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1. Lymphocyte-Specific Protein-1 Suppresses Xenobiotic-Induced Constitutive Androstane Receptor and Subsequent Yes-Associated Protein–Activated Hepatocyte Proliferation

Author

Kelly Koral, Bharat Bhushan, Anne Orr, John Stoops, William C. Bowen, Matthew A. Copeland, Joseph Locker, Wendy M. Mars, and George K. Michalopoulos

Subjects
Mice, Liver, Liver Neoplasms, Microfilament Proteins, Hepatocytes, Animals, YAP-Signaling Proteins, Hypertrophy, Lymphocytes, Constitutive Androstane Receptor, Cell Proliferation, Xenobiotics, Pathology and Forensic Medicine
Abstract

Activation of constitutive androstane receptor (CAR) transcription factor by xenobiotics promotes hepatocellular proliferation, promotes hypertrophy without liver injury, and induces drug metabolism genes. Previous work demonstrated that lymphocyte-specific protein-1 (LSP1), an F-actin binding protein and gene involved in human hepatocellular carcinoma, suppresses hepatocellular proliferation after partial hepatectomy. The current study investigated the role of LSP1 in liver enlargement induced by chemical mitogens, a regenerative process independent of tissue loss. 1,4-Bis [2-(3,5-dichloropyridyloxy)] benzene (TCPOBOP), a direct CAR ligand and strong chemical mitogen, was administered to global Lsp1 knockout and hepatocyte-specific Lsp1 transgenic (TG) mice and measured cell proliferation, hypertrophy, and expression of CAR-dependent drug metabolism genes. TG livers displayed a significant decrease in Ki-67 labeling and liver/body weight ratios compared with wild type on day 2. Surprisingly, this was reversed by day 5, due to hepatocyte hypertrophy. There was no difference in CAR-regulated drug metabolism genes between wild type and TG. TG livers displayed increased Yes-associated protein (YAP) phosphorylation, decreased nuclear YAP, and direct interaction between LSP1 and YAP, suggesting LSP1 suppresses TCPOBOP-driven hepatocellular proliferation, but not hepatocyte volume, through YAP. Conversely, loss of LSP1 led to increased hepatocellular proliferation on days 2, 5, and 7. LSP1 selectively suppresses CAR-induced hepatocellular proliferation, but not drug metabolism, through the interaction of LSP1 with YAP, supporting the role of LSP1 as a selective growth suppressor.

Published
2022

2. Yes‐Associated Protein Is Crucial for Constitutive Androstane Receptor‐Driven Hepatocyte Proliferation But Not for Induction of Drug Metabolism Genes in Mice

Author

John Stoops, Anne Orr, Swati Banerjee, George K. Michalopoulos, Shirish Paranjpe, Bharat Bhushan, Kelly Koral, Satdarshan P.S. Monga, Wendy M. Mars, Laura Molina, and Joseph Locker

Subjects
0301 basic medicine, Liver Biology and Pathobiology, 03 medical and health sciences, 0302 clinical medicine, Cyclin D1, Constitutive androstane receptor, Animals, Humans, Constitutive Androstane Receptor, Cyclin, Cell Proliferation, Mice, Knockout, Hepatology, biology, Chemistry, Kinase, Cell Cycle, Retinoblastoma protein, YAP-Signaling Proteins, Original Articles, Cell cycle, Liver regeneration, Cell biology, Liver Regeneration, Cyclin E1, 030104 developmental biology, Gene Expression Regulation, Genes, Inactivation, Metabolic, biology.protein, Hepatocytes, 030211 gastroenterology & hepatology, Original Article, Female, Transcriptome
Abstract

