Food-Effect Bioavailability Study of AQ-13, a Candidate Antimalarial



Status:Recruiting
Conditions:Infectious Disease
Therapuetic Areas:Immunology / Infectious Diseases
Healthy:No
Age Range:21 - 45
Updated:4/2/2016
Start Date:March 2007
Contact:Fawaz Mzayek, MD, PhD
Email:fmzayek@tulane.edu
Phone:504-988-1062

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The purpose of this study is to test the safety of a 2100 mg dose of AQ-13, a new candidate
antimalarial active against drug-resistant P. falciparum infection, and to determine the
effect of a standard fatty meal on the absorption of the drug from the gut and its blood
levels.

This is a 2-stage, randomized crossover study of a 2100 mg AQ-13 dose in healthy volunteers.
Fourteen healthy volunteers will be randomized to receive the drug either on an empty
stomach or after a standard fatty meal under continuous monitoring in the hospital. After a
washout period of 8 weeks, the volunteers will be admitted to the hospital again to receive
the same dose of the drug after a fatty meal or on an empty stomach in reverse – so each
volunteer will receive AQ-13 with and without a fatty meal.

Study Population:

Healthy young men and women, 21-45 years of age who are taking no chronic medications with
the exception of birth control pills will be invited to participate in this food-effect
bioavailability study at the Tulane-LSU General Clinical Research Center in New Orleans.
Exclusion criteria include pregnancy, breast feeding, abnormal liver or kidney function
tests, anemia (Hb < 12 gm per dL), chronic medications other than birth control pills, and
an abnormal baseline ECG or Holter recording.

Randomization:

Allocation codes will be generated by the biostatistician in blocks, using computer
software, and will be sealed in numbered, opaque envelopes. Block sizes will be determined
at random and will not be known to the study personnel. The envelopes containing the
randomization codes will be hand-delivered to the study pharmacist and kept in the Research
Pharmacy, which is outside the GCRC.

Blinding:

The investigators and laboratory personnel performing the laboratory tests and comparing
those results, electrocardiograms and Holter recordings for AQ-13 doses will be blinded to
which AQ-13 doses were administered with or without a fatty meal. However, the volunteers
themselves and the nursing personnel in the GCRC will know which doses were administered
with and without a fatty meal. Therefore, this is a single-blinded study.

Informed Consent:

Informed consent will be obtained from each participant before screening. According to IRB
guidelines, the informed consent form will be revised at yearly intervals and whenever new
information on AQ-13 or its side effects becomes available.

In-patient Procedures:

On the evening of admission, pregnancy testing will be repeated and CK will be measured
before drug administration the following morning. The drug administration protocol will
follow the design outlined in the FDA “Guidance for Industry” for food-effect
bioavailability studies (1-2). The 2100 mg AQ-13 dose will be divided into three doses of
700 mg each to be administered once a day in the morning on an empty stomach with 240 ml
water after 10 hours fasting for the empty stomach arm. For the fatty meal arm, the AQ-13
dose on day 1 will be administered within 30 minutes of a standard fatty meal, prepared as
described in the FDA “Guidance” and administered with 240 ml water after 10 hours of
fasting. The fatty meal should be eaten within 30 minutes and the drug should be
administered 30 minutes after start of the fatty meal. For both arms, water will not be
allowed for 1 hour before or after the dose; and food will not be allowed for 4 hours after
the dose (2). A small needle with plastic tubing and a blood thinner will be placed in the
participant’s arm and kept in place with paper tape to draw blood samples. The participant
will then be monitored for heart rhythm, using a Holter monitor for four days beginning at
the time of the first dose, and will have an electrocardiogram taken 4 hours after each
dose. The purpose of the cardiac monitoring is to test whether the drug affects the QTc
interval or the heart rhythm. Three 24-hr urine samples will be collected starting at the
time of the first dose.

Outpatient follow up:

After the inpatient studies at the General Clinical Research Center (GCRC), participants
will be asked to return to the GCRC as outpatients twice per week for 4 weeks to give (5 ml)
of blood to follow the drug levels in their blood. At the 2 week follow up visit, an
electrocardiogram, Holter recording, blood testing for hematology and chemistry, and visual
exam will be done. At the 4 week follow up, an additional ECG and Holter recording will be
obtained.

In the second stage of the study, all in-patient and out-patient follow up procedures will
be the same as in the first stage, except that the study drug will be administered on an
empty stomach for volunteers who took the drug after a fatty meal in the first stage and
vice versa. At least an 8 week washout period must pass between participating in the two
stages of the study.

References:

1. http://www.fda.gov/oc/initiatives/hiv/hivguidance.html

2. http://www.fda.gov/cder/guidance/5194fnl.pdf

Inclusion Criteria:

- Healthy volunteers 21-45 years of age taking no chronic medications other than
birth-control pills

Exclusion Criteria:

- Pregnancy,

- Breast-feeding,

- Chronic disease
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