Abstrakt
Aim: Phenobarbital (PB) pharmacokinetics (PK) in asphyxiated newborns show large variability, not only explained by hypothermia (HT). We evaluated potential relevant covariates of PK of PB in newborns treated with or without HT for hypoxic-ischemic encephalopathy (HIE).
Methods: Clearance (CL), distribution volume (Vd) and elimination half-life (t(1/2)) were calculated using one-compartment analysis. Covariates were clinical characteristics (weight, gestational age, hepatic, renal, and circulatory status), comedication and HIE severity [time to reach normal aEEG pattern (T(norm)aEEG), dichotomous, within 24 h] and asphyxia severity [severe aspyhxia = pH = 24 h in 12/26 (group(2-HT))].
Severe asphyxia was present in 26/40 [5/14 non-HT, 11/14 and 10/12 in both HT groups]. PB-CL, Vd and t(1/2) were similar between the non-HT and HT group.
However, within the HT group, PB-CL was significantly different between group(1-HT) and group(2-HT) (p = .043). ANOVA showed that HT (p = .034) and severity of asphyxia (p = .038) reduced PB-CL (-50%).
Conclusion: The interaction of severity of asphyxia and HT is associated with a clinical relevant reduced PB-CL, suggesting the potential relevance of disease characteristics beyond HT itself.