Intrauterine growth in chromatinopathies: A long road for better understanding and for improving clinical management

Author:

Avagliano Laura1ORCID,Castiglioni Silvia2ORCID,Lettieri Antonella2,Parodi Chiara2,Di Fede Elisabetta23,Taci Esi23,Grazioli Paolo2ORCID,Colombo Elisa Adele2,Gervasini Cristina23,Massa Valentina23ORCID

Affiliation:

1. Università degli Studi di Milano Milan Italy

2. Department of Health Sciences Università Degli Studi di Milano Milan Italy

3. Aldo Ravelli Center for Neurotechnology and Experimental Brain Therapeutics Università Degli Studi di Milano Milan Italy

Abstract

AbstractBackgroundChromatinopathies are a heterogeneous group of genetic disorders caused by pathogenic variants in genes coding for chromatin state balance proteins. Remarkably, many of these syndromes present unbalanced postnatal growth, both under‐ and over‐, although little has been described in the literature. Fetal growth measurements are common practice in pregnancy management and values within normal ranges indicate proper intrauterine growth progression; on the contrary, abnormalities in intrauterine fetal growth open the discussion of possible pathogenesis affecting growth even in the postnatal period.MethodsAmong the numerous chromatinopathies, we have selected six of the most documented in the literature offering evidence about two fetal overgrowth (Sotos and Weaver syndrome) and four fetal undergrowth syndromes (Bohring Opitz, Cornelia de Lange, Floating‐Harbor, and Meier Gorlin syndrome), describing their molecular characteristics, maternal biochemical results and early pregnancy findings, prenatal ultrasound findings, and postnatal characteristics.Results/ConclusionTo date, the scarce data in the literature on prenatal findings are few and inconclusive, even though these parameters may contribute to a more rapid and accurate diagnosis, calling for a better and more detailed description of pregnancy findings.

Publisher

Wiley

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