Your search keyword '"Dorothy H. Slentz"' showing total 27 results

1. Chemotherapeutic drug screening in 3D-Bioengineered human myobundles provides insight into taxane-induced myotoxicities

Author

Maria J. Torres, Xu Zhang, Dorothy H. Slentz, Timothy R. Koves, Hailee Patel, George A. Truskey, and Deborah M. Muoio

Subjects

Pharmacology, Biological sciences, Cancer, Bioengineering, Science

Abstract

Summary: Two prominent frontline breast cancer (BC) chemotherapies commonly used in combination, doxorubicin (DOX) and docetaxel (TAX), are associated with long-lasting cardiometabolic and musculoskeletal side effects. Whereas DOX has been linked to mitochondrial dysfunction, mechanisms underlying TAX-induced myotoxicities remain uncertain. Here, the metabolic and functional consequences of TAX ± DOX were investigated using a 3D-bioengineered model of adult human muscle and a drug dosing regimen designed to resemble in vivo pharmacokinetics. DOX potently reduced mitochondrial respiratory capacity, 3D-myobundle size, and contractile force, whereas TAX-induced acetylation and remodeling of the microtubule network led to perturbations in glucose uptake, mitochondrial respiratory sensitivity, and kinetics of fatigue, without compromising tetanic force generation. These findings suggest TAX-induced remodeling of the microtubule network disrupts glucose transport and respiratory control in skeletal muscle and thereby have important clinical implications related to the cardiometabolic health and quality of life of BC patients and survivors.

Published

2022

2. Nicotinamide riboside supplementation confers marginal metabolic benefits in obese mice without remodeling the muscle acetyl-proteome

Author

Ashley S. Williams, Timothy R. Koves, Yasminye D. Pettway, James A. Draper, Dorothy H. Slentz, Paul A. Grimsrud, Olga R. Ilkayeva, and Deborah M. Muoio

Subjects

Physiology, Proteomics, Nutrition, Science

Abstract

Summary: Nicotinamide riboside supplements (NRS) have been touted as a nutraceutical that promotes cardiometabolic and musculoskeletal health by enhancing nicotinamide adenine dinucleotide (NAD+) biosynthesis, mitochondrial function, and/or the activities of NAD-dependent sirtuin deacetylase enzymes. This investigation examined the impact of NRS on whole body energy homeostasis, skeletal muscle mitochondrial function, and corresponding shifts in the acetyl-lysine proteome, in the context of diet-induced obesity using C57BL/6NJ mice. The study also included a genetically modified mouse model that imposes greater demand on sirtuin flux and associated NAD+ consumption, specifically within muscle tissues. In general, whole body glucose control was marginally improved by NRS when administered at the midpoint of a chronic high-fat diet, but not when given as a preventative therapy upon initiation of the diet. Contrary to anticipated outcomes, the study produced little evidence that NRS increases tissue NAD+ levels, augments mitochondrial function, and/or mitigates diet-induced hyperacetylation of the skeletal muscle proteome.

Published

2022

3. Respiratory Phenomics across Multiple Models of Protein Hyperacylation in Cardiac Mitochondria Reveals a Marginal Impact on Bioenergetics

Author

Kelsey H. Fisher-Wellman, James A. Draper, Michael T. Davidson, Ashley S. Williams, Tara M. Narowski, Dorothy H. Slentz, Olga R. Ilkayeva, Robert D. Stevens, Gregory R. Wagner, Rami Najjar, Mathew D. Hirschey, J. Will Thompson, David P. Olson, Daniel P. Kelly, Timothy R. Koves, Paul A. Grimsrud, and Deborah M. Muoio

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Acyl CoA metabolites derived from the catabolism of carbon fuels can react with lysine residues of mitochondrial proteins, giving rise to a large family of post-translational modifications (PTMs). Mass spectrometry-based detection of thousands of acyl-PTMs scattered throughout the proteome has established a strong link between mitochondrial hyperacylation and cardiometabolic diseases; however, the functional consequences of these modifications remain uncertain. Here, we use a comprehensive respiratory diagnostics platform to evaluate three disparate models of mitochondrial hyperacylation in the mouse heart caused by genetic deletion of malonyl CoA decarboxylase (MCD), SIRT5 demalonylase and desuccinylase, or SIRT3 deacetylase. In each case, elevated acylation is accompanied by marginal respiratory phenotypes. Of the >60 mitochondrial energy fluxes evaluated, the only outcome consistently observed across models is a ∼15% decrease in ATP synthase activity. In sum, the findings suggest that the vast majority of mitochondrial acyl PTMs occur as stochastic events that minimally affect mitochondrial bioenergetics. : Fisher-Wellman et al. use a recently developed mitochondrial diagnostics platform for deep phenotyping of heart mitochondria derived from three disparate genetic models of protein hyperacylation. Their findings oppose the notion that hyperacylation of the mitochondrial proteome leads to broad-ranging vulnerabilities in respiratory function and bioenergetics. Keywords: mitochondrial diagnostics, lysine acylation, malonylation, ATP synthase

Published

2019

4. Obesity and lipid stress inhibit carnitine acetyltransferase activity[S]

Author

Sarah E. Seiler, Ola J. Martin, Robert C. Noland, Dorothy H. Slentz, Karen L. DeBalsi, Olga R. Ilkayeva, Jie An, Christopher B. Newgard, Timothy R. Koves, and Deborah M. Muoio

Subjects

acetyl-coenzyme A, acylcarnitines, lipid metabolism, mitochondria, muscle, diabetes, Biochemistry, QD415-436

Abstract

Carnitine acetyltransferase (CrAT) is a mitochondrial matrix enzyme that catalyzes the interconversion of acetyl-CoA and acetylcarnitine. Emerging evidence suggests that this enzyme functions as a positive regulator of total body glucose tolerance and muscle activity of pyruvate dehydrogenase (PDH), a mitochondrial enzyme complex that promotes glucose oxidation and is feedback inhibited by acetyl-CoA. Here, we used tandem mass spectrometry-based metabolic profiling to identify a negative relationship between CrAT activity and muscle content of lipid intermediates. CrAT specific activity was diminished in muscles from obese and diabetic rodents despite increased protein abundance. This reduction in enzyme activity was accompanied by muscle accumulation of long-chain acylcarnitines (LCACs) and acyl-CoAs and a decline in the acetylcarnitine/acetyl-CoA ratio. In vitro assays demonstrated that palmitoyl-CoA acts as a direct mixed-model inhibitor of CrAT. Similarly, in primary human myocytes grown in culture, nutritional and genetic manipulations that promoted mitochondrial influx of fatty acids resulted in accumulation of LCACs but a pronounced decrease of CrAT-derived short-chain acylcarnitines. These results suggest that lipid-induced antagonism of CrAT might contribute to decreased PDH activity and glucose disposal in the context of obesity and diabetes.

