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1. 'Rhizoproduct', a biofertilizer containing spores of Bacillus cereus strain RS87 for early rice seedling enhancement and with potential for partial fertilizer substitution

Author

Kanchalee Jetiyanon, Sakchai Wittaya-Areekul, Pinyupa Plianbangchang, and Ornrat Lohitnavy

Subjects
Rhizo-product, early rice seedlings promotion, 50% chemical fertilizer replacement, rice yield enhancement, Technology, Technology (General), T1-995, Science, Science (General), Q1-390
Abstract

The objectives of this study were to investigate the seed to seedling enhancement of Rhizo-product under laboratory conditions and to explore the efficacy of the product for partial fertilizer substitution in rice growth and yield production under submerged soil. Results showed that rice seedlings treated with Rhizo-product was significantly promoted compared to the non-bacterized control. Greenhouse experiments revealed that the growth parameters of all rice cultivars treated at 50% recommended fertilizer rate (RFR) and supplemented with Rhizo-product were better than, or equal to, the growth parameters of rice plants treated with full fertilizer rate (FFR) alone. Additionally, yield production of all rice cultivars receiving 50% RFR supplemented with the product was similar to rice treated with FFR alone. In conclusion, Rhizo-product stimulated early rice seed to seedling growth and exhibited growth and yield production at 50% RFR that was comparable to growth and yield production at FFR.

Published
2017

2. Association of HLA-B*5701 Genotypes and Abacavir-Induced Hypersensitivity Reaction: A Systematic Review and Meta-Analysis

Author

Wimonchat Tangamornsuksan, Ornrat Lohitnavy, Chuenjid Kongkaew, Nathorn Chaiyakunapruk, Brad Reisfeld, Norman Charles Scholfield, and Manupat Lohitnavy

Subjects
Therapeutics. Pharmacology, RM1-950, Pharmacy and materia medica, RS1-441
Abstract

OBJECTIVES: This study aimed to systematically review and quantitatively synthesize the association between HLA-B*5701 and abacavir-induced hypersensitivity reaction (ABC-HSR). METHODS: We searched for studies that investigated the association between HLA-B genotype and ABC-HSR and provided information about the frequency of carriers of HLA-B genotypes among cases and controls. We then performed a meta-analysis with a random-effects model to pool the data and to investigate the sources of heterogeneity. RESULTS: From 1,026 articles identified, ten studies were included. Five using clinical manifestation as their diagnostic criteria, 409 and 1,883 subjects were included as cases and controls. Overall OR was 23.6 (95% CI = 15.4 – 36.3). Whereas, the another five studies using confirmed immunologic test as their diagnostic criteria, 110 and 1,968 subjects were included as cases and controls, respectively. The association of ABC-HSR was strong in this populations with HLA-B*5701. Overall OR was 1,056.2 (95% CI = 345.0 – 3,233.3). CONCLUSIONS: Using meta-analysis technique, the association between HLA-B*5701 and ABC-HSR is strong in the studies using immunologic confirmation to identify ABC-HSR. These results support the US FDA recommendations for screening HLA-B*5701 allele before initiating abacavir therapy. This article is open to POST-PUBLICATION REVIEW. Registered readers (see “For Readers”) may comment by clicking on ABSTRACT on the issue’s contents page.

Published
2015
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3. Additive Synergism between Asbestos and Smoking in Lung Cancer Risk: A Systematic Review and Meta-Analysis.

Author

Yuwadee Ngamwong, Wimonchat Tangamornsuksan, Ornrat Lohitnavy, Nathorn Chaiyakunapruk, C Norman Scholfield, Brad Reisfeld, and Manupat Lohitnavy

Subjects
Medicine, Science
Abstract

Smoking and asbestos exposure are important risks for lung cancer. Several epidemiological studies have linked asbestos exposure and smoking to lung cancer. To reconcile and unify these results, we conducted a systematic review and meta-analysis to provide a quantitative estimate of the increased risk of lung cancer associated with asbestos exposure and cigarette smoking and to classify their interaction. Five electronic databases were searched from inception to May, 2015 for observational studies on lung cancer. All case-control (N = 10) and cohort (N = 7) studies were included in the analysis. We calculated pooled odds ratios (ORs), relative risks (RRs) and 95% confidence intervals (CIs) using a random-effects model for the association of asbestos exposure and smoking with lung cancer. Lung cancer patients who were not exposed to asbestos and non-smoking (A-S-) were compared with; (i) asbestos-exposed and non-smoking (A+S-), (ii) non-exposure to asbestos and smoking (A-S+), and (iii) asbestos-exposed and smoking (A+S+). Our meta-analysis showed a significant difference in risk of developing lung cancer among asbestos exposed and/or smoking workers compared to controls (A-S-), odds ratios for the disease (95% CI) were (i) 1.70 (A+S-, 1.31-2.21), (ii) 5.65; (A-S+, 3.38-9.42), (iii) 8.70 (A+S+, 5.8-13.10). The additive interaction index of synergy was 1.44 (95% CI = 1.26-1.77) and the multiplicative index = 0.91 (95% CI = 0.63-1.30). Corresponding values for cohort studies were 1.11 (95% CI = 1.00-1.28) and 0.51 (95% CI = 0.31-0.85). Our results point to an additive synergism for lung cancer with co-exposure of asbestos and cigarette smoking. Assessments of industrial health risks should take smoking and other airborne health risks when setting occupational asbestos exposure limits.

