Missense Mutations of the Pro65 Residue of PCGF2 Cause a Recognizable Syndrome Associated with Craniofacial, Neurological, Cardiovascular, and Skeletal Features

Overview

Journal Am J Hum Genet

Publisher Cell Press

Specialty Genetics

Date 2018 Oct 23

PMID 30343942

Citations 10

Authors

Peter D Turnpenny

Michael J Wright

Melissa Sloman

Richard Caswell

Anthony J van Essen

Erica Gerkes

Rolph Pfundt

Susan M White

Nava Shaul-Lotan

Lori Carpenter

G Bradley Schaefer

Alan Fryer

A Micheil Innes

Kirsten P Forbes

Wendy K Chung

Heather McLaughlin

Lindsay B Henderson

Amy E Roberts

Karen E Heath

Beatriz Paumard-Hernandez

Blanca Gener

Katherine A Fawcett

Romana Gjergja-Juraski

Daniela T Pilz

Andrew E Fry

Affiliations

Soon will be listed here.

Abstract

PCGF2 encodes the polycomb group ring finger 2 protein, a transcriptional repressor involved in cell proliferation, differentiation, and embryogenesis. PCGF2 is a component of the polycomb repressive complex 1 (PRC1), a multiprotein complex which controls gene silencing through histone modification and chromatin remodelling. We report the phenotypic characterization of 13 patients (11 unrelated individuals and a pair of monozygotic twins) with missense mutations in PCGF2. All the mutations affected the same highly conserved proline in PCGF2 and were de novo, excepting maternal mosaicism in one. The patients demonstrated a recognizable facial gestalt, intellectual disability, feeding problems, impaired growth, and a range of brain, cardiovascular, and skeletal abnormalities. Computer structural modeling suggests the substitutions alter an N-terminal loop of PCGF2 critical for histone biding. Mutant PCGF2 may have dominant-negative effects, sequestering PRC1 components into complexes that lack the ability to interact efficiently with histones. These findings demonstrate the important role of PCGF2 in human development and confirm that heterozygous substitutions of the Pro65 residue of PCGF2 cause a recognizable syndrome characterized by distinctive craniofacial, neurological, cardiovascular, and skeletal features.

Citing Articles

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