Your search keyword '"Bhupendra S. Kaphalia"' showing total 94 results

1. Spatial and Sex-Dependent Responses of Adult Endogenous Neural Stem Cells to Alcohol Consumption

Author

Erica L. McGrath, Junling Gao, Yong-Fang Kuo, Tiffany J. Dunn, Moniqua J. Ray, Kelly T. Dineley, Kathryn A. Cunningham, Bhupendra S. Kaphalia, and Ping Wu

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Summary: Chronic alcohol abuse results in alcohol-related neurodegeneration, and critical gaps in our knowledge hinder therapeutic development. Neural stem cells (NSCs) are a subpopulation of cells within the adult brain that contribute to brain maintenance and recovery. While it is known that alcohol alters NSCs, little is known about how NSC response to alcohol is related to sex, brain region, and stage of differentiation. Understanding these relationships will aid in therapeutic development. Here, we used an inducible transgenic mouse model to track the stages of differentiation of adult endogenous NSCs and observed distinct NSC behaviors in three brain regions (subventricular zone, subgranular zone, and tanycyte layer) after long-term alcohol consumption. Particularly, chronic alcohol consumption profoundly affected the survival of NSCs in the subventricular zone and altered NSC differentiation in all three regions. Significant differences between male and female mice were further discovered. : Wu and colleagues demonstrate that adult endogenous neural stem cells in three key brain regions have individual responses to alcohol consumption. Further, they show that these regional changes are affected by the sex of mice. Keywords: neural stem cell, chronic alcohol, subgranular zone, subventricular zone, tanycyte, sex differences, neuronal differentiation

Published

2017

2. Recent Advances in Understanding the Complexity of Alcohol-Induced Pancreatic Dysfunction and Pancreatitis Development

Author

Karuna Rasineni, Mukund P. Srinivasan, Appakalai N. Balamurugan, Bhupendra S. Kaphalia, Shaogui Wang, Wen-Xing Ding, Stephen J. Pandol, Aurelia Lugea, Liz Simon, Patricia E. Molina, Peter Gao, Carol A. Casey, Natalia A. Osna, and Kusum K. Kharbanda

Subjects

alcohol, fatty acid ethyl esters, pancreatitis, endoplasmic reticulum stress, autophagy, lysosome, Microbiology, QR1-502

Abstract

Chronic excessive alcohol use is a well-recognized risk factor for pancreatic dysfunction and pancreatitis development. Evidence from in vivo and in vitro studies indicates that the detrimental effects of alcohol on the pancreas are from the direct toxic effects of metabolites and byproducts of ethanol metabolism such as reactive oxygen species. Pancreatic dysfunction and pancreatitis development are now increasingly thought to be multifactorial conditions, where alcohol, genetics, lifestyle, and infectious agents may determine the initiation and course of the disease. In this review, we first highlight the role of nonoxidative ethanol metabolism in the generation and accumulation of fatty acid ethyl esters (FAEEs) that cause multi-organellar dysfunction in the pancreas which ultimately leads to pancreatitis development. Further, we discuss how alcohol-mediated altered autophagy leads to the development of pancreatitis. We also provide insights into how alcohol interactions with other co-morbidities such as smoking or viral infections may negatively affect exocrine and endocrine pancreatic function. Finally, we present potential strategies to ameliorate organellar dysfunction which could attenuate pancreatic dysfunction and pancreatitis severity.

Published

2020

3. Linking Dysregulated AMPK Signaling and ER Stress in Ethanol-Induced Liver Injury in Hepatic Alcohol Dehydrogenase Deficient Deer Mice

Author

Mukund P. Srinivasan, Kamlesh K. Bhopale, Samir M. Amer, Jie Wan, Lata Kaphalia, Ghulam S. Ansari, and Bhupendra S. Kaphalia

Subjects

alcoholic liver disease, alcohol dehydrogenase, ampk signaling, er stress, deer mice, Microbiology, QR1-502

Abstract

Ethanol (EtOH) metabolism itself can be a predisposing factor for initiation of alcoholic liver disease (ALD). Therefore, a dose dependent study to evaluate liver injury was conducted in hepatic alcohol dehydrogenase (ADH) deficient (ADH−) and ADH normal (ADH+) deer mice fed 1%, 2% or 3.5% EtOH in the liquid diet daily for 2 months. Blood alcohol concentration (BAC), liver injury marker (alanine amino transferase (ALT)), hepatic lipids and cytochrome P450 2E1 (CYP2E1) activity were measured. Liver histology, endoplasmic reticulum (ER) stress, AMP-activated protein kinase (AMPK) signaling and cell death proteins were evaluated. Significantly increased BAC, plasma ALT, hepatic lipids and steatosis were found only in ADH− deer mice fed 3.5% EtOH. Further, a significant ER stress and increased un-spliced X-box binding protein 1 were evident only in ADH− deer mice fed 3.5% EtOH. Both strains fed 3.5% EtOH showed deactivation of AMPK, but increased acetyl Co-A carboxylase 1 and decreased carnitine palmitoyltransferase 1A favoring lipogenesis were found only in ADH− deer mice fed 3.5% EtOH. Therefore, irrespective of CYP2E1 overexpression; EtOH dose and hepatic ADH deficiency contribute to EtOH-induced steatosis and liver injury, suggesting a linkage between ER stress, dysregulated hepatic lipid metabolism and AMPK signaling.

Published

2019

4. Dysregulated pancreatic lipid phenotype, inflammation and cellular injury in a chronic ethanol feeding model of hepatic alcohol dehydrogenase-deficient deer mice

Author

Mukund P. Srinivasan, Kamlesh K. Bhopale, Anna A. Caracheo, Lata Kaphalia, Vsevolod L. Popov, Paul J. Boor, and Bhupendra S. Kaphalia

Subjects

General Medicine, General Pharmacology, Toxicology and Pharmaceutics, General Biochemistry, Genetics and Molecular Biology

Published

2023

5. Exposure to binge ethanol and fatty acid ethyl esters exacerbates chronic ethanol-induced pancreatic injury in hepatic alcohol dehydrogenase-deficient deer mice

Author

Mukund P. Srinivasan, Kamlesh K. Bhopale, Anna A. Caracheo, Lata Kaphalia, Bin Gong, Vsevolod L. Popov, Paul J. Boor, G. A. Shakeel Ansari, and Bhupendra S. Kaphalia

Subjects

Peromyscus, Hepatology, Ethanol, Pancreatitis, Alcoholic, Physiology, Physiology (medical), Fatty Acids, Gastroenterology, Alcohol Dehydrogenase, Animals, Blood Alcohol Content, Esters, Research Article

Abstract

Alcoholic chronic pancreatitis (ACP) is a fibroinflammatory disease of the pancreas. However, metabolic basis of ACP is not clearly understood. In this study, we evaluated differential pancreatic injury in hepatic alcohol dehydrogenase-deficient (ADH(−)) deer mice fed chronic ethanol (EtOH), chronic plus binge EtOH, and chronic plus binge EtOH and fatty acid ethyl esters (FAEEs, nonoxidative metabolites of EtOH) to understand the metabolic basis of ACP. Hepatic ADH(−) and ADH normal (ADH(+)) deer mice were fed Lieber-DeCarli liquid diet containing 3% (wt/vol) EtOH for 3 mo. One week before the euthanization, chronic EtOH-fed mice were further administered with an oral gavage of binge EtOH with/without FAEEs. Blood alcohol concentration (BAC), pancreatic injury, and inflammatory markers were measured. Pancreatic morphology, ultrastructural changes, and endoplasmic reticulum (ER)/oxidative stress were examined using H&E staining, electron microscopy, immunostaining, and/or Western blot, respectively. Overall, BAC was substantially increased in chronic EtOH-fed groups of ADH(−) versus ADH(+) deer mice. A significant change in pancreatic acinar cell morphology, with mild to moderate fibrosis and ultrastructural changes evident by dilatations and disruption of ER cisternae, ER/oxidative stress along with increased levels of inflammatory markers were observed in the pancreas of chronic EtOH-fed groups of ADH(−) versus ADH(+) deer mice. Furthermore, chronic plus binge EtOH and FAEEs exposure elevated BAC, enhanced ER/oxidative stress, and exacerbated chronic EtOH-induced pancreatic injury in ADH(−) deer mice suggesting a role of increased body burden of EtOH and its metabolism under reduced hepatic ADH in initiation and progression of ACP. NEW & NOTEWORTHY We established a chronic EtOH feeding model of hepatic alcohol dehydrogenase-deficient (ADH(−)) deer mice, which mimics several fibroinflammatory features of human alcoholic chronic pancreatitis (ACP). The fibroinflammatory and morphological features exacerbated by chronic plus binge EtOH and FAEEs exposure provide a strong case for metabolic basis of ACP. Most importantly, several pathological and molecular targets identified in this study provide a much broader understanding of the mechanism and avenues to develop therapeutics for ACP.

Published

2022

6. Alcohol-induced ketonemia is associated with lowering of blood glucose, downregulation of gluconeogenic genes, and depletion of hepatic glycogen in type 2 diabetic db/db mice

Author

Muthusamy Thangaraju, Mukund P. Srinivasan, Bhupendra S. Kaphalia, Lakshman Segar, and Noha M. Shawky

Subjects

Blood Glucose, Male, 0301 basic medicine, G6PC, medicine.medical_specialty, Diabetic ketoacidosis, Down-Regulation, Ketone Bodies, Biochemistry, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Animals, Phosphorylation, Glycogen synthase, Mice, Knockout, Pharmacology, Glycogen Synthase Kinase 3 beta, Ethanol, biology, Chemistry, Gluconeogenesis, Ketosis, medicine.disease, Liver Glycogen, Ketoacidosis, Fatty Liver, 030104 developmental biology, Endocrinology, Diabetes Mellitus, Type 2, Gene Expression Regulation, Glycogenesis, 030220 oncology & carcinogenesis, Ketone bodies, biology.protein, Steatosis

Abstract

Alcoholic ketoacidosis and diabetic ketoacidosis are life-threatening complications that share the characteristic features of high anion gap metabolic acidosis. Ketoacidosis is attributed in part to the massive release of ketone bodies (e.g., β-hydroxybutyrate; βOHB) from the liver into the systemic circulation. To date, the impact of ethanol consumption on systemic ketone concentration, glycemic control, and hepatic gluconeogenesis and glycogenesis remains largely unknown, especially in the context of type 2 diabetes. In the present study, ethanol intake (36% ethanol- and 36% fat-derived calories) by type 2 diabetic db/db mice for 9 days resulted in significant decreases in weight gain (∼19.5% ↓) and caloric intake (∼30% ↓). This was accompanied by a transition from macrovesicular-to-microvesicular hepatic steatosis with a modest increase in hepatic TG (∼37% ↑). Importantly, ethanol increased systemic βOHB concentration (∼8-fold ↑) with significant decreases in blood glucose (∼4-fold ↓) and plasma insulin and HOMA-IR index (∼3-fold ↓). In addition, ethanol enhanced hepatic βOHB content (∼5-fold ↑) and hmgcs2 mRNA expression (∼3.7-fold ↑), downregulated key gluconeogenic mRNAs (e.g., Pcx, Pck1, and G6pc), and depleted hepatic glycogen (∼4-fold ↓). Furthermore, ethanol intake led to significant decreases in the mRNA/protein expression and allosteric activation of glycogen synthase (GS) in liver tissues regardless of changes in the phosphorylation of GS, GSK-3β, or Akt. Together, our findings suggest that ethanol-induced ketonemia may occur in concomitance with significant lowering of blood glucose concentration, which may be attributed to suppression of gluconeogenesis in the setting of glycogen depletion in type 2 diabetes.

Published

2019

7. Differential Cytotoxicity, ER/Oxidative Stress, Dysregulated AMPKα Signaling and Mitochondrial Stress by Ethanol and its Metabolites in Human Pancreatic Acinar Cells

Author

Mukund P. Srinivasan, Appakalai N. Balamurugan, Kamlesh K. Bhopale, Gopalakrishnan Loganathan, Lata Kaphalia, Cristiana Rastellini, Bhupendra S. Kaphalia, and Anna A. Caracheo

Subjects

medicine.medical_specialty, XBP1, Cell Survival, 030508 substance abuse, Medicine (miscellaneous), Oxidative phosphorylation, Acetaldehyde, Acinar Cells, AMP-Activated Protein Kinases, Toxicology, medicine.disease_cause, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Downregulation and upregulation, AMP-Activated Protein Kinase Kinases, Internal medicine, medicine, Acinar cell, Humans, Mitogen-Activated Protein Kinase 9, Mitogen-Activated Protein Kinase 8, Pancreas, Mitogen-Activated Protein Kinase 1, Mitogen-Activated Protein Kinase 3, Carnitine O-Palmitoyltransferase, Ethanol, Central Nervous System Depressants, Esters, Metabolism, Endoplasmic Reticulum Stress, Mitochondria, Psychiatry and Mental health, Oxidative Stress, Endocrinology, chemistry, Unfolded protein response, 0305 other medical science, 030217 neurology & neurosurgery, Oxidative stress, Acetyl-CoA Carboxylase

Abstract

Background Alcoholic chronic pancreatitis (ACP) is a serious inflammatory disorder of the exocrine pancreatic gland. A previous study from this laboratory showed that ethanol (EtOH) causes cytotoxicity, dysregulates AMPKα and ER/oxidative stress signaling, and induces inflammatory responses in primary human pancreatic acinar cells (hPACs). Here we examined the differential cytotoxicity of EtOH and its oxidative (acetaldehyde) and nonoxidative (fatty acid ethyl esters; FAEEs) metabolites in hPACs was examined to understand the metabolic basis and mechanism of ACP. Methods We evaluated concentration-dependent cytotoxicity, AMPKα inactivation, ER/oxidative stress, and inflammatory responses in hPACs by incubating them for 6 h with EtOH, acetaldehyde, or FAEEs at clinically relevant concentrations reported in alcoholic subjects using conventional methods. Cellular bioenergetics (mitochondrial stress and a real-time ATP production rate) were determined using Seahorse XFp Extracellular Flux Analyzer in AR42J cells treated with acetaldehyde or FAEEs. Results We observed concentration-dependent increases in LDH release, inactivation of AMPKα along with upregulation of ACC1 and FAS (key lipogenic proteins), downregulation of p-LKB1 (an oxidative stress-sensitive upstream kinase regulating AMPKα) and CPT1A (involved in β-oxidation of fatty acids) in hPACs treated with EtOH, acetaldehyde, or FAEEs. Concentration-dependent increases in oxidative stress and ER stress as measured by GRP78, unspliced XBP1, p-eIF2α, and CHOP along with activation of p-JNK1/2, p-ERK1/2, and p-P38MAPK were present in cells treated with EtOH, acetaldehyde, or FAEEs, respectively. Furthermore, a significant decrease was observed in the total ATP production rate with subsequent mitochondrial stress in AR42J cells treated with acetaldehyde and FAEEs. Conclusions EtOH and its metabolites, acetaldehyde and FAEEs, caused cytotoxicity, ER/oxidative and mitochondrial stress, and dysregulated AMPKα signaling, suggesting a key role of EtOH metabolism in the etiopathogenesis of ACP. Because oxidative EtOH metabolism is negligible in the exocrine pancreas, the pathogenesis of ACP could be attributable to the formation of FAEEs and related pancreatic acinar cell injury.

