A Microdose Cocktail to Evaluate Drug Interactions in Patients with Renal Impairment

Tatosian, Daniel; Yee, Ka Lai; Zhang, Zufei; Mostoller, Kate; Paul, Erina; Sutradhar, Santosh; Larson, Patrick; Chhibber, Aparna; Wen, Jianzhong; Wang, Ya Juan; Lassman, Michael E.; Latham, Andrew H.; Pang, Jianmei; Crumley, Tami; Gillespie, Anne Marie; Marricco, Nadia Cardillo; Marenco, Ted; Murphy, Matthew; Lasseter, Kenneth C.; Marbury, Thomas; Tweedie, Donald J.; Chu, Xiaoyan; Evers, Raymond; Stoch, S. Aubrey

doi:10.1002/cpt.1998

Cited by 37 publications

(84 citation statements)

References 39 publications

(114 reference statements)

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“…Additionally, as MDZ is an intermediate hepatic extraction drug, a physiological reduction of hepatic blood flow anticipated in the elderly might also contribute to the observed reduction in hepatic clearance of MDZ (Dundee et al, 1986;Amrein and Hetzel, 1990). Our finding that CKD was not associated with changes in pharmacokinetic profiles of MDZ was consistent with a previous study where neither AUC nor C max of MDZ was affected by renal impairment (Tatosian et al, 2020).…”

Section: Discussionsupporting

confidence: 91%

“…The cocktail drugs include 1) midazolam (MDZ), a specific and selective substrate for CYP3A; 2) dabigatran etexilate (DABE), a selective substrate for intestinal P-gp; 3) pitavastatin (PTV), a relatively selective substrate for OATP1B; 4) rosuvastatin (RSV), a substrate of BCRP and OATP1B; and 5) atorvastatin (ATV), a substrate of CYP3A, OATP1B, BCRP, and P-gp. This cocktail was subsequently studied in patients with CKD, and the study results suggested that CKD reduces intestinal P-gp and BCRP activity (Tatosian et al, 2020). However, whether the observed changes were due solely to CKD or as a consequence of advancing age, remains inconclusive.…”

Section: Introductionmentioning

confidence: 99%

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Quantification of CYP3A and Drug Transporters Activity in Healthy Young, Healthy Elderly and Chronic Kidney Disease Elderly Patients by a Microdose Cocktail Approach

et al. 2021

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Background: Ageing and chronic kidney disease (CKD) affect pharmacokinetic (PK) parameters. Since mechanisms are related and remain unclear, cytochrome P450 (CYP) 3A and drug transporter activities were investigated in the elderly with or without CKD and compared to healthy adults using a microdose cocktail.Methods: Healthy young participants (n = 20), healthy elderly participants (n = 16) and elderly patients with CKD (n = 17) received, in study period 1, a single dose of microdose cocktail probe containing 30 µg midazolam, 750 µg dabigatran etexilate, 100 µg atorvastatin, 10 µg pitavastatin, and 50 µg rosuvastatin. After a 14-day wash-out period, healthy young participants continued to study period 2 with the microdose cocktail plus rifampicin. PK parameters including area under the plasma concentration-time curve (AUC), maximum plasma drug concentration (Cmax), and half-life were estimated before making pairwise comparisons of geometric mean ratios (GMR) between groups.Results: AUC and Cmax GMR (95% confidence interval; CI) of midazolam, a CYP3A probe substrate, were increased 2.30 (1.70–3.09) and 2.90 (2.16–3.88) fold in healthy elderly and elderly patients with CKD, respectively, together with a prolonged half-life. AUC and Cmax GMR (95%CI) of atorvastatin, another CYP3A substrate, was increased 2.14 (1.52–3.02) fold in healthy elderly and 4.15 (2.98–5.79) fold in elderly patients with CKD, indicating decreased CYP3A activity related to ageing. Associated AUC changes in the probe drug whose activity could be modified by intestinal P-glycoprotein (P-gp) activity, dabigatran etexilate, were observed in patients with CKD. However, whether the activity of pitavastatin and rosuvastatin is modified by organic anion transporting polypeptide 1B (OATP1B) and of breast cancer resistance protein (BCRP), respectively, in elderly participants with or without CKD was inconclusive.Conclusions: CYP3A activity is reduced in ageing. Intestinal P-gp function might be affected by CKD, but further confirmation appears warranted.Clinical Trial Registration:http://www.thaiclinicaltrials.org/ (TCTR 20180312002 registered on March 07, 2018)