Published

2014

5. Pyruvate-supported flux through medium-chain ketothiolase promotes mitochondrial lipid tolerance in cardiac and skeletal muscles

Author

Timothy R. Koves, Guo-Fang Zhang, Michael T. Davidson, Alec B. Chaves, Scott B. Crown, Jordan M. Johnson, Dorothy H. Slentz, Paul A. Grimsrud, and Deborah M. Muoio

Subjects

Physiology, Cell Biology, Molecular Biology

Published

2023

6. Nicotinamide riboside supplementation confers marginal metabolic benefits in obese mice without remodeling the muscle acetyl-proteome

Author

Ashley S. Williams, Timothy R. Koves, Yasminye D. Pettway, James A. Draper, Dorothy H. Slentz, Paul A. Grimsrud, Olga R. Ilkayeva, and Deborah M. Muoio

Subjects

Proteomics, Multidisciplinary, Physiology, Science, Article, Nutrition

Abstract

Summary Nicotinamide riboside supplements (NRS) have been touted as a nutraceutical that promotes cardiometabolic and musculoskeletal health by enhancing nicotinamide adenine dinucleotide (NAD+) biosynthesis, mitochondrial function, and/or the activities of NAD-dependent sirtuin deacetylase enzymes. This investigation examined the impact of NRS on whole body energy homeostasis, skeletal muscle mitochondrial function, and corresponding shifts in the acetyl-lysine proteome, in the context of diet-induced obesity using C57BL/6NJ mice. The study also included a genetically modified mouse model that imposes greater demand on sirtuin flux and associated NAD+ consumption, specifically within muscle tissues. In general, whole body glucose control was marginally improved by NRS when administered at the midpoint of a chronic high-fat diet, but not when given as a preventative therapy upon initiation of the diet. Contrary to anticipated outcomes, the study produced little evidence that NRS increases tissue NAD+ levels, augments mitochondrial function, and/or mitigates diet-induced hyperacetylation of the skeletal muscle proteome., Graphical abstract, Highlights • Dietary NR supplementation (NRS) raises plasma and muscle NAM levels in obese mice • NRS given post obesity slightly improved glucose control and mitochondrial function • NRS did not oppose obesity-induced remodeling of the muscle acetyl-proteome • NRS during weight gain did not protect glucose control and mitochondrial function, Physiology; Proteomics; Nutrition

Published

2021

7. Chemotherapeutic drug screening in 3D-Bioengineered human myobundles provides insight into taxane-induced myotoxicities

Author

Maria J. Torres, Xu Zhang, Dorothy H. Slentz, Timothy R. Koves, Hailee Patel, George A. Truskey, and Deborah M. Muoio

Subjects

Multidisciplinary

Abstract

Two prominent frontline breast cancer (BC) chemotherapies commonly used in combination, doxorubicin (DOX) and docetaxel (TAX), are associated with long-lasting cardiometabolic and musculoskeletal side effects. Whereas DOX has been linked to mitochondrial dysfunction, mechanisms underlying TAX-induced myotoxicities remain uncertain. Here, the metabolic and functional consequences of TAX ± DOX were investigated using a 3D-bioengineered model of adult human muscle and a drug dosing regimen designed to resemble

Published

2021

8. Abstract P284: The Chemotherapeutic Agent Docetaxel Disrupts Mitochondrial Energetics in 3D Human Bioengineered Myobundles

Author

Maria J Torres Alcalde, Timothy R. Koves, Dorothy H. Slentz, Deborah M. Muoio, Xu Zang, and George A. Truskey

Subjects

Breast cancer, Docetaxel, business.industry, Physiology (medical), medicine, Cancer research, Mitochondrial energetics, Doxorubicin, Mitochondrion, Cardiology and Cardiovascular Medicine, business, medicine.disease, medicine.drug

Abstract

Taxanes (i.e. docetaxel, (TAX)) comprise the first line-treatment for breast cancer (BC), mostly in combination with anthracyclines like doxorubicin (DOX). The efficacy of these drugs as antineoplastic agents has helped to boost 10-year survival rates to > 90%, leading to a fast-growing population of over 3 million BC survivors in the US. However, epidemiological evidence shows that the highly abrasive nature of these therapies can give rise to a vicious cycle of metabolic decline and physical inactivity that compromises quality of life and increases risk of numerous musculoskeletal and cardio-metabolic disorders including arthritis, sarcopenic obesity, cardiovascular disease and type 2 diabetes. Major side effects of TAX include peripheral neuropathy, arthralgia, myalgia and muscle weakness. Taxanes act primarily by stabilizing microtubules (MTs), which causes cell cycle arrest. Importantly, MT dynamics can also impact mitochondrial function. For example, the MT protein unit, tubulin, can bind to the outer mitochondrial protein channel, VDAC, and thereby affect ATP transport to the cytosol. Herein, we sought to test the hypothesis that TAX exacerbates DOX-induced mitochondrial dysfunction, which is thought to underlie anthracyclines’ cardiotoxicity. To this end, we leveraged a newly developed 3-D bioengineered model of human muscle organoids (myobundles), derived from primary human skeletal muscle progenitor cells (HSkM), to study mechanisms of TAX-induced myotoxicity and its interactions with DOX. Preliminary findings in primary HSkM cells exposed to 3 daily x 3 h treatments with TAX (1 - 100 nM) +/- 10 nM DOX caused a robust ~10-fold acetylation of a-tubulin at lysine 40 (AcK40), reflecting marked stabilization of MTs. TAX treatment decreased basal and ATP-linked respiration (JO 2 ) up to 30 % (p2 (+FCCP) remained unchanged, suggesting TAX disrupts mitochondrial thermodynamics and energy transfer, rather than maximal oxidative phosphorylation capacity. Exposure of 3D myobundles to a TAX+/-DOX regimen that mimicked human pharmacokinetics post-infusion led to a 30-fold increase (p2 response to ADP (KM ADP 2- and 4-fold higher, p2 (pADP . We hypothesize that the TAX-driven stabilization of MTs leads to detrimental MT-mitochondria interactions that disrupt ATP/ADP transfer between cellular compartments, exacerbating DOX toxicity and ultimately impairing muscle function. The present findings provide novel insights into the mechanisms of TAX-induced myotoxicities, which is of paramount importance for developing therapeutic strategies to improve cardiovascular health and quality of life of long-term breast cancer survivors.

