Your search keyword '"drug interaction"' showing total 20 results

1. Effect of propranolol on pharmacokinetics of clozapine in schizophrenic patients: a meta-analysis.

Author

Yang, Xiding, Yan, Qiangyong, Yang, Lingfeng, Li, Jingjing, Fan, Xiao, Chen, Jindong, Wu, Haishan, Yang, Yongyu, Zhu, Ronghua, and Fang, Pingfei

Subjects

*PROPRANOLOL, *RESEARCH funding, *TREATMENT effectiveness, *META-analysis, *DECISION making in clinical medicine, *DRUG interactions, *PHYSICIAN practice patterns, *TACHYCARDIA, *HEALTH facilities, *DATA analysis software, *CONFIDENCE intervals, *BIOAVAILABILITY, *DRUG prescribing, *CLOZAPINE, *PHARMACODYNAMICS, *EVALUATION, DRUG therapy for schizophrenia

Abstract

Purpose: Clozapine is the effective therapy for treatment-refractory schizophrenia. However, the use of clozapine is limited by its adverse effects. As propranolol is frequently used for the prevention and treatment of clozapine-induced tachycardia, we performed a meta-analysis to evaluate the effects of propranolol on steady state pharmacokinetics of clozapine in schizophrenic patients. Methods: We included 16 retrospective studies on the effects of propranolol on steady state pharmacokinetics of clozapine in schizophrenic patients, with data from both generic and brand name treatment phases in eight clozapine bioequivalence studies conducted in a single center in China from 2018 to 2022. Review Manager 5.4 was used for meta-analysis of the included studies. Results: The SMDs with 95% CIs of AUC0–12, Cmax,ss, C, and C were calculated to be 0.44 (0.23, 0.64), 0.40 (0.20, 0.61), 0.43 (0.22, 0.63), and 0.44 (0.23, 0.64), respectively. These findings proved that combination with propranolol would increase the systemic exposure of clozapine. T1/2 of clozapine was significantly longer in the presence of propranolol than in the absence of propranolol (SMD = 0.32, 95% CI [0.12, 0.52], p = 0.002). There was no statistically significant difference for T of clozapine in the presence or absence of propranolol (SMD = − 0.05, 95% CI [− 0.25, 0.15], p = 0.63). Conclusion: The combination with propranolol could significantly increase systemic exposure and extended T1/2 of clozapine, and thus need to be considered in prescribing decisions. [ABSTRACT FROM AUTHOR]

Published

2024

2. A brief history of clozapine in China with a look forward.

Author

Ruan, Can-Jun, Wang, Chuan-Yue, Zang, Yan-Nan, Liu, Chen-Geng, Dong, Fang, Li, An-Ning, Wan, Zhou, Guo, Wei, and Wang, Gang

Subjects

*COMBINATION drug therapy, *ASPIRATION pneumonia, *CLOZAPINE, *MENTAL illness, CHINESE history

Abstract

Clozapine was first manufactured in China in 1976. Clozapine is currently used not only for treatment-refractory schizophrenia (TRS), but also continues to be used in the treatment of patients with non-TRS and other mental disorders; moreover, low-dose clozapine is also used in sedative-hypnotic therapy and in combination with other drugs. There is need for studies in China using various titrations and assessing their risk for myocarditis and aspiration pneumonia. The Chinese clozapine package insert will also greatly benefit from these changes. [ABSTRACT FROM AUTHOR]

Published

2024

3. Dabigatran-related serious medication errors: an analysis using data from VigiBase.

Author

Zhang, Qingxia, Ding, Qian, and Yue, Qun-Ying

Subjects

*ANTICOAGULANTS, *DRUG overdose, *PHARMACOLOGY, *PATIENT compliance, *MEDICATION errors, *ISCHEMIA, *RESEARCH funding, *HOSPITAL care, *DRUG administration, *CATASTROPHIC illness, *TREATMENT effectiveness, *DRUG interactions, *DISEASE complications, *ADVERSE health care events, *HEMORRHAGE

Abstract

Objective: To analyze the serious medication errors (MEs) on dabigatran, and their related factors, in order to avoid or reduce the occurrence of adverse events. Methods: Serious MEs related to dabigatran were extracted from the WHO global database of reported potential side effects of medicinal products (VigiBase) by using "Medication errors and other product use errors and issues" High Level Group Term (HLGT) of the international Medical Dictionary for Regulatory Activities (MedDRA). Well-documented reports, vigiGrade completeness score ≥ 0.80, or with an informative narrative were analyzed with a focus on the clinical features of the cases. The PCNE Classification for drug-related problems (DRP) was used to classify medication errors in our analysis of cases. Results: Until January 26, 2020, there were 453 cases with serious MEs related to dabigatran in VigiBase, and 113 were well-documented. Among these, 69 patients (61%) were hospitalized or had prolonged hospitalization, 16 (14%) had life-threatening events, and 12 (11%) died. The MEs occurred in the prescription phase in 77 cases, in administration in 35, and at the dispensing stage in one case. The MEs in prescription were related to a drug selection error in 44 cases (24 concerning contraindications and 20 drug interactions) and to dose error in 33 cases (17 with excessive dose; eight with insufficient frequency; four had an incorrect time; in three, the dose was too low; and in one, too frequent). The MEs in administration were medical-staff-related errors in five cases (three with wrong administration route, one administration omission, and one overdose), patient-related errors in 28 (14 insufficient dose or no administration, seven improper drug storage, four wrong administration method, and three over prescribed dose), and other errors in two (without efficacy monitoring). The dispensing error of a wrong drug strength occurred in a pharmacy. The main adverse events in the 113 patients were haemorrhage in 57 cases (50%) and ischemia in 29 cases (26%). Conclusion: Based on the analysis of reports in VigiBase, serious MEs related to dabigatran mainly occurred during prescription and administration. Although the incidence of MEs with clinical consequences in the use of dabigatran cannot be determined, attention should be paid to selection of the appropriate dose to a right patient in the prescription, and to patient compliance and storage in drug administration. The patient harm mainly manifested itself as bleeding or ischemia including fatal outcome in rare patients. [ABSTRACT FROM AUTHOR]

Published

2024

4. Effect of posaconazole on the concentration of intravenous and oral cyclosporine in patients undergoing hematopoietic stem cell transplantation.

