Your search keyword '"Vadivel Ganapathy"' showing total 618 results

101. Hydroxyurea differentially modulates activator and repressors of γ-globin gene in erythroblasts of responsive and non-responsive patients with sickle cell disease in correlation with Index of Hydroxyurea Responsiveness

Author

Vadivel Ganapathy, Hongyan Xu, Wenhu Pi, Yongchao Wang, Meng Hsuan Ho, Abdullah Kutlar, Ferdane Kutlar, Xingguo Zhu, Dorothy Tuan, Jeong Hyeon Choi, Tianxiang Hu, Niren Patel, and Miao Yu

Subjects

0301 basic medicine, medicine.medical_specialty, Erythroblasts, Anemia, Sickle Cell, Biology, Article, 03 medical and health sciences, Transcription (biology), hemic and lymphatic diseases, Internal medicine, Fetal hemoglobin, medicine, Humans, Hydroxyurea, gamma-Globins, MYB, RNA, Messenger, Red Cell Biology & its Disorders, Gene, Transcription factor, Cells, Cultured, Fetal Hemoglobin, Regulation of gene expression, Activator (genetics), RNA, Hematology, Molecular biology, 3. Good health, 030104 developmental biology, Endocrinology, Gene Expression Regulation, Transcription Factors

Abstract

Hydroxyurea (HU), the first of two drugs approved by the US Food and Drug Administration for treating patients with sickle cell disease (SCD), produces anti-sickling effect by re-activating fetal γ-globin gene to enhance production of fetal hemoglobin. However, approximately 30% of the patients do not respond to HU therapy. The molecular basis of non-responsiveness to HU is not clearly understood. To address this question, we examined HU-induced changes in the RNA and protein levels of transcription factors NF-Y, GATA-1, -2, BCL11A, TR4, MYB and NF-E4 that assemble the γ-globin promoter complex and regulate transcription of γ-globin gene. In erythroblasts cultured from peripheral blood CD34+ cells of patients with SCD, we found that HU-induced changes in the protein but not the RNA levels of activator GATA-2 and repressors GATA-1, BCL11A and TR4 correlated with HU-induced changes in fetal hemoglobin (HbF) levels in the peripheral blood of HU high and low responders. However, HU did not significantly induce changes in the protein or RNA levels of activators NF-Y and NF-E4. Based on HU-induced changes in the protein levels of GATA-2, -1 and BCL11A, we calculated an Index of Hydroxyurea Responsiveness (IndexHU-3). Compared to the HU-induced fold changes in the individual transcription factor protein levels, the numerical values of IndexHU-3 statistically correlated best with the HU-induced peripheral blood HbF levels of the patients. Thus, IndexHU-3 can serve as an appropriate indicator for inherent HU responsiveness of patients with SCD.

Published

2017

102. Gut Microbiome and Colon Cancer: Role of Bacterial Metabolites and Their Molecular Targets in the Host

Author

Jiro Ogura, Yangzom D. Bhutia, Vadivel Ganapathy, and Sathish Sivaprakasam

Subjects

0301 basic medicine, Hepatology, Gastroenterology, Inflammation, Biology, medicine.disease_cause, Article, 03 medical and health sciences, 030104 developmental biology, Histone, Immune system, Oncology, Nuclear receptor, Biochemistry, DNA methylation, medicine, biology.protein, Epigenetics, medicine.symptom, Signal transduction, Carcinogenesis

Abstract

The relationship between colonic bacteria and the host is symbiotic, but how communication between the two partners occurs is just beginning to be understood at the molecular level. Here, we highlight specific products of bacterial metabolism that are present in the colonic lumen and their molecular targets in the host that facilitate this communication. Colonic epithelial cells and mucosal immune cells express several cell surface receptors and nuclear receptors that are activated by specific bacterial metabolites, which impact multiple signaling pathways and expression of many genes. In addition, some bacterial metabolites also possess the ability to cause epigenetic changes in these cells via inhibition of selective enzymes involved in the maintenance of histone acetylation and DNA methylation patterns. Colonic bacteria communicate with their host with selective metabolites that interact with host molecular targets. This chemical communication underlies a broad range of the biology and function of colonic epithelial cells and mucosal immune cells, which protect against inflammation and carcinogenesis in the colon under normal physiological conditions.

Published

2017

103. Embryonic lethality in mice due to carnitine transporter OCTN2 defect and placental carnitine deficiency

Author

Vadivel Ganapathy, Srinivas Sonne, Prem S. Shekhawat, and Dietrich Matern

Subjects

0301 basic medicine, medicine.medical_specialty, Placenta, Mutation, Missense, Embryonic Development, Mitochondrion, SLC22A5, Mice, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Carnitine, Internal medicine, medicine, Animals, Solute Carrier Family 22 Member 5, biology, Chemistry, Obstetrics and Gynecology, Trophoblast, Biological Transport, Transporter, Embryonic stem cell, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Reproductive Medicine, biology.protein, Female, 030217 neurology & neurosurgery, Developmental Biology, medicine.drug, Transforming growth factor

Abstract

l-Carnitine plays a crucial role in uptake and subsequent β-oxidation of long-chain fatty acids in the mitochondria. Placental trophoblast cells oxidize long-chain fatty acids for energy production. Here we present data showing that l-carnitine deficiency due to a defect in the carnitine transporter OCTN2 (SLC22A5) in a mouse model leads to embryonic lethality. Placental levels of l-carnitine are reduced to10% of normal and deficiency of l-carnitine is associated with markedly reduced expression of several growth factors and transforming growth factor β (TGF-β) genes. This report links for the first time reduced l-carnitine levels in the placenta to embryonic lethality.

Published

2018

104. Rescue of mutant gonadotropin-releasing hormone receptor function independent of cognate receptor activity

Author

Jo Ann Janovick, Louis Scampavia, Thomas D. Bannister, Timothy P. Spicer, Justin Shumate, Emery Smith, and Vadivel Ganapathy

Subjects

0301 basic medicine, Agonist, Protein Folding, Cell biology, medicine.drug_class, Inositol Phosphates, Mutant, Drug Evaluation, Preclinical, lcsh:Medicine, 01 natural sciences, Article, Gonadotropin-Releasing Hormone, Small Molecule Libraries, 03 medical and health sciences, Hypogonadotropic hypogonadism, medicine, Humans, Receptor, Inositol phosphate, lcsh:Science, chemistry.chemical_classification, Multidisciplinary, Protein transport, Chemistry, GNRHR, lcsh:R, medicine.disease, 0104 chemical sciences, High-Throughput Screening Assays, 010404 medicinal & biomolecular chemistry, 030104 developmental biology, Hormone receptor, Mutation, lcsh:Q, Calcium, Gonadotropin-releasing hormone receptor, Receptors, LHRH, HeLa Cells, Cell signalling

Abstract

Molecules that correct the folding of protein mutants, restoring their functional trafficking, are called pharmacoperones. Most are clinically irrelevant and possess intrinsic antagonist or agonist activity. Here, we identify compounds capable of rescuing the activity of mutant gonadotropin-releasing hormone receptor or GnRHR which, is sequestered within the cell and if dysfunctional leads to Hypogonadotropic Hypogonadism. To do this we screened the E90K GnRHR mutant vs. a library of 645,000 compounds using a cell-based calcium detection system. Ultimately, we identified 399 compounds with EC50 ≤ 5 µM with no effect in counterscreen assays. Medicinal chemistry efforts confirmed activity of 70 pure samples and mode of action studies, including radioligand binding, inositol phosphate, and toxicity assays, proved that we have a series of tractable compounds that can be categorized into structural clusters. These early lead molecules rescue mutant GnRHR function and are neither agonist nor antagonists of the GnRHR cognate receptor, a feature required for potential clinical utility.

Published

2019

105. Lactate/GPR81 signaling and proton motive force in cancer: Role in angiogenesis, immune escape, nutrition, and Warburg phenomenon

Author

Vadivel Ganapathy and Timothy P. Brown

Subjects

0301 basic medicine, Angiogenesis, GPR81, Receptors, G-Protein-Coupled, 03 medical and health sciences, Paracrine signalling, 0302 clinical medicine, Immune system, Cancer-Associated Fibroblasts, Neoplasms, medicine, Animals, Humans, Pharmacology (medical), Lactic Acid, Autocrine signalling, Pharmacology, Tumor microenvironment, Neovascularization, Pathologic, Chemistry, Cancer, Membrane Transport Proteins, Proton-Motive Force, medicine.disease, Cell biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, Signal Transduction

Abstract

Reprogramming of biochemical pathways is a hallmark of cancer cells, and generation of lactic acid from glucose/glutamine represents one of the consequences of such metabolic alterations. Cancer cells export lactic acid out to prevent intracellular acidification, not only increasing lactate levels but also creating an acidic pH in extracellular milieu. Lactate and protons in tumor microenvironment are not innocuous bystander metabolites but have special roles in promoting tumor-cell proliferation and growth. Lactate functions as a signaling molecule by serving as an agonist for the G-protein-coupled receptor GPR81, involving both autocrine and paracrine mechanisms. In the autocrine pathway, cancer cell-generated lactate activates GPR81 on cancer cells; in the paracrine pathway, cancer cell-generated lactate activates GPR81 on immune cells, endothelial cells, and adipocytes present in tumor stroma. The end result of GPR81 activation is promotion of angiogenesis, immune evasion, and chemoresistance. The acidic pH creates an inwardly directed proton gradient across the cancer-cell plasma membrane, which provides driving force for proton-coupled transporters in cancer cells to enhance supply of selective nutrients. There are several molecular targets in the pathways involved in the generation of lactic acid by cancer cells and its role in tumor promotion for potential development of novel anticancer therapeutics.

Published

2019

106. Renal iron accelerates the progression of diabetic nephropathy in the HFE gene knockout mouse model of iron overload

Author

Vadivel Ganapathy, Sudha Ananth, Rajalakshmi Veeranan-Karmegam, Kapil Chaudhary, Ashok Mandala, Aruna Chilakala, Folami L. Powell, and Jaya P. Gnana-Prakasam

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Iron Overload, Physiology, Diabetic rat, Iron, Hfe gene, Disease, Iron Chelating Agents, Kidney, Diabetes Mellitus, Experimental, Diabetic nephropathy, Renin-Angiotensin System, 03 medical and health sciences, Mice, 0302 clinical medicine, Internal medicine, Renin–angiotensin system, Renin, Medicine, Animals, Deferiprone, Diabetic Nephropathies, Hemochromatosis Protein, Hemochromatosis, Mice, Knockout, business.industry, High mortality, medicine.disease, 030104 developmental biology, Endocrinology, Knockout mouse, Disease Progression, 030211 gastroenterology & hepatology, business

Abstract

Diabetic nephropathy (DN) is the most common cause of end-stage renal disease associated with high mortality worldwide. Increases in iron levels have been reported in diabetic rat kidneys as well as in human urine of patients with diabetes. In addition, a low-iron diet or iron chelators delay the progression of DN in patients with diabetes and in animal models of diabetes. Possible maladaptive mechanisms of organ damage by tissue iron accumulation have not been well studied. We recently reported that iron induced the retinal renin-angiotensin system (RAS) and accelerated the progression of diabetic retinopathy. However, whether iron regulates the systemic RAS is unknown. To explore if iron alters the expression of intrarenal RAS and its role in the progression of DN, we used the high Fe iron (HFE) knockout mouse, a genetic model of systemic iron overload. We found that diabetes upregulated the expression of iron regulatory proteins and augmented tissue iron accumulation in the kidneys of both type 1 and type 2 diabetic mouse models. Iron accumulation in the kidneys of HFE knockout mice was associated with increase in serum and intrarenal renin expression. Induction of diabetes in HFE knockout mice using streptozotocin caused a much higher accumulation of renal iron and accelerated the progression of nephropathy compared with diabetic wild-type mice. Treatment of diabetic mice with the iron chelator deferiprone reversed the renin upregulation and reduced kidney injury. Thus, our results establish a new link between renal iron and RAS activity. Exploring the mechanisms of iron-induced RAS activation further may have a significant therapeutic impact on hypertension and DN.

Published

2019

107. Transport Mechanisms for the Nutritional Supplement β-Hydroxy-β-Methylbutyrate (HMB) in Mammalian Cells

Author

Yangzom D. Bhutia, Kei Higuchi, Vadivel Ganapathy, Seiji Miyauchi, Suzette L. Pereira, Ricardo Rueda, Masayuki Masuda, Toshihiro Sato, Jiro Ogura, and Ellappan Babu

Subjects

Monocarboxylic Acid Transporters, Anabolism, Pharmaceutical Science, 02 engineering and technology, 030226 pharmacology & pharmacy, Cell Line, 03 medical and health sciences, Mice, Xenopus laevis, 0302 clinical medicine, Valerates, Gene silencing, Myocyte, Animals, Humans, Pharmacology (medical), Gene Silencing, Lactic Acid, RNA, Small Interfering, skin and connective tissue diseases, Pharmacology, Monocarboxylate transporter, Muscle Cells, biology, Chemistry, Organic Chemistry, Sodium, Transporter, Biological Transport, Epithelial Cells, 021001 nanoscience & nanotechnology, Molecular biology, Cell culture, Dietary Supplements, biology.protein, MCF-7 Cells, Molecular Medicine, Signal transduction, 0210 nano-technology, human activities, C2C12, Biotechnology, Signal Transduction

Abstract

β-Hydroxy-β-methylbutyrate (HMB), a nutritional supplement, elicits anabolic activity in muscle. Here we investigated the mechanism of HMB uptake in muscle cells. Murine muscle cells (C2C12) and human mammary epithelial cells (MCF7) were used for uptake. As HMB is a monocarboxylate, focus was on monocarboxylate transporters, monitoring interaction of HMB with H+-coupled lactate uptake, and influence of H+ directly on HMB uptake. Involvement of MCT1–4 was studied using selective inhibitors and gene silencing. Involvement of human Na+/monocarboxylate transporter SMCT1 was also assessed using Xenopus oocytes. H+-coupled lactate uptake was inhibited by HMB in both mammalian cells. HMB uptake was H+-coupled and inhibited by lactate. C2C12 cells expressed MCT1 and MCT4; MCF7 cells expressed MCT1–4; undifferentiated C2C12 cells expressed SMCT1. SMCT1 mediated Na+-coupled HMB transport. Inhibitors of MCT1/4, siRNA-mediated gene silencing, and expression pattern showed that MCT1–4 were responsible only for a small portion of HMB uptake in these cells. HMB uptake in C2C12 and MCF7 cells is primarily H+-coupled and inhibited by lactate, but MCT1–4 are only partly responsible for HMB uptake. SMCT1 also transports HMB, but in a Na+-coupled manner. Other, yet unidentified, transporters mediate the major portion of HMB uptake in C2C12 and MCF7 cells.