Published

2019

9. Disruption of Acetyl-Lysine Turnover in Muscle Mitochondria Promotes Insulin Resistance and Redox Stress without Overt Respiratory Dysfunction

Author

Deborah M. Muoio, Scott B. Crown, Louise Lantier, Michael T. Davidson, Paul A. Grimsrud, James A. Draper, Tara M. Narowski, Ashley S. Williams, Dorothy H. Slentz, Kelsey H. Fisher-Wellman, Timothy R. Koves, Maria J. Torres, and David H. Wasserman

Subjects

0301 basic medicine, Male, Proteome, Physiology, Lysine, Context (language use), Mitochondrion, Diet, High-Fat, Article, Mitochondrial Proteins, 03 medical and health sciences, Mice, 0302 clinical medicine, Insulin resistance, Acetyl Coenzyme A, Sirtuin 3, medicine, Animals, Homeostasis, Insulin, Respiratory function, Molecular Biology, Beta oxidation, Creatine Kinase, Membrane Potential, Mitochondrial, Mice, Knockout, Carnitine O-Acetyltransferase, biology, Chemistry, Acetylation, Cell Biology, Hydrogen Peroxide, medicine.disease, Cell biology, Mitochondria, Muscle, Oxidative Stress, 030104 developmental biology, Sirtuin, biology.protein, Thermodynamics, Insulin Resistance, Energy Metabolism, Oxidation-Reduction, 030217 neurology & neurosurgery

Abstract

This study sought to examine the functional significance of mitochondrial protein acetylation using a double knockout (DKO) mouse model harboring muscle-specific deficits in acetyl CoA buffering and lysine deacetylation, due to genetic ablation of carnitine acetyltransferase and Sirtuin 3, respectively. DKO mice are highly susceptible to extreme hyperacetylation of the mitochondrial proteome and develop a more severe form of diet-induced insulin resistance than either single KO mouse line. However, the functional phenotype of hyperacetylated DKO mitochondria is largely normal. Of the >120 measures of respiratory function assayed, the most consistently observed traits of a markedly heightened acetyl-lysine landscape are enhanced oxygen flux in the context of fatty acid fuel and elevated rates of electron leak. In sum, the findings challenge the notion that lysine acetylation causes broad-ranging damage to mitochondrial quality and performance, and raise the possibility that acetyl-lysine turnover, rather than acetyl-lysine stoichiometry, modulates redox balance and carbon flux.

Published

2019

10. Respiratory Phenomics across Multiple Models of Protein Hyperacylation in Cardiac Mitochondria Reveals a Marginal Impact on Bioenergetics

Author

Daniel P. Kelly, Michael T. Davidson, Gregory R. Wagner, Paul A. Grimsrud, Dorothy H. Slentz, David P. Olson, J. Will Thompson, Mathew D. Hirschey, Olga Ilkayeva, Deborah M. Muoio, James A. Draper, Tara M. Narowski, Rami Najjar, Timothy R. Koves, Kelsey H. Fisher-Wellman, Robert Stevens, and Ashley S. Williams

Subjects

0301 basic medicine, Male, SIRT5, SIRT3, Bioenergetics, Carboxy-Lyases, Cell Respiration, General Biochemistry, Genetics and Molecular Biology, Mitochondria, Heart, Article, 03 medical and health sciences, Acyl-CoA, chemistry.chemical_compound, Mice, 0302 clinical medicine, Sirtuin 3, Animals, Sirtuins, lcsh:QH301-705.5, ATP synthase, biology, Catabolism, Acetylation, Malonyl-CoA decarboxylase, Mice, Inbred C57BL, 030104 developmental biology, lcsh:Biology (General), chemistry, Biochemistry, Proteome, biology.protein, Energy Metabolism, Protein Processing, Post-Translational, 030217 neurology & neurosurgery

Abstract

SUMMARY Acyl CoA metabolites derived from the catabolism of carbon fuels can react with lysine residues of mitochondrial proteins, giving rise to a large family of post-translational modifications (PTMs). Mass spectrometry-based detection of thousands of acyl-PTMs scattered throughout the proteome has established a strong link between mitochondrial hyperacylation and cardiometabolic diseases; however, the functional consequences of these modifications remain uncertain. Here, we use a comprehensive respiratory diagnostics platform to evaluate three disparate models of mitochondrial hyperacylation in the mouse heart caused by genetic deletion of malonyl CoA decarboxylase (MCD), SIRT5 demalonylase and desuccinylase, or SIRT3 deacetylase. In each case, elevated acylation is accompanied by marginal respiratory phenotypes. Of the >60 mitochondrial energy fluxes evaluated, the only outcome consistently observed across models is a ~15% decrease in ATP synthase activity. In sum, the findings suggest that the vast majority of mitochondrial acyl PTMs occur as stochastic events that minimally affect mitochondrial bioenergetics., Graphical Abstract, In Brief Fisher-Wellman et al. use a recently developed mitochondrial diagnostics platform for deep phenotyping of heart mitochondria derived from three disparate genetic models of protein hyperacylation. Their findings oppose the notion that hyperacylation of the mitochondrial proteome leads to broad-ranging vulnerabilities in respiratory function and bioenergetics.

Published

2018

11. Muscle-Specific Overexpression of PGC-1α Does Not Augment Metabolic Improvements in Response to Exercise and Caloric Restriction

Author

Karen L. DeBalsi, Karen I. Crain, Olga Ilkayeva, Michael Kinter, Robert Stevens, Sarah E. Seiler, Dorothy H. Slentz, C. Lawrence Kien, Catherine R. Mikus, Kari E. Wong, and Deborah M. Muoio

Subjects

Male, Proteomics, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Transgene, Metabolite, Oxidative phosphorylation, Mitochondrion, Biology, Motor Activity, Energy homeostasis, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Internal medicine, Physical Conditioning, Animal, Internal Medicine, medicine, Animals, Muscle, Skeletal, 030304 developmental biology, Caloric Restriction, 2. Zero hunger, 0303 health sciences, Insulin, Dietary Fats, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Mitochondria, Muscle, Endocrinology, Metabolism, Mitochondrial biogenesis, chemistry, Lipotoxicity, Gene Expression Regulation, Energy Metabolism, Oxidation-Reduction, 030217 neurology & neurosurgery, Transcription Factors

Abstract

This study used mice with muscle-specific overexpression of PGC-1α, a transcriptional coactivator that promotes mitochondrial biogenesis, to determine whether increased oxidative potential facilitates metabolic improvements in response to lifestyle modification. MCK-PGC1α mice and nontransgenic (NT) littermates were fed a high-fat diet (HFD) for 10 weeks, followed by stepwise exposures to voluntary wheel running (HFD+Ex) and then 25% caloric restriction with exercise (Ex/CR), each for an additional 10 weeks with continued HFD. Running and CR improved weight and glucose control similarly in MCK-PGC1α and NT mice. Sedentary MCK-PGC1α mice were more susceptible to diet-induced glucose intolerance, and insulin action measured in isolated skeletal muscles remained lower in the transgenic compared with the NT group, even after Ex/CR. Comprehensive profiling of >200 metabolites and lipid intermediates revealed dramatic group-specific responses to the intervention but did not produce a lead candidate that tracked with changes in glucose tolerance irrespective of genotype. Instead, principal components analysis identified a chemically diverse metabolite cluster that correlated with multiple measures of insulin responsiveness. These findings challenge the notion that increased oxidative capacity defends whole-body energy homeostasis and suggest that the interplay between mitochondrial performance, lipotoxicity, and insulin action is more complex than previously proposed.

