This study is a randomized, investigator blind, subject blind, sponsor-open, placebo controlled, multiple dose escalating, sequential, parallel cohort study of PF-04287881. Subjects will undergo screening procedures within 28 days prior to dosing. At least 1 day after the Screening visit, eligible subjects who meet the entry criteria will be admitted to the Clinical Research Unit (CRU) and confined in the unit until discharge on Day 15. Approximately 60 healthy volunteers (20 volunteers of Japanese origin for Cohorts 5 and 6), 18 to 55 years of age, males and females (women of non childbearing potential only) will be enrolled and randomized in a 4:1 ratio to treatment with either PF-04287881 or placebo within each cohort. Each cohort will have a 10 day dosing period and each will consist of 10 subjects (8 active and 2 placebo). In each cohort, each subject will receive a single daily oral dose of either placebo or PF-04287881 under fasted state for 10 days.
Following a Serious Adverse Event (potential Hy's Law case), a risk-benefit assessment review of all preliminary safety data, and a review by Pfizer's internal hepatic injury advisory panel, it was concluded that PF-04287881 had an unacceptable therapeutic window. The FDA was notified of our intention to discontinue development as of 09April2010.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Masking
DOUBLE
Enrollment
39
500 mg once daily for 10 days
To match 500 mg dose once daily for 10 days
750 mg once daily for 10 days
To match 750 mg dose once daily for 10 days
1100 mg once daily for 10 days
To match 1100 mg dose once daily for 10 days
Optional cohort with dose not greater than 1100 mg
Optional cohort to match dose not greater than 1100 mg
750 mg dose once daily for 10 days
To match 750 mg dose once daily for 10 days
1100 mg dose once daily for 10 days
To match 1100 mg dose once daily for 10 days
Pfizer Investigational Site
New Haven, Connecticut, United States
Standard safety assessments including assessment of AEs, laboratory tests, ECGs, and vital signs.
Time frame: Screening, Dosing days 1-10, through follow-up
The primary pharmacokinetic endpoints to be evaluated for PF-04287881 include Cmax, Tmax, and AUC(0-24) on Day 1 and Day 10.
Time frame: Day 1 and 10
Secondary parameters include AUCinf and t1/2 as data permit, apparent oral clearance (CL/F), apparent volume of distribution (Vz/F) and accumulation ratio (Rac).
Time frame: Days 1, 5 and 10
Urine concentrations of PF 04287881 in Cohorts 2 and 5 will be used to determine total amount excreted (Ae), %Ae relative to dose given and renal clearance (CLR).
Time frame: Day 10
Concentrations of PF 04287881 will be measured in white blood cell (WBC) polymorphonuclear cells (PMNs) in Cohorts 2 and 5 to determine total exposure in WBC.
Time frame: Days 1 and 10
Plasma samples from Cohort 2 will be used for exploratory investigation of circulating metabolites.
Time frame: Days 1 and 10
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