Published
2015
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8. Paraquat exposure and Parkinson’s disease: A systematic review and meta-analysis

Author

Manupat Lohitnavy, Rosarin Sruamsiri, Brad Reisfeld, Wimonchat Tangamornsuksan, C. Norman Scholfield, Ornrat Lohitnavy, and Nathorn Chaiyakunapruk

Subjects
Paraquat, Oncology, medicine.medical_specialty, Parkinson's disease, Health, Toxicology and Mutagenesis, Disease, 010501 environmental sciences, Toxicology, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Risk Factors, Occupational Exposure, Internal medicine, Odds Ratio, medicine, Humans, 0105 earth and related environmental sciences, General Environmental Science, business.industry, Public Health, Environmental and Occupational Health, Parkinson Disease, Environmental Exposure, medicine.disease, 030210 environmental & occupational health, chemistry, Meta-analysis, business
Abstract

To reconcile and unify available results regarding paraquat exposure and Parkinson's disease (PD), we conducted a systematic review and meta-analysis to provide a quantitative estimate of the risk of PD associated with paraquat exposure. Six scientific databases including PubMed, Cochrane libraries, EMBASE, Scopus, ISI Web of Knowledge, and TOXLINE were systematically searched. The overall odds ratios (ORs) with corresponding 95% CIs were calculated using a random-effects model. Of 7,309 articles identified, 13 case control studies with 3,231 patients and 4,901 controls were included into our analysis. Whereas, one prospective cohort studies was included into our systematic review. A subsequent meta-analysis showed an association between PD and paraquat exposure (odds ratio = 1.64 (95% CI: 1.27-2.13

Published
2018
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9. A physiologically-based pharmacokinetic model of methotrexate incorporating hepatic excretion via multidrug-resistance-associated protein 2 (Mrp2) in mice, rats, dogs, and humans

Author

Yasong Lu, Raymond S. H. Yang, Ornrat Lohitnavy, and Manupat Lohitnavy

Subjects
0301 basic medicine, Physiologically based pharmacokinetic modelling, business.industry, Multidrug resistance-associated protein 2, Pharmacology, Rats, Hepatobiliary Elimination, 03 medical and health sciences, Biliary excretion, Mice, 030104 developmental biology, Dogs, Methotrexate, Pharmacokinetics, Liver, Hepatic Excretion, Model simulation, Medicine, Animals, Humans, business, medicine.drug
Abstract

An updated physiologically-based pharmacokinetic (PBPK) model of methotrexate (MTX) was built based on an earlier model developed by Bischoff et al. (1971). MTX has been known to be a substrate of multidrug-resistance-associated protein 2 (Mrp2). A three-dimensional quantitative structure-activity relationship model (3D-QSAR) of Mrp2 was developed by Hirono et al. (2005). In our updated PBPK model of MTX, using the computational chemistry-derived binding affinity (K m ), a Mrp2-mediated biliary excretion process was incorporated as the MTX excretory pathway. Our model simulation results are consistent with numerous datasets obtained from mice, rats, dogs, and humans, at a variety of dose levels. Comparisons were made between our updated PBPK model and the earlier one from Bischoff et al. using a PBPK Index approach. Our new PBPK model was further verified against additional pharmacokinetic datasets from rats under special experimental conditions (cannulated bile duct) and Eisai hyperbirilubinemic rats.

Published
2017

10. Development of a physiologically based pharmacokinetic model of paraquat

Author

Ornrat Lohitnavy, Kritsada Jomprasert, Manupat Lohitnavy, Brad Reisfeld, and Arnon Chitsakhon

Subjects
0301 basic medicine, Paraquat, Physiologically based pharmacokinetic modelling, Pulmonary toxicity, Pharmacology, Models, Biological, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, medicine, Animals, heterocyclic compounds, Tissue Distribution, Kidney, Lung, Herbicides, Transporter, Acute toxicity, Markov Chains, Rats, 030104 developmental biology, medicine.anatomical_structure, chemistry, Monte Carlo Method, 030217 neurology & neurosurgery
Abstract

Paraquat (N, N'-dimethyl-4,4'-bipyridium dichloride) is a potent and widely used herbicide in agricultural countries, including Thailand. The presence of this chemical in the body can lead to toxic effects in the liver, kidney, and lung. Pulmonary toxicity has been identified as the main cause of acute toxicity in animals and humans. Chronic exposure to paraquat is associated with Parkinson's disease in humans. Paraquat is transported into the lungs by neutral amino acid transporter. Therefore, a physiologically based pharmacokinetic (PBPK) model of paraquat was developed with a description of the protein transporter mechanism. To develop a PBPK model of paraquat, a pharmacokinetic study of paraquat in rats was selected from the ThaiLIS and Pubmed database. The selected study contained tissue-specific concentration-time course information such as paraquat concentration levels in liver, kidney and lung. Physiologic parameters were acquired from the literature or determined using a Markov-Chain Monte Carlo (MCMC) technique. The developed PBPK model consisted of 5 organ compartments (i.e. kidney, liver, slowly perfused organs, richly perfuse organs and lung), featuring an incorporation of neutral amino acid transporter in the lung. Our model simulations could explain the data from the literature and adequately describe pharmacokinetics of paraquat in the rats. This developed PBPK model may be able help in understanding of paraquat-induced Parkinson's disease as well as in risk assessment of paraquat.

Published
2017

11. A pharmacokinetic model of drug-drug interaction between clopidogrel and omeprazole at CYP2C19 in humans

Author

Ornrat Lohitnavy, Wimonchat Tangamornsuksan, Pongpak Thiansupornpong, Manupat Lohitnavy, and Thirawut Morasuk

Subjects
Ticlopidine, CYP2B6, medicine.drug_class, Drug-drug interaction, Proton-pump inhibitor, CYP2C19, 030204 cardiovascular system & hematology, Pharmacology, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, medicine, Humans, Drug Interactions, cardiovascular diseases, Omeprazole, Active metabolite, business.industry, Clopidogrel, Cytochrome P-450 CYP2C19, business, circulatory and respiratory physiology, medicine.drug
Abstract