Author

Zhu, Li-E, Huang, Hui-Ping, Cai, Yi-Peng, Wang, Yan, Xu, Bao-Hua, Liu, Mao-Bai, and Wu, Xue-Mei

Subjects

*ANTIFUNGAL agents, *INTRAVENOUS therapy, *ACADEMIC medical centers, *ORAL drug administration, *SURGERY, *PATIENTS, *RETROSPECTIVE studies, *CYCLOSPORINE, *PRE-tests & post-tests, *COMPARATIVE studies, *DRUG interactions, *DESCRIPTIVE statistics, *HEMATOPOIETIC stem cell transplantation, *LONGITUDINAL method, *PHARMACODYNAMICS

Abstract

Purpose: This study aimed to investigate the interactions between posaconazole (POS) and intravenously/orally administered cyclosporine A (CsA) in allogeneic hematopoietic stem cell transplant (HSCT) recipients. Methods: We included 118 allogeneic HSCT patients who received CsA and POS simultaneously between January 2017 and June 2020 in this study. The ratio of CsA blood concentration (ng/mL) to dosage (mg/day) (C/D) before and after POS initiation was compared. Results: After the initiation of POS, the level of CsA increased 1 to 2 times in 66% (78/118) of patients compared to those without POS. However, the CsA C/D ratio increased by more than threefold in 6% (7/118) of patients after POS initiation, with an increase of more than fourfold in two patients. The median C/D ratio of CsA increased from 0.89 to 1.23 (P < 0.001) and 0.78 to 1.22 (P < 0.001) after POS initiation when CsA was administered intravenously and orally, respectively. In patients who received POS at the time of transition from intravenous to oral CsA, the value increased from 1.01 to 1.38 (P = 0.001). The route of administration had no significant effect on the change in the CsA C/D ratio (P = 0.615). Additionally, we observed the time required for the C/D ratio to reach a plateau after POS initiation was similar on days 13, 8, and 15 under various scenarios. Conclusion: POS treatment increased blood CsA levels. A large variability was found in the fold-change in the CsA C/D ratio. Therefore, CsA doses should be adjusted by closely monitoring the blood levels of CsA after POS initiation. [ABSTRACT FROM AUTHOR]

Published

2022

5. Evaluation of the effect of Bovis Calculus Artifactus on eight rat liver cytochrome P450 isozymes using LC-MS/MS and cocktail approach.

Author

Zhang, Yun-Jing, Zhou, Wen-Li, Yu, Fei, Wang, Qian, Peng, Can, and Kan, Jia-Yi

Subjects

*CYTOCHROME P-450, *LIQUID chromatography-mass spectrometry, *ISOENZYMES, *DRUG interactions, *DRUG utilization

Abstract

Bovis Calculus Artifactus (BCA) is the main substitute for natural Calculus bovis, a traditional drug in China used to treat high fever, convulsion, and sore throat. The effect of BCA on cytochrome P450 (CYP) activities is unknown. This study was to investigate the effect of BCA on eight rat hepatic microsomal CYPisozymes to evaluate the potential drug interactions using the cocktail approach. Metabolites of the eight isoform probe substrates of CYP isozymes were quantified by LC-MS/MS. The method was validated by incubating known CYP inhibitors α-naphthoflavone (CYP1A2), thiotepa (CYP2B1), quercetin (CYP2C7), sulfaphenazole (CYP2C6), ticlopidine (CYP2C11), quinidine (CYP2D1), ketoconazole (CYP3A1),4-methylpyrazole (CYP2E1) with individual probe substrate and rat liver microsomes. The formation rates of the corresponding metabolites of the eight probe substrates were determined to evaluate the activity of each isozyme. The results showed that BCA has different degrees of inhibitory effect on four CYP450 isoforms (CYP2C6, CYP2C11, CYP2D1, CYP3A1) (p < 0.05), but no significant influence on CYP1A2, 2B1, 2C7 or 2E1 (p > 0.05). Attention should be paid to the BCA-drug interactions by careful monitoring and appropriate dosage adjustments in the concurrent use of the drugs which are metabolized by CYP1A2, CYP2C19, and CYP3A4. Abbreviations: BCA, bovis calculus artifactus; CYP, cytochrome P450; DDIs, drug-drug interactions; ESI, electrospray ionization; MRM, multiple reaction monitoring; NBC, Natural Bovis Calculus; QC, quality control; T CM, traditional Chinese medicine. [ABSTRACT FROM AUTHOR]

Published

2021

6. Characteristic and Mechanism of Drug-Herb Interaction Between Acetylsalicylic Acid and Danhong Injection Mediated by Organic Anion Transporters.

Author

Li, Jianping, Lu, Jingbo, Peng, Yin, Xu, Xuejun, Chen, Chenkai, Gao, Ming, Lin, Ling, Guo, Jianming, and Duan, Jinao

Subjects

ORGANIC anion transporters, DRUG-herb interactions, ASPIRIN, ARISTOLOCHIC acid, SALICYLIC acid, KIDNEY glomerulus

Abstract

The mixture of Salvia miltiorrhiza and Carthamus tinctorius (Danhong injection, DHI) is widely prescribed in China for the treatment of cardiovascular and cerebrovascular diseases. In most cases, DHI is used in combination with acetylsalicylic acid (aspirin, ASA). However, the interaction between DHI and ASA remains largely undefined. The purpose of this study is to explore the interaction profile and mechanism between DHI and ASA. The frequency of drug combination of DHI and ASA was analyzed based on 5,183 clinical cases. The interaction characteristics were evaluated by analyzing the pharmacokinetics and disposition profile of salicylic acid (SA, the primary metabolite of ASA) in rats. The interaction mechanisms were explored through evaluating the hydrolysis of ASA regulated by ASA esterase, the tubular secretion of SA mediated by influx and efflux transporters, and the tubular reabsorption of SA regulated by urinary acidity-alkalinity. The inhibitory potential of DHI on organic anion transporters (OATs) was further verified in aristolochic acid I (AAI) induced nephropathy. Clinical cases analysis showed that DHI and ASA were used in combination with high frequency of 70.73%. In drug combination of DHI and ASA, the maximum plasma concentration of SA was significantly increased by 1.37 times, while the renal excretion of SA was significantly decreased by 32.54%. The mechanism study showed that DHI significantly inhibited the transport function, gene transcription and protein expression of OATs. In OATs mediated AAI nephropathy, DHI significantly reduced the renal accumulation of AAI by 55.27%, and alleviated renal damage such as glomerulus swelling, tubular blockage and lymphocyte filtration. In drug combination of DHI and ASA, DHI increased the plasma concentration of SA not through enhancing the hydrolysis of ASA, and the tubular reabsorption of SA was not significantly affected. Inhibition of tubular secretion of SA mediated by OATs might be the reason that contributes to the decrease of SA renal excretion. [ABSTRACT FROM AUTHOR]

