Your search keyword '"Orotic Acid toxicity"' showing total 55 results

1. The pharmacokinetics of mycophenolic acid in rats with orotic acid induced nonalcoholic fatty liver disease.

Author

Subali D, Kwon MH, Bang WS, and Kang HE

Subjects

Animals, Male, Mycophenolic Acid administration & dosage, Non-alcoholic Fatty Liver Disease chemically induced, Non-alcoholic Fatty Liver Disease metabolism, Rats, Rats, Sprague-Dawley, Tissue Distribution, Glucuronides pharmacokinetics, Microsomes, Liver metabolism, Mycophenolic Acid analogs & derivatives, Mycophenolic Acid pharmacokinetics, Non-alcoholic Fatty Liver Disease pathology, Orotic Acid toxicity

Abstract

Post-transplantation nonalcoholic fatty liver disease (NAFLD) is common in liver transplant recipients. Changes in the expression levels and activities of drug-metabolizing enzymes and drug transporters have been reported in patients with NAFLD and relevant rodent models. Here, we evaluated whether the pharmacokinetics of mycophenolic acid (MPA), an immunosuppressant, would be altered in rats with NAFLD. NAFLD was induced by feeding a diet containing 1% ( w / w ) orotic acid for 20 days. The extent of hepatic glucuronidation of MPA to a major metabolite, mycophenolic acid-7- O -glucuronide (MPAG), did not differ between rats with NAFLD and controls. The expression levels of hepatic multidrug resistance-associated protein 2, responsible for biliary excretion of MPAG, were comparable in rats with NAFLD and controls; the biliary excretion of MPAG was also similar in the two groups. Compared with control rats, rats with NAFLD did not exhibit significant changes in the areas under the plasma concentration - time curves of MPA or MPAG after intravenous (5 mg/kg) or oral (10 mg/kg) administration of MPA. However, delayed oral absorption of MPA was observed in rats with NAFLD compared with controls; the MPA and MPAG peak plasma concentrations fell significantly and the times to achieve them were prolonged following oral administration of MPA.

Published

2020

2. Regulation effects of rosemary (Rosmarinus officinalis Linn.) on hepatic lipid metabolism in OA induced NAFLD rats.

Author

Wang SJ, Chen Q, Liu MY, Yu HY, Xu JQ, Wu JQ, Zhang Y, and Wang T

Subjects

Abietanes chemistry, Abietanes pharmacology, Animals, Cinnamates chemistry, Cinnamates pharmacology, Depsides chemistry, Depsides pharmacology, Hep G2 Cells, Humans, Lipid Metabolism drug effects, Male, Plant Extracts chemistry, Rats, Rats, Sprague-Dawley, Rosmarinic Acid, Non-alcoholic Fatty Liver Disease drug therapy, Orotic Acid toxicity, Plant Extracts pharmacology, Rosmarinus chemistry

Abstract

Rosmarinus officinalis Linn. is a kind of medicinal and edible homologous plant, which is popular in the Mediterranean region with a significant effect on mind tranquilization, anti-oxidation, and metabolic improvement. However, the hypolipidemic effects and mechanism of rosemary ethanol extract (RO) and their metabolites are less known. In this study, the hypolipidemic effects of RO and its active compounds were clarified. The results showed that RO, rosmarinic acid (RA) and carnosic acid (CA) significantly reduced the contents of liver triglyceride (TG), total cholesterol (TC), free fatty acids (FFA) and improved cell hypertrophy, vacuolation, and cell necrosis in the liver of orotic acid induced non-alcoholic fatty liver disease (NAFLD) model rats. The mechanism and related pathways of RO and its main metabolites against lipid disorder were related to the up-regulation of the phosphorylation of adenosine 5'-monophosphate(AMP)-activated protein kinase (AMPK) and the inhibition of the sterol regulatory element binding protein-1c (SREBP-1c) cracking into the nucleus, following the down-regulation of fatty acid synthesis. In conclusion, our study demonstrates that RA and CA are active substances of RO, and provides scientific evidence to support functional food product development for improving NAFLD.

Published

2019

3. Long-term fatty liver-induced insulin resistance in orotic acid-induced nonalcoholic fatty liver rats.

Author

Han X, Liu C, Xue Y, Wang J, Xue C, Yanagita T, Gao X, and Wang Y

Subjects

Animals, Gene Expression, Gluconeogenesis, Glucose Tolerance Test, Insulin blood, Male, Non-alcoholic Fatty Liver Disease chemically induced, Rats, Rats, Wistar, Signal Transduction, Up-Regulation, Insulin Resistance, Non-alcoholic Fatty Liver Disease physiopathology, Orotic Acid toxicity

Abstract

We investigated whether fatty liver preceded insulin resistance or vice versa using a long-term orotic acid (OA)-induced nonalcoholic fatty liver disease (NAFLD) model without the confounding effects of obesity and hyperlipidemia and explored the role of the liver in insulin resistance. Male Wistar rats were fed with or without OA supplementation for 30, 60, and 90 days. The NAFLD group showed increased liver lipid at 30, 60, and 90 days; glucose intolerance was noted at 60 and 90 days. Furthermore, partial liver proteins and gene expressions related to upstream signaling of insulin were decreased. However, the liver glycogen content was elevated, and gluconeogenesis genes expressions were obviously decreased at 90 days. The occurrence of fatty liver preceded insulin resistance in OA-induced NAFLD without the interference of obesity and hyperlipidemia, and hepatic insulin resistance may not play a conclusive role in insulin resistance in this model.

Published

2016

4. pyrF as a Counterselectable Marker for Unmarked Genetic Manipulations in Treponema denticola.

Author

Kurniyati K and Li C

Subjects

Drug Resistance, Bacterial, Orotic Acid analogs & derivatives, Orotic Acid toxicity, Treponema denticola drug effects, Treponema denticola growth & development, Gene Knockout Techniques methods, Genetics, Microbial methods, Orotidine-5'-Phosphate Decarboxylase genetics, Selection, Genetic, Treponema denticola genetics

Abstract

The pathophysiology of Treponema denticola, an oral pathogen associated with both periodontal and endodontic infections, is poorly understood due to its fastidious growth and recalcitrance to genetic manipulations. Counterselectable markers are instrumental in constructing clean and unmarked mutations in bacteria. Here, we demonstrate that pyrF, a gene encoding orotidine-5'-monophosphate decarboxylase, can be used as a counterselectable marker in T. denticola to construct marker-free mutants. T. denticola is susceptible to 5-fluoroorotic acid (5-FOA). To establish a pyrF-based counterselectable knockout system in T. denticola, the pyrF gene was deleted. The deletion conferred resistance to 5-FOA in T. denticola. Next, a single-crossover mutant was constructed by reintroducing pyrF along with a gentamicin resistance gene (aacC1) back into the chromosome of the pyrF mutant at the locus of choice. In this study, we chose flgE, a flagellar hook gene that is located within a large polycistronic motility gene operon, as our target gene. The obtained single-crossover mutant (named FlgE(in)) regained the susceptibility to 5-FOA. Finally, FlgE(in) was plated on solid agar containing 5-FOA. Numerous colonies of the 5-FOA-resistant mutant (named FlgE(out)) were obtained and characterized by PCR and Southern blotting analyses. The results showed that the flgE gene was deleted and FlgE(out) was free of selection markers (i.e., pyrF and aacC1). Compared to previously constructed flgE mutants that contain an antibiotic selection marker, the deletion of flgE in FlgE(out) has no polar effect on its downstream gene expression. The system developed here will provide us with a new tool for investigating the genetics and pathogenicity of T. denticola., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2015

5. Orotic acid induces hypertension associated with impaired endothelial nitric oxide synthesis.

Author

Choi YJ, Yoon Y, Lee KY, Kang YP, Lim DK, Kwon SW, Kang KW, Lee SM, and Lee BH

Subjects

Human Umbilical Vein Endothelial Cells, Humans, Insulin pharmacology, Metformin pharmacology, Nitric Oxide biosynthesis, Nitric Oxide Synthase Type III metabolism, Phosphorylation, Hypertension chemically induced, Nitric Oxide Synthase Type III biosynthesis, Orotic Acid toxicity

Abstract

Orotic acid (OA) is an intermediate of pyrimidine nucleotide biosynthesis. Hereditary deficiencies in some enzymes associated with pyrimidine synthesis or the urea cycle induce OA accumulation, resulting in orotic aciduria. A link between patients with orotic aciduria and hypertension has been reported; however, the molecular mechanisms remain elusive. In this study, to elucidate the role of OA in vascular insulin resistance, we investigated whether OA induced endothelial dysfunction and hypertension. OA inhibited insulin- or metformin-stimulated nitric oxide (NO) production and endothelial NO synthase (eNOS) phosphorylation in human umbilical vein endothelial cells. A decreased insulin response by OA was mediated by impairment of the insulin-stimulated phosphoinositide 3-kinase (PI3K)-protein kinase B (PKB/Akt) signaling pathway in cells overexpressing the p110-PI3K catalytic subunit. Impaired effects of metformin on eNOS phosphorylation and NO production were reversed in cells transfected with constitutively active AMP-activated protein kinase. Moreover, experimental induction of orotic aciduria in rats caused insulin resistance, measured as a 125% increase in the homeostasis model assessment, and hypertension, measured as a 25% increase in systolic blood pressure. OA increased the plasma concentration of endothelin-1 by 201% and significantly inhibited insulin- or metformin-induced vasodilation. A compromised insulin or metformin response on the Akt/eNOS and AMP-activated protein kinase/eNOS pathway was observed in aortic rings of OA-fed rats. Taken together, we showed that OA induces endothelial dysfunction by contributing to vascular and systemic insulin resistance that affects insulin- or metformin-induced NO production, leading to the development of hypertension., (© The Author 2015. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2015

6. Improvement of ClosTron for successive gene disruption in Clostridium cellulolyticum using a pyrF-based screening system.