Background and aims Constitutive androstane receptor (CAR) agonists, such as 1,4-bis [2-(3,5-dichloropyridyloxy)] benzene (TCPOBOP), are known to cause robust hepatocyte proliferation and hepatomegaly in mice along with induction of drug metabolism genes without any associated liver injury. Yes-associated protein (Yap) is a key transcription regulator that tightly controls organ size, including that of liver. Our and other previous studies suggested increased nuclear localization and activation of Yap after TCPOBOP treatment in mice and the potential role of Yap in CAR-driven proliferative response. Here, we investigated a direct role of Yap in CAR-driven hepatomegaly and hepatocyte proliferation using hepatocyte-specific Yap-knockout (KO) mice. Approach and results Adeno-associated virus 8-thyroxine binding globulin promoter-Cre recombinase vector was injected to Yap-floxed mice for achieving hepatocyte-specific Yap deletion followed by TCPOBOP treatment. Yap deletion did not decrease protein expression of CAR or CAR-driven induction of drug metabolism genes (including cytochrome P450 [Cyp] 2b10, Cyp2c55, and UDP-glucuronosyltransferase 1a1 [Ugt1a1]). However, Yap deletion substantially reduced TCPOBOP-induced hepatocyte proliferation. TCPOBOP-driven cell cycle activation was disrupted in Yap-KO mice because of delayed (and decreased) induction of cyclin D1 and higher expression of p21, resulting in decreased phosphorylation of retinoblastoma protein. Furthermore, the induction of other cyclins, which are sequentially involved in progression through cell cycle (including cyclin E1, A2, and B1), and important mitotic regulators (such as Aurora B kinase and polo-like kinase 1) was remarkably reduced in Yap-KO mice. Microarray analysis revealed that 26% of TCPOBOP-responsive genes that were mainly related to proliferation, but not to drug metabolism, were altered by Yap deletion. Yap regulated these proliferation genes through alerting expression of Myc and forkhead box protein M1, two critical transcriptional regulators of CAR-mediated hepatocyte proliferation. Conclusions Our study revealed an important role of Yap signaling in CAR-driven hepatocyte proliferation; however, CAR-driven induction of drug metabolism genes was independent of Yap.

Published
2021

4. Phosphorylated Ezrin (Thr567) Regulates Hippo Pathway and Yes-Associated Protein (Yap) in Liver

Author

Andrew W. Duncan, John Stoops, Bharat Bhushan, George K. Michalopoulos, Jianhua Luo, Anne Orr, Yanping Yu, William C. Bowen, Wendy M. Mars, Yuhua Xue, and Junyan Tao

Subjects
0301 basic medicine, macromolecular substances, Protein Serine-Threonine Kinases, environment and public health, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, 0302 clinical medicine, Ezrin, Cell Line, Tumor, Animals, Humans, Epidermal growth factor receptor, Phosphorylation, Receptor, Adaptor Proteins, Signal Transducing, Cell Proliferation, YAP1, Hippo signaling pathway, biology, Chemistry, Signal transducing adaptor protein, Regular Article, Liver regeneration, Cell biology, Cytoskeletal Proteins, 030104 developmental biology, 030220 oncology & carcinogenesis, Hepatocytes, biology.protein, Signal Transduction
Abstract

The activation of CD81 [the portal of entry of hepatitis C virus (HCV)] by agonistic antibody results in phosphorylation of Ezrin via Syk kinase and is associated with inactivation of the Hippo pathway and increase in yes-associated protein (Yap1). The opposite occurs when glypican-3 or E2 protein of HCV binds to CD81. Hepatocyte-specific glypican-3 transgenic mice have decreased levels of phosphorylated (p)-Ezrin (Thr567) and Yap, increased Hippo activity, and suppressed liver regeneration. The role of Ezrin in these processes has been speculated, but not proved. We show that Ezrin has a direct role in the regulation of Hippo pathway and Yap. Forced expression of plasmids expressing mutant Ezrin (T567D) that mimics p-Ezrin (Thr567) suppressed Hippo activity and activated Yap signaling in hepatocytes in vivo and enhanced activation of pathways of β-catenin and leucine rich repeat containing G protein-coupled receptor 4 (LGR4) and LGR5 receptors. Hepatoma cell lines JM1 and JM2 have decreased CD81 expression and Hippo activity and up-regulated p-Ezrin (T567). NSC668394, a p-Ezrin (Thr567) antagonist, significantly decreased hepatoma cell proliferation. We additionally show that p-Ezrin (T567) is controlled by epidermal growth factor receptor and MET. Ezrin phosphorylation, mediated by CD81-associated Syk kinase, is directly involved in regulation of Hippo pathway, Yap levels, and growth of normal and neoplastic hepatocytes. The finding has mechanistic and potentially therapeutic applications in hepatocyte growth biology, hepatocellular carcinoma, and HCV pathogenesis.