Published

2019

108. Development and radiosynthesis of the first

Author

Masoud, Sadeghzadeh, Rareş-Petru, Moldovan, Steffen, Fischer, Barbara, Wenzel, Friedrich-Alexander, Ludwig, Rodrigo, Teodoro, Winnie, Deuther-Conrad, Shirisha, Jonnalagadda, Sravan K, Jonnalagadda, Emilis, Gudelis, Algirdas, Šačkus, Kei, Higuchi, Vadivel, Ganapathy, Venkatram R, Mereddy, Lester R, Drewes, and Peter, Brust

Subjects

Monocarboxylic Acid Transporters, Fluorine Radioisotopes, Mice, Radiochemistry, Acrylates, Symporters, Cell Line, Tumor, Isotope Labeling, Animals, Humans, Muscle Proteins, Chemistry Techniques, Synthetic

Abstract

Monocarboxylate transporters 1 and 4 (MCT1 and MCT4) are involved in tumor development and progression. Their expression levels are related to clinical disease prognosis. Accordingly, both MCTs are promising drug targets for treatment of a variety of human cancers. The noninvasive imaging of these MCTs in cancers is regarded to be advantageous for assessing MCT-mediated effects on chemotherapy and radiosensitization using specific MCT inhibitors. Herein, we describe a method for the radiosynthesis of [

Published

2019

109. Structural Insights and Classification of the Disease-Causing Mutations in Human Na+- Coupled Citrate Transporter (NACT) using a Homology Modeling Approach

Author

Valeria Jaramillo-Martinez, Vadivel Ganapathy, and Ina L. Urbatsch

Subjects

Chemistry, Citrate transporter, Biophysics, Homology modeling, Disease, Computational biology

Published

2021

110. Oral Monomethyl Fumarate Therapy Ameliorates Retinopathy in a Humanized Mouse Model of Sickle Cell Disease

Author

Manuela Bartoli, Alan Saul, Wanwisa Promsote, Diana Gutsaeva, Sylvia B. Smith, Pamela M. Martin, Shanu Markand, Folami L. Powell, Vadivel Ganapathy, Menaka Thounaojam, and Satyam Veean

Subjects

Vascular Endothelial Growth Factor A, 0301 basic medicine, Physiology, Clinical Biochemistry, Cell, Administration, Oral, Gene Expression, Retinal Pigment Epithelium, medicine.disease_cause, Biochemistry, Mice, chemistry.chemical_compound, 0302 clinical medicine, Fumarates, Oral administration, Blood-Retinal Barrier, General Environmental Science, Neovascularization, Pathologic, Nuclear Proteins, Intercellular Adhesion Molecule-1, DNA-Binding Proteins, Original Research Communications, medicine.anatomical_structure, medicine.symptom, Retinal Neurons, Retinopathy, NF-E2-Related Factor 2, Inflammation, Anemia, Sickle Cell, Retina, 03 medical and health sciences, Retinal Diseases, In vivo, Electroretinography, medicine, Animals, Humans, Molecular Biology, business.industry, Retinal, Cell Biology, medicine.disease, Repressor Proteins, Disease Models, Animal, Oxidative Stress, 030104 developmental biology, Gene Expression Regulation, chemistry, Immunology, Humanized mouse, 030221 ophthalmology & optometry, General Earth and Planetary Sciences, gamma-Globulins, Carrier Proteins, business, Oxidative stress

Abstract

Sickle retinopathy (SR) is a major cause of blindness in sickle cell disease (SCD). The genetic mutation responsible for SCD is known, however; oxidative stress and inflammation also figure prominently in the development and progression of pathology. Development of therapies for SR is hampered by the lack of (a) animal models that accurately recapitulate human SR and (b) strategies for noninvasive yet effective retinal drug delivery. This study addressed both issues by validating the Townes humanized SCD mouse as a model of SR and demonstrating the efficacy of oral administration of the antioxidant fumaric acid ester monomethyl fumarate (MMF) in the disease.In vivo ophthalmic imaging, electroretinography, and postmortem histological RNA and protein analyses were used to monitor retinal health and function in normal (HbAA) and sickle (HbSS) hemoglobin-producing mice over a one-year period and in additional HbAA and HbSS mice treated with MMF (15 mg/ml) for 5 months. Functional and morphological abnormalities and molecular hallmarks of oxidative stress/inflammation were evident early in HbSS retinas and increased in number and severity with age. Treatment with MMF, a known inducer of Nrf2, induced γ-globin expression and fetal hemoglobin production, improved hematological profiles, and ameliorated SR-related pathology. Innovation and Conclusion: United States Food and Drug Administration-approved formulations in which MMF is the primary bioactive ingredient are currently available to treat multiple sclerosis; such drugs may be effective for treatment of ocular and systemic complications of SCD, and given the pleiotropic effects, other nonsickle-related diseases in which oxidative stress, inflammation, and retinal vascular pathology figure prominently. Antioxid. Redox Signal. 25, 921-935.

Published

2016

111. Amino acid transporter SLC6A14 is a novel and effective drug target for pancreatic cancer

Author

Vadivel Ganapathy, Sha Cao, Shengping Yang, Yangzom D. Bhutia, C. P. Reynolds, Ying Xu, Puttur D. Prasad, Jiro Ogura, Veena Coothankandaswamy, and Pankaj K. Singh

Subjects

0301 basic medicine, Pharmacology, chemistry.chemical_classification, Transporter, Biology, medicine.disease, In vitro, Amino acid, 03 medical and health sciences, 030104 developmental biology, chemistry, In vivo, Cell culture, Pancreatic cancer, Cancer cell, medicine, Amino acid transporter

Abstract

Background and Purpose Pancreatic cancer is a solid tumour that is often fatal. Hence, there is an urgent need to identify new drug targets for this disease. Highly proliferating cancer cells have an increased demand for nutrients and, therefore, need to up-regulate selective amino acid transporters. Here, we investigated which amino acid transporters are up-regulated in pancreatic cancer and whether any of these transporters has potential as a drug target for this fatal disease. Experimental Approach The expression of amino acid transporters in pancreatic cancer was analysed using publicly available microarray datasets, and the findings with the transporter SLC6A14 were validated by mRNA and protein analysis. The potential of SLC6A14 as a drug target was evaluated using a pharmacological blocker in vitro and in vivo. Key Results SLC6A14 was up-regulated several fold in patient-derived xenografts, primary tumour tissues and pancreatic cancer cells lines compared to normal pancreatic tissue or normal pancreatic epithelial cells. The magnitude of the up-regulation of SLC6A14 was the highest among the amino acid transporters examined. A pharmacological blocker of SLC6A14, α-methyltryptophan, induced amino acid starvation in pancreatic cancer cells and reduced the growth and proliferation of these cells, both in vitro and in vivo. Conclusion and Implications The salient features of this study are that SLC6A14 is markedly up-regulated in pancreatic cancer and that pharmacological blockade of this transporter interferes with amino acid nutrition and reduces growth and proliferation of pancreatic cancer cells. These findings identify SLC6A14 as a novel druggable target for pancreatic cancer.

Published

2016

112. Glutamine transporters in mammalian cells and their functions in physiology and cancer

Author

Vadivel Ganapathy and Yangzom D. Bhutia

Subjects

0301 basic medicine, Glutamine, Biological Transport, Active, Biology, Article, Substrate Specificity, Mice, 03 medical and health sciences, Neoplasms, Animals, Humans, Molecular Targeted Therapy, Molecular Biology, Peptide sequence, Mammals, Mice, Knockout, chemistry.chemical_classification, Cell Membrane, Protein primary structure, Transporter, Cell Biology, Neoplasm Proteins, Solute carrier family, Amino acid, 030104 developmental biology, chemistry, Biochemistry, Multigene Family, Efflux, Carrier Proteins, Metabolism, Inborn Errors, Function (biology)

Abstract

The SLC (solute carrier)-type transporters (~ 400 in number) in mammalian cells consist of 52 distinct gene families, grouped solely based on the amino acid sequence (primary structure) of the transporter proteins and not on their transport function. Among them are the transporters for amino acids. Fourteen of them, capable of transporting glutamine across the plasma membrane, are found in four families: SLC1, SLC6, SLC7, and SLC38. However, it is generally thought that the members of the SLC38 family are the principal transporters for glutamine. Some of the glutamine transporters are obligatory exchangers whereas some function as active transporters in one direction. While most glutamine transporters mediate the influx of the amino acid into cells, some actually mediate the efflux of the amino acid out of the cells. Glutamine transporters play important roles in a variety of tissues, including the liver, brain, kidney, and placenta, as clearly evident from the biological and biochemical phenotypes resulting from the deletion of specific glutamine transporters in mice. Owing to the obligatory role of glutamine in growth and proliferation of tumor cells, there is increasing attention on glutamine transporters in cancer biology as potential drug targets for cancer treatment. Selective blockers of certain glutamine transporters might be effective in preventing the entry of glutamine and other important amino acids into tumor cells, thus essentially starving these cells to death. This could represent the beginning of a new era in the discovery of novel anticancer drugs with a previously unexplored mode of action. This article is part of a Special Issue entitled: Mitochondrial Channels edited by Pierre Sonveaux, Pierre Maechler and Jean-Claude Martinou.

Published

2016

113. Re-programming tumour cell metabolism to treat cancer: no lone target for lonidamine

Author

Vadivel Ganapathy, Ellappan Babu, and Yangzom D. Bhutia

Subjects

0301 basic medicine, Indazoles, Antineoplastic Agents, pyruvate carrier, Pharmacology, Biology, Mitochondrion, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Commentaries, Neoplasms, lonidamine, medicine, Humans, Glycolysis, Molecular Biology, monocarboxylate transporters, hexokinase II, Lonidamine, Cancer, Cell Biology, medicine.disease, 3. Good health, 030104 developmental biology, Cell metabolism, chemistry, Mitochondrial permeability transition pore, Cancer cell, Cancer research, Commentary, Signal transduction, metabolism, Signal Transduction

Abstract

Tumour cell metabolism is very different from normal cell metabolism; cancer cells re-programme the metabolic pathways that occur in normal cells in such a manner that it optimizes their proliferation, growth and survival. Although this metabolic re-programming obviously operates to the advantage of the tumour, it also offers unique opportunities for effective cancer therapy. Molecules that target the tumour cell-specific metabolic pathways have potential as novel anti-cancer drugs. Lonidamine belongs to this group of molecules and is already in use in some countries for cancer treatment. It has been known for a long time that lonidamine interferes with energy production in tumour cells by inhibiting hexokinase II (HKII), a glycolytic enzyme. However, subsequent studies have uncovered additional pharmacological targets for the drug, which include the electron transport chain and the mitochondrial permeability transition pore, thus expanding the pharmacological effects of the drug on tumour cell metabolism. A study by Nancolas et al. in a recent issue of the Biochemical Journal identifies two additional new targets for lonidamine: the pyruvate transporter in the mitochondria and the H+-coupled monocarboxylate transporters in the plasma membrane (PM). It is thus becoming increasingly apparent that the anti-cancer effects of lonidamine do not occur through a single target; the drug works at multiple sites. Irrespective of the molecular targets, what lonidamine does in the end is to undo what the tumour cells have done in terms of re-programming cellular metabolism and mitochondrial function.

