Optimization of the betamethasone and dexamethasone dosing regimen during pregnancy: a combined placenta perfusion and pregnancy physiologically based pharmacokinetic modeling approach - 12/06/24

Doi : 10.1016/j.ajog.2024.05.012

Joyce E.M. Van Der Heijden, MSc ^a,^⁎ , Hedwig Van Hove, MSc ^a, Niki M. Van Elst, BSc ^a, Petra Van Den Broek, BSc ^a, Joris Van Drongelen, MD, PhD ^b, Hubertina C.J. Scheepers, MD, PhD ^c, Saskia N. De Wildt, MD, PhD ^a,^d, Rick Greupink, PharmD, PhD ^a
^a Division of Pharmacology and Toxicology, Department of Pharmacy, Radboud University Medical Center, Nijmegen, The Netherlands
^b Department of Obstetrics and Gynecology, Radboud University Medical Center, Nijmegen, The Netherlands
^c Department of Obstetrics and Gynecology, GROW School for Oncology and Reproduction, Maastricht University Medical Centre, Maastricht, The Netherlands
^d Department of Pediatric and Neonatal Intensive Care, Erasmus MC-Sophia Children's Hospital, Rotterdam, The Netherlands

^∗Corresponding author: Joyce E.M. van der Heijden, MSc.

Sous presse. Épreuves corrigées par l'auteur. Disponible en ligne depuis le Wednesday 12 June 2024

Abstract

Background

Antenatal betamethasone and dexamethasone are prescribed to women who are at high risk of premature birth to prevent neonatal respiratory distress syndrome (RDS). The current treatment regimens, effective to prevent neonatal RDS, may be suboptimal. Recently, concerns have been raised regarding possible adverse long-term neurological outcomes due to high fetal drug exposures. Data from nonhuman primates and sheep suggest maintaining a fetal plasma concentration above 1 ng/mL for 48 hours to retain efficacy, while avoiding undesirable high fetal plasma levels.

Objective

We aimed to re-evaluate the current betamethasone and dexamethasone dosing strategies to assess estimated fetal exposure and provide new dosing proposals that meet the efficacy target but avoid excessive peak exposures.

Study design

A pregnancy physiologically based pharmacokinetic (PBPK) model was used to predict fetal drug exposures. To allow prediction of the extent of betamethasone and dexamethasone exposure in the fetus, placenta perfusion experiments were conducted to determine placental transfer. Placental transfer rates were integrated in the PBPK model to predict fetal exposure and model performance was verified using published maternal and fetal pharmacokinetic data. The verified pregnancy PBPK models were then used to simulate alternative dosing regimens to establish a model-informed dose.

Results

Ex vivo data showed that both drugs extensively cross the placenta. For betamethasone 15.7±1.7% and for dexamethasone 14.4±1.5%, the initial maternal perfusate concentration reached the fetal circulations at the end of the 3-hour perfusion period. Pregnancy PBPK models that include these ex vivo-derived placental transfer rates accurately predicted maternal and fetal exposures resulting from current dosing regimens. The dose simulations suggest that for betamethasone intramuscular, a dose reduction from 2 dosages 11.4 mg, 24 hours apart, to 4 dosages 1.425 mg, 12 hours apart would avoid excessive peak exposures and still meet the fetal response threshold. For dexamethasone, the dose may be reduced from 4 times 6 mg every 12 hours to 8 times 1.5 mg every 6 hours.

Conclusion

A combined placenta perfusion and pregnancy PBPK modeling approach adequately predicted both maternal and fetal drug exposures of 2 antenatal corticosteroids (ACSs). Strikingly, our PBPK simulations suggest that drug doses might be reduced drastically to still meet earlier proposed efficacy targets and minimize peak exposures. We propose the provided model-informed dosing regimens are used to support further discussion on an updated ACS scheme and design of clinical trials to confirm the effectiveness and safety of lower doses.

Le texte complet de cet article est disponible en PDF.

Video

(17.96 Mo)

Le texte complet de cet article est disponible en PDF.

Key words : antenatal corticosteroids, fetal exposure/fetus, model-informed dose, physiologically-based pharmacokinetic model, pregnancy

Plan

Introduction

Methods

Ex vivo human placental perfusion experiments

Pregnancy PBPK modeling

Results

Ex vivo human placental perfusion experiments and PBMP modeling

Pregnancy PBPK modeling

Comment

Principal findings

Results in the context of what is known

Clinical implications

Research implications

Strengths and limitations

Conclusions

	J.E.M.V.D.H. and H.V.H. contributed equally to this work.
	The authors report no conflict of interest.
	This research was funded by the Bill & Melinda Gates Foundation (INV-023795). The findings and conclusions contained within are those of the authors and do not necessarily reflect positions or policies of the Bill & Melinda Gates Foundation.
	Ethics approval: The regional institutional medical ethical committee provided a waiver for formal approval based on the Dutch Law for Human research (CMO Arnhem/Nijmegen File 2014-1397 and 2022-13523) to collect human placentas and perform placenta perfusion experiments.
	Presented orally and as poster at the 124th annual meeting of the American Society for Clinical Pharmacology & Therapeutics (ASCPT), Atlanta, GA, Mar. 22–24, 2023.
	Cite this article as: Van Der Heijden JEM, Van Hove H, Van Elst NM, et al. Optimization of the betamethasone and dexamethasone dosing regimen during pregnancy: a combined placenta perfusion and pregnancy physiologically based pharmacokinetic modeling approach. Am J Obstet Gynecol 2024;XXX:XX–XX.