The importance of objective assessment of prenatal exposure to alcohol through measurement of biomarkers in meconium

Oscar Garcia-Algar1,2,3*, Luigi Tarani4, Francesco Paolo Busardò5, Simona Pichini3,5, Emilia Marchei5

1. Neonatology Unit, Hospital Clinic-Maternitat, ICGON, BCNatal, Barcelona Centre for Maternal Foetal and Neonatal Medicine, Hospital Sant Joan de Déu and Hospital Clínic, Barcelona, Spain
2. Department de Cirurgia i Especialitats Mèdico-Quirúrgiques, Universitat de Barcelona, Barcelona, Spain
3. European Foetal Alcohol Spectrum Disorders Alliance (EUFASD), Stockholm, Sweden
4. Department of Pediatrics, Sapienza University of Rome, Rome, Italy
5. National Centre on Addiction and Doping, Istituto Superiore di Sanità, Rome, Italy

Dear Editor,
We read with attention the paper by Henderson et al. concerning comparison of confidential postnatal maternal interview and measurement of alcohol biomarkers in meconium (1). We would like to draw attention on their conclusion: “Fatty acid ethyl esters (FAEEs) and Ethylglucuronide (EtG) measured in meconium have low sensitivity and specificity for self-reported alcohol consumption after 20 weeks’ gestation in an unselected Scottish population and measurement of these alcohol biomarkers in meconium cannot currently be recommended for the identification of newborns at risk of Fetal Alcohol Spectrum Disorders (FASD).”
It has been more than 20 years since meconium analysis has been used to objectively assess prenatal exposure to alcohol (2-12). Several studies have been reported in the literature regarding the use of this biological matrix for the determination of alcohol biomarkers such as FAEEs and EtG and to be used in epidemiological studies verifying alcohol drinking during pregnancy and consequentially prenatal exposure. These studies not only assessed prenatal exposure to gestational alcohol, but also demonstrated underreporting and misreporting of pregnant women concerning gestational drinking habits. To this concern, the majority of studies from our group showed no relationship between biomarker measurement and maternal self-reported declarations, at least in the Mediterranean area where investigations were carried out (13-26).
In this paper, an anonymised, observational population-based study questionnaire on alcohol consumption in pregnancy was matched with measurement of alcohol biomarkers in meconium in a cohort of mother/infant dyads from Glasgow, UK. Of 828 women enrolled in the study, 384 (46.4%) reported alcohol consumption at any time in pregnancy and for 114 (13.6%) this was after 20 weeks’ gestation. When meconium was positive for FAEEs (≥ 600 ng/g) and for EtG (≥ 30 ng/g), 14.5% and 10.7% of mothers reported alcohol consumption after 20 weeks’ gestation, respectively. Similar percentages were observed when meconium was negative for FAEEs (13.0%, ≤ 600 ng/g) and for EtG (14.0%, ≤ 30 ng/g). The authors concluded that FAEE and EtG measured in meconium showed low sensitivity and specificity for self-reported alcohol consumption after 20 weeks of gestation.
Based on the determination of biomarkers, FAEEs were identified in all meconium samples analyzed and 39.6% had a concentration greater than or equal to 600 ng/mg (cut-off used to discriminate positive from negative samples). As far as EtG is concerned, 14.5% of the analyzed meconium samples had a concentration greater than or equal to 30 ng/g (cut-off used to discriminate positive samples from negative ones). In summary, if the biomarkers are also considered, the percentage of potentially exposed children increases, therefore it is possible to intervene also on those who, from the questionnaire, would have appeared to be newborns of non-drinking women and therefore excluded from any follow-up.
Early diagnosis of foetal alcohol spectrum disorders is of crucial importance to perform a targeted follow up of newborns prenatally exposed to alcohol and avoid secondary neurodevelopmental disabilities. A positive meconium testing for the presence of EtG or FAEEs is an objective first element to assess prenatal exposure to alcohol, whereas a maternal self-reported admission of gestational consumption of alcohol is not.
The only use of self-reported questionnaires to disclose alcohol drinking during pregnancy can’t be recommended. In addition, we do not have to forget transplacental passage of this teratogen, which differs in each mother-infant dyad and can either allow or prevent alcohol migration from the mother to the foetus.
In conclusion, we reiterate the importance of objective assessment of gestational drinking and consequent foetal exposure by measuring alcohol metabolites not only in neonatal meconium, but also in maternal hair to associate the results of these measurements to a potential brief intervention on the risks of gestational alcohol to mothers and neurodevelopmental targeted follow up for exposed newborns (18, 26).

References
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