Published

2020

7. Determination of vericiguat in rat plasma by UPLC-MS/MS and its application to drug interaction.

Author

Ding, Congyang, Guo, Caihui, Fang, Lingzhi, Li, Yajing, Wang, Zhi, and Dong, Zhanjun

Subjects

*DRUG interactions, *P-glycoprotein, *LIQUID chromatography-mass spectrometry, *CHINESE medicine, *GUANYLATE cyclase, *GRADIENT elution (Chromatography), *LIQUID-liquid extraction

Abstract

• Develop and validate a UPLC-MS/MS method for the identification of vericiguat • Astragaloside IV significantly reduces C max of vericiguat • Drug-drug interaction might happen between vericiguat and astragaloside IV • Astragaloside IV might decrease vericiguat exposure via P-glycoprotein Vericiguat (VER) is a novel soluble guanylate cyclase stimulator treating symptomatic chronic heart failure (HF), and it is a substrate of both transporters P-glycoprotein and breast cancer resistance protein (BCRP). Astragaloside IV (ASIV) is the main active ingredient in Radix Astragali (Huangqi), a traditional Chinese medicine widely used for HF treatment in China. ASIV's effect on the protein expression of P-glycoprotein and BCRP has been observed, its impact on VER metabolism remain uncertain. In the present study, male Sprague-Dawley rats were administered with 20 mg/kg ASIV and 1 mg/kg VER to study their pharmacokinetics. Blood samples were subject to liquid-liquid extraction, and riociguat was employed as the internal standard (IS). The analytical method involved a C18 column (XSelect® HSS T3 column, 2.1 × 100 mm, 2.5 μm) with a mobile phase of 0.1% formic acid and acetonitrile for gradient elution. The flow rate of the mobile phase was set at 0.2 mL/min, and 5 µL of the sample was used for analysis. The positive ion multi-response monitoring mode was utilized with a transition of m/z 427.4→109.1 for VER and m/z 423.3→109.1 for the IS. The method exhibited good linearity within the concentration range of 0.1 to 300 ng/mL (r = 0.9987), and all the validation processes were conducted in accordance with the requirements of biological analysis. The pharmacokinetic results revealed that ASIV did not significantly alter the main parameters of VER, except for C max , which decreased by 33.2% (P < 0.05). Overall, our study successfully established a selective, sensitive and repeatable ultra-high performance liquid chromatography-tandem mass spectrometry (UPLC-MS/MS) analysis for detecting VER in rat plasma. [ABSTRACT FROM AUTHOR]

Published

2023

8. Two cases of high serum clozapine concentrations occurring during inflammation in Chinese patients.

Author

Ruan, Can-Jun, Zhang, Xiao-Ling, Guo, Wei, Li, Wen-Biao, Zhuang, Hong-Yan, Li, Ya-Qiong, Wang, Chuan-Yue, Tang, Yi-Lang, Zhou, Fu-Chun, and de Leon, Jose

Subjects

CLOZAPINE, DRUG interactions, DOSE-effect relationship in pharmacology, INFECTION, INFLAMMATION, INFLUENZA, SKIN inflammation, SAMPLE size (Statistics)

Abstract

Objective Serious infections or inflammations have been associated with serum clozapine concentration increases and sometimes with clozapine toxicity. Method These two cases describe Chinese patients (Case 1: a 57-year-old female nonsmoker with severe dermatitis and Case 2: a 47-year-old male nonsmoker with influenza and secondary infection). Results In both cases, the Drug Interaction Probability Scale established the presence of a probable drug–drug interaction. In both cases, the clozapine and the total clozapine concentration-to-dose ratios followed a temporal pattern (normal–high–normal), consistent with an inhibition of clozapine metabolism during peak inflammation. In the first case, the total clozapine concentration-to-dose ratio (8 with no/low inflammation: median of 3.10 and 2 at peak inflammation: median of 3.90) provided a significant difference (P = 0.044). In the second patient, because of the smaller sample size and reduced statistical power (4 with no infection: a median of 1.59 and 2 at peak infection: 3.46), the increase did not reach significance (P = 0.13). In the first case, the median baseline clozapine concentration-to-dose ratio increased by a factor of 1.45 from 2.00 to a peak of 2.89. To compensate for the inhibition of clozapine metabolism, the dose correction factor was 0.69 (1/1.45) or a decrease in dose of approximately one-third. In the second case, the median baseline clozapine concentration-to-dose ratio increased by a factor of 2.56 from 1.15 to a peak of 2.94. Conclusion This provided a dose correction factor of 0.40 (1/2.56) or approximately half the dose, similar to published cases in Caucasians with serious respiratory infections. [ABSTRACT FROM AUTHOR]

Published

2018

9. Syndrome of inappropriate antidiuretic hormone secretion from concomitant use of itraconazole and vindesine.

Author

Zhou, H., Li, L., Zhou, Y., and Han, Y.

