Purpose:
Complementary and alternative medicines are widely used in the HIV-infected population.
Recent data have shown serious drug interactions between certain complementary medicines and
protease inhibitors. Silymarin (Milk thistle) is a commonly used dietary supplement in
HIV-infected patients for treatment of hepatitis or as a hepato-protectant. Data are
available suggesting that it may alter cytochrome P4503A4-mediated drug metabolism. To
evaluate the effect of milk thistle on the protease inhibitor, indinavir (IDV), ten healthy
subjects will receive IDV (Crixivan) alone and in combination with an over-the-counter
silymarin preparation. IDV will initially be administered alone at a dose of 800 mg Q8H for
four doses and serial samples will be collected for determination of IDV pharmacokinetics
after the morning dose on day 2. Subjects will then initiate therapy will milk thistle
using a standardized formulation and dose for three weeks after which subjects will then
again take 4 doses of IDV and have serial samples collected for IDV plasma concentrations.
There will then be a 11-day washout period with no drugs, after which IDV will again be
given for 4 doses and samples will be collected evaluate the offset of the effects of milk
thistle. To examine the effect of milk thistle on other CYP450 pathways, subjects will
receive a single dose of caffeine and dextromethorphan and have urine collected before and
after milk thistle, and after the washout period. Indinavir, caffeine, and dextromethorphan
concentrations in plasma or urine will be determined using validated HPLC methods.
Steady-state noncompartmental parameters of indinavir in the presence and absence of milk
thistle will be determined. Pharmacokinetic parameters will be compared using ANOVA that
will include factors for a period effect and a treatment effect. Statistical analyses will
include calculation of the mean ratio of the AUC in the treatment phases compared to IDV
alone and determination of 95% confidence intervals. This study will help define the drug
interaction potential of complementary and alternative therapies in HIV-infected patients.
Study summary:
Complementary and alternative medicines are widely used in the HIV-infected population.
Recent data have shown serious drug interactions between certain complementary medicines and
protease inhibitors. Silymarin (Milk thistle) is a commonly used dietary supplement in
HIV-infected patients for treatment of hepatitis or as a hepato-protectant. Data are
available suggesting that it may alter cytochrome P4503A4-mediated drug metabolism. To
evaluate the effect of milk thistle on the protease inhibitor, indinavir (IDV), ten healthy
subjects will receive IDV (Crixivan) alone and in combination with an over-the-counter
silymarin preparation. IDV will initially be administered alone at a dose of 800 mg Q8H for
four doses and serial samples will be collected for determination of IDV pharmacokinetics
after the morning dose on day 2. Subjects will then initiate therapy will milk thistle
using a standardized formulation and dose for three weeks after which subjects will then
again take 4 doses of IDV and have serial samples collected for IDV plasma concentrations.
There will then be an 11-day washout period with no drugs, after which IDV will again be
given for 4 doses and samples will be collected evaluate the offset of the effects of milk
thistle. To examine the effect of milk thistle on other CYP450 pathways, subjects will
receive a single dose of caffeine and dextromethorphan and have urine collected before and
after milk thistle, and after the washout period. Indinavir, caffeine, and dextromethorphan
concentrations in plasma or urine will be determined using validated HPLC methods.
Steady-state noncompartmental parameters of indinavir in the presence and absence of milk
thistle will be determined. Pharmacokinetic parameters will be compared using ANOVA that
will include factors for a period effect and a treatment effect. Statistical analyses will
include calculation of the mean ratio of the AUC in the treatment phases compared to IDV
alone and determination of 95% confidence intervals. This study will help define the drug
interaction potential of complementary and alternative therapies in HIV-infected patients.
Criteria:
Age 18 to 65 years.
Healthy by medical history and physical exam.
No concurrent chronic medications, including oral contraceptives.
Non-smoker or not having smoked for the past 6 months or longer.
Laboratory values within established NIAID guidelines for participation in clinical
studies: AST/SGOT less than or equal to 2 times ULN; Serum creatinine less then or equal
to ULN; Hemoglobin greater than or equal to 10 g/dl.
Ability to abstain from caffeine containing foods/beverages, ethanol, grapefruit or
grapefruit juice and charbroiled foods for 72 hours prior to, and the day of, phenotyping
procedures.
Ability to abstain from dextromethorphan-containing over the counter preparations for 72
hours prior to, and the day of, phenotyping procedures.
No concomitant therapy with other inhibitors or inducers of cytochrome P-450 mediated drug
metabolism within 30 days of study (including grapefruit juice).
No ingestion of dietary supplements within the past 30 days.
Ability to obtain venous access for sample collection.
No presence of life-threatening or unstable renal, hepatic, cardiovascular, hematologic,
neurologic, psychiatric, or respiratory disease or any other condition that may interfere
with the interpretation of the study results or not be in the best interests of the
patient in the opinion of the investigator.
Patients must not have a positive pregnancy test.
No presence of persistent diarrhea or malabsorption that would interfere with the
patient's ability to adequately absorb drugs.
No drug or alcohol use that may impair safety or adherence.
No history of intolerance to milk thistle, indinavir, caffeine, or dextromethorphan
preparations.
Brief Title:
The Effect of Milk Thistle on the Pharmacokinetics of Indinavir
Official Title:
The Effect of Milk Thistle on the Pharmacokinetics of Indinavir
Study Source:
National Institutes of Health Clinical Center (CC)
Oversight Authority:
United States: Federal Government
Study Design:
Endpoint Classification: Safety Study, Primary Pu
Study Outcomes
There are no available Study Outcomes
Study Arms
There are no available Study Arms
Sample and Retention Information
There are no available Sample and Retention Information
Study Links
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