Published

2014

12. Obesity and lipid stress inhibit carnitine acetyltransferase activity[S]

Author

Deborah M. Muoio, Karen L. DeBalsi, Timothy R. Koves, Dorothy H. Slentz, Robert C. Noland, Ola J. Martin, Olga Ilkayeva, Sarah E. Seiler, Jie An, and Christopher B. Newgard

Subjects

Male, medicine.medical_specialty, muscle, Muscle Fibers, Skeletal, Pyruvate Dehydrogenase Complex, QD415-436, Mitochondrion, Biology, Biochemistry, Endocrinology, Acetyl Coenzyme A, acylcarnitines, Carnitine, Internal medicine, acetyl-coenzyme A, lipid metabolism, Diabetes Mellitus, medicine, Animals, Humans, Carnitine palmitoyltransferase II, Obesity, Carnitine O-palmitoyltransferase, Rats, Wistar, Carnitine O-acetyltransferase, Acetylcarnitine, Cells, Cultured, Research Articles, Carnitine O-Acetyltransferase, Carnitine O-Palmitoyltransferase, diabetes, Cell Biology, Pyruvate dehydrogenase complex, Enzyme assay, Rats, Zucker, mitochondria, biology.protein, medicine.drug

Abstract

Carnitine acetyltransferase (CrAT) is a mitochondrial matrix enzyme that catalyzes the interconversion of acetyl-CoA and acetylcarnitine. Emerging evidence suggests that this enzyme functions as a positive regulator of total body glucose tolerance and muscle activity of pyruvate dehydrogenase (PDH), a mitochondrial enzyme complex that promotes glucose oxidation and is feedback inhibited by acetyl-CoA. Here, we used tandem mass spectrometry-based metabolic profiling to identify a negative relationship between CrAT activity and muscle content of lipid intermediates. CrAT specific activity was diminished in muscles from obese and diabetic rodents despite increased protein abundance. This reduction in enzyme activity was accompanied by muscle accumulation of long-chain acylcarnitines (LCACs) and acyl-CoAs and a decline in the acetylcarnitine/acetyl-CoA ratio. In vitro assays demonstrated that palmitoyl-CoA acts as a direct mixed-model inhibitor of CrAT. Similarly, in primary human myocytes grown in culture, nutritional and genetic manipulations that promoted mitochondrial influx of fatty acids resulted in accumulation of LCACs but a pronounced decrease of CrAT-derived short-chain acylcarnitines. These results suggest that lipid-induced antagonism of CrAT might contribute to decreased PDH activity and glucose disposal in the context of obesity and diabetes.

Published

2014

13. Targeted Metabolomics Connects Thioredoxin-interacting Protein (TXNIP) to Mitochondrial Fuel Selection and Regulation of Specific Oxidoreductase Enzymes in Skeletal Muscle

Author

Simon T. Hui, Karen L. DeBalsi, Sarah E. Seiler, Christopher G. R. Perry, Timothy R. Koves, P. Darrell Neufer, Olga Ilkayeva, Kari E. Wong, Robert Stevens, Luke I. Szweda, Deborah M. Muoio, Dorothy H. Slentz, Daniel S. Lark, and April H. Wittmann

Subjects

Thioredoxin-Interacting Protein, Bioenergetics, Oxidative phosphorylation, Mitochondrion, Biology, Biochemistry, Mice, Thioredoxins, Animals, Metabolomics, Muscle, Skeletal, Molecular Biology, Mice, Knockout, chemistry.chemical_classification, Reactive oxygen species, Catabolism, Cell Biology, Mitochondria, Mice, Inbred C57BL, Citric acid cycle, Metabolism, chemistry, Carrier Proteins, Energy Metabolism, Oxidoreductases, Oxidation-Reduction, TXNIP

Abstract

Thioredoxin-interacting protein (TXNIP) is an α-arrestin family member involved in redox sensing and metabolic control. Growing evidence links TXNIP to mitochondrial function, but the molecular nature of this relationship has remained poorly defined. Herein, we employed targeted metabolomics and comprehensive bioenergetic analyses to evaluate oxidative metabolism and respiratory kinetics in mouse models of total body (TKO) and skeletal muscle-specific (TXNIP(SKM-/-)) Txnip deficiency. Compared with littermate controls, both TKO and TXNIP(SKM-/-) mice had reduced exercise tolerance in association with muscle-specific impairments in substrate oxidation. Oxidative insufficiencies in TXNIP null muscles were not due to perturbations in mitochondrial mass, the electron transport chain, or emission of reactive oxygen species. Instead, metabolic profiling analyses led to the discovery that TXNIP deficiency causes marked deficits in enzymes required for catabolism of branched chain amino acids, ketones, and lactate, along with more modest reductions in enzymes of β-oxidation and the tricarboxylic acid cycle. The decrements in enzyme activity were accompanied by comparable deficits in protein abundance without changes in mRNA expression, implying dysregulation of protein synthesis or stability. Considering that TXNIP expression increases in response to starvation, diabetes, and exercise, these findings point to a novel role for TXNIP in coordinating mitochondrial fuel switching in response to nutrient availability.

Published

2014

14. Metabolic Remodeling of Human Skeletal Myocytes by Cocultured Adipocytes Depends on the Lipolytic State of the System

Author

Deborah M. Muoio, Y. Renee Lea-Currie, Benjamin M. Buehrer, William E. Kraus, Robert Stevens, James B. Nicoll, Joseph A. Houmard, Karen Everingham, Jean Paul Kovalik, Dorothy H. Slentz, and C. Lawrence Kien

Subjects

medicine.medical_specialty, Lipolysis, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Muscle Fibers, Skeletal, Gene Expression, 030209 endocrinology & metabolism, Fatty Acids, Nonesterified, Carbohydrate metabolism, Proinflammatory cytokine, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Insulin resistance, Thinness, Carnitine, Adipocyte, Internal medicine, Adipocytes, Internal Medicine, medicine, Humans, Insulin, Myocyte, Obesity, Triglycerides, 030304 developmental biology, 0303 health sciences, biology, medicine.disease, Coculture Techniques, Insulin receptor, Glucose, Metabolism, Endocrinology, chemistry, Adipogenesis, biology.protein, Female, Insulin Resistance

Abstract

OBJECTIVE Adipocyte infiltration of the musculoskeletal system is well recognized as a hallmark of aging, obesity, and type 2 diabetes. Intermuscular adipocytes might serve as a benign storage site for surplus lipid or play a role in disrupting energy homeostasis as a result of dysregulated lipolysis or secretion of proinflammatory cytokines. This investigation sought to understand the net impact of local adipocytes on skeletal myocyte metabolism. RESEARCH DESIGN AND METHODS Interactions between these two tissues were modeled using a coculture system composed of primary human adipocytes and human skeletal myotubes derived from lean or obese donors. Metabolic analysis of myocytes was performed after coculture with lipolytically silent or activated adipocytes and included transcript and metabolite profiling along with assessment of substrate selection and insulin action. RESULTS Cocultured adipocytes increased myotube mRNA expression of genes involved in oxidative metabolism, regardless of the donor and degree of lipolytic activity. Adipocytes in the basal state sequestered free fatty acids, thereby forcing neighboring myotubes to rely more heavily on glucose fuel. Under this condition, insulin action was enhanced in myotubes from lean but not obese donors. In contrast, when exposed to lipolytically active adipocytes, cocultured myotubes shifted substrate use in favor of fatty acids, which was accompanied by intracellular accumulation of triacylglycerol and even-chain acylcarnitines, decreased glucose oxidation, and modest attenuation of insulin signaling. CONCLUSIONS The effects of cocultured adipocytes on myocyte substrate selection and insulin action depended on the metabolic state of the system. These findings are relevant to understanding the metabolic consequences of intermuscular adipogenesis.