Subjects

*ANTINEOPLASTIC agents, *DRUG interactions, *DRUG side effects, *LYMPHOBLASTIC leukemia, *NEUROTOXICOLOGY, *SYNDROMES, *TRISMUS, *INDOLE compounds, *INAPPROPRIATE ADH syndrome, *ITRACONAZOLE

Abstract

What is known and objective Several studies have reported that itraconazole-induced inhibition of vincristine ( VCR) metabolism might result in neurological impairment and syndrome of inappropriate antidiuretic hormone ( SIADH). However, there are few reports concerning adverse drug reactions ( ADRs) resulting from concomitant use of vindesine ( VDS) and itraconazole. Here, we report the first case of adverse drug interactions ( ADIs) between itraconazole and VDS in a Chinese child with acute lymphocytic leukaemia ( ALL). Case summary A 4-year-old boy was diagnosed with standard-risk ALL and was receiving VDS (3 mg/m2) for maintenance therapy and itraconazole for IFI recurrence. Severe neurotoxicity, consisting mainly of trismus and SIADH, was noticed after 7 days of VDS administration. After discontinuation of itraconazole and its replacement with caspofungin, the patient recovered from neurological signs and symptoms. The ADIs can be explained by VDS accumulation owing to inherent loss of CYP3A5 (*3/*3) function, and inhibition of CYP3A4 activity by itraconazole. What is new and conclusion Syndrome of inappropriate antidiuretic hormone from co-administration of itraconazole and VDS has not previously been reported to our knowledge. We suggest that the concomitant use of these drugs should be avoided if possible. The use of alternative antifungal drugs ( AFDs) should be considered, and ADRs should be closely monitored when the combination of itraconazole and VDS is unavoidable. [ABSTRACT FROM AUTHOR]

Published

2018

10. Drug-drug interaction between valproic acid and meropenem: a retrospective analysis of electronic medical records from neurosurgery inpatients.

Author

Wen, Z.‐P., Fan, S.‐S., Du, C., Yin, T., Zhou, B.‐T., Peng, Z.‐F., Xie, Y.‐Y., Zhang, W., Chen, Y., Xiao, J., and Chen, X.‐P.

Subjects

*SPASMS, *SEIZURES (Medicine), *DRUG interactions, *DRUG monitoring, *NEUROSURGERY, *PATIENTS, *PROBABILITY theory, *RESEARCH funding, *SERUM albumin, *SURGERY, *T-test (Statistics), *VALPROIC acid, *RETROSPECTIVE studies, *DATA analysis software, *DESCRIPTIVE statistics, *ONE-way analysis of variance, *MEROPENEM, *PREVENTION

Abstract

What is known and objective A series of studies have indicated that valproic acid ( VPA) plasma concentration decreased rapidly when used concomitantly with carbapenem antibiotics, including meropenem ( MEPM), imipenem and panipenem, which may increase the risk of seizure breakthrough. However, the cause for the change in VPA pharmacokinetics is unclear. A retrospective analysis of VPA therapeutic drug monitoring ( TDM) records was performed to investigate this VPA pharmacokinetics drug-drug interaction. Methods Three hundred and eighty one VPA TDM records from the Department of Neurosurgery of Xiangya Hospital from January 2012 to December 2014 were collected. The VPA TDM records were categorized by VPA and MEPM daily dosages in grams/day (g/day). A comparison of VPA plasma levels among different groups was performed to investigate the change in VPA level in this drug interaction. Results and discussion Remarkable decreases in VPA plasma level were observed when the drug was used concomitantly with MEPM in both 1.2 g/d and 1.6 g/d VPA groups (67·3 ± 4·6 μg/mL, n = 21 vs. 15·3 ± 1·9 μg/mL, n = 15, P < 0·001; 67·6 ± 1·2 μg/mL vs. 18·1 ± 2·6 μg/mL, n = 38, P < 0·001). No significant difference in VPA plasma concentrations was observed between the 1·2 g/day VPA + MEPM, 1·6 g/day VPA + MEPM and 2·0 g/day VPA + MEPM groups (15·3 ± 1·9 μg/mL, n = 15 vs. 18·1 ± 2·6 μg/mL, n = 38 vs. 9·0 ± 3·0 μg/mL, n = 7; P = 0·252). The decrease in VPA concentration was independent of MEPM daily dose (14·0 ± 5·1 μg/mL, n = 4 for high MEPM daily dose vs. 16·5 ± 1·9 μg/mL, n = 56 for low MEPM daily dose; P = 0·729). After discontinuation of MEPM for more than 7 days, VPA plasma concentration recovered to a value comparable to that before MPEM initiation (69·7 ± 4·2 μg/mL, n = 21 vs. 51·2 ± 8·1 μg/mL, n = 9; P = 0·48). What is new and conclusion This is the first study using a large number of VPA TDM records to investigate the change in VPA levels caused by concomitant use of MEPM. Our results imply that the decrease in drug concentration cannot be reversed by increasing VPA dose. Moreover, MEPM daily dose did not influence the drop in VPA plasma level. At least 7 days are required for the recovery of VPA plasma concentration after discontinuation of MEPM. [ABSTRACT FROM AUTHOR]

Published

2017

11. Lotus leaf alkaloid fraction can strongly inhibit CYP2D6 isoenzyme activity.

Author

Ye, Lin-Hu, Kong, Ling-Ti, Yan, Ming-Zhu, Cao, Fang-Rui, Wang, Li-Sha, Liao, Yong-Hong, Pan, Rui-Le, and Chang, Qi

Subjects

*MEDICINAL plants, *ALKALOIDS, *ALTERNATIVE medicine, *ANIMAL experimentation, *BIOLOGICAL models, *ENZYME inhibitors, *ISOENZYMES, *LEAVES, *LIQUID chromatography, *MASS spectrometry, *DRUG-herb interactions, *METOPROLOL, *PROBABILITY theory, *RATS, *PLANT extracts, *STATISTICAL significance, *DEXTROMETHORPHAN, *DESCRIPTIVE statistics, *IN vitro studies, *IN vivo studies, *CHEMICAL inhibitors, *PHARMACODYNAMICS

