In vitro and in vivo metabolism of verproside in rats

Verproside, a catalpol derivative iridoid glycoside isolated from Pseudolysimachion rotundum var. subintegrum, is a biologically active compound with anti-inflammatory, antinociceptic, antioxidant, and anti-asthmatic properties. Twenty-one metabolites were identified in bile and urine samples obtain...

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Published in	Molecules (Basel, Switzerland) Vol. 17; no. 10; pp. 11990 - 12002
Main Authors	Kim, Min Gi, Hwang, Deok-Kyu, Jeong, Hyeon-Uk, Ji, Hye Young, Oh, Sei-Ryang, Lee, Yongnam, Yoo, Ji Seok, Shin, Dae Hee, Lee, Hye Suk
Format	Journal Article
Language	English
Published	Switzerland MDPI AG 12.10.2012 MDPI
Subjects	Animals Asthma Bile Chromatography Cytokines Drug dosages Electronic mail systems Hepatocytes - metabolism Iridoid Glucosides - administration & dosage Iridoid Glucosides - chemistry Iridoid Glucosides - metabolism LC-HRMS Male Mass spectrometry Metabolic Networks and Pathways Metabolism Metabolites rat bile rat hepatocytes rat urine Rats Rats, Sprague-Dawley Scientific imaging Urine verproside metabolism
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Abstract	Verproside, a catalpol derivative iridoid glycoside isolated from Pseudolysimachion rotundum var. subintegrum, is a biologically active compound with anti-inflammatory, antinociceptic, antioxidant, and anti-asthmatic properties. Twenty-one metabolites were identified in bile and urine samples obtained after intravenous administration of verproside in rats using liquid chromatography-quadrupole Orbitrap mass spectrometry. Verproside was metabolized by O-methylation, glucuronidation, sulfation, and hydrolysis to verproside glucuronides (M1 and M2), verproside sulfates (M3 and M4), picroside II (M5), M5 glucuronide (M7), M5 sulfate (M9), isovanilloylcatalpol (M6), M6 glucuronide (M8), M6 sulfate (M10), 3,4-dihydroxybenzoic acid (M11), M11 glucuronide (M12), M11 sulfates (M13 and M14), 3-methyoxy-4-hydroxybenzoic acid (M15), M15 glucuronides (M17 and M18), M15 sulfate (M20), 3-hydroxy-4-methoxybenzoic acid (M16), M16 glucuronide (M19), and M16 sulfate (M21). Incubation of verproside with rat hepatocytes resulted in thirteen metabolites (M1-M11, M13, and M14). Verproside sulfate, M4 was a major metabolite in rat hepatocytes. After intravenous administration of verproside, the drug was recovered in bile (0.77% of dose) and urine (4.48% of dose), and O-methylation of verproside to picroside II (M5) and isovanilloylcatalpol (M6) followed by glucuronidation and sulfation was identified as major metabolic pathways compared to glucuronidation and sulfation of verproside in rats.
AbstractList	Verproside, a catalpol derivative iridoid glycoside isolated from Pseudolysimachion rotundum var. subintegrum, is a biologically active compound with anti-inflammatory, antinociceptic, antioxidant, and anti-asthmatic properties. Twenty-one metabolites were identified in bile and urine samples obtained after intravenous administration of verproside in rats using liquid chromatography-quadrupole Orbitrap mass spectrometry. Verproside was metabolized by O-methylation, glucuronidation, sulfation, and hydrolysis to verproside glucuronides (M1 and M2), verproside sulfates (M3 and M4), picroside II (M5), M5 glucuronide (M7), M5 sulfate (M9), isovanilloylcatalpol (M6), M6 glucuronide (M8), M6 sulfate (M10), 3,4-dihydroxybenzoic acid (M11), M11 glucuronide (M12), M11 sulfates (M13 and M14), 3-methyoxy-4-hydroxybenzoic acid (M15), M15 glucuronides (M17 and M18), M15 sulfate (M20), 3-hydroxy-4-methoxybenzoic acid (M16), M16 glucuronide (M19), and M16 sulfate (M21). Incubation of verproside with rat hepatocytes resulted in thirteen metabolites (M1-M11, M13, and M14). Verproside sulfate, M4 was a major metabolite in rat hepatocytes. After intravenous administration of verproside, the drug was recovered in bile (0.77% of dose) and urine (4.48% of dose), and O-methylation of verproside to picroside II (M5) and isovanilloylcatalpol (M6) followed by glucuronidation and sulfation was identified as major metabolic pathways compared to glucuronidation and sulfation of verproside in rats. Verproside, a catalpol derivative iridoid glycoside isolated from Pseudolysimachion rotundum var. subintegrum, is a biologically active compound with anti-inflammatory, antinociceptic, antioxidant, and anti-asthmatic properties. Twenty-one metabolites were identified in bile and urine samples obtained after intravenous administration of verproside in rats using liquid chromatography-quadrupole Orbitrap mass spectrometry. Verproside was metabolized by O-methylation, glucuronidation, sulfation, and hydrolysis to verproside glucuronides (M1 and M2), verproside sulfates (M3 and M4), picroside II (M5), M5 glucuronide (M7), M5 sulfate (M9), isovanilloylcatalpol (M6), M6 glucuronide (M8), M6 sulfate (M10), 3,4-dihydroxybenzoic acid (M11), M11 glucuronide (M12), M11 sulfates (M13 and M14), 