Published

2016

114. Increased Retinal Expression of the Pro-Angiogenic Receptor GPR91 via BMP6 in a Mouse Model of Juvenile Hemochromatosis

Author

Mariappan Gurusamy, Pachiappan Arjunan, Muthusamy Thangaraju, Veeranan Karmegam Rajalakshmi, Puttur D. Prasad, Jaya P. Gnana-Prakasam, Michelle A. Romej, Sudha Ananth, Vadivel Ganapathy, Yangzom D. Bhutia, and Pamela M. Martin

Subjects

0301 basic medicine, medicine.medical_specialty, Chromatin Immunoprecipitation, Bone Morphogenetic Protein 6, BMP6 signaling, Blotting, Western, retinal pigment epithelium, Biology, Bone morphogenetic protein, Real-Time Polymerase Chain Reaction, Retina, Cell Line, Receptors, G-Protein-Coupled, 03 medical and health sciences, Mice, Downregulation and upregulation, Internal medicine, succinate receptor-GPR91, medicine, Animals, Humans, Fluorescent Antibody Technique, Indirect, age-related macular degeneration, Hemojuvelin, Regulation of gene expression, juvenile hemochromatosis, Mice, Knockout, Retinal pigment epithelium, Reverse Transcriptase Polymerase Chain Reaction, medicine.disease, Juvenile hemochromatosis, eye diseases, Cell biology, Up-Regulation, Bone morphogenetic protein 6, Disease Models, Animal, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Retinal Cell Biology, Gene Expression Regulation, RNA, sense organs, Hemochromatosis, Signal transduction, Signal Transduction

Abstract

Purpose Hemochromatosis, an iron-overload disease, occurs as adult and juvenile types. Mutations in hemojuvelin (HJV), an iron-regulatory protein and a bone morphogenetic protein (BMP) coreceptor, underlie most of the juvenile type. Hjv(-/-) mice accumulate excess iron in retina and exhibit aberrant vascularization and angiomas. A succinate receptor, GPR91, is pro-angiogenic in retina. We hypothesized that Hjv(-/-) retinas have increased BMP signaling and increased GPR91 expression as the basis of angiomas. Methods Expression of GPR91 was examined by qPCR, immunofluorescence, and Western blot in wild-type and Hjv(-/-) mouse retinas and pRPE cells. Influence of excess iron and BMP6 on GPR91 expression was investigated in ARPE-19 cells, and wild-type and Hjv(-/-) pRPE cells. Succinate was used to activate GPR91 and determine the effects of GPR91 signaling on VEGF expression. Signaling of BMP6 was studied by the expression of Smad1/5/8 and pSmad4, and the BMP-target gene Id1. The interaction of pSmad4 with GPR91 promoter was studied by ChIP. Results Expression of GPR91 was higher in Hjv(-/-) retinas and RPE than in wild-type counterparts. Unexpectedly, BMP signaling was increased, not decreased, in Hjv(-/-) retinas and RPE. Bone morphogenetic protein 6 induced GPR91 in RPE, suggesting that increased BMP signaling in Hjv(-/-) retinas was likely responsible for GPR91 upregulation. Exposure of RPE to excess iron and succinate as well as BMP6 and succinate increased VEGF expression. Bone morphogenetic protein 6 promoted the interaction of pSmad4 with GPR91 promoter in RPE. Conclusions G-protein-coupled receptor 91 is a BMP6 target and Hjv deletion enhances BMP signaling in retina, thus underscoring a role for excess iron and hemochromatosis in abnormal retinal vascularization.

Published

2016

115. Expression of Functional Human Na+- Coupled Citrate Transporter (SLC13A5) in the Yeast Pichia pastoris

Author

Vadivel Ganapathy, Ina L. Urbatsch, and Valeria Jaramillo-Martinez

Subjects

Biochemistry, biology, Chemistry, Citrate transporter, Biophysics, biology.organism_classification, Yeast, Pichia pastoris

Published

2020

116. Transport of 2,4-dichloro phenoxyacetic acid by human Na

Author

Kazuaki, Sugio, Daisei, Inoda, Masayuki, Masuda, Isao, Azumaya, Shotaro, Sasaki, Kazumi, Shimono, Vadivel, Ganapathy, and Seiji, Miyauchi

Subjects

Monocarboxylic Acid Transporters, Xenopus laevis, Microvilli, Herbicides, Animals, Humans, Biological Transport, Female, Rabbits, 2,4-Dichlorophenoxyacetic Acid

Abstract

Using X. laevis oocyte expression system, we investigated whether human Na

Published

2018

117. Recent advances in drug delivery via the organic cation/carnitine transporter 2 (OCTN2/SLC22A5)

Author

Ruijie Chen, Rui Sun, Vadivel Ganapathy, Longfa Kou, and Qing Yao

Subjects

0301 basic medicine, Clinical Biochemistry, SLC22A5, 03 medical and health sciences, Drug Delivery Systems, Carnitine, Drug Discovery, Animals, Humans, Prodrugs, Solute Carrier Family 22 Member 5, Pharmacology, biology, Chemistry, Cell Membrane, Organic Cation-Carnitine Transporter 2, Transporter, Biological Transport, Prodrug, CARNITINE TRANSPORTER 2, 030104 developmental biology, Membrane, Biochemistry, Drug delivery, biology.protein, Molecular Medicine, Nanoparticles

Abstract

Transporters in the plasma membrane have been exploited successfully for the delivery of drugs in the form of prodrugs and nanoparticles. Organic cation/carnitine transporter 2 (OCTN2, SLC22A5) has emerged as a viable target for drug delivery. OCTN2 is a Na

Published

2018

118. Gpr109a limits microbiota-induced IL-23 production to constrain ILC3-mediated colonic inflammation

Author

Peng Zeng, Vadivel Ganapathy, Honglin Li, Lixin Dong, Sathish Sivaprakasam, Nikhil Patel, Pamela Shiao, Haiyan Xiao, Siyi Li, Ravindra Kolhe, Brinda Bhatt, Huabin Zhu, Nagendra Singh, and Daniel Levy-Bercowski

Subjects

0301 basic medicine, Colon, Immunology, Inflammation, chemical and pharmacologic phenomena, Gut flora, Interleukin-23, Article, Receptors, G-Protein-Coupled, 03 medical and health sciences, Mice, Immune system, RAR-related orphan receptor gamma, medicine, Interleukin 23, Immunology and Allergy, Animals, Lymphocytes, Intestinal Mucosa, Immunity, Mucosal, Mice, Knockout, Innate immune system, biology, Innate lymphoid cell, biology.organism_classification, Colitis, Gastrointestinal Microbiome, Mice, Inbred C57BL, 030104 developmental biology, Mucosal immunology, medicine.symptom, Inflammation Mediators

Abstract

A set of coordinated interactions between gut microbiota and the immune cells surveilling the intestine play a key role in shaping local immune responses and intestinal health. Gpr109a is a G protein–coupled receptor expressed at a very high level on innate immune cells and previously shown to play a key role in the induction of colonic regulatory T cells. In this study, we show that Gpr109a−/−Rag1−/− mice exhibit spontaneous rectal prolapse and colonic inflammation, characterized by the presence of an elevated number of IL-17–producing Rorγt+ innate lymphoid cells (ILCs; ILC3). Genetic deletion of Rorγt alleviated the spontaneous colonic inflammation in Gpr109a−/−Rag1−/− mice. Gpr109a-deficient colonic dendritic cells produce higher amounts of IL-23 and thereby promote ILC3. Moreover, the depletion of gut microbiota by antibiotics treatment decreased IL-23 production, ILC3, and colonic inflammation in Gpr109a−/−Rag1−/− mice. The ceca of Gpr109a−/−Rag1−/− mice showed significantly increased colonization by members of Bacteroidaceae, Porphyromonadaceae, Prevotellaceae, Streptococcaceae, Christensenellaceae, and Mogibacteriaceae, as well as IBD-associated microbiota such as Enterobacteriaceae and Mycoplasmataceae, compared with Rag1−/− mice, housed in a facility positive for Helicobacter and murine norovirus. Niacin, a Gpr109a agonist, suppressed both IL-23 production by colonic DCs and ILC3 number in a Gpr109a-dependent manner. Collectively, our data present a model suggesting that targeting Gpr109a will be potentially beneficial in the suppression of IL-23–mediated immunopathologies.

Published

2018

119. RETRACTED ARTICLE: Identification of a novel Na+-coupled Fe3+-citrate transport system, distinct from mammalian INDY, for uptake of citrate in mammalian cells

Author

Elizebeta Nemeth, Sabarish Ramachandran, Vadivel Ganapathy, Seiji Miyauchi, Yangzom D. Bhutia, Jiro Ogura, and Ellappan Babu

Subjects

0301 basic medicine, Multidisciplinary, biology, Chemistry, Science, medicine.medical_treatment, Ferroportin, Stimulation, Transporter, Iron supplement, Citrate transport, 03 medical and health sciences, Metabolic pathway, 030104 developmental biology, Biochemistry, Cell culture, medicine, biology.protein, Medicine, Ferric, medicine.drug

Abstract

NaCT is a Na+-coupled transporter for citrate expressed in hepatocytes and neurons. It is the mammalian ortholog of INDY (I’m Not Dead Yet), a transporter which modifies lifespan in Drosophila. Here we describe a hitherto unknown transport system for citrate in mammalian cells. When liver and mammary epithelial cells were pretreated with the iron supplement ferric ammonium citrate (FAC), uptake of citrate increased >10-fold. Iron chelators abrogated the stimulation of citrate uptake in FAC-treated cells. The iron exporter ferroportin had no role in this process. The stimulation of citrate uptake also occurred when Fe3+ was added during uptake without pretreatment. Similarly, uptake of Fe3+ was enhanced by citrate. The Fe3+-citrate uptake was coupled to Na+. This transport system was detectable in primary hepatocytes and neuronal cell lines. The functional features of this citrate transport system distinguish it from NaCT. Loss-of-function mutations in NaCT cause early-onset epilepsy and encephalopathy; the newly discovered Na+-coupled Fe3+-citrate transport system might offer a novel treatment strategy for these patients to deliver citrate into affected neurons independent of NaCT. It also has implications to iron-overload conditions where circulating free iron increases, which would stimulate cellular uptake of citrate and consequently affect multiple metabolic pathways.

Published

2018

120. Identification of a novel Na+-coupled Fe3+-citrate transport system, distinct from mammalian INDY, for uptake of citrate in mammalian cells

Author

Jiro, Ogura, Ellappan, Babu, Seiji, Miyauchi, Sabarish, Ramachandran, Elizebeta, Nemeth, Yangzom D, Bhutia, and Vadivel, Ganapathy

Subjects

Retraction Note, Article

Abstract

NaCT is a Na+-coupled transporter for citrate expressed in hepatocytes and neurons. It is the mammalian ortholog of INDY (I’m Not Dead Yet), a transporter which modifies lifespan in Drosophila. Here we describe a hitherto unknown transport system for citrate in mammalian cells. When liver and mammary epithelial cells were pretreated with the iron supplement ferric ammonium citrate (FAC), uptake of citrate increased >10-fold. Iron chelators abrogated the stimulation of citrate uptake in FAC-treated cells. The iron exporter ferroportin had no role in this process. The stimulation of citrate uptake also occurred when Fe3+ was added during uptake without pretreatment. Similarly, uptake of Fe3+ was enhanced by citrate. The Fe3+-citrate uptake was coupled to Na+. This transport system was detectable in primary hepatocytes and neuronal cell lines. The functional features of this citrate transport system distinguish it from NaCT. Loss-of-function mutations in NaCT cause early-onset epilepsy and encephalopathy; the newly discovered Na+-coupled Fe3+-citrate transport system might offer a novel treatment strategy for these patients to deliver citrate into affected neurons independent of NaCT. It also has implications to iron-overload conditions where circulating free iron increases, which would stimulate cellular uptake of citrate and consequently affect multiple metabolic pathways.

Published

2018

121. Protein Digestion and Absorption

Author

Yangzom D. Bhutia and Vadivel Ganapathy

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030217 neurology & neurosurgery

Published

2018

122. Contributors

Author

Yasutada Akiba, Denise Al Alam, Rana Al-Sadi, Qasim Aziz, Eric J. Battaglioli, Adil E. Bharucha, Richard S. Blumberg, Natacha Bohin, Joel C. Bornstein, Stuart M. Brierley, Simon J.H. Brookes, Joel Castro, Eugene B. Chang, Benoit Chassaing, Mary Cheung, Matthew A. Ciorba, Sheila E. Crowe, Michael Czerwinski, Soula Danopoulos, Soumita Das, Peter J. Dempsey, Gerco den Hartog, Hideki Enomoto, Andelain Erickson, Peter B. Ernst, Adam D. Farmer, Jaime P.P. Foong, Mark R. Frey, Andrew T. Gewirtz, Fayez K. Ghishan, Fiona M. Gribble, Luke Grundy, Marlene M. Hao, Andrea M. Harrington, Grant W. Hennig, Hongzhen Hu, Jan D. Huizinga, Shankar S. Iyer, Izumi Kaji, Purna C. Kashyap, Jonathan D. Kaunitz, Jennifer S. Labus, Brigitte Lavoie, Cambrian Y. Liu, Thomas Y. Ma, Xiaoya Ma, Gary M. Mawe, Juanita L. Merchant, Jeannette S. Messer, Larry Miller, Bruce D. Naliboff, Mark T. Nelson, Donald F. Newgreen, Prashant Nighot, Monica Passi, D. Brent Polk, Maria J. Pozo, Frank Reimann, Geoffrey P. Roberts, Bani C. Roland, James K. Ruffle, Hyder Said, Linda C. Samuelson, Michael A. Schumacher, Yatrik M. Shah, Terez Shea-Donohue, Noah F. Shroyer, Jason R. Spence, Nick J. Spencer, Stephanie N. Spohn, Lincon A. Stamp, William F. Stenson, Miyako Takaki, Kirsten Tillisch, Toshihiro Uesaka, Gijs R. van den Brink, Willemijn A. van Dop, Anil Vegesna, Jakob von Moltke, Arnold Wald, B. Florien Westendorp, Mathew Whitson, Jackie D. Wood, Hua Xu, Vincent W. Yang, Heather M. Young, Vincent B. Young, Nada A. Abumrad, Waddah A. Alrefai, Rana Ammoury, Gregory J. Anderson, Shinji Asano, Giorgos Bamias, Yangzom D. Bhutia, Niviann M. Blondet, Patrick Borel, Vincenza Cifarelli, James F. Collins, Robert J. Cousins, Nicholas O. Davidson, Paul A. Dawson, Guillaume de Lartigue, Charles Desmarchelier, Pradeep K. Dudeja, Shireen R.L. Flores, Vadivel Ganapathy, Chiara Ghezzi, Ravinder K. Gill, Fred S. Gorelick, Matthew B. Grisham, Earl H. Harrison, Gail A. Hecht, Dawn A. Israel, James D. Jamieson, Bryson W. Katona, Pawel R. Kiela, Rachel E. Kopec, Kris V. Kowdley, Nicholas F. LaRusso, Seong M. Lee, Rodger A. Liddle, Juan P. Liuzzi, Donald D.F. Loo, John P. Lynch, Anatoliy I. Masyuk, Tatyana V. Masyuk, Donald J. Messner, Mark B. Meyer, Karen F. Murray, Ebba Nexo, Curtis T. Okamoto, Bernardo Ortega, Stephen Pandol, Richard M. Peek, J. Wesley Pike, Shubha Priyamvada, Gordon B. Proctor, Vazhaikkurichi M. Rajendran, Helen E. Raybould, Jesus Rivera-Nieves, Hamid M. Said, Hideki Sakai, Seema Saksena, Monica Sala-Rabanal, Jörg-Dieter Schulzke, Ursula E. Seidler, Abeer K. Shaalan, Irshad A. Sheikh, Jay R. Thiagarajah, Alan S. Verkman, Xiaoyu Wang, Paul A. Welling, Allan W. Wolkoff, and Ernest M. Wright

