Your search keyword '"Do Gyeong Oh"' showing total 7 results

1. Role of Intestinal Microbiota in Baicalin-Induced Drug Interaction and Its Pharmacokinetics

Author

Keumhan Noh, Youra Kang, Mahesh Raj Nepal, Ki Sun Jeong, Do Gyeong Oh, Mi Jeong Kang, Sangkyu Lee, Wonku Kang, Hye Gwang Jeong, and Tae Cheon Jeong

Subjects

baicalin, baicalein, drug interaction, pharmacokinetics, intestinal microbiota, Organic chemistry, QD241-441

Abstract

Since many glycoside compounds in natural products are hydrolyzed by intestinal microbiota when administered orally, it is of interest to know whether their pharmacological effects are derived from the glycoside itself or from the aglycone form in vivo. An interesting example is baicalin versus baicalein, the aglycone of baicalin, which is contained in some herbs from Labiatae including Scutellaria baicalensis Georgi and Scutellaria lateriflora Linne. The herbs have been extensively used for treatment of inflammatory diseases in Asia. Although there have been numerous reports regarding the pharmacological effects of baicalin and baicalein in vivo and in vitro, some reports indicated that the glycoside form would hardly be absorbed in the intestine and that it should be hydrolyzed to baicalein in advance for absorption. Therefore, the role of metabolism by intestinal microbiota should also be considered in the metabolism of baicalin. In addition, baicalin contains a glucuronide moiety in its structure, by which baicalin and baicalein show complex pharmacokinetic behaviors, due to the interconversion between them by phase II enzymes in the body. Recently, concerns about drug interaction with baicalin and/or baicalein have been raised, because of the co-administration of Scutellaria species with certain drugs. Herein, we reviewed the role of intestinal microbiota in pharmacokinetic characteristics of baicalin and baicalein, with regards to their pharmacological and toxicological effects.

Published

2016

2. Pharmacokinetic Interaction of Chrysin with Caffeine in Rats

Author

Wonku Kang, Keumhan Noh, Ki Sun Jeong, Mahesh Raj Nepal, Yongjoo Choi, Hye Gwang Jeong, Mi Jeong Kang, Tae Cheon Jeong, and Do Gyeong Oh

Subjects

0301 basic medicine, Drug interaction, Pharmacology, 030226 pharmacology & pharmacy, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Caffeine, Drug Discovery, medicine, Pharmacokinetics, Theophylline, Chrysin, Theobromine, Paraxanthine, Chemistry, Propolis, Bioavailability, in vivo, 030104 developmental biology, Molecular Medicine, Original Article, Glucuronide, medicine.drug

Abstract

Pharmacokinetic interaction of chrysin, a flavone present in honey, propolis and herbs, with caffeine was investigated in male Sprague-Dawley rats. Because chrysin inhibited CYP1A-selective ethoxyresorufin O-deethylase and methoxyresorufin O-demethylase activities in enriched rat liver microsomes, the pharmacokinetics of caffeine, a CYP 1A substrate, was studied following an intragastric administration with 100 mg/kg chrysin. In addition to the oral bioavailability of chrysin, its phase 2 metabolites, chrysin sulfate and chrysin glucuronide, were determined in rat plasma. As results, the pharmacokinetic parameters for caffeine and its three metabolites (i.e., paraxanthine, theobromine and theophylline) were not changed following chrysin treatment in vivo, despite of its inhibitory effect on CYP 1A in vitro. The bioavailability of chrysin was found to be almost zero, because chrysin was rapidly metabolized to its sulfate and glucuronide conjugates in rats. Taken together, it was concluded that the little interaction of chrysin with caffeine might be resulted from the rapid metabolism of chrysin to its phase 2 metabolites which would not have inhibitory effects on CYP enzymes responsible for caffeine metabolism.

Published

2016

3. The effect of gut microbiota on drug metabolism

Author

Hye Gwang Jeong, Ghee Hwan Kim, Do Gyeong Oh, Chae Shin Seo, Ji Won Han, Yeon Ji Um, Hyung Gyun Kim, Hyun J. Cho, Jin Sung Kim, Tae Cheon Jeong, and Mi Jeong Kang

Subjects

Drug, media_common.quotation_subject, Metabolite, Gut flora, Toxicology, digestive system, Xenobiotics, Microbiology, Synthetic drugs, chemistry.chemical_compound, fluids and secretions, Animals, Humans, media_common, Pharmacology, biology, Microbiota, General Medicine, Metabolism, biology.organism_classification, Gastrointestinal Tract, stomatognathic diseases, Liver, Pharmaceutical Preparations, chemistry, Biochemistry, Xenobiotic, Drug metabolism, Toxicant

