Benefits of a Single Dose of Betamethasone in Imminent Preterm Labour

Natalia Saldaña-García; María Gracia Espinosa-Fernández; Celia Gómez-Robles; Antonio Javier Postigo-Jiménez; Nicholas Bello; Francisca Rius-Díaz; Tomás Sánchez-Tamayo

doi:10.3390/jcm11010020

Benefits of a Single Dose of Betamethasone in Imminent Preterm Labour

J Clin Med. 2021 Dec 21;11(1):20. doi: 10.3390/jcm11010020.

Authors

Natalia Saldaña-García^{1

2}, María Gracia Espinosa-Fernández¹, Celia Gómez-Robles¹, Antonio Javier Postigo-Jiménez¹, Nicholas Bello¹, Francisca Rius-Díaz³, Tomás Sánchez-Tamayo^{1

4}

Affiliations

¹ Department of Neonatology, Regional University Hospital of Malaga, 29010 Malaga, Spain.
² School of Medicine, Malaga University, 29071 Malaga, Spain.
³ Department of Preventive Medicine and Public Health, Biostatistics, School of Medicine, Malaga University, 29071 Malaga, Spain.
⁴ Pediatrics Division, Malaga University, 29071 Malaga, Spain.

Abstract

Background: A complete course of prenatal corticosteroids reduces the possibility of morbimortality and neonatal respiratory distress syndrome (RDS). Occasionally, it is not possible to initiate or complete the maturation regimen, and the preterm neonate is born in a non-tertiary hospital. This study aimed to assess the effects of a single dose of betamethasone within 3 h before delivery on serious outcomes (mortality and serious sequelae) and RDS in preterm neonates born in tertiary vs. non-tertiary hospitals.

Materials and methods: Preterm neonates who were <35 weeks and ≤1500 g, treated during a period of five years in a level IIIC NICU, were included in this retrospective cohort study. Participants were divided into groups as follows: NM, non-matured; PM, partial maturation (one dose of betamethasone up to 3 h antepartum). They were further divided based on their place of birth (NICU-IIIC vs. non-tertiary hospitals). The morbimortality rates and the severity of neonatal RDS were evaluated.

Results: A total of 76 preterm neonates were included. A decrease in serious outcomes was found in the PM group in comparison to the NM group (OR = 0.2; 95%CI (0.07-0.9)), as well as reduced need for mechanical ventilation (54% vs. 68%). The mean time between maternal admission and birth was similar in both cohorts. The mean time from the administration of betamethasone to delivery was 1 h in the PM cohort. With regard to births in NICU-IIIC, the PM group performed better in terms of serious outcomes (32% vs. 45%) and the duration of mechanical ventilation (117.75 vs. 132.18 h) compared to the NM group. In neonates born in non-tertiary hospitals with PM in comparison to the NM group, a trend towards a reduced serious outcome (28.5% vs. 62.2%) and a decreased need for mechanical ventilation (OR = 0.09; 95%CI (0.01-0.8)) and maximum FiO₂ (p = 0.01) was observed.

Conclusions: A single dose of betamethasone up to 3 h antepartum may reduce the rate of serious outcomes and the severity of neonatal RDS, especially in non-tertiary hospitals.

Keywords: antenatal corticosteroids; betamethasone; mortality; preterm infant; respiratory distress syndrome.