Published

2018

123. Extracellular citrate affects critical elements of cancer cell metabolism and supports cancer development in vivo

Author

Sven A. Lang, Peter J. Oefner, Cornelia Prehn, Margareta Lantow, Katharina Schmidt, Karl Kunzelmann, Gudrun E. Koehl, Maria E. Mycielska, Petra Rümmele, Jerzy Adamski, Vadivel Ganapathy, Moritz Schladt, Gregor M. Madej, Alexander Cecil, Christine Ziegler, Hans Juergen Schlitt, Christian H. Wetzel, Christian J. Wachsmuth, Vladimir M. Milenkovic, Elke Eggenhofer, Katja Dettmer, Wolfgang Jagla, Andreas Gaumann, and E. K. Geissler

Subjects

0301 basic medicine, Cancer Research, Fatty acid metabolism, Cancer, Citrate transport, medicine.disease, Citric acid cycle, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Oncology, chemistry, 030220 oncology & carcinogenesis, Cancer cell, medicine, Extracellular, Cancer research, Glycolysis, Fatty acid synthesis

Abstract

Glycolysis and fatty acid synthesis are highly active in cancer cells through cytosolic citrate metabolism, with intracellular citrate primarily derived from either glucose or glutamine via the tricarboxylic acid cycle. We show here that extracellular citrate is supplied to cancer cells through a plasma membrane-specific variant of the mitochondrial citrate transporter (pmCiC). Metabolomic analysis revealed that citrate uptake broadly affected cancer cell metabolism through citrate-dependent metabolic pathways. Treatment with gluconate specifically blocked pmCiC and decreased tumor growth in murine xenografts of human pancreatic cancer. This treatment altered metabolism within tumors, including fatty acid metabolism. High expression of pmCiC was associated with invasion and advanced tumor stage across many human cancers. These findings support the exploration of extracellular citrate transport as a novel potential target for cancer therapy. Significance: Uptake of extracellular citrate through pmCiC can be blocked with gluconate to reduce tumor growth and to alter metabolic characteristics of tumor tissue. Cancer Res; 78(10); 2513–23. ©2018 AACR.

Published

2018

124. Abstract LB-062: Deficiency of dietary fiber inSlc5a8-null mice promotes bacterial dysbiosis and inflammatory milieu in colon

Author

Sivaprakasam, Sathish, primary, Ganapathy, Pramodh K., additional, Ramachandran, Sabarish, additional, Kottapalli, Kameswara Rao, additional, and Vadivel, Ganapathy, additional

Published

2019

125. Progesterone Receptor Membrane Component 1 (PGRMC1) Expression in Murine Retina

Author

Vadivel Ganapathy, Eric P. Zorrilla, Shanu Markand, Kathryn E. Bollinger, Jing Zhao, Arul Shanmugam, Sylvia B. Smith, Barbara A. Mysona, A. Sanders, Jing Wang, and Amany Tawfik

Subjects

Retinal Ganglion Cells, 0301 basic medicine, medicine.medical_specialty, Ependymoglial Cells, Immunoblotting, Biology, Article, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, Internal medicine, Progesterone receptor, medicine, Animals, RNA, Messenger, Receptor, PGRMC1, Corneal epithelium, Mice, Knockout, Retina, Retinal pigment epithelium, Reverse Transcriptase Polymerase Chain Reaction, Membrane Proteins, Sensory Systems, Cell biology, Mice, Inbred C57BL, Ophthalmology, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Gene Expression Regulation, Membrane protein, Lens (anatomy), Models, Animal, sense organs, Receptors, Progesterone

Abstract

Sigma receptors 1 (σR1) and 2 (σR2) are thought to be two distinct proteins which share the ability to bind multiple ligands, several of which are common to both receptors. Whether σR1 and σR2 share overlapping biological functions is unknown. Recently, progesterone receptor membrane component 1 (PGRMC1) was shown to contain the putative σR2 binding site. PGRMC1 has not been studied in retina. We hypothesize that biological interactions between σR1 and PGRMC1 will be evidenced by compensatory upregulation of PGRMC1 in σR1Immunofluorescence, RT-PCR, and immunoblotting methods were used to analyze expression of PGRMC1 in wild-type mouse retina. Tissues from σR1In the eye, PGRMC1 is expressed in corneal epithelium, lens, ciliary body epithelium, and retina. In retina, PGRMC1 is present in Müller cells and retinal pigment epithelium. This expression pattern is similar, but not identical to σR1. PGRMC1 protein levels in neural retina and eye cup from σR1Despite potential biological overlap, deletion of σR1 did not result in a compensatory change in PGRMC1 protein levels in σR1

Published

2015

126. Sigma 1 receptor regulates the oxidative stress response in primary retinal Müller glial cells via NRF2 signaling and system xc−, the Na+-independent glutamate–cystine exchanger

Author

Shanu Markand, Vadivel Ganapathy, Arul Shanmugam, Sylvia B. Smith, Jing Wang, and Eric P. Zorrilla

Subjects

Transcriptional Activation, GPX1, Mice, 129 Strain, Amino Acid Transport System y+, NF-E2-Related Factor 2, Ependymoglial Cells, Primary Cell Culture, Mitochondrion, Biology, medicine.disease_cause, Biochemistry, Neuroprotection, Article, chemistry.chemical_compound, Physiology (medical), medicine, Animals, Receptors, sigma, Cells, Cultured, Adaptor Proteins, Signal Transducing, Mice, Knockout, Retina, Kelch-Like ECH-Associated Protein 1, Endoplasmic reticulum, Glutathione, KEAP1, Antioxidant Response Elements, Cell biology, Mice, Inbred C57BL, Cytoskeletal Proteins, Oxidative Stress, medicine.anatomical_structure, chemistry, Female, sense organs, Reactive Oxygen Species, Oxidative stress, Signal Transduction

Abstract

Oxidative stress figures prominently in retinal diseases, including diabetic retinopathy, and glaucoma. Ligands for σ1R, a unique transmembrane protein localized to the endoplasmic reticulum, mitochondria, and nuclear and plasma membranes, have profound retinal neuroprotective properties in vitro and in vivo. Studies to determine the mechanism of σ1R-mediated retinal neuroprotection have focused mainly on neurons. Little is known about the effects of σ1R on Müller cell function, yet these radial glial cells are essential for homeostatic support of the retina. Here we investigated whether σ1R mediates the oxidative stress response of Müller cells using wild-type (WT) and σ1R-knockout (σ1RKO) mice. We observed increased endogenous reactive oxygen species (ROS) levels in σ1RKO Müller cells compared to WT, which was accompanied by decreased expression of Sod1, catalase, Nqo1, Hmox1, Gstm6, and Gpx1. The protein levels of SOD1, CAT, NQO1, and GPX1 were also significantly decreased. The genes encoding these antioxidants contain an antioxidant response element (ARE), which under stress is activated by NRF2, a transcription factor that typically resides in the cytoplasm bound by KEAP1. In the σ1RKO Müller cells Nrf2 expression was decreased significantly at the gene (and protein) level, whereas Keap1 gene (and protein) levels were markedly increased. NRF2-ARE binding affinity was decreased markedly in σ1RKO Müller cells. We investigated system xc(-), the cystine-glutamate exchanger important for synthesis of glutathione (GSH), and observed decreased function in σ1RKO Müller cells compared to WT as well as decreased GSH and GSH/GSSG ratios. This was accompanied by decreased gene and protein levels of xCT, the unique component of system xc(-). We conclude that Müller glial cells lacking σ1R manifest elevated ROS, perturbation of antioxidant balance, suppression of NRF2 signaling, and impaired function of system xc(-). The data suggest that the oxidative stress-mediating function of retinal Müller glial cells may be compromised in the absence of σ1R. The neuroprotective role of σ1R may be linked directly to the oxidative stress-mediating properties of supportive glial cells.

Published

2015

127. Slc5a8, a Na+-coupled high-affinity transporter for short-chain fatty acids, is a conditional tumour suppressor in colon that protects against colitis and colon cancer under low-fibre dietary conditions

Author

Yangzom D. Bhutia, Sathish Sivaprakasam, Vadivel Ganapathy, Nagendra Singh, Thomas Boettger, and Ashish Gurav

Subjects

Dietary Fiber, Monocarboxylic Acid Transporters, Colon, Histamine Antagonists, Butyrate, Biology, T-Lymphocytes, Regulatory, Biochemistry, Aldehyde Dehydrogenase 1 Family, Article, Immune tolerance, Interferon-gamma, Mice, Immune system, Immune Tolerance, medicine, Animals, Indoleamine-Pyrrole 2,3,-Dioxygenase, Interferon gamma, Colitis, Cation Transport Proteins, Immunity, Mucosal, Molecular Biology, Mice, Knockout, Tumor Suppressor Proteins, Fatty Acids, Retinal Dehydrogenase, FOXP3, Forkhead Transcription Factors, Transporter, Dendritic Cells, Cell Biology, Dendritic cell, Aldehyde Dehydrogenase, medicine.disease, Cell biology, Colonic Neoplasms, Butyric Acid, medicine.drug

Abstract

Mammalian colon harbours trillions of bacteria under physiological conditions; this symbiosis is made possible because of a tolerized response from the mucosal immune system. The mechanisms underlying this tolerogenic phenomenon remain poorly understood. In the present study we show that Slc5a8 (solute carrier gene family 5a, member 8), a Na+-coupled high-affinity transporter in colon for the bacterial fermentation product butyrate, plays a critical role in this process. Among various immune cells in colon, dendritic cells (DCs) are unique not only in their accessibility to luminal contents but also in their ability to induce tolerogenic phenotype in T-cells. We found that DCs exposed to butyrate express the immunosuppressive enzymes indoleamine 2,3-dioxygenase 1 (IDO1) and aldehyde dehydrogenase 1A2 (Aldh1A2), promote conversion of naive T-cells into immunosuppressive forkhead box P3+ (FoxP3+) Tregs (regulatory T-cells) and suppress conversion of naive T-cells into pro-inflammatory interferon (IFN)-γ-producing cells. Slc5a8-null DCs do not induce IDO1 and Aldh1A2 and do not generate Tregs or suppress IFN-γ-producing T-cells in response to butyrate. We also provide in vivo evidence for an obligatory role for Slc5a8 in suppression of IFN-γ-producing T-cells. Furthermore, Slc5a8 protects against colitis and colon cancer under conditions of low-fibre intake but not when dietary fibre intake is optimal. This agrees with the high-affinity nature of the transporter to mediate butyrate entry into cells. We conclude that Slc5a8 is an obligatory link between dietary fibre and mucosal immune system via the bacterial metabolite butyrate and that this transporter is a conditional tumour suppressor in colon linked to dietary fibre content.