Published

2021

8. Activation of AMP-activated protein kinase attenuates ethanol-induced ER/oxidative stress and lipid phenotype in human pancreatic acinar cells

Author

Shamis Khan, Appakalai N. Balamurugan, Samir M. Amer, Mukund P. Srinivasan, Lata Kaphalia, Bhupendra S. Kaphalia, Gopalakrishnan Loganathan, Kamlesh K. Bhopale, and Anna A. Caracheo

Subjects

0301 basic medicine, Adult, Male, Acinar Cells, AMP-Activated Protein Kinases, Fatty Acids, Nonesterified, medicine.disease_cause, Endoplasmic Reticulum, Biochemistry, Article, 03 medical and health sciences, 0302 clinical medicine, AMP-activated protein kinase, Acinar cell, medicine, Humans, Protein kinase A, Endoplasmic Reticulum Chaperone BiP, Pancreas, Cells, Cultured, Pharmacology, biology, Dose-Response Relationship, Drug, Ethanol, Chemistry, Endoplasmic reticulum, Middle Aged, Lipids, Cell biology, Oxidative Stress, 030104 developmental biology, Phenotype, Mitochondrial biogenesis, 030220 oncology & carcinogenesis, Lipogenesis, Unfolded protein response, biology.protein, Female, Oxidative stress, Acyltransferases

Abstract

Primary toxicity targets of alcohol and its metabolites in the pancreas are cellular energetics and endoplasmic reticulum (ER). Therefore, the role of AMP-Activated Protein Kinase (AMPKα) in amelioration of ethanol (EtOH)-induced pancreatic acinar cell injury including ER/oxidative stress, inflammatory responses, the formation of fatty acid ethyl esters (FAEEs) and mitochondrial bioenergetics were determined in human pancreatic acinar cells (hPACs) and AR42J cells incubated with/without AMPKα activator [5-aminoimidazole-4-carboxamide ribonucleotide (AICAR)]. EtOH treated hPACs showed concentration and time-dependent increases for FAEEs and inactivation of AMPKα, along with the upregulation of ACC1 and FAS (key lipogenic proteins) and downregulation of CPT1A (involved β-oxidation of fatty acids). These cells also showed significant ER stress as evidenced by the increased expression for GRP78, IRE1α, and PERK/CHOP arm of unfolded protein response promoting apoptosis and activating p-JNK1/2 and p-ERK1/2 with increased secretion of cytokines. AR42J cells treated with EtOH showed increased oxidative stress, impaired mitochondrial biogenesis, and decreased ATP production rate. However, AMPKα activation by AICAR attenuated EtOH-induced ER/oxidative stress, lipogenesis, and inflammatory responses as well as the formation of FAEEs and restored mitochondrial function in hPACs as well as AR42J cells. Therefore, it is likely that EtOH-induced inactivation of AMPKα plays a crucial role in acinar cell injury leading to pancreatitis. Findings from this study also suggest that EtOH-induced inactivation of AMPKα is closely related to ER/oxidative stress and synthesis of FAEEs, as activation of AMPKα by AICAR attenuates formation of FAEEs, ER/oxidative stress and lipogenesis, and improves inflammatory responses and mitochondrial bioenergetics.

Published

2020

9. Ethanol-Induced Mitochondrial Bioenergetic Dysfunctions Are Attributed to Ethanol Metabolites in Bronchial Epithelial Cells

Author

Mukund P. Srinivasan, Bhupendra S. Kaphalia, William J. Calhoun, and Lata Kaphalia

Subjects

chemistry.chemical_compound, Ethanol, Bioenergetics, Biochemistry, Chemistry

Published

2020

10. Recent Advances in Understanding the Complexity of Alcohol-Induced Pancreatic Dysfunction and Pancreatitis Development

Author

Mukund P. Srinivasan, Natalia A. Osna, Carol A. Casey, Bhupendra S. Kaphalia, Karuna Rasineni, Appakalai N. Balamurugan, Stephen J. Pandol, Wen-Xing Ding, Liz Simon, Peter Gao, Shaogui Wang, Aurelia Lugea, Kusum K. Kharbanda, and Patricia E. Molina

Subjects

0301 basic medicine, autophagy, lcsh:QR1-502, pancreatitis, Disease, Review, Bioinformatics, Biochemistry, lcsh:Microbiology, 03 medical and health sciences, 0302 clinical medicine, Lysosome, Insulin Secretion, medicine, Endocrine system, Animals, Humans, Ethanol metabolism, Molecular Biology, chemistry.chemical_classification, Reactive oxygen species, business.industry, alcohol, Autophagy, medicine.disease, Alcoholism, 030104 developmental biology, medicine.anatomical_structure, chemistry, transcription factor EB (TFEB), endoplasmic reticulum stress, lysosome, Unfolded Protein Response, Pancreatitis, 030211 gastroenterology & hepatology, fatty acid ethyl esters, Pancreas, business

Abstract

Chronic excessive alcohol use is a well-recognized risk factor for pancreatic dysfunction and pancreatitis development. Evidence from in vivo and in vitro studies indicates that the detrimental effects of alcohol on the pancreas are from the direct toxic effects of metabolites and byproducts of ethanol metabolism such as reactive oxygen species. Pancreatic dysfunction and pancreatitis development are now increasingly thought to be multifactorial conditions, where alcohol, genetics, lifestyle, and infectious agents may determine the initiation and course of the disease. In this review, we first highlight the role of nonoxidative ethanol metabolism in the generation and accumulation of fatty acid ethyl esters (FAEEs) that cause multi-organellar dysfunction in the pancreas which ultimately leads to pancreatitis development. Further, we discuss how alcohol-mediated altered autophagy leads to the development of pancreatitis. We also provide insights into how alcohol interactions with other co-morbidities such as smoking or viral infections may negatively affect exocrine and endocrine pancreatic function. Finally, we present potential strategies to ameliorate organellar dysfunction which could attenuate pancreatic dysfunction and pancreatitis severity.

Published

2020

11. Spatial and Sex-Dependent Responses of Adult Endogenous Neural Stem Cells to Alcohol Consumption

Author

Kelly T. Dineley, Kathryn A. Cunningham, Tiffany J. Dunn, Erica L. McGrath, Yong Fang Kuo, Junling Gao, Moniqua J. Ray, Ping Wu, and Bhupendra S. Kaphalia

Subjects

0301 basic medicine, sex differences, Male, Endogeny, Biochemistry, Subgranular zone, neural stem cell, Mice, 0302 clinical medicine, Neural Stem Cells, Lateral Ventricles, chronic alcohol, lcsh:QH301-705.5, reproductive and urinary physiology, Neurons, lcsh:R5-920, Brain Mapping, Tanycyte, Neurodegeneration, subventricular zone, Cell Differentiation, Anatomy, Neural stem cell, Adult Stem Cells, medicine.anatomical_structure, Female, biological phenomena, cell phenomena, and immunity, lcsh:Medicine (General), Alcohol consumption, Genetically modified mouse, Alcohol Drinking, Subventricular zone, Mice, Transgenic, Biology, Article, 03 medical and health sciences, Genetics, medicine, Animals, neuronal differentiation, Cell Biology, tanycyte, medicine.disease, subgranular zone, nervous system diseases, Disease Models, Animal, 030104 developmental biology, lcsh:Biology (General), nervous system, Alcohols, Nerve Degeneration, Neuroscience, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Summary Chronic alcohol abuse results in alcohol-related neurodegeneration, and critical gaps in our knowledge hinder therapeutic development. Neural stem cells (NSCs) are a subpopulation of cells within the adult brain that contribute to brain maintenance and recovery. While it is known that alcohol alters NSCs, little is known about how NSC response to alcohol is related to sex, brain region, and stage of differentiation. Understanding these relationships will aid in therapeutic development. Here, we used an inducible transgenic mouse model to track the stages of differentiation of adult endogenous NSCs and observed distinct NSC behaviors in three brain regions (subventricular zone, subgranular zone, and tanycyte layer) after long-term alcohol consumption. Particularly, chronic alcohol consumption profoundly affected the survival of NSCs in the subventricular zone and altered NSC differentiation in all three regions. Significant differences between male and female mice were further discovered., Highlights • Alcohol alters neural stem cell differentiation in a region-dependent manner • Sex plays a role in neural stem cell response to alcohol consumption • Sex contributes to regional differences of neural stem cell response to alcohol, Wu and colleagues demonstrate that adult endogenous neural stem cells in three key brain regions have individual responses to alcohol consumption. Further, they show that these regional changes are affected by the sex of mice.

Published

2017

12. Proteomic Profiling of Liver and Plasma in Chronic Ethanol Feeding Model of Hepatic Alcohol Dehydrogenase-Deficient Deer Mice

Author

Kamlesh K. Bhopale, Samir M. Amer, Lata Kaphalia, Ghulam Ansari, Bhupendra S. Kaphalia, John E. Wiktorowicz, and Kizhake V. Soman

Subjects

Male, Proteomics, 0301 basic medicine, Alcoholic liver disease, medicine.medical_specialty, Medicine (miscellaneous), Biology, Toxicology, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, Peromyscus, 0302 clinical medicine, Internal medicine, medicine, Animals, Liver Diseases, Alcoholic, Alcohol dehydrogenase, chemistry.chemical_classification, Ethanol, Alcohol Dehydrogenase, Carbamoyl phosphate synthetase, Ornithine, medicine.disease, Blood proteins, Psychiatry and Mental health, 030104 developmental biology, Endocrinology, Enzyme, Liver, chemistry, biology.protein, Steatosis, Carbonic anhydrase 3, 030217 neurology & neurosurgery

Abstract

Background Chronic alcohol abuse, a major risk factor for such diseases as hepatitis and cirrhosis, impairs hepatic alcohol dehydrogenase (ADH; key ethanol [EtOH]-metabolizing enzyme). Therefore, differentially altered hepatic and plasma proteomes were identified in chronic EtOH feeding model of hepatic ADH-deficient (ADH−) deer mice to understand the metabolic basis of alcoholic liver disease (ALD). Methods ADH− deer mice were fed 3.5 g% EtOH via Lieber–DeCarli liquid diet daily for 3 months and histology of the liver assessed. Liver and plasma proteins were separated by 2-dimensional gel electrophoresis. The proteins differentially expressed were identified by matrix-assisted laser desorption ionization-time of flight mass spectrometry. Results Histology of the liver showed panlobular steatosis and infiltration of T lymphocytes. Using the criteria of ≥1.5 for fold change (p-value ≤0.05) with expectation value (E ≤10−3) and protein score (≥64), 18 proteins in the livers and 5 in the plasma of EtOH-fed mice were differentially expressed and identified. Prolyl 4-hydroxylase, cytochrome b-5, endo A cytokeratin, ATP synthase, heat-shock 70 kD proteins, enoyl CoA hydratase, stress-70 protein, peroxiredoxin 1, and ornithine carbamoyl transferase were up-regulated in the livers. However, carbonic anhydrase 3, mitochondrial ATP synthase, aldolase 2, actin γ, laminin receptor, and carbamoyl phosphate synthase were down-regulated. Contrary to the increased expression of creatine kinase M-type, a decreased expression of serine protease inhibitor A3A precursor, sulfated glycoprotein-2 (clusterin), and apolipoprotein E isoforms were found in the plasma of EtOH group. Conclusions Chronic EtOH feeding in ADH− deer mice causes steatosis and infiltration of T lymphocytes in the livers along with increased expression of proteins involved in endoplasmic reticulum (ER) stress, fibrosis, fatty acid β oxidation and biogenesis, and decreased expression of proteins involved in ATP synthesis, carbohydrate metabolism, in cell regulation and architecture. Reduced expression of various carrier proteins as found in the plasma of EtOH group has a biomarker potential.

Published

2017

13. Proteins Differentially Expressed in the Pancreas of Hepatic Alcohol Dehydrogenase–Deficient Deer Mice Fed Ethanol For 3 Months

Author

Samir M. Amer, Lata Kaphalia, Kamlesh K. Bhopale, Kizhake V. Soman, Ghulam Ansari, John E. Wiktorowicz, and Bhupendra S. Kaphalia

Subjects

0301 basic medicine, medicine.medical_specialty, Ethanol, Liquid diet, Hepatology, biology, Pancreatic tissue, Endocrinology, Diabetes and Metabolism, Alcohol, Proteomics, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Endocrinology, medicine.anatomical_structure, chemistry, 030220 oncology & carcinogenesis, Internal medicine, Internal Medicine, medicine, biology.protein, Pancreas, Alcohol dehydrogenase

Abstract

ObjectivesThe aim of this study was to identify differentially expressed proteins in the pancreatic tissue of hepatic alcohol dehydrogenase–deficient deer mice fed ethanol to understand metabolic basis and mechanism of alcoholic chronic pancreatitis.MethodsMice were fed liquid diet containing 3.5 g%

Published

2017

14. Ethanol exposure impairs AMPK signaling and phagocytosis in human alveolar macrophages: Role of ethanol metabolism

Author

Ramu Kakumanu, William J. Calhoun, Mukund P. Srinivasan, Bhupendra S. Kaphalia, and Lata Kaphalia

Subjects

medicine.medical_specialty, Phagocytosis, 030508 substance abuse, Medicine (miscellaneous), AMP-Activated Protein Kinases, Toxicology, medicine.disease_cause, Article, 03 medical and health sciences, 0302 clinical medicine, Transforming Growth Factor beta, Internal medicine, mental disorders, Macrophages, Alveolar, medicine, Humans, Ethanol metabolism, Protein kinase A, Protein Kinase Inhibitors, Chemokine CCL2, Ethanol, Chemistry, Endoplasmic reticulum, Interleukins, Fatty Acids, AMPK, Esters, Ribonucleotides, Aminoimidazole Carboxamide, Endoplasmic Reticulum Stress, Psychiatry and Mental health, Oxidative Stress, Endocrinology, Alveolar macrophage, Unfolded protein response, 0305 other medical science, 030217 neurology & neurosurgery, Oxidative stress, Signal Transduction

Abstract

Background Chronic alcohol consumption impairs alveolar macrophage's (AM) function and increases risk for developing lung infection and pneumonia. However, the mechanism and metabolic basis of alcohol-induced AM dysfunction leading to lung infection are not well defined, but may include altered ethanol (EtOH) and reactive oxygen species metabolism and cellular energetics. Therefore, oxidative stress, endoplasmic reticulum (ER) stress, the formation of fatty acid ethyl esters [FAEEs, nonoxidative metabolites of EtOH], AMP-activated protein kinase (AMPK) signaling, and phagocytic function were examined in freshly isolated AM incubated with EtOH. Methods AMs separated from bronchoalveolar lavage fluid samples obtained from normal volunteers were incubated with EtOH for 24 hours. AMPK signaling and ER stress were assessed using Western blotting, FAEEs by GC-MS, oxidative stress by immunofluorescence using antibodies to 4-hydroxynonenal, and phagocytosis by latex beads. Oxidative stress was also measured in EtOH-treated AMs with/without AMPK activator [5-aminoimidazole-4-carboxamide ribonucleotide (AICAR)] or inhibitor (Compound C), and in AMs incubated with FAEEs. mRNA expression for interleukins (IL-6 and IL-8), monocyte chemoattractant protein (MCP)-1, and transforming growth factor (TGF)-β was measured in AM treated with EtOH or FAEEs using RT-PCR. Results EtOH exposure to AM increased oxidative stress, ER stress, and synthesis of FAEEs, decreased phosphorylated AMPK, and impaired phagocytosis. Attenuation or exacerbation of EtOH-induced oxidative stress by AICAR or Compound C, respectively, suggests a link between AMPK signaling, EtOH metabolism, and related oxidative stress. The formation of FAEEs may contribute to EtOH-induced oxidative stress as FAEEs also produced concentration-dependent oxidative stress. An increased mRNA expression of IL-6, IL-8, and MCP-1 by FAEEs is key finding to suggest a metabolic basis of EtOH-induced inflammatory response. Conclusions EtOH-induced impaired phagocytosis, oxidative stress, ER stress, and dysregulated AMPK signaling are plausibly associated with the formation of FAEEs and may participate in the pathogenesis of nonspecific pulmonary inflammation.