Author

Cui GZ, Zhang J, Hong W, Xu C, Feng Y, Cui Q, and Liu YJ

Subjects

Orotic Acid analogs & derivatives, Orotic Acid toxicity, Orotidine-5'-Phosphate Decarboxylase metabolism, Plasmids, Clostridium cellulolyticum genetics, Gene Knockout Techniques, Orotidine-5'-Phosphate Decarboxylase genetics, Selection, Genetic

Abstract

Clostridium includes a number of species, such as thermophilic Clostridium thermocellum and mesophilic Clostridium cellulolyticum, producing biofuels and chemicals from lignocellulose, while genetic engineering is necessary to improve wild-type strains to fulfill the requirement of industrialization. ClosTron system is widely used in the gene targeting of Clostridium because of its high efficiency and operability. However, the targetron plasmid present in cell hinders the successive gene disruption. To solve this problem, a pyrF-based screening system was developed and implemented in C. cellulolyticum strain H10 in this study for efficient targetron plasmid curing. The screening system was composed of a pyrF-deleted cell chassis (H10ΔpyrF) constructed via homologous recombination and a PyrF expression cassette located in a targetron plasmid containing an erythromycin resistance gene. With the screening system, the gene targeting could be achieved following a two-step procedure, including the first step of gene disruption through targetron transformation and erythromycin selection and the second step of plasmid curing by screening with 5-fluoroorotic acid. To test the developed screening system, successive inactivation of the major cellulosomal exocellulase Cel48F and the scaffoldin protein CipC was achieved in C. cellulolyticum, and the efficient plasmid curing was confirmed. With the assistance of the pyrF-based screening system, the targetron plasmid-cured colonies can be rapidly selected by one-plate screening instead of traditional days' unguaranteed screening, and the successive gene disruption becomes accomplishable with ClosTron system with improved stability and efficiency, which may promote the metabolic engineering of Clostridium species aiming at enhanced production of biofuels and chemicals.

Published

2014

7. Counterselection system for Geobacillus kaustophilus HTA426 through disruption of pyrF and pyrR.

Author

Suzuki H, Murakami A, and Yoshida K

Subjects

Drug Resistance, Bacterial, Orotic Acid analogs & derivatives, Orotic Acid toxicity, Recombination, Genetic, Uracil metabolism, Bacterial Proteins genetics, Gene Knockout Techniques, Genetics, Microbial methods, Geobacillus isolation & purification, Molecular Biology methods, Selection, Genetic

Abstract

Counterselection systems facilitate marker-free genetic modifications in microbes by enabling positive selections for both the introduction of a marker gene into the microbe and elimination of the marker from the microbe. Here we report a counterselection system for Geobacillus kaustophilus HTA426, established through simultaneous disruption of the pyrF and pyrR genes. The pyrF gene, essential for pyrimidine biosynthesis and metabolization of 5-fluoroorotic acid (5-FOA) to toxic metabolites, was disrupted by homologous recombination. The resultant MK54 strain (ΔpyrF) was auxotrophic for uracil and resistant to 5-FOA. MK54 complemented with pyrF was prototrophic for uracil but insensitive to 5-FOA in the presence of uracil. To confer 5-FOA sensitivity, the pyrR gene encoding an attenuator to repress pyrimidine biosynthesis by sensing uracil derivatives was disrupted. The resultant MK72 strain (ΔpyrF ΔpyrR) was auxotrophic for uracil and resistant to 5-FOA. MK72 complemented with pyrF was prototrophic for uracil and 5-FOA sensitive even in the presence of uracil. The results suggested that pyrF could serve as a counterselection marker in MK72, which was demonstrated by efficient marker-free integrations of heterologous β-galactosidase and α-amylase genes. The integrated genes were functionally expressed in G. kaustophilus and conferred new functions on the thermophile. This report describes the first establishment of a pyrF-based counterselection system in a Bacillus-related bacterium, along with the first demonstration of homologous recombination and heterologous gene expression in G. kaustophilus. Our results also suggest a new strategy for establishment of counterselection systems.

Published

2012

8. Proliferating effect of orotic acid through mTORC1 activation mediated by negative regulation of AMPK in SK-Hep1 hepatocellular carcinoma cells.

Author

Jung EJ, Lee KY, and Lee BH

Subjects

AMP-Activated Protein Kinases genetics, Aminoimidazole Carboxamide analogs & derivatives, Aminoimidazole Carboxamide metabolism, Apoptosis drug effects, Blotting, Western, Cell Cycle drug effects, Cell Line, Tumor, Humans, Mechanistic Target of Rapamycin Complex 1, Multiprotein Complexes, Phosphorylation, Proteins genetics, Ribonucleotides genetics, Ribonucleotides metabolism, Signal Transduction, TOR Serine-Threonine Kinases, AMP-Activated Protein Kinases metabolism, Cell Proliferation drug effects, Orotic Acid toxicity, Proteins metabolism

Abstract

Orotic acid (OA) is a tumor promoter of experimental liver carcinogenesis initiated by DNA reactive carcinogens, the molecular mechanisms of which have not been fully elucidated. OA increases cell proliferation and decreases apoptosis in serum-starved SK-Hep1 hepatocellular carcinoma cells, which may ascribe to the inhibition of AMP-activated protein kinase (AMPK) phosphorylation and thus activation of mammalian target of rapamycin complex 1 (mTORC1). The effects of OA on mTORC1 activation, cell proliferation, and cell-cycle progression to S and G2/M phases were completely reversed by rapamycin. Activation of AMPK by a constitutively active mutant or aminoimidazole carboxamide ribonucleotide (AICAR) rescued the effects of OA. In conclusion, OA increases the proliferation and decreases the starvation-induced apoptosis of SK-Hep1 cells via mTORC1 activation mediated by negative regulation of AMPK.

Published

2012

9. Study on possible mechanism of orotic acid-induced fatty liver in rats.

Author

Wang YM, Hu XQ, Xue Y, Li ZJ, Yanagita T, and Xue CH

Subjects

Animals, Carnitine O-Palmitoyltransferase metabolism, Cholesterol blood, Cholesterol, VLDL blood, Cholesterol, VLDL metabolism, Diet, Fatty Acid Synthases genetics, Fatty Liver pathology, Liver pathology, Male, Phospholipids blood, RNA, Messenger metabolism, Rats, Rats, Wistar, Sterol Regulatory Element Binding Protein 1 genetics, Triglycerides blood, Up-Regulation, Fatty Acid Synthases metabolism, Fatty Liver chemically induced, Lipid Metabolism, Liver metabolism, Orotic Acid toxicity

Abstract

Objective: The aim of this study was to investigate the possible mechanism of orotic acid-induced fatty liver in rats., Methods: Rats were randomly divided into two groups and fed an AIN-93 diet with 1% orotic acid or without orotic acid for 10 d. Hepatic lipid concentrations, such as triacylglycerol, total cholesterol, and phospholipids, were examined. To clarify the mechanism of orotic acid-induced fatty liver, hepatic enzyme activities and mRNA levels of key enzymes related in lipid metabolism and hepatic gene expression of transcription factors were determined., Results: Orotic acid administration significantly increased hepatic triacylglycerol concentration. The activity and mRNA level of fatty acid synthase were obviously upregulated by orotic acid treatment, whereas the activities and mRNA concentrations of carnitine palmitoyl transferase and microsomal triacylglycerol transfer protein were significantly depressed. Furthermore, orotic acid stimulated the mRNA expression of sterol regulatory element binding protein-1c but did not alter the mRNA concentration of peroxisome proliferator-activated receptor-α in the liver., Conclusion: The stimulation of triacylglycerol synthesis induced by orotic acid is mainly caused by enhancement of sterol regulatory element binding protein-1c and its target gene involved in fatty acid biosynthesis. In contrast, the inhibition of fatty acid β-oxidation and very-low-density lipoprotein secretion were related to the observed lipid accumulation., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

10. Use of the pyrG gene as a food-grade selection marker in Monascus.

Author

Wang BH, Xu Y, and Li YP

Subjects

Aspergillus flavus enzymology, Aspergillus flavus genetics, Cloning, Molecular, DNA Primers genetics, DNA, Fungal chemistry, DNA, Fungal genetics, Fungal Proteins genetics, Molecular Sequence Data, Monascus isolation & purification, Monascus radiation effects, Mutagenesis, Orotic Acid analogs & derivatives, Orotic Acid toxicity, Orotidine-5'-Phosphate Decarboxylase deficiency, Orotidine-5'-Phosphate Decarboxylase genetics, Plasmids, Point Mutation, Polymerase Chain Reaction methods, Selection, Genetic, Sequence Analysis, DNA, Sequence Homology, Amino Acid, Ultraviolet Rays, Fungal Proteins metabolism, Genetic Engineering methods, Genetic Vectors, Genetics, Microbial methods, Monascus enzymology, Monascus genetics, Orotidine-5'-Phosphate Decarboxylase metabolism

Abstract

Ma-pyrG was cloned from Monascus aurantiacus AS3.4384 using degenerate PCR with primers designed with an algorithm called CODEHOP, and its complete sequence was obtained by a PCR-based strategy for screening a Monascus fosmid library. Ma-pyrG encodes orotidine-5'-phosphate decarboxylase (OMPdecase), a 283-aminoacid protein with 81% sequence identity to that from Aspergillus flavus NRRL 3357. A pyrG mutant strain from M. aurantiacus AS3.4384, named UM28, was isolated by resistance to 5-fluoroorotic acid after UV mutagenesis. Sequence analysis of this mutated gene revealed that it contained a point mutation at nucleotide position +220. Plasmid pGFP-pyrG, bearing the green fluorescent protein gene (GFP) as a model gene and Ma-pyrG as a selection marker, were constructed. pGFP-pyrG were successfully transformed into UM28 by using the PEG method.

Published

2010

11. Development of pyrF-based genetic system for targeted gene deletion in Clostridium thermocellum and creation of a pta mutant.

