Journal article

A neural crest origin for cohesinopathy heart defects

K Schuster, B Leeke, M Meier, Y Wang, T Newman, S Burgess, JA Horsfield

Human Molecular Genetics | OXFORD UNIV PRESS | Published : 2015

DOI: 10.1093/hmg/ddv402

Abstract

Mutations in subunits or regulators of cohesin cause a spectrum of disorders in humans known as the 'cohesinopathies'. Cohesinopathies, including the best known example Cornelia de Lange syndrome (CdLS), are characterized by broad spectrum, multifactorial developmental anomalies. Heart defects occur at high frequency and can reach up to 30% in CdLS. The mechanisms by which heart defects occur are enigmatic, but assumed to be developmental in origin. In this study,we depleted cohesin subunit Rad21 by 70-80% in a zebrafish cohesinopathy model. The hearts of Rad21-depleted animals were smaller, often failed to loop, and functioned less efficiently than size-matched controls. Functional deficien..

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University of Melbourne Researchers

Grants

Awarded by National Institutes of Health

Funding Acknowledgements

This work was supported by the Neurological Foundation of NZ (to J.A.H.) and the Royal Society of NZ Marsden Fund (grant number 11-UOO-027 to J.A.H.). S.B. is supported by National Institutes of Health (grant number R01 GM075119).

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Keywords

1.1 Normal Biological Development and Functioning
Neurosciences
Brain Disorders
Pediatric Research Initiative
3105 Genetics
Sister-Chromatid Cohesion
Genetics & Heredity
Life Sciences & Biomedicine
Congenital Structural Anomalies
2.1 Biological and Endogenous Factors
De-Lange-Syndrome
Hdac8 Mutations
Biochemistry & Molecular Biology
Human Homolog
Gene-Expression
Cells
Genetics
Phenotype
Contributes
Cardiovascular
Cornelia
Congenital Heart Disease
Intellectual and Developmental Disabilities (idd)
Science & Technology
Specification
31 Biological Sciences
Rare Diseases
Heart Disease