Published

2019

15. DISTRIBUTION OF PETROGENIC POLYCYCLIC AROMATIC HYDROCARBONS (PAHs) IN SEAFOOD FOLLOWING DEEPWATER HORIZON OIL SPILL

Author

Cornelis J. Elferink, Kamlesh K. Bhopale, G. A. Shakeel Ansari, Harshica Fernando, Ramu Kakumanu, Sharon Croisant, Bhupendra S. Kaphalia, and Hyunsu Ju

Subjects

0106 biological sciences, Oyster, Brachyura, Food Contamination, 010501 environmental sciences, Aquatic Science, Oceanography, Quechers, 01 natural sciences, Article, Gas Chromatography-Mass Spectrometry, Mississippi, Penaeidae, biology.animal, Animals, Petroleum Pollution, Polycyclic Aromatic Hydrocarbons, 0105 earth and related environmental sciences, biology, 010604 marine biology & hydrobiology, Contamination, Coastal community, Crude oil, Louisiana, Pollution, Ostreidae, Shrimp, Seafood, Deepwater horizon, Environmental chemistry, Oil spill, Alabama, Environmental science, Water Pollutants, Chemical, Environmental Monitoring

Abstract

A community-based participatory research was utilized to address the coastal community's concern regarding Deepwater Horizon oil contamination of seafood. Therefore, we analyzed polycyclic aromatic hydrocarbons (PAHs), major toxic constituents of crude oil, in the seafood collected from gulf coast (Louisiana, Alabama and Mississippi) during December 2011-February 2014. PAHs were extracted from edible part of shrimp, oysters, and crabs by the QuEChERS/dsPE procedure and analyzed by gas chromatography-mass spectrometry. The total PAHs data were further analyzed using the General Linear Mixed Model procedure of the SAS (Version 9.3, SAS Institute, Inc., Cary, NC) statistical software. Brown shrimp showed statistically significant differences in PAHs levels with respect to time and locations while white shrimp showed differences at various time points. PAHs levels in oyster and crab samples were not statistically different at the Type I error of 0.05. Overall, the PAHs levels are far below FDA levels of concern for human consumption.

Published

2019

16. Over Expression of Cathepsin B and Its Induction by Ethanol in Asthmatic Vs Non-Asthmatic Bronchial Epithelial Cells and Related AMPKα and ER Stress Signaling

Author

Lata Kaphalia, William J. Calhoun, Bhupendra S. Kaphalia, and Mukund P. Srinivasan

Subjects

medicine.medical_specialty, chemistry.chemical_compound, Endocrinology, Ethanol, Chemistry, Internal medicine, medicine, Over expression, Unfolded protein response, Cathepsin B

Published

2019

17. Contributors

Author

Arturo Anadón, Vellareddy Anantharam, Anthony E. Archibong, Irma Ares, Adam D. Aulbach, Nikee Awasthee, Aryamitra Banerjee, Leah D. Banks, Frank A. Barile, Sudheer R. Beedanagari, Charalampos Belantis, Enrico Bergamaschi, Sadikshya Bhandari, Sneha P. Bhatia, Karyn Bischoff, David J. Borts, Emily Brehm, Subash Chandra Gupta, Saurabh Chatterjee, Catheryne Chiang, Anirudh J. Chintalapati, P. Cohn, Robert W. Coppock, Lucio G. Costa, Tirupapuliyur V. Damodaran, Clinton D'Souza, Wolf-D. Dettbarn, Amy A. Devlin, Robin B. Doss, Shiwangi Dwivedi, Margitta M. Dziwenka, Jorge Estévez, Daniel S. Fabricant, A.M. Fan, Vanessa A. Fitsanakis, John Flaskos, Jodi A. Flaws, Swaran J.S. Flora, Sue M. Ford, Jessica S. Fortin, Domniki Fragou, Shayne C. Gad, Bianca Galateanu, Dale R. Gardner, George Georgiadis, Fernando Gil, Saryu Goel, Mary Gulumian, P.K. Gupta, Ramesh C. Gupta, Rekha K. Gupta, Sharon Gwaltney-Brant, Alan J. Hargreaves, Kelly L. Harris, Kenneth J. Harris, Holly E. Hatfield, Wallace A. Hayes, Ioannis Heretis, Antonio F. Hernández, Corey J. Hilmas, Darryl B. Hood, Pasi Huuskonen, Stewart B. Jacobson, Sandra A. James-Yi, Huajun Jin, Jun Kanno, Arthi Kanthasamy, Anumantha G. Kanthasamy, Shilpa N. Kaore, Navinchandra M. Kaore, Bhupendra S. Kaphalia, Vesa Karttunen, Gurjot Kaur, Ravneet Kaur, Prasada Rao S. Kodavanti, Urmila P. Kodavanti, George A. Kontadakis, Gopala Krishna, Priya A. Krishna, Kavya A. Krishna, Maria Kummu, George D. Kymionis, Rajiv Lall, P. Lin, Bommanna G. Loganathan, Jarkko Loikkanen, Marcello Lotti, Michael A. Lynes, Brinda Mahadevan, Jitendra K. Malik, Charalampos Mamoulakis, Jane A. Mantey, María Rosa Martínez-Larrañaga, María Aránzazu Martínez, Charalampos Mavridis, Roger O. McClellan, Vincent P. Meador, Lars Friis Mikkelsen, Dejan Milatovic, Ida R. Miller Mukherjee, Anupama Mukherjee, Pushpinder Kaur Multani, Päivi Myllynen, Kirsi Myöhänen, Rekek Negga, Carolina Negrei, Meliton N. Novilla, Stephanie Padilla, Carlos M. Palmeira, Kip E. Panter, Markku Pasanen, Daniel J. Patrick, Sofia Pavanello, Henrik Duelund Pedersen, Olavi Pelkonen, Michael A. Pellizzon, Jason Pitt, Argyro Plaka, Aramandla Ramesh, Saniya Rattan, Jenni Repo, Matthew R. Ricci, Anabela P. Rolo, Magdalini Sachana, Heidi Sahlman, Nitin Saini, Vandana Saini, Kai Savolainen, Ratanesh Kumar Seth, Abha Sharma, Anurag Sharma, Elina Sieppi, Rui Silva, Anita Sinha, Iordanis Skamagkas, Samantha J. Snow, Miguel A. Sogorb, Ajay Srivastava, Szabina A. Stice, Markus Storvik, David T. Szabo, João S. Teodoro, Aristidis M. Tsatsakis, John Tsiaoussis, Kirsi Vähäkangas, Sumit Singh Verma, Eugenio Vilanova, Suryanarayana V. Vulimiri, Genoa R. Warner, Kevin D. Welch, Christina Wilson-Frank, S.H. You, Snjezana Zaja-Milatovic, Ioannis E. Zisis, and Csaba K. Zoltani

Published

2019

18. Early Biomarkers of Acute and Chronic Pancreatitis

Author

Bhupendra S. Kaphalia

Subjects

Poor prognosis, medicine.medical_specialty, business.industry, Omics, medicine.disease, Gastroenterology, Internal medicine, Clinical diagnosis, medicine, Biomarker (medicine), Serum lipase, Acute pancreatitis, Pancreatitis, In patient, business

Abstract

Advanced stages of chronic pancreatitis and pancreatic cancers (PCs) are very serious diseases with very poor prognosis. Therefore, identification of reliable and specific biomarker(s) at early stages of the diseases could be key to their early prevention and therapy. In this chapter, currently used and putative biomarkers of acute and chronic pancreatitis and PC are summarized. Total serum lipase and/or amylase are most widely used biomarkers of acute pancreatitis; lipase assay being more sensitive and specific than that of amylase. Imaging technologies provide key support for the diagnosis of both acute and chronic pancreatitis. Biomarkers of chronic pancreatitis are poorly developed and remain challenging because of impaired secretory components of exocrine pancreas. The focus of future clinical diagnosis of chronic pancreatitis and PC lies in identification of biomarkers using omics and microRNA arrays along with imaging technologies in well-defined experimental models and their validation in patients diagnosed with various stages of chronic pancreatitis and PC.

Published

2019

19. Adult Neural Stem Cells Show Regional and Sex‐Dependent Responses to Chronic Poly‐Drug Administration

Author

Sonja J. Stutz, Kelly T. Dineley, Kathryn A. Cunningham, Robert O. Fox, Caitlin R. Schlagal, Bhupendra S. Kaphalia, Ping Wu, Junling Gao, Tiffany J. Dunn, and Erica L. McGrath

Subjects

business.industry, Genetics, Medicine, Drug administration, Pharmacology, business, Molecular Biology, Biochemistry, Neural stem cell, Biotechnology

Published

2018

20. Hepatic alcohol dehydrogenase deficiency induces pancreatic injury in chronic ethanol feeding model of deer mice

Author

Vsevolod L. Popov, Inas H. El-Mehallawi, Magdy M. Ashmawy, Samir M. Amer, G. A. Shakeel Ansari, Bhupendra S. Kaphalia, Bill A. Rampy, Ramu Kakumanu, and Kamlesh K. Bhopale

Subjects

0301 basic medicine, medicine.medical_specialty, Glucose-regulated protein, Clinical Biochemistry, Endoplasmic Reticulum, Cathepsin B, Article, Pathology and Forensic Medicine, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Peromyscus, Internal medicine, medicine, Animals, Inositol, Molecular Biology, Pancreas, Alcohol dehydrogenase, biology, Ethanol, ATF6, Fatty Acids, Alcohol Dehydrogenase, medicine.disease, Endoplasmic Reticulum Stress, Alcoholism, Disease Models, Animal, Ethyl Ethers, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, chemistry, Liver, biology.protein, Unfolded protein response, Pancreatitis, 030211 gastroenterology & hepatology, Blood Alcohol Content

Abstract

The single most common cause of chronic pancreatitis (CP, a serious inflammatory disease) is chronic alcohol abuse, which impairs hepatic alcohol dehydrogenase (ADH, a major ethanol oxidizing enzyme). Previously, we found ~5 fold greater fatty acid ethyl esters (FAEEs), and injury in the pancreas of hepatic ADH deficient (ADH-) vs. hepatic normal ADH (ADH+) deer mice fed 3.5g% ethanol via liquid diet daily for two months. Therefore, progression of ethanol-induced pancreatic injury was determined in ADH- deer mice fed ethanol for four months to delineate the mechanism and metabolic basis of alcoholic chronic pancreatitis (ACP). In addition to a substantially increased blood alcohol concentration and plasma FAEEs, significant degenerative changes, including atrophy and loss of acinar cells in some areas, ultrastructural changes evident by such features as swelling and disintegration of endoplasmic reticulum (ER) cisternae and ER stress were observed in the pancreas of ethanol-fed ADH- deer mice vs. ADH+ deer mice. These changes are consistent with noted increases in pancreatic injury markers (plasma lipase, pancreatic trypsinogen activation peptide, FAEE synthase and cathepsin B) in ethanol-fed ADH- deer mice. Most importantly, an increased levels of pancreatic glucose regulated protein (GRP) 78 (a prominent ER stress marker) were found to be closely associated with increased phosphorylated eukaryotic initiation factor (eIF) 2α signaling molecule in PKR-like ER kinase branch of unfolded protein response (UPR) as compared to X box binding protein 1S and activating transcription factor (ATF)6 - 50kDa protein of inositol requiring enzyme 1α and ATF6 branches of UPR, respectively, in ethanol-fed ADH- vs. ADH+ deer mice. These results along with findings on plasma FAEEs, and pancreatic histology and injury markers suggest a metabolic basis of ethanol-induced pancreatic injury, and provide new avenues to understand metabolic basis and molecular mechanism of ACP.