Background: Clopidogrel is a thienopryridine antiplatelet agent commonly used in the management of cardiovascular diseases. Clopidogrel is metabolized by hepatic CYP2C19 and CYP2B6, therefore, co-administration of clopidogrel and CYP2C19 inhibitors can alter pharmacokinetics of clopidogrel. Omeprazole is a proton pump inhibitor used for decreasing gastric acid production. Omeprazole is known to be a potent inhibitor of CYP2C19. Thus when the drugs are simultaneously administered, clopidogrel plasma concentration levels can be increased. However, plasma levels of the active metabolite of clopidogrel can be significantly decreased, thereby, its antiplatelet activity is reduced. Objectives: We aimed to develop a mathematical model describing a drug-drug interaction between clopidogrel and omeprazole in humans. Methods: Searching for pharmacokinetic interaction studies between clopidogrel and omeprazole in humans was performed in PubMed. Six studies were selected into our modeling purposes to develop 3 mathematical models (i.e. 4 studies for clopidogrel alone, 1 study for omeprazole alone and 1 study for clopidogrel-omeprazole interaction). Subsequently, concentration-time course data from the selected studies were extracted. Computer codes and simulations were performed using the Advanced Continuous Simulating Language Extreme (ACSLX) program. Results: We successfully developed 3 mathematical models which are able to describe all of the datasets. Conclusions: Our clopidogrel-omeprazole pharmacokinetic interaction model with a description of competitive inhibition at CYP2C19 could successfully describe concentration-time courses from the selected datasets. Our interaction model may be useful in predicting plasma levels of clopidogrel and its active metabolite.

Published
2017
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13. Comparative pharmacokinetics and bioequivalence of two tablet formulations of 2 mg risperidone in healthy Thai male volunteers

Author

A Srichaiya, J Sayasathid, Nantaka Khorana, S Maphanta, and Ornrat Lohitnavy

Subjects
Adult, Male, Adolescent, medicine.drug_class, Chemistry, Pharmaceutical, Cmax, Atypical antipsychotic, Bioequivalence, Pharmacology, Pharmacokinetics, Humans, Medicine, Pharmacology (medical), Active metabolite, Cross-Over Studies, Risperidone, business.industry, Crossover study, Bioavailability, Therapeutic Equivalency, Area Under Curve, business, Antipsychotic Agents, Tablets, medicine.drug
Abstract

Background Risperidone is an atypical antipsychotic drug with potent serotonin and moderate dopamine antagonistic properties. It possesses good bioavailability following oral administration. Risperidone is primarily converted by the cytochrome P450 2D6 (CYP2D6) and 3A4 (CYP3A4) enzymes to 9-hydroxyrisperidone, its active metabolite with equivalent potency to the parent compound. Objective This study aimed to compare the pharmacokinetics and determine bioequivalence of two risperidone immediate release oral tablets, a test formulation (Risperidone GPO® or "Test") and a reference formulation (Risperdal® or "Reference"). Method A single-dose, randomized, fasting, 2-period, 2-sequence, crossover study design with a 2-week washout period was conducted in 23 healthy Thai male volunteers. Blood samples were collected predose and at 0.25, 0.5, 0.75, 1, 1.5, 2, 3, 4, 5, 6, 8, 12, 24, 36, 48, 72 and 96 h following an oral administration of 2 mg risperidone. The plasma concentrations of risperidone and 9-hydroxyrisperidone were determined by using a validated HPLC method. Pharmacokinetic parameters of Test and Reference were obtained by noncompartmental analysis. Results The 90% confidence intervals for Test/Reference ratios of the pharmacokinetic parameters (Cmax, AUC0-t and AUC0-∞) of both risperidone and its active metabolite (9-hydroxyrisperidone) fell within the acceptable bioequivalence range (80 - 125%) according to ASEAN guideline. Conclusion The two risperidone formulations are bioequivalent. The test formulation may be used for generic substitution where applicable.

Published
2011
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14. An Updated Physiologically Based Pharmacokinetic Model for Hexachlorobenzene: Incorporation of Pathophysiological States following Partial Hepatectomy and Hexachlorobenzene Treatment

Author

Ornrat Lohitnavy, Amanda K. Ashley, Raymond S. H. Yang, Yasong Lu, Micaela B. Reddy, and Manupat Lohitnavy

Subjects
Male, Physiologically based pharmacokinetic modelling, medicine.medical_treatment, Lumen (anatomy), Absorption (skin), Pharmacology, Toxicology, Models, Biological, Rats, Sprague-Dawley, chemistry.chemical_compound, Pharmacokinetics, Hexachlorobenzene, medicine, Animals, Hepatectomy, Bioassay, Rats, Wistar, Glutathione Transferase, Rats, Inbred F344, Rats, Liver, chemistry, Female, Xenobiotic
Abstract

Physiologically based pharmacokinetic (PBPK) modeling is generally used for describing xenobiotic disposition in animals and humans with normal physiological conditions. We describe here an updated PBPK model for hexachlorobenzene (HCB) in male F344 rats with the incorporation of pathophysiological conditions. Two more features contribute to the distinctness of this model from the earlier published versions. This model took erythrocyte binding into account, and a particular elimination process of HCB, the plasma-to-gastrointestinal (GI) lumen passive diffusion (i.e., exsorption), was incorporated. Our PBPK model was developed using data mined from multiple pharmacokinetic studies in the literature, and then modified to simulate HCB disposition under the conditions of our integrated pharmacokinetics/liver foci bioassay. This model included plasma, erythrocytes, liver, fat, rapidly and slowly perfused compartments, and GI lumen. To account for the distinct characteristics of HCB absorption, the GI lumen was split into an upper and a lower part. HCB was eliminated through liver metabolism and the exsorption process. The pathophysiological changes after partial hepatectomy, such as alterations in the liver and body weights and fat volume, were incorporated in our model. With adjustment of the transluminal diffusion-related parameters, the model adequately described the data from the literature and our bioassay. Our PBPK model simulation suggests that HCB absorption and exsorption processes depend on exposure conditions; different exposure conditions dictate different absorption and exsorption rates. This model forms a foundation for our further exploration of the quantitative relationship between HCB exposure and development of preneoplastic liver foci.