Abstract

Ethnopharmacological relevance The Chinese herbal medicine He-Ye, the leaves of the lotus ( Nelumbo nucifera ) plant, is traditionally used in China for the treatment of sunstroke, thirst, diarrhea, and fever. Currently, the leaf is used not only as an herbal tea to reduce lipid level and control body weight, but also as a major ingredient in some lipid-lowering Chinese patented medicines. Our previous study demonstrated that the alkaloid fraction (AF) of the herb has a strong inhibitory effect on CYP2D6 isoenzyme activity in vitro . The present study aims to further verify this activity using the in vivo rat model and to explore the inhibitory mechanism on CYP2D6 using human liver microsomes (HLMs). Materials and methods After a continuous 7-d oral dose of AF (50 mg/kg) or a vehicle, Sprague Dawley rats received a single intravenous dose of dextromethorphan or metoprolol. Blood samples were collected at various time points, and the plasma concentrations of the relevant metabolites dextrorphan and hydroxymetoprolol were assayed by LC-MS/MS for evaluating the effect of AF on their pharmacokinetics and CYP2D6 activity. Dextromethorphan as a probe at different concentrations was incubated with HLMs in an incubation buffer system, in the presence or absence of AF at different concentrations. After incubation, the produced metabolite was assayed. Results After being pretreated with AF in rats, the plasma concentrations of dextrorphan and hydroxymetoprolol significantly decreased, with C max going from 79.44 to 29.96 and 151.18 to 83.39 h ng/mL (P<0.05), AUC all from 167.27 to 62.25 and 347.68 to 223.24 h ng/mL (P<0.05), and AUC inf from 183.39 to 84.76 and 350.59 to 234.57 h ng/mL (P<0.05), respectively, in comparison with those of untreated rats. The t 1/2 of hydroxymetoprolol significantly increased from 1.14 to 1.99 h (P<0.05). The in vitro incubation test showed that AF competitively inhibited the CYP2D6, with apparent K i value of 0.64 µg/mL. Conclusions AF can strongly inhibit the activity of CYP2D6 enzyme, as confirmed by in vivo and in vitro models. Possible drug interactions may occur between AF and other medications metabolized by CYP2D6. Thus, caution should be paid when the lotus leaf and its preparations are concurrently administered with conventional medicines. [ABSTRACT FROM AUTHOR]

Published

2016

12. TOXICIDADE DO GOJI BERRY (Lycium barbarum).

Author

GIBIN MARTINS, GISLAINE SUSSAI, BATISTA EVANGELISTA COIMBRA, CLAUDIA CRISTINA, and RUIZ SCHLICHTING, CARMEN LÚCIA

Subjects

*SOLANACEAE, *DRUG side effects, *DRUG interactions, *PHYTOTHERAPY, *MEDICINAL plants, *WARFARIN

Abstract

The Lycium barbarum (Goji Berry) is a plant of the solanaceous family found in China and the Himalayan regions, for a thousand years positioned on top of the 8,000 Chinese herbs and dressing table food, being considered a herbal medicine widely used for its potential antioxidant effect and revitalizing . Because of its regenerative action of organs, glycemic control and cholesterol, these berries are much used today, without much information about adverse effects. This article aims to look through the literature review, data on drug interaction with warfarin Goji Berry and adverse reactions such as photosensitivity, besides the probable contamination of berries from Goji Berry by heavy metals and pesticides, contributing with information necessary for the population to educate patients and clinicians of the importance of the pharmaceutical and medical guidance in the use of herbal medicines. [ABSTRACT FROM AUTHOR]

Published

2014

13. PXR polymorphisms and their impact on pharmacokinetics/pharmacodynamics of repaglinide in healthy Chinese volunteers.

Author

Du, Qing-qing, Wang, Zhi-jun, He, Lin, Jiang, Xue-hua, and Wang, Ling

Subjects

*ANALYSIS of variance, *CELL receptors, *CONFIDENCE intervals, *GENETIC polymorphisms, *HIGH performance liquid chromatography, *HYPOGLYCEMIC agents, *MASS spectrometry, *OXIDOREDUCTASES, *STATISTICS, *T-test (Statistics), *DATA analysis, *OXACILLIN, *DESCRIPTIVE statistics, *PHARMACODYNAMICS

Abstract

Purpose: CYP3A4 is the main isoform of cytochrome P450 oxidases involved in the metabolism of approximately 60 % drugs, and its expression level is highly variable in human subjects. CYP3A4 is regulated by many transcription factors, among which the pregnane X receptor/steroid and xenobiotic receptor (PXR/SXR, NR1I2) have been identified as the most critical. Genetic polymorphisms (such as SNPs) in PXR may affect the expression level of CYP3A4. Although numerous SNPs have been identified in PXR and have appeared to affect PXR function, their impact on the expression of CYP3A4 in human subjects has not been well studied. Thus, a clinical study in healthy Chinese subjects was conducted to investigate the impact of PXR polymorphisms on repaglinide (an endogenous marker for CYP3A4 activity) pharmacokinetics used alone or in combination with a PXR inducer, flucloxacillin. Method: Two SNPs, −298A>G and 11193T>C, were identified as the tag SNPs to represent the overall genetic polymorphic profile of PXR. To evaluate the potential functional change of these two SNPs, 24 healthy subjects were recruited in a pharmacokinetics/pharmacodynamics study of repaglinide with or without flucloxacillin. Results: The pharmacokinetic parameters including AUC and T were significantly different among the PXR genotype groups. The SNPs of −298G/G and 11193C/C were found to be associated with a lower PXR activity resulting in reduction of CYP3A4 activity in vivo. After administration of flucloxacillin, a significant drug-drug interaction was observed. The clearance of repagnilide was significantly increased by concomitant flucloxacillin in a genotype dependent manner. The subjects with SNPs of −298G/G and 11193C/C appeared to be less sensitive to flucloxacillin. Conclusion: Our study results demonstrated for the first time the impact of genetic polymorphisms of PXR on the PK and PD of repaglinide, and showed that subjects with genotype of −298G/G and 11193C/C in PXR has a decreased elimination rate of 3A4/2C8. Furthermore, flucloxacillin was able to induce 3A4/2C8 expression mediated by PXR in a genotype dependent manner. [ABSTRACT FROM AUTHOR]

Published

2013

14. Effects of itraconazole and rifampicin on the pharmacokinetics and safety of youkenafil, a novel phosphodiesterase type 5 inhibitor, in healthy Chinese subjects.

