Prospective Identification of Predictors of Neonatal Respiratory Distress for Newborns With Prenatally Diagnosed Congenital Lung Malformations : A Population-based, Nationally Representative Study

Brief Summary

Detailed Description

The main objective of the study is to develop a prognostic model for estimating the risk of neonatal respiratory distress in children with prenatally diagnosed congenital pulmonary malformation. The study will be offered to all pregnant women referred to a Center for Prenatal Diagnosis (CPD), due to the identification of a congenital lung malformations in the fetus. This study does not induce any changes in clinical and therapeutic monitoring proposed by the team in charge of the mother. At inclusion, and at each prenatal evaluation, prenatal parameters are entered in an e-CRF. In an effort to minimize any potential intra- and interoperator variability in malformation measurements over time, this study includes a standardized and centralized evaluation of ultrasound and MRI (if available) acquisitions of volume measurements. When the place of delivery is determined, a contact is made before birth with the teams (maternity, neonatology, intensive care unit), so that neonatal data are also collected prospectively. A phone call to the family is planned for the end of the first postnatal month, to identify any respiratory event that would have occurred between returning home after childbirth and the first month. The routine follow-up of these children is then ensured in accordance with current national recommendations, in conjunction with the reference centers for rare respiratory diseases in children (28 university hospitals, spread across all regions of France). A telephone survey every 6 months with the referring physician in this specialized center or, alternatively, with the family, will collect clinical outcome until the age of 2 years. If a surgical intervention is planned within this interval, consent to collect part of the surgical specimen for research purposes will be solicited. This tissue will be immediately frozen at -80 ° C, to allow laser microdissection and DNA extraction from epithelial cells lining the malformation (Inserm U955). Frozen tissue will be conserved at the biobank of Necker-Enfants Malades.

Primary Outcomes

Secondary Outcomes

• Therapeutic abortion - fetal death(At Birth of the child)
• Severe respiratory distress(At Birth of the child)
• CFTR protein expression(2 years)
• Response to inhibitors of basolateral K+ secretion : ΔBarium ; ΔChromanol(2 years)
• CFTR gene expression(2 years)
• Response to ENaC inhibitors : ΔAmiloride, Δbenzamil(2 years)
• Protein expression of other channels : ENaC, SLC26A9, CaCC, KVLQT1 and KCa3.1(2 years)
• Effects of other potentiators on CFTR activity : ΔGenistein, ΔVX-770(2 years)
• Inhibition of CFTR (inh-172) : ΔInh-172(2 years)
• Activation of Calcium Dependant Channels : ΔUTP(2 years)
• Inhibition of SLC26A9 : ΔGlyH-101(2 years)
• Secretion of HCO3- in response to forskoline : Δ HCO3- primary culture(2 years)
• Gene expression of other channels : ENaC, SLC26A9, CaCC, KVLQT1 and KCa3.1(2 years)
• Necessity of antenatal treatment(At Birth of the child)
• Identification of KRAS mutation(2 years)
• Level in delta Forskoline/IBMX Short Circuit Current (µA/cm2)(2 years)
• Basal short circuit current : Isc Basal(2 years)