Published
2020

5. A Noncanonical Role for Plasminogen Activator Inhibitor Type 1 in Obesity-Induced Diabetes

Author

Bharat Bhushan, Anne Orr, Wendy M. Mars, George K. Michalopoulos, Jon D. Piganelli, Kelly Koral, Dana M. Previte, Sojin Lee, Gina M. Coudriet, H. Henry Dong, and John Stoops

Subjects
Male, 0301 basic medicine, medicine.medical_specialty, medicine.medical_treatment, Inflammation, Type 2 diabetes, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, Internal medicine, Diabetes mellitus, Antifibrinolytic agent, Plasminogen Activator Inhibitor 1, Fibrinolysis, Animals, Medicine, Obesity, Mice, Knockout, Hepatocyte Growth Factor, business.industry, Proto-Oncogene Proteins c-met, medicine.disease, Dietary Fats, 030104 developmental biology, Endocrinology, Diabetes Mellitus, Type 2, 030220 oncology & carcinogenesis, Hepatocyte growth factor, medicine.symptom, business, Plasminogen activator, medicine.drug
Abstract

Obesity is a major risk factor for type 2 diabetes because of chronic hepatic inflammation and resultant insulin resistance. Hepatocyte growth factor (HGF) is responsible for resetting hepatic homeostasis after injury following activation by urokinase-type plasminogen activator (u-PA; encoded by the PLAU gene). Plasminogen activator inhibitor type-1 (PAI-1; encoded by the SERPINE1 gene), a u-PA inhibitor and antifibrinolytic agent, is often elevated in obesity and is linked to cardiovascular events. We hypothesized that, in addition to its role in preventing fibrinolysis, elevated PAI-1 inhibits HGF's activation by u-PA and the resultant anti-inflammatory and hepatoprotective properties. Wild-type and PAI-1 knockout (KO) mice on a high-fat diet both became significantly heavier than lean controls; however, the obese KO mice demonstrated improved glucose metabolism compared with wild-type mice. Obese KO mice also exhibited an increase in conversion of latent single-chain HGF to active two-chain HGF, coinciding with an increase in the phosphorylation of the HGF receptor (HGFR or MET, encoded by the MET gene), as well as dampened inflammation. These results strongly suggest that, in addition to its other functions, PAI-mediated inhibition of HGF activation prohibits the resolution of inflammation in the context of obesity-induced type 2 diabetes.

Published
2019

6. Pharmacologic Inhibition of Epidermal Growth Factor Receptor Suppresses Nonalcoholic Fatty Liver Disease in a Murine Fast‐Food Diet Model

Author

Anne Orr, Swati Banerjee, John Stoops, Bharat Bhushan, William C. Bowen, Kelly Koral, Wendy M. Mars, Shirish Paranjpe, George K. Michalopoulos, and Joseph Locker

Subjects
Male, 0301 basic medicine, Morpholines, Perilipin 2, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Non-alcoholic Fatty Liver Disease, Nonalcoholic fatty liver disease, medicine, Animals, EGFR inhibitors, Hepatology, Canertinib, biology, Lipid metabolism, Lipid Metabolism, medicine.disease, Liver regeneration, ErbB Receptors, Mice, Inbred C57BL, Disease Models, Animal, Fatty acid synthase, 030104 developmental biology, chemistry, Hepatocyte nuclear factor 4 alpha, biology.protein, Cancer research, Fast Foods, 030211 gastroenterology & hepatology
Abstract