Abstract

Numerous drugs and toxicants must be metabolized to an active form. Metabolic activation by host tissues, such as the liver, has been well studied. However, drug and toxicant metabolism by the intestinal microbiota is an unexplored, but essential, field of study in pharmacology and toxicology. The taxonomic diversity and sheer numbers of the intestinal microbiota, and their capacity to metabolize xenobiotics, underscore the importance of this mode of metabolism.Metabolism by the intestinal microbiota has focused on the natural products of glycosides hydrolyzed by intestinal microbiota enzymes, but not by host tissues. Metabolism of synthetic drugs by the intestinal microbiota has been less-intensively investigated. This review provides an overview of xenobiotic metabolism by the intestinal microbiota of both natural products and synthetic drugs.Metabolism by the intestinal microbiota might result in a different metabolite profile than that produced by host tissues. This could potentially result in either activation or inactivation of the pharmacological and/or toxicological actions of the compound in question. The contribution of the intestinal microbiota to drug metabolism remains relatively unexplored. Therefore, studies of xenobiotic metabolism by the intestinal microbiota need to be included in new drug development as well as classical studies of host tissue metabolism.

Published

2013

4. Role of intestinal microflora in xenobiotic-induced toxicity

Author

Mi Jeong Kang, Hyung Gyun Kim, Jin Sung Kim, Tae Cheon Jeong, Do Gyeong Oh, Hye Gwang Jeong, and Sangkyu Lee

Subjects

Gastrointestinal tract, Biological activity, Metabolism, Biology, Pharmacology, Xenobiotics, Microbiology, Intestines, chemistry.chemical_compound, chemistry, Inactivation, Metabolic, Models, Animal, Toxicity, Animals, Humans, Intestinal Mucosa, Xenobiotic, Digestion, Drug metabolism, Food Science, Biotechnology

Abstract

In addition to its role in digestion of food in the gastrointestinal tract, the intestinal microflora is also capable of biotransforming numerous drugs. Likewise, the intestinal microflora may significantly modulate xenobiotic-induced toxicity by either activating or inactivating xenobiotics via metabolism. To date, most investigations of xenobiotic metabolism have focused not only on metabolism in host tissues, but the modulation of the pharmacological activity of drugs by the intestinal microflora. Despite its importance, the presumed role of intestinal microflora metabolism in xenobiotic-induced toxicity has been understudied. Therefore, it is appropriate to briefly review our current situation, and state which research in xenobiotic metabolism by intestinal microflora, particularly in the field of toxicology, is needed.

Published

2012

5. Nephrotoxic potential and toxicokinetics of melamine combined with cyanuric acid in rats

Author

Keumhan Noh, Ghee Hwan Kim, Wonku Kang, Hyung Sik Kim, Do Gyeong Oh, Hangun Kim, Tae Cheon Jeong, Hye Gwang Jeong, Mi Jeong Kang, and Kwang Youl Lee

Subjects

Male, medicine.medical_specialty, Health, Toxicology and Mutagenesis, Administration, Oral, Toxicology, Kidney, Nephrotoxicity, Excretion, Rats, Sprague-Dawley, chemistry.chemical_compound, hemic and lymphatic diseases, Internal medicine, medicine, Toxicokinetics, Animals, neoplasms, Inflammation, Dose-Response Relationship, Drug, Triazines, Body Weight, Kidney metabolism, Rats, carbohydrates (lipids), Endocrinology, medicine.anatomical_structure, Biochemistry, chemistry, Toxicity, Melamine, Cyanuric acid

Abstract

To investigate the nephrotoxic potential of melamine (MEL) and cyanuric acid (CA) in male Sprague-Dawley rats, 7-d repeated-dose studies were performed. The experimental groups of MEL100 and CA100 were orally administered with MEL and CA at 100 mg/kg/d for 7 d, respectively. In groups dosed with MEL-CA mixtures, melamine and cyanuric acid (1:1) were simultaneously administered at 4, 20, or 100 mg/kg/d for 7 d (i.e., MEL-CA4, MEL-CA20, or MEL-CA100, respectively). Body weights were not markedly affected in MEL100, CA100, and MEL-CA4 groups, but significantly reduced in MEL-CA 20 and 100 rats. Most parameters determined in sera and tissues were not markedly altered in MEL100, CA100, and MEL-CA4-treated rodents. However, BUN, creatinine, total protein, and kidney weights were significantly increased in MEL-CA20- and MEL-CA100-treated animals. Renal histopathologic findings also revealed signs of toxicity, including tubular dilatation, crystal deposition, granulomatous tubulo-interstitial inflammation, and tubular necrosis with regeneration. Data suggested that the combination of MEL and CA might be responsible for observed nephrotoxicity that was not seen following individual exposure to either MEL or CA alone. Subsequently, the concentrations of MEL and CA were determined in serum, urine, and kidney tissues by using liquid chromatography-mass spectrometry. Toxicokinetic studies indicated that MEL or CA alone might be eliminated almost completely within 24 h after dosing showing no accumulation in kidney. However, the combined MEL-CA dose produced marked accumulation of chemicals in blood and kidneys. These results suggested that combined MEL and CA might produce renal toxicity due to significant chemical accumulation in kidney accompanied by low excretion.

