Compound Heterozygous Mutations in the Gene PIGP Are Associated with Early Infantile Epileptic Encephalopathy

Overview

Journal Hum Mol Genet

Specialties Genetics
Molecular Biology

Date 2017 Mar 24

PMID 28334793

Citations 19

Authors

Devon L Johnstone

Thi-Tuyet-Mai Nguyen

Yoshiko Murakami

Kristin D Kernohan

Martine Tetreault

Claire Goldsmith

Asif Doja

Justin D Wagner

Lijia Huang

Taila Hartley

Anik St-Denis

Francoise Le Deist

Jacek Majewski

Dennis E Bulman

Taroh Kinoshita

David A Dyment

Kym M Boycott

Philippe M Campeau

Affiliations

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Abstract

There are over 150 known human proteins which are tethered to the cell surface via glycosylphosphatidylinositol (GPI) anchors. These proteins play a variety of important roles in development, and particularly in neurogenesis. Not surprisingly, mutations in the GPI anchor biosynthesis and remodeling pathway cause a number of developmental disorders. This group of conditions has been termed inherited GPI deficiencies (IGDs), a subgroup of congenital disorders of glycosylation; they present with variable phenotypes, often including seizures, hypotonia and intellectual disability. Here, we report two siblings with compound heterozygous variants in the gene phosphatidylinositol glycan anchor biosynthesis, class P (PIGP) (NM_153681.2: c.74T > C;p.Met25Thr and c.456delA;p.Glu153AsnFs*34). PIGP encodes a subunit of the enzyme that catalyzes the first step of GPI anchor biosynthesis. Both children presented with early-onset refractory seizures, hypotonia, and profound global developmental delay, reminiscent of other IGD phenotypes. Functional studies with patient cells showed reduced PIGP mRNA levels, and an associated reduction of GPI-anchored cell surface proteins, which was rescued by exogenous expression of wild-type PIGP. This work associates mutations in the PIGP gene with a novel autosomal recessive IGD, and expands our knowledge of the role of PIG genes in human development.

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