Published

2018

21. Ethanol metabolism, oxidative stress, and endoplasmic reticulum stress responses in the lungs of hepatic alcohol dehydrogenase deficient deer mice after chronic ethanol feeding

Author

William J. Calhoun, Ju Hyunsu, Nahal Boroumand, Lata Kaphalia, and Bhupendra S. Kaphalia

Subjects

Male, medicine.medical_specialty, Time Factors, Alcohol Drinking, Genotype, Acetaldehyde, Lung injury, Endoplasmic Reticulum, Toxicology, medicine.disease_cause, Article, chemistry.chemical_compound, Peromyscus, Internal medicine, medicine, Animals, Ethanol metabolism, Lung, Alcohol dehydrogenase, Pharmacology, Caspase 8, Esterification, Ethanol, biology, Caspase 3, Alcoholic lung disease, Fatty Acids, Alcohol Dehydrogenase, Cytochrome P-450 CYP2E1, Esters, CYP2E1, Endoplasmic Reticulum Stress, Oxidative Stress, Phenotype, Endocrinology, Liver, chemistry, Immunology, Unfolded Protein Response, biology.protein, Unfolded protein response, Oxidative stress

Abstract

Consumption and over-consumption of alcoholic beverages are well-recognized contributors to a variety of pulmonary disorders, even in the absence of intoxication. The mechanisms by which alcohol (ethanol) may produce disease include oxidative stress and prolonged endoplasmic reticulum (ER) stress. Many aspects of these processes remain incompletely understood due to a lack of a suitable animal model. Chronic alcohol over-consumption reduces hepatic alcohol dehydrogenase (ADH), the principal canonical metabolic pathway of ethanol oxidation. We therefore modeled this situation using hepatic ADH-deficient deer mice fed 3.5% ethanol daily for 3 months. Blood ethanol concentration was 180 mg% in ethanol fed mice, compared to

Published

2014

22. Linking Dysregulated AMPK Signaling and ER Stress in Ethanol-Induced Liver Injury in Hepatic Alcohol Dehydrogenase Deficient Deer Mice

Author

Samir M. Amer, Mukund P. Srinivasan, Bhupendra S. Kaphalia, Ghulam Ansari, Lata Kaphalia, Kamlesh K. Bhopale, and Jie Wan

Subjects

Male, 0301 basic medicine, Alcoholic liver disease, lcsh:QR1-502, AMP-Activated Protein Kinases, er stress, Biochemistry, lcsh:Microbiology, Gene Knockout Techniques, Mice, 0302 clinical medicine, ampk signaling, deer mice, Liver injury, biology, Chemistry, alcohol dehydrogenase, Alanine Transaminase, CYP2E1, Endoplasmic Reticulum Stress, Liver, Lipogenesis, Blood Alcohol Content, 030211 gastroenterology & hepatology, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, alcoholic liver disease, endocrine system, medicine.medical_specialty, Article, 03 medical and health sciences, Internal medicine, mental disorders, medicine, Animals, AMPK signaling, ER stress, Liver Diseases, Alcoholic, Molecular Biology, Alcohol dehydrogenase, Ethanol, urogenital system, AMPK, Lipid Metabolism, medicine.disease, Disease Models, Animal, 030104 developmental biology, Endocrinology, biology.protein, Unfolded protein response, Steatosis

Abstract

Ethanol (EtOH) metabolism itself can be a predisposing factor for initiation of alcoholic liver disease (ALD). Therefore, a dose dependent study to evaluate liver injury was conducted in hepatic alcohol dehydrogenase (ADH) deficient (ADH−) and ADH normal (ADH+) deer mice fed 1%, 2% or 3.5% EtOH in the liquid diet daily for 2 months. Blood alcohol concentration (BAC), liver injury marker (alanine amino transferase (ALT)), hepatic lipids and cytochrome P450 2E1 (CYP2E1) activity were measured. Liver histology, endoplasmic reticulum (ER) stress, AMP-activated protein kinase (AMPK) signaling and cell death proteins were evaluated. Significantly increased BAC, plasma ALT, hepatic lipids and steatosis were found only in ADH− deer mice fed 3.5% EtOH. Further, a significant ER stress and increased un-spliced X-box binding protein 1 were evident only in ADH− deer mice fed 3.5% EtOH. Both strains fed 3.5% EtOH showed deactivation of AMPK, but increased acetyl Co-A carboxylase 1 and decreased carnitine palmitoyltransferase 1A favoring lipogenesis were found only in ADH− deer mice fed 3.5% EtOH. Therefore, irrespective of CYP2E1 overexpression; EtOH dose and hepatic ADH deficiency contribute to EtOH-induced steatosis and liver injury, suggesting a linkage between ER stress, dysregulated hepatic lipid metabolism and AMPK signaling.

Published

2019

23. Liver proteomics in progressive alcoholic steatosis

Author

John E. Wiktorowicz, Bhupendra S. Kaphalia, M. Firoze Khan, G. A. Shakeel Ansari, Harshica Fernando, and Kizhake V. Soman

Subjects

Male, Proteomics, medicine.medical_specialty, Alcoholic liver disease, Toxicology, Article, Liver disease, chemistry.chemical_compound, Internal medicine, medicine, Animals, Electrophoresis, Gel, Two-Dimensional, Alcohol dehydrogenase, Pharmacology, Methionine, Ethanol, biology, Fatty liver, medicine.disease, Rats, Inbred F344, Rats, Disease Models, Animal, Endocrinology, Gene Expression Regulation, Biochemistry, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, Regression Analysis, Steatosis, Steatohepatitis, Fatty Liver, Alcoholic

Abstract

Fatty liver is an early stage of alcoholic and nonalcoholic liver disease (ALD and NALD) that progresses to steatohepatitis and other irreversible conditions. In this study, we identified proteins that were differentially expressed in the livers of rats fed 5% ethanol in a Lieber–DeCarli diet daily for 1 and 3 months by discovery proteomics (two-dimensional gel electrophoresis and mass spectrometry) and non-parametric modeling (Multivariate Adaptive Regression Splines). Hepatic fatty infiltration was significantly higher in ethanol-fed animals as compared to controls, and more pronounced at 3 months of ethanol feeding. Discovery proteomics identified changes in the expression of proteins involved in alcohol, lipid, and amino acid metabolism after ethanol feeding. At 1 and 3 months, 12 and 15 different proteins were differentially expressed. Of the identified proteins, down regulation of alcohol dehydrogenase (− 1.6) at 1 month and up regulation of aldehyde dehydrogenase (2.1) at 3 months could be a protective/adaptive mechanism against ethanol toxicity. In addition, betaine-homocysteine S-methyltransferase 2 a protein responsible for methionine metabolism and previously implicated in fatty liver development was significantly up regulated (1.4) at ethanol-induced fatty liver stage (1 month) while peroxiredoxin-1 was down regulated (− 1.5) at late fatty liver stage (3 months). Nonparametric analysis of the protein spots yielded fewer proteins and narrowed the list of possible markers and identified d -dopachrome tautomerase (− 1.7, at 3 months) as a possible marker for ethanol-induced early steatohepatitis. The observed differential regulation of proteins have potential to serve as biomarker signature for the detection of steatosis and its progression to steatohepatitis once validated in plasma/serum.

Published

2013

24. The MET Receptor Tyrosine Kinase Confers Repair of Murine Pancreatic Acinar Cells following Acute and Chronic Injury

Author

Cornelis J. Elferink, Zobeida Cruz-Monserrate, Bhupendra S. Kaphalia, Karen Pereira de Castro, Lisa A. Elferink, Lynn Soong, Aditya D. Joshi, Dwayne Carter, Paul J. Boor, Daniel Jackson, Craig D. Logsdon, Xinrong Tao, Ivana Gaziova, and Suimin Qiu

Subjects

0301 basic medicine, Pathology, Acinar Cells, Pathology and Laboratory Medicine, Biochemistry, White Blood Cells, Animal Cells, Medicine and Health Sciences, Edema, Immune Response, Ceruletide, Multidisciplinary, Alcohol Consumption, Cell Death, Animal Models, Proto-Oncogene Proteins c-met, medicine.anatomical_structure, Cell Processes, Acute Disease, Medicine, Collagen, medicine.symptom, Pancreatic injury, Cellular Types, Anatomy, Pancreas, Research Article, medicine.medical_specialty, Alcohol Drinking, Science, Immune Cells, Immunology, Inflammation, Mouse Models, Endocrine System, Biology, Research and Analysis Methods, 03 medical and health sciences, Model Organisms, Signs and Symptoms, Exocrine Glands, Diagnostic Medicine, Pancreatitis, Chronic, medicine, Acinar cell, Animals, Humans, Regeneration, Nutrition, Wound Healing, Blood Cells, Macrophages, Biology and Life Sciences, Proteins, Cell Biology, medicine.disease, Diet, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Hepatocyte Growth Factor Receptor, Chronic Disease, Pancreatitis, Wound healing, Collagens, Gene Deletion

Abstract

Acinar cells represent the primary target in necroinflammatory diseases of the pancreas, including pancreatitis. The signaling pathways guiding acinar cell repair and regeneration following injury remain poorly understood. The purpose of this study was to determine the importance of Hepatocyte Growth Factor Receptor/MET signaling as an intrinsic repair mechanism for acinar cells following acute damage and chronic alcohol-associated injury. Here, we generated mice with targeted deletion of MET in adult acinar cells (MET-/-). Acute and repetitive pancreatic injury was induced in MET-/- and control mice with cerulein, and chronic injury by feeding mice Lieber-DeCarli diets containing alcohol with or without enhancement of repetitive pancreatic injury. We examined the exocrine pancreas of these mice histologically for acinar death, edema, inflammation and collagen deposition and changes in the transcriptional program. We show that MET expression is relatively low in normal adult pancreas. However, MET levels were elevated in ductal and acinar cells in human pancreatitis specimens, consistent with a role for MET in an adaptive repair mechanism. We report that genetic deletion of MET in adult murine acinar cells was linked to increased acinar cell death, chronic inflammation and delayed recovery (regeneration) of pancreatic exocrine tissue. Notably, increased pancreatic collagen deposition was detected in MET knockout mice following repetitive injury as well alcohol-associated injury. Finally, we identified specific alterations of the pancreatic transcriptome associated with MET signaling during injury, involved in tissue repair, inflammation and endoplasmic reticulum stress. Together, these data demonstrate the importance of MET signaling for acinar repair and regeneration, a novel finding that could attenuate the symptomology of pancreatic injury.

Published

2016

25. Alcoholic Steatosis in Different Strains of Rat: A Comparative Study

Author

G. A. Shakeel Ansari, Harshica Fernando, Shakuntala Kondraganti, Bhupendra S. Kaphalia, Paul J. Boor, and Kamlesh K. Bhopale

Subjects

medicine.medical_specialty, Alcoholic liver disease, Liquid diet, Biology, Article, lipids, chemistry.chemical_compound, Internal medicine, transcription factors, Gene expression, medicine, steatosis, genes, Pathological, fatty liver, chemistry.chemical_classification, Ethanol, alcohol, Fatty liver, rat strains, Fatty acid, medicine.disease, Psychiatry and Mental health, Clinical Psychology, Endocrinology, chemistry, ethanol, Steatosis, alcoholic liver disease

Abstract

Background. Different strains of rats have been used to study alcoholic liver disease (ALD) while the reason for selecting a particular rat strain was not apparent. Purpose. The aim of our study was to compare outbred (Wistar) and inbred (Fischer) strains to evaluate pathological, biochemical changes, and gene expression differences associated with ethanol-induced early hepatic steatosis. Study Design. Male Wistar and Fischer-344 rats were pair-fed for 6 weeks with or without 5% ethanol in Lieber-DeCarli liquid diet. Livers were analyzed for histological and lipid-related differences. Results. Hepatic midzonal steatosis was mainly found in Wistar rats while Fischer rats showed mostly pericentral steatosis. Increased hepatic steatosis in ethanol-fed Wistar rats is supported by increases in lipids with related genes and transcription factors involved in fatty acid and triglyceride synthesis. Conclusion. Our data showed that Fischer rats are relatively less prone to ethanol-mediated steatosis with pericentral lipid deposition pattern in the liver which is similar to humans and show no trace level of lipid accumulation in pair-fed controls as observed in Wistar (outbred) strain. Therefore, Fischer rats are better suited for lipid studies in an early development of ALD.

Published

2016

26. Lipidomic changes in rat liver after long-term exposure to ethanol

Author

Bhupendra S. Kaphalia, Kamlesh K. Bhopale, Harshica Fernando, Shakuntala Kondraganti, and G. A. Shakeel Ansari

Subjects

Male, medicine.medical_specialty, Alcoholic liver disease, Magnetic Resonance Spectroscopy, Toxicology, medicine.disease_cause, Article, chemistry.chemical_compound, Internal medicine, Phosphatidylcholine, Lipidomics, medicine, Animals, Metabolomics, Aspartate Aminotransferases, Liver Diseases, Alcoholic, Pharmacology, Principal Component Analysis, Ethanol, biology, Body Weight, Fatty liver, Alanine Transaminase, Lipid metabolism, Organ Size, Lipid Metabolism, medicine.disease, Immunohistochemistry, Rats, Inbred F344, Rats, Oxidative Stress, Endocrinology, Liver, chemistry, Biochemistry, Alanine transaminase, biology.protein, Oxidative stress

Abstract

Alcoholic liver disease (ALD) is a serious health problem with significant morbidity and mortality. In this study we examined the progression of ALD along with lipidomic changes in rats fed ethanol for 2 and 3 months to understand the mechanism, and identify possible biomarkers. Male Fischer 344 rats were fed 5% ethanol or caloric equivalent of maltose–dextrin in a Lieber-DeCarli diet. Animals were killed at the end of 2 and 3 months and plasma and livers were collected. Portions of the liver were fixed for histological and immunohistological studies. Plasma and the liver lipids were extracted and analyzed by nuclear magnetic resonance (NMR) spectroscopy. A time dependent fatty infiltration was observed in the livers of ethanol-fed rats. Mild inflammation and oxidative stress were observed in some ethanol-fed rats at 3 months. The multivariate and principal component analysis of proton and phosphorus NMR spectroscopy data of extracted lipids from the plasma and livers showed segregation of ethanol-fed groups from the pair-fed controls. Significant hepatic lipids that were increased by ethanol exposure included fatty acids and triglycerides, whereas phosphatidylcholine (PC) decreased. However, both free fatty acids and PC decreased in the plasma. In liver lipids unsaturation of fatty acyl chains increased, contrary to plasma, where it decreased. Our studies confirm that over-accumulation of lipids in ethanol-induced liver steatosis accompanied by mild inflammation on long duration of ethanol exposure. Identified metabolic profile using NMR lipidomics could be further explored to establish biomarker signatures representing the etiopathogenesis, progression and/or severity of ALD.