Author

Wang K, Ding J, Li X, Guo W, Zhu X, Su Y, Sun L, Zhou H, and Ding L

Subjects

Area Under Curve, China, Cross-Over Studies, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors adverse effects, Cytochrome P-450 CYP3A Inhibitors pharmacokinetics, Cytochrome P-450 Enzyme System metabolism, Drug Interactions, Humans, Male, Phosphodiesterase 5 Inhibitors adverse effects, Phosphodiesterase 5 Inhibitors pharmacokinetics, Itraconazole pharmacokinetics, Rifampin adverse effects, Rifampin pharmacokinetics

Abstract

Youkenafil is a novel selective phosphodiesterase type 5 inhibitor to treat erectile dysfunction. In order to study the drug-drug interactions of youkenafil, in vitro experiments were conducted with human liver microsomes and recombinant isoenzymes to identify the effect of cytochrome P450 (CYP) enzymes on the metabolism of youkenafil. Then two clinical studies were performed to investigate the effects of itraconazole and rifampicin (potent CYP3A4/5 inhibitor and inducer, respectively) on the pharmacokinetics of youkenafil and its main metabolite, N-desethyl youkenafil (M1). Each study enrolled thirty healthy male subjects. In study 1, subjects were given a single dose of youkenafil (50 mg on Days 1 and 13) and multiple doses of itraconazole (200 mg once daily from Days 6 to 14). In study 2, subjects were given a single dose of youkenafil (100 mg on Days 1 and 20) and multiple doses of rifampicin (600 mg once daily from Days 6 to 20). The results showed that youkenafil was mainly metabolized through CYP3A4/5 in vitro. Itraconazole increased youkenafil AUC and C max by about 12- and 6-fold, respectively, and increased M1 AUC and C max by 5- and 1.3-fold, respectively. Conversely, rifampicin reduced youkenafil AUC and C max both by about 98%. It did not change the AUC of M1 significantly, but increased the C max by 30%. All treatments were well tolerated by subjects in both studies. Therefore, co-administration of youkenafil with potent inhibitors or inducers of CYP3A4/5 should be avoided or carefully monitored., (Copyright © 2022 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2022

15. Effect of a traditional Chinese medicine Liu Wei Di Huang Wan on the activities of CYP2C19, CYP2D6 and CYP3A4 in healthy volunteers.

Author

Chen, Y., Ouyang, D.-S., Kang, Z., Yang, G.-P., Tan, Z.-R., Zhou, G., and Yan, J.

Subjects

*KIDNEY disease treatments, *CHINESE medicine, *LIU wei di huang, *DRUG interactions, *PHARMACEUTICAL powders, *DRUG efficacy

Abstract

Liu Wei Di Huang Wan (LDW), a well-known traditional Chinese medicine, is widely used for the treatment of various diseases in China. This study was designed to investigate the potential herb–drug interactions of LDW in healthy volunteers and attempted to ascertain whether the interaction might be affected by genotypes. We assessed the effect of LDW on the activities of CYP2C19, CYP2D6 and CYP3A4 in 12 Chinese healthy subjects in a single-center, controlled, non-blinded, two-way crossover clinical trial. The subject pool consisted of six extensive metabolizers with CYP2C19*1/*1 and six poor metabolizers with CYP2C19*2/*2. Placebo or 4.8 g LDW (12 pills, 0.2 g/pill, twice daily) was given to each participant for 14 continuous days with a wash-out period of 2 weeks after an oral administration of 30 mg omeprazole, 30 mg dextromethorphan hydrobromide and 7.5 mg midazolam. The activities of CYP2C19, CYP2D6 and CYP3A4 were ascertained by their respective plasma or urinary metabolic ratios on day 14 post-treatment. There is no difference in the activities of the three tested enzymes before or after a 14-day administration of LDW. LDW had no effect on the pharmacokinetic parameters of the substrates and their metabolites. A 14-day administration of LDW did not affect the activities of CYP2C19, CYP2D6 and CYP3A4. LDW is unlikely to cause pharmacokinetic interaction when it is combined with other medications predominantly metabolized by these enzymes. [ABSTRACT FROM AUTHOR]

Published

2012

16. Effect of genistein on the activities of cytochrome P450 3A and P-glycoprotein in Chinese healthy participants.

Author

Xiao, C.-Q., Chen, R., Lin, J., Wang, G., Chen, Y., Tan, Z.-R., and Zhou, H.-H.

Subjects

*GENISTEIN, *CYTOCHROME P-450, *GLYCOPROTEINS, *ISOFLAVONOIDS, *CHINESE people, *CROSSOVER trials, *DRUG administration, *DISEASES

Abstract

To determine the effect of genistein on cytochrome P450 3A (CYP3A) and P-glycoprotein (P-gp) function using the probe substrates midazolam and talinolol, respectively. Eighteen healthy adult male participants were enrolled in a two-phase randomized crossover design. In each phase, the participants received placebo or genistein for 14 days. On the 15th day, midazolam and talinolol were administered and blood samples were obtained. Midazolam and talinolol pharmacokinetic parameter values were calculated and compared before and after genistein administration. Co-administration of genistein decreased the area under the concentration–time curve from 0 to 36 h (AUC 0-36) (143.65 ± 55.40 ng h/mL versus 126.10 ± 40.14 ng h/mL, p < 0.05), and the area under the concentration–time curve from zero to infinity (AUC 0-∞) (209.18 ± 56.61 ng h/mL versus 180.59 ± 43.03 ng h/mL, p < 0.05), and also maximum concentration (Cmax) of midazolam (48.86 ± 20.21 ng/mL versus 36.25 ± 14.35 ng/mL p < 0.05). Similarly, AUC 0-36 (2490.282 ± 668.79 ng h/mL versus 2114.46 ± 861.11 ng h/mL, p < 0.05), AUC 0-∞ (2980.45 ± 921.09 ng h/mL versus 2626.92 ± 1003.78 ng h/mL, p < 0.05) and Cmax of talinolol (326.58 ± 197.67 ng/mL versus 293.42 ± 127.19 ng/mL, p < 0.05) were reduced by genistein co-administration. The oral clearance of midazolam (1.68 ± 0.85 h-1 versus 3.98 ± 0.59 h-1, p < 0.05) and talinolol (3.34 ± 1.24 h-1 versus 3.79 ± 1.55 h-1, p<0.05) were increased by genistien significantly. Administration of genistein can result in a modest induction of CYP3A and possibly P-gp activity in healthy volunteers. [ABSTRACT FROM AUTHOR]

Published

2012

17. The influence of genetic polymorphisms and interacting drugs on initial response to warfarin in Chinese patients with heart valve replacement.

