Drug Metabolizing Enzyme and Transporter Function in Chronic Kidney Disease
Status: | Recruiting |
---|---|
Conditions: | Renal Impairment / Chronic Kidney Disease, Gastrointestinal |
Therapuetic Areas: | Gastroenterology, Nephrology / Urology |
Healthy: | No |
Age Range: | 18 - 70 |
Updated: | 9/20/2018 |
Start Date: | October 2014 |
End Date: | August 2019 |
Contact: | Melanie Joy, PharmD, PhD |
Email: | melanie.joy@ucdenver.edu |
Phone: | 303-724-7416 |
This study investigates the effect of vitamin D deficiency on drug metabolism and transport
in patients with chronic kidney disease (CKD) and in healthy controls.
The central hypothesis is that vitamin D concentrations independently affect metabolism and
transport function in CKD patients. An over-arching goal of this proposal is to make drug
therapies safer and more effective to reduce the significant morbidity and mortality in
patients with CKD.
in patients with chronic kidney disease (CKD) and in healthy controls.
The central hypothesis is that vitamin D concentrations independently affect metabolism and
transport function in CKD patients. An over-arching goal of this proposal is to make drug
therapies safer and more effective to reduce the significant morbidity and mortality in
patients with CKD.
Specific Aim 1: Determine the effect of vitamin D deficiency and repletion on xenobiotic
clearance in vivo. The study will mechanistically evaluate the function of major pathways of
metabolism and transport by prospectively studying clearance phenotypes utilizing "probe"
drugs commonly used for this purpose in CKD patients and healthy volunteers under vitamin D
deficient and replete states. Bupropion, midazolam, olmesartan, fexofenadine, in addition to
an endogenous probe (N-methylnicotinamide), will be used to phenotype major phase I drug
metabolizing enzymes [cytochrome P450 2B6 (CYP2B6), cytochrome P450 3A4/5 (CYP3A4/5)], and
transporters [multidrug resistance associated protein 2 (MRP2), P-glycoprotein (P-gp), and
multidrug and toxin extrusion protein 1/2K (MATE1/2K)], respectively. Hypothesis: The in vivo
function of individual pathways of xenobiotic metabolism and transport are affected by
vitamin D status (and CKD).
Specific Aim 2: Determine the effect of CKD on the in vivo function of individual CYPs
responsible for vitamin D metabolism and the pharmacokinetics of cholecalciferol (vitamin
D3). The research will prospectively measure the activity of CYP450s responsible for
cholecalciferol metabolism, and simultaneously evaluate the pharmacokinetics (PK) of
cholecalciferol after single- and multiple-dose administration to CKD patients (stages 1-5)
and healthy volunteers. Hypothesis: CKD alters the activity of individual CYPs responsible
for vitamin D metabolism, leading to modified clearance of cholecalciferol.
clearance in vivo. The study will mechanistically evaluate the function of major pathways of
metabolism and transport by prospectively studying clearance phenotypes utilizing "probe"
drugs commonly used for this purpose in CKD patients and healthy volunteers under vitamin D
deficient and replete states. Bupropion, midazolam, olmesartan, fexofenadine, in addition to
an endogenous probe (N-methylnicotinamide), will be used to phenotype major phase I drug
metabolizing enzymes [cytochrome P450 2B6 (CYP2B6), cytochrome P450 3A4/5 (CYP3A4/5)], and
transporters [multidrug resistance associated protein 2 (MRP2), P-glycoprotein (P-gp), and
multidrug and toxin extrusion protein 1/2K (MATE1/2K)], respectively. Hypothesis: The in vivo
function of individual pathways of xenobiotic metabolism and transport are affected by
vitamin D status (and CKD).
Specific Aim 2: Determine the effect of CKD on the in vivo function of individual CYPs
responsible for vitamin D metabolism and the pharmacokinetics of cholecalciferol (vitamin
D3). The research will prospectively measure the activity of CYP450s responsible for
cholecalciferol metabolism, and simultaneously evaluate the pharmacokinetics (PK) of
cholecalciferol after single- and multiple-dose administration to CKD patients (stages 1-5)
and healthy volunteers. Hypothesis: CKD alters the activity of individual CYPs responsible
for vitamin D metabolism, leading to modified clearance of cholecalciferol.
Inclusion criteria for CKD patients:
- vitamin D deficient (<30 ng/mL)
- hemoglobin >10 g/dL
- willing to abstain from fruit juices or alcohol within 7 days of PK assessments
- no changes in prescription or nonprescription medications within 4 wks of study start
- age 18-70 yrs
- If a diagnosis of CKD, must be due to diabetes mellitus or hypertension
- Signed informed consent
Inclusion Criteria for Healthy Controls:
- vitamin D deficient (<30 ng/mL)
- hemoglobin >10 g/dL
- willing to abstain from fruit juices or alcohol within 7 days of PK assessments
- no changes in prescription or nonprescription medications within 4 wks of study start
- age 18-70 yrs
- Signed informed consent
Exclusion criteria for CKD patients:
- History of >14 alcoholic drinks/wk
- Not likely to be compliant with study visits
- Pregnant or lactating
- Predisposition to or history of hypercalcemia
- History of allergy, sensitivity, or contraindication to probe drugs (seizures, drug
metabolism interactions, etc)
- Use of prescribed or nonprescribed therapies that could interact with probe drugs
(including prototypical inhibitors or inducers)
- Active autoimmune disease or active/recent infections requiring antimicrobial
treatment within the previous 4 wks will be excluded to minimize inflammatory-mediated
changes in vitamin D status and patient heterogeneity.
- Presence of clinically significant hepatic insufficiency (total bilirubin greater than
1.5 times the upper limit of normal or transaminase (ALT, AST) elevations greater than
2 times the upper limit of the laboratory reference range or liver disease
- Active seizure disorder or those patients receiving large doses of medications that
are known to reduce seizure threshold
- Currently receiving cholecalciferol or a vitamin D analogue
Exclusion Criteria for Healthy Controls:
- History of >14 alcoholic drinks/wk
- Not likely to be compliant with study visits
- Pregnant or lactating
- Predisposition to or history of hypercalcemia
- History of allergy, sensitivity, or contraindication to probe drugs (seizures, drug
metabolism interactions, etc)
- Use of prescribed or nonprescribed therapies that could interact with probe drugs
(including prototypical inhibitors or inducers)
- Active autoimmune disease or active/recent infections requiring antimicrobial
treatment within the previous 4 wks will be excluded to minimize inflammatory-mediated
changes in vitamin D status and patient heterogeneity.
- Presence of clinically significant hepatic insufficiency (total bilirubin greater than
1.5 times the upper limit of normal or transaminase (ALT, AST) elevations greater than
2 times the upper limit of the laboratory reference range or liver disease
- Active seizure disorder or those patients receiving large doses of medications that
are known to reduce seizure threshold
- Currently receiving cholecalciferol or a vitamin D analogue
- Any clinical evidence of chronic kidney disease as defined by the National Kidney
Foundation Dialysis Outcomes Quality Initiative (NKF DOQI) guidelines
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sites
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4200 Fifth Ave
Pittsburgh, Pennsylvania 15260
Pittsburgh, Pennsylvania 15260
(412) 624-4141
Phone: 412-624-4683
University of Pittsburgh The University of Pittsburgh is a state-related research university, founded as the...
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