Epidermal growth factor receptor (EGFR) is a critical regulator of hepatocyte proliferation and liver regeneration. Our recent work indicated that EGFR can also regulate lipid metabolism during liver regeneration after partial hepatectomy. Based on these findings, we investigated the role of EGFR in a mouse model of nonalcoholic fatty liver disease (NAFLD) using a pharmacological inhibition strategy. C57BL6/J mice were fed a chow diet or a fast-food diet (FFD) with or without EGFR inhibitor (canertinib) for 2 months. EGFR inhibition completely prevented development of steatosis and liver injury in this model. In order to study if EGFR inhibition can reverse NAFLD progression, mice were fed the FFD for 5 months, with or without canertinib treatment for the last 5 weeks of the study. EGFR inhibition remarkably decreased steatosis, liver injury, and fibrosis and improved glucose tolerance. Microarray analysis revealed that ~40% of genes altered by the FFD were differentially expressed after EGFR inhibition and, thus, are potentially regulated by EGFR. Several genes and enzymes related to lipid metabolism (particularly fatty acid synthesis and lipolysis), which were disrupted by the FFD, were found to be modulated by EGFR. Several crucial transcription factors that play a central role in regulating these lipid metabolism genes during NAFLD, including peroxisome proliferator-activated receptor gamma (PPARγ), sterol regulatory element-binding transcription factor 1 (SREBF1), carbohydrate-responsive element-binding protein, and hepatocyte nuclear factor 4 alpha, were also found to be modulated by EGFR. In fact, chromatin immunoprecipitation analysis revealed that PPARγ binding to several crucial lipid metabolism genes (fatty acid synthase, stearoyl-coenzyme A desaturase 1, and perilipin 2) was drastically reduced by EGFR inhibition. Further upstream, EGFR inhibition suppressed AKT signaling, which is known to control these transcription factors, including PPARγ and SREBF1, in NAFLD models. Lastly, the effect of EGFR in FFD-induced fatty-liver phenotype was not shared by receptor tyrosine kinase MET, investigated using MET knockout mice. Conclusion: Our study revealed a role of EGFR in NAFLD and the potential of EGFR inhibition as a treatment strategy for NAFLD.

Published
2019

8. p‐Ezrin (Thr567) synergizes with Akt signaling to accelerate Yap mediated cholangiocarcinogenesis, but correlates with favorable prognosis in human intrahepatic cholangiocarcinoma(ICC) patients

Author

George K. Michalopoulos, Wendy M. Mars, John Stoops, Yuhua Xue, Anne Orr, William C. Bowen, and Junyan Tao

Subjects
Ezrin, business.industry, Genetics, Cancer research, Medicine, Favorable prognosis, business, Molecular Biology, Biochemistry, Protein kinase B, Intrahepatic Cholangiocarcinoma, Biotechnology
Published
2021

9. Hepatocyte‐specific YAP deletion suppresses hepatocyte proliferation and hepatomegaly induced by CAR agonist, TCPOBOP (1,4‐Bis [2‐(3,5‐Dichloropyridyloxy)] benzene), in mice

Author

John Stoops, Anne Orr, William C. Bowen, George K. Michalopoulos, Bharat Bhushan, Swati Banerjee, Wendy M. Mars, and Shirish Paranjpe

Subjects
Agonist, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, medicine.drug_class, Hepatocyte, Genetics, medicine, Cancer research, Benzene, Molecular Biology, Biochemistry, Biotechnology
Published
2019

13. p‐Ezrin (Thr567) regulates Hippo pathway and Yap in liver

Author

John Stoops, Yanping Yu, William C. Bowen, Yuhua Xue, Junyan Tao, Anne Orr, Wendy M. Mars, George K. Michalopoulos, Jianhua Luo, Bharat Bhushan, and Andrew W. Duncan

Subjects
Hippo signaling pathway, Ezrin, Genetics, Biology, Molecular Biology, Biochemistry, Biotechnology, Cell biology
Published
2020

17. Combined Systemic Disruption of MET and Epidermal Growth Factor Receptor Signaling Causes Liver Failure in Normal Mice

Author

William C. Bowen, Anastasia Tsagianni, Bharat Bhushan, Shirish Paranjpe, Anne Orr, George C. Tseng, Wendy M. Mars, George K. Michalopoulos, Silvia Liu, and John Stoops

Subjects
0301 basic medicine, Male, Programmed cell death, MAP Kinase Signaling System, medicine.medical_treatment, Morpholines, Mice, Transgenic, Article, Pathology and Forensic Medicine, 03 medical and health sciences, medicine, Animals, Epidermal growth factor receptor, Protein Kinase Inhibitors, Cell Proliferation, biology, business.industry, Hepatocyte Growth Factor, Organ Size, Proto-Oncogene Proteins c-met, Liver regeneration, Liver Regeneration, ErbB Receptors, 030104 developmental biology, medicine.anatomical_structure, Apoptosis, Hepatocyte, Cancer research, biology.protein, Hepatocytes, Signal transduction, Hepatectomy, business, Tyrosine kinase, Liver Failure
Abstract