Published
2006
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15. Reduced oral itraconazole bioavailability by antacid suspension

Author

O. Thangkeattiyanon, Ornrat Lohitnavy, Manupat Lohitnavy, and W. Srichai

Subjects
Adult, Male, Antifungal Agents, Magnesium Hydroxide, Adolescent, Itraconazole, medicine.medical_treatment, Cmax, Biological Availability, Aluminum Hydroxide, Pharmacology, Intestinal absorption, Suspensions, Pharmacokinetics, Oral administration, Antacid, medicine, Humans, Pharmacology (medical), Cross-Over Studies, Chemistry, Area under the curve, Middle Aged, Crossover study, Drug Combinations, Intestinal Absorption, Area Under Curve, Antacids, Drug Antagonism, medicine.drug
Abstract

Summary Aims: To investigate the effects of antacid suspension on oral absorption of itraconazole. Methods: A randomized, open-labelled, two-period, crossover study with a 1-week washout period was conducted in 12 healthy Thai male volunteers. The participants were allocated in either treatment A or B in the first period. In treatment A, the volunteers were orally administered with 200 mg of itraconazole alone. In treatment B, the volunteers were administered orally with 200 mg of itraconazole co-administered with antacid suspension. Serial serum samples were collected over the period of 24 h and subsequently analysed by using a validated high-pressure liquid chromatographic method with ultraviolet detection. Pharmacokinetic parameters were determined by non-compartmental analysis. Results: Time to reach maximal concentration (Tmax), maximal concentration (Cmax) and area under the curve (AUC0--∞) were markedly decreased in antacid-treated group. Tmax for treatment A was 3·0 ± 0·4 and 5·1 ± 2·7 h for treatment B. Cmax and AUC0--∞ of treatments A and B were 146·3 ± 70·5 vs. 43·6 ± 16·9 (ng/mL) and 1928·5 ± 1114·6 vs. 654·8 ± 452·2 (ng·h/mL) respectively. 90% Confidence interval (90% CI) of Cmax and AUC0--∞ were 24·1–42·1 and 16·2–65·9 respectively. Conclusions: Rate and extent of itraconazole oral absorption were markedly decreased by concurrent use of antacid suspension. Hence, co-administration of itraconazole and antacid suspension should be avoided.

Published
2005
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16. Average bioequivalence study of clarithromycin tablets in healthy male volunteers

Author

Sareekan K, Manupat Lohitnavy, W. Chaiyaput, and Ornrat Lohitnavy

Subjects
Pharmacology, business.industry, Area under the curve, Cmax, Bioequivalence, Crossover study, Animal science, Pharmacokinetics, Clarithromycin, Anesthesia, medicine, Pharmacology (medical), business, Volunteer, medicine.drug, Antibacterial agent
Abstract

Summary Objective: To evaluate the average bioequivalence of two formulations of 500 mg clarithromycin tablets in 24 healthy Thai male volunteers. Methods: In a randomized, single dose, fasting state, two-period, crossover study design with a 1-week washout period, each subject received a 500 mg clarithromycin tablet. Plasma samples were collected over a 24-h period after administration and were analysed by using a validated HPLC-ECD method. Pharmacokinetic parameters were determined by using non-compartmental analysis. Results: The time to reach the maximal concentration (tmax, h), the peak concentration (Cmax, ng/mL) and the area under the curve (AUC0–∞, ng h/mL) of the Reference and Test formulations were 2·0 ± 0·9 vs. 1·8 ± 1·1, 3018 ± 841 vs. 3014 ± 752 and 23142 ± 7348 vs. 22810 ± 6027, respectively. The 90% confidence interval of Cmax and AUC0–∞ were 90·6–109·4 and 89·6–110·1%. Conclusion: Bioequivalence between the Test and Reference formulation can be concluded.

Published
2003
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17. Average bioequivalence of generic clarithromycin tablets in healthy thai male volunteers

Author

Prawit Taytiwat, Sanglar Polnok, Kannika Sareekan, Ornrat Lohitnavy, and Manupat Lohitnavy

Subjects
Male, Pharmacology, Chromatography, business.industry, Area under the curve, Pharmaceutical Science, General Medicine, Bioequivalence, Thailand, Crossover study, Bioavailability, Therapeutic Equivalency, Pharmacokinetics, Clarithromycin, medicine, Drugs, Generic, Humans, Pharmacology (medical), business, Volunteer, Tablets, Antibacterial agent, medicine.drug
Abstract

The objective of this study was to assess bioequivalence of 500-mg clarithromycin tablets in 24 healthy volunteers. In a randomized, single dose, fasting state, two-period, crossover study design with a 1-week washout period, each subject received a 500-mg clarithromycin tablet. Plasma samples were collected over a 24-h period after administration and were analyzed by using a validated method using high performance liquid chromatography (HPLC) with electrochemical detection. The time to reach the maximal concentration (t(max),h), the peak concentration (C(max),ng/ml) and the area under the curve (AUC(0- infinity),ng h/ml) of the Reference and Test formulations were 2.1+/-0.7 vs 2.1+/-0.7, 2474+/-702 vs 2559+/-744 and 15803+/-6120 vs 17683+/-6650, respectively. Relative bioavailability was 1.12. The 90% confidence interval (90% CI) of C(max) and AUC(0- infinity) were 95.6-110.8% and 3.5-122.0%, respectively. Bioequivalence between the test and reference preparation can be concluded.