Published

2011

15. Creation of versatile cloning platforms for transgene expression and dCas9-based epigenome editing

Author

Dorothy H. Slentz, Christopher B. Newgard, Michelle Arlotto, Jonathan M. Haldeman, Deborah M. Muoio, Amanda E. Conway, and Thomas C. Becker

Subjects

Epigenomics, Genetic Vectors, Context (language use), Computational biology, Biology, Adenoviridae, 03 medical and health sciences, Islets of Langerhans, Mice, 0302 clinical medicine, Genetics, Epigenome editing, Animals, Humans, Vector (molecular biology), Epigenetics, Transgenes, Enhancer, Promoter Regions, Genetic, 030304 developmental biology, Gene Editing, Histone Demethylases, Homeodomain Proteins, 0303 health sciences, Cas9, Lentivirus, Epigenome, Sleeping Beauty transposon system, Rats, Enhancer Elements, Genetic, HEK293 Cells, Gene Expression Regulation, DNA Transposable Elements, Trans-Activators, Methods Online, Insulinoma, CRISPR-Cas Systems, Genetic Engineering, 030217 neurology & neurosurgery, RNA, Guide, Kinetoplastida

Abstract

Genetic manipulation via transgene overexpression, RNAi, or Cas9-based methods is central to biomedical research. Unfortunately, use of these tools is often limited by vector options. We have created a modular platform (pMVP) that allows a gene of interest to be studied in the context of an array of promoters, epitope tags, conditional expression modalities, and fluorescent reporters, packaged in 35 custom destination vectors, including adenovirus, lentivirus, PiggyBac transposon, and Sleeping Beauty transposon, in aggregate >108,000 vector permutations. We also used pMVP to build an epigenetic engineering platform, pMAGIC, that packages multiple gRNAs and either Sa-dCas9 or x-dCas9(3.7) fused to one of five epigenetic modifiers. Importantly, via its compatibility with adenoviral vectors, pMAGIC uniquely enables use of dCas9/LSD1 fusions to interrogate enhancers within primary cells. To demonstrate this, we used pMAGIC to target Sa-dCas9/LSD1 and modify the epigenetic status of a conserved enhancer, resulting in altered expression of the homeobox transcription factor PDX1 and its target genes in pancreatic islets and insulinoma cells. In sum, the pMVP and pMAGIC systems empower researchers to rapidly generate purpose-built, customized vectors for manipulation of gene expression, including via targeted epigenetic modification of regulatory elements in a broad range of disease-relevant cell types.

Published

2018

16. Mitochondrial Overload and Incomplete Fatty Acid Oxidation Contribute to Skeletal Muscle Insulin Resistance

Author

Jason R.B. Dyck, Timothy R. Koves, Gary D. Lopaschuk, Christopher B. Newgard, James R. Bain, Merrie Mosedale, Robert C. Noland, Olga Ilkayeva, Dorothy H. Slentz, Robert Stevens, John R. Ussher, and Deborah M. Muoio

Subjects

Blood Glucose, medicine.medical_specialty, Carboxy-Lyases, Physiology, Muscle Fibers, Skeletal, HUMDISEASE, 030209 endocrinology & metabolism, Mitochondrion, Cell Line, 03 medical and health sciences, Mice, 0302 clinical medicine, Carnitine palmitoyltransferase 1, Insulin resistance, Internal medicine, medicine, Animals, Obesity, Muscle, Skeletal, Beta oxidation, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, Mice, Knockout, 0303 health sciences, biology, Catabolism, Fatty Acids, Fatty acid, Skeletal muscle, Cell Biology, Glucose Tolerance Test, medicine.disease, Lipid Metabolism, Dietary Fats, Mitochondria, Rats, Insulin receptor, Endocrinology, medicine.anatomical_structure, chemistry, SIGNALING, biology.protein, Insulin Resistance, Oxidation-Reduction

Abstract

Summary Previous studies have suggested that insulin resistance develops secondary to diminished fat oxidation and resultant accumulation of cytosolic lipid molecules that impair insulin signaling. Contrary to this model, the present study used targeted metabolomics to find that obesity-related insulin resistance in skeletal muscle is characterized by excessive β-oxidation, impaired switching to carbohydrate substrate during the fasted-to-fed transition, and coincident depletion of organic acid intermediates of the tricarboxylic acid cycle. In cultured myotubes, lipid-induced insulin resistance was prevented by manipulations that restrict fatty acid uptake into mitochondria. These results were recapitulated in mice lacking malonyl-CoA decarboxylase (MCD), an enzyme that promotes mitochondrial β-oxidation by relieving malonyl-CoA-mediated inhibition of carnitine palmitoyltransferase 1. Thus, mcd −/− mice exhibit reduced rates of fat catabolism and resist diet-induced glucose intolerance despite high intramuscular levels of long-chain acyl-CoAs. These findings reveal a strong connection between skeletal muscle insulin resistance and lipid-induced mitochondrial stress.

Published

2008

17. Morphology and ultrastructure of differentiating three-dimensional mammalian skeletal muscle in a collagen gel

Author

Dorothy A. Lowell, Mary C. Reedy, George A. Truskey, Sarah J. Zhang, Dorothy H. Slentz, Caroline Rhim, and William E. Kraus

Subjects

Sarcomeres, Pathology, medicine.medical_specialty, Myofilament, Physiology, Cell Culture Techniques, Biology, Sarcomere, Mice, Cellular and Molecular Neuroscience, Imaging, Three-Dimensional, Microscopy, Electron, Transmission, Physiology (medical), Myosin, medicine, Animals, Myocyte, Muscle, Skeletal, Cells, Cultured, Actin, Mice, Inbred C3H, Myogenesis, Skeletal muscle, Cell Differentiation, Cell biology, medicine.anatomical_structure, Collagen, Neurology (clinical), Myofibril

Abstract

Because previous studies of three-dimensional skeletal muscle cultures have shown limited differentiation, the goal of this study was to establish conditions that would produce mature sarcomeres in a mammalian-derived skeletal muscle construct. We evaluated the differentiation of bioartificial muscles generated from C(2)C(12) myoblasts in a collagen gel cultured under steady, passive tension for up to 36 days. Staining for alpha-actinin, myosin, and F-actin indicated the presence of striated fibers as early as 6 days post-differentiation. Electron microscopy at 16 days post-differentiation revealed multinucleated myotubes with ordered, striated myofibers. At 33 days, the cultures contained collagen fibers and showed localization of paxillin at the fiber termini, suggesting that myotendinous junctions were forming. The present study demonstrates mature muscle synthesis in a three-dimensional system using a pure mammalian myoblast cell line. Our results suggest that this culture model can be used to evaluate the effects of various mechanical and biochemical cues on muscle development under normal and pathological conditions.