Author

Tripathi SA, Olson DG, Argyros DA, Miller BB, Barrett TF, Murphy DM, McCool JD, Warner AK, Rajgarhia VB, Lynd LR, Hogsett DA, and Caiazza NC

Subjects

Bacterial Proteins genetics, Carboxylic Acids metabolism, Metabolic Networks and Pathways genetics, Orotic Acid analogs & derivatives, Orotic Acid toxicity, Phosphate Acetyltransferase genetics, Plasmids, Selection, Genetic, Clostridium thermocellum genetics, Gene Deletion, Gene Knockout Techniques methods, Molecular Biology methods

Abstract

We report development of a genetic system for making targeted gene knockouts in Clostridium thermocellum, a thermophilic anaerobic bacterium that rapidly solubilizes cellulose. A toxic uracil analog, 5-fluoroorotic acid (5-FOA), was used to select for deletion of the pyrF gene. The ΔpyrF strain is a uracil auxotroph that could be restored to a prototroph via ectopic expression of pyrF from a plasmid, providing a positive genetic selection. Furthermore, 5-FOA was used to select against plasmid-expressed pyrF, creating a negative selection for plasmid loss. This technology was used to delete a gene involved in organic acid production, namely pta, which encodes the enzyme phosphotransacetylase. The C. thermocellum Δpta strain did not produce acetate. These results are the first examples of targeted homologous recombination and metabolic engineering in C. thermocellum, a microbe that holds an exciting and promising future in the biofuel industry and development of sustainable energy resources.

Published

2010

12. Comparative in vitro toxicity of seven zinc-salts towards neuronal PC12 cells.

Author

Pavlica S, Gaunitz F, and Gebhardt R

Subjects

Adenosine Triphosphate analysis, Animals, Caspases physiology, Cell Survival drug effects, Chlorides toxicity, Glutathione analysis, Orotic Acid toxicity, PC12 Cells, Rats, Zinc Acetate toxicity, Zinc Sulfate toxicity, Neurons drug effects, Zinc Compounds toxicity

Abstract

Currently much attention has been given to the neurotoxicity of zinc, yet little is known about the influence of the counterions present. Therefore, we investigated the influence of different Zn(2+)-salts (concentrations range 0.05-0.3 mM) on cell viability, ATP and glutathione concentration and caspase activation in differentiated PC12 cells as a model for neuronal cells. Generally, at concentrations of 0.05 mM most Zn(2+)-salts were not cytotoxic except for zinc-citrate. At concentrations between 0.1 and 0.3 mM Zn(2+) a significant decrease in GSH and ATP levels preceded cell death induced by all salts, except of zinc-histidinate. Zinc-citrate and zinc-sulphate turned out to be the most toxic salts particularly at low concentrations. Analyses of caspase 3/7 activity showed that dependent on the concentration and the type of the salt used cell death may show more or less signs of both, necrosis and apoptosis. Interestingly, the uptake of Zn(2+) from zinc-sulphate and zinc-citrate was significantly higher than that of other salts, implicating a correlation between uptake and toxicity. In conclusion, Zn(2+)-salts could be divided into three categories with high (zinc-citrate, zinc-sulphate), moderate (zinc-orotate, zinc-acetate, zinc-chloride(,) zinc-gluconate) and low cytotoxicity (zinc-histidinate).

Published

2009

13. Fenofibrate prevents orotic acid--induced hepatic steatosis in rats.

Author

Ferreira AV, Parreira GG, Porto LC, Mario EG, Delpuerto HL, Martins AS, and Botion LM

Subjects

Acyl-CoA Oxidase biosynthesis, Adipocytes drug effects, Adipocytes metabolism, Adrenergic beta-Agonists pharmacology, Animals, Cell Separation, Diet, Hepatic Insufficiency pathology, Hypoglycemic Agents pharmacology, Insulin pharmacology, Isoproterenol pharmacology, Lipid Metabolism drug effects, Lipids biosynthesis, Lipolysis drug effects, Lipoprotein Lipase metabolism, Liver pathology, Male, PPAR alpha biosynthesis, Rats, Rats, Wistar, Reverse Transcriptase Polymerase Chain Reaction, Fenofibrate therapeutic use, Hepatic Insufficiency chemically induced, Hepatic Insufficiency prevention & control, Hypolipidemic Agents therapeutic use, Orotic Acid antagonists & inhibitors, Orotic Acid toxicity

Abstract

The experiments performed in this report were designed to investigate the mechanisms involved in the metabolic alterations associated with orotic acid-induced hepatic steatosis and the effect of fenofibrate, a stimulant of peroxisome proliferators-activated receptor alpha (PPARalpha), on these alterations. Male Wistar rats were divided into three experimental groups: 1) fed a balanced diet (C); 2) fed a balanced diet supplemented with 1% orotic acid (OA); 3) fed OA diet containing 100 mg.kg(-1) bw.day(-1) fenofibrate (OA+F), for 9 days. Administration of OA to rats induced significant increase in the hepatic total lipids content, marked microvesicular steatosis and decrease in plasma lipids concentrations compared to control group. Fenofibrate treatment prevented fatty liver induction, caused an additional reduction on plasma lipids concentrations and caused a 40% decrease in the lipogenic rate in adipose tissue. The results also showed a 40% increase in lipoprotein lipase (LPL) activity in adipose tissue from OA treated group and fenofibrate administration induced a 50% decrease in LPL activity. The liver mRNA expression of PPARalpha and ACO (acyl CoA oxidase) were 85% and 68% decreased in OA group when compared to control, respectively. Fenofibrate treatment increased the PPARalpha and ACO expressions whereas the CPT-1 (carnitine palmitoyl transferase-1) expression was not altered. Our results have shown that fenofibrate treatment decreases the hepatic lipid content induced by OA which is mediated by an important increase in fatty acid oxidation consequent to an increase in hepatic mRNA expression of PPARalpha and ACO.

Published

2008

14. Integration of genomic and metabonomic data in systems biology--are we 'there' yet?

Author

Thomas CE and Ganji G

Subjects

Acetaminophen pharmacokinetics, Acetaminophen toxicity, Animals, Biomarkers analysis, Databases, Genetic, Gene Expression Profiling, Gene Expression Regulation, Humans, Hydrazines pharmacokinetics, Hydrazines toxicity, Liver drug effects, Models, Biological, Orotic Acid pharmacokinetics, Orotic Acid toxicity, Systems Integration, Computational Biology trends, Genomics trends, Proteomics trends

Abstract

The measurement of genes, proteins and metabolites has gained increasing acceptance as a means by which to study the response of an organism to stimuli, whether they are environmental, genetic, pharmacological, toxicological, etc. Typically referred to as genomics, proteomics, and metabonomics or metabolomics, respectively, these methods as independent entities have undoubtedly provided new biological insight that was not attainable a decade ago. Not surprisingly, scientists continue to push the boundaries to extract knowledge from data, and it is currently recognized that the full realization of these technologies is limited by a lack of tools to enable data integration. Integration of these 'omic datasets, or integromics, is desirable as it links the individual biological elements together to provide a more complete understanding of dynamic biological processes. Accordingly, in addition to developing new data analysis methods to extract further details from each of the high-content datasets individually, effort is also being expended to create or improve statistical methods, databases, annotations and pathway mapping to maximize our learning. There are several recent examples, in both mammalian and non-mammalian systems, in which genes, proteins and/or metabolites have been integrated using either biology- or data-driven strategies. Herein, key findings are reviewed, gaps in our current tools and technologies are identified and illustrated, and perspective is provided on the potential of integromics in biological research.

Published

2006

15. Dietary phosphatidylcholine alleviates fatty liver induced by orotic acid.

Author

Buang Y, Wang YM, Cha JY, Nagao K, and Yanagita T

Subjects

Animals, Carnitine O-Palmitoyltransferase genetics, Carnitine O-Palmitoyltransferase metabolism, Cholesterol blood, Fatty Acid Synthases genetics, Fatty Acid Synthases metabolism, Fatty Liver chemically induced, Fatty Liver enzymology, Liver chemistry, Liver enzymology, Male, Organ Size drug effects, Orotic Acid toxicity, Oxidation-Reduction, Phosphatidylcholines administration & dosage, Phosphatidylcholines metabolism, Phospholipids blood, Phospholipids metabolism, RNA, Messenger metabolism, Random Allocation, Rats, Rats, Sprague-Dawley, Triglycerides administration & dosage, Triglycerides blood, Triglycerides metabolism, Fatty Liver drug therapy, Liver drug effects, Phosphatidylcholines therapeutic use

Abstract

Objective: We compared the effect of dietary phosphatidylcholine (PC) with that of triacylglycerol (TG), both with the same fatty acid profiles, on fatty infiltration in orotic acid (OA)-induced fatty liver of Sprague-Dawley rats., Methods: Rats were fed an OA-supplemented diets containing TG (TG+OA group) or PC (20% of dietary lipid, PC+OA group) for 10 d. Rats fed the TG diet without OA supplementation served as the basal group., Results: Administering OA significantly increased the weights and TG accumulation in livers of the TG+OA group compared with the basal group. These changes were attributed to significant increases in the activities of fatty acid synthase, malic enzyme, and glucose-6-phosphate dehydrogenase, which are fatty acid synthetic enzymes, and phosphatidate phosphohydrolase, a rate-limiting enzyme of TG synthesis. However, the PC+OA group did not show TG accumulation and OA-induced increases of these enzyme activities. Further, a significant increase in the activity of carnitine palmitoyl transferase, a rate-limiting enzyme of fatty acid beta-oxidation, was found in the PC+OA group., Conclusions: Dietary PC appears to alleviate the OA-induced hepatic steatosis and hepatomegaly, mainly through the attenuation of hepatic TG synthesis and enhancement of fatty acid beta-oxidation in Sprague-Dawley rats.

