Bi-allelic loss of ERGIC1 causes relatively mild arthrogryposis.
Caterina MarconiLaure LemmensFrédéric MasclauxFrancesca MattioliJoël FlussPhilippe ExtermannPurificacion MendezRussia Ha-Vinh LeuchterElissavet StathakiSacha LaurentEva HammarAnne VannierKonstantinos VarvagiannisMichel GuipponiFrédérique Sloan-BenaJean-Louis BlouinMarc AbramowiczSiv FokstuenPublished in: Clinical genetics (2021)
Arthrogryposis describes the presence of multiple joint-contractures. Clinical severity of this phenotype is variable, and more than 400 causative genes have been proposed. Among these, ERGIC1 is a recently reported candidate encoding a putative transmembrane protein of the ER-Golgi interface. Two homozygous missense variants have been reported in patients with relatively mild non-syndromic arthrogryposis. In a consanguineous family with two affected siblings presenting congenital arthrogryposis and some facial dysmorphism we performed prenatal array-CGH, postnatal targeted exome and genome sequencing. Genome sequencing identified a homozygous 22.6 Kb deletion encompassing the promoter and first exon of ERGIC1. mRNA quantification showed the complete absence of ERGIC1 expression in the two affected siblings and a decrease in heterozygous parents. Our observations validate the pathogenic role of ERGIC1 in congenital arthrogryposis and demonstrate that complete loss of function causes a relatively mild phenotype. These findings will contribute to improve genetic counseling of ERGIC1 mutations.
Keyphrases
- intellectual disability
- genome wide
- copy number
- binding protein
- dna methylation
- single cell
- pregnant women
- poor prognosis
- gene expression
- endoplasmic reticulum
- preterm infants
- autism spectrum disorder
- high resolution
- cancer therapy
- high throughput
- smoking cessation
- small molecule
- human immunodeficiency virus
- mass spectrometry
- antiretroviral therapy
- high density