Add to ORKGWe report two brothers with severe global cognitive and motor delay, cortical visual impairment and sick sinus syndrome who were born to consanguineous parents. Standard genetic evaluations did not reveal the cause of their mental retardation. As expected, chromosomal microarray (CMA) revealed extensive regions of homozygosity. Exome sequencing revealed that both affected boys were homozygous for a nonsense mutation in the G-protein β5 (GNB5) gene (NM_016194.3:c.1032C > G; Tyr344Ter), and that the parents were carriers of this mutation. No other DNA variants that were explanatory for the sick sinus or the developmental delay/intellectual disability were identified, and no other clinical parameters are likely to have contributed...
Neurogenetic studies have revolutionised our understanding of the genetic and molecular basis of inh...
[Purpose]: This study aimed to identify the genetic cause of a new multiple congenital anomalies syn...
We present two brothers with mutations in UPF3B, an X-linked intellectual disability gene. Our famil...
Identification of a novel compound heterozygous of GNB5 in a patient with intellectual developmental...
Homozygous and compound heterozygous mutations in GNB5 gene have been associated with a wide spectru...
Homozygous and compound heterozygous pathogenic variants in GNB5 have been recently associated with ...
The chromosomal segment 6q24-q25 comprises a contiguous gene microdeletion syndrome characterized by...
Background: Syndromic dilated cardiomyopathy (DCM) includes a group of complex disorders with a very...
Intellectual disability (ID) and autism spectrum disorder (ASD) are complex neurodevelopmental disor...
GNB5 encodes the G protein β subunit 5 and is involved in inhibitory G protein signaling. Here, we r...
Background: Intellectual disability (ID) is both a clinically diverse and genetically heterogeneous ...
GNB5 encodes the G protein β subunit 5 and is involved in inhibitory G protein signaling. Here, we r...
Background: 1q21 microdeletion syndrome is a rare contiguous gene deletion disorder with de novo or ...
Whole genome sequencing can enable an unbiased approach to the diagnosis and to the understanding of...
Abstract Background Developmental disabilities have diverse genetic causes that must be identified t...
Neurogenetic studies have revolutionised our understanding of the genetic and molecular basis of inh...
[Purpose]: This study aimed to identify the genetic cause of a new multiple congenital anomalies syn...
We present two brothers with mutations in UPF3B, an X-linked intellectual disability gene. Our famil...
Identification of a novel compound heterozygous of GNB5 in a patient with intellectual developmental...
Homozygous and compound heterozygous mutations in GNB5 gene have been associated with a wide spectru...
Homozygous and compound heterozygous pathogenic variants in GNB5 have been recently associated with ...
The chromosomal segment 6q24-q25 comprises a contiguous gene microdeletion syndrome characterized by...
Background: Syndromic dilated cardiomyopathy (DCM) includes a group of complex disorders with a very...
Intellectual disability (ID) and autism spectrum disorder (ASD) are complex neurodevelopmental disor...
GNB5 encodes the G protein β subunit 5 and is involved in inhibitory G protein signaling. Here, we r...
Background: Intellectual disability (ID) is both a clinically diverse and genetically heterogeneous ...
GNB5 encodes the G protein β subunit 5 and is involved in inhibitory G protein signaling. Here, we r...
Background: 1q21 microdeletion syndrome is a rare contiguous gene deletion disorder with de novo or ...
Whole genome sequencing can enable an unbiased approach to the diagnosis and to the understanding of...
Abstract Background Developmental disabilities have diverse genetic causes that must be identified t...
Neurogenetic studies have revolutionised our understanding of the genetic and molecular basis of inh...
[Purpose]: This study aimed to identify the genetic cause of a new multiple congenital anomalies syn...
We present two brothers with mutations in UPF3B, an X-linked intellectual disability gene. Our famil...