Cytochrom p450 3A4 and 1A2 Phenotyping for the Individualization of Treatment With Sunitinib or Erlotinib in Cancer Patients
NCT ID: NCT01402089
Last Updated: 2016-02-02
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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COMPLETED
PHASE4
54 participants
INTERVENTIONAL
2012-01-31
2015-11-30
Brief Summary
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Detailed Description
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The primary objective of this study is to show that the individual CYP3A4 and CYP1A2-phenotype as assessed by probe drugs predicts drug exposure to sunitinib and erlotinib. Secondary objectives of the study are to define the correlation between the individual CYP-phenotype and treatment-related toxicity, testing the feasibility of drug bioanalysis from patient's dry blood spots (DBS), build an integrated covariate model on sunitinib and erlotinib pharmacokinetics and define a dosing algorithm for both sunitinib and erlotinib based on the individual CYP-phenotype.
Study endpoints:
Primary endpoint:
• To show that individual drug clearance of sunitinib or erlotinib is significantly higher in patients with a high-activity CYP3A4/1A2-phenotype.
Secondary endpoints:
* To specify the correlation between the CYP-phenotype and treatment-related toxicity.
* To assess the feasibility of drug bioanalysis from patient's dry blood spots (DBS).
* To build an integrated covariate model of sunitinib and erlotinib pharmacokinetics to define the quantitative relationship between the CYP-phenotype activity and drug exposure.
* To define a dosing algorithm for both sunitinib and erlotinib based on the individual CYP-phenotype using data simulations on the previously defined population covariate model.
Trial Design:
Prospective, nonrandomized, pharmacological cohort study.
Main selection criteria
* Histologically or cytologically confirmed renal-cell cancer (sunitinib), gastrointestinal stromal tumor (sunitinib) or non small-cell lung cancer (erlotinib)
* Both early or advanced tumor stage
* Indication for the therapeutic use of either sunitinib or erlotinib
* Written informed consent and willing to undergo PK-sampling
* Adequate organ function
* No concurrent radiotherapy or systemic anticancer treatment with another drug
Trial Duration The present study is projected to start in June 2011, with the inclusion of a total of 60 patients (at least 25 patients for each sunitinib and erlotinib). The study is expected to finalize patient accrual in December 2013.
Statistical considerations The trial is designed to show a linear inverse relationship between the individual CYP-phenotype and total drug steady-state AUC (sunitinib plus SU12662 and erlotinib plus OSI-420, respectively), whereat CYP1A2 only accounts for the metabolism of erlotinib. With the inclusion of 60 patients, the study has a power of 90% to detect a relevant relationship between the CYP-phenotype activity and sunitinib/erlotinib steady-state AUC, with a regression coefficient of \>0.4 for the H1-hypothesis (and accepting a regression coefficient of \>0.1 for the H0-hypothesis) at the 5% significance level.
Trial Treatment Sunitinib: 50 mg p.o. daily for 4 out of 6 weeks, or 37.5 mg daily continuous until disease progression, unacceptable toxicity or withdrawal of informed consent.
Erlotinib: 150 mg p.o. daily until disease progression, unacceptable toxicity or withdrawal of informed consent.
Potential study outcome This study makes a significant contribution to global efforts for more individualized anticancer treatment. If successful, we will be able to make dosing recommendations for sunitinib and erlotinib based on a simple probe drug assay.
Conditions
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Study Design
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NA
SINGLE_GROUP
TREATMENT
NONE
Interventions
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Sunitinib
Patients with renal-cell cancer or GIST are receiving conventional treatment with sunitinib (50mg/day for 4 out of 6 weeks)
Erlotinib
Patients with non small-cell lung cancer receive conventional treatment with erlotinib 150mg/day.
Midazolam
For phenotyping of CYP3A4, all patients receive one-time midazolam 2mg as a drinking solution at the start of study treatment.
Caffeine
For phenotyping of CYP1A2, patients with non small-cell lung cancer receive additionally one-time caffeine 100mg as a tablet.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Both early or advanced tumor stage
* Indication for the therapeutic use of either sunitinib or erlotinib
* Written informed consent and willing to undergo PK-sampling
* Patients \> 18 years of age
* ECOG performance status or ≤2
* Adequate laboratory parameters:
i. Serum creatinine and serum bilirubin ≤ 1.5 X ULN ii. Serum ALT and AST ≤ 2.5 X ULN (or ≤ 5 in case of liver metastases) iii. Serum calcium ≤ 11,6 mg/dl (2.9 mmol/L)
Exclusion Criteria
* Known hypersensitivity to trial drug or any compounds of the drug
* Concurrent radiotherapy
* Concurrent systemic anticancer treatment with the exception of bisphosphonates and bevacizumab in patients with non small-cell lung cancer
18 Years
ALL
No
Sponsors
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University of Basel
OTHER
Markus Joerger
OTHER
Responsible Party
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Markus Joerger
MD-PhD-ClinPharm
Principal Investigators
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Markus Joerger, MD PhD
Role: STUDY_CHAIR
Cantonal Hospital St. Gallen, Switzerland
Locations
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Cantonal Hospital St.Gallen
Sankt Gallen, , Switzerland
Countries
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Related Links
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Institute research homepage
Other Identifiers
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SG 327/10
Identifier Type: -
Identifier Source: org_study_id
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