Published

2005

16. Alleviation of fatty liver by alpha-linolenic acid.

Author

Buang Y, Cha JY, Nagao K, Wang YM, Inoue N, and Yanagita T

Subjects

Animals, Fatty Liver chemically induced, Fatty Liver enzymology, Male, Organ Size drug effects, Random Allocation, Rats, Rats, Sprague-Dawley, Triglycerides biosynthesis, Fatty Liver metabolism, Linoleic Acid pharmacology, Orotic Acid toxicity, Phosphatidate Phosphatase metabolism, alpha-Linolenic Acid pharmacology

Abstract

We compared the efficacy of alpha-linolenic acid (alpha-LNA, n-3) and linoleic acid (LA, n-6) on orotic acid (OA)-induced fatty liver in Sprague-Dawley rats. Rats were fed semi-synthetic diets containing either LA or alpha-LNA with or without 1% OA for 2 wk. OA supplementation lowered serum lipids in LA+OA groups. In addition to the decline of serum lipids in alpha-LNA groups compared to LA groups, a further decrease was found in alpha-LNA+OA groups compared to LA+OA groups. OA-containing diets significantly increased the liver weights and triacylglycerol (TG) accumulations compared with the OA-free diets. These results were attributed to the significant increases in the activities of phosphatidate phosphohydrolase (PAP), a rate-limiting enzyme of TG synthesis, and glucose-6-phosphate dehydrogenase, a fatty acid synthesis-related enzyme. However, the increase of PAP activity was significantly less in the alpha-LNA+OA group as compared with the LA+OA group. These results suggest that dietary alpha-LNA alleviates OA-induced hepatic TG accumulation through the attenuation of hepatic TG synthesis in rats.

Published

2004

17. Effects of oral administration of orotic acid on hepatic morphologic characteristics and serum biochemical variables in cats.

Author

VanSteenhouse JL, Dimski DS, Taylor HW, Swenson DH, Taboada J, and Hosgood G

Subjects

Administration, Oral, Alanine Transaminase blood, Alkaline Phosphatase blood, Animals, Aspartate Aminotransferases blood, Cats, Creatinine urine, Fatty Liver chemically induced, Fatty Liver pathology, Female, Liver metabolism, Liver pathology, Orotic Acid administration & dosage, Orotic Acid toxicity, Creatinine blood, Liver drug effects, Orotic Acid pharmacology

Abstract

Objective: To evaluate orotic acid (OA) as a possible etiologic factor in cats with idiopathic hepatic lipidosis (HL)., Animals: 20 clinically normal adult female cats., Procedure: Cats were fed a control diet or a diet containing less protein. On day 1 of the control period, blood, urine, and liver biopsy specimens were obtained. Each cat was given an oral dose of water daily. On days 8, 15, and 22, blood and urine specimens were collected as on day 1. On day 29, liver, blood, and urine samples were obtained as on day 1. After a resting period of 30 to 60 days, cats were treated with orotic acid. Serum biochemical analyses, urinary OA-to-creatinine ratios, and liver biopsy specimens were evaluated. Cats were given OA orally (suspension or capsules) for 29 days. Sample collection and data obtained were identical to those described for the control period., Results: Urinary OA-to-creatinine ratios were significantly higher in all treated cats, but ratios were significantly higher in those receiving OA in capsules than in those receiving OA in suspension. Diet or treatment did not alter hepatic biochemical or histologic variables significantly. However, 7 cats given the highest dose of OA in capsules developed azotemia, urolithiasis, and renal changes., Conclusions: Most concentrations of OA used in this study did not induce HL in cats during a 29-day period, but the highest dosage used did result in renal disease., Clinical Relevance: Orotic acid does not appear to be involved in the genesis of HL in cats.

Published

1999

18. Prevention of orotic-acid-induced fatty liver in male rats by dehydroepiandrosterone and/or phenobarbital.

Author

Goto H, Yamashita S, and Makita T

Subjects

Analysis of Variance, Animals, Cells, Cultured, Dietary Sucrose toxicity, Energy Intake drug effects, Liver pathology, Male, Organ Size drug effects, Rats, Rats, Sprague-Dawley, Weight Gain drug effects, Dehydroepiandrosterone pharmacology, Fatty Liver chemically induced, Fatty Liver prevention & control, Liver drug effects, Orotic Acid toxicity, Phenobarbital pharmacology

Abstract

Dehydroepiandrosterone (DHEA) is a steroid hormone which induces the peroxisome proliferation in rodents. The fatty liver induced by orotic acid and a high sucrose diet in male rats was prevented by the administration of DHEA and/or phenobarbital (PB). A significant increase in the liver weight was induced in the DHEA group (relative weight) and the DHEA + PB group (absolute and relative weight). The liver weight increased more conspicuously in the DHEA + PB group than in the DHEA group. The increase in the liver weight was caused by an increase in the cell size and peroxisome number. In addition, the administration of DHEA alone and the combination of DHEA and PB prevented the lipid droplet accumulation in hepatocytes. The administration of PB alone also prevented the accumulation of lipid droplets without any increase in the liver weight.

Published

1998

19. Association between hepatic triacylglycerol accumulation induced by administering orotic acid and enhanced phosphatidate phosphohydrolase activity in rats.

Author

Cha JY, Mameda Y, Yamamoto K, Oogami K, and Yanagita T

Subjects

Animals, Diet, Fatty Acids, Omega-3 pharmacology, Fatty Acids, Omega-6, Fatty Acids, Unsaturated pharmacology, Fatty Liver chemically induced, Fatty Liver metabolism, Male, Rats, Rats, Sprague-Dawley, Triglycerides blood, Liver drug effects, Liver metabolism, Orotic Acid toxicity, Phosphatidate Phosphatase metabolism, Triglycerides metabolism

Abstract

Orotic acid is known to cause fatty liver, but it is unclear whether this is caused partly by stimulation of the enzymes for triacylglycerol (TG) synthesis. To understand the change of hepatic TG metabolism in fatty liver induced by orotic acid, we determined the liver tissue TG level and phosphatidate phosphohydrolase (PAP) activity over time in rats fed on a diet containing orotic acid (OA). A dietary lipid content of 10% was achieved by using n-6 fatty acid-rich corn oil in experiment 1, and n-6 fatty acid-rich safflower oil (SO) and n-3 fatty acid-rich fish oil (FO) with the same polyunsaturated fatty acid/monounsaturated fatty acid/saturated fatty acid (P/M/S) ratio in experiment 2. In experiment 1, an increase in the hepatic TG level due to OA intake was observed from day 5 onwards, the level rising approximately 6-fold by day 10. The activity of hepatic microsomal PAP, the rate-limiting enzyme in TG synthesis, increased markedly from day 5 onwards, concurrent with the liver diacylglycerol concentration. A strong correlation (r = 0.974) was observed between the hepatic TG level and microsome-bound PAP activity. In experiment 2, we investigated the effects of dietary fatty acid on OA-induced fatty liver. Compared with the n-6 fatty acid-rich vegetable oil diet, the relative increase in hepatic TG was smaller with the n-3 fatty acid-rich FO diet, and hepatic PAP activity fell markedly to the level for an OA-free diet. In addition, the hepatic TG accumulation and serum TG concentration were lower in the FO group than in the SO group. Nevertheless, because the hepatic TG level was low, it seems that the inhibition of liver PAP activity by FO possibly had a strong influence on the accumulation of TG in the liver. In conclusion, enhanced TG synthesis mediated by changes in liver PAP activity was involved in the hepatic TG accumulation induced by OA administration, this change being markedly suppressed by dietary n-3 fatty acids.

Published

1998

20. Pyrimidine antagonists and antifolates as antimalarial drugs.

Author

Christopherson RI, Seymour KK, and Yeo AE

Subjects

Animals, Dapsone pharmacology, Drug Resistance, Multiple, Orotic Acid toxicity, Plasmodium falciparum metabolism, Proguanil pharmacology, Pyrimidines antagonists & inhibitors, Antimalarials toxicity, Deoxyribonucleotides metabolism, Enzyme Inhibitors toxicity, Folic Acid Antagonists toxicity, Orotic Acid analogs & derivatives, Plasmodium falciparum drug effects, Ribonucleotides metabolism

Published

1998

21. Chemoprevention by S-adenosyl-L-methionine of rat liver carcinogenesis initiated by 1,2-dimethylhydrazine and promoted by orotic acid.

Author

Pascale RM, Simile MM, De Miglio MR, Nufris A, Daino L, Seddaiu MA, Rao PM, Rajalakshmi S, Sarma DS, and Feo F

Subjects

1,2-Dimethylhydrazine, Animals, Liver drug effects, Liver Neoplasms, Experimental pathology, Male, Precancerous Conditions pathology, Rats, Rats, Inbred F344, Anticarcinogenic Agents therapeutic use, Cocarcinogenesis, Dimethylhydrazines toxicity, Liver Neoplasms, Experimental chemically induced, Liver Neoplasms, Experimental prevention & control, Orotic Acid toxicity, Precancerous Conditions chemically induced, Precancerous Conditions prevention & control, S-Adenosylmethionine therapeutic use

Abstract

Chemoprevention of liver carcinogenesis by S-adenosyl-L-methionine (SAM) was studied in F344 male rats. The rats were given 1,2-dimethylhydrazine (1,2-DMH) 2 HCl (100 mg/kg, i.p.) 18 h after two-thirds hepatectomy. One week later they were fed a semisynthetic basal diet containing 1% orotic acid (OA) for 29 weeks. At this time the rats were transferred to the basal semisynthetic diet and were killed 3 weeks later. SAM treatment (384 mumol/kg/day, i.m.), was started 1 week after 1,2-DMH and was continued up to the end of the experiment. Controls received solvent alone. SAM exerted an inhibitory effect on the induction of preneoplastic and neoplastic lesions. For example, nodules with diameters of 1-2 and 2-6 mm exhibited a decrease in both incidence and number per liver, while no such inhibitory effect was seen in the category of larger nodules. Furthermore, hepatocellular carcinoma (HCC) also exhibited a decrease in the SAM-treated group. The number/liver and incidence were 0.04 and 4.8% respectively in the SAM-treated group, compared to 0.38 and 37.8% in the control group. Microscopic examination showed the presence of well-differentiated carcinomas and atypical nodules in control rats, while only one small, well-differentiated tumor and one nodule with patterns of initial transformation were seen in SAM-treated rats. No patchy staining of glutathione-S-transferase, indicative of remodeling, was observed in nodules of both SAM-treated and control rats. Nodules and HCCs developing in SAM-treated rats exhibited a relatively high number of apoptotic bodies. Apoptotic bodies count showed 2.8- and 1.8-fold increases in nodules and HCCs of SAM-treated rats with respect to controls. These results indicate that SAM exerts a chemopreventive effect on hepatocarcinogenesis induced by the OA model. SAM seems to be more effective in inhibiting nodule to HCC progression than on the growth of nodule per se. The inhibitory effect is associated with an increase in cell loss by apoptosis in nodules and HCC.