Published

2007

18. Metabolomic Quantitative Trait Loci (mQTL) Mapping Implicates the Ubiquitin Proteasome System in Cardiovascular Disease Pathogenesis

Author

Elizabeth R. Hauser, Simon G. Gregory, Carol Haynes, Dorothy H. Slentz, Deidre R. Krupp, William E. Kraus, Elizabeth Grass, Robert Stevens, Michael J. Muehlbauer, Deborah M. Muoio, Damian M. Craig, James R. Bain, Xuejun Qin, Christopher B. Newgard, Svati H. Shah, and Lydia Coulter Kwee

Subjects

Cancer Research, Proteasome Endopeptidase Complex, lcsh:QH426-470, Quantitative Trait Loci, Genome-wide association study, Single-nucleotide polymorphism, 030204 cardiovascular system & hematology, Quantitative trait locus, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, 0302 clinical medicine, Metabolomics, Risk Factors, Carnitine, Genetics, Humans, Epigenetics, Molecular Biology, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, 0303 health sciences, Ubiquitin, DNA Methylation, Endoplasmic Reticulum Stress, 3. Good health, lcsh:Genetics, Cardiovascular Diseases, Expression quantitative trait loci, DNA methylation, Unfolded protein response, Research Article

Abstract

Levels of certain circulating short-chain dicarboxylacylcarnitine (SCDA), long-chain dicarboxylacylcarnitine (LCDA) and medium chain acylcarnitine (MCA) metabolites are heritable and predict cardiovascular disease (CVD) events. Little is known about the biological pathways that influence levels of most of these metabolites. Here, we analyzed genetics, epigenetics, and transcriptomics with metabolomics in samples from a large CVD cohort to identify novel genetic markers for CVD and to better understand the role of metabolites in CVD pathogenesis. Using genomewide association in the CATHGEN cohort (N = 1490), we observed associations of several metabolites with genetic loci. Our strongest findings were for SCDA metabolite levels with variants in genes that regulate components of endoplasmic reticulum (ER) stress (USP3, HERC1, STIM1, SEL1L, FBXO25, SUGT1) These findings were validated in a second cohort of CATHGEN subjects (N = 2022, combined p = 8.4x10-6–2.3x10-10). Importantly, variants in these genes independently predicted CVD events. Association of genomewide methylation profiles with SCDA metabolites identified two ER stress genes as differentially methylated (BRSK2 and HOOK2). Expression quantitative trait loci (eQTL) pathway analyses driven by gene variants and SCDA metabolites corroborated perturbations in ER stress and highlighted the ubiquitin proteasome system (UPS) arm. Moreover, culture of human kidney cells in the presence of levels of fatty acids found in individuals with cardiometabolic disease, induced accumulation of SCDA metabolites in parallel with increases in the ER stress marker BiP. Thus, our integrative strategy implicates the UPS arm of the ER stress pathway in CVD pathogenesis, and identifies novel genetic loci associated with CVD event risk., Author Summary Cardiovascular disease is a strongly heritable trait. Despite application of the latest genomic technologies, the genetic architecture of disease risk remains poorly defined, and mechanisms underlying this susceptibility are incompletely understood. In this study, we performed genome-wide mapping of heart disease-related metabolites measured in the blood as the genetic traits of interest (instead of the disease itself), in a large cohort of 3512 patients at risk of heart disease from the CATHGEN study. Our goal was to discover new cardiovascular disease genes and thereby mechanisms of disease pathogenesis by understanding the genes that regulate levels of these metabolites. These analyses identified novel genetic variants associated with metabolite levels and with cardiovascular disease itself. Importantly, by utilizing an unbiased systems-based approach integrating genetics, gene expression, epigenetics and metabolomics, we uncovered a novel pathway of heart disease pathogenesis, that of endoplasmic reticulum (ER) stress, represented by elevated levels of circulating short-chain dicarboxylacylcarnitine (SCDA) metabolites.

Published

2015

19. Peroxisome Proliferator-activated Receptor-γ Co-activator 1α-mediated Metabolic Remodeling of Skeletal Myocytes Mimics Exercise Training and Reverses Lipid-induced Mitochondrial Inefficiency

Author

Jie An, Christopher B. Newgard, Dorothy H. Slentz, Takayuki Akimoto, Timothy R. Koves, Deborah M. Muoio, Ping Li, G. Lynis Dohm, Zhen Yan, and Olga Ilkayeva

Subjects

medicine.medical_specialty, Peroxisome proliferator-activated receptor, Mitochondrion, Biology, Biochemistry, Insulin resistance, Physical Conditioning, Animal, Internal medicine, medicine, Animals, Myocyte, PPAR alpha, Rats, Wistar, Muscle, Skeletal, Molecular Biology, Beta oxidation, chemistry.chemical_classification, Muscle Cells, Skeletal muscle, Cell Biology, Peroxisome, medicine.disease, Lipids, Mitochondria, Muscle, Rats, Endocrinology, medicine.anatomical_structure, Mitochondrial biogenesis, chemistry, Energy Metabolism

Abstract

Peroxisome proliferator-activated receptor-gamma co-activator 1alpha (PGC1alpha) is a promiscuous co-activator that plays a key role in regulating mitochondrial biogenesis and fuel homeostasis. Emergent evidence links decreased skeletal muscle PGC1alpha activity and coincident impairments in mitochondrial performance to the development of insulin resistance in humans. Here we used rodent models to demonstrate that muscle mitochondrial efficiency is compromised by diet-induced obesity and is subsequently rescued by exercise training. Chronic high fat feeding caused accelerated rates of incomplete fatty acid oxidation and accumulation of beta-oxidative intermediates. The capacity of muscle mitochondria to fully oxidize a heavy influx of fatty acid depended on factors such as fiber type and exercise training and was positively correlated with expression levels of PGC1alpha. Likewise, an efficient lipid-induced substrate switch in cultured myocytes depended on adenovirus-mediated increases in PGC1alpha expression. Our results supported a novel paradigm in which a high lipid supply, occurring under conditions of low PGC1alpha, provokes a disconnect between mitochondrial beta-oxidation and tricarboxylic acid cycle activity. Conversely, the metabolic remodeling that occurred in response to PGC1alpha overexpression favored a shift from incomplete to complete beta-oxidation. We proposed that PGC1alpha enables muscle mitochondria to better cope with a high lipid load, possibly reflecting a fundamental metabolic benefit of exercise training.