MET and epidermal growth factor receptor (EGFR) tyrosine kinases are crucial for liver regeneration and normal hepatocyte function. Recently, we demonstrated that in mice, combined inhibition of these two signaling pathways abolished liver regeneration after hepatectomy, with subsequent hepatic failure and death at 15 to 18 days after resection. Morbidity was associated with distinct and specific alterations in important downstream signaling pathways that led to decreased hepatocyte volume, reduced proliferation, and shutdown of many essential hepatocyte functions, such as fatty acid synthesis, urea cycle, and mitochondrial functions. Herein, we explore the role of MET and EGFR signaling in resting mouse livers that are not subjected to hepatectomy. Mice with combined disruption of MET and EGFR signaling were noticeably sick by 10 days and died at 12 to 14 days. Mice with combined disruption of MET and EGFR signaling mice showed decreased liver/body weight ratios, increased apoptosis in nonparenchymal cells, impaired liver metabolic functions, and activation of distinct downstream signaling pathways related to inflammation, cell death, and survival. The present study demonstrates that, in addition to controlling the regenerative response, MET and EGFR synergistically control baseline liver homeostasis in normal mice in such a way that their combined disruption leads to liver failure and death.

Published
2018

18. Glypican 3 (GPC3)‐CD81 axis regulates Ezrin mediated Hippo pathway via cross talking with HGF/c‐Met axis in hepatocytes and hepatocellular carcinoma (HCC)

Author

Anne Orr, George K. Michalopoulos, William C. Bowen, Wendy M. Mars, John Stoops, and Yuhua Xue

Subjects
Hippo signaling pathway, C-Met, medicine.disease, Biochemistry, Glypican 3, chemistry.chemical_compound, Ezrin, chemistry, Hepatocellular carcinoma, Genetics, medicine, Cancer research, Molecular Biology, Biotechnology, CD81
Published
2018

19. TCPOBOP-Induced Hepatomegaly and Hepatocyte Proliferation are Attenuated by Combined Disruption of MET and EGFR Signaling

Author

Anne Orr, John Stoops, William C. Bowen, George K. Michalopoulos, Bharat Bhushan, Shirish Paranjpe, and Wendy M. Mars

Subjects
0301 basic medicine, Pyridines, medicine.medical_treatment, Receptors, Cytoplasmic and Nuclear, Protein Serine-Threonine Kinases, Receptor tyrosine kinase, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Constitutive androstane receptor, medicine, Animals, Hippo Signaling Pathway, Epidermal growth factor receptor, Constitutive Androstane Receptor, Cell Proliferation, Mice, Knockout, Hepatology, Canertinib, biology, Growth factor, Gene Expression Profiling, Cell Cycle, Forkhead Box Protein M1, Proto-Oncogene Proteins c-met, Liver regeneration, ErbB Receptors, 030104 developmental biology, chemistry, Hepatocyte Nuclear Factor 4, Hepatocyte nuclear factor 4 alpha, Cancer research, biology.protein, Hepatocytes, 030211 gastroenterology & hepatology, Female, Signal transduction, Hepatomegaly, Signal Transduction
Abstract

TCPOBOP (1,4-Bis [2-(3,5-Dichloropyridyloxy)] benzene) is a constitutive androstane receptor (CAR) agonist that induces robust hepatocyte proliferation and hepatomegaly without any liver injury or tissue loss. TCPOBOP-induced direct hyperplasia has been considered to be CAR-dependent with no evidence of involvement of cytokines or growth factor signaling. Receptor tyrosine kinases (RTKs), MET and epidermal growth factor receptor (EGFR), are known to play a critical role in liver regeneration after partial hepatectomy, but their role in TCPOBOP-induced direct hyperplasia, not yet explored, is investigated in the current study. Disruption of the RTK-mediated signaling was achieved using MET knockout (KO) mice along with Canertinib treatment for EGFR inhibition. Combined elimination of MET and EGFR signaling [MET KO + EGFR inhibitor (EGFRi)], but not individual disruption, dramatically reduced TCPOBOP-induced hepatomegaly and hepatocyte proliferation. TCPOBOP-driven CAR activation was not altered in [MET KO + EGFRi] mice, as measured by nuclear CAR translocation and analysis of typical CAR target genes. However, TCPOBOP-induced cell cycle activation was impaired in [MET KO + EGFRi] mice due to defective induction of cyclins, which regulate cell cycle initiation and progression. TCPOBOP-driven induction of FOXM1, a key transcriptional regulator of cell cycle progression during TCPOBOP-mediated hepatocyte proliferation, was greatly attenuated in [MET KO + EGFRi] mice. Interestingly, TCPOBOP treatment caused transient decline in hepatocyte nuclear factor 4 alpha expression concomitant to proliferative response; this was not seen in [MET KO + EGFRi] mice. Transcriptomic profiling revealed the vast majority (~40%) of TCPOBOP-dependent genes primarily related to proliferative response, but not to drug metabolism, were differentially expressed in [MET KO + EGFRi] mice. Conclusion: Taken together, combined disruption of EGFR and MET signaling lead to dramatic impairment of TCPOBOP-induced proliferative response without altering CAR activation.