Published

2011

27. Differentially Altered Plasma Proteins in Patients diagnosed with Alcoholic and Nonalcoholic Fatty Liver Disease

Author

G.A.S. Ansari, Kizhake V. Soman, Anthony O. Okorodudu, Dhananjaya Nauduri, Bhupendra S. Kaphalia, Gagan K Sood, and Kamlesh K. Bhopale

Subjects

medicine.medical_specialty, Endocrinology, business.industry, Internal medicine, Fatty liver, medicine, Disease, medicine.disease, business, Blood proteins

Published

2011

28. 1H and 31P NMR Lipidome of Ethanol-Induced Fatty Liver

Author

Muniasamy Neerathilingam, Bhupendra S. Kaphalia, Bruce A. Luxon, Paul J. Boor, Harshica Fernando, Kamlesh K. Bhopale, G. A. Shakeel Ansari, Shakuntala Kondraganti, and David E. Volk

Subjects

Alcoholic liver disease, medicine.medical_specialty, Cirrhosis, Triglyceride, Chemistry, Fatty liver, Medicine (miscellaneous), Lipid metabolism, Toxicology, medicine.disease, Psychiatry and Mental health, chemistry.chemical_compound, Endocrinology, Biochemistry, Internal medicine, Lipidomics, medicine, Steatosis, Steatohepatitis

Abstract

Background: Hepatic steatosis (fatty liver), an early and reversible stage of alcoholic liver disease, is characterized by triglyceride deposition in hepatocytes, which can advance to steatohepatitis, fibrosis, cirrhosis, and ultimately to hepatocellular carcinoma. In the present work, we studied altered plasma and hepatic lipid metabolome (lipidome) to understand the mechanisms and lipid pattern of early-stage alcohol-induced-fatty liver. Methods: Male Fischer 344 rats were fed 5% alcohol in a Lieber-DeCarli diet. Control rats were pair-fed an equivalent amount of maltose-dextrin. After 1 month, animals were killed and plasma collected. Livers were excised for morphological, immunohistochemical, and biochemical studies. The lipids from plasma and livers were extracted with methyl-tert-butyl ether and analyzed by 750/800 MHz proton nuclear magnetic resonance (1H NMR) and phosphorus (31P) NMR spectroscopy on a 600 MHz spectrometer. The NMR data were then subjected to multivariate statistical analysis. Results: Hematoxylin and Eosin and Oil Red O stained liver sections showed significant fatty infiltration. Immunohistochemical analysis of liver sections from ethanol-fed rats showed no inflammation (absence of CD3 positive cells) or oxidative stress (absence of malondialdehyde reactivity or 4-hydroxynonenal positive staining). Cluster analysis and principal component analysis of 1H NMR data of lipid extracts of both plasma and livers showed a significant difference in the lipid metabolome of ethanol-fed versus control rats. 31P NMR data of liver lipid extracts showed significant changes in phospholipids similar to 1H NMR data. 1H NMR data of plasma and liver reflected several changes, while comparison of 1H NMR and 31P NMR data offered a correlation among the phospholipids. Conclusions: Our results show that alcohol consumption alters metabolism of cholesterol, triglycerides, and phospholipids that could contribute to the development of fatty liver. These studies also indicate that fatty liver precedes oxidative stress and inflammation. The similarities observed in plasma and liver lipid profiles offer a potential methodology for detecting early-stage alcohol-induced fatty liver disease by analyzing the plasma lipid profile.

Published

2010

29. Pancreatic injury in hepatic alcohol dehydrogenase-deficient deer mice after subchronic exposure to ethanol

Author

Paul J. Boor, Kamlesh K. Bhopale, G. A. Shakeel Ansari, Hai Wu, Bhupendra S. Kaphalia, and Shakuntala Kondraganti

Subjects

Male, medicine.medical_specialty, Pancreatic disease, Pancreatitis, Alcoholic, Trypsinogen, Acetaldehyde, Endoplasmic Reticulum, Toxicology, Article, Cathepsin B, Mice, chemistry.chemical_compound, Internal medicine, medicine, Animals, HSP70 Heat-Shock Proteins, Trypsinogen activation, Pancreas, Alcohol dehydrogenase, Pharmacology, Ethanol, biology, Fatty Acids, Alcohol Dehydrogenase, Membrane Proteins, Lipase, medicine.disease, Disease Models, Animal, Ethyl Ethers, medicine.anatomical_structure, Endocrinology, Liver, chemistry, biology.protein, Pancreatitis, Pancreatic injury, Oligopeptides

Abstract

Pancreatitis caused by activation of digestive zymogens in the exocrine pancreas is a serious chronic health problem in alcoholic patients. However, mechanism of alcoholic pancreatitis remains obscure due to lack of a suitable animal model. Earlier, we reported pancreatic injury and substantial increases in endogenous formation of fatty acid ethyl esters (FAEEs) in the pancreas of hepatic alcohol dehydrogenase (ADH)-deficient (ADH(-)) deer mice fed 4% ethanol. To understand the mechanism of alcoholic pancreatitis, we evaluated dose-dependent metabolism of ethanol and related pancreatic injury in ADH(-) and hepatic ADH-normal (ADH(+)) deer mice fed 1%, 2% or 3.5% ethanol via Lieber-DeCarli liquid diet daily for 2months. Blood alcohol concentration (BAC) was remarkably increased and the concentration was ∼1.5-fold greater in ADH(-) vs. ADH(+) deer mice fed 3.5% ethanol. At the end of the experiment, remarkable increases in pancreatic FAEEs and significant pancreatic injury indicated by the presence of prominent perinuclear space, pyknotic nuclei, apoptotic bodies and dilation of glandular ER were found only in ADH(-) deer mice fed 3.5% ethanol. This pancreatic injury was further supported by increased plasma lipase and pancreatic cathepsin B (a lysosomal hydrolase capable of activating trypsinogen), trypsinogen activation peptide (by-product of trypsinogen activation process) and glucose-regulated protein 78 (endoplasmic reticulum stress marker). These findings suggest that ADH-deficiency and high alcohol levels in the body are the key factors in ethanol-induced pancreatic injury. Therefore, determining how this early stage of pancreatic injury advances to inflammation stage could be important for understanding the mechanism(s) of alcoholic pancreatitis.

Published

2010

30. Ethanol-induced cytotoxicity in rat pancreatic acinar AR42J cells: Role of fatty acid ethyl esters

Author

Bhupendra S. Kaphalia, Kamlesh K. Bhopale, Ghulam Ansari, and Hai Wu

Subjects

Metabolite, Apoptosis, chemistry.chemical_compound, Cell Line, Tumor, medicine, Animals, Humans, Ethyl oleate, Cytotoxicity, chemistry.chemical_classification, Ethanol, Dose-Response Relationship, Drug, ATP synthase, biology, Cytotoxins, Fatty Acids, Fatty acid, Esters, General Medicine, Molecular biology, Pancreas, Exocrine, Rats, medicine.anatomical_structure, chemistry, Biochemistry, biology.protein, Pancreas

Abstract

Aims: To understand the mechanism(s) of alcoholic pancreatitis and role of fatty acid ethyl esters (FAEEs, non-oxidative metabolites of ethanol) in ethanol-induced pancreatic injury. Methods: A time- and concentration-dependent synthesis of FAEEs and the cytotoxicity of ethanol and its predominant fatty acid esters were studied in rat pancreatic tumour (AR42J) cells in cultures. Role of FAEEs in ethanol-induced cytotoxicity was investigated by measuring the synthesis of FAEEs, injury markers and apoptosis in cells incubated simultaneously with ethanol and FAEE synthase inhibitor, 3-benzyl-6-chloro-2-pyrone. The cells were pre-incubated with caspase-3 inhibitor (N-acetyl-DEVD-CHO) to measure the effect of caspase-3 inhibition on ethanol-induced apoptosis. Results: The levels of FAEEs synthesized in cell cultures incubated with 800 mg% ethanol for 6 h were ∼10-fold higher (60 nmol/25 × 106 cells) than those in cells incubated with 100 mg% ethanol (5.4 nmol/25 × 106 cells). Ethanol exposure resulted in a concentration-dependent apoptosis (10, 12 and 13% at 200, 400 and 800 mg% ethanol, respectively, vs 5% in controls). A similar concentration-dependent apoptosis was also found in the cells incubated with ethyl oleate (one of the predominant FAEEs reported in alcoholic patients). Inhibition of FAEE synthesis and resultant apoptosis was found in the cells incubated simultaneously with pancreatic FAEE synthase inhibitor and ethanol. Ethanol-induced apoptosis was significantly inhibited in cells pre-incubated with caspase-3 inhibitor. Conclusions: These results support our hypothesis that ethanol-induced cytotoxicity in AR42J cells is mediated by the non-oxidative metabolite(s) of ethanol, and caspase-3 mediated apoptosis could be one of the mechanisms involved in ethanol-induced pancreatic injury.

Published

2007

31. Comparative effects of cocaine and cocaethylene on alveolar epithelial type II cells

Author

Eseosa A, Bazuaye-Ekwuyasi, John O, Ogunbileje, Bhupendra S, Kaphalia, Mahmoud A, Eltorky, and Anthony O, Okorodudu

Subjects

Colony-Forming Units Assay, Oxidative Stress, Cocaine, Dopamine Uptake Inhibitors, Cell Survival, Illicit Drugs, Alveolar Epithelial Cells, Cell Line, Tumor, Cell Cycle, Humans, Reactive Oxygen Species, Cell Proliferation

Abstract

Abuse of cocaine (COC) and alcohol have been among the leading causes of non-prescription drug-related deaths in the USA and are known to cause acute and chronic lung diseases. The co-abuse of COC and alcohol results in the production of an active metabolite, cocaethylene (CE). The effects of COC and its metabolites on the respiratory system have been scarcely studied. This study was aimed at comparing the toxic effects of eqimolar concentration (1 mM) of COC and CE on alveolar epithelial type II cells. This was performed by measuring cell growth, viability, clonogenic activity, cell cycle and reactive oxygen species (ROS) generation. The treatment of CE and COC resulted in a significant inhibition of cell proliferation with the formation of an average of three colonies which measured about 1.74×10(-15) m each and 25 colonies each of about 5.73×10(-15) m, respectively, while untreated cells yielded 31 colonies of 8.75×10(-15) m (p0.05). The treatments of CE and COC resulted in the reduction of the growth fraction of alveolar epithelial type II cells without significant decrease in viability. In addition, there was an approximately twofold increase in ROS generation as compared to the controls (p0.05). Therefore, CE-induced inhibition of cellular proliferation may contribute to the pathogenesis of diffuse alveolar damage in co-abusers of COC and alcohol.

Published

2015

32. Effects of acute ethanol exposure on cytokine production by primary airway smooth muscle cells

Author

Bhupendra S. Kaphalia, William J. Calhoun, Mridul Kalita, and Lata Kaphalia

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, medicine.medical_treatment, Myocytes, Smooth Muscle, Toxicology, medicine.disease_cause, Proinflammatory cytokine, 03 medical and health sciences, chemistry.chemical_compound, Internal medicine, mental disorders, medicine, Humans, Lung, reproductive and urinary physiology, Pharmacology, biology, Dose-Response Relationship, Drug, Ethanol, Chemistry, Sirtuin 1, NF-κB, CYP2E1, Oxidative Stress, 030104 developmental biology, Cytokine, Endocrinology, biology.protein, Unfolded protein response, Cytokines, Tumor necrosis factor alpha, Oxidative stress

Abstract

Both chronic and binge alcohol abuse can be significant risk factors for inflammatory lung diseases such as acute respiratory distress syndrome and chronic obstructive pulmonary disease. However, metabolic basis of alcohol-related lung disease is not well defined, and may include key metabolites of ethanol [EtOH] in addition to EtOH itself. Therefore, we investigated the effects of EtOH, acetaldehyde [ACE], and fatty acid ethyl esters [FAEEs] on oxidative stress, endoplasmic reticulum (ER) stress, AMP-activated protein kinase (AMPK) signaling and nuclear translocation of phosphorylated (p)-NF-κB p65 in primary human airway smooth muscle (HASM) cells stimulated to produce cytokines using LPS exposure. Both FAEEs and ACE induced evidence of cellular oxidative stress and ER stress, and increased p-NF-κB in nuclear extracts. EtOH and its metabolites decreased p-AMPKα activation, and induced expression of fatty acid synthase, and decreased expression of sirtuin 1. In general, EtOH decreased secretion of IP-10, IL-6, eotaxin, GCSF, and MCP-1. However, FAEEs and ACE increased these cytokines, suggesting that both FAEEs and ACE as compared to EtOH itself are proinflammatory. A direct effect of EtOH could be consistent with blunted immune response. Collectively, these two features of EtOH exposure, coupled with the known inhibition of innate immune response in our model might explain some clinical manifestations of EtOH exposure in the lung.

Published

2015

33. Autoimmune response in MRL+/+ mice following treatment with dichloroacetyl chloride or dichloroacetic anhydride

Author

Rolf König, M. Firoze Khan, Suimin Qiu, Bhupendra S. Kaphalia, Ping Cai, and Ghulam Ansari

Subjects

Mice, Inbred MRL lpr, medicine.medical_specialty, CD3 Complex, medicine.medical_treatment, T cell, CD3, Acetic Anhydrides, Immunoglobulins, Autoimmunity, Spleen, Acetates, Toxicology, medicine.disease_cause, Mice, CD28 Antigens, Internal medicine, medicine, Splenocyte, Animals, Lymphocytes, Antibodies, Blocking, Cells, Cultured, Pharmacology, Dichloroacetic Acid, biology, Chemistry, Homozygote, Pulmonary Alveoli, Cytokine, medicine.anatomical_structure, Endocrinology, Antibodies, Antinuclear, Toxicity, biology.protein, Cytokines, Female, Cytokine secretion

Abstract

Dichloroacetyl chloride (DCAC) is formed from trichloroethene (TCE), which is implicated in inducing/accelerating autoimmune response. Due to its potent acylating activity, DCAC may convert proteins to neo-antigens and thus could induce autoimmune responses. Dichloroacetic anhydride (DCAA), which is a similar acylating agent, might also induce autoimmune responses. To evaluate if chloroacylation plays a role in the induction of autoimmunity, we have measured the autoimmune responses following treatment with DCAC or DCAA in autoimmune-prone MRL+/+ mice. Five-week-old female mice were injected intraperitoneally (twice weekly) with 0.2 mmol/kg of DCAC or DCAA in corn oil for 6 weeks. Total serum IgG, IgG1, and IgE levels were significantly increased in DCAC-treated mice as compared to controls. These increases corresponded with increases in DCAC-specific IgG and IgG1 levels. Total serum IgM was decreased in both DCAC- and DCAA-treated mice. Antinuclear antibodies, measured as an indication of systemic autoimmune responses, were increased in both DCAC- and DCAA-treated mice. Of eight Th1/Th2 cytokines measured in the serum, only IL-5 was significantly decreased in both treatment groups. The cytokine secretion patterns of splenic lymphocytes after stimulation with antibodies against CD3 (T cell receptor-mediated signal) and CD28 (costimulatory signal) differed between treatment and control groups. Levels of IL-1, IL-3, IL-6, IFN-gamma, G-CSF, and KC were higher in cultures of stimulated splenocytes from either DCAC- or DCAA-treated mice than from controls. The level of IL-17 was only increased in cultures from DCAC-treated mice. Increased lymphocytic populations were found in the red pulp of spleens following treatment with either DCAC or DCAA. In addition, thickening of the alveolar septa in the lungs of DCAC- or DCAA-treated mice was observed. The lung histopathology in exposed mice was consistent with the symptomology observed in welders exposed to DCAC/phosgene. Thickening was more pronounced in DCAC-treated mice. Our data suggest that DCAC and DCAA elicit autoimmune responses in MRL+/+ mice that might be reflective of their chloroacylation potential in vivo.