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Section: Discussionsupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Quantification of CYP3A and Drug Transporters Activity in Healthy Young, Healthy Elderly and Chronic Kidney Disease Elderly Patients by a Microdose Cocktail Approach

et al. 2021

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“…Simulated decreased AUCR in 521CC is consistent with data reported with clinical OATP1B probes 3,6 and suggests the risk of underestimation of the magnitude of transporter-mediated interaction if these subjects are included in a CPI-drug interaction study, which is more likely to happen in clinical studies performed without prior genotyping (e.g., first-in-human study) or in populations with higher prevalence of 521CC. 48 In contrast, any changes in CPI synthesis did not affect fraction transported via OATP1B and simulated AUCR, highlighting no risk of underestimation of the OATP1B interaction magnitude if female subjects are included in the study. As exemplified here, the modeling of CPI gives us prospective insights of clinical output and enables optimal clinical design to increase likelihood of success.…”

Section: Prospective Application Of the Developed Cpi Modelmentioning

confidence: 89%

“…As exemplified here, the modeling of CPI gives us prospective insights of clinical output and enables optimal clinical design to increase likelihood of success. Furthermore, the physiological description of the liver processes in the CPI model enables the extension of the model to other special populations (e.g., evaluation of the changes in OATP1B activity in the chronic kidney disease population) 49,50 …”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, the physiological description of the liver processes in the CPI model enables the extension of the model to other special populations (e.g., evaluation of the changes in OATP1B activity in the chronic kidney disease population). 49,50 In conclusion, this study evaluated the impact of the genotype of OATP1B1 c521T>C, ethnicity, and sex on CPI baseline and its OATP1B-mediated interaction potential. For the first time, this revised CPI population PBPK model implemented reduced active uptake due to OATP1B1 polymorphism, ethnic differences in active uptake between Asian-Indians and Caucasians, and reduced CPI synthesis in women.…”

Section: Prospective Application Of the Developed Cpi Modelmentioning

confidence: 99%

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PBPK Model of Coproporphyrin I: Evaluation of the Impact of SLCO1B1 Genotype, Ethnicity, and Sex on its Inter‐Individual Variability

Takita

Barnett

Zhang

et al. 2021

CPT Pharmacom & Syst Pharma

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Coproporphyrin I (CPI) is an endogenous biomarker of OATP1B activity and associated drug-drug interactions. In this study, a minimal physiologically-based pharmacokinetic model was developed to investigate the impact of OATP1B1 genotype (c.521T>C), ethnicity, and sex on CPI pharmacokinetics and interindividual variability in its baseline. The model implemented mechanistic descriptions of CPI hepatic transport between liver blood and liver tissue and renal excretion. Key model parameters (e.g., endogenous CPI synthesis rate, and CPI hepatic uptake clearance) were estimated by fitting the model simultaneously to three independent CPI clinical datasets (plasma and urine data) obtained from white (n = 16, men and women) and Asian-Indian (n = 26, all men) subjects, with c.521 variants (TT, TC, and CC). The optimized CPI model successfully described the observed data using c.521T>C genotype, ethnicity, and sex as covariates. CPI hepatic active was 79% lower in 521CC relative to the wild type and 42% lower in Asian-Indians relative to white subjects, whereas CPI synthesis was 23% higher in male relative to female subjects. Parameter sensitivity analysis showed marginal impact of the assumption of CPI synthesis site (blood or liver), resulting in comparable recovery of plasma and urine CPI data. Lower magnitude of CPI-drug interaction was simulated in 521CC subjects, suggesting the risk of underestimation of CPI-drug interaction without prior OATP1B1 genotyping. The CPI model incorporates key covariates contributing to interindividual variability in its baseline and highlights the utility of the CPI modeling to facilitate the design of prospective clinical studies to maximize the sensitivity of this biomarker. Hepatic uptake via OATP1B1 and 1B3 has been widely recognized as a rate-limiting step in the clearance of anionic drugs, such as statins. 1,2 Considering the high degree of drug-drug interactions (DDIs) associated with OATP1B1 and therapeutic implications, regulatory agencies suggest elucidating factors that can change pharmacokinetics (PKs) of OATP1B1 substrates (https://www.fda.gov/media/ 13458 1/download, https://www.ema.europa.eu/en/docum ents/ scien tific-guide line/guide line-inves tigat ion-drug-inter actio ns-revis ion-1_en.pdf). Genetic polymorphism of SLCO1B1

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Drug Transport in the Liver

et al. 2022

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A Microdose Cocktail to Evaluate Drug Interactions in Patients with Renal Impairment

Cited by 37 publications

References 39 publications

Quantification of CYP3A and Drug Transporters Activity in Healthy Young, Healthy Elderly and Chronic Kidney Disease Elderly Patients by a Microdose Cocktail Approach

Quantification of CYP3A and Drug Transporters Activity in Healthy Young, Healthy Elderly and Chronic Kidney Disease Elderly Patients by a Microdose Cocktail Approach

PBPK Model of Coproporphyrin I: Evaluation of the Impact of SLCO1B1 Genotype, Ethnicity, and Sex on its Inter‐Individual Variability

Drug Transport in the Liver

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