Author

Zhong, Shi-Long, Liu, Yuan, Yu, Xi-Yong, Xu, Dan, Tan, Hong-Hong, Lin, Qiu-Xiong, Yang, Min, Lao, Hai-Yan, and Lin, Shu-Guang

Subjects

*AGE distribution, *AMIODARONE, *ANALYSIS of variance, *ANTIFUNGAL agents, *ANTILIPEMIC agents, *BIOLOGICAL assay, *BLOOD coagulation tests, *CHI-squared test, *CHINESE people, *COMPUTER software, *CONFIDENCE intervals, *DRUG interactions, *ENZYME inhibitors, *FISHER exact test, *GENES, *GENETIC polymorphisms, *PROSTHETIC heart valves, *HEALTH outcome assessment, *REGRESSION analysis, *RESEARCH funding, *STATISTICS, *SURVIVAL analysis (Biometry), *WARFARIN, *DATA analysis, *TREATMENT effectiveness, *PROPORTIONAL hazards models, *RETROSPECTIVE studies, THROMBOEMBOLISM prevention

Abstract

Purpose: Compared with genetic factors, drug interactions were largely unexplored in warfarin pharmacogenetic studies. This study sought to systematically investigate the effects of genetic polymorphisms of VKORC1, STX4A, CYP2C9, CYP3A4, and GGCX and interacting drugs on the initial responses to warfarin in Chinese patients with heart valve replacement (HVR). Methods: A retrospective study was conducted in 809 patients starting warfarin therapy after HVR. The relationships between 12 polymorphisms plus 47 drugs and primary outcomes of the time to the first international normalized ratio (INR) ≥ 1.8 and the time to the first INR > 3.5 and the secondary outcomes of the proportion of time INR < 1.8, the proportion of time INR > 3.5, and the daily warfarin dose in the first 28 days after the initiation of warfarin treatment were analyzed. Results: Genetic polymorphisms and interacting drugs could significantly affect the primary and secondary outcomes. The time to the first INR ≥ 1.8 was significantly influenced by the body surface area (BSA), VKORC1 g.3588G > A allele, and CYP2C9*3 allele, with hazard ratio (HR; 95% confidence interval [CI]) of 0.34 (0.17-0.66), 2.71 (2.2-3.35) and 1.43 (1.07-1.93) respectively. The time to the first INR > 3.5 was affected not only by BSA, VKORC1 g.3588G > A allele, and CYP2C9*3 allele with HR (95%CI) of 0.26 (0.07-0.99), 2.76 (1.61-4.72), and 3.09 (2.02-4.74) respectively, but also by age and interacting drugs, including fluconazole, amiodarone, and simvastatin with HR (95%CI) of 1.02 (1.01-1.04), 2.66 (1.16-6.08), 1.78 (1.17-2.73), and 5.33 (1.67-16.96) respectively. Conclusions: Not only VKORC1 and CYP2C9 genotypes, but also interacting drugs, had a significant impact on the variability of the initial response to warfarin. [ABSTRACT FROM AUTHOR]

Published

2011

18. The impact of rifampicin on the pharmacokinetics of fuzuloparib in healthy Chinese male volunteers.

Author

Zhang Q, Kai J, Zhai Y, Xu N, Shentu J, Zhang Y, Liang Y, Wang Y, and Wu L

Subjects

Area Under Curve, China, Cross-Over Studies, Drug Interactions, Healthy Volunteers, Humans, Male, Cytochrome P-450 CYP3A Inducers adverse effects, Rifampin adverse effects

Abstract

Aims: This clinical study was conducted to evaluate the impact of rifampicin on the pharmacokinetics of fuzuloparib., Methods: In this single-centre, single-arm, open-label, fixed-sequence study, healthy male subjects took a single 50 mg dose of fuzuloparib on two separate occasions: the first was on Day 1 as monotherapy, and the second was on Day 12 after oral administration of rifampicin 600 mg once daily for 8 days. Series of blood samples were obtained before and after fuzuloparib administration at different time points: pre-dose, and 0.5, 1, 2, 3, 4, 6, 8, 10, 12, 24, 36, 48 and 72 hours post-dose. All samples were examined using liquid chromatography with tandem mass spectrometry. PK parameters were estimated by using a non-compartmental method with Phoenix WinNonlin software. Safety was assessed by monitoring for changes in vital signs and laboratory tests, physical examinations, and incidences of adverse events (AEs)., Results: A total of 16 Chinese male subjects were enrolled. Of these, 16 and 15 cases were evaluable for PK analysis following administration with fuzuloparib alone and pretreatment with rifampicin, respectively. Pretreatment with rifampicin resulted in a statistically significant reduction in the systemic exposure to fuzuloparib. The treatment ratio and 90% confidence intervals (CIs) for AUC 0-∞ and C max were 0.10 (0.095-0.115) and 0.32 (0.281-0.365), respectively. A single administration of fuzuloparib after multiple oral dosing of rifampicin was well-tolerated, without severe AEs., Conclusion: The exposure of fuzuloparib was dramatically decreased when pretreated with rifampicin. Strong CYP3A4 inducers should be avoided during fuzuloparib treatment., (© 2021 British Pharmacological Society.)

