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Pharmacokinetics of Once-daily Fosamprenavir 1400 mg plus Atazanavir 400 mg without Ritonavir in HIV-negative Subjects
Patrick Clay*1, P Anderson2, P Smith3, D Lein4, and A Glaros1
1Kansas City Univ of Med and Biosci, MO, US; 2Univ of Colorado Hlth Sci Sch of Pharm, Denver, US; 3Univ of Buffalo Sch of Pharm, NY, US; and 4Kansas City Free Hlth Clin, MO, US
Background: Atazanavir (ATV) + fosamprenavir
(FPV) is a potentially useful double-protease inhibitor (PI) combination with
components that may offer a mutually beneficial resistance profile. As a formal
drug interaction study of ATV+FPV has not been conducted, we evaluated the
pharmacokinetics and tolerability of ATV and FPV when administered alone and in
combination without ritonavir (RTV) in HIV persons.
Methods: COL100683 was a
prospective, randomized, open-label, 3-way crossover study with 3-week washout
periods, in which 21 HIV adults received, in random order: FPV 1400
mg, ATV 400 mg, or both by mount once-daily for 14 days. At the end of each
period (day 14), a 24-hour pharmacokinetic study (10 samples) was completed,
including standardized diets. Drug levels (FPV reported as APV) were assayed by
a validated high-performance liquid chromatography (HPLC) method. Pharmacokinetic
parameters were determined by standard noncompartmental
methods and compared by paired t-test
on log-transformed data. Bioequivalence was assessed by geometric mean ratios
(GMR). Adverse event data were analyzed using student’s t-test.
Results: Of the total, 21
subjects completed the study (11 men, 48% non-white) with a mean age of 31.7
(9.5 SD) years. Clinical adverse events were >99% (123 of 124) grade 1.
Laboratory adverse events were not different between either agent (p = 0.3), single and dual regimens (p = 0.47) or baseline and safety
follow-up (p = 0.16). Only 1 serious adverse
events unrelated to study drugs (grade 3 acute pancreatitis) occurred. All grade 2 to 4 laboratory adverse
events (41 of 148) represented transient increases in direct or indirect bilirubin and resolved before the next period initiation or
safety follow-up visit. Pharmacokinetic parameters are reported below. No
differences occurred with respect to periods or sequences.
|
|
ATV
|
APV
|
|
|
ATV alone
|
ATV + FPV
|
GMR
(90% CI)
|
% change
|
FPV alone
|
FPV + ATV
|
GMR
(90% CI)
|
% change
|
|
AUC
mg.h/mL
|
17.9 (65)
|
11.9 (54)
|
0.67
(0.51 - 0.88)
|
¯ 33%*
|
21.7 (44)
|
38.7 (27)
|
1.78
(1.47 - 2.12)
|
78%*
|
|
Cmax
mg/mL
|
2.6 (59)
|
1.8 (54)
|
0.70
(0.53 - 0.93)
|
¯ 30%*
|
4.8 (55)
|
6.5 (34)
|
1.36
(1.09 - 1.72)
|
36%*
|
|
C24
mg/mL
|
0.14 (135)
|
0.06 (104)
|
0.43
(0.24 - 0.56)
|
¯ 57%*
|
0.06 (89)
|
0.23 (178)
|
3.83
(2.43 - 6.76)
|
283%*
|
*p <0.05;
data presented as geometric mean (CV%)
Conclusions: ATV+FPV was well tolerated. ATV significantly enhanced exposure of unboosted, once-daily FPV. ATV exposure was reduced when
co-administered with FPV. The clinical relevance of these findings will remain
unknown until controlled efficacy studies are completed.
|