Published

2006

34. Metabolic basis of ethanol-induced cytotoxicity in recombinant HepG2 cells: Role of nonoxidative metabolism

Author

Hai Wu, Thomas R. Jerrells, Bhupendra S. Kaphalia, Ping Cai, G. A. Shakeel Ansari, and Dahn L. Clemens

Subjects

Carcinoma, Hepatocellular, Apoptosis, Transfection, Toxicology, Mice, chemistry.chemical_compound, Adenosine Triphosphate, Cell Line, Tumor, Animals, Humans, Ethanol metabolism, Alcohol dehydrogenase, Pharmacology, Ethanol, Dose-Response Relationship, Drug, biology, Fatty Acids, Alcohol Dehydrogenase, Central Nervous System Depressants, Cytochrome P450, Cytochrome P-450 CYP2E1, Esters, Metabolism, CYP2E1, Biochemistry, chemistry, Cell culture, Caspases, Hepatocytes, biology.protein, Microsome, Oxidation-Reduction, Acyltransferases

Abstract

Chronic alcohol abuse, a major health problem, causes liver and pancreatic diseases and is known to impair hepatic alcohol dehydrogenase (ADH). Hepatic ADH-catalyzed oxidation of ethanol is a major pathway for the ethanol disposition in the body. Hepatic microsomal cytochrome P450 (CYP2E1), induced in chronic alcohol abuse, is also reported to oxidize ethanol. However, impaired hepatic ADH activity in a rat model is known to facilitate a nonoxidative metabolism resulting in formation of nonoxidative metabolites of ethanol such as fatty acid ethyl esters (FAEEs) via a nonoxidative pathway catalyzed by FAEE synthase. Therefore, the metabolic basis of ethanol-induced cytotoxicity was determined in HepG2 cells and recombinant HepG2 cells transfected with ADH (VA-13), CYP2E1 (E47) or ADH + CYP2E1 (VL-17A). Western blot analysis shows ADH deficiency in HepG2 and E47 cells, compared to ADH-overexpressed VA-13 and VL-17A cells. Attached HepG2 cells and the recombinant cells were incubated with ethanol, and nonoxidative metabolism of ethanol was determined by measuring the formation of FAEEs. Significantly higher levels of FAEEs were synthesized in HepG2 and E47 cells than in VA-13 and VL-17A cells at all concentrations of ethanol (100-800 mg%) incubated for 6 h (optimal time for the synthesis of FAEEs) in cell culture. These results suggest that ADH-catalyzed oxidative metabolism of ethanol is the major mechanism of its disposition, regardless of CYP2E1 overexpression. On the other hand, diminished ADH activity facilitates nonoxidative metabolism of ethanol to FAEEs as found in E47 cells, regardless of CYP2E1 overexpression. Therefore, CYP2E1-mediated oxidation of ethanol could be a minor mechanism of ethanol disposition. Further studies conducted only in HepG2 and VA-13 cells showed lower ethanol disposition and ATP concentration and higher accumulation of neutral lipids and cytotoxicity (apoptosis) in HepG2 cells than in VA-13 cells. The apoptosis observed in HepG2 vs. VA-13 cells incubated with ethanol appears to be mediated by release of mitochondrial cytochrome c via activation of caspase-9 and caspase-3. These results strongly support our hypothesis that diminished hepatic ADH activity facilitates nonoxidative metabolism of ethanol and the products of ethanol nonoxidative metabolism cause apoptosis in HepG2 cells via intrinsic pathway.

Published

2006

35. Efficient high performance liquid chromatograph/ultraviolet method for determination of diclofenac and 4′-hydroxydiclofenac in rat serum

Author

Mary Treinen-Moslen, Mary F. Kanz, Lata Kaphalia, Bhupendra S. Kaphalia, and Santosh Kumar

Subjects

Male, Diclofenac, Metabolite, Clinical Biochemistry, Biochemistry, Analytical Chemistry, Rats, Sprague-Dawley, chemistry.chemical_compound, Pharmacokinetics, Spectrophotometry, medicine, Animals, Antipyretic, Chromatography, High Pressure Liquid, Detection limit, Chromatography, medicine.diagnostic_test, Extraction (chemistry), Reproducibility of Results, Cell Biology, General Medicine, Rats, stomatognathic diseases, chemistry, Spectrophotometry, Ultraviolet, Quantitative analysis (chemistry), medicine.drug

Abstract

A rapid and sensitive high-performance liquid chromatographic method was developed for determination of diclofenac and its major metabolite, 4'-hydroxydiclofenac, in serum from rats treated with diclofenac. The method is simple with a one-step extraction procedure, isocratic HPLC separation, and UV detection at 280 nm. Use of N-phenylanthranilic acid as the internal standard provided good accuracy without interference by endogenous compounds or 5-hydroxydiclofenac, another metabolite of interest. Limits of detection for diclofenac and 4'-hydroxydiclofenac were 0.0225 and 0.0112 microg/ml, respectively. Average extraction efficiencies of diclofenac, 4'-hydroxydiclofenac, and the internal standard were >/=76%. The method was applied to serum collected at 3h after rats were treated with an experimentally useful dosage range of 3, 10 and 50mg/kg diclofenac. Recovery (as a percentage of dose) for the 4'-hydroxy metabolite in serum was found to consistently average from 0.10 to 0.12% following each dosage, whereas recovery of diclofenac in serum declined from 0.45 to 0.37%. Thus, the method is suitable for measurement of a major diclofenac metabolite in experimental studies.

Published

2006

36. RSV-induced prostaglandin E2 production occurs via cPLA2 activation: Role in viral replication

Author

Bhupendra S. Kaphalia, Wahiduz A. Zaman, Antonella Casola, Roberto P. Garofalo, G. A. Shakeel Ansari, and Tianshuang Liu

Subjects

Transcription, Genetic, Prostaglandin, viruses, Blotting, Western, Inflammation, Virus Replication, Airway epithelial cells, Dinoprostone, Phospholipases A, Cell Line, Proinflammatory cytokine, chemistry.chemical_compound, Phospholipase A2, Virology, medicine, Humans, Secretion, RNA, Messenger, Prostaglandin E2, Arachidonic Acid, biology, NF-kappa B, RSV, Epithelial Cells, Lipid signaling, Blotting, Northern, Respiratory Syncytial Viruses, Cell biology, Phospholipases A2, chemistry, Viral replication, Cyclooxygenase 2, Immunology, biology.protein, medicine.symptom, medicine.drug

Abstract

Prostaglandins (PGs) are lipid mediators that participate in the regulation of immunological and inflammatory responses, and PG production can affect viral replication. In this study, we have investigated the mechanism of PGE2 production in airway epithelial cells, following respiratory syncytial virus (RSV) infection, and its role in viral replication. We show that RSV infection strongly induces PGE2 secretion, in a time- and replication-dependent manner, through increased cyclooxygenase-2 (COX-2) expression, which occurs independently from viral or cellular protein synthesis. RSV infection induces arachidonic acid release through induction of cytoplasmic phospholipase A2 (cPLA2) enzymatic activity and its membrane translocation. Specific inhibitors of cPLA2 significantly block RSV-induced PGE2 secretion, indicating a key role of cPLA2 in viral-induced PG production. Blocking PG secretion, through cPLA2 or COX-2 inhibition, results in impairment of RSV replication and subsequent RSV-mediated epithelial cell responses, suggesting that inhibition of PG secretion could be beneficial in RSV infection by reducing proinflammatory mediator production.

Published

2005

37. In Vitro Conjugation of Ethanolamine with Fatty Acids by Rat Liver Subcellular Fractions

Author

Bhupendra S. Kaphalia, Ghulam Ansari, and Shagufta H. Khan

Subjects

chemistry.chemical_classification, Analysis of Variance, Magnetic Resonance Spectroscopy, Fatty acid amide, Chromatography, Chemistry, Health, Toxicology and Mutagenesis, Fatty Acids, Substrate (chemistry), Fatty acid, Toxicology, Rats, chemistry.chemical_compound, Oleic acid, Enzyme, Ethanolamine, Biochemistry, Ethanolamines, Microsomes, Liver, Microsome, Animals, Ethanolamide, lipids (amino acids, peptides, and proteins), Oleic Acid

Abstract

Previous studies from our laboratory have shown the enzymic formation of fatty acid (FA) conjugates of xenobiotic alcohols and amines. In the present study, the formation of FA conjugates of a bifunctional compound, ethanolamine was investigated by incubating [1-14C]oleic acid (1 mM) with ethanolamine (25 mM) at 37 degrees C in the presence of various rat liver subcellular fractions. The resultant product (or products) was separated by thin-layer chromatography (TLC) and the radioactivity corresponding to the relative flow of fatty acid amide was determined. Under similar conditions, formation of ethanolamides of palmitic, stearic, linoleic, linolenic, and arachidonic acids were also examined. The formation of ethanolamine conjugate with oleic acid was found to be 16.3 nmol/h/mg protein as compared to 6.7, 6.2, 8.1, 8.3, and 7.6 nmol/h/mg protein for palmitic, stearic, linoleic, linolenic, and arachidonic acids, respectively. The formation of oleoyl ethanolamide was found to be 18.9, 40.1, 65.9, and 0.3 nmol/h/mg protein in postnuclear, mitochondrial, microsomal, and cytosolic fractions, respectively. Mass spectrometric and nuclear magnetic resonance spectroscopic data of the TLC-purified product confirm the formation of oleoyl ethanolamide, and amidation appeared to be a preferred reaction over esterification. The results of this study suggest that the enzyme responsible for the amidation of fatty acids resides mainly in the microsomal fraction of the liver, and that oleic acid is a better substrate than other fatty acids used in the present study.

Published

2005

38. Fatty acid ethyl esters: markers of alcohol abuse and alcoholism

Author

M. Firoze Khan, Bhupendra S. Kaphalia, Ping Cai, Ghulam Ansari, and Anthony O. Okorodudu

Subjects

Adult, Male, Time Factors, Health (social science), Alcohol abuse, Physiology, Alcohol, Toxicology, Biochemistry, Behavioral Neuroscience, chemistry.chemical_compound, Humans, Medicine, Ethyl oleate, Aged, chemistry.chemical_classification, Ethanol, business.industry, Fatty Acids, Age Factors, Fatty acid, Esters, General Medicine, Metabolism, Middle Aged, medicine.disease, Alcoholism, Neurology, chemistry, Ethyl palmitate, Biomarker (medicine), Female, business, Biomarkers

Abstract

Chronic alcoholism, which is associated with hepatic, pancreatic, and myocardial diseases, is one of the major health problems in the United States with high morbidity and mortality. Many individuals who abuse alcohol chronically die even before reaching the clinical stage of the disease. Reliable biomarkers of the diseases induced by chronic alcohol abuse, as well as for alcoholism, currently are not available. In the current study, we measured plasma concentrations of fatty acid ethyl esters [(FAEEs), nonoxidative metabolites of ethanol] in 39 patients with a detectable concentration of alcohol in their blood samples. In turn, we determined the relation of FAEE concentrations with blood alcohol concentration (BAC). Of 39 patients in whom we evaluated this relation, only five had a history of chronic alcohol abuse, and six had a history of acute alcohol abuse. Patients' age ranged from 25 to 71 years. Within this age range, greater concentrations of FAEEs were found in the plasma samples obtained from patients in the 41- to 50-year age group. There were no sex-related differences in BAC, nor in FAEE concentrations. Thirteen patients had a BAC greater than 300 mg%. For 11 patients, the BAC ranged between 200 and 299 mg%, and, for 12 patients, the BAC ranged between 100 and 199 mg%. In comparison with findings for patients with a BAC that ranged between 100 and 299 mg%, the FAEE concentrations were approximately twofold higher in patients with a BAC greater than 300 mg%. Ethyl palmitate and ethyl oleate were the main FAEEs detected in most patients. In general, FAEE concentrations increased with increasing BAC. However, in comparison with patients with a history of acute alcohol abuse, a greater increase in total FAEE concentrations was observed in patients with a history of chronic alcohol abuse (4,250 ng/ml and 15,086 ng/ml, respectively). Fatty acid ethyl esters were either detected in trace amounts or not detectable in the plasma of control subjects with no known alcohol ingestion. These results support our hypothesis that nonoxidative metabolism of ethanol to FAEEs is an important pathway of ethanol disposition during chronic alcohol abuse, and that FAEE concentrations can be a more reliable biomarker of chronic alcohol abuse than a history of acute alcohol abuse.

Published

2004

39. Mechanism of differential inhibition of hepatic and pancreatic fatty acid ethyl ester synthase by inhibitors of serine-esterases: in vitro and cell culture studies

Author

Kelly A. Mericle, Ghulam Ansari, and Bhupendra S. Kaphalia

Subjects

Swine, Microdialysis, Biology, Toxicology, Esterase, Carboxylesterase, Substrate Specificity, Nitrophenols, Serine, Organophosphorus Compounds, In vivo, Cell Line, Tumor, medicine, Animals, Cholinesterases, Humans, Pancreas, Pharmacology, chemistry.chemical_classification, Esterases, Fatty acid, Metabolism, Enzyme, medicine.anatomical_structure, Liver, chemistry, Biochemistry, Pyrones, Indicators and Reagents, Acyltransferases

Abstract

Earlier, we have shown that rat hepatic and pancreatic fatty acid ethyl ester (FAEE) synthases are structurally and functionally similar to rat liver carboxylesterase (CE) and pancreatic cholesterol esterase (ChE), respectively. We have also reported that only hepatic FAEE synthase is inhibited by tri-o-tolylphosphate (TOTP) in vivo and in human hepatocellular carcinoma (HepG2) cells. The metabolism of TOTP is a prerequisite for the inhibition of hepatic FAEE synthase as well as esterase activity. To further elucidate the mechanism of such differential inhibition by inhibitors of serine esterases, we synthesized two metabolites of TOTP, 2-(o-cresyl)-4H-1:3:2-benzodioxaphosphoran-2-one (CBDP; cyclic saligenin phosphate) and di-o-tolyl-o-( proportional, variant -hydroxy)tolylphosphate (HO-TOTP), and one ChE inhibitor, 3-benzyl-6-chloro-2-pyrone (3-BCP). The inhibitory effect of CBDP, HO-TOTP, and 3-BCP on FAEE synthase and esterase activity was studied using rat hepatic and pancreatic postnuclear (PN) fractions, commercial porcine hepatic CE and pancreatic ChE, and in HepG2 and rat pancreatic tumor (AR42J) cell lines. Only HO-TOTP and CBDP inhibited FAEE synthase as well as esterase activity of hepatic PN fraction and commercial CE and ChE in a concentration-dependent manner, and the inhibition was found to be irreversible. However, no inhibition was found in pancreatic PN fraction by both TOTP metabolites and 3-BCP. Although 3-BCP inhibited only the esterase activity of commercial ChE in a concentration-dependent manner, the activity was reversible within 30 min of incubation. Studies with HepG2 cells also showed a significant inhibition of FAEE synthase-esterase activity by CBDP and HO-TOTP within 15 min of incubation, while no inhibition was observed in AR42J cells. 3-BCP did not inhibit FAEE synthase-esterase activity either in HepG2 or AR42J cells. Such differential inhibitory effect of the TOTP metabolites on hepatic and pancreatic FAEE synthase-esterase is supported by our earlier in vivo and in vitro studies. Further investigations are needed to understand the biochemical mechanism(s) of inactivation of TOTP metabolites and 3-BCP in the pancreas and AR42J cells towards FAEE synthase-esterase activities.