3-methyoxy-4-hydroxybenzoic acid (M15), M15 glucuronides (M17 and M18), M15 sulfate (M20), 3-hydroxy-4-methoxybenzoic acid (M16), M16 glucuronide (M19), and M16 sulfate (M21). Incubation of verproside with rat hepatocytes resulted in thirteen metabolites (M1–M11, M13, and M14). Verproside sulfate, M4 was a major metabolite in rat hepatocytes. After intravenous administration of verproside, the drug was recovered in bile (0.77% of dose) and urine (4.48% of dose), and O-methylation of verproside to picroside II (M5) and isovanilloylcatalpol (M6) followed by glucuronidation and sulfation was identified as major metabolic pathways compared to glucuronidation and sulfation of verproside in rats. Verproside, a catalpol derivative iridoid glycoside isolated from Pseudolysimachion rotundum var . subintegrum , is a biologically active compound with anti-inflammatory, antinociceptic, antioxidant, and anti-asthmatic properties. Twenty-one metabolites were identified in bile and urine samples obtained after intravenous administration of verproside in rats using liquid chromatography-quadrupole Orbitrap mass spectrometry. Verproside was metabolized by O -methylation, glucuronidation, sulfation, and hydrolysis to verproside glucuronides (M1 and M2), verproside sulfates (M3 and M4), picroside II (M5), M5 glucuronide (M7), M5 sulfate (M9), isovanilloylcatalpol (M6), M6 glucuronide (M8), M6 sulfate (M10), 3,4-dihydroxybenzoic acid (M11), M11 glucuronide (M12), M11 sulfates (M13 and M14), 3-methyoxy-4-hydroxybenzoic acid (M15), M15 glucuronides (M17 and M18), M15 sulfate (M20), 3-hydroxy-4-methoxybenzoic acid (M16), M16 glucuronide (M19), and M16 sulfate (M21). Incubation of verproside with rat hepatocytes resulted in thirteen metabolites (M1–M11, M13, and M14). Verproside sulfate, M4 was a major metabolite in rat hepatocytes. After intravenous administration of verproside, the drug was recovered in bile (0.77% of dose) and urine (4.48% of dose), and O -methylation of verproside to picroside II (M5) and isovanilloylcatalpol (M6) followed by glucuronidation and sulfation was identified as major metabolic pathways compared to glucuronidation and sulfation of verproside in rats.
Author	Oh, Sei-Ryang Yoo, Ji Seok Jeong, Hyeon-Uk Hwang, Deok-Kyu Shin, Dae Hee Lee, Yongnam Ji, Hye Young Lee, Hye Suk Kim, Min Gi
AuthorAffiliation	1 Drug Metabolism & Bioanalysis Laboratory, College of Pharmacy, The Catholic University of Korea, Bucheon 420-743, Korea; Email: minki8637@naver.com (M.G.M.); myhdg@naver.com (D.-K.H.); wjd1375@hanmail.net (H.-U.J.); hychi@catholic.ac.kr (H.Y.J.) 3 Central R&D Institute, Yungjin Pharm. Co., Ltd., Suwon 443-270, Korea; Email: nami0209@yungjin.co.kr (Y.L.); jsyoo@yungjin.co.kr (J.S.Y.); jkyk58@yungjin.co.kr (D.H.S.) 2 Natural Medicine Research Center, Korea Research Institute of Bioscience and Biotechnology, Ochang-eup, Cheongwon-gun, Chungbuk 363-883, Korea; Email: seiryang@kribb.re.kr
AuthorAffiliation_xml	– name: 1 Drug Metabolism & Bioanalysis Laboratory, College of Pharmacy, The Catholic University of Korea, Bucheon 420-743, Korea; Email: minki8637@naver.com (M.G.M.); myhdg@naver.com (D.-K.H.); wjd1375@hanmail.net (H.-U.J.); hychi@catholic.ac.kr (H.Y.J.) – name: 2 Natural Medicine Research Center, Korea Research Institute of Bioscience and Biotechnology, Ochang-eup, Cheongwon-gun, Chungbuk 363-883, Korea; Email: seiryang@kribb.re.kr – name: 3 Central R&D Institute, Yungjin Pharm. Co., Ltd., Suwon 443-270, Korea; Email: nami0209@yungjin.co.kr (Y.L.); jsyoo@yungjin.co.kr (J.S.Y.); jkyk58@yungjin.co.kr (D.H.S.)
Author_xml	– sequence: 1 givenname: Min Gi surname: Kim fullname: Kim, Min Gi organization: Drug Metabolism & Bioanalysis Laboratory, College of Pharmacy, The Catholic University of Korea, Bucheon 420-743, Korea – sequence: 2 givenname: Deok-Kyu surname: Hwang fullname: Hwang, Deok-Kyu – sequence: 3 givenname: Hyeon-Uk surname: Jeong fullname: Jeong, Hyeon-Uk – sequence: 4 givenname: Hye Young surname: Ji fullname: Ji, Hye Young – sequence: 5 givenname: Sei-Ryang surname: Oh fullname: Oh, Sei-Ryang – sequence: 6 givenname: Yongnam surname: Lee fullname: Lee, Yongnam – sequence: 7 givenname: Ji Seok surname: Yoo fullname: Yoo, Ji Seok – sequence: 8 givenname: Dae Hee surname: Shin fullname: Shin, Dae Hee – sequence: 9 givenname: Hye Suk surname: Lee fullname: Lee, Hye Suk
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SubjectTerms	Animals Asthma Bile Chromatography Cytokines Drug dosages Electronic mail systems Hepatocytes - metabolism Iridoid Glucosides - administration & dosage Iridoid Glucosides - chemistry Iridoid Glucosides - metabolism LC-HRMS Male Mass spectrometry Metabolic Networks and Pathways Metabolism Metabolites rat bile rat hepatocytes rat urine Rats Rats, Sprague-Dawley Scientific imaging Urine verproside metabolism
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Title	In vitro and in vivo metabolism of verproside in rats
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