TY - JOUR T1 - Potentially harmful excipients in neonatal medicines: a pan-European observational study JF - Archives of Disease in Childhood JO - Arch Dis Child SP - 694 LP - 699 DO - 10.1136/archdischild-2014-307793 VL - 100 IS - 7 AU - Georgi Nellis AU - Tuuli Metsvaht AU - Heili Varendi AU - Karolin Toompere AU - Jana Lass AU - Inge Mesek AU - Anthony J Nunn AU - Mark A Turner AU - Irja Lutsar Y1 - 2015/07/01 UR - http://adc.bmj.com/content/100/7/694.abstract N2 - Objectives We aimed to describe administration of eight potentially harmful excipients of interest (EOI)—parabens, polysorbate 80, propylene glycol, benzoates, saccharin sodium, sorbitol, ethanol and benzalkonium chloride—to hospitalised neonates in Europe and to identify risk factors for exposure.Methods All medicines administered to neonates during 1 day with individual prescription and demographic data were registered in a web-based point prevalence study. Excipients were identified from the Summaries of Product Characteristics. Determinants of EOI administration (geographical region, gestational age (GA), active pharmaceutical ingredient, unit level and hospital teaching status) were identified using multivariable logistical regression analysis.Results Overall 89 neonatal units from 21 countries participated. Altogether 2095 prescriptions for 530 products administered to 726 neonates were recorded. EOI were found in 638 (31%) prescriptions and were administered to 456 (63%) neonates through a relatively small number of products (n=142; 27%). Parabens, found in 71 (13%) products administered to 313 (43%) neonates, were used most frequently. EOI administration varied by geographical region, GA and route of administration. Geographical region remained a significant determinant of the use of parabens, polysorbate 80, propylene glycol and saccharin sodium after adjustment for the potential covariates including anatomical therapeutic chemical class of the active ingredient.Conclusions European neonates receive a number of potentially harmful pharmaceutical excipients. Regional differences in EOI administration suggest that EOI-free products are available and provide the potential for substitution to avoid side effects of some excipients. ER -