Published

2005

20. Regulation of the insulin-like growth factor axis by increasing cell number in intestinal epithelial (IEC-6) cells

Author

Mark R. Corkins, Dorothy H. Slentz, Richard G. MacDonald, Diane V. Davis, and Jung Han Yoon Park

Subjects

Cell division, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Cell Count, Biology, Cell Line, Iodine Radioisotopes, Insulin-like growth factor, Endocrinology, Insulin-Like Growth Factor II, medicine, Animals, Secretion, RNA, Messenger, Northern blot, Insulin-Like Growth Factor I, Messenger RNA, Growth factor, Epithelial Cells, Intestinal epithelium, Rats, Cell biology, Intestines, Insulin-Like Growth Factor Binding Protein 2, Cell culture, Culture Media, Conditioned, Cell Division

Abstract

Insulin-like growth factor binding protein-2 (IGFBP-2) production as a function of cell number by intestinal epithelial cells (IEC-6) was regulated such that the IGFBP-2 concentration in 24-h conditioned medium reached a maximum, which was maintained despite increasing cell number. Northern blot analysis revealed that this effect could largely be attributed to decreasing IGFBP-2 mRNA. In contrast to IGFBP-2, secretion of IGF-II and accumulation of IGF-II mRNA by IEC-6 cells correlated positively with cell number. The highest level of IGF-II protein detected by immunoblotting of conditioned medium occurred in post-confluent cells. IGF-I stimulated the cells to grow to a high cellular density and inhibited IGFBP-2 secretion in a concentration-dependent fashion. We conclude that expression of IGF-II and IGFBP-2 are regulated in IEC-6 cells by cellular density, and IGF-II may act as a survival factor at high cell density.

Published

1999

21. Expression of insulin-like growth factor-II and insulin-like growth factor binding proteins during Caco-2 cell proliferation and differentiation

Author

Jon A. Vanderhoof, Dorothy H. Slentz, Mark R. Corkins, Marjorie J. Hrbek, Jung H.Y. Park, Robert H. McCusker, Nia M. Caruso, Beverly S. Schaffer, and Richard G. MacDonald

Subjects

biology, Physiology, Cell growth, Growth factor, medicine.medical_treatment, Cellular differentiation, Clinical Biochemistry, Cell, Cell Biology, Molecular biology, Insulin-like growth factor-binding protein, medicine.anatomical_structure, medicine, biology.protein, Northern blot, Autocrine signalling, Fetal bovine serum

Abstract

The components of the insulin-like growth factor (IGF) axis and their roles in regulating proliferation and differentiation of the human colon adenocarcinoma cell line, Caco-2, have been investigated. Caco-2 cells proliferated in serum-free medium at 75% the rate observed in medium containing 10% fetal bovine serum. IGF-I (10 nM) increased Caco-2 cell growth in serum-free medium, but not to the rate seen with serum. Multiple IGF-II mRNA species were produced by Caco-2 cells, but IGF-I mRNA was undetectable. Secretion of radioimmunoassayable IGF-II corresponded with steady-state levels of IGF-II mRNA, neither of which was observed to change markedly over the course of 16 days of Caco-2 cell differentiation. Levels of sucrase-isomaltase mRNA, a marker for enterocytic differentiation, increased 12-fold between days 5 and 16 of culture. Northern blotting of total RNA and ligand blot and immunoblot analyses of serum-free conditioned medium revealed that Caco-2 cells produce several IGF binding proteins (IGFBPs), including IGFBP-2, -3, and -4, as well as a 31,000 M(r) species that was not identified. The pattern of IGFBP secretion changed dramatically during Caco-2 cell differentiation: IGFBP-3 and IGFBP-2 increased 8.5-fold and 5-fold, respectively, whereas IGFBP-4 and the 31,000 M(r) species decreased 43% and 90%. Caco-2 cell clones stably transfected with a human IGFBP-4 cDNA construct exhibited a 60% increase in steady-state level of IGFBP-4 mRNA, and secreted twice as much IGFBP-4 protein as controls. Moreover, IGFBP-4-overexpressing cells proliferated at only 25% the rate of control cells in serum-free medium, in conjunction with a 70% increase in expression of sucrase-isomaltase. In summary, these studies indicate that a complex IGF axis is involved in autocrine regulation of Caco-2 cell proliferation and differentiation.

Published

1996

22. Truncated forms of the insulin-like growth factor II (IGF-II)/mannose 6-phosphate receptor encompassing the IGF-II binding site: characterization of a point mutation that abolishes IGF-II binding

Author

Dorothy H. Slentz, Farideh Garmroudi, Gayathri R. Devi, Richard G. MacDonald, and Beverly S. Schaffer

Subjects

Immunoprecipitation, Mannose 6-phosphate, Biology, Receptor, IGF Type 2, Substrate Specificity, Iodine Radioisotopes, chemistry.chemical_compound, Endocrinology, Insulin-Like Growth Factor II, Animals, Humans, Binding site, Receptor, Molecular Biology, Repetitive Sequences, Nucleic Acid, Mannose 6-phosphate receptor, Binding Sites, Point mutation, General Medicine, Molecular biology, Precipitin Tests, Recombinant Proteins, Cross-Linking Reagents, chemistry, Mutation, Mutation testing, Binding domain

Abstract

Complete understanding of the functional significance of insulin-like growth factor II (IGF-II) binding by the IGF-II/mannose-6-phosphate (Man-6-P) receptor requires mapping and ultimately mutational analysis of the receptor's IGF-II binding domain. Recent advances have localized the IGF-II binding site to extracytoplasmic repeats 10-11. To improve resolution of the binding site map, a nested set of epitope-tagged, truncated forms of the human IGF-II/Man-6-P receptor were transiently expressed in COS-7 cells. The IGF-II binding properties of truncated receptors immunoprecipitated from cell lysates and conditioned media were determined by affinity cross-linking. From the largest truncated receptor, encompassing extracytoplasmic repeats 8-11 (M(r) 68 K), through the smallest, comprised primarily of repeat 11 (M(r) 23 K), all were able to bind and cross-link to IGF-II. As a group, the truncated receptors had similar affinities for IGF-II, but with relative binding affinities 5-to 10-fold lower than those of full-length receptors. A point mutation substituting threonine for isoleucine at residue 1572, located in the NH2-terminal half of repeat 11, completely abolished IGF-II binding. We conclude that repeat 11 of the IGF-II/Man-6-P receptor's extracytoplasmic domain contains the minimal elements required for binding and cross-linking to IGF-II, and that lle1572 and other residues within the NH2-terminal half of repeat 11 are particularly important for IGF-II interaction.