Published
2003
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18. A possible role of multidrug resistance-associated protein 2 (Mrp2) in hepatic excretion of PCB126, an environmental contaminant: PBPK/PD modeling

Author

Ornrat Lohitnavy, Raymond S. H. Yang, Yasong Lu, Laura S. Chubb, Manupat Lohitnavy, and Shuichi Hirono

Subjects
Male, Physiologically based pharmacokinetic modelling, Pharmacology, Toxicology, Models, Biological, Rats, Sprague-Dawley, Pharmacokinetics, Animals, Computer Simulation, biology, Chemistry, Multidrug resistance-associated protein 2, Area under the curve, Transporter, Aryl hydrocarbon receptor, Polychlorinated Biphenyls, Multidrug Resistance-Associated Protein 2, Rats, Inbred F344, Rats, Liver, Pharmacodynamics, Toxicity, biology.protein, Environmental Pollutants, Female, Multidrug Resistance-Associated Proteins
Abstract

3,3',4,4',5'-Pentachlorobiphenyl (PCB126) is a carcinogenic environmental pollutant and its toxicity is mediated through binding with aryl hydrocarbon receptor (AhR). Earlier, we found that PCB126 treated F344 rats had 110-400 times higher PCB126 concentration in the liver than in the fat. Protein binding was suspected to be a major factor for the high liver concentration of PCB126 despite its high lipophilicity. In this research, we conducted a combined pharmacokinetic/pharmacodynamic study in male F344 rats. In addition to blood and tissue pharmacokinetics, we use the development of hepatic preneoplastic foci (glutathione-S-transferase placental form [GSTP]) as a pharmacodynamic endpoint. Experimental data were utilized for building a physiologically based pharmacokinetic/pharmacodynamic (PBPK/PD) model. PBPK/PD modeling was consistent with the experimental PK and PD data. Salient features of this model include: (1) bindings between PCB126 and hepatic proteins, particularly the multidrug resistance-associated protein (Mrp2), a protein transporter; (2) Mrp2-mediated excretion; and (3) a relationship between area under the curve of PCB126 in the livers and % volume of GSTP foci. Mrp2 involvement in PCB126 pharmacokinetics is supported by computational chemistry calculation using a three-dimensional quantitative structure-activity relationship model of Mrp2 developed by S. Hirono et al. (2005, Pharm. Res. 22, 260-269). This work, for the first time, provided a plausible role of a versatile hepatic transporter for drugs, Mrp2, in the disposition of an important environmental pollutant, PCB126.

Published
2008

19. Quantitative analysis of liver GST-P foci promoted by a chemical mixture of hexachlorobenzene and PCB 126: implication of size-dependent cellular growth kinetics

Author

Yihua Xu, Rory B. Conolly, Yasong Lu, Raymond S. H. Yang, Ornrat Lohitnavy, Micaela B. Reddy, Elizabeth E Eickman, Amanda K. Ashley, Lisa Gerjevic, and Manupat Lohitnavy

Subjects
Male, Chemical compound, Carcinogenicity Tests, Health, Toxicology and Mutagenesis, Kinetics, Administration, Oral, Toxicology, Models, Biological, chemistry.chemical_compound, Hexachlorobenzene, Bioassay, Animals, Computer Simulation, Carcinogen, Dose-Response Relationship, Drug, Cell growth, General Medicine, Glutathione, Polychlorinated Biphenyls, Rats, Inbred F344, Rats, Biochemistry, chemistry, Glutathione S-Transferase pi, Liver, Carcinogens, Biological Assay, Environmental Pollutants, Quantitative analysis (chemistry)
Abstract

The objectives of this study were twofold: (1) evaluating the carcinogenic potential of the mixture of two persistent environmental pollutants, hexachlorobenzene (HCB) and 3,3′,4,4′,5-pentachlorobiphenyl (PCB 126), in an initiation-promotion bioassay involving the development of π glutathione S-transferase (GST-P) liver foci, and (2) analyzing the GST-P foci data using a biologically-based computer model (i.e., clonal growth model) with an emphasis on the effect of focal size on the growth kinetics of initiated cells. The 8-week bioassay involved a series of treatments of initiator, two-thirds partial hepatectomy, and daily oral gavage of the mixture of two doses in male F344 rats. The mixture treatment significantly increased liver GST-P foci development, indicating carcinogenic potential of this mixture. Our clonal growth model was developed to simulate the appearance and development of initiated GST-P cells in the liver over time. In the model, the initiated cells were partitioned into two subpopulations with the same division rate but different death rates. Each subpopulation was further categorized into single cells, mini- (2–11 cells), medium- (12–399 cells), and large-foci (>399 cells) with different growth kinetics. Our modeling suggested that the growth of GST-P foci is size-dependent; in general, the larger the foci, the higher the rate constants of division and death. In addition, the modeling implied that the two doses promoted foci development in different manners even though the experimental foci data appeared to be similar between the two doses. This study further illustrated how clonal growth modeling may facilitate our understanding in chemical carcinogenic process.

Published
2007

20. Additive Synergism between Asbestos and Smoking in Lung Cancer Risk: A Systematic Review and Meta-Analysis

Author

Manupat Lohitnavy, Nathorn Chaiyakunapruk, C. Norman Scholfield, Wimonchat Tangamornsuksan, Yuwadee Ngamwong, Brad Reisfeld, and Ornrat Lohitnavy

Subjects
Male, medicine.medical_specialty, Pathology, Lung Neoplasms, Databases, Factual, lcsh:Medicine, medicine.disease_cause, Asbestos, Risk Factors, Internal medicine, Chrysotile, Epidemiology, medicine, Humans, lcsh:Science, Lung cancer, Multidisciplinary, business.industry, lcsh:R, Smoking, Case-control study, Odds ratio, medicine.disease, Relative risk, Cohort, lcsh:Q, Female, business, Research Article
Abstract

Smoking and asbestos exposure are important risks for lung cancer. Several epidemiological studies have linked asbestos exposure and smoking to lung cancer. To reconcile and unify these results, we conducted a systematic review and meta-analysis to provide a quantitative estimate of the increased risk of lung cancer associated with asbestos exposure and cigarette smoking and to classify their interaction. Five electronic databases were searched from inception to May, 2015 for observational studies on lung cancer. All case-control (N = 10) and cohort (N = 7) studies were included in the analysis. We calculated pooled odds ratios (ORs), relative risks (RRs) and 95% confidence intervals (CIs) using a random-effects model for the association of asbestos exposure and smoking with lung cancer. Lung cancer patients who were not exposed to asbestos and non-smoking (A-S-) were compared with; (i) asbestos-exposed and non-smoking (A+S-), (ii) non-exposure to asbestos and smoking (A-S+), and (iii) asbestos-exposed and smoking (A+S+). Our meta-analysis showed a significant difference in risk of developing lung cancer among asbestos exposed and/or smoking workers compared to controls (A-S-), odds ratios for the disease (95% CI) were (i) 1.70 (A+S-, 1.31-2.21), (ii) 5.65; (A-S+, 3.38-9.42), (iii) 8.70 (A+S+, 5.8-13.10). The additive interaction index of synergy was 1.44 (95% CI = 1.26-1.77) and the multiplicative index = 0.91 (95% CI = 0.63-1.30). Corresponding values for cohort studies were 1.11 (95% CI = 1.00-1.28) and 0.51 (95% CI = 0.31-0.85). Our results point to an additive synergism for lung cancer with co-exposure of asbestos and cigarette smoking. Assessments of industrial health risks should take smoking and other airborne health risks when setting occupational asbestos exposure limits.