Published

1995

22. An earlier proliferative response of hepatocytes in gamma-glutamyl transferase positive foci to partial hepatectomy.

Author

Laconi E, Vasudevan S, Rao PM, Rajalakshmi S, Pani P, and Sarma DS

Subjects

Animals, Cell Division, Hepatectomy, Male, Orotic Acid toxicity, Rats, Rats, Inbred F344, Liver Neoplasms, Experimental pathology, Precancerous Conditions pathology, gamma-Glutamyltransferase analysis

Abstract

One of the hallmarks of initiated hepatocytes is their resistance to several hepatotoxins. This property forms the basis for their selective growth under conditions which are inhibitory to the non-initiated hepatocytes. Selective growth of initiated hepatocytes also occurs, albeit at a low level, in initiated rat liver without exposure to any known promoting regimen and/or in the absence of any known selective pressure to which initiated hepatocytes can possibly be resistant. This latter phenotypic property of initiated hepatocytes was further characterized by comparing the kinetics of response of hepatocytes in gamma-glutamyl transferase positive foci and in the surrounding liver to 2/3 partial hepatectomy both in the presence and in the absence of a promoting regimen. Male Fischer 344 rats (130-150 g) were initiated with a single dose of diethylnitrosamine and 1 week later they were placed on either a semi-synthetic basal diet or a promoting diet containing 1% orotic acid. Partial hepatectomy was performed 15 weeks after initiation and animals from both groups were killed at 12, 16, 20, 24, 30, 36, 48, 72 or 96 h after operation. Each animal received a pulse of 3H-labelled thymidine 1 h prior to killing. Autoradiographic studies revealed that hepatocytes in gamma-glutamyl transferase positive foci in the livers of rats fed the basal diet were significantly labelled at 16 h post-partial hepatectomy while surrounding hepatocytes were still virtually quiescent (LI 12.7 +/- 4.7 versus 1.2 +/- 0.5%, respectively). Higher labelling index in foci compared to the surrounding liver was also seen at 20 h post-PH (36.9 +/- 2.6 versus 21.5 +/- 2.4). Similar earlier response of hepatocytes in gamma-glutamyl transferase positive foci was also seen in initiated rats exposed to dietary orotic acid. In addition, orotic acid treatment appears to have imposed a slight delay on the entry of hepatocytes in the surrounding liver into 'S' phase and thereby enhancing the differential of growth response between these two populations.

Published

1994

23. Cytotoxic effects of inhibitors of de novo pyrimidine biosynthesis upon Plasmodium falciparum.

Author

Seymour KK, Lyons SD, Phillips L, Rieckmann KH, and Christopherson RI

Subjects

Amides, Animals, Atovaquone, Bicarbonates metabolism, Carbon Radioisotopes, Chromatography, High Pressure Liquid, Dihydroorotase antagonists & inhibitors, Dihydroorotase isolation & purification, Dihydroorotate Dehydrogenase, Erythrocytes parasitology, Humans, Kinetics, Malaria blood, Naphthoquinones toxicity, Orotic Acid pharmacology, Orotic Acid toxicity, Oxidoreductases isolation & purification, Oxidoreductases metabolism, Plasmodium falciparum drug effects, Plasmodium falciparum growth & development, Pyrazoles, Pyrimidines biosynthesis, Pyrimidines isolation & purification, Ribonucleosides pharmacology, Ribose, Antimalarials pharmacology, Dihydroorotase metabolism, Naphthoquinones pharmacology, Orotic Acid analogs & derivatives, Orotidine-5'-Phosphate Decarboxylase antagonists & inhibitors, Oxidoreductases Acting on CH-CH Group Donors, Plasmodium falciparum metabolism, Pyrimidines metabolism

Abstract

The malarial parasite Plasmodium falciparum can only synthesize pyrimidine nucleotides via the de novo pathway which is therefore a suitable target for development of antimalarial drugs. New assay procedures have been developed using high-pressure liquid chromatography (HPLC) which enable concurrent measurement of pyrimidine intermediates in malaria. Synchronized parasites growing in erythrocytes were pulse-labeled with [14C]bicarbonate at 6-h intervals around the 48-h asexual life cycle. Analysis of malarial extracts by HPLC showed tht incorporation of [14C]bicarbonate into pyrimidine nucleotides was maximal during the transition from trophozoites to schizonts. The reaction, N-carbamyl-L-aspartate-->L-dihydroorotate (CA-asp-->DHO) catalyzed by malarial dihydroorotase is inhibited by L-6-thiodihydroorotate (TDHO) in vitro (Ki = 6.5 microM), and TDHO, as the free acid or methyl ester, induces a major accumulation of CA-asp in malaria. Atovaquone, a naphthoquinone, is a moderate inhibitor of dihydroorotate dehydrogenase in vitro (Ki = 27 microM) but induces major accumulations of CA-asp and DHO. Pyrazofurin induces accumulation of orotate and orotidine in malaria, consistent with inhibition of orotidine 5'-monophosphate (OMP) decarboxylase with subsequent dephosphorylation of the OMP accumulated. Although TDHO, atovaquone, and pyrazofurin arrest the growth of P. falciparum, only moderate decreases in UTP, CTP, and dTTP were observed. 5-Fluoroorotate also arrests the growth of P. falciparum with major accumulations of 5-fluorouridine mono-, di-, and triphosphates and the most significant inhibition of de novo biosynthesis of pyrimidine nucleotides.

Published

1994

24. Resistance of hepatic nodules to orotic acid-induced accumulation of uridine nucleotides.

Author

Backway KL, Laconi E, Manjeshwar S, Rao PM, Rajalakshmi S, and Sarma DS

Subjects

Animals, Cells, Cultured, Drug Resistance, Liver metabolism, Liver pathology, Male, Rats, Rats, Inbred F344, Liver drug effects, Orotic Acid toxicity, Uracil Nucleotides metabolism

Abstract

It has been hypothesized that orotic acid (OA) promotes rat liver carcinogenesis by a differential mitoinhibitory mode. Consistent with this hypothesis, hepatic nodules are relatively resistant to OA-induced mitoinhibition. OA-induced mitoinhibition is dependent on the metabolism of OA to uridine nucleotides. The present studies investigate the uptake and metabolic pathway of OA, both in vivo and in vitro, as a possible basis for the resistance of hepatic nodules to OA-induced mitoinhibition. Rats bearing hepatic nodules exposed to 1% dietary OA exhibited increased levels of uridine nucleotides in the surrounding non-nodular liver (from 0.44 to 0.70 mg/g liver) but not in the hepatic nodules. Further, following administration of [3H]OA i.p., nodules have significantly lower levels of acid-soluble radioactivity compared to the non-nodular surrounding tissue. Furthermore, most of the acid-soluble radioactivity was present as uridine nucleotides, suggesting that the OA taken up was converted to uridine nucleotides. Similarly, hepatocytes from nodules in primary culture incubated with radiolabeled OA, have significantly lower levels (46-60%) of acid-soluble radioactivity. These results suggest that the decreased uptake of OA by hepatic nodules may be a factor contributing to the observed resistance of hepatic nodules to the mitoinhibitory effects of OA.

Published

1994

25. Toxic and vascular nephropathy associated with orotic acid administration in laboratory cats.

Author

Dimski DS, Taylor HW, Taboada J, Van Steenhouse JL, Swenson DH, and Marx BD

Subjects

Animals, Cats, Kidney blood supply, Kidney pathology, Urinary Calculi chemically induced, Urinary Calculi pathology, Vasculitis chemically induced, Vasculitis pathology, Kidney drug effects, Orotic Acid toxicity

Published

1994

26. The development of hepatocellular carcinoma in initiated rat liver after a brief exposure to orotic acid coupled with partial hepatectomy.

Author

Laconi E, Vasudevan S, Rao PM, Rajalakshmi S, Pani P, and Sarma DS

Subjects

Animals, Body Weight, Hepatectomy, Liver pathology, Liver surgery, Male, Organ Size, Precancerous Conditions chemically induced, Rats, Rats, Inbred F344, Carcinogens toxicity, Liver drug effects, Liver Neoplasms, Experimental chemically induced, Orotic Acid toxicity

Abstract

Previous work from this laboratory has revealed that a minimum of 10-20 weeks of continuous exposure to 1% dietary orotic acid (OA) is necessary for this regimen to exert a significant promoting effect on the carcinogenic process in rat liver. The present study investigates the effect of partial hepatectomy (PH), given during a short-term exposure (4 weeks) to OA, on the development of hepatocyte nodules (HN) and hepatocellular carcinoma (HCC) initiated by diethylnitrosamine (DEN). Male Fischer 344 rats (130-150 g) were given a single dose of DEN (200 mg/kg body wt i.p.). Starting a week later they were fed either a semisynthetic basal diet (BD) or the same diet containing 1% OA for 2 weeks; two-thirds PH was then performed followed by another 2 weeks of BD or OA diet respectively. At the end of this treatment some animals from both groups were killed while the rest were continued on BD and killed at 20 or 56 weeks thereafter. The results showed no difference between the two groups in the incidence of gamma-glutamyltransferase-positive foci when rats were killed at 2 weeks after PH. However, 4 week exposure to OA coupled with PH significantly enhanced the incidence of HN and HCC when this protocol was followed by 20 or 56 weeks of BD feeding respectively, leading to 63% incidence of HCC in the OA-fed group, while no HCC was observed in control animals. It is concluded that a type of stable or permanent change(s) ('imprinting' or 'memory effect') is induced in the initiated rat liver by this treatment, which imposes a promoting environment in the liver even after withdrawal of the promoter.

