnostic marker and therapeutic target during NASH fibrosis progression., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

3. Single-Cell RNA Sequencing Identifies Yes-Associated Protein 1-Dependent Hepatic Mesothelial Progenitors in Fibrolamellar Carcinoma.

Author

Jewell ML, Gibson JR, Guy CD, Hyun J, Du K, Oh SH, Premont RT, Hsu DS, Ribar T, Gregory SG, and Diehl AME

Subjects

Adaptor Proteins, Signal Transducing genetics, Animals, Biomarkers, Tumor, Carcinoma, Hepatocellular genetics, Carcinoma, Hepatocellular metabolism, Epithelium metabolism, Gene Expression Regulation, Neoplastic, High-Throughput Nucleotide Sequencing, Humans, Liver metabolism, Liver Neoplasms genetics, Liver Neoplasms metabolism, Mesothelin, Mice, Mice, SCID, Stem Cells metabolism, Transcription Factors genetics, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, YAP-Signaling Proteins, Adaptor Proteins, Signal Transducing metabolism, Carcinoma, Hepatocellular pathology, Epithelium pathology, Liver pathology, Liver Neoplasms pathology, Single-Cell Analysis methods, Stem Cells pathology, Transcription Factors metabolism

Abstract

Fibrolamellar carcinoma (FLC) is characterized by in-frame fusion of DnaJ heat shock protein family (Hsp40) member B1 (DNAJB1) with protein kinase cAMP-activated catalytic subunit α (PRKACA) and by dense desmoplasia. Surgery is the only effective treatment because mechanisms supporting tumor survival are unknown. We used single-cell RNA sequencing to characterize a patient-derived FLC xenograft model and identify therapeutic targets. Human FLC cells segregated into four discrete clusters that all expressed the oncogene Yes-associated protein 1 (YAP1). The two communities most enriched with cells coexpressing FLC markers [CD68, A-kinase anchoring protein 12 (AKAP12), cytokeratin 7, epithelial cell adhesion molecule (EPCAM), and carbamoyl palmitate synthase-1] also had the most cells expressing YAP1 and its proproliferative target genes (AREG and CCND1), suggesting these were proliferative FLC cell clusters. The other two clusters were enriched with cells expressing profibrotic YAP1 target genes, ACTA2, ELN, and COL1A1, indicating these were fibrogenic FLC cells. All clusters expressed the YAP1 target gene and mesothelial progenitor marker mesothelin, and many mesothelin-positive cells coexpressed albumin. Trajectory analysis predicted that the four FLC communities were derived from a single cell type transitioning among phenotypic states. After establishing a novel FLC cell line that harbored the DNAJB1-PRKACA fusion, YAP1 was inhibited, which significantly reduced expression of known YAP1 target genes as well as cell growth and migration. Thus, both FLC epithelial and stromal cells appear to arise from DNAJB1-PRKACA fusion in a YAP1-dependent liver mesothelial progenitor, identifying YAP1 as a target for FLC therapy., (Copyright © 2020 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.)

Published

2020

4. Hedgehog-YAP Signaling Pathway Regulates Glutaminolysis to Control Activation of Hepatic Stellate Cells.

Author

Du K, Hyun J, Premont RT, Choi SS, Michelotti GA, Swiderska-Syn M, Dalton GD, Thelen E, Rizi BS, Jung Y, and Diehl AM

Subjects

Adaptor Proteins, Signal Transducing genetics, Animals, Case-Control Studies, Cell Cycle Proteins, Cell Proliferation, Cell Transdifferentiation, Cells, Cultured, Cellular Reprogramming, Gene Expression Regulation, Glutaminase metabolism, Hedgehog Proteins genetics, Hepatic Stellate Cells pathology, Humans, Ketoglutaric Acids metabolism, Liver pathology, Liver Cirrhosis genetics, Liver Cirrhosis pathology, Liver Cirrhosis, Experimental genetics, Liver Cirrhosis, Experimental metabolism, Liver Cirrhosis, Experimental pathology, Mice, Inbred C57BL, Mice, Knockout, Mitochondria, Liver metabolism, Mitochondria, Liver pathology, Myofibroblasts pathology, Phenotype, Phosphoproteins genetics, RNA Interference, Rats, Signal Transduction, Smoothened Receptor genetics, Smoothened Receptor metabolism, Time Factors, Transcription Factors, Transfection, YAP-Signaling Proteins, Adaptor Proteins, Signal Transducing metabolism, Energy Metabolism, Glutamine metabolism, Hedgehog Proteins metabolism, Hepatic Stellate Cells metabolism, Liver metabolism, Liver Cirrhosis metabolism, Myofibroblasts metabolism, Phosphoproteins metabolism

