Two Novel FAM20C Variants in a Family with Raine Syndrome

Author:

Hernández-Zavala AraceliORCID,Cortés-Camacho Fernando,Palma-Lara Icela,Godínez-Aguilar Ricardo,Espinosa Ana María,Pérez-Durán Javier,Villanueva-Ocampo Patricia,Ugarte-Briones Carlos,Serrano-Bello Carlos Alberto,Sánchez-Santiago Paula Jesús,Bonilla-Delgado JoséORCID,Yáñez-López Marco Antonio,Victoria-Acosta Georgina,López-Ornelas Adolfo,García Alonso-Themann Patricia,Moreno JoséORCID,Palacios-Reyes CarmenORCID

Abstract

Two siblings from a Mexican family who carried lethal Raine syndrome are presented. A newborn term male (case 1) and his 21 gestational week brother (case 2), with a similar osteosclerotic pattern: generalized osteosclerosis, which is more evident in facial bones and cranial base. Prenatal findings at 21 weeks and histopathological features for case 2 are described. A novel combination of biallelic FAM20C pathogenic variants were detected, a maternal cytosine duplication at position 456 and a paternal deletion of a cytosine in position 474 in exon 1, which change the reading frame with a premature termination at codon 207 and 185 respectively. These changes are in concordance with a negative detection of the protein in liver and kidney as shown in case 2. Necropsy showed absence of pancreatic Langerhans Islets, which are reported here for the first time. Corpus callosum absence is added to the few reported cases of brain defects in Raine syndrome. This report shows two new FAM20C variants not described previously, and negative protein detection in the liver and the kidney. We highlight that lethal Raine syndrome is well defined as early as 21 weeks, including mineralization defects and craniofacial features. Pancreas and brain defects found here in FAM20C deficiency extend the functional spectrum of this protein to previously unknown organs.

Publisher

MDPI AG

Subject

Genetics(clinical),Genetics

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