Published

1993

27. Isolation, characterization and mapping of pyrimidine auxotrophs of Phycomyces blakesleeanus.

Author

Campuzano V, del Valle P, de Vicente JI, Eslava AP, and Alvarez MI

Subjects

Cell-Free System, Drug Resistance, Microbial, Genetic Complementation Test, Genetic Linkage, Genetic Markers, Genotype, Orotic Acid analogs & derivatives, Orotic Acid toxicity, Phycomyces isolation & purification, Phycomyces metabolism, Recombination, Genetic, Restriction Mapping, Spores, Fungal metabolism, Orotate Phosphoribosyltransferase genetics, Phycomyces genetics, Pyrimidines metabolism

Abstract

A total of seven pyrimidine auxotrophs of Phycomyces were isolated from among 5-fluoroorotate acid (5-FOA)-resistant mutants. They were classified by complementation into two groups. A representative mutant strain belonging to one group was deficient in orotate phosphoribosyl transferase (OPRTase; EC 2.4.2.10) activity; the mutant strain belonging to the second group was deficient in orotidine-5'-monophosphate decarboxylase (OMPdecase; EC 4.1.1.23). These mutants are defective in the genes pyrF and pyrG respectively. The results from random spore analysis, tetrad analysis, and gene-centromere distances showed that these two markers are located in linkage group VI, with pyrG being a proximal marker and pyrF a distal one.

Published

1993

28. Increasing the interval between initiation and the onset of exposure to orotic acid decreases its promoting effect on rat liver carcinogenesis.

Author

Laconi E, Vasudevan S, Rao PM, Rajalakshmi S, Pani P, and Sarma DS

Subjects

Animals, Diethylnitrosamine, Drug Synergism, Male, Neoplasm Metastasis, Rats, Rats, Inbred F344, Time Factors, Carcinogens toxicity, Liver Neoplasms, Experimental chemically induced, Orotic Acid toxicity

Abstract

The present study was designed to determine whether a delay in the start of the promoting regimen after the administration of a carcinogen would influence the promoting efficacy of orotic acid on the development of hepatocellular carcinoma in rats. Male Fischer 344 rats weighing 130-150 g were injected with a single dose of diethylnitrosamine (200 mg/kg body wt i.p.) then divided into 3 groups: groups 1 and 2 were given semi-synthetic basal diet or the same diet containing 1% orotic acid (OA) respectively starting 1 week after the carcinogen; group 3 received the OA diet starting 5 weeks after the administration of diethylnitrosamine. Animals from these 3 groups were sacrificed after 25, 32, 42 and 60 weeks of being fed their respective diets. The results indicated that delaying the start of the OA diet after the carcinogen resulted in about a 50% decrease in the incidence of hepatic nodules and/or hepatocellular carcinomas at various time points during the experiment. This decrease in promoting efficacy of OA was not apparently explainable by lack of metabolic effects of OA, at least in terms of induction of nucleotide pool imbalance, a condition that appears to be important for OA to exert its tumor promoting effects.

Published

1993

29. Induction of hepatic nodules in the rat by aristolochic acid.

Author

Rossiello MR, Laconi E, Rao PM, Rajalakshmi S, and Sarma DS

Subjects

Animals, Cell Division drug effects, Cocarcinogenesis, Hepatectomy, Liver pathology, Male, Necrosis chemically induced, Orotic Acid toxicity, Rats, Rats, Inbred F344, Aristolochic Acids, Carcinogens toxicity, Liver drug effects, Liver Neoplasms chemically induced, Phenanthrenes toxicity

Abstract

Aristolochic acid (AA), used as an anti-inflammatory agent in the past, is known to be mutagenic and carcinogenic to several organs of the rat, including forestomach, renal pelvis and urinary bladder. However, despite the induction of DNA adducts in the liver, no carcinogenic potential of AA has been reported in the latter organ. The present study was based on the rationale that the lack of carcinogenicity of AA to the liver could be because this chemical may not be necrogenic at the doses examined and liver cell proliferation has been established as an essential component for initiation of liver carcinogenesis in the rat. The results indicated that AA is non-necrogenic to the rat liver. However, a single non-necrogenic dose of AA (10 mg/kg b.w., i.p.) given 18 hours after 2/3 partial hepatectomy initiated liver cell carcinogenesis. The initiated cells are promotable with 1% dietary orotic acid, a liver tumor promoter, to form glutathione-S-transferase 7-7 positive hepatic foci and nodules.

Published

1993

30. Inhibition of DNA synthesis by phenobarbital in primary cultures of hepatocytes from normal rat liver and from hepatic nodules.

Author

Manjeshwar S, Rao PM, Rajalakshmi S, and Sarma DS

Subjects

Animals, Cells, Cultured, Epidermal Growth Factor physiology, ErbB Receptors metabolism, Liver cytology, Liver metabolism, Liver pathology, Male, Orotic Acid toxicity, Rats, Rats, Inbred F344, Transforming Growth Factor alpha physiology, Carcinogens toxicity, DNA Replication drug effects, Liver drug effects, Liver Diseases metabolism, Phenobarbital toxicity

Abstract

One of the many hypotheses put forward to explain the mechanism by which phenobarbital (PB) promotes hepatocarcinogenesis is by differential mitoinhibition of surrounding hepatocytes while allowing the initiated hepatocytes to respond to growth stimuli and form foci and nodules. Given the similarity in structures between PB and orotic acid (OA), another rat liver tumor promoter, the present investigation was designed to determine (i) whether PB, like OA, exerts its mitoinhibitory effect at a site beyond the growth factor receptor and receptor mediated early events; and (ii) whether PB exerts a differential mitoinhibitory effect by selectively inhibiting the non-initiated hepatocytes but not the initiated hepatocytes in vitro. Our studies demonstrate that, like OA, PB also inhibits DNA synthesis in hepatocytes from normal rat liver in a dose dependent manner with 80-90% at a dose of 6 mM. One target site may lie beyond the growth factor receptor mediated early events because PB inhibited DNA synthesis in hepatocytes primed with the growth factor 24 h earlier. Interestingly, PB inhibited DNA synthesis not only in hepatocytes from non-nodular surrounding liver but also in hepatocytes from persistent hepatic nodules initiated with 1,2-dimethylhydrazine and promoted with OA. Therefore, our results suggest that although PB is a mitoinhibitor of DNA synthesis in hepatocytes, it does not appear to create as strong a differential mitoinhibition between non-nodular surrounding and initiated hepatocytes as is evident in the resistant hepatocyte and OA models. These results raise the question whether differential mitoinhibition is the major contributing factor in the PB mediated rat liver tumor promotion.

Published

1992

31. Mitogen-induced liver hyperplasia does not substitute for compensatory regeneration during promotion of chemical hepatocarcinogenesis.

Author

Ledda-Columbano GM, Coni P, Curto M, Giacomini L, Faa G, Sarma DS, and Columbano A

Subjects

Animals, Cell Division drug effects, Hyperplasia chemically induced, Liver drug effects, Liver enzymology, Liver Neoplasms, Experimental chemically induced, Liver Regeneration, Male, Rats, Rats, Inbred Strains, gamma-Glutamyltransferase, 2-Acetylaminofluorene toxicity, Carbon Tetrachloride toxicity, Diethylnitrosamine toxicity, Lead toxicity, Liver pathology, Nitrates toxicity, Orotic Acid toxicity, Phenobarbital toxicity

Abstract

Experiments were designed to determine the efficacy of different types of liver cell proliferative stimuli given during exposure to several liver tumor-promoting regimens, on the formation of foci of enzyme-altered hepatocytes. Male Wistar rats were initiated with diethylnitrosamine (150 mg/kg body wt). After a 2 week recovery period animals were subjected to promoting regimens, the resistant hepatocyte model, the phenobarbital model and the orotic acid model. While the rats were on these regimens they were given liver cell proliferative stimulus, either a compensatory type (two-thirds partial hepatectomy or a necrogenic dose of carbon tetrachloride) or a direct hyperplastic stimulus such as that induced by the primary mitogen, lead nitrate. Initiated cells so promoted by these regimens were monitored as foci of enzyme-altered hepatocytes positive for gamma-glutamyltransferase and placental glutathione S-transferase or deficient for adenosine triphosphatase. While carbon tetrachloride and partial hepatectomy-induced compensatory regeneration stimulated the promoting ability of the regimens used, direct hyperplasia could not stimulate the formation of foci and/or nodules from initiated hepatocytes. Evaluation of thymidine incorporation indicated that there was no significant difference in the extent of DNA synthesis in both the proliferative stimuli irrespective of the promoting procedure used.

Published

1992

32. Biochemical and immunohistochemical analysis of orotic acid-induced fatty liver.

Author

Murakoshi M, Suemizu H, Takekoshi S, Misawa M, and Watanabe K

Subjects

Animals, Fatty Liver metabolism, Fatty Liver pathology, Glutathione Peroxidase metabolism, Immunohistochemistry, Lipid Peroxidation drug effects, Lipid Peroxides metabolism, Male, Rats, Rats, Inbred Strains, Fatty Liver chemically induced, Orotic Acid toxicity

Abstract

Orotic acid-induced fatty livers were examined by biochemical and immunohistochemical approaches. Lipid peroxide levels by the thiobarbituric acid method and glutathione-peroxidase (GSH-PO) activity in the liver homogenates from orotic administered rats were similar to those of controls. Immunohistochemical localization of GSH-PO in orotic acid-induced fatty liver was mainly observed in the portal zone of the hepatic lobules. This staining pattern of GSH-PO was similar to that of the controls. No remarkable changes in GSH-PO staining patterns were detected in orotic acid-induced fatty liver. Our data strongly suggested that no lipid peroxidation is actively involved in the genesis of fatty liver due to the administration of orotic acid, and GSH-PO a protective enzyme against lipid peroxidation, was not inhibited by orotic acid-induced fatty liver.