Abstract

Background & Aims: Cirrhosis results from accumulation of myofibroblasts derived from quiescent hepatic stellate cells (Q-HSCs); it regresses when myofibroblastic HSCs are depleted. Hedgehog signaling promotes transdifferentiation of HSCs by activating Yes-associated protein 1 (YAP1 or YAP) and inducing aerobic glycolysis. However, increased aerobic glycolysis alone cannot meet the high metabolic demands of myofibroblastic HSCs. Determining the metabolic processes of these cells could lead to strategies to prevent progressive liver fibrosis, so we investigated whether glutaminolysis (conversion of glutamine to alpha-ketoglutarate) sustains energy metabolism and permits anabolism when Q-HSCs become myofibroblastic, and whether this is controlled by hedgehog signaling to YAP., Methods: Primary HSCs were isolated from C57BL/6 or Smo flox/flox mice; we also performed studies with rat and human myofibroblastic HSCs. We measured changes of glutaminolytic genes during culture-induced primary HSC transdifferentiation. Glutaminolysis was disrupted in cells by glutamine deprivation or pathway inhibitors (bis-2-[5-phenylacetamido-1,2,4-thiadiazol-2-yl] ethyl sulfide, CB-839, epigallocatechin gallate, and aminooxyacetic acid), and effects on mitochondrial respiration, cell growth and migration, and fibrogenesis were measured. Hedgehog signaling to YAP was disrupted in cells by adenovirus expression of Cre-recombinase or by small hairpin RNA knockdown of YAP. Hedgehog and YAP activity were inhibited by incubation of cells with cyclopamine or verteporfin, and effects on glutaminolysis were measured. Acute and chronic liver fibrosis were induced in mice by intraperitoneal injection of CCl 4 or methionine choline-deficient diet. Some mice were then given injections of bis-2-[5-phenylacetamido-1,2,4-thiadiazol-2-yl] ethyl sulfide to inhibit glutaminolysis, and myofibroblast accumulation was measured. We also performed messenger RNA and immunohistochemical analyses of percutaneous liver biopsies from healthy human and 4 patients with no fibrosis, 6 patients with mild fibrosis, and 3 patients with severe fibrosis., Results: Expression of genes that regulate glutaminolysis increased during transdifferentiation of primary Q-HSCs into myofibroblastic HSCs, and inhibition of glutaminolysis disrupted transdifferentiation. Blocking glutaminolysis in myofibroblastic HSCs suppressed mitochondrial respiration, cell growth and migration, and fibrogenesis; replenishing glutaminolysis metabolites to these cells restored these activities. Knockout of the hedgehog signaling intermediate smoothened or knockdown of YAP inhibited expression of glutaminase, the rate-limiting enzyme in glutaminolysis. Hedgehog and YAP inhibitors blocked glutaminolysis and suppressed myofibroblastic activities in HSCs. In livers of patients and of mice with acute or chronic fibrosis, glutaminolysis was induced in myofibroblastic HSCs. In mice with liver fibrosis, inhibition of glutaminase blocked accumulation of myofibroblasts and fibrosis progression., Conclusions: Glutaminolysis controls accumulation of myofibroblast HSCs in mice and might be a therapeutic target for cirrhosis., (Copyright © 2018 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2018

5. Editor's Highlight: Metformin Protects Against Acetaminophen Hepatotoxicity by Attenuation of Mitochondrial Oxidant Stress and Dysfunction.

Author

Du K, Ramachandran A, Weemhoff JL, Chavan H, Xie Y, Krishnamurthy P, and Jaeschke H

Subjects

Animals, Cell Line, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Cytoprotection, Disease Models, Animal, Enzyme Activation, Hepatocytes metabolism, Hepatocytes pathology, Humans, JNK Mitogen-Activated Protein Kinases metabolism, Liver metabolism, Liver pathology, Male, Mice, Inbred C57BL, Mitochondria, Liver metabolism, Mitochondria, Liver pathology, Necrosis, Time Factors, Acetaminophen, Antioxidants pharmacology, Chemical and Drug Induced Liver Injury prevention & control, Hepatocytes drug effects, Liver drug effects, Metformin pharmacology, Mitochondria, Liver drug effects, Oxidative Stress drug effects