Published
2015
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21. A pharmacokinetic model of the gastrointestinal tract consisting of two segments can describe the concentration-time course of itraconazole

Author

Lu Y, Ornrat Lohitnavy, and Manupat Lohitnavy

Subjects
Pharmacology, Male, Gastrointestinal tract, Clinical Trials as Topic, Antifungal Agents, Time Factors, business.industry, Itraconazole, Metabolic Clearance Rate, Administration, Oral, Biological Availability, Models, Biological, Gastrointestinal Tract, Pharmacokinetics, Time course, Medicine, Humans, Pharmacology (medical), business, medicine.drug
Published
2006

22. Bioequivalence study of two formulations of simvastatin tablets in healthy Thai volunteers

Author

Ornrat Lohitnavy, Sanglar Polnok, Kasinee Chaijittiprasert, Manupat Lohitnavy, and Prawit Taytiwat

Subjects
Adult, Male, Simvastatin, Spectrometry, Mass, Electrospray Ionization, Adolescent, Metabolite, Chemistry, Pharmaceutical, Cmax, Bioequivalence, Pharmacology, Dosage form, chemistry.chemical_compound, Pharmacokinetics, Drug Discovery, medicine, Humans, Chromatography, High Pressure Liquid, Cross-Over Studies, business.industry, Anticholesteremic Agents, Middle Aged, Thailand, Crossover study, Bioavailability, chemistry, Therapeutic Equivalency, Area Under Curve, business, medicine.drug, Half-Life, Tablets
Abstract

The bioequivalence of two formulations of 10 mg tablets of simvastatin (CAS 79902-63-9), Vascor® as test and a commercially available preparation as reference, in 18 healthy Thai male volunteers was assessed. In a randomized, single dose, two-period, crossover study design with a 1 -week wash-out period, each subject received 4 tablets of 10-mg simvastatin tablets. Plasma samples were collected over a 24-h period after administration. Subsequently, plasma concentrations of simvastatin and its hydroxy acid metabolite were analyzed by using LC/MS/MS. Pharmacokinetic parameters were determined by using non-compart-mental analysis. The results showed that 90% confidence intervals of the peak concentration (Cmax) and the area under the concentration-time curve (AUC) of simvastatin and its hydroxy acid metabolite of reference and test were within 80 %–125 %. Consequently the bioequivalence of these two preparations can be concluded.

Published
2004

23. Relative bioavailability study of 20-mg enalapril tablets in healthy male volunteers

Author

Ornrat, Lohitnavy, Manupat, Lohitnavy, Sanglar, Polnok, and Prawit, Taytiwat

Subjects
Adult, Male, Volunteers, Cross-Over Studies, Adolescent, Enalapril, Enalaprilat, Biological Availability, Humans, Middle Aged, Antihypertensive Agents
Abstract

The pharmacokinetic and relative bioavailability studies of 20-mg enalapril tablets, the test product manufactured by Biolab, Thailand compared to the reference product (Merck SharpDohme, USA) was conducted in 14 healthy Thai male volunteers following a single dose, two-period, crossover design. Each subject received 20-mg enalapril tablets of both formulations with a 1-week washout period. Plasma samples collected over a 24-h period after administration were analyzed by LC/MS/MS. Pharmacokinetic parameters were determined by using non-compartmental analysis. Regarding bioequivalence testing, the 90 per cent confidence intervals of Cmax and AUC(0-infinity) ratios (test/reference) of enalapril were 101.8-134.9 per cent and 105.9-121.4 per cent and those of enalaprilat were 104.2-122.3 per cent and 104.5-118.1 per cent. Based on the European bioequivalence guideline, the 90 per cent confidence intervals of Cmax and AUC(0-infinity) ratios of both parent and metabolite forms were within the acceptable ranges of 70-143 per cent and 80-125 per cent, respectively. It was concluded that the test formulation was bioequivalent to the reference formulation and both formulations can be used interchangeably in clinical practice.

Published
2003

24. Average bioequivalence of clarithromycin immediate released tablet formulations in healthy male volunteers

Author

Sanglar Polnok, W. Chaiyaput, Sakchai Wittaya-areekul, Sareekan K, Manupat Lohitnavy, and Ornrat Lohitnavy

Subjects
Adult, Male, Cmax, Pharmaceutical Science, Biological Availability, Pharmacology, Bioequivalence, Dosage form, Pharmacokinetics, Clarithromycin, Drug Discovery, Medicine, Humans, Chromatography, High Pressure Liquid, Antibacterial agent, Chromatography, Cross-Over Studies, business.industry, Organic Chemistry, Area under the curve, Crossover study, Bioavailability, Anti-Bacterial Agents, Solubility, Therapeutic Equivalency, Area Under Curve, business, Half-Life, Tablets
Abstract

The objective of this study was to assess average bioequivalence of two immediate released tablet formulations of 500-mg clarithromycin tablets in 24 healthy Thai male volunteers. In a randomized, single dose, fasting state, two-period, crossover study design with a 1-week washout period, each subject received a 500-mg clarithromycin tablet. Plasma samples were collected over a 24-hour period after oral administration and were analyzed by using a validated method using high performance liquid chromatography with electrochemical detection. Pharmacokinetic parameters were determined by using noncompartmental analysis. The time to reach the maximal concentration (tmax, h), the peak concentration (Cmax, ng/mL), and the area under the curve (AUC0-infinity, ng x h/mL) of the Reference and Test formulations were 2.0 +/- 0.8 vs. 2.2 +/- 0.9, 2793 +/- 1338 vs. 2642 +/- 1344, and 17912 +/- 7360 vs. 17660 +/- 7992, respectively. Relative bioavailability was 0.99. The 90% confidence interval of Cmax and AUC0-infinity were 82.6-112.1% and 84.7-112.0%. Bioequivalence between the Test and Reference formulation can be concluded.

