A RANDOMIZED DOUBLE-BLIND TRIAL OF THE ADDITION OF LAMIVUDINE OR MATCHING PLACEBO TO CURRENT NUCLEOSIDE ANALOG REVERSE-TRANSCRIPTASE INHIBITOR THERAPY IN HIV-INFECTED CHILDREN - THE PENTA-4 TRIAL
Jp. Aboulker et al., A RANDOMIZED DOUBLE-BLIND TRIAL OF THE ADDITION OF LAMIVUDINE OR MATCHING PLACEBO TO CURRENT NUCLEOSIDE ANALOG REVERSE-TRANSCRIPTASE INHIBITOR THERAPY IN HIV-INFECTED CHILDREN - THE PENTA-4 TRIAL, AIDS, 12(14), 1998, pp. 151-160
Objectives: To evaluate the toxicity, tolerability and effect on labor
atory markers of adding lamivudine (3TC) to nucleoside analogue revers
e transcriptase inhibitors (NRTI) in children with HIV-1 infection. De
sign: Randomized double-blind trial. Methods: HIV-l-infected children
on stable NRTI therapy were randomized to receive 3TC syrup or tablets
(4 mg/kg twice daily) or matching placebo in addition to existing the
rapy. Endpoints were serious adverse events, and changes in CD4 cell c
ount and plasma HIV-1 RNA. Analyses were on an intention-to-treat basi
s. Results: A total of 162 (81 on 3TC, 81 on placebo) children [median
age, 6.5 years; interquartile range (IQR), 4.1-10.1 years] were inclu
ded. At randomization, 52 were receiving zidovudine (ZDV), 39 didanosi
ne (ddl), 54 ZDV-ddl and 17 ZDV-zalcitabine (ddC); 32 (20%) had AIDS;
median CD4 cell count was 328 x 10(6)/l (IQR, 127-696 x 10(6)/l), and
median HIV-1 RNA was 4.9 log(10) copies/ml (IQR, 4.3-5.4 log(10) copie
s/ml). Median follow-up was 40 weeks (IQR, 29-49 weeks) and 76% of fol
low-up was on blinded therapy for both 3TC and placebo groups. There w
ere 11 serious adverse events in the blinded phase [two clinical (both
placebo) and nine laboratory (five 3TC, four placebo)], five (two 3TC
,three placebo) resulting in stopping trial drug. At 24 weeks, the CD4
cell count was greater in the 3TC group by a median of 47 x 10(6)/l a
nd HIV-1 RNA was lower by 0.30 log(10) copies/ml (P = 0.03 and 0.002,
respectively, versus the placebo group). The difference in reduction i
n HIV-1 RNA up to 24 weeks, as measured by area under the curve minus
baseline, between 3TC and placebo groups was 0.38 log(10) copies/ml (9
5% confidence interval, 0.12-0.65) greater in children taking ZDV-cont
aining regimens at baseline, compared with those on ddl monotherapy (P
= 0.005), after adjusting for other factors at baseline. Thirteen chi
ldren developed new AIDS events (six on 3TC, four on placebo) of whom
three died (all placebo). Conclusions: The addition of 3TC to current
NRTI therapy in children was safe and well-tolerated. There was eviden
ce that treatment changes in HIV-1 RNA viral load were greater in chil
dren taking regimens that included ZDV. (C) 1998 Lippincott Williams &
Wilkins.