Published
2018

20. A hepatocyte growth factor receptor (Met)−insulin receptor hybrid governs hepatic glucose metabolism

Author

Xinping Tan, Reza Zarnegar, Jianhua Luo, Marie C. DeFrances, John Stoops, Arlee Fafalios, and Jihong Ma

Subjects
Blood Glucose, Male, medicine.medical_specialty, IRS, glucose metabolism, medicine.medical_treatment, Down-Regulation, Mice, Transgenic, Article, General Biochemistry, Genetics and Molecular Biology, Mice, Insulin resistance, insulin resistance, Internal medicine, Insulin receptor substrate, medicine, Animals, Humans, Insulin, HGF, insulin receptor, Phosphorylation, RNA, Small Interfering, Insulin-like growth factor 1 receptor, biology, Hepatocyte Growth Factor, HGFR, Hep G2 Cells, Receptor Cross-Talk, General Medicine, Proto-Oncogene Proteins c-met, medicine.disease, Receptor, Insulin, IRS2, Insulin receptor, Glucose, Endocrinology, Diabetes Mellitus, Type 2, Liver, Hepatocyte Growth Factor Receptor, Models, Animal, Met, biology.protein, Female, type 2 diabetes, Tyrosine kinase, Signal Transduction
Abstract

Met is the transmembrane tyrosine kinase cell surface receptor for hepatocyte growth factor (HGF) and is structurally related to the insulin receptor (INSR) tyrosine kinase. Here we report that the HGF-Met axis regulates metabolism by stimulating hepatic glucose uptake and suppressing hepatic glucose output. We show that Met is essential for an optimal hepatic insulin response by directly engaging INSR to form a Met-INSR hybrid complex, which culminates in a robust signal output. We also found that the HGF-Met system restores insulin responsiveness in a mouse model of insulin refractoriness. These results provide new insights into the molecular basis of hepatic insulin resistance and suggest that HGF may have therapeutic potential for type 2 diabetes in the clinical setting.

Published
2011

21. Lack of Fas antagonism by Met in human fatty liver disease

Author

Chunbin Zou, George K. Michalopoulos, John Stoops, Zhenqi Zhu, Carla Johnson, Lida Guo, Jihong Ma, Marie C. DeFrances, Amanda E. Eaker, Reza Zarnegar, Stephen C. Strom, and Xue Wang

Subjects
Carcinoma, Hepatocellular, Cirrhosis, Molecular Sequence Data, Apoptosis, Biology, General Biochemistry, Genetics and Molecular Biology, Fas ligand, Jurkat Cells, Liver disease, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Extracellular, Humans, Receptors, Growth Factor, Amino Acid Sequence, fas Receptor, Liver Neoplasms, Fatty liver, General Medicine, Proto-Oncogene Proteins c-met, medicine.disease, Fas receptor, Immunohistochemistry, Peptide Fragments, Fatty Liver, Kinetics, Protein Subunits, Biochemistry, Hepatocyte Growth Factor Receptor, Hepatocytes, Cancer research, Collagen
Abstract

Hepatocytes in fatty livers are hypersensitive to apoptosis and undergo escalated apoptotic activity via death receptor-mediated pathways, particularly that of Fas-FasL, causing hepatic injury that can eventually proceed to cirrhosis and end-stage liver disease. Here we report that the hepatocyte growth factor receptor, Met, plays an important part in preventing Fas-mediated apoptosis of hepatocytes by sequestering Fas. We also show that Fas antagonism by Met is abrogated in human fatty liver disease (FLD). Through structure-function studies, we found that a YLGA amino-acid motif located near the extracellular N terminus of the Met alpha-subunit is necessary and sufficient to specifically bind the extracellular portion of Fas and to act as a potent FasL antagonist and inhibitor of Fas trimerization. Using mouse models of FLD, we show that synthetic YLGA peptide tempers hepatocyte apoptosis and liver damage and therefore has therapeutic potential.

