Language Delay And Attention Deficit-Hyperactivity Disorder/cognitive Impairment With Or Without Cardiac Arrhythmia
A number sign (#) is used with this entry because of evidence that language delay and attention deficit-hyperactivity disorder/cognitive impairment with or without cardiac arrhythmia (LADCI) is caused by homozygous mutation in the GNB5 gene (604447) on chromosome 15q21.
Biallelic loss-of-function mutations in the GNB5 gene can cause intellectual developmental disorder with cardiac arrhythmia (IDDCA; 617173), a more severe disorder with overlapping features.
DescriptionLADCI is an autosomal recessive neurodevelopmental disorder characterized by severe expressive and receptive language delay apparent from early childhood. Affected individuals have additional developmental or behavioral abnormalities, including attention deficit, hyperactivity, or mild intellectual disability. Some patients develop cardiac arrhythmias reminiscent of sick sinus syndrome (summary by Lodder et al., 2016 and Shamseldin et al., 2016).
Clinical FeaturesLodder et al. (2016) reported 3 patients from 2 unrelated families (family E of Moroccan descent and family F of Brazilian descent) with LADCI with cardiac arrhythmia. Two Moroccan sibs, 13 and 8 years of age, presented in early childhood with sinus node dysfunction manifest as sinus bradycardia and sinus arrhythmia without structural heart abnormalities; one child required pacemaker implantation. Both had late speech development associated with mild learning delay or mild mental retardation; one child also had impaired fine motor skills. Neither had seizures or ocular abnormalities; brain imaging and EEG were normal in 1 patient. A 23-year-old man, born of consanguineous Brazilian parents, had borderline to mild intellectual disability, keratoconus, and sinus arrhythmia.
Shamseldin et al. (2016) reported a large consanguineous Saudi family in which 5 girls had severe language delay. In 1 sibship, 3 sisters, aged 10, 9, and 3, had expressive and receptive language delay. The oldest also had hyperactivity and was diagnosed with attention deficit-hyperactivity disorder (ADHD), whereas the middle sister had no hyperactivity and was diagnosed with inattentive type ADHD; the youngest was too young to assess for ADHD. All had normal cognition. A 5-year-old first cousin had motor delay, hypotonia, and delayed language with normal cognition. A distant cousin had ADHD, severely delayed language, and mild motor delay. Additional features or involvement of other organ systems, such as cardiac, were not reported in any of the patients.
InheritanceThe transmission pattern of LADCI in the families reported by Lodder et al. (2016) and Shamseldin et al. (2016) was consistent with autosomal recessive inheritance.
Molecular GeneticsIn 3 patients from 2 unrelated families (family E of Moroccan ancestry and family F from Brazil) with LADCI with cardiac arrhythmia, Lodder et al. (2016) identified a homozygous missense mutation in the GNB5 gene (S81L; 604447.0006). The mutations, which were found by whole-exome sequencing and confirmed by Sanger sequencing, segregated with the disorder in the families. Functional studies of the variant were not performed. These patients were part of a cohort of 9 patients from 6 families who were found to have GNB5 mutations: those with truncating mutations had a more severe phenotype (IDDCA) than those with the missense mutation, suggesting a genotype/phenotype correlation.
In 5 girls from a large consanguineous Saudi family with LADCI without cardiac arrhythmia, Shamseldin et al. (2016) identified a homozygous S81L substitution in the GNB5 gene. The mutation, which was found by a combination of linkage analysis and exome sequencing, segregated with the disorder in the family. In vitro functional expression assays showed that the S81L mutation resulted in severe but incomplete loss of function, leading to weaker activity of RGS complexes and a decreased ability to deactivate DRD2 (126450)-mediated signaling by dopamine. Shamseldin et al. (2016) noted that knockdown of the Gnb5 gene in C. elegans results in increased locomotor activity (Porter et al., 2010), and that knockdown of the murine ortholog results in hyperactivity and abnormal motor coordination (Xie et al., 2012), making the gene a candidate for ADHD (see ANIMAL MODEL).
Animal ModelXie et al. (2012) found that Gnb5-null mice had hyperactivity and motor learning deficits, as well as a paradoxical adaptation to a novel environment. Gnb5-null mouse brains had lower levels of extracellular dopamine as well as slowed dopamine release and reuptake compared to wildtype. There was also increased sensitivity to inhibitory pre- and postsynaptic G protein-coupled receptor signaling, consistent with the loss of the inhibitory effects of Gnb5/RGS on other receptor signaling pathways. Pharmacologic treatment with monoamine reuptake inhibitors were ineffective in reducing hyperactivity; however, NMDA receptor blockade completely reversed hyperactivity, suggesting that the mutant mice had changes in glutamatergic signaling. The findings indicated that Gnb5-RGS complexes serve as key modulators of signaling pathways that control neuronal excitability and motor activity.
Lodder et al. (2016) used CRISPR/Cas9 genome editing to generate complete loss of gnb5 function in zebrafish; mutant zebrafish had impaired swimming activity, remained small, and died 7 to 14 days postfertilization, likely due to an inability to feed. Treatment of mutant larvae with carbachol, a parasympathomimetic compound that activates the GNB5/RGS/GIRK (G protein-coupled inward rectifier potassium) channel pathway, resulted in a strong decrease in heart rate compared to controls. Treatment with a sympathetic agonist resulted in an increased heart rate similar to controls. These findings indicated that loss of gnb5 caused a loss of negative regulation of the cardiac GIRK channel and parasympathetic control, without effects on sympathetic control. Mutant larvae were predominantly unresponsive to repeated tactile stimulation, apparently due to neurologic deficits, not muscle dysfunction, and showed impaired optokinetic responses, also with normal eye muscle function. The findings indicated that Gnb5 is important for neuronal signaling and autonomic function.