568 
Steady-state Pharmacokinetic Evaluation of Emtricitabine in Neonates Exposed to HIV in utero
M Robert Blum*1, D Ndiweni2, G Chittick1, N Adda1, D Kargl1, and D Josipovic3
1Gilead Sci, Durham, NC, US; 2Johannesburg Hosp, Parktown, South Africa; and 3Chris Hani Baragwanath Hosp, Univ of the Witwatersrand, Johannesburg, South Africa
Background: Emtricitabine (FTC)
is a potent once-daily nucleoside reverse transcriptase inhibitor (NRTI) approved
for the treatment of HIV infection in adults and children ³3
months in age in combination with other antiviral agents. Since FTC is primarily eliminated by renal
excretion, and because renal function matures during the first few months of
life, FTC pharmacokinetics was examined at steady-state following short-term
administration in HIV-exposed infants <3 months to determine an appropriate
dose for this age group that would provide drug exposure similar to that
achieved by regimens shown to be safe and efficacious in pediatric patients (6
mg/kg oral solution £240
mg once daily) and adult patients (200 mg capsules once daily).
Methods: Neonates born to women with confirmed HIV-1
infection, and who received 6 weeks of postnatal zidovudine prophylaxis for
perinatal HIV exposure, received 2 short courses of FTC (each 3 mg/kg once
daily for 4 days) as oral solution during the first 12 weeks of life. Confirmed
HIV-infected neonates were excluded from the study. The first FTC course was
administered during the first 28 days of life and the second administered as
long as 8 weeks later and staggered among neonates. Plasma pharmacokinetics was
assessed over 48 hours following the administration of the last dose of each
course.
Results: We enrolled 22 infants, and 20 completed
both pharmacokinetic assessments. One infant received 1 dose of FTC and was
lost to follow-up, and 1 discontinued due to anemia unrelated to FTC.
(Pharmacokinetic parameters are summarized in the table.) FTC area under the
curve (AUC) decreased with increasing age over the first 3 months of life which
correlated with an increase in apparent total body clearance (CL/F). However, the AUC in
neonates receiving 3 mg/kg FTC QD during the first 3 months of life was in the
range of pediatric patients ³3 months to 17 years receiving 6 mg/kg oral solution to
as much as 240 mg once daily as or 200-mg capsules once daily.
.
|
Age range
(days)
|
N
|
Age (days)
(mean, range)
|
Cmin
(mg/mL)
|
Cmax
(mg/mL)
|
AUC(0-24)
(h*mg/mL)
|
|
0-21
|
18
|
13, 5-21
|
0.126 (41%)
|
1.601 (28%)
|
13.44 (28%)
|
|
22-42
|
10
|
33, 23-42
|
0.065 (42%)
|
1.416 (23%)
|
8.55 (15%)
|
|
43-90
|
12
|
55, 43-81
|
0.092 (89%)
|
1.639 (52%)
|
9.27 (48%)
|
Conclusions: Results indicate that 3 mg/kg FTC once daily
in neonates <3 months old produces plasma levels similar to those shown to
be safe and efficacious in HIV-infected adults and pediatric patients ³3
months.
|