Published

1996

23. Growth stimulation by transfection of intestinal epithelial cells with an antisense insulin-like growth factor binding protein-2 construct

Author

Jung H.Y. Park, Jon A. Vanderhoof, Mark R. Corkins, Richard G. MacDonald, and Dorothy H. Slentz

Subjects

Cell division, medicine.medical_treatment, Biophysics, Endogeny, Transfection, Biochemistry, Insulin-like growth factor-binding protein, DNA, Antisense, Epithelium, Insulin-Like Growth Factor II, Somatomedins, medicine, Animals, RNA, Messenger, Molecular Biology, Cells, Cultured, Messenger RNA, Expression vector, biology, DNA synthesis, Growth factor, Epithelial Cells, Cell Biology, Molecular biology, Cell biology, Rats, Intestines, Insulin-Like Growth Factor Binding Protein 2, biology.protein, Carrier Proteins, Cell Division

Abstract

IEC-6 cells, an intestinal epithelial cell line, produce insulin-like growth factor (IGF)-II and IGF-binding protein-2 (IGFBP-2). Exogenous IGFs stimulate and IGFBP-2 attenuates DNA synthesis. To investigate whether endogenously secreted IGFBP-2 inhibits proliferation, IEC-6 cells were transfected with a full-length rat IGFBP-2 cDNA antisense expression construct. The steady-state level of IGFBP-2 mRNA decreased by 54% in the antisense cDNA-transfected cells (denoted revBP2) compared with vector-transfected controls. Moreover, revBP2 cells secreted less IGFBP-2 than controls (maximally a 68% decrease). In serum-containing medium, revBP2 cells exhibited a 35% increase in log-phase proliferation rate and growth-arrested at a maximum density 14% higher than controls. We conclude that endogenous IGFBP-2 inhibits proliferation of IEC-6 cells, probably by sequestering IGFs.

Published

1995

24. EFFECTS OF CHRONIC EXPOSURE TO SIMULATED MICROGRAVITY ON SKELETAL MUSCLE CELL PROLIFERATION AND DIFFERENTIATION

Author

William E. Kraus, George A. Truskey, and Dorothy H. Slentz

Subjects

Cellular differentiation, Skeletal muscle, Cell Biology, General Medicine, Cell cycle, Biology, Cell biology, medicine.anatomical_structure, Cell culture, Skeletal muscle cell proliferation, Myosin, medicine, Myocyte, Stem cell, Developmental Biology

Abstract

Cell culture models that mimic long-term exposure to microgravity provide important insights into the cellular biological adaptations of human skeletal muscle to long-term residence in space. We developed insert scaffolding for the NASA-designed rotating cell culture system (RCCS) in order to study the effects of time-averaged microgravity on the proliferation and differentiation of anchorage-dependent skeletal muscle myocytes. We hypothesized that prolonged microgravity exposure would result in the retardation of myocyte differentiation. Microgravity exposure in the RCCS resulted in increased cellular proliferation. Despite shifting to media conditions promoting cellular differentiation, 5 d later, there was an increase in cell number of approximately 62%, increases in total cellular protein (52%), and cellular proliferating cell nuclear antigen (PCNA) content (2.7 times control), and only a modest (insignificant) decrease (10%) in sarcomeric myosin protein expression. We grew cells in an inverted orientation on membrane inserts. Changes in cell number and PCNA content were the converse to those observed for cells in the RCCS. We also grew cells on inserts at unit gravity with constant mixing. Mixing accounted for part, but not all, of the effects of microgravity exposure on skeletal muscle cell cultures (53% of the RCCS effect on PCNA at 4–6 d). In summary, the mechanical effects of simulated microgravity exposure in the RCCS resulted in the maintenance of cellular proliferation, manifested as increases in cell number and expression of PCNA relative to control conditions, with only a modest reciprocal inhibition of cellular differentiation. Therefore, this model provides conditions wherein cellular differentiation and proliferation appear to be uncoupled.

Published

2001

25. OVEREXPRESSION OF INSULIN-LIKE GROWTH FACTOR BINDING PROTEIN (IGFBP)-4 RESULTS IN INCREASED PROLIFERATION RATE AND MUC3 EXPRESSION

Author

M A Hollingsworth, Richard G. MacDonald, Jon A. Vanderhoof, Dorothy H. Slentz, Mac k, and Mark R. Corkins

Subjects

biology, business.industry, Proliferation rate, Pediatrics, Perinatology and Child Health, Gastroenterology, biology.protein, Medicine, business, Insulin-like growth factor-binding protein, Cell biology

Published

1995

26. 10 STIMULATION OF CELL PROLIFERATION BY EXPRESSION OF A REVERSE INSULIN-LIKE GROWTH FACTOR BINDING PROTEIN-2 (IGFBP-2) CONSTRUCT IN INTESTINAL EPITHELIAL CELLS (IEC-6)

Author

Richard G. MacDonald, Jung H.Y. Park, Dorothy H. Slentz, Jon A. Vanderhoof, Mark R. Corkins, and R. M. Caruso

Subjects

biology, Cell growth, business.industry, Pediatrics, Perinatology and Child Health, Gastroenterology, biology.protein, Medicine, Stimulation, business, Insulin-like growth factor-binding protein, Cell biology

Published

1994

27. Metabolomic Quantitative Trait Loci (mQTL) Mapping Implicates the Ubiquitin Proteasome System in Cardiovascular Disease Pathogenesis.

Author

William E Kraus, Deborah M Muoio, Robert Stevens, Damian Craig, James R Bain, Elizabeth Grass, Carol Haynes, Lydia Kwee, Xuejun Qin, Dorothy H Slentz, Deidre Krupp, Michael Muehlbauer, Elizabeth R Hauser, Simon G Gregory, Christopher B Newgard, and Svati H Shah

Subjects

Genetics, QH426-470

Abstract

Levels of certain circulating short-chain dicarboxylacylcarnitine (SCDA), long-chain dicarboxylacylcarnitine (LCDA) and medium chain acylcarnitine (MCA) metabolites are heritable and predict cardiovascular disease (CVD) events. Little is known about the biological pathways that influence levels of most of these metabolites. Here, we analyzed genetics, epigenetics, and transcriptomics with metabolomics in samples from a large CVD cohort to identify novel genetic markers for CVD and to better understand the role of metabolites in CVD pathogenesis. Using genomewide association in the CATHGEN cohort (N = 1490), we observed associations of several metabolites with genetic loci. Our strongest findings were for SCDA metabolite levels with variants in genes that regulate components of endoplasmic reticulum (ER) stress (USP3, HERC1, STIM1, SEL1L, FBXO25, SUGT1) These findings were validated in a second cohort of CATHGEN subjects (N = 2022, combined p = 8.4x10-6-2.3x10-10). Importantly, variants in these genes independently predicted CVD events. Association of genomewide methylation profiles with SCDA metabolites identified two ER stress genes as differentially methylated (BRSK2 and HOOK2). Expression quantitative trait loci (eQTL) pathway analyses driven by gene variants and SCDA metabolites corroborated perturbations in ER stress and highlighted the ubiquitin proteasome system (UPS) arm. Moreover, culture of human kidney cells in the presence of levels of fatty acids found in individuals with cardiometabolic disease, induced accumulation of SCDA metabolites in parallel with increases in the ER stress marker BiP. Thus, our integrative strategy implicates the UPS arm of the ER stress pathway in CVD pathogenesis, and identifies novel genetic loci associated with CVD event risk.

Published

2015