Abstract

Overdose of acetaminophen (APAP) causes severe liver injury and even acute liver failure in both mice and human. A recent study by Kim et al. (2015, Metformin ameliorates acetaminophen hepatotoxicity via Gadd45β-dependent regulation of JNK signaling in mice. J. Hepatol. 63, 75-82) showed that metformin, a first-line drug to treat type 2 diabetes mellitus, protected against APAP hepatotoxicity in mice. However, its exact protective mechanism has not been well clarified. To investigate this, C57BL/6J mice were treated with 400 mg/kg APAP and 350 mg/kg metformin was given 0.5 h pre- or 2 h post-APAP. Our data showed that pretreatment with metformin protected against APAP hepatotoxicity, as indicated by the over 80% reduction in plasma alanine aminotransferase (ALT) activities and significant decrease in centrilobular necrosis. Metabolic activation of APAP, as indicated by glutathione depletion and APAP-protein adducts formation, was also slightly inhibited. However, 2 h post-treatment with metformin still reduced liver injury by 50%, without inhibition of adduct formation. Interestingly, neither pre- nor post-treatment of metformin inhibited c-jun N-terminal kinase (JNK) activation or its mitochondrial translocation. In contrast, APAP-induced mitochondrial oxidant stress and dysfunction were greatly attenuated in these mice. In addition, mice with 2 h post-treatment with metformin also showed significant inhibition of complex I activity, which may contribute to the decreased mitochondrial oxidant stress. Furthermore, the protection was reproduced in JNK activation-absent HepaRG cells treated with 20 mM APAP followed by 0.5 or 1 mM metformin 6 h later, confirming JNK-independent protection mechanisms. Thus, metformin protects against APAP hepatotoxicity by attenuating the mitochondrial oxidant stress and subsequent mitochondrial dysfunction, and may be a potential therapeutic option for APAP overdose patients., (© The Author 2016. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2016

6. Liuweiwuling tablets protect against acetaminophen hepatotoxicity: What is the protective mechanism?

Author

Du K and Jaeschke H

Subjects

Animals, Male, Acetaminophen, Chemical and Drug Induced Liver Injury prevention & control, Drugs, Chinese Herbal pharmacology, Liver drug effects, Liver Regeneration drug effects

Abstract

Study of the effects of natural products, including traditional Chinese Medicines, on acetaminophen hepatotoxicity has gained considerable popularity in recent years, and some of them showed positive results and even promising therapeutic potentials. A recent report suggested that Liuweiwuling tablets protect against acetaminophen hepatotoxicity and promote liver regeneration in a rodent model through alleviating the inflammatory response. However, several concerns exist regarding the limitations of the experimental design and interpretation of the data presented in this manuscript.

Published

2016

7. Mitochondrial protein adducts formation and mitochondrial dysfunction during N-acetyl-m-aminophenol (AMAP)-induced hepatotoxicity in primary human hepatocytes.

Author

Xie Y, McGill MR, Du K, Dorko K, Kumer SC, Schmitt TM, Ding WX, and Jaeschke H

Subjects

Animals, Cell Death drug effects, Cells, Cultured, Chemical and Drug Induced Liver Injury metabolism, Chemical and Drug Induced Liver Injury pathology, Dose-Response Relationship, Drug, Glutamate Dehydrogenase metabolism, Glutathione metabolism, Hepatocytes metabolism, Hepatocytes pathology, Humans, JNK Mitogen-Activated Protein Kinases metabolism, L-Lactate Dehydrogenase metabolism, Liver metabolism, Liver pathology, Mice, Mitochondria, Liver metabolism, Mitochondria, Liver pathology, Phosphorylation, Primary Cell Culture, Protein Binding, Signal Transduction drug effects, Species Specificity, Time Factors, Acetanilides toxicity, Chemical and Drug Induced Liver Injury etiology, Hepatocytes drug effects, Liver drug effects, Mitochondria, Liver drug effects, Mitochondrial Proteins metabolism

