Tissue distribution of berberine and its metabolites after oral administration in rats.

Tissue distribution of berberine and its metabolites after oral administration in rats.

Berberine (BBR) has been confirmed to have multiple bioactivities in clinic, such as cholesterol-lowering, anti-diabetes, cardiovascular protection and anti- inflammation. However, BBR's plasma level is very low; it cannot explain its pharmacological effects in patients. We consider that the in...

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Main Authors: Xiang-Shan Tan, Jing-Yi Ma, Ru Feng, Chao Ma, Wen-Jing Chen, Yu-Peng Sun, Jie Fu, Min Huang, Chi-Yu He, Jia-Wen Shou, Wen-Yi He, Yan Wang, Jian-Dong Jiang
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3815028?pdf=render
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spelling doaj-00e78cfc51ab463cb867e9949a11771b2020-11-25T01:09:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01810e7796910.1371/journal.pone.0077969Tissue distribution of berberine and its metabolites after oral administration in rats.Xiang-Shan TanJing-Yi MaRu FengChao MaWen-Jing ChenYu-Peng SunJie FuMin HuangChi-Yu HeJia-Wen ShouWen-Yi HeYan WangJian-Dong JiangBerberine (BBR) has been confirmed to have multiple bioactivities in clinic, such as cholesterol-lowering, anti-diabetes, cardiovascular protection and anti- inflammation. However, BBR's plasma level is very low; it cannot explain its pharmacological effects in patients. We consider that the in vivo distribution of BBR as well as of its bioactive metabolites might provide part of the explanation for this question. In this study, liquid chromatography coupled to ion trap time-of-flight mass spectrometry (LC/MS(n)-IT-TOF) as well as liquid chromatography that coupled with tandem mass spectrometry (LC-MS/MS) was used for the study of tissue distribution and pharmacokinetics of BBR in rats after oral administration (200 mg/kg). The results indicated that BBR was quickly distributed in the liver, kidneys, muscle, lungs, brain, heart, pancreas and fat in a descending order of its amount. The pharmacokinetic profile indicated that BBR's level in most of studied tissues was higher (or much higher) than that in plasma 4 h after administration. BBR remained relatively stable in the tissues like liver, heart, brain, muscle, pancreas etc. Organ distribution of BBR's metabolites was also investigated paralleled with that of BBR. Thalifendine (M1), berberrubine (M2) and jatrorrhizine (M4), which the metabolites with moderate bioactivity, were easily detected in organs like the liver and kidney. For instance, M1, M2 and M4 were the major metabolites in the liver, among which the percentage of M2 was up to 65.1%; the level of AUC (0-t) (area under the concentration-time curve) for BBR or the metabolites in the liver was 10-fold or 30-fold higher than that in plasma, respectively. In summary, the organ concentration of BBR (as well as its bioactive metabolites) was higher than its concentration in the blood after oral administration. It might explain BBR's pharmacological effects on human diseases in clinic.http://europepmc.org/articles/PMC3815028?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Xiang-Shan Tan
Jing-Yi Ma
Ru Feng
Chao Ma
Wen-Jing Chen
Yu-Peng Sun
Jie Fu
Min Huang
Chi-Yu He
Jia-Wen Shou
Wen-Yi He
Yan Wang
Jian-Dong Jiang
spellingShingle Xiang-Shan Tan
Jing-Yi Ma
Ru Feng
Chao Ma
Wen-Jing Chen
Yu-Peng Sun
Jie Fu
Min Huang
Chi-Yu He
Jia-Wen Shou
Wen-Yi He
Yan Wang
Jian-Dong Jiang
Tissue distribution of berberine and its metabolites after oral administration in rats.
PLoS ONE
author_facet Xiang-Shan Tan
Jing-Yi Ma
Ru Feng
Chao Ma
Wen-Jing Chen
Yu-Peng Sun
Jie Fu
Min Huang
Chi-Yu He
Jia-Wen Shou
Wen-Yi He
Yan Wang
Jian-Dong Jiang
author_sort Xiang-Shan Tan
title Tissue distribution of berberine and its metabolites after oral administration in rats.
title_short Tissue distribution of berberine and its metabolites after oral administration in rats.
title_full Tissue distribution of berberine and its metabolites after oral administration in rats.
title_fullStr Tissue distribution of berberine and its metabolites after oral administration in rats.
title_full_unstemmed Tissue distribution of berberine and its metabolites after oral administration in rats.
title_sort tissue distribution of berberine and its metabolites after oral administration in rats.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Berberine (BBR) has been confirmed to have multiple bioactivities in clinic, such as cholesterol-lowering, anti-diabetes, cardiovascular protection and anti- inflammation. However, BBR's plasma level is very low; it cannot explain its pharmacological effects in patients. We consider that the in vivo distribution of BBR as well as of its bioactive metabolites might provide part of the explanation for this question. In this study, liquid chromatography coupled to ion trap time-of-flight mass spectrometry (LC/MS(n)-IT-TOF) as well as liquid chromatography that coupled with tandem mass spectrometry (LC-MS/MS) was used for the study of tissue distribution and pharmacokinetics of BBR in rats after oral administration (200 mg/kg). The results indicated that BBR was quickly distributed in the liver, kidneys, muscle, lungs, brain, heart, pancreas and fat in a descending order of its amount. The pharmacokinetic profile indicated that BBR's level in most of studied tissues was higher (or much higher) than that in plasma 4 h after administration. BBR remained relatively stable in the tissues like liver, heart, brain, muscle, pancreas etc. Organ distribution of BBR's metabolites was also investigated paralleled with that of BBR. Thalifendine (M1), berberrubine (M2) and jatrorrhizine (M4), which the metabolites with moderate bioactivity, were easily detected in organs like the liver and kidney. For instance, M1, M2 and M4 were the major metabolites in the liver, among which the percentage of M2 was up to 65.1%; the level of AUC (0-t) (area under the concentration-time curve) for BBR or the metabolites in the liver was 10-fold or 30-fold higher than that in plasma, respectively. In summary, the organ concentration of BBR (as well as its bioactive metabolites) was higher than its concentration in the blood after oral administration. It might explain BBR's pharmacological effects on human diseases in clinic.
url http://europepmc.org/articles/PMC3815028?pdf=render
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