Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats

Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats

Background. This study was to explore the pharmacokinetics of saxagliptin (Sax) in Goto–Kakizaki (GK) rats complicated with depression induced by chronic unpredicted mild stress (CUMS). The comorbidity of diabetic patients with depression is becoming more and more epidemic. Whether depression mental...

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Main Authors: Zhengchao Xia, Hongyan Wei, Jingjing Duan, Ting Zhou, Zhen Yang, Feng Xu
Format: Article
Language:English
Published: PeerJ Inc. 2016-01-01
Series:PeerJ
Subjects:
Pharmacokinetics
Depression
Diabetes
CUMS
Saxagliptin
Rat
Online Access:https://peerj.com/articles/1611.pdf
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spelling doaj-562a3947f2fb492a8b84a50f2bba6cb52020-11-24T22:39:01ZengPeerJ Inc.PeerJ2167-83592016-01-014e161110.7717/peerj.1611Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK ratsZhengchao Xia0Hongyan Wei1Jingjing Duan2Ting Zhou3Zhen Yang4Feng Xu5Department of Pharmacy, Fengxian Central Hospital Graduate Training Base, Liaoning Medical University, Shanghai, ChinaDepartment of Pharmacy, Southern Medical University Affiliated Fengxian Central Hospital, Shanghai, ChinaDepartment of Pharmacy, Southern Medical University Affiliated Fengxian Central Hospital, Shanghai, ChinaDepartment of Pharmacy, Southern Medical University Affiliated Fengxian Central Hospital, Shanghai, ChinaDepartment of Pharmacy, Fengxian Central Hospital Graduate Training Base, Liaoning Medical University, Shanghai, ChinaDepartment of Pharmacy, Fengxian Central Hospital Graduate Training Base, Liaoning Medical University, Shanghai, ChinaBackground. This study was to explore the pharmacokinetics of saxagliptin (Sax) in Goto–Kakizaki (GK) rats complicated with depression induced by chronic unpredicted mild stress (CUMS). The comorbidity of diabetic patients with depression is becoming more and more epidemic. Whether depression mental disorder alters the pharmacokinetics of hypoglycemic drugs in diabetes patients is not clear.Methods. Five-week-old male GK rats were kept in the cage for 7 weeks in a specific pathogen free (SPF)-grade lab until the emergence of diabetes and were then divided into two groups: control group and depression model group. Rats in the CUMS-induced depression group were exposed to a series of stressors for 8 weeks. Plasma serotonin and dopamine levels and behavior of open-field test were used to confirm the establishment of the depression model. All rats were given 0.5 mg/kg Sax orally after 8 weeks and blood samples were collected at different time points. The Sax concentration was assayed by high performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS). The CYP450 activity of the liver microsomes was determined by using cocktails of probe drugs in which the activities of CYP enzymes were assessed through the determination of the production of the probe drugs.Results. Statistically significant differences in Sax pharmacokinetics were observed for area under curve, clearance, peak concentration, peak time and mean residence time between the depression rats and the control rats, while no statistical differences were observed for half-time and distribution volume by HPLC-MS/MS analysis. The CYP450 activity had different changes in the depression group.Conclusions. These results indicated that CUMS-induced depression alters the drug metabolic process of Sax and CYP450 activity of the liver microsomal enzymes in GK rats.https://peerj.com/articles/1611.pdfPharmacokineticsDepressionDiabetesCUMSSaxagliptinRat
collection DOAJ
language English
format Article
sources DOAJ
author Zhengchao Xia
Hongyan Wei
Jingjing Duan
Ting Zhou
Zhen Yang
Feng Xu
spellingShingle Zhengchao Xia
Hongyan Wei
Jingjing Duan
Ting Zhou
Zhen Yang
Feng Xu
Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats
PeerJ
Pharmacokinetics
Depression
Diabetes
CUMS
Saxagliptin
Rat
author_facet Zhengchao Xia
Hongyan Wei
Jingjing Duan
Ting Zhou
Zhen Yang
Feng Xu
author_sort Zhengchao Xia
title Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats
title_short Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats
title_full Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats
title_fullStr Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats
title_full_unstemmed Chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and CYP450 activity in GK rats
title_sort chronic unpredicted mild stress-induced depression alter saxagliptin pharmacokinetics and cyp450 activity in gk rats
publisher PeerJ Inc.
series PeerJ
issn 2167-8359
publishDate 2016-01-01
description Background. This study was to explore the pharmacokinetics of saxagliptin (Sax) in Goto–Kakizaki (GK) rats complicated with depression induced by chronic unpredicted mild stress (CUMS). The comorbidity of diabetic patients with depression is becoming more and more epidemic. Whether depression mental disorder alters the pharmacokinetics of hypoglycemic drugs in diabetes patients is not clear.Methods. Five-week-old male GK rats were kept in the cage for 7 weeks in a specific pathogen free (SPF)-grade lab until the emergence of diabetes and were then divided into two groups: control group and depression model group. Rats in the CUMS-induced depression group were exposed to a series of stressors for 8 weeks. Plasma serotonin and dopamine levels and behavior of open-field test were used to confirm the establishment of the depression model. All rats were given 0.5 mg/kg Sax orally after 8 weeks and blood samples were collected at different time points. The Sax concentration was assayed by high performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS). The CYP450 activity of the liver microsomes was determined by using cocktails of probe drugs in which the activities of CYP enzymes were assessed through the determination of the production of the probe drugs.Results. Statistically significant differences in Sax pharmacokinetics were observed for area under curve, clearance, peak concentration, peak time and mean residence time between the depression rats and the control rats, while no statistical differences were observed for half-time and distribution volume by HPLC-MS/MS analysis. The CYP450 activity had different changes in the depression group.Conclusions. These results indicated that CUMS-induced depression alters the drug metabolic process of Sax and CYP450 activity of the liver microsomal enzymes in GK rats.
topic Pharmacokinetics
Depression
Diabetes
CUMS
Saxagliptin
Rat
url https://peerj.com/articles/1611.pdf
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AT jingjingduan chronicunpredictedmildstressinduceddepressionaltersaxagliptinpharmacokineticsandcyp450activityingkrats
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AT zhenyang chronicunpredictedmildstressinduceddepressionaltersaxagliptinpharmacokineticsandcyp450activityingkrats
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