Published

1991

33. Effect of orotic acid on the generation of reactive oxygen and on lipid peroxidation in rat liver.

Author

Scholz W, Wolf A, Kunz W, Willenbrock R, and Steffen C

Subjects

Administration, Oral, Animals, Body Weight drug effects, Cytochrome P-450 Enzyme System metabolism, DNA Damage drug effects, DNA, Single-Stranded, Female, Glutathione metabolism, Male, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Organ Size drug effects, Oxidation-Reduction, Rats, Rats, Inbred Strains, Lipid Peroxidation drug effects, Microsomes, Liver drug effects, Orotic Acid toxicity

Abstract

The pyrimidine precursor orotic acid (OA) is a constituent of dairy products and therapeutic drugs. Several recent publications point towards a tumor promoting activity of OA in rat liver. An increased production of reactive oxygen has been discussed as a possible mechanism, leading to lipid peroxidation and DNA single strand breaks. In view of contradictory results, this postulated prooxidative action of OA was reexamined with new experimental techniques. Weanling Sprague-Dawley rats were fed 1% OA in different diets for 4-35 days. The NADPH-mediated lipid peroxidation in liver homogenate and microsomes was determined in vitro by analysis of low-level chemiluminescence (CL) and the strongly correlated formation of malondialdehyde (MDA). In no case did treatment with OA result in an increase of lipid peroxidation in vitro nor did such treatment enhance the generation of reactive oxygen as measured by lucigenin CL. In accordance, the total cytochrome P-450 content as well as the activity of individual P-450 isoenzymes were unchanged. Treatment with OA did not elevate the MDA content of fresh liver homogenate when butylated hydroxytoluene (BHT) was present in the test system. However, when the antioxidant was omitted, increased levels of thiobarbituric acid reactive material were found which correlated with the triglyceride content. This could explain some published data that have been taken as indication for a prooxidative action of OA. Evidence against an increased lipid peroxidation in vivo is given by the analysis of ethane exhalation. Furthermore, no increase in DNA single strand breaks by OA treatment could be observed by the alkaline elution technique. These results do not support the hypothesis of a prooxidative activity of OA. The observed reversible decrease of the GSH/GSSG ratio is assumed to result from the reduced size of the phosphopyridine nucleotide pool due to purine deficiency and an increased consumption of NADPH by the enhanced reductive degradation of pyrimidines.

Published

1991

34. Antimalarial activity of a combination of 5-fluoroorotate and uridine in mice.

Author

Gómez ZM and Rathod PK

Subjects

Animals, Drug Combinations, Malaria parasitology, Male, Mice, Orotic Acid pharmacokinetics, Orotic Acid therapeutic use, Orotic Acid toxicity, Plasmodium yoelii, Uridine pharmacokinetics, Uridine toxicity, Malaria drug therapy, Orotic Acid analogs & derivatives, Uridine therapeutic use

Abstract

Malarial parasites, in contrast to mammalian cells, utilize orotic acid more efficiently than uracil or uridine. Recently, chloroquine-susceptible and chloroquine-resistant clones of Plasmodium falciparum were shown to be inhibited by 5-fluoroorotate, with a 50% inhibitory concentration of 6 nM in vitro. Mammalian cells were far less sensitive to 5-fluoroorotate, particularly in the presence of uridine. In this report, the antimalarial activity of 5-fluoroorotate was tested in vivo. Initially, levels of 5-fluoroorotate in plasma were determined in Swiss mice injected intraperitoneally with radioactive 5-fluoroorotate. On the basis of the pharmacokinetics profile, mice infected with Plasmodium yoelii were treated with 5-fluoroorotate at a dose of 0.2 or 5 mg/kg (body weight) every 4 h for 3 days. At the nontoxic dose of 0.2 mg/kg, the reduction in parasitemia was followed by a temporary resurgence of parasitemia. This second wave of parasitemia cleared without additional 5-fluoroorotate treatment. To radically eliminate P. yoelii from mice and avoid the second wave of parasitemia, a higher dose of 5 mg of 5-fluoroorotate per kg had to be used. In the absence of uridine, repeated doses of 5 mg/kg were toxic to mice, as judged by weight loss, diarrhea, decreased numbers of leukocytes, and increased mortality. However, in the presence of uridine, repeated doses of 5 mg/kg could be used for antimalarial chemotherapy without obvious toxicity. Mice cured with 5-fluoroorotate and uridine were immune to subsequent challenge with a potentially lethal inoculum of P. yoelii.

Published

1990

35. Sex differences in response to four promotion regimens in spite of common first cellular steps in the hepatocellular cancer process initiated by diethylnitrosamine.

Author

Cameron RG, Blanck A, and Armstrong D

Subjects

Animals, Cell Division drug effects, Female, Glutathione Transferase analysis, Liver drug effects, Liver enzymology, Liver pathology, Liver Neoplasms, Experimental enzymology, Liver Neoplasms, Experimental pathology, Male, Rats, Rats, Inbred F344, Sex Factors, gamma-Glutamyltransferase analysis, 2-Acetylaminofluorene toxicity, Choline Deficiency complications, Deoxycholic Acid toxicity, Diethylnitrosamine, Liver Neoplasms, Experimental chemically induced, Orotic Acid toxicity

Abstract

Female adult rats were as responsive as males to initiation by diethylnitrosamine (DEN) as measured by numbers of GST-P positive hepatocytes appearing early, and do develop hepatocellular cancers. However, when females and males were exposed to four promotion regimens including orotic acid (OA), choline deficiency, deoxycholic acid (DOC), or selection for resistance (to 2-acetylaminofluorene; 2-AAF) after DEN initiation, very significant sex differences were observed with respect to oval cell proliferation and growth rates of hepatocytic foci. These results suggest that responses to promotion such as growth of foci and oval cell proliferation can accompany carcinogenesis but may not be essential to the development of hepatocellular cancer.

Published

1990

36. Studies on the effect of dietary orotic acid on mouse liver carcinogenesis induced by diethylnitrosamine.

Author

Laconi E, Vasudevan S, Rao CS, Rao PM, Rajalakshmi S, and Sarma DS

Subjects

Animals, Diet, Diethylnitrosamine, Liver analysis, Liver drug effects, Male, Mice, Mice, Inbred BALB C, Nucleotides analysis, Rats, Rats, Inbred F344, Species Specificity, Liver Neoplasms, Experimental chemically induced, Orotic Acid toxicity

Abstract

The present study was designed to determine whether orotic acid, a liver tumor promoter in the rat, also promotes liver carcinogenesis in the mouse. Eight-week-old male BALB/c mice were initiated with diethylnitrosamine (90 mg/kg i.p.). One week later they were divided into 2 groups and given either a basal diet or the basal diet containing 1% orotic acid (OA). They were killed at 6 or 10 months after the administration of the carcinogen. At 6 months, no nodular lesions were seen in mice whether or not they were exposed to OA. However by 10 months 100% of mice in both groups developed hepatic nodules. OA neither shortened the latent period for the appearance of the nodular lesions not did it increase the size of the nodules. Although BALB/c mice exhibited an increase in uridine nucleotides and a decrease in adenosine nucleotides in the liver upon exposure to OA, the magnitude of the change was less compared with that seen in the rat liver. The resistance of BALB/c mouse to the tumor-promoting effects of OA may reflect in part the resistance of the mouse to OA-induced nucleotide pool imbalance.

Published

1990

37. Effects of gomisin A on liver functions in hepatotoxic chemicals-treated rats.

Author

Maeda S, Takeda S, Miyamoto Y, Aburada M, and Harada M

Subjects

1-Naphthylisothiocyanate toxicity, Animals, Bile metabolism, Carbon Tetrachloride Poisoning physiopathology, Galactosamine toxicity, Indocyanine Green, Liver Function Tests, Male, Orotic Acid toxicity, Rats, Rats, Inbred Strains, Chemical and Drug Induced Liver Injury physiopathology, Cyclooctanes, Dioxoles, Lignans, Liver drug effects, Polycyclic Compounds pharmacology

Abstract

The effects of gomisin A, which is a lignan component of schizandra fruits, on liver functions in various experimental liver injuries and on bile secretion in CCl4-induced liver injury were studied. Gomisin A weakly accelerated the disappearance of plasma ICG by itself at a high dose (100 mg/kg, i.p.). All of the hepatotoxic chemicals used in this study inhibited the excretion of ICG from plasma. Gomisin A showed a tendency to prevent the delays of the disappearance of plasma ICG induced by CCl4, d-galactosamine and orotic acid, but not that by ANIT. Bile flow and biliary outputs of total bile acids and electrolytes (Na+, K+, Cl- and HCO3-) were decreased in CCl4-treated rats. Gomisin A maintained bile flow and biliary output of each electrolyte nearly to the level of the vehicle-treated group, but did not affect biliary output of total bile acids. These findings suggest that gomisin A possesses a liver function-facilitating property in normal and liver injured rats and that its preventive action on CCl4-induced cholestasis is due to maintaining the function of the bile acids-independent fraction.

Published

1985

38. Liver tumour promotion by chemicals: models and mechanisms.

Author

Sarma DS, Rao PM, and Rajalakshmi S

Subjects

Cell Division, Choline Deficiency complications, Cocarcinogenesis, Humans, Orotic Acid toxicity, Phenotype, Liver Neoplasms chemically induced, Phenobarbital toxicity

Abstract

Tumour promotion is defined as the process whereby a carcinogen initiated organ develops focal proliferations such as nodules, polyps or papillomas, one or more of which become precursors for subsequent steps in the carcinogenic process. The available models for a sequential analysis of carcinogenesis in liver have been examined within the framework of this operational definition with respect to the models themselves as well as the promoted hepatocytes. Using initiation-promotion protocols, several promoters which differ in the biological responses they elicit have been identified. The key issue in promotion pertains to the mechanisms involved in the focal proliferation of the initiated hepatocytes. The resistant hepatocyte model and perhaps the phenobarbital model suggest that focal proliferation of the initiated hepatocyte is induced by exerting a selective mitoinhibitory effect on the surrounding cells while permitting the initiated hepatocyte to respond to the proliferative stimulus, whether it is exogenous or endogenous. The promoter orotic acid, on the other hand, is a natural precursor of pyrimidine nucleotide biosynthesis and is neither an inducer nor an inhibitor of liver cell proliferation but it creates an imbalance in cellular nucleotide pools. Since nucleotides are intermediates in DNA synthesis as well as in the glycosylation of proteins and lipids including that of membranes, it has been postulated that the promotional effect of orotic acid is mediated through this imbalance affecting both DNA and membranes. There is some experimental evidence for this. The importance of this hypothesis is that it raises the possibility of achieving promotion in several organs by disturbing the normal nucleotide pool patterns. Indeed orotic acid has also been found to promote duodenal cancer. The finding that hepatic nodules, regardless of how they have been promoted, exhibit a common biochemical pattern with resistance to several agents has raised some important issues. For example, what is the basis for the resistant phenotype and how is it related to cancer development? Are all initiated hepatocytes identical? If not, do all promoters exert their effect on the same population of initiated hepatocytes? Is the heterogeneity of the initiated hepatocyte population generated by the carcinogen due to the induction of more than one critical lesion: a primary lesion responsible for initiation and secondary lesions in which different types of initiated cells are selected by different promoters?(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1986