Published

2004

40. Quantitation of Acrolein–Protein Adducts: Potential Biomarker of Acrolein Exposure

Author

Bhupendra S. Kaphalia, Hui Li, M Khan, Ghulam Ansari, and Jianling Wang

Subjects

Male, Health, Toxicology and Mutagenesis, medicine.medical_treatment, Formaldehyde, Enzyme-Linked Immunosorbent Assay, Toxicology, Aldehyde, Adduct, Rats, Sprague-Dawley, chemistry.chemical_compound, medicine, Animals, Acrolein, chemistry.chemical_classification, Chromatography, biology, Albumin, Hemocyanin, Blood Proteins, Environmental Exposure, Malondialdehyde, Rats, chemistry, Biochemistry, biology.protein, Environmental Pollutants, Antibody, Biomarkers, Environmental Monitoring, Protein Binding

Abstract

Acrolein, an alpha,beta-unsaturated aldehyde, is a ubiquitous environmental toxic pollutant. Because of potential human exposure, there is a need for a sensitive, reliable, and specific method to monitor acrolein exposure. Acrolein is a potent electrophile and reacts with proteins mainly through Michael addition reaction, leading to acrolein-protein adducts (APA). The present study aimed to develop a competitive enzyme-linked immunosorbent assay (ELISA) method for the quantitation of APA in biological samples. Antibody to acrolein-keyhole limpet hemocyanin adduct was raised in rabbits, and the specificity of the antibody was determined by ELISA using acrolein-albumin adduct (AAA) or native albumin. A dose-dependent response was observed with AAA, but no immunoreactivity with native albumin. Further, lack of cross-reactivity of anti-acrolein antibody with formaldehyde-, malondialdehyde-, or 4-hydroxynonenal-albumin adducts indicates its specificity for acrolein. For the competitive ELISA, 1:16,000 diluted antisera was used with varying concentrations of AAA, which provided a linear detection range between 250 and 10,000 pg. To test the efficacy of the method for possible use as a biomarker of acrolein exposure, SD rats were orally administered 1 or 7 doses of 9.2 mg/kg/d acrolein. APA levels, quantitated in the serum, showed significantly greater formation (32% and 58% after 1 and 7 doses, respectively) in acrolein-treated rats as compared to the controls. Western blot analyses of APA in the sera from acrolein-treated rats showed APA bands (especially 29, 31, and 100 kD) with greater intensity in comparison to controls, further supporting our ELISA results. These results suggest that quantitation of APA has potential to be used as biomarker of acrolein exposure and eventually for molecular dosimetry and risk assessment.

Published

2004

41. Nitrotyrosine formation in splenic toxicity of aniline

Author

Paul J. Boor, Xiaohong Wu, Bhupendra S. Kaphalia, M. Firoze Khan, and Ghulam Ansari

Subjects

Male, White pulp, Blotting, Western, Administration, Oral, Nitric Oxide Synthase Type II, Toxicology, Nitric oxide, Rats, Sprague-Dawley, chemistry.chemical_compound, medicine, Animals, Cellular localization, Aniline Compounds, biology, Nitrotyrosine, Immunohistochemistry, Molecular biology, Rats, Nitric oxide synthase, medicine.anatomical_structure, Biochemistry, chemistry, Enzyme Induction, Toxicity, biology.protein, Red pulp, Tyrosine, Nitric Oxide Synthase, Spleen, Peroxynitrite

Abstract

Splenic toxicity of aniline is characterized by vascular congestion, hyperplasia, fibrosis and development of a variety of sarcomas in rats. However, the mechanisms of this selective splenic toxicity are not well understood. Previously we showed that aniline exposure causes oxidative damage to spleen. To further explore the oxidative mechanisms of aniline toxicity, we evaluated the contributions of nitric oxide. Nitric oxide reacts with superoxide anion to form peroxynitrite, a powerful oxidant that converts the tyrosine residues of proteins to nitrotyrosine (NT). Therefore, aim of this study was to establish the role of nitric oxide through the formation and localization of NT in the spleen of rats exposed to aniline. Male Sprague–Dawley (SD) rats were given 1 mmol/kg per day aniline hydrochloride in water by gavage for 7 days, while the controls received water only. Immunohistochemical analysis for NT showed an intense staining in the red pulp areas of spleen from aniline-treated rats, localized in macrophages and sinusoidal cells. Occasionally mild NT immunostaining was also evident in the white pulp. Western blot analyses of the post-nuclear fraction of the spleens showed major nitrated proteins with molecular weights of 49, 30 and 18 kDa. Immunohistochemical analysis of inducible nitric oxide synthase (iNOS) also showed increased expression in the red pulp of the spleens from aniline-treated rats; the cellular localization was similar to nitrated proteins. These studies suggest that oxidative stress in aniline toxicity also includes aberration in nitric oxide production leading to nitration of proteins. Functional consequences of such nitration will further elucidate the contribution of nitric oxide to the splenic toxicity of aniline.

Published

2003

42. Regional- and sex-dependent effects of chronic ethanol and cocaine co-administration on adult neural stem cell survival and differentiation

Author

Junling Gao, Bhupendra S. Kaphalia, Kelly T. Dineley, Kathryn A. Cunningham, Ping Wu, Tiffany J. Dunn, Javier Allende-labastida, Erica L. McGrath, and Auston Cody Grant

Subjects

Pharmacology, Psychiatry and Mental health, chemistry.chemical_compound, Ethanol, chemistry, Pharmacology (medical), Biology, Toxicology, Neural stem cell, Co administration

Published

2017

43. Fatty acid ethyl ester synthase inhibition ameliorates ethanol-induced Ca2+-dependent mitochondrial dysfunction and acute pancreatitis

Author

Alexei V. Tepikin, Michael Chvanov, Jane A Armstrong, Yan Li, Matthew C Cane, Robert Sutton, Bhupendra S. Kaphalia, Nicole Cash, Muhammad A. Javed, David Booth, Ole H. Petersen, Mohammed Jaffar, William Greenhalf, Hayley Dingsdale, Wei Huang, David N. Criddle, Rajarshi Mukherjee, and Victoria Elliott

Subjects

medicine.medical_specialty, Pancreatitis, Alcoholic, Apoptosis, Acinar Cells, Oxidative phosphorylation, Mitochondrion, Biology, Carboxylesterase, Fatty Acids, Monounsaturated, Mice, Necrosis, chemistry.chemical_compound, In vivo, Internal medicine, medicine, Animals, Palmitoleic acid, Calcium Signaling, Ethanol metabolism, Pancreas, Cells, Cultured, Fomepizole, Membrane Potential, Mitochondrial, chemistry.chemical_classification, Ethanol, Fatty Acids, Gastroenterology, Fatty acid, Alcohol-Induced Injury, Mitochondria, ACUTE Pancreatitis, Disease Models, Animal, Endocrinology, chemistry, Pyrones, Pancreatic Damage, Pyrazoles, Calcium, NAD+ kinase, Acyltransferases, NADP

Abstract

Objective: Non-oxidative metabolism of ethanol (NOME) produces fatty acid ethyl esters (FAEEs) via carboxylester lipase (CEL) and other enzyme action implicated in mitochondrial injury and acute pancreatitis (AP). This study investigated the relative importance of oxidative and non-oxidative pathways in mitochondrial dysfunction, pancreatic damage and development of alcoholic AP, and whether deleterious effects of NOME are preventable. \ud \ud Design: Intracellular calcium ([Ca2+]C), NAD(P)H, mitochondrial membrane potential and activation of apoptotic and necrotic cell death pathways were examined in isolated pancreatic acinar cells in response to ethanol and/or palmitoleic acid (POA) in the presence or absence of 4-methylpyrazole (4-MP) to inhibit oxidative metabolism. A novel in vivo model of alcoholic AP induced by intraperitoneal administration of ethanol and POA was developed to assess the effects of manipulating alcohol metabolism. \ud \ud Results: Inhibition of OME with 4-MP converted predominantly transient [Ca2+]C rises induced by low ethanol/POA combination to sustained elevations, with concurrent mitochondrial depolarisation, fall of NAD(P)H and cellular necrosis in vitro. All effects were prevented by 3-benzyl-6-chloro-2-pyrone (3-BCP), a CEL inhibitor. 3-BCP also significantly inhibited rises of pancreatic FAEE in vivo and ameliorated acute pancreatic damage and inflammation induced by administration of ethanol and POA to mice. \ud \ud Conclusions: A combination of low ethanol and fatty acid that did not exert deleterious effects per se became toxic when oxidative metabolism was inhibited. The in vitro and in vivo damage was markedly inhibited by blockade of CEL, indicating the potential for development of specific therapy for treatment of alcoholic AP via inhibition of FAEE generation.

Published

2014

44. Purification and characterization of rat hepatic microsomal low molecular weight fatty acid ethyl ester synthase and its relationship to carboxylesterases

Author

Bhupendra S. Kaphalia and Ghulam Ansari

Subjects

Health, Toxicology and Mutagenesis, Size-exclusion chromatography, Toxicology, Biochemistry, Isozyme, Carboxylesterase, Animals, Molecular Biology, Chromatography, High Pressure Liquid, Ammonium sulfate precipitation, chemistry.chemical_classification, Chromatography, ATP synthase, biology, Isoelectric focusing, Chemistry, food and beverages, Fatty acid, General Medicine, Chromatography, Ion Exchange, Rats, Molecular Weight, Isoelectric point, Chromatography, Gel, Microsomes, Liver, biology.protein, Molecular Medicine, Electrophoresis, Polyacrylamide Gel, Isoelectric Focusing, Carboxylic Ester Hydrolases, Acyltransferases

Abstract

We reported purification of a high molecular weight (HMW) (ca. 180 kD) and a low molecular weight (LMW) (ca. 60 kD) protein fractions from digitonized rat liver microsomes using ammonium sulfate precipitation followed by ion exchange and gel filtration column chromatography. Both fractions expressed fatty acid ethyl ester (FAEE) synthase as well as p-nitrophenyl acetate (PNPA)–hydrolyzing (esterase) activities. The HMW fraction was found to be a trimer with subunit molecular weight ca. 60 kD and structurally and functionally similar to rat hepatic microsomal carboxylesterase (CE, pI 6.1) and adipose tissue FAEE synthase. In this article, we report further purification and characterization of the LMW (minor) fraction expressing FAEE synthase activity and its structural and functional relationship to hepatic microsomal CEs. Using isoelectric focusing (IEF) followed by gel filtration–high-performance liquid chromatography (GF-HPLC), five proteins were purified, which expressed FAEE synthase as well as PNPA-hydrolyzing activity. The isoelectric point values of 6.5, 5.8, 5.6, 5.3, and 5.0 were found for the purified LMW proteins by IEF and each showed a peak corresponding to ca. 60 kD molecular weight by GF-HPLC, which expressed FAEE synthase as well as PNPA-hydrolyzing activity. Sodium dodecyl sulfate–polyacrylamide gel elecrophoresis (SDS-PAGE) analysis of the GF-HPLC purified LMW proteins revealed that these proteins are monomers (ca. 60 kD). All the purified LMW proteins cross-reacted with antibodies to rat adipose tissue FAEE synthase. Coelution of PNPA-hydrolyzing and FAEE synthase activity at each step of purification and cross-reactivity with rat adipose tissue FAEE synthase antibodies suggest that the purified proteins are related to various hepatic microsomal CEs. This conclusion is further supported by the homology of N-terminal amino acid sequence of the purified LMW proteins to various hepatic microsomal CEs and protease precursors. Therefore, LMW FAEE synthase activity most probably is expressed by various isozymes of hepatic microsomal CEs, which are also involved in the biotransformation of xenobiotic alcohols and amines. © 2001 John Wiley & Sons, Inc. J Biochem Mol Toxicol 15:165–171, 2001

Published

2001

45. Fatty acid anilides: In vivo formation and relevance to toxic oil syndrome

Author

Ghulam Ansari, Bhupendra S. Kaphalia, and M. Firoze Khan

Subjects

chemistry.chemical_classification, Chemistry, Health, Toxicology and Mutagenesis, Fatty acid, General Medicine, Metabolism, Toxicology, medicine.disease, Biochemistry, chemistry.chemical_compound, Toxicity, medicine, Microsome, Molecular Medicine, Ingestion, Food science, Xenobiotic, Molecular Biology, Toxic oil syndrome, Whole blood

Abstract

Toxic oil syndrome (TOS), a multisystemic epidemic outbreak in 1981 in Spain, was caused by the ingestion of a cooking oil mixture containing rapeseed oil denatured with aniline. The mechanisms and causative agents responsible for the TOS are still not known. Although primary lesions observed in TOS patients could not be reproduced experimentally, the levels of fatty acid anilides (FAAs) and aniline in TOS-related cooking oil were considered proximate markers of TOS. Aniline, available from free aniline and FAAs ingested with TOS-related cooking oil, and its reconjugation with endogenous fatty acids could be an early event leading to TOS. Therefore, the present study was undertaken to determine the formation of FAAs following an oral dose of 2 mmol/kg aniline hydrochloride (AH) via gavage in rats. Here, 16:0, 18:0, 18:1, 18:2, 18:3, and 20:4 FAAs were analyzed in the whole blood, brown fat, liver, and pancreas at 0 (control), 0.25, 0.5, 1, 3, 6, 12, 24, and 48 hours. Generally, 16:0 and 18:1 FAAs were detected in the whole blood, brown fat, and liver of AH-treated rats with highest mean levels at 0.25 or 0.5 hour, except 3 hours for the whole blood. Only 16:0 FAA was detectable in the pancreas of AH-treated animals. The 18:0 FAA was also detected frequently in the liver while other FAAs were either in trace amounts or not detectable in the tissues analyzed in the present study. Overall, highest formation of the 16:0 FAA was found in the liver followed by pancreas and of 18:1 FAA in the whole blood and brown fat. These results indicate a rapid formation and further metabolism and disposition of FAAs in rat model and support our previous findings that 18:1 and 16:0 fatty acids are better substrates for the conjugation with aniline. Surprisingly, a small or trace amount of a few FAAs also detected in the tissues of control rats indicates their endogenous biosynthesis and/or presence. Results of 18:1 fatty acid incubation and aniline in the presence of fatty acid ethyl ester synthase, purified to homogeneity from rat liver microsome, suggest that formation of FAAs is catalyzed by an enzyme involved in the conjugation of fatty acids with xenobiotic alcohols. Because the FAAs are known to exert a wide range of toxicity in experimental animals and primary cell cultures, in vivo formation of FAAs could be an early event leading to TOS.

