Invasive Aspergillosis Clinical Trial
Official title:
F901318 - A Phase I, Double-Blind, Placebo Controlled, Multiple Ascending Oral Dose Safety, Tolerability and Pharmacokinetic Study in Healthy Male and Female Subjects
Double blind, placebo controlled, ascending multiple (10) oral dose, sequential group study.
Twenty-four subjects will complete the study in 3 cohorts (Groups A to C), each group
consisting of 8 subjects. Each cohort will consist of 4 male and 4 female subjects. Each
subject will be dosed for 10 days and will be on study for approximately 7 weeks. Each
subject will participate in one treatment cohort only, residing at the Clinical Research
Unit (CRU) from Day -1 (the day before dosing) to Day 15 (120 hours post the last dose). The
dose will range between 2 and 10 mg/kg daily, given as either a single daily dose or as two
doses divided over the 24-hour dosing period.
All subjects will return for a post-study visit 8 to 10 days after the last dose of study
medication.
Cohorts will be dosed at least at 3 weekly intervals. There will be a review of the safety
and pharmacokinetic data of each cohort prior to each dose escalation.
Male and female healthy subjects conforming to the selection criteria will be invited to
take part in the study.
Screening visit (Visit 1) After giving fully informed, written consent, subjects will attend
the clinic.
Subjects will undergo screening within 28 days prior to the first dose administration. Prior
to the screening visit, subjects will:
- Refrain from vigorous exercise for 7 days
- Abstain from alcohol for 48 hours
- Subjects will sign the consent form in the presence of a CRU physician prior to any
screening procedures being performed. The information recorded for all subjects,
regardless of their suitability for the study, will be retained and archived.
The following information and procedures will be recorded and performed as part of the
screening assessments:
- Medical history
- Ethnic origin, sex, age, height, weight, and BMI
- Vital signs: supine blood pressure, supine pulse rate, and oral body temperature
- Resting 12 lead ECG
- Physical examination
- Urine drugs of abuse screen, cotinine and alcohol breath test
- Pregnancy test, which must be negative
- Fasting clinical laboratory and serology investigations
- All females will be asked to give the approximate date of the last menstrual period.
- Ophthalmological assessments (Performed at a second screening visit in subjects who
have been shown at the first screening visit to meet eligibility criteria for the
study)
Up to 28 days after screening, subjects will attend the clinic. Subjects will be admitted to
the research unit at approximately 09:00 hours in the morning the day before dosing (Day
-1). Urine will be subjected to a screen for drugs of abuse and detection of any of these
substances which will disqualify the subject from the study. A physical examination, check
of inclusion/exclusion criteria, clinical laboratory evaluations, pregnancy test where
relevant and which must be negative, oral temperature and body weight will be performed.
Subjects will be asked whether they have experienced any adverse events or taken any
concomitant medication since their previous visit. Supper will be served starting at
approximately 19.30 hours and a snack at approximately 21.00 hours after which they will
fast overnight and until 4 hours post dose. Water will be allowed ad libitum throughout.
On Day 1, the total first urine void of the morning for each subject will be collected into
a polyethylene container and, from this, a sample will be taken for urinalysis and pre-dose
/ baseline F901318 concentration. Within one hour before dosing commences ( 1 hour), blood
will be drawn for laboratory safety assessments (haematology and clinical chemistry), and
pre-dose baseline F901318 and metabolites concentration. Supine and standing blood pressure
and pulse rate in duplicate, body temperature and a 12-lead ECG will be recorded. The
subjects will also be connected to continuous ECG recording from -1 hour) until at least 12
hours after the start of dosing.
Subjects will be asked whether they have experienced any adverse events overnight. Any
concomitant medications will be recorded.
Subjects will then be dosed. This will be an oral suspension washed down with 250 mL of
phosphate buffer. Subjects will be dosed with regular intervals between each subject.
After dosing, the following measurements and observations will be obtained:
- Blood samples for analysis of F901318 plasma concentration will be drawn at 15min, 30
min, 45min, 1, 1.5, 2, 3, 4, 5, 6, 7, 8, 10, 12 and 16 hours after dosing on Day 1.
- On Days 2 to 9, pharmacokinetic blood samples will be drawn within 15 minutes prior to
dosing and 2 and 4 hours later.
- On Day 10, blood samples for pharmacokinetic analysis will be drawn within 15 minutes
of the commencement of dosing and 15min, 30 min, 45min,1, 1.5, 2, 3, 4, 5, 6, 7, 8, 10,
12, 24, 36, 48, 72, 96 and 120 hours following dosing.
- Pharmacokinetic blood samples will be analysed and reviewed before each dose
escalation. After the first dose level administration, the dose level and the timing of
each blood sample may be adjusted for the subsequent dose escalation. The basis for
this decision will depend upon the pharmacokinetic profiles obtained from the preceding
group of subjects. All changes will be documented in a file note. The number of samples
or volume of blood drawn must not be increased without prior approval of the relevant
ethics committee.
- If it appears that Cmax may exceed the stopping criteria, the daily dose for that
cohort will be divided into to two halves given 6-12 hours apart with the exception of
Day 10 on which a single morning half dose will be given. The changes will be made on
the basis of pharmacokinetic predictions using data obtained from previous cohorts. In
that case, blood and urine sampling times will be adjusted accordingly and documented
in a note to file. The number of blood samples drawn for pharmacokinetics will not
exceed 68 without approval of the relevant ethics committee.
- Blood samples will be drawn for metabolite measurements 4 and 8 hours after the morning
dose on Day 1 and within 15 minutes prior to and 4 and 8 hours after the dose on Day
10.
- Blood will be collected for safety measurements (haematology and clinical chemistry)
and a urine sample will be obtained for urinalysis on Days 2, 3, 4, 5, 6, 7, 8 and 9 in
the 15 minutes prior to the morning dose and 24, 48 and 72 hours after the dose on Day
10.
- Complete urine collections for analysis of F901318 urine concentration will be made for
the following intervals in relation to dosing: 0-4, 4-8, 8-12, 12-24 hours on Day 1 and
0-4, 4-8, 8-12, 12-16, 16-24, 24-48, 48-72, 72-96 and 96-120 hours after the dose on
Day 10.
- Supine and standing pulse rate and blood pressure and body temperature (vital signs)
will be recorded 30, 60 and 120 minutes, 4, 8 and 12 hours after dosing on Day 1, prior
to (within 30 minutes) dosing on Days 2 - 10 and 4 hours after dosing on Days 2 - 10.
- Twelve-lead ECGs will be obtained 1, 4, 8, and 12 hours after dosing on Day 1 and
within 30 minutes before and 4 hours after dosing on Days 3, 6 and 10.
- The continuous ECG recording will cease 12 hours after dosing on Day 1. It may be
extended to 24 hours at the discretion of the PI. A further continuous recording will
be obtained from one hour prior to and for 12 hours after the dose on Day 10. It also
may be extended to 24 hours at the discretion of the PI.
- Spontaneously reported adverse events and concomitant medications will be noted
throughout.
- Lunch will be served approximately 4 hours after each morning dose but after all the 4
hour observations and blood sampling have been completed and a main meal will be served
approximately 8 hours and a snack approximately 11.5 hours after each morning dose.
- Ophthalmological evaluation will be conducted 24 hours post Day 10 dosing (+/- 4 hours)
- A pregnancy test will be performed on Day 15 in females of child bearing potential.
Subjects may leave the Research Unit on Day 15, unless they have experienced adverse events
that, in the opinion of the Investigator, warrant further observation and/or treatment.
All subjects will be followed up 8-10 days after the last dose of study drug with a
post-study visit.
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