39. Lysine-orotate potentiates the toxicity of an extract of the mushroom Amanita phalloides.

Author

Halacheva K, Zhelev Z, Pajpanova T, Hubenova A, Spassova M, Alexiev C, and Golovinsky E

Subjects

Amanitins metabolism, Animals, Drug Synergism, Male, Mice, Protein Binding, Amanitins toxicity, Lysine toxicity, Orotic Acid toxicity

Abstract

Upon simultaneous administration lysine-orotate increases (about 40-fold) the toxicity in mice of a crude Amanita phalloides extract. This effect, though less prominent, is also observed if these two compounds are injected 1 hr apart. The potentiating effect of lysine-orotate is dose dependent and neither L-lysine nor orotic acid exert any effect on the toxicity of the crude A. phalloides extract. Lysine-orotate increases the toxicity of amatoxins (alpha-amanitin) only, not affecting the toxicity of phalloidins. Thin layer chromatography on silica gel plates and column chromatography on Sephadex LH-20 has proven the formation of a relatively stable complex of amanitin and lysine-orotate. The results demonstrate that lysine-orotate should not be used as a hepatoprotective agent in cases of Amanita intoxication.

Published

1988

40. Orotic acid, a promoter of liver carcinogenesis induces DNA damage in rat liver.

Author

Rao PM, Rajalakshmi S, Alam A, Sarma DS, Pala M, and Parodi S

Subjects

Animals, Male, Rats, Rats, Inbred F344, Carcinogens, DNA, Liver drug effects, Liver Neoplasms chemically induced, Orotic Acid toxicity

Abstract

Orotic acid, a precursor of pyrimidine nucleotide biosynthesis and a promoter for liver carcinogenesis, when fed at 1% level in a diet for 5 weeks resulted in liver DNA damage. The damage can be monitored as alkali-labile lesions using alkaline sucrose gradients as well as alkaline elution technique. Furthermore, the induced DNA damage persists for up to three weeks after withdrawal of the orotic acid diet. The fact that several skin-tumour promoters also induce DNA damage raises the question whether DNA damage is a component in tumour promotion.

Published

1985

41. Dietary and metabolic manipulations of the carcinogenic process: role of nucleotide pool imbalances in carcinogenesis.

Author

Rao PM, Laconi E, Vasudevan S, Denda A, Rajagopal S, Rajalakshmi S, and Sarma DS

Subjects

Animals, Duodenal Neoplasms chemically induced, Liver drug effects, Liver enzymology, Liver pathology, Liver Neoplasms, Experimental etiology, Male, Orotic Acid pharmacology, Rats, Rats, Inbred F344, gamma-Glutamyltransferase metabolism, Azo Compounds toxicity, Azoxymethane toxicity, Carcinogens, Diet, Duodenal Neoplasms etiology, Galactosamine pharmacology, Liver Neoplasms, Experimental pathology, Orotic Acid toxicity, Ribonucleotides metabolism

Abstract

Perturbations in DNA and/or membranes are considered to be important for the carcinogenic process. A search for nutritional and metabolic means of disturbing the homeostasis of DNA and membranes revealed that nucleotide pools offer an exciting possibility. An imbalance in nucleotide pools can exert a two-pronged attack on both DNA and membranes. When given to rats, orotic acid, a precursor of pyrimidine nucleotides, results in an imbalance in nucleotide pools (an increase in uridine nucleotides and a decrease in inosine/adenine nucleotides), alterations in both DNA and membranes, and promotion of carcinogenesis in the liver initiated by chemical carcinogens. Agents such as adenine and allopurinol, which inhibit the metabolism of orotic acid and thereby decrease the formation of uridine nucleotides, and galactosamine, which traps uridine nucleotides, inhibited the promotional effects of orotic acid in the liver. These results suggested that orotic acid needs to be metabolized to uridine nucleotides and the creation of a subsequent imbalance in nucleotide pools is important for the promotional effects of orotic acid. To determine whether the creation of a nucleotide pool imbalance is a more general mechanism of tumor promotion, two lines of approach were investigated. One was to determine the effect of orotic acid on promotion of carcinogenesis in other organs, and the second approach was to determine how to induce nucleotide pool imbalances by means other than orotic acid administration. It is interesting to note that orotic acid promotes carcinogenesis in duodenum initiated by azoxymethane. Regarding the second approach, it became apparent that several metabolic disturbances result in increased orotic acid synthesis and alterations in nucleotide pools.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1987

42. [Studies on the toxicity of thiaminedisulfide monoorotate. Short communication (author's transl)].

Author

Szirmai E, Szirmai M, McGuigan FJ, and Klosa J

Subjects

Animals, Female, Lethal Dose 50, Male, Mice, Orotic Acid toxicity, Thiamine toxicity, Time Factors, Orotic Acid analogs & derivatives, Thiamine analogs & derivatives

Abstract

The water soluble thiaminedisulfide monoorotate (thiooratin) was studied in mice and rats for its acute and subchronic toxicity. After continuous administration over 8 weeks no organic damages, in particular no fatty livers, were found.

Published

1977

43. The effect of nonviral liver damage on the T-lymphocyte helper/suppressor ratio.

Author

Klein A, Pappas SC, Gordon P, Wong A, Kellen J, Kolin A, Robinson JB, and Malkin A

Subjects

Animals, Chemical and Drug Induced Liver Injury pathology, Galactosamine toxicity, Leukocyte Count, Necrosis, Orotic Acid toxicity, Rats, Chemical and Drug Induced Liver Injury immunology, T-Lymphocytes immunology, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Regulatory immunology

Abstract

In the present investigation an attempt was made to ascertain whether nonviral liver impairment in rats affects the THelper/TSuppressor ratio. Two hepatotoxic agents were used: (i) galactosamine (GA), which causes a drug-induced hepatitis-like damage, and (ii) orotic acid (OA), which induces fatty changes. Since these two substances act as antidotes to one another they were administered to rats either separately or simultaneously. GA caused severe liver damage documented by a 104-, 48-, and 1.6- fold rise in the plasma concentrations of ALT, AST, and ALP and by multiple foci of hepatocyte necrosis. This was followed by a drop in TH/TS ratio from 2.25 observed in the controls to 0.89 in the GA-treated rats. All of these phenomena were prevented by concurrent administration of GA and OA. OA alone did not show an effect on the liver with respect to changes in plasma enzyme concentrations and by light microscopic analysis. However, OA caused a drop in the TH/TS ratio from 2.25 to 1.55. Neither GA nor OA produced a change in TH/TS ratios in in vitro experiments.

Published

1988

44. The mechanism of inhibition of lipoprotein synthesis by orotic acid.

Author

Roheim PS, Switzer S, Girard A, and Eder HA

Subjects

Animals, Cholesterol toxicity, Dietary Fats toxicity, Perfusion, Rats, Fatty Liver etiology, Lipoproteins biosynthesis, Orotic Acid pharmacology, Orotic Acid toxicity

Published

1965

45. [Contribution to the toxicity of Neotan].

Author

Müller J, Zajícová P, and Sobek V

Subjects

Animals, Dosage Forms, Kidney drug effects, Mice, Neomycin toxicity, Orotic Acid toxicity

Published

1969

46. Toxicological studies with Kavaform.

Author

Hapke HJ, Sterner W, Heisler E, and Bräuer H

Subjects

Animals, Appetite drug effects, Blood Cell Count, Blood Coagulation drug effects, Blood Glucose, Body Weight drug effects, Dogs, Female, Fetus drug effects, Male, Metabolism drug effects, Rats, Transaminases blood, Dioxoles toxicity, Lactones toxicity, Magnesium toxicity, Orotic Acid toxicity, Plants, Medicinal

Published

1971

47. Fatty liver induction by orotic acid.

Subjects

Humans, Fatty Liver, Liver Diseases, Orotic Acid toxicity

Published

1960

48. A salt of orotic acid and neomycin.

Author

Sobek V and Král Z

Subjects

Animals, Body Weight drug effects, Diaphragm drug effects, Guinea Pigs, Heart drug effects, In Vitro Techniques, Kidney drug effects, Kidney pathology, Mice, Muscle Contraction drug effects, Neomycin analysis, Neomycin blood, Neomycin toxicity, Organ of Corti pathology, Orotic Acid analysis, Orotic Acid blood, Orotic Acid toxicity, Rats, Salts pharmacology, Neomycin pharmacology, Orotic Acid pharmacology

Published

1967

49. Vitamin E and hepatotoxic agents. 2. Lipid peroxidation and poisoning with orotic acid, ethanol and thioacetamide in rats.

Author

Bunyan J, Cawthorne MA, Diplock AT, and Green J

Subjects

Aldehydes analysis, Aniline Compounds pharmacology, Animals, Fatty Liver chemically induced, In Vitro Techniques, Liver analysis, Liver pathology, Peroxides metabolism, Rats, Selenium pharmacology, Triglycerides analysis, Vitamin E Deficiency metabolism, Amides toxicity, Ethanol toxicity, Lipid Metabolism, Liver drug effects, Orotic Acid toxicity, Sulfhydryl Compounds toxicity, Vitamin E pharmacology

Published

1969

50. Porphyria induced in rats by orotic acid and the effect of adenine-5'-monophosphoric acid.

Author

Gajdos A, Gajdos-Török M, Palma-Carlos A, and Palma-Carlos L

Subjects

Adenosine Triphosphate analysis, Animals, Erythrocytes analysis, Feces analysis, Levulinic Acids, Ligases metabolism, Liver cytology, Liver enzymology, Mitochondria enzymology, Rats, Adenine Nucleotides pharmacology, Orotic Acid toxicity, Porphyrias chemically induced

Published

1966