Published
2003

25. Bioequivalence study of enalapril tablets in healthy Thai male volunteers

Author

Ornrat, Lohitnavy, Manupat, Lohitnavy, Prawit, Taytiwat, and Sanglar, Polnok

Subjects
Adult, Male, Cross-Over Studies, Adolescent, Enalapril, Therapeutic Equivalency, Confidence Intervals, Humans, Angiotensin-Converting Enzyme Inhibitors, Middle Aged, Thailand
Abstract

The bioequivalence study of 5-mg enalapril tablets, Enaril (Biolab, Thailand) compared to Renitec (Merck SharpDohme, USA) was conducted in 14 healthy Thai male volunteers following a single dose, two-period, crossover design. Each subject received 4 tablets of 5-mg enalapril tablets of both formulations with a 1-week washout period. Plasma samples collected over a 24-hour period after administration were analyzed by LC/MS/MS. Pharmacokinetic parameters were determined by using non-compartmental analysis. Regarding bioequivalence testing, the 90 per cent confidence intervals of Cmax and AUC(0-infinity) ratios (Enaril/Renitec) of enalapril were 86.3-126.1 per cent and 93.0-118.5 per cent and those of enalaprilat were 86.4-124.1 per cent and 90.3-116.8 per cent. Based on the European bioequivalence guideline, the 90 per cent confidence interval of Cmax and AUC(0-infinity) ratios of both parent and metabolite forms were within acceptable ranges of 70-143 per cent and 80-125 per cent, respectively. It was concluded that Enaril 5 mg tablet was bioequivalent to Renitec 5 mg tablet.

Published
2002

26. Bioequivalence study of ondansetron tablet in healthy Thai male volunteers

Author

Manupat, Lohitnavy, Kasinee, Chaijittiprasert, Sanglar, Polnok, Ornrat, Lohitnavy, and Prawit, Taytiwat

Subjects
Adult, Male, Adolescent, Therapeutic Equivalency, Reference Values, Administration, Oral, Antiemetics, Humans, Middle Aged, Thailand, Ondansetron, Tablets
Abstract

To assess the average bioequivalence of two formulations of 8-mg ondansetron tablets--test product (Unison Laboratories, Thailand) and reference product (Glaxo Wellcome, USA)--in 14 healthy Thai male volunteers.In a randomized, single dose, fasting, two-period, crossover study design with a 1-week washout period, each subject received an 8-mg ondansetron tablet. Serum samples were collected over a 24-hour period after administration. Subsequently serum concentrations of ondansetron were analyzed by using a validated HPLC-UV method. Pharmacokinetic parameters were determined by using non-compartmental analysis.No significant difference was observed in any of the pharmacokinetic parameters analyzed. The time to reach the maximal concentration (Tmax, hour), the peak concentration (Cmax, ng/ ml) and the area under the concentration-time curve (AUC(0-infinity), ng x h/ml) of ondansetron for reference and test preparations were 2.6 + 1.8 vs 2.2 + 0.6, 49.5 +/- 18.9 vs 48.5 +/- 13.7 and 352.2 +/- 184.7 vs 323.8 +/- 154.5, respectively. The 90 per cent confidence intervals for Test/Reference ratio of Cmax and AUC(0-infinity) were found within the bioequivalence range of 80-125 per cent (90.3-110.0% and 88.4-99.6%, respectively).The bioequivalence of these two ondansetron preparations was demonstrated.

Published
2002

27. Increase in Lactate Dehydrogenase Isoenzyme-4 and Splenocyte Toxicity in Methomyl-Treated Rats

Author

Ornrat Lohitnavy and Palarp Sinhaseni

Subjects
carbamates, cholinesterases, insecticides, lactate dehydrogenase, methomyl, rats, spelnocyte, splenotoxicity, insekticidi, karbamati, kolinesteraza, laktat dehidrogenaze, metomil, slezena, štakori
Abstract

The toxic effect of methomyl was studied in rats after a single or repeated oral administration. Rats treated with a single dose of methomyl (3, 5, or 7 mg/kg) showed significant increase (P, Istraživani su učinci karbamatnog insekticida metomila u štakora. Nakon jednokratne peroralne doze od 3, 5 ili 7 mg/kg nađeno je značajno povećanje sveukupne aktivnosti laktat dehidrogenaze (LDH) nakon prvog dana tretmana. Najveća je aktivnost utvrđena trećeg dana nakon tretmana metomilom u dozi od 7 mg/kg. Enzimska aktivnost postepeno se smanjivala i sedmoga se dana normalizirala. Posebno je zapaženo povećanje aktivnosti izoenzima LDH-3 i LDH-4. U posebnim je pokusima utvrđeno značajno smanjenje težine slezene i vijabilnosti splenocita u štakora tretiranih sa 6 mg/kg i 8 mg/kg metomila i to nakon prvog i nakon trećeg dana tretmana. Toksični učinci na slezenu mogli su se spriječiti pretretiranjem sa 60 mg/kg N-acetilcisteina. Prema rezultatima ovih pokusa čini se da bi toksični učinak metomila na slezenu mogao biti izravan učinak metomila na stanice slezene a ne putem kolinergičnog mehanizma. Važnost ovakvog citotoksičnog učinka i mehanizme citotoksičnosti i njihove povezanosti s reaktivnim oksidativnim procesima pri staničnom oštećenju valja još istraživati.