Published
2007

22. PI3K is negatively regulated by PIK3IP1, a novel p110 interacting protein

Author

Zhenqi Zhu, Carla Johnson, Amanda E. Eaker, David S. Stoffer, Aaron Bell, Reza Zarnegar, Xin He, John Stoops, and Marie C. DeFrances

Subjects
Regulation of gene expression, Cell growth, Protein subunit, Biophysics, Regulator, Cell Biology, Plasma protein binding, Biology, Biochemistry, Cell biology, Signal transduction, Molecular Biology, Peptide sequence, PI3K/AKT/mTOR pathway
Abstract

Signaling initiated by Class Ia phosphatidylinositol-3-kinases (PI3Ks) is essential for cell proliferation and survival. We discovered a novel protein we call PI3K interacting protein 1 (PIK3IP1) that shares homology with the p85 regulatory PI3K subunit. Using a variety of in vitro and cell based assays, we demonstrate that PIK3IP1 directly binds to the p110 catalytic subunit and down modulates PI3K activity. Our studies suggest that PIK3IP1 is a new type of PI3K regulator.

Published
2007

23. PIK3IP1, a negative regulator of PI3K, suppresses the development of hepatocellular carcinoma

Author

Zhenqi Zhu, John Stoops, Carla Johnson, Marie C. DeFrances, Xin He, William C. Bowen, and Amanda E. Eaker

Subjects
Genetically modified mouse, Male, Cancer Research, Carcinoma, Hepatocellular, Regulator, Apoptosis, Mice, Transgenic, Biology, Gene Expression Regulation, Enzymologic, Article, Mice, Phosphatidylinositol 3-Kinases, In vivo, medicine, Animals, Humans, PI3K/AKT/mTOR pathway, Liver Neoplasms, Intracellular Signaling Peptides and Proteins, Cancer, Membrane Proteins, medicine.disease, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Ki-67 Antigen, Oncology, Hepatocyte, Cancer research, Hepatocytes, Liver function, Liver cancer, Signal Transduction
Abstract

Phosphatidylinositol-3-kinase (PI3K) is a well-known regulator of cell division, motility, and survival in most cell types. Recently, we characterized a novel protein that we call PI3K Interacting Protein 1 (PIK3IP1), which binds to the p110 catalytic subunit of PI3K and reduces its activity in vitro. Little is known about the role of PIK3IP1 in normal and neoplastic growth in vivo. Proper liver function and development depend on intact PI3K signal transduction; when dysregulated, the PI3K pathway is linked to the development of liver cancer. To begin to dissect the contribution of PIK3IP1 to hepatic PI3K signaling in vivo and to liver tumorigenesis in particular, we formulated the following hypothesis: because PIK3IP1 down-regulates PI3K signaling and uncontrolled PI3K signaling is associated with liver cancer, then PIK3IP1-mediated down-regulation of the PI3K pathway should inhibit hepatocellular carcinoma (HCC) development. To test this idea, we generated transgenic mice overexpressing PIK3IP1 in hepatocytes in a mouse strain prone to develop HCC. Isolated PIK3IP1 transgenic mouse hepatocytes showed blunted PI3K signaling, DNA synthetic activity, motility, and survival compared with controls. In vivo, spontaneous liver tumorigenesis was significantly dampened in the transgenic animals. This was accompanied by decreased hepatic PI3K activity and reduced hepatocyte proliferation in the transgenics compared with controls. We also observed that human HCC expressed less PIK3IP1 protein than adjacent matched liver tissue. Our data show that PIK3IP1 is an important regulator of PI3K in vivo, and its dysregulation can contribute to liver carcinogenesis. [Cancer Res 2008;68(14):5591–8]

Published
2008

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