Abstract

3'-Hydroxyacetanilide orN-acetyl-meta-aminophenol (AMAP) is generally regarded as a non-hepatotoxic analog of acetaminophen (APAP). Previous studies demonstrated the absence of toxicity after AMAP in mice, hamsters, primary mouse hepatocytes and several cell lines. In contrast, experiments with liver slices suggested that it may be toxic to human hepatocytes; however, the mechanism of toxicity is unclear. To explore this,we treated primary human hepatocytes (PHH) with AMAP or APAP for up to 48 h and measured several parameters to assess metabolism and injury. Although less toxic than APAP, AMAP dose-dependently triggered cell death in PHH as indicated by alanine aminotransferase (ALT) release and propidium iodide (PI) staining. Similar to APAP, AMAP also significantly depleted glutathione (GSH) in PHH and caused mitochondrial damage as indicated by glutamate dehydrogenase (GDH) release and the JC-1 assay. However, unlike APAP, AMAP treatment did not cause relevant c-jun-N-terminal kinase (JNK) activation in the cytosol or phospho-JNK translocation to mitochondria. To compare, AMAP toxicity was assessed in primary mouse hepatocytes (PMH). No cytotoxicity was observed as indicated by the lack of lactate dehydrogenase release and no PI staining. Furthermore, there was no GSH depletion or mitochondrial dysfunction after AMAP treatment in PMH. Immunoblotting for arylated proteins suggested that AMAP treatment caused extensive mitochondrial protein adduct formation in PHH but not in PMH. In conclusion, AMAP is hepatotoxic in PHH and the mechanism involves the formation of mitochondrial protein adducts and mitochondrial dysfunction.

Published

2015

8. Resveratrol prevents protein nitration and release of endonucleases from mitochondria during acetaminophen hepatotoxicity.

Author

Du K, McGill MR, Xie Y, Bajt ML, and Jaeschke H

Subjects

Animals, Apoptosis Inducing Factor antagonists & inhibitors, Apoptosis Inducing Factor metabolism, DNA Fragmentation drug effects, Drug Overdose drug therapy, Endonucleases antagonists & inhibitors, Hepatocytes drug effects, JNK Mitogen-Activated Protein Kinases metabolism, Liver pathology, Male, Mice, Mice, Inbred C57BL, Mitochondria enzymology, Oxidative Stress drug effects, Peroxynitrous Acid metabolism, Protein Binding, Resveratrol, Tyrosine analogs & derivatives, Tyrosine metabolism, Acetaminophen poisoning, Chemical and Drug Induced Liver Injury drug therapy, Endonucleases metabolism, Liver drug effects, Mitochondria drug effects, Stilbenes pharmacology

Abstract

Overdose of acetaminophen (APAP) is a common cause of acute liver injury and liver failure. The mechanism involves formation of a reactive metabolite, protein binding, oxidative stress and activation of c-Jun N-terminal kinase (JNK), mitochondrial dysfunction, and nuclear DNA fragmentation caused by endonucleases released from damaged mitochondria. Previous work has shown that the natural product resveratrol (RSV) can protect against APAP hepatotoxicity in mice through prevention of lipid peroxidation and anti-inflammatory effects. However, these earlier studies did not take into consideration several fundamental aspects of the pathophysiology. To address this, we treated C57Bl/6 mice with 300 mg/kg APAP followed by 50 mg/kg RSV 1.5 h later. Our results confirmed that RSV reduced liver injury after APAP overdose in mice. Importantly, RSV did not inhibit reactive metabolite formation and protein bindings, nor did it reduce activation of JNK. However, RSV decreased protein nitration after APAP treatment, possibly through direct scavenging of peroxynitrite. Interestingly, RSV also inhibited release of apoptosis-inducing factor and endonuclease G from mitochondria independent of Bax pore formation and prevented the downstream nuclear DNA fragmentation. Our data show that RSV protects against APAP hepatotoxicity both through antioxidant effects and by preventing mitochondrial release of endonucleases and nuclear DNA damage., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

9. Hedgehog Signaling: Implications in Liver Pathophysiology.

Author

Dutta, Rajesh Kumar, Jun, JiHye, Du, Kuo, and Diehl, Anna Mae

Subjects

HEDGEHOG signaling proteins, FATTY liver, PATHOLOGICAL physiology, LIVER, LIVER cells

Abstract

This article explores the role of Hedgehog signaling in liver pathophysiology. Hedgehog signaling is a complex pathway that regulates various aspects of liver function, including glucose and lipid metabolism. Disruption of this pathway can lead to metabolic abnormalities and liver damage. The article also discusses the involvement of different cell types in the liver in regulating Hedgehog signaling and how dysregulation of this pathway contributes to inflammation, fibrosis, and disease progression. The findings have implications for understanding and potentially treating liver diseases such as fatty liver disease and liver cancer. [Extracted from the article]

Published

2023