Published

2015

128. IFNγ Induces DNA Methylation–Silenced GPR109A Expression via pSTAT1/p300 and H3K18 Acetylation in Colon Cancer

Author

Vadivel Ganapathy, Christopher M. Heaton, Yangzom D. Bhutia, Dafeng Yang, May R. Chen, Muthusamy Thangaraju, Keni Gu, Jeffrey R. Lee, Kankana Bardhan, Amy V. Paschall, Pamela M. Martin, Kebin Liu, Priscilla S. Simon, and Darren D. Browning

Subjects

Cancer Research, Colorectal cancer, medicine.medical_treatment, Immunology, Apoptosis, Receptors, Nicotinic, Biology, Article, Chromatin remodeling, Receptors, G-Protein-Coupled, Interferon-gamma, Mice, Transcription (biology), Cell Line, Tumor, medicine, Animals, Humans, Gene silencing, Genes, Tumor Suppressor, Mice, Knockout, Mice, Inbred BALB C, Carcinoma, Acetylation, Promoter, Methylation, DNA Methylation, medicine.disease, Molecular biology, Disease Models, Animal, Cytokine, Colonic Neoplasms, DNA methylation, E1A-Associated p300 Protein

Abstract

Short-chain fatty acids, metabolites produced by colonic microbiota from fermentation of dietary fiber, act as anti-inflammatory agents in the intestinal tract to suppress proinflammatory diseases. GPR109A is the receptor for short-chain fatty acids. The functions of GPR109A have been the subject of extensive studies; however, the molecular mechanisms underlying GPR109A expression is largely unknown. We show that GPR109A is highly expressed in normal human colon tissues, but is silenced in human colon carcinoma cells. The GPR109A promoter DNA is methylated in human colon carcinoma. Strikingly, we observed that IFNγ, a cytokine secreted by activated T cells, activates GPR109A transcription without altering its promoter DNA methylation. Colon carcinoma grows significantly faster in IFNγ-deficient mice than in wild-type mice in an orthotopic colon cancer mouse model. A positive correlation was observed between GPR109A protein level and tumor-infiltrating T cells in human colon carcinoma specimens, and IFNγ expression level is higher in human colon carcinoma tissues than in normal colon tissues. We further demonstrated that IFNγ rapidly activates pSTAT1 that binds to the promoter of p300 to activate its transcription. p300 then binds to the GPR109A promoter to induce H3K18 hyperacetylation, resulting in chromatin remodeling in the methylated GPR109A promoter. The IFNγ-activated pSTAT1 then directly binds to the methylated but hyperacetylated GPR109 promoter to activate its transcription. Overall, our data indicate that GPR109A acts as a tumor suppressor in colon cancer, and the host immune system might use IFNγ to counteract DNA methylation–mediated GPR109A silencing as a mechanism to suppress tumor development. Cancer Immunol Res; 3(7); 795–805. ©2015 AACR.

Published

2015

129. Deletion of the amino acid transporter Slc6a14 suppresses tumour growth in spontaneous mouse models of breast cancer

Author

Muthusamy Thangaraju, Vadivel Ganapathy, Yangzom D. Bhutia, Puttur D. Prasad, Sabarish Ramachandran, Jaya P. Gnana-Prakasam, and Ellappan Babu

Subjects

Commentary Articles, medicine.medical_specialty, Amino Acid Transport Systems, Commentary Article, cancer metabolism, Estrogen receptor, Biology, Plasma Membrane Neurotransmitter Transport Proteins, Biochemistry, amino acid transporter, Mice, Drug Delivery Systems, SLC6A14 (ATB0,+), Internal medicine, medicine, Animals, Amino acid transporter, Molecular Biology, PI3K/AKT/mTOR pathway, Cell Proliferation, Mice, Knockout, chemistry.chemical_classification, Messenger RNA, TOR Serine-Threonine Kinases, RPTOR, Mammary Neoplasms, Experimental, Transporter, Cell Biology, targeted therapy, Neoplasm Proteins, Amino acid, oestrogen receptor-positive (ER+) breast cancer, Endocrinology, chemistry, Knockout mouse, Cancer research, Female, Gene Deletion, Signal Transduction

Abstract

The cancer-specific nutrient transporter, SLC6A14, could be a means to target cancer metabolism as described by Babu et al. in this issue., Rapidly proliferating cancer cells increase flux through anabolic pathways to build the mass necessary to support cell division. Imported amino acids and glucose lie at the apex of the anabolic pyramid. Consistent with this, elevated expression of nutrient transporter proteins is characteristic of aggressive and highly malignant cancers. Because tumour cells are more dependent than their normal neighbours on accelerated nutrient import, these up-regulated transporters could be excellent targets for selective anti-cancer therapies. A study by Babu et al. in a recent issue of the Biochemical Journal definitively shows that SLC6A14 (where SLC is solute carrier) is one such cancer-specific amino acid transporter. Although mice completely lacking SLC6A14 are viable and exhibit normal mammary gland development, these animals are highly resistant to mammary tumour initiation and progression driven by potent oncogenes. Because SLC6A14 is essential for tumour growth yet dispensable for normal development and tissue maintenance, small molecules that block amino acid import through this transporter could be effective and selective anti-cancer agents, particularly as components of rational drug combinations.

Published

2015

130. Amino Acid Transporters in Cancer and Their Relevance to 'Glutamine Addiction': Novel Targets for the Design of a New Class of Anticancer Drugs

Author

Yangzom D. Bhutia, Sabarish Ramachandran, Vadivel Ganapathy, and Ellappan Babu

Subjects

Drug, Cancer Research, Amino Acid Transport Systems, Glutamine, media_common.quotation_subject, Antineoplastic Agents, SLC7A11, Neoplasms, medicine, Protein biosynthesis, Animals, Humans, Molecular Targeted Therapy, media_common, chemistry.chemical_classification, biology, Oncogene, Cancer, Transporter, medicine.disease, Amino acid, Oncology, Biochemistry, chemistry, biology.protein

Abstract

Tumor cells have an increased demand for amino acids because of their rapid proliferation rate. In addition to their need in protein synthesis, several amino acids have other roles in supporting cancer growth. There are approximately two-dozen amino acid transporters in humans, and tumor cells must upregulate one or more of these transporters to satisfy their demand for amino acids. If the transporters that specifically serve this purpose in tumor cells are identified, they can be targeted for the development of a brand new class of anticancer drugs; the logical basis of such a strategy would be to starve the tumor cells of an important class of nutrients. To date, four amino acid transporters have been found to be expressed at high levels in cancer: SLC1A5, SLC7A5, SLC7A11, and SLC6A14. Their induction occurs in a cancer type–specific manner with a direct or indirect involvement of the oncogene c-Myc. Further, these transporters are functionally coupled, thus maximizing their ability to promote cancer growth and chemoresistance. Progress has been made in preclinical studies, exploiting these transporters as drug targets in cancer therapy. These transporters also show promise in development of new tumor-imaging probes and in tumor-specific delivery of appropriately designed chemotherapeutic agents. Cancer Res; 75(9); 1782–8. ©2015 AACR.

Published

2015

131. Species-Specific Influence of Lithium on the Activity of SLC13A5 (NaCT): Lithium-Induced Activation Is Specific for the Transporter in Primates

Author

Sabarish Ramachandran, Yangzom D. Bhutia, Elangovan Gopal, Puttur D. Prasad, Ellappan Babu, and Vadivel Ganapathy

Subjects

Pan troglodytes, Mutant, Stimulation, Biology, medicine.disease_cause, Cell Line, Mice, Xenopus laevis, Dogs, Species Specificity, medicine, Animals, Humans, Citrates, Caenorhabditis elegans, Zebrafish, Pharmacology, chemistry.chemical_classification, Mutation, Symporters, Tryptophan, Biological Transport, Transporter, Macaca mulatta, Rats, Amino acid, Citric acid cycle, Biochemistry, chemistry, Cell culture, Lithium Compounds, Oocytes, Molecular Medicine, Female

Abstract

NaCT (SLC13A5) is a Na(+)-coupled transporter for Krebs cycle intermediates and is expressed predominantly in the liver. Human NaCT is relatively specific for citrate compared with other Krebs cycle intermediates. The transport activity of human NaCT is stimulated by Li(+), whereas that of rat NaCT is inhibited by Li(+). We studied the influence of Li(+) on NaCTs cloned from eight different species. Li(+) stimulated the activity of only NaCTs from primates (human, chimpanzee, and monkey); by contrast, NaCTs from nonprimate species (mouse, rat, dog, and zebrafish) were inhibited by Li(+). Caenorhabditis elegans NaCT was not affected by Li(+). With human NaCT, the Li(+)-induced increase in transport activity was associated with the conversion of the transporter from a low-affinity/high-capacity type to a high-affinity/low-capacity type. H(+) was able to substitute for Li(+) in eliciting the stimulatory effect. The amino acid Phe500 in human NaCT was critical for Li(+)/H(+)-induced stimulation. Mutation of this amino acid to tryptophan (F500W) markedly increased the basal transport activity of human NaCT in the absence of Li(+), but the ability of Li(+) to stimulate the transporter was almost completely lost with this mutant. Substitution of Phe500 with tryptophan in human NaCT converted the transporter from a low-affinity/high-capacity type to a high-affinity/low-capacity type, an effect similar to that of Li(+) on the wild-type NaCT. These studies show that Li(+)-induced activation of NaCT is specific for the transporter in primates and that the region surrounding Phe500 in primate NaCTs is important for the Li(+) effect.

Published

2015

132. The Na+/Cl−-Coupled, Broad-Specific, Amino Acid Transporter SLC6A14 (ATB0,+): Emerging Roles in Multiple Diseases and Therapeutic Potential for Treatment and Diagnosis

Author

Shengping Yang, Yangzom D. Bhutia, Mohd. Omar Faruk Sikder, and Vadivel Ganapathy

Subjects

0301 basic medicine, chemistry.chemical_classification, Cell growth, Pharmaceutical Science, Transporter, mTORC1, Biology, Amino acid, 03 medical and health sciences, 030104 developmental biology, Biochemistry, chemistry, microRNA, Gene family, Amino acid transporter, Cellular compartment

Abstract

Amino acids are essential building blocks of all mammalian cells, and amino acid transporters play a vital role in transporting them into cells and their further distribution among the various cellular compartments. There are ~ 430 known transporters in the solute-linked carrier (SLC) gene family, divided into 52 distinct families. Eleven of these gene families contain one or more amino acid transporters. These transporters differ significantly from each other in terms of substrate specificity, ion dependence, and energetics. Given the variety of roles they fulfill in human physiology, it is not surprising that a number of diseases are associated with the malfunction of these transporters. In particular, as amino acids are critical for cell growth, survival, and proliferation, the role of amino acid transporters in cancer is gaining increasing attention in recent years. The present review primarily focuses on one particular amino acid transporter, SLC6A14 (also known as ATB0,+), with regard to its relevance to specific diseases, including cancer, and the molecular mechanisms underlying the disease-related alterations in the expression of the transporter. Furthermore, the review highlights the possible utility of this transporter in drug delivery and also its therapeutic potential for the treatment and diagnosis of cancer.

Published

2017

133. L-Carnitine-conjugated nanoparticles to promote permeation across blood-brain barrier and to target glioma cells for drug delivery via the novel organic cation/carnitine transporter OCTN2

Author

Menglin Wang, Gang Wang, Weiling Guo, Qiang Fu, Longfa Kou, Zhonggui He, Jin Sun, Yanxian Hou, Qing Yao, and Vadivel Ganapathy

Subjects

0301 basic medicine, Biodistribution, Paclitaxel, Biomedical Engineering, Pharmaceutical Science, Medicine (miscellaneous), macromolecular substances, 02 engineering and technology, Pharmacology, Blood–brain barrier, Permeability, 03 medical and health sciences, chemistry.chemical_compound, Drug Delivery Systems, In vivo, Glioma, Carnitine, medicine, Humans, Solute Carrier Family 22 Member 5, Chemistry, technology, industry, and agriculture, General Medicine, 021001 nanoscience & nanotechnology, medicine.disease, Neoplasm Proteins, Endothelial stem cell, PLGA, 030104 developmental biology, medicine.anatomical_structure, Transcytosis, Blood-Brain Barrier, Drug delivery, Biophysics, Nanoparticles, Caco-2 Cells, 0210 nano-technology, Glioblastoma, Biotechnology

Abstract

Overcoming blood–brain barrier (BBB) and targeting tumor cells are two key steps for glioma chemotherapy. By taking advantage of the specific expression of Na+-coupled carnitine transporter 2 (OCTN2) on both brain capillary endothelial cells and glioma cells, l-carnitine conjugated poly(lactic-co-glycolic acid) nanoparticles (LC-PLGA NPs) were prepared to enable enhanced BBB permeation and glioma-cell targeting. Conjugation of l-carnitine significantly enhanced the uptake of PLGA nanoparticles in the BBB endothelial cell line hCMEC/D3 and the glioma cell line T98G. The uptake was dependent on Na+ and inhibited by the excessive free l-carnitine, suggesting involvement of OCTN2 in the process. In vivo mouse studies showed that LC-PLGA NPs resulted in high accumulation in the brain as indicated by the biodistribution and imaging assays. Furthermore, compared to Taxol and paclitaxel-loaded unmodified PLGA NPs, the drug-loaded LC-PLGA NPs showed improved anti-glioma efficacy in both 2D-cell and 3D-spheroid models. The PEG spacer length of the ligand attached to the nanoparticles was optimized, and the formulation with PEG1000 (LC-1000-PLGA NPs) showed the maximum targeting efficiency. We conclude that l-carnitine-mediated cellular recognition and internalization via OCTN2 significantly facilitate the transcytosis of nanoparticles across BBB and the uptake of nanoparticles in glioma cells, resulting in improved anti-glioma efficacy.