Published
1998

28. Average bioequivalence of generic clarithromycin tablets in healthy thai male volunteers.

Author

Ornrat Lohitnavy, Manupat Lohitnavy, Kannika Sareekan, Sanglar Polnok, and Prawit Taytiwat

Subjects
*THERAPEUTIC equivalency in drugs, *LIQUID chromatography, *ELECTROCHEMISTRY, *CHEMISTRY, *PHYSIOLOGY
Abstract

The objective of this study was to assess bioequivalence of 500-mg clarithromycin tablets in 24 healthy volunteers. In a randomized, single dose, fasting state, two-period, crossover study design with a 1-week washout period, each subject received a 500-mg clarithromycin tablet. Plasma samples were collected over a 24-h period after administration and were analyzed by using a validated method using high performance liquid chromatography (HPLC) with electrochemical detection. The time to reach the maximal concentration (tmax,h), the peak concentration (Cmax,ng/ml) and the area under the curve (AUC0–∞,ng h/ml) of the Reference and Test formulations were 2.1±0.7 vs 2.1±0.7, 2474±702 vs 2559±744 and 15803±6120 vs 17683±6650, respectively. Relative bioavailability was 1.12. The 90% confidence interval (90% CI) of Cmax and AUC0–∞ were 95.6–110.8% and 3.5–122.0%, respectively. Bioequivalence between the test and reference preparation can be concluded. Copyright © 2003 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published
2003
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29. Association of HLA-B*5701 genotypes and abacavir-induced hypersensitivity reaction: A sysyematic review and meta-analysis

Author

Brad Reisfeld, Norman Charles Scholfield, Wimonchat Tangamornsuksan, Nathorn Chaiyakunapruk, Ornrat Lohitnavy, Manupat Lohitnavy, and Chuenjid Kongkaew

Subjects
medicine.medical_specialty, Genotype, Anti-HIV Agents, MEDLINE, Pharmaceutical Science, lcsh:RS1-441, Human leukocyte antigen, Drug Hypersensitivity, lcsh:Pharmacy and materia medica, Abacavir, Internal medicine, medicine, Humans, Allele, Association (psychology), Alleles, Pharmacology, business.industry, lcsh:RM1-950, Dideoxynucleosides, Hypersensitivity reaction, lcsh:Therapeutics. Pharmacology, HLA-B Antigens, Meta-analysis, Immunology, business, medicine.drug
Abstract

OBJECTIVES: This study aimed to systematically review and quantitatively synthesize the association between HLA-B*5701 and abacavir-induced hypersensitivity reaction (ABC-HSR). METHODS: We searched for studies that investigated the association between HLA-B genotype and ABC-HSR and provided information about the frequency of carriers of HLA-B genotypes among cases and controls. We then performed a meta-analysis with a random-effects model to pool the data and to investigate the sources of heterogeneity. RESULTS: From 1,026 articles identified, ten studies were included. Five using clinical manifestation as their diagnostic criteria, 409 and 1,883 subjects were included as cases and controls. Overall OR was 23.6 (95% CI = 15.4 – 36.3). Whereas, the another five studies using confirmed immunologic test as their diagnostic criteria, 110 and 1,968 subjects were included as cases and controls, respectively. The association of ABC-HSR was strong in this populations with HLA-B*5701. Overall OR was 1,056.2 (95% CI = 345.0 – 3,233.3). CONCLUSIONS: Using meta-analysis technique, the association between HLA-B*5701 and ABC-HSR is strong in the studies using immunologic confirmation to identify ABC-HSR. These results support the US FDA recommendations for screening HLA-B*5701 allele before initiating abacavir therapy.This article is open to POST-PUBLICATION REVIEW. Registered readers (see “For Readers”) may comment by clicking on ABSTRACT on the issue’s contents page.

30. A Possible Role of Multidrug Resistance-Associated Protein 2 (Mrp2) in Hepatic Excretion of PCB126, an Environmental Contaminant: PBPK/PD Modeling.

Author

Manupat Lohitnavy, Yasong Lu, Ornrat Lohitnavy, Laura S. Chubb, Shuichi Hirono, and Raymond S. H. Yang

Subjects
HYDROCARBONS, PROTEIN binding, PHARMACOKINETICS, TRANSFERASES
Abstract

3,3′,4,4′,5′-Pentachlorobiphenyl (PCB126) is a carcinogenic environmental pollutant and its toxicity is mediated through binding with aryl hydrocarbon receptor (AhR). Earlier, we found that PCB126 treated F344 rats had 110–400 times higher PCB126 concentration in the liver than in the fat. Protein binding was suspected to be a major factor for the high liver concentration of PCB126 despite its high lipophilicity. In this research, we conducted a combined pharmacokinetic/pharmacodynamic study in male F344 rats. In addition to blood and tissue pharmacokinetics, we use the development of hepatic preneoplastic foci (glutathione-S-transferase placental form [GSTP]) as a pharmacodynamic endpoint. Experimental data were utilized for building a physiologically based pharmacokinetic/pharmacodynamic (PBPK/PD) model. PBPK/PD modeling was consistent with the experimental PK and PD data. Salient features of this model include: (1) bindings between PCB126 and hepatic proteins, particularly the multidrug resistance–associated protein (Mrp2), a protein transporter; (2) Mrp2-mediated excretion; and (3) a relationship between area under the curve of PCB126 in the livers and % volume of GSTP foci. Mrp2 involvement in PCB126 pharmacokinetics is supported by computational chemistry calculation using a three-dimensional quantitative structure–activity relationship model of Mrp2 developed by S. Hirono et al. (2005, Pharm. Res. 22, 260–269). This work, for the first time, provided a plausible role of a versatile hepatic transporter for drugs, Mrp2, in the disposition of an important environmental pollutant, PCB126. [ABSTRACT FROM AUTHOR]

Published
2008
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