Published

2022

19. Mobile Apps for Drug-Drug Interaction Checks in Chinese App Stores: Systematic Review and Content Analysis.

Author

Shen C, Jiang B, Yang Q, Wang C, Lu KZ, Gu M, and Yuan J

Subjects

China, Delivery of Health Care, Drug Interactions, Humans, Mobile Applications, Pharmaceutical Preparations

Abstract

Background: As a computerized drug-drug interaction (DDI) alert system has not been widely implemented in China, health care providers are relying on mobile health (mHealth) apps as references for checking drug information, including DDIs., Objective: The main objective of this study was to evaluate the quality and content of mHealth apps supporting DDI checking in Chinese app stores., Methods: A systematic review was carried out in November 2020 to identify mHealth apps providing DDI checking in both Chinese iOS and Android platforms. We extracted the apps' general information (including the developer, operating system, costs, release date, size, number of downloads, and average rating), scientific or clinical basis, and accountability, based on a multidimensional framework for evaluation of apps. The quality of mHealth apps was evaluated by using the Mobile App Rating Scale (MARS). Descriptive statistics, including numbers and percentages, were calculated to describe the characteristics of the apps. For each app selected for evaluation, the section-specific MARS scores were calculated by taking the arithmetic mean, while the overall MARS score was described as the arithmetic mean of the section scores. In addition, the Cohen kappa (κ) statistic was used to evaluate the interrater agreement., Results: A total of 7 apps met the selection criteria, and only 3 included citations. The average rating score for Android apps was 3.5, with a minimum of 1.0 and a maximum of 4.9, while the average rating score for iOS apps was 4.7, with a minimum of 4.2 and a maximum of 4.9. The mean MARS score was 3.69 out of 5 (95% CI 3.34-4.04), with the lowest score of 1.96 for Medication Guidelines and the highest score of 4.27 for MCDEX mobile. The greatest variation was observed in the information section, which ranged from 1.41 to 4.60. The functionality section showed the highest mean score of 4.05 (95% CI 3.71-4.40), whereas the engagement section resulted in the lowest average score of 3.16 (95% CI 2.81-3.51). For the information quality section, which was the focus of this analysis, the average score was 3.42, with the MCDEX mobile app having the highest score of 4.6 and the Medication Guidelines app having the lowest score of 1.9. For the overall MARS score, the Cohen interrater κ was 0.354 (95% CI 0.236-0.473), the Fleiss κ was 0.353 (95% CI, 0.234-0.472), and the Krippendorff α was 0.356 (95% CI 0.237-0.475)., Conclusions: This study systematically reviewed the mHealth apps in China with a DDI check feature. The majority of investigated apps demonstrated high quality with accurate and comprehensive information on DDIs. However, a few of the apps that had a massive number of downloads in the Chinese market provided incorrect information. Given these apps might be used by health care providers for checking potential DDIs, this creates a substantial threat to patient safety., (©Chunying Shen, Bin Jiang, Qilian Yang, Chengnan Wang, Kevin Z Lu, Meng Gu, Jing Yuan. Originally published in JMIR mHealth and uHealth (https://mhealth.jmir.org), 15.06.2021.)

Published

2021

20. Effect of Fluconazole on the Pharmacokinetic Properties of Imrecoxib, a Novel NSAID: A Single-center, Open-label, Self-controlled Study in Healthy Chinese Male Volunteers.

Author

Zuo CZ, Gong Y, Hou XY, Zhang YF, Peng WX, Zhu RH, Zhong DF, and Chen XY

Subjects

Administration, Oral, Adult, Area Under Curve, China, Cross-Over Studies, Cyclooxygenase 2 Inhibitors adverse effects, Cyclooxygenase 2 Inhibitors blood, Drug Interactions, Healthy Volunteers, Humans, Male, Pyrroles adverse effects, Pyrroles blood, Random Allocation, Sulfides adverse effects, Sulfides blood, Young Adult, Antifungal Agents pharmacology, Cyclooxygenase 2 Inhibitors pharmacokinetics, Fluconazole pharmacology, Pyrroles pharmacokinetics, Sulfides pharmacokinetics

Abstract

Purpose: Imrecoxib is one type of cyclooxygenase-2 inhibitor with the capability of reducing the potential cardiovascular risk caused by other NSAIDs. Co-administration with other medications can affect the cytochrome P450 (CYP) 2C9 enzyme function; thus, imrecoxib metabolism can be affected. The purpose of this research was to evaluate the effects of fluconazole, which is known to inhibit CYP2C9, on imrecoxib's pharmacokinetic (PK) parameters., Methods: In this single-center, single-arm, open-label, self-controlled study, 12 healthy Chinese male volunteers (mean [SD] age, 22.6 [2.43] years) received the following 2 treatments separated by a washout period of 8 days under a fasting state: (1) a single oral dose of imrecoxib 100 mg; and (2) fluconazole 200 mg/d over 6 days followed by concurrent dosing of imrecoxib 100 mg and fluconazole 200 mg. Plasma concentrations of imrecoxib (M0) and its metabolites (4'-hydroxymethyl metabolite [M1] and 4'-carboxylic acid metabolite [M2]) for PK analysis were obtained at 0 (baseline) and 0.5, 1, 1.5, 2, 3, 4, 8, 12, 24, 48, and 72 hours after imrecoxib dosing. Safety and tolerability assessments were performed throughout the study., Findings: All subjects completed the study. There was 1 adverse event; drug-induced liver damage in 1 subject occurred after he received imrecoxib plus fluconazole, and the subject recovered without any sequelae. Coadministration with fluconazole resulted in much higher plasma imrecoxib concentrations, with an increase of 88% in C max and 72% in AUC 0-t compared with only imrecoxib treatment, which showed that fluconazole may increase plasma exposure to imrecoxib. Fluconazole also caused a small, but not clinically relevant, decrease in M1 and M2 mean C max (13% and 14%, respectively), but there was minimal change in M1 and M2 mean AUC 0-t (3% and 2%). However, there were no statistically significant differences in vital signs, clinical laboratory test results, ECGs, or adverse events between treatments., Implications: Concurrent administration of imrecoxib and fluconazole did not seem to change imrecoxib's safety profile. The ratio (imrecoxib + fluconazole/imrecoxib) for AUC 0-t was 1.72 (90% CI, 1.41-2.11) and for Cmax it was 1.88 (90% CI, 1.59-2.21). Hence, it is necessary to adjust the imrecoxib dose when it is concurrently used with other CYP2C9 inhibitors., (Copyright © 2018. Published by Elsevier Inc.)

Published

2018