Published

2017

134. Monomethyl fumarate inhibits pain behaviors and amygdala activity in a rat arthritis model

Author

Volker Neugebauer, Vadivel Ganapathy, Guangchen Ji, Hyunyoung G. Kim, and Jeremy M. Thompson

Subjects

0301 basic medicine, Male, Microdialysis, Arthritis, Pain, Stimulation, Pharmacology, Amygdala, Neuroprotection, Article, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Fumarates, Neuroplasticity, medicine, Monoarthritis, Premovement neuronal activity, Animals, Maze Learning, Neurons, Neuronal Plasticity, business.industry, medicine.disease, Disease Models, Animal, 030104 developmental biology, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Neurology, Neurology (clinical), Vocalization, Animal, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

Neuroplasticity in the amygdala, a brain center for emotions, leads to increased neuronal activity and output that can generate emotional-affective behaviors and modulate nocifensive responses. Mechanisms of increased activity in the amygdala output region (central nucleus, CeA) include increased reactive oxygen species, and so we explored beneficial effects of monomethyl fumarate (MMF), which can have neuroprotective effects through the nuclear factor (erythroid-derived 2)-like 2 (Nrf2) antioxidant response pathway. Systemic (intraperitoneal) MMF dose-dependently inhibited vocalizations and mechanosensitivity (hindlimb withdrawal reflexes) of rats in an arthritis pain model (kaolin-carrageenan-induced monoarthritis in the knee). Stereotaxic administration of MMF into the CeA by microdialysis also inhibited vocalizations but had a limited effect on mechanosensitivity, suggesting a differential contribution to emotional-affective vs sensory pain aspects. Extracellular single-unit recordings of CeA neurons in anesthetized rats showed that stereotaxic administration of MMF into the CeA by microdialysis inhibited background activity and responses of CeA neurons to knee joint stimulation in the arthritis pain model. Monomethyl fumarate had no effect on behaviors and neuronal activity under normal conditions. The results suggest that MMF can inhibit emotional-affective responses in an arthritis pain model through an action that involves the amygdala (CeA).

Published

2017

135. The Na

Author

Mohd Omar F, Sikder, Shengping, Yang, Vadivel, Ganapathy, and Yangzom D, Bhutia

Subjects

Male, Amino Acid Transport Systems, Neutral, Amino Acid Transport Systems, Crohn Disease, Cystic Fibrosis, Neoplasms, Humans, Obesity, Infertility, Male

Abstract

Amino acids are essential building blocks of all mammalian cells, and amino acid transporters play a vital role in transporting them into cells and their further distribution among the various cellular compartments. There are ~ 430 known transporters in the solute-linked carrier (SLC) gene family, divided into 52 distinct families. Eleven of these gene families contain one or more amino acid transporters. These transporters differ significantly from each other in terms of substrate specificity, ion dependence, and energetics. Given the variety of roles they fulfill in human physiology, it is not surprising that a number of diseases are associated with the malfunction of these transporters. In particular, as amino acids are critical for cell growth, survival, and proliferation, the role of amino acid transporters in cancer is gaining increasing attention in recent years. The present review primarily focuses on one particular amino acid transporter, SLC6A14 (also known as ATB

Published

2017

136. Cell-Surface and Nuclear Receptors in the Colon as Targets for Bacterial Metabolites and Its Relevance to Colon Health

Author

Sathish Sivaprakasam, Sabarish Ramachandran, Yangzom D. Bhutia, and Vadivel Ganapathy

Subjects

0301 basic medicine, symbiotic relationship, immune tolerance, Colon, molecular targets, colitis, Receptors, Cytoplasmic and Nuclear, nuclear receptors, Receptors, Cell Surface, lcsh:TX341-641, Review, Butyrate, colonic bacteria, 03 medical and health sciences, Immune system, Humans, Receptor, bacterial metabolites, Pregnane X receptor, Nutrition and Dietetics, Bacteria, biology, Aryl hydrocarbon receptor, biology.organism_classification, cell-surface receptors, 030104 developmental biology, Nuclear receptor, Biochemistry, colon cancer, biology.protein, Farnesoid X receptor, lcsh:Nutrition. Foods and food supply, Food Science

Abstract

The symbiotic co-habitation of bacteria in the host colon is mutually beneficial to both partners. While the host provides the place and food for the bacteria to colonize and live, the bacteria in turn help the host in energy and nutritional homeostasis, development and maturation of the mucosal immune system, and protection against inflammation and carcinogenesis. In this review, we highlight the molecular mediators of the effective communication between the bacteria and the host, focusing on selective metabolites from the bacteria that serve as messengers to the host by acting through selective receptors in the host colon. These bacterial metabolites include the short-chain fatty acids acetate, propionate, and butyrate, the tryptophan degradation products indole-3-aldehyde, indole-3-acetic, acid and indole-3-propionic acid, and derivatives of endogenous bile acids. The targets for these bacterial products in the host include the cell-surface G-protein-coupled receptors GPR41, GPR43, and GPR109A and the nuclear receptors aryl hydrocarbon receptor (AhR), pregnane X receptor (PXR), and farnesoid X receptor (FXR). The chemical communication between these bacterial metabolite messengers and the host targets collectively has the ability to impact metabolism, gene expression, and epigenetics in colonic epithelial cells as well as in mucosal immune cells. The end result, for the most part, is the maintenance of optimal colonic health.

Published

2017

137. Carbidopa is an activator of aryl hydrocarbon receptor with potential for cancer therapy

Author

Shengping Yang, Sathisha J. Gonchigar, Yangzom D. Bhutia, Vadivel Ganapathy, Seiji Miyauchi, Jiro Ogura, and Kazumi Shimono

Subjects

Agonist, medicine.drug_class, CYP1B1, Active Transport, Cell Nucleus, Pharmacology, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, In vivo, Pancreatic cancer, medicine, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, Molecular Biology, Kynurenine, Cell Nucleus, biology, Chemistry, Liver Neoplasms, Carbidopa, Cell Biology, Hep G2 Cells, respiratory system, medicine.disease, Aryl hydrocarbon receptor, In vitro, Neoplasm Proteins, Pancreatic Neoplasms, Receptors, Aryl Hydrocarbon, 030220 oncology & carcinogenesis, biology.protein, Aryl Hydrocarbon Hydroxylases, Liver cancer, 030217 neurology & neurosurgery, medicine.drug, Signal Transduction

Abstract

Carbidopa is used with l-DOPA (l-3,4-dihydroxyphenylalanine) to treat Parkinson's disease (PD). PD patients exhibit lower incidence of most cancers including pancreatic cancer, but with the notable exception of melanoma. The decreased cancer incidence is not due to l-DOPA; however, the relevance of Carbidopa to this phenomenon has not been investigated. Here, we tested the hypothesis that Carbidopa, independent of l-DOPA, might elicit an anticancer effect. Carbidopa inhibited pancreatic cancer cell proliferation both in vitro and in vivo. Based on structural similarity with phenylhydrazine, an inhibitor of indoleamine-2,3-dioxygenase-1 (IDO1), we predicted that Carbidopa might also inhibit IDO1, thus providing a molecular basis for its anticancer effect. The inhibitory effect was confirmed using human recombinant IDO1. To demonstrate the inhibition in intact cells, AhR (aryl hydrocarbon receptor) activity was monitored as readout for IDO1-mediated generation of the endogenous AhR agonist kynurenine in pancreatic and liver cancer cells. Surprisingly, Carbidopa did not inhibit but instead potentiated AhR signaling, evident from increased CYP1A1 (cytochrome P450 family 1 subfamily A member 1), CYP1A2, and CYP1B1 expression. In pancreatic and liver cancer cells, Carbidopa promoted AhR nuclear localization. AhR antagonists blocked Carbidopa-dependent activation of AhR signaling. The inhibitory effect on pancreatic cancer cells in vitro and in vivo and the activation of AhR occurred at therapeutic concentrations of Carbidopa. Chromatin immunoprecipitation assay further confirmed that Carbidopa promoted AhR binding to its target gene CYP1A1 leading to its induction. We conclude that Carbidopa is an AhR agonist and suppresses pancreatic cancer. Hence, Carbidopa could potentially be re-purposed to treat pancreatic cancer and possibly other cancers as well.

Published

2017

138. Cell-surface G-protein-coupled receptors for tumor-associated metabolites: A direct link to mitochondrial dysfunction in cancer

Author

Yangzom D. Bhutia, Vadivel Ganapathy, and Bojana Ristic

Subjects

0301 basic medicine, Pyruvate decarboxylation, Cancer Research, biology, Succinate dehydrogenase, Cell Membrane, GPR81, Oxidative phosphorylation, Mitochondrion, DNA Methylation, Pyruvate dehydrogenase complex, Warburg effect, Article, Mitochondria, Receptors, G-Protein-Coupled, Citric acid cycle, 03 medical and health sciences, 030104 developmental biology, Oncology, Biochemistry, Neoplasms, Genetics, biology.protein, Animals, Humans

Abstract

Mitochondria are the sites of pyruvate oxidation, citric acid cycle, oxidative phosphorylation, ketogenesis, and fatty acid oxidation. Attenuation of mitochondrial function is one of the most significant changes that occurs in tumor cells, directly linked to oncogenesis, angiogenesis, Warburg effect, and epigenetics. In particular, three mitochondrial enzymes are inactivated in cancer: pyruvate dehydrogenase (PDH), succinate dehydrogenase (SDH), and 3-hydroxy-3-methylglutaryl CoA synthase-2 (HMGCS2). These enzymes are subject to regulation via acetylation/deacetylation. SIRT3, the predominant mitochondrial deacetylase, directly targets these enzymes for deacetylation and maintains their optimal catalytic activity. SIRT3 is a tumor suppressor, and deacetylation of these enzymes contributes to its biological function. PDH catalyzes the oxidative decarboxylation of pyruvate into acetyl CoA, SDH oxidizes succinate into fumarate, and HMGCS2 controls the synthesis of the ketone body β-hydroxybutyrate. As the activities of these enzymes are decreased in cancer, tumor cells accumulate lactate and succinate but produce less amounts of β-hydroxybutyrate. Apart from their role in cellular energetics, these metabolites function as signaling molecules via specific cell-surface G-protein-coupled receptors. Lactate signals via GPR81, succinate via GPR91, and β-hydroxybutyrate via GPR109A. In addition, lactate activates hypoxia-inducible factor HIF1α and succinate promotes DNA methylation. GPR81 and GPR91 are tumor promoters, and increased production of lactate and succinate as their agonists drives tumorigenesis by enhancing signaling via these two receptors. In contrast, GPR109A is a tumor suppressor, and decreased synthesis of β-hydroxybutyrate as its agonist suppresses signaling via this receptor, thus attenuating the tumor-suppressing function of GPR109A. In parallel with the opposing changes in lactate/succinate and β-hydroxybutyrate levels, tumor cells upregulate GPR81 and GPR91 but downregulate GPR109A. As such, these three metabolite receptors play a critical role in cancer and represent a new class of drug targets with selective antagonists of GPR81 and GPR91 for cancer treatment and agonists of GPR109A for cancer prevention.

Published

2017

139. Cotransporting Ion is a Trigger for Cellular Endocytosis of Transporter-Targeting Nanoparticles: A Case Study of High-Efficiency SLC22A5 (OCTN2)-Mediated Carnitine-Conjugated Nanoparticles for Oral Delivery of Therapeutic Drugs

Author

Jian Wang, Longfa Kou, Qiuhua Luo, Gang Wang, Chunnuan Wu, Yuqian Du, Mengchi Sun, Zhonggui He, Qiang Fu, Vadivel Ganapathy, Jia Wang, Jin Sun, and Qing Yao

Subjects

0301 basic medicine, Drug, Materials science, Paclitaxel, media_common.quotation_subject, Biomedical Engineering, Pharmaceutical Science, Administration, Oral, Biological Availability, 02 engineering and technology, Endocytosis, Intestinal absorption, Biomaterials, Lymphatic System, 03 medical and health sciences, chemistry.chemical_compound, Polylactic Acid-Polyglycolic Acid Copolymer, Carnitine, Humans, Lactic Acid, RNA, Messenger, Solute Carrier Family 22 Member 5, media_common, Ions, Photoelectron Spectroscopy, Sodium, technology, industry, and agriculture, Transporter, Membrane transport, 021001 nanoscience & nanotechnology, Molecular Docking Simulation, PLGA, 030104 developmental biology, Biochemistry, Transcytosis, chemistry, Intestinal Absorption, Docking (molecular), Biophysics, Nanoparticles, Caco-2 Cells, 0210 nano-technology, Polyglycolic Acid

Abstract

OCTN2 (SLC22A5) is a Na+ -coupled absorption transporter for l-carnitine in small intestine. This study tests the potential of this transporter for oral delivery of therapeutic drugs encapsulated in l-carnitine-conjugated poly(lactic-co-glycolic acid) (PLGA) nanoparticles (LC-PLGA NPs) and discloses the molecular mechanism for cellular endocytosis of transporter-targeting nanoparticles. Conjugation of l-carnitine to a surface of PLGA-NPs enhances the cellular uptake and intestinal absorption of encapsulated drug. In both cases, the uptake process is dependent on cotransporting ion Na+ . Computational OCTN2 docking analysis shows that the presence of Na+ is important for the formation of the energetically stable intermediate complex of transporter-Na+ -LC-PLGA NPs, which is also the first step in cellular endocytosis of nanoparticles. The transporter-mediated intestinal absorption of LC-PLGA NPs occurs via endocytosis/transcytosis rather than via the traditional transmembrane transport. The portal blood versus the lymphatic route is evaluated by the plasma appearance of the drug in the control and lymph duct-ligated rats. Absorption via the lymphatic system is the predominant route in the oral delivery of the NPs. In summary, LC-PLGA NPs can effectively target OCTN2 on the enterocytes for enhancing oral delivery of drugs and the critical role of cotransporting ions should be noticed in designing transporter-targeting nanoparticles.

