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The most recent version of this article was published on 1 November 2008

Arch. Dis. Child. Fetal Neonatal Ed.. Published Online First: 1 May 2008. doi:10.1136/adc.2007.128470
Copyright © 2008 BMJ Publishing Group Ltd & Royal College of Paediatrics and Child Health
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Original articles

Antenatal glucocorticoid treatment is not associated with long-term metabolic risks in individuals born before 32 weeks of gestation

Martijn JJ Finken 1*, Mandy G Keijzer-Veen 2, Friedo W Dekker 1, Marijke Frolich 1, Frans J Walther 1, Johannes A Romijn 1, Bert J van der Heijden 2 and Jan M Wit 1

1 Leiden University Medical Center, Netherlands
2 Erasmus MC-Sophia Children's Hospital, Netherlands

* To whom correspondence should be addressed. E-mail: m.j.j.finken{at}lumc.nl.

Accepted 25 March 2008


*   Abstract

Background: A single course of maternal glucocorticoid treatment is effective in reducing neonatal mortality after preterm birth. However, in animals, maternal glucocorticoid treatment is associated with lifelong hyperglycaemia and hypertension, and impaired nephrogenesis in offspring. Findings from studies in humans on this topic are highly contradictory due to a number of methodologic flaws and renal function after glucocorticoid exposure has never been assessed.

Objectives: To assess in individuals born <32 gestational weeks whether antenatal glucocorticoid treatment for preterm birth is associated with long-term metabolic risks, including renal function, in adulthood.

Design: Birth cohort study.

Setting: Multicenter study.

Patients: 412 Nineteen-year-olds born <32 gestational weeks from the Project On Preterm and Small-for-gestational-age infants (POPS) cohort.

Interventions:Maternal betamethasone 12 mg administered twice with a 24-h interval.

Main outcome measures: Body composition, insulin resistance, the serum lipid profile, blood pressure and estimated renal function

Results: We did not find any long-term adverse effects of antenatal betamethasone, with the exception of an effect on glomerular filtration rate (GFR). In 19-year-old survivors, GFR was lower after betamethasone: -5.2 (95% CI: -8.9 to -1.4) ml/min per 1.73 m2.

Conclusions: The reduction in neonatal mortality associated with a single course of maternal betamethasone is not accompanied by long-term metabolic risks in survivors of preterm birth. The only adverse effect found was lower GFR. Although this difference was not clinically relevant at 19 years, it might predict an increased risk of chronic renal failure in prematurely born individuals who were exposed antenatally to betamethasone.




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