Published

2014

6. Role of metabolism by intestinal microbiota in pharmacokinetics of oral baicalin

Author

Wonku Kang, Keumhan Noh, Won Ki Yoon, Jin Sung Kim, Mi Jeong Kang, Tae Cheon Jeong, Gyu Sub Ko, Hyoung Chin Kim, Do Gyeong Oh, and Hye Gwang Jeong

Subjects

Male, medicine.drug_class, Scutellaria, Antibiotics, Cmax, Erythromycin, Administration, Oral, Oxytetracycline, Pharmacology, Rats, Sprague-Dawley, chemistry.chemical_compound, Pharmacokinetics, Drug Discovery, medicine, Animals, Intestinal Mucosa, Flavonoids, biology, Microbiota, Organic Chemistry, biology.organism_classification, Rats, chemistry, Intestinal Absorption, Cefadroxil, Molecular Medicine, Scutellaria baicalensis, Baicalin, medicine.drug

Abstract

Baicalin (baicalein-7-glucuronide) is a flavonoid purified from Scutellaria baicalensis Georgi that has traditionally been used for treatment of hypertension, cardiovascular diseases, and viral hepatitis. In this study, the effects of intestinal microbiota on the pharmacokinetics of baicalin were investigated in normal and antibiotic-pretreated rats following p.o. administration of 100 mg/kg baicalin by using liquid chromatography/ion trap mass spectrometry. When rats were pretreated orally with cefadroxil, oxytetracycline and erythromycin for 3 days to control the number of intestinal bacteria, the pharmacokinetic parameters of oral baicalin were significantly affected by antibiotics: Cmax, T1/2(β), Kel and AUC values were significantly changed compared to those in normal rats. These results indicate that intestinal microbiota might play a key role in the oral pharmacokinetics of baicalin.

Published

2013

7. Role of Intestinal Microbiota in Baicalin-Induced Drug Interaction and Its Pharmacokinetics

Author

Ki Sun Jeong, Do Gyeong Oh, Sangkyu Lee, Mi Jeong Kang, Keumhan Noh, Hye Gwang Jeong, Mahesh Raj Nepal, Wonku Kang, Tae Cheon Jeong, and Youra Kang

Subjects

intestinal microbiota, baicalein, Pharmaceutical Science, Review, Pharmacology, 030226 pharmacology & pharmacy, Intestinal absorption, Analytical Chemistry, lcsh:QD241-441, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, lcsh:Organic chemistry, Intestinal mucosa, Drug Discovery, Animals, Humans, Drug Interactions, Scutellaria lateriflora, Intestinal Mucosa, Physical and Theoretical Chemistry, baicalin, Flavonoids, drug interaction, Molecular Structure, biology, Organic Chemistry, biology.organism_classification, Gastrointestinal Microbiome, Rats, Baicalein, Aglycone, Intestinal Absorption, chemistry, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, Flavanones, Scutellaria, Molecular Medicine, Scutellaria baicalensis, pharmacokinetics, Baicalin, Biomarkers

Abstract

Since many glycoside compounds in natural products are hydrolyzed by intestinal microbiota when administered orally, it is of interest to know whether their pharmacological effects are derived from the glycoside itself or from the aglycone form in vivo. An interesting example is baicalin versus baicalein, the aglycone of baicalin, which is contained in some herbs from Labiatae including Scutellaria baicalensis Georgi and Scutellaria lateriflora Linne. The herbs have been extensively used for treatment of inflammatory diseases in Asia. Although there have been numerous reports regarding the pharmacological effects of baicalin and baicalein in vivo and in vitro, some reports indicated that the glycoside form would hardly be absorbed in the intestine and that it should be hydrolyzed to baicalein in advance for absorption. Therefore, the role of metabolism by intestinal microbiota should also be considered in the metabolism of baicalin. In addition, baicalin contains a glucuronide moiety in its structure, by which baicalin and baicalein show complex pharmacokinetic behaviors, due to the interconversion between them by phase II enzymes in the body. Recently, concerns about drug interaction with baicalin and/or baicalein have been raised, because of the co-administration of Scutellaria species with certain drugs. Herein, we reviewed the role of intestinal microbiota in pharmacokinetic characteristics of baicalin and baicalein, with regards to their pharmacological and toxicological effects.

Published

2016