Published

1999

46. List of Contributors

Author

Angela Aliberti, Patrick Allard, Arturo Anadón, Vellareddy Anantharam, Anthony E. Archibong, Adam D. Aulbach, Aryamitra Banerjee, Leah D. Banks, Frank A. Barile, Sudheer R. Beedanagari, Enrico Bergamaschi, Sneha P. Bhatia, Karyn Bischoff, Víctor Castellano, Daniel T. Chang, James J. Chen, Deborah Citrin, Rory Conolly, R.W. Coppock, Lucio G. Costa, T.V. Damodaran, Kellye K. Daniels, Curtis C. Dary, Robin B. Doss, Filipe V. Duarte, Margitta M. Dziwenka, Stephen Edwards, Jorge Estévez, Daniel S. Fabricant, Anna M. Fan, Ali Faqi, Suzanne E. Fenton, Vanessa A Fitsanakis, John Flaskos, Swaran J.S. Flora, Sue M. Ford, Domniki Fragou, Shayne C. Gad, Niels-Christian Ganderup, Dale R. Gardner, Ronette Gehring, Fernando Gil, Saryu Goel, Michael-Rock Goldsmith, Christopher M. Grulke, Mary Gulumian, P.K. Gupta, Ramesh C. Gupta, Sharon Gwaltney-Brant, Alan J Hargreaves, Kelly L. Harris, Holly E. Hatfield, Diane E. Heck, Antonio F. Hernández, Corey J. Hilmas, Evangelia Hondroulis, Darryl B. Hood, Kathryn Hudak, Pasi Huuskonen, Stewart B. Jacobson, Huajun Jin, Laurie B. Joseph, Jun Kanno, Anumantha G. Kanthasamy, Arthi Kanthasamy, Navinchandra M. Kaore, Shilpa N. Kaore, Bhupendra S. Kaphalia, Vesa Karttunen, Greer E. Kaufman, Ravneet Kaur, Hong Duck Kim, Prasada Rao S. Kodavanti, Urmila P. Kodavanti, George A. Kontadakis, Péter Krajcsi, Gopala Krishna, Kavya A. Krishna, Maria Kummu, George D. Kymionis, Michelle A. Lasher, Chen-zhong Li, Wei-Jiun Lin, Bommanna G. Loganathan, Jarkko Loikkanen, Anna E. Lokshin, Marcello Lotti, Tzu-Pin Lu, Yi Lu, Chikezie Madu, Rémi Magnan, Brinda Mahadevan, Jane A. Mantey, María Rosa Martínez-Larrañaga, Vincent P. Meador, Dejan Milatovic, Pushpinder K. Multani, Päivi Myllynen, Kirsi Myöhänen, Rekek Negga, Jairo Nelson, Brian M. Nolen, Meliton N. Novilla, Stephanie Padilla, Carlos M. Palmeira, Kip E. Panter, Markku Pasanen, Daniel J. Patrick, Sofia Pavanello, Olavi Pelkonen, Claudia Pellacani, Michael A. Pellizzon, Andrew D. Penman, Martin Phillips, Jason Pitt, Argyro Plaka, Aramandla Ramesh, Kausik Ray, Casey E. Reed, Jenni Repo, Matthew R. Ricci, Anabela P. Rolo, Magdalini Sachana, Heidi Sahlman, Nitin Saini, William F. Salminen, Kai Savolainen, Laura K. Schnackenberg, D.T. Selvam, Praveen Sharma, Qiang Shi, Elina Sieppi, Jon Sobus, Miguel A. Sogorb, Melissa Stick, Markus Storvik, David T. Szabo, Yu-Mei Tan, João S. Teodoro, Rogelio Tornero-Velez, Beáta Toth, Aristides M. Tsatsakis, Kirsi Vähäkangas, Deon van der Merwe, Ana T. Varela, Eugenio Vilanova, Suryanarayana V. Vulimiri, Kevin D. Welch, Xi Yang, Snjezana Zaja-Milatovic, and Csaba K. Zoltani

Published

2014

47. Biomarkers of acute and chronic pancreatitis

Author

Bhupendra S. Kaphalia

Subjects

medicine.medical_specialty, Pathology, Poor prognosis, business.industry, medicine.disease, Molecular biomarkers, Gastroenterology, Exocrine pancreas, Internal medicine, Pancreatic cancer, medicine, Pancreatitis, Acute pancreatitis, Stage (cooking), business, Microrna array

Abstract

Pancreatitis and pancreatic cancers are very serious diseases with very poor prognosis, and many patients die before even reaching the clinical stage. Therefore, identification of reliable and specific biomarkers at early stages of pancreatitis and pancreatic cancers could be the key to their early prevention and therapy. In this chapter, currently used and putative biomarkers of acute and chronic pancreatitis are summarized. Serum total amylase and lipase in combination or individually remain the most widely used biomarkers for clinical diagnostics of acute pancreatitis. Definitely, lipase assay has an advantage over amylase in clinical diagnostics of acute pancreatitis rather than chronic pancreatitis and appears to have greater specificity. However, imaging technologies strongly support the diagnosis of both acute and chronic pancreatitis. Identification and development of biomarkers of chronic pancreatitis remain challenging because of the impaired secretory component of the exocrine pancreas due to slow destruction of the gland during chronic pancreatitis, particularly at later stages. Therefore, the focus of future research lies in identification of molecular biomarkers by utilizing proteomic, metabolomic, and microRNA array technologies in well-defined experimental models followed by their confirmation in large cohorts of patient populations with acute and various stages of chronic pancreatitis.

Published

2014

48. Purification and Characterization of Rat Liver Microsomal Fatty Acid Ethyl and 2-Chloroethyl Ester Synthase and Their Relationship with Carboxylesterase (pI 6.1)

Author

Bhupendra S. Kaphalia, Ghulam Ansari, and Richard R. Fritz

Subjects

Male, Molecular Sequence Data, Adipose tissue, Toxicology, Carboxylesterase, Rats, Sprague-Dawley, Structure-Activity Relationship, Column chromatography, Pi, Animals, Amino Acid Sequence, Isoelectric Point, chemistry.chemical_classification, Chromatography, ATP synthase, biology, Chemistry, Fatty acid, General Medicine, Rats, Kinetics, Biochemistry, Rat liver, Microsomes, Liver, biology.protein, Microsome, Carboxylic Ester Hydrolases, Acyltransferases

Abstract

Previous studies have shown that fatty acid ethyl ester synthase (FAEES) which catalyzes the formation of ethyl or 2-chloroethyl esters of long-chain fatty acids is localized in the microsomal fraction of rat liver. A recent study suggests that rat adipose tissue FAEES is similar to rat liver microsomal carboxylesterase (CE) [Tsujita and Okuda (1992) J. Biol. Chem. 267, 23489-23494]. Since the interrelationships among FAEES, 2-chloroethyl ester synthase (FACEES), and cholesterol esterase (ChE) are also not clear at present, we purified and characterized FAEES and FACEES from rat hepatic microsomes and studied their functional and structural relationships with CE and ChE. The results of these studies showed that CE, FAEES, and FACEES activities copurified during each step of purification. Although gel-filtration column chromatography of DEAE-Sephacel purified microsomal protein resolved into two peaks with an estimated molecular weight of 180 (major) and 60 kDa (minor, this paper describes characterization of only the 180 kDa protein. CE, FAEES, and FACEES activities associated with homogeneous 180 kDa protein could be inhibited by a beta-esterase inhibitor (diisopropyl fluorophosphate) in an identical manner. This protein, however, showed only the hydrolytic activity, but not the synthetic activity for cholesterol oleate, indicating that it is distinct from ChE. The purified protein could be immunoprecipitated with the antibodies raised against rat adipose tissue FAEES, but not with antibodies against rat pancreatic ChE, demonstrating again that the purified protein is distinct from ChE. A single band corresponding to 60 kDa upon SDS-PAGE, under reduced denaturing conditions, indicates that the purified protein is a trimer. N-terminal amino acid sequence of the first 27 residues were identical to that of rat hepatic microsomal CE [Robbi et al. (1990) Biochem. J., 451-458] which suggests structural similarity of the purified protein with rat hepatic microsomal CE. Therefore, the functional and structural properties of the purified protein demonstrate that FAEES, FACEES, as well as CE activities are expressed by the same protein, purified in this study, which exists as a trimer (180 kDa) and is involved in biosynthesis of long-chain fatty acid esters of xenobiotic alcohols. Further studies on purification and characterization of the enzymes responsible for the esterification of xenobiotic alcohols with endogenous fatty acids from various target organs need to be conducted to determine their functional and structural interrelationships. Inhibition and induction studies of these enzyme(s) and the extent of observed toxicity could be important in understanding their role in etiology of chronic diseases induced by alcohol abuse.

Published

1997

49. Alcohol oxidizing enzymes and ethanol-induced cytotoxicity in rat pancreatic acinar AR42J cells

Author

Kamlesh K. Bhopale, Bhupendra S. Kaphalia, Miriam Falzon, and Ghulam Ansari

Subjects

Alcohol, Apoptosis, Acinar Cells, Pharmacology, Article, chemistry.chemical_compound, Pancreatitis, Chronic, Acinar cell, Animals, Viability assay, Ethanol metabolism, Pancreas, Alcohol dehydrogenase, Fomepizole, Ethanol, biology, Fatty Acids, Alcohol Dehydrogenase, Cell Biology, General Medicine, CYP2E1, Rats, Alcoholism, Biochemistry, chemistry, biology.protein, Pyrazoles, Oxidation-Reduction, Developmental Biology

Abstract

Alcoholic chronic pancreatitis (ACP) is a serious inflammatory disease causing significant morbidity and mortality. Due to lack of a suitable animal model, the underlying mechanism of ACP is poorly understood. Chronic alcohol abuse inhibits alcohol dehydrogenase (ADH) and facilitates nonoxidative metabolism of ethanol to fatty acid ethyl esters (FAEEs) in the pancreas frequently damaged during chronic ethanol abuse. Earlier, we reported a concentration-dependent formation of FAEEs and cytotoxicity in ethanol-treated rat pancreatic tumor (AR42J) cells, which express high FAEE synthase activity as compared to ADH and cytochrome P450 2E1. Therefore, the present study was undertaken to investigate the role of various ethanol oxidizing enzymes in ethanol-induced pancreatic acinar cell injury. Confluent AR42J cells were pre-treated with inhibitors of ADH class I and II [4-methylpyrazole (MP)] or class I, II, and III [1,10-phenanthroline (PT)], cytochrome P450 2E1 (trans-1,2-dichloroethylene) or catalase (sodium azide) followed by incubation with 800 mg% ethanol at 37°C for 6 h. Ethanol metabolism, cell viability, cytotoxicity (apoptosis and necrosis), cell proliferation status, and formation of FAEEs in AR42J cells were measured. The cell viability and cell proliferation rate were significantly reduced in cells pretreated with 1,10-PT + ethanol followed by those with 4-MP + ethanol. In situ formation of FAEEs was twofold greater in cells incubated with 1,10-PT + ethanol and ∼1.5-fold in those treated with 4-MP + ethanol vs. respective controls. However, cells treated with inhibitors of cytochrome P450 2E1 or catalase in combination of ethanol showed no significant changes either for FAEE formation, cell death or proliferation rate. Therefore, an impaired ADH class I-III catalyzed oxidation of ethanol appears to be a key contributing factor in ethanol-induced pancreatic injury via formation of nonoxidative metabolites of ethanol.

Published

2013

50. NONOXIDATIVE METABOLISM OF 2 BUTOXYETHANOL VIA FATTY ACID CONJUGATION IN FISCHER 344 RATS

Author

Ghulam Ansari, Burhan I. Ghanayem, and Bhupendra S. Kaphalia

Subjects

Male, Administration, Oral, Ether, Toxicology, High-performance liquid chromatography, chemistry.chemical_compound, 2-Butoxyethanol, Animals, Organic chemistry, Carbon Radioisotopes, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Fatty Acids, Fatty acid, Esters, Metabolism, Pollution, Rats, Inbred F344, Rats, Solvent, Enzyme, Liver, chemistry, Solvents, Ethylene Glycols, Oxidation-Reduction, Ethylene glycol, Acyltransferases

Abstract

Nonoxidative metabolism of ethylene glycol monobutyl ether (2-butoxyethanol or BE) via fatty acid conjugation was studied in the liver of Fischer 344 male rats following a single oral administration of 500 mg/kg body weight [ethyl-1,2-14C]BE (70 microCi/kg). Animals were killed 2 h after the treatment, hepatic lipids extracted, and the neutral lipids were separated using solid-phase extraction. The neutral lipid fraction was subjected to preparative thin-layer chromatography, and the esters corresponding to the relative flow of authentic fatty acid 2-butoxyethyl esters were recovered and analyzed by reversed-phase high-performance liquid chromatography (HPLC) using methanol-water (37:3, v/v) as solvent. Approximately 85% of the 14C label present in the ester fraction was coeluted at retention times corresponding to the different fatty acid 2-butoxyethyl ester standards. The radioactive fractions were analyzed by electron impact mass spectrometry. Molecular ion peaks and fragmentation patterns similar to that of 16:0, 18:0, 18:1, 18:2, and 20:4 fatty acid 2-butoxyethyl ester standards were detected in the corresponding radioactive HPLC fractions. Fatty acid ethyl ester synthase (FAEES), purified from the rat liver microsomal fraction, was also found to catalyze the formation of 18:1 fatty acid 2-butoxyethyl ester. These studies demonstrate that BE is metabolized nonoxidatively via conjugation with long-chain fatty acids, and the formation of these esters appears to be catalyzed by the enzyme(s) involved in fatty acid conjugation of xenobiotic alcohols. However, the biological significance of BE conjugation with fatty acids remains to be investigated.

Published

1996