Published

2017

140. Alterations of Retinal Vasculature in Cystathionine–β-Synthase Heterozygous Mice

Author

Shawn E. Bearden, Shanu Markand, Sylvia B. Smith, Jamie N. Mayo, Mohamed Al-Shabrawey, Jason J. Reynolds, Vadivel Ganapathy, and Amany Tawfik

Subjects

Pathology, medicine.medical_specialty, biology, medicine.diagnostic_test, Angiogenesis, Ischemia, Retinal, Fluorescein angiography, Occludin, medicine.disease, Cystathionine beta synthase, 3. Good health, Pathology and Forensic Medicine, Neovascularization, chemistry.chemical_compound, chemistry, Gliosis, biology.protein, medicine, medicine.symptom

Abstract

Mild to moderate hyperhomocysteinemia is prevalent in humans and is implicated in neurovascular diseases, including recently in certain retinal diseases. Herein, we used hyperhomocysteinemic mice deficient in the Cbs gene encoding cystathionine–β-synthase (Cbs+/−) to evaluate retinal vascular integrity. The Cbs+/+ (wild type) and Cbs+/− (heterozygous) mice (aged 16 to 52 weeks) were subjected to fluorescein angiography and optical coherence tomography to assess vasculature in vivo. Retinas harvested for cryosectioning or flat mount preparations were subjected to immunofluorescence microscopy to detect blood vessels (isolectin-B4), angiogenesis [anti-vascular endothelial growth factor (VEGF) and anti-CD105], gliosis [anti-glial fibrillary acidic protein (GFAP)], pericytes (anti-neural/glial antigen 2), blood-retinal barrier [anti–zonula occludens protein 1 (ZO-1) and anti-occludin], and hypoxia [anti–pimonidazole hydrochloride (Hypoxyprobe-1)]. Levels of VEGF, GFAP, ZO-1, and occludin were determined by immunoblotting. Results of these analyses showed a mild vascular phenotype in young mice, which progressed with age. Fluorescein angiography revealed progressive neovascularization and vascular leakage in Cbs+/− mice; optical coherence tomography confirmed new vessels in the vitreous by 1 year. Immunofluorescence microscopy demonstrated vascular patterns consistent with ischemia, including a capillary-free zone centrally and new vessels with capillary tufts midperipherally in older mice. This was associated with increased VEGF, CD105, and GFAP and decreased ZO-1/occludin levels in the Cbs+/− retinas. Retinal vein occlusion was observed in some Cbs+/− mouse retinas. We conclude that mild to moderate elevation of homocysteine in Cbs+/− mice is accompanied by progressive alterations in retinal vasculature characterized by ischemia, neovascularization, incompetent blood-retinal barrier, and vascular occlusion.

Published

2014

141. Abstract 1479: Bacterial dysbiosis in the mouse model of hemochromatosis: Increased risk of colitis and colitis-associated colon cancer

Author

Rao Kottapalli, Bojana Ristic, Abdul N. Hamood, Vadivel Ganapathy, and Sathish Sivaprakasam

Subjects

Cancer Research, Azoxymethane, business.industry, Colorectal cancer, Cancer, medicine.disease, medicine.disease_cause, digestive system diseases, chemistry.chemical_compound, Oncology, chemistry, medicine, Cancer research, Colitis, Carcinogenesis, Liver cancer, business, Dysbiosis, Hemochromatosis

Abstract

Hemochromatosis, an inherited iron-overload disease, causes tissue damage due to deposition of iron in toxic levels in most tissues including the liver, heart, kidney, pancreas and colon. Free iron, both in the inorganic form (i.e, non-transferrin-bound and non-ferritin-bound) and organic form (i.e. heme), facilitates Fenton reaction to generate hydroxyl radicals and to induce cellular oxidative damage that is observed in carcinogenesis. The primary site of iron deposition in hemochromatosis patients is liver, and therefore, liver cancer formation in these patients has been studied extensively. However, little is known about the iron-elicited colonic pathologies, mainly colonic inflammation and colon cancer. Here we postulate that iron overload as observed in hemochromatosis disrupts healthy colonic homeostasis and exacerbates the development of colon inflammation and colon cancer. To test our hypothesis, we examined the progression and severity of colitis and colon cancer in Hfe-/- mouse and the wild type control. Hfe-/- mouse is a model for classical hemochromatosis. Besides serum and liver, high concentrations of iron and heme deposits are found in the colon of Hfe-/- mouse. Experimental colitis was induced by administration of Dextran Sodium Sulfate (DSS) in drinking water. Colitis-associated colon cancer was initiated by the intraperitoneal injection of carcinogen, azoxymethane (AOM) and the carcinogenesis was driven by DSS administration. Colonic inflammation was more severe in the Hfe-/- mouse than in control. In addition, hemochromatosis mouse developed more and larger colonic polyps than the control group. We observed that this high susceptibility to colitis and colon cancer in Hfe-/- but not wild type mouse, lies in the differences in strains regarding the bacterial composition and colonic defense machinery. 16S ribosomal RNA sequencing of fecal bacteria revealed that the microbiota composition of Hfe-/- mouse altered to favor the pathogenic bacteria that belong to phyla Proteobacteria and TM7. In addition, the Hfe-/- proinflammatory bacteria adhered to colon and thus increased the colonic bacterial load. This phenomenon, addressed as bacterial dysbiosis, is considered a hallmark of colon inflammation and colon cancer. Furthermore, we observed that the colonic epithelial cells of Hfe-/- mouse had a lower expression of antimicrobial peptides and thus a defective first line defense against the pathogens. Finally, hemochromatosis mouse colon under inflammation released higher concentration of the pro-inflammatory cytokines that contributed to the creation of the hostile colonic environment. In summary, iron overload as seen in hemochromatosis, impairs the colonic defense machinery and it causes bacterial dysbiosis, thus providing the ideal environment for the colitis and colon cancer development. Citation Format: Bojana Ristic, Sathish Sivaprakasam, Rao Kottapalli, Abdul Hamood, Vadivel Ganapathy. Bacterial dysbiosis in the mouse model of hemochromatosis: Increased risk of colitis and colitis-associated colon cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 1479.

Published

2019

142. Abstract 3585: Amino acid transporter SLC6A14: A novel drug target for colorectal cancer

Author

Sathish Sivaprakasam, Vadivel Ganapathy, and Mohd. Omar Faruk Sikder

Subjects

chemistry.chemical_classification, Cancer Research, Arginine, Chemistry, Colorectal cancer, Cancer, medicine.disease, Amino acid, Glutamine, Oncology, Downregulation and upregulation, Cancer research, medicine, Amino acid transporter, PI3K/AKT/mTOR pathway

Abstract

SLC6A14 is a Na+/Cl− -dependent amino acid transporter capable of transporting 18 of the 20 proteinogenic amino acids, including arginine, leucine (mTOR activators) and glutamine (necessary for nucleotide biosynthesis). This transporter is expressed at basal levels in normal colon but significantly upregulated in colorectal cancer (CRC). However, the relevance of this upregulation to disease progression remains unknown. We postulated that deletion of SLC6A14 or pharmacological blockade of its function would suppress CRC by depleting amino acids and interfering with mTOR signaling selectively in tumor cells. To test this postulate, we first used Slc6a14-null mice. With two different models of spontaneous CRC (Apcmin/- and DSS/AOM), we found the tumor incidence and tumor growth were much lower in mice with Slc6a14-null background than in mice with Slc6a14. To evaluate the impact of pharmacologic blockade of the transporter on tumor growth we used a syngeneic tumor mouse model with MC-38 cells (a mouse CRC cell line); blockade of Slc6a14 with alpha-methyl tryptophan (α-MT) markedly reduced tumor growth. We then determined the transcriptome profiles of colonic epithelial cells and colonic non-epithelial cells from wild type mice and Slc6a14-null mice by RNAseq. There were hundreds of genes that were either upregulated or downregulated in the null mice. Ingenuity pathway analysis (IPA) of these data revealed predictive activation of canonical AMPK signaling pathway in colonic epithelial of Slc6a14-null mice. AMPK has anticancer activities by modulating multiple pathways including negatively regulating mTOR signaling. Moreover, upstream analysis showed predictive inactivation of two important tumor growth and survival signaling pathways ERK and EGF in the colon of the null mice. Likewise, significant upregulation of APC downregulated 1 (APCDD1) in epithelial cells in null mice implies predictive suppression of canonical Wnt signaling pathway. We also found marked differences in fecal microbiota as a result of Slc6a14 deletion. There was an increase in the relative abundance of beneficial microbiota including those capable of generating short chain fatty acids and lactic acid in null mice. We conclude that deletion of Slc6a14 or its pharmacological blockade protects against CRC by inducing amino acid starvation in tumor cells, thereby causing changes in multiple signaling pathways and in colonic microbiome. These studies identify SLC6A14 as a novel drug target for the treatment of colorectal cancer. Citation Format: Mohd Omar Faruk Sikder, Sathish Sivaprakasam, Vadivel Ganapathy. Amino acid transporter SLC6A14: A novel drug target for colorectal cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 3585.

Published

2019

143. Abstract 4357: The lactate receptor Gpr81 on non-cancer cells promotes an immunosuppressive phenotype in the tumor microenvironment

Author

Timothy Brown, Sabarish Ramachandran, Stefan Offermanns, and Vadivel Ganapathy

Subjects

Cancer Research, Oncology

Abstract

Cancer cells display a unique phenomenon in which, even in the presence of oxygen, cells switch from oxidative phosphorylation to glycolysis as the primary source of ATP with consequent production of lactic acid. This phenomenon, called the Warburg Effect, is a hallmark of cancer. Lactic acid has long been considered as the necessary end product of this metabolic switch, where lactic acid is effluxed out of tumor cells to prevent intracellular acidification. Recent evidence however suggests that lactate and the excess protons in the tumor microenvironment play an active role in tumor growth. In particular, lactate has been shown to function as an agonist for GPR81, a G-protein-coupled receptor expressed on the surface of tumor cells. This autocrine signaling of lactate promotes tumor growth and metastasis, as well as angiogenesis and immune evasion. The present study assesses whether tumor cell-derived lactate has any paracrine role via its receptor in non-cancer cells present in the tumor microenvironment. We generated MMTV-PyMT-Tg mice, a spontaneous model for breast cancer, on Gpr81+/+ and Gpr81-/- backgrounds. The absence of Gpr81 reduced the mammary tumor incidence, delayed mammary tumor progression, and reduced lung metastasis. These data demonstrate the essential role of GPR81 in breast cancer growth and metastasis, but does not differentiate between Gpr81 in tumor cells versus Gpr81 in the tumor microenvironment. We then used the syngeneic transplant of the mouse mammary tumor cell line AT-3 into the mammary fat pads of wild type and Gpr81-/- mice to assess the involvement of Gpr81 in the microenvironment. AT-3 cells are negative for Gpr81, and therefore our model limits Gpr81 expression to non-tumor cells in the host mouse. We found the growth of transplanted tumor cells was significantly reduced in Gpr81-/- mice than in wild type mice. Preliminary RNA-sequencing transcriptome analysis of AT-3 tumors suggest an immunosuppressive function of Gpr81, where tumors grown in a Gpr81-/- background have much stronger gene expression profiles in T-cell signaling pathways. Specifically, AT-3 tumors grown in Gpr81-/- host express significantly higher levels of genes that are specific for T cells and antigen-presenting cells such as MHC-II complex molecules, T-cell co-stimulatory molecules, and transmembrane CD8. It is well established that tumor-cell derived lactate promotes tumor growth in an autocrine manner via Gpr81 expressed on tumor cells; our studies extend the tumor-promoting role of lactate beyond this autocrine function to include paracrine signaling via Gpr81 expressed on immune cells and possibly other cell types in the tumor microenvironment. Citation Format: Timothy Brown, Sabarish Ramachandran, Stefan Offermanns, Vadivel Ganapathy. The lactate receptor Gpr81 on non-cancer cells promotes an immunosuppressive phenotype in the tumor microenvironment [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 4357.

Published

2019

144. Abstract 5735: Amino acid transporter SLC6A14: A novel drug target for colorectal cancer and colitis and its transcriptional regulation by TCF4/beta-catenin pathway

Author

Sikder, Mohd Omar, primary, Sivaprakasam, Sathish, additional, and Vadivel, Ganapathy, additional

Published

2018

145. Transporters and receptors for short-chain fatty acids as the molecular link between colonic bacteria and the host

Author

Vadivel Ganapathy, Puttur D. Prasad, Nagendra Singh, Muthusamy Thangaraju, and Pamela M. Martin

Subjects

Pharmacology, chemistry.chemical_classification, Bacteria, Colon, Host (biology), Microbial metabolism, Membrane Transport Proteins, Receptors, Cell Surface, Inflammation, Transporter, Butyrate, Biology, Fatty Acids, Volatile, Biochemistry, chemistry, Drug Discovery, medicine, Propionate, Animals, Humans, Fermentation, medicine.symptom, Receptor

Abstract

The mutually beneficial relationship between colonic bacteria and the host has been recognized but the molecular aspects of the relationship remain poorly understood. Dietary fiber is critical to this relationship. The short-chain fatty acids acetate, propionate and butyrate, generated by bacterial fermentation of dietary fiber, serve as messengers between colonic bacteria and the host. The beneficial effects of these bacterial metabolites in colon include, but are not limited to, suppression of inflammation and prevention of cancer. Recent studies have identified the plasma membrane transporter SLC5A8 and the cell-surface receptors GPR109A and GPR43 as essential for the biologic effects of short-chain fatty acids in colon. These three proteins coded by the host genome provide the molecular link between colonic bacteria and the host.

