Biallelic variants in COPB1 cause a novel, severe intellectual disability syndrome with cataracts and variable microcephaly

William L. Macken; Annie Godwin; Gabrielle Wheway; Karen Stals; Liliya Nazlamova; Sian Ellard; Ahmed Alfares; Taghrid Aloraini; Lamia AlSubaie; Majid Alfadhel; Sulaiman Alajaji; Htoo A. Wai; Jay Self; Andrew G. L. Douglas; Alexander P. Kao; Matthew Guille; Diana Baralle

doi:10.1186/s13073-021-00850-w

Genome Medicine (Feb 2021)

Biallelic variants in COPB1 cause a novel, severe intellectual disability syndrome with cataracts and variable microcephaly

William L. Macken,
Annie Godwin,
Gabrielle Wheway,
Karen Stals,
Liliya Nazlamova,
Sian Ellard,
Ahmed Alfares,
Taghrid Aloraini,
Lamia AlSubaie,
Majid Alfadhel,
Sulaiman Alajaji,
Htoo A. Wai,
Jay Self,
Andrew G. L. Douglas,
Alexander P. Kao,
Matthew Guille,
Diana Baralle

Affiliations

William L. Macken: Wessex Clinical Genetics Service, Princess Anne Hospital, University Hospital Southampton NHS Foundation Trust
Annie Godwin: European Xenopus Resource Centre, University of Portsmouth School of Biological Sciences
Gabrielle Wheway: Faculty of Medicine, University of Southampton, Duthie Building, Southampton General Hospital
Karen Stals: Exeter Genomics Laboratory, Level 3 RILD building, Royal Devon & Exeter NHS Foundation Trust
Liliya Nazlamova: Faculty of Medicine, University of Southampton, Duthie Building, Southampton General Hospital
Sian Ellard: Exeter Genomics Laboratory, Level 3 RILD building, Royal Devon & Exeter NHS Foundation Trust
Ahmed Alfares: Department of Pediatrics, College of Medicine, Qassim University
Taghrid Aloraini: Department of Pathology and Laboratory Medicine, King Abdulaziz Medical City
Lamia AlSubaie: Division of Genetics, Department of Pediatrics, King Abdullah Specialized Children Hospital, King Abdulaziz Medical City, Ministry of National Guard Health Affairs (MNGHA)
Majid Alfadhel: Division of Genetics, Department of Pediatrics, King Abdullah Specialized Children Hospital, King Abdulaziz Medical City, Ministry of National Guard Health Affairs (MNGHA)
Sulaiman Alajaji: King Saud bin Abdulaziz University for Health Sciences, Ministry of National Guard Health Affairs (MNGHA)
Htoo A. Wai: Faculty of Medicine, University of Southampton, Duthie Building, Southampton General Hospital
Jay Self: Faculty of Medicine, University of Southampton, Duthie Building, Southampton General Hospital
Andrew G. L. Douglas: Wessex Clinical Genetics Service, Princess Anne Hospital, University Hospital Southampton NHS Foundation Trust
Alexander P. Kao: Zeiss Global Centre, School of Mechanical and Design Engineering, University of Portsmouth
Matthew Guille: European Xenopus Resource Centre, University of Portsmouth School of Biological Sciences
Diana Baralle: Wessex Clinical Genetics Service, Princess Anne Hospital, University Hospital Southampton NHS Foundation Trust

DOI: https://doi.org/10.1186/s13073-021-00850-w
Journal volume & issue: Vol. 13, no. 1
pp. 1 – 19

Abstract

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Abstract Background Coat protein complex 1 (COPI) is integral in the sorting and retrograde trafficking of proteins and lipids from the Golgi apparatus to the endoplasmic reticulum (ER). In recent years, coat proteins have been implicated in human diseases known collectively as “coatopathies”. Methods Whole exome or genome sequencing of two families with a neuro-developmental syndrome, variable microcephaly and cataracts revealed biallelic variants in COPB1, which encodes the beta-subunit of COPI (β-COP). To investigate Family 1’s splice donor site variant, we undertook patient blood RNA studies and CRISPR/Cas9 modelling of this variant in a homologous region of the Xenopus tropicalis genome. To investigate Family 2’s missense variant, we studied cellular phenotypes of human retinal epithelium and embryonic kidney cell lines transfected with a COPB1 expression vector into which we had introduced Family 2’s mutation. Results We present a new recessive coatopathy typified by severe developmental delay and cataracts and variable microcephaly. A homozygous splice donor site variant in Family 1 results in two aberrant transcripts, one of which causes skipping of exon 8 in COPB1 pre-mRNA, and a 36 amino acid in-frame deletion, resulting in the loss of a motif at a small interaction interface between β-COP and β’-COP. Xenopus tropicalis animals with a homologous mutation, introduced by CRISPR/Cas9 genome editing, recapitulate features of the human syndrome including microcephaly and cataracts. In vitro modelling of the COPB1 c.1651T>G p.Phe551Val variant in Family 2 identifies defective Golgi to ER recycling of this mutant β-COP, with the mutant protein being retarded in the Golgi. Conclusions This adds to the growing body of evidence that COPI subunits are essential in brain development and human health and underlines the utility of exome and genome sequencing coupled with Xenopus tropicalis CRISPR/Cas modelling for the identification and characterisation of novel rare disease genes.

Published in Genome Medicine

ISSN: 1756-994X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Genetics
Website: https://genomemedicine.biomedcentral.com/

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