GNB5 Mutations Cause an Autosomal-Recessive Multisystem Syndrome with Sinus Bradycardia and Cognitive Disability
Lodder, Elisabeth M.; De Nittis, Pasquelena; Koopman, Charlotte D.; Wiszniewski, Wojciech; Moura de Souza, Carolina Fischinger; Lahrouchi, Najim; Guex, Nicolas; Napolioni, Valerio; Tessadori, Federico; Beekman, Leander; Nannenberg, Eline A.; Boualla, Lamiae; Blom, Nico A.; de Graaff, Wim; Kamermans, Maarten; Cocciadiferro, Dario; Malerba, Natascia; Mandriani, Barbara; Akdemir, Zeynep Hande Coban; Fish, Richard J.; Eldomery, Mohammad K.; Ratbi, Ilham; Wilde, Arthur A M; de Boer, Teun; Simonds, William F.; Neerman-Arbez, Marguerite; Sutton, V. Reid; Kok, Fernando; Lupski, James R.; Reymond, Alexandre; Bezzina, Connie R.; Bakkers, Jeroen; Merla, Giuseppe
(2016) American Journal of Human Genetics, volume 99, issue 3, pp.
(Article)
Abstract
. GNB5 encodes the G protein β subunit 5 and is involved in inhibitory G protein signaling. Here, we report mutations in . GNB5 that are associated with heart-rate disturbance, eye disease, intellectual disability, gastric problems, hypotonia, and seizures in nine individuals from six families. We observed an association between
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the nature of the variants and clinical severity; individuals with loss-of-function alleles had more severe symptoms, including substantial developmental delay, speech defects, severe hypotonia, pathological gastro-esophageal reflux, retinal disease, and sinus-node dysfunction, whereas related heterozygotes harboring missense variants presented with a clinically milder phenotype. Zebrafish . gnb5 knockouts recapitulated the phenotypic spectrum of affected individuals, including cardiac, neurological, and ophthalmological abnormalities, supporting a direct role of GNB5 in the control of heart rate, hypotonia, and vision.
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Keywords: G-protein signaling, Heart rate, Hypotonia, Intellectual disability, Parasympathetic system, Whole-exome sequencing, Genetics, Genetics(clinical), Journal Article
ISSN: 0002-9297
Publisher: Cell Press
(Peer reviewed)