Published

2013

146. Betaine acts on a ligand-gated ion channel in the nervous system of the nematode C. elegans

Author

Erik M. Jorgensen, Vadivel Ganapathy, Guoliang Jiang, Kenneth J. Murfitt, Aude S. Peden, Eric A. Miska, Julian L. Griffin, You Jun Fei, Patrick Mac, and Cecilia Castro

Subjects

1702 Cognitive Sciences, Receptors, Nicotinic, Betaine transporter, Nervous System, Membrane Potentials, Animals, Genetically Modified, chemistry.chemical_compound, 0302 clinical medicine, Betaine, Body Size, Caenorhabditis elegans, chemistry.chemical_classification, 0303 health sciences, Neurotransmitter Agents, biology, General Neuroscience, Antinematodal Agents, Gene Expression Regulation, Developmental, Amino acid, Biochemistry, Osmolyte, Larva, C. elegans, Ligand-gated ion channel, Signal transduction, phospholipase Cβ, Ion Channel Gating, Mechanoreceptors, Allosteric modulator, betaine transporter, Green Fluorescent Proteins, Article, 03 medical and health sciences, Animals, Humans, Caenorhabditis elegans Proteins, 030304 developmental biology, ACR-23, egl-8, Neurology & Neurosurgery, Dose-Response Relationship, Drug, Ligand-Gated Ion Channels, biology.organism_classification, SNF-3, betaine receptor, chemistry, 1701 Psychology, Mutation, 1109 Neurosciences, 030217 neurology & neurosurgery

Abstract

Prior to the advent of synthetic nematocides, natural products such as seaweed were used to control nematode infestations. The nematocidal agent in seaweed is betaine, an amino acid that functions as an osmolyte and methyl donor. However, the molecular mechanisms of betaine toxicity are unknown. We identified the betaine transporter SNF-3 and the betaine receptor ACR-23 in the nematode C. elegans. Mutating snf-3 in a sensitized background caused the worms to be hypercontracted and paralyzed, presumably as a result of excess extracellular betaine. These behavioral defects were suppressed by mutations in acr-23, which encodes a ligand-gated cation channel of the cys-loop family. ACR-23 was activated by betaine and functioned in the mechanosensory neurons to maintain basal levels of locomotion. However, overactivation of the receptor by excess betaine or by the allosteric modulator monepantel resulted in hypercontraction and death of the nematode. Thus, monepantel targets a betaine signaling pathway in nematodes.

Published

2013

147. Molecular Mechanism of SLC5A8 Inactivation in Breast Cancer

Author

Rajneesh Pathania, Vadivel Ganapathy, Patricia V. Schoenlein, Ellappan Babu, Puttur D. Prasad, Thomas Boettger, Muthusamy Thangaraju, Sabarish Ramachandran, Sylvia B. Smith, Lesleyann Hawthorn, Sudha Ananth, Selvakumar Elangovan, Sonne R. Srinivas, and Ravi Padia

Subjects

DNA (Cytosine-5-)-Methyltransferase 1, Male, Monocarboxylic Acid Transporters, Genetically modified mouse, Carcinogenesis, Immunoblotting, Transplantation, Heterologous, Mice, Nude, Breast Neoplasms, Mice, Transgenic, Biology, medicine.disease_cause, Cell Line, Proto-Oncogene Proteins p21(ras), Mice, RNA interference, Cell Line, Tumor, medicine, Animals, Humans, Gene silencing, DNA (Cytosine-5-)-Methyltransferases, HRAS, Cation Transport Proteins, Molecular Biology, Mice, Knockout, Mammary tumor, Reverse Transcriptase Polymerase Chain Reaction, Cancer, Articles, Cell Biology, HCT116 Cells, medicine.disease, Gene Expression Regulation, Neoplastic, Mutation, DNA methylation, MCF-7 Cells, Cancer research, Female, RNA Interference

Abstract

SLC5A8 is a putative tumor suppressor that is inactivated in more than 10 different types of cancer, but neither the oncogenic signaling responsible for SLC5A8 inactivation nor the functional relevance of SLC5A8 loss to tumor growth has been elucidated. Here, we identify oncogenic HRAS (HRAS(G12V)) as a potent mediator of SLC5A8 silencing in human nontransformed normal mammary epithelial cell lines and in mouse mammary tumors through DNMT1. Further, we demonstrate that loss of Slc5a8 increases cancer-initiating stem cell formation and promotes mammary tumorigenesis and lung metastasis in an HRAS-driven murine model of mammary tumors. Mammary-gland-specific overexpression of Slc5a8 (mouse mammary tumor virus-Slc5a8 transgenic mice), as well as induction of endogenous Slc5a8 in mice with inhibitors of DNA methylation, protects against HRAS-driven mammary tumors. Collectively, our results provide the tumor-suppressive role of SLC5A8 and identify the oncogenic HRAS as a mediator of tumor-associated silencing of this tumor suppressor in mammary glands. These findings suggest that pharmacological approaches to reactivate SLC5A8 expression in tumor cells have potential as a novel therapeutic strategy for breast cancer treatment.

Published

2013

148. Hyperhomocysteinemia is detrimental to pregnancy in mice and is associated with preterm birth

Author

Vadivel Ganapathy, Srinivas Sonne, Scott A. Barman, Puttur D. Prasad, Shu Zhu, Sylvia B. Smith, Vinod K. Bhalla, Stefan Offermanns, Richard E. White, and T. M. Newman

Subjects

medicine.medical_specialty, Hyperhomocysteinemia, Niacin receptor, Homocysteine, Prostaglandin E2, Placenta, Uterus, Cystathionine beta-Synthase, Receptors, Nicotinic, Dinoprostone, Cell Line, Mice, chemistry.chemical_compound, Pregnancy, Internal medicine, medicine, Animals, Humans, Cyclooxygenase-2, Large-Conductance Calcium-Activated Potassium Channel alpha Subunits, Molecular Biology, Cyclooxygenase 2 Inhibitors, biology, Myometrium, Trophoblast, Preterm birth, medicine.disease, Cystathionine beta synthase, Oxytocin receptor, Trophoblasts, Up-Regulation, Mice, Inbred C57BL, Pregnancy Complications, Endocrinology, medicine.anatomical_structure, chemistry, Cyclooxygenase 2, Receptors, Oxytocin, biology.protein, Premature Birth, Molecular Medicine, Female, Muscle Contraction

Abstract

Elevated levels of homocysteine produce detrimental effects in humans but its role in preterm birth is not known. Here we used a mouse model of hyperhomocysteinemia to examine the relevance of homocysteine to preterm birth. The mouse carries a heterozygous deletion of cystathionine β-synthase (Cbs+/−). Gestational period was monitored in wild type and Cbs+/− female mice. Mouse uterine and placental tissues, human primary trophoblast cells, and human myometrial and placental cell lines were used to determine the influence of homocysteine on expression of specific genes in vitro. The activity of BKCa channel in the myometrial cell line was monitored using the patch-clamp technique. We found that hyperhomocysteinemia had detrimental effects on pregnancy and induced preterm birth in mice. Homocysteine increased the expression of oxytocin receptor and Cox-2 as well as PGE2 production in uterus and placenta, and initiated premature uterine contraction. A Cox-2 inhibitor reversed these effects. Gpr109a, a receptor for niacin, induced Cox-2 in uterus. Homocysteine upregulated GPR109A and suppressed BKCa channel activity in human myometrial cells. Deletion of Gpr109a in Cbs+/− mice reversed premature birth. We conclude that hyperhomocysteinemia causes preterm birth in mice through upregulation of the Gpr109a/Cox-2/PGE2 axis and that pharmacological blockade of Gpr109a may have potential in prevention of preterm birth.

Published

2013

149. Enzymes involved in l-carnitine biosynthesis are expressed by small intestinal enterocytes in mice: Implications for gut health

Author

Prem S. Shekhawat, Srinivas Sonne, Dietrich Matern, A. Lee Carter, and Vadivel Ganapathy

Subjects

gamma-Butyrobetaine Dioxygenase, Gene Expression, Biology, Real-Time Polymerase Chain Reaction, Article, Mixed Function Oxygenases, Mice, Intestinal mucosa, Carnitine, Intestine, Small, medicine, Animals, Carnitine palmitoyltransferase II, Intestinal Mucosa, In Situ Hybridization, Glycine Hydroxymethyltransferase, Mice, Inbred C3H, Gastroenterology, General Medicine, Aldehyde Oxidoreductases, Intestinal epithelium, Molecular biology, Small intestine, Enterocytes, medicine.anatomical_structure, Hypoxanthine-guanine phosphoribosyltransferase, Carnitine biosynthesis, Gamma-butyrobetaine dioxygenase, medicine.drug

Abstract

Background: Carnitine is essential for mitochondrial β-oxidation of long-chain fatty acids. Deficiency of carnitine leads to severe gut atrophy, ulceration and inflammation in animal models of carnitine deficiency. Genetic studies in large populations have linked mutations in the carnitine transporters OCTN1 and OCTN2 with Crohn's disease (CD), while other studies at the same time have failed to show a similar association and report normal serum carnitine levels in CD patients. Methods: In this report, we have studied the expression of carnitine-synthesizing enzymes in intestinal epithelial cells to determine the capability of these cells to synthesize carnitine de novo . We studied expression of five enzymes involved in carnitine biosynthesis, namely 6- N -trimethyllysine dioxygenase (TMLD), 4-trimethylaminobutyraldehyde dehydrogenase (TMABADH), serine hydroxymethyltransferase 1 and 2 (SHMT1 and 2) and γ-butyrobetaine hydroxylase (BBH) by real-time PCR in mice (C3H strain). We also measured activity of γ-BBH in the intestine using an ex vivo assay and localized its expression by in situ hybridization. Results: Our investigations show that mouse intestinal epithelium expresses all five enzymes required for de novo carnitine biosynthesis; the expression is localized mainly in villous surface epithelial cells throughout the intestine. The final rate-limiting enzyme γ-BBH is highly active in the small intestine; its activity was 9.7 ± 3.5 pmol/mg/min, compared to 22.7 ± 7.3 pmol/mg/min in the liver. Conclusions: We conclude that mouse gut epithelium is able to synthesize carnitine de novo . This capacity to synthesize carnitine in the intestine may play an important role in gut health and can help explain lack of clinical carnitine deficiency signs in subjects with mutations with OCTN transporters. * Abbreviations: : TMLD : 6- N -trimethyllysine dioxygenase TMABA : 4-trimethylaminobutyraldehyde HTMLA : β-hydroxy-e- N -trimethyllysine aldolase SHMT1 and 2 : serine hydroxymethyltransferase 1 and 2 TMABA-DH : TMABA dehydrogenase γ-BBH : γ-butyrobetaine hydroxylase OCTN : organic cation transporter novel HPRT : hypoxanthine phosphoribosyl transferase CD : Crohn's disease IBD : inflammatory bowel disease.

Published

2013

150. LactobacillusGG and Tributyrin Supplementation Reduce Antibiotic-Induced Intestinal Injury

Author

Laura E. Nagy, Gail A. Cresci, and Vadivel Ganapathy

Subjects

medicine.medical_specialty, Lactobacillus GG, Tributyrin, medicine.drug_class, medicine.medical_treatment, Antibiotics, Gene Expression, Medicine (miscellaneous), Butyrate, Gut flora, digestive system, Article, Microbiology, Mice, chemistry.chemical_compound, Internal medicine, Gene expression, medicine, Animals, RNA, Messenger, Intestinal Mucosa, Saline, Triglycerides, Tight Junction Proteins, Nutrition and Dietetics, biology, Microbiota, Probiotics, Membrane Proteins, biology.organism_classification, Anti-Bacterial Agents, Intestines, Mice, Inbred C57BL, Butyrates, Intestinal Diseases, Lactobacillus, Diarrhea, Endocrinology, chemistry, Dysbiosis, Female, medicine.symptom

Abstract

Antibiotic therapy negatively alters the gut microbiota. Lactobacillus GG (LGG) decreases antibiotic-associated diarrhea (AAD) symptoms, but the mechanisms are unknown. Butyrate has beneficial effects on gut health. Altered intestinal gene expression occurs in the absence of gut microbiota. We hypothesized that antibiotic-induced changes in gut microbiota reduce butyrate production, varying genes involved with gut barrier integrity and water and electrolyte absorption, lending to AAD, and that simultaneous supplementation with LGG and/or tributyrin would prevent these changes.C57BL/6 mice aged 6-8 weeks received a chow diet while divided into 8 treatment groups (± saline, ± LGG, ± tributyrin, or both). Mice received treatments orally for 7 days with ± broad-spectrum antibiotics. Water intake was recorded daily and body weight was measured. Intestine tissue samples were obtained and analyzed for expression of genes and proteins involved with water and electrolyte absorption, butyrate transport, and gut integrity via polymerase chain reaction and immunohistochemistry.Antibiotics decreased messenger RNA (mRNA) expression (butyrate transporter and receptor, Na(+)/H(+) exchanger, Cl(-)/HCO3 (-), and a water channel) and protein expression (butyrate transporter, Na(+)/H(+) exchanger, and tight junction proteins) in the intestinal tract. LGG and/or tributyrin supplementation maintained intestinal mRNA expression to that of the control animals, and tributyrin maintained intestinal protein intensity expression to that of control animals.Broad-spectrum antibiotics decrease expression of anion exchangers, butyrate transporter and receptor, and tight junction proteins in mouse intestine. Simultaneous oral supplementation with LGG and/or tributyrin minimizes these losses. Optimizing intestinal health with LGG and/or tributyrin may offer a preventative therapy for AAD.

Published

2013