AI Article Synopsis
- The gene is part of the GATOR1 complex that helps regulate the mTORC1 pathway, playing a critical role in brain development and neurogenesis; its deletion or mutation can lead to focal epilepsy and related conditions.
- A case study describes a 10-year-old boy who faced a long diagnostic journey due to nocturnal episodes, which were initially misdiagnosed; he eventually tested positive for a deletion linked to both his epilepsy and α-thalassemia trait.
- This study stresses the importance of thorough genetic testing for children with epilepsy and related symptoms, highlighting how recognizing overlapping symptoms can prevent misdiagnoses and lead to more accurate and timely treatments.
Article Abstract
: The gene is a critical component of the GATOR1 complex, which negatively regulates the mTORC1 pathway, essential for neurogenesis and brain development. Located on chromosome 16p13.3, is situated near the α-globin gene cluster. Haploinsufficiency of , either by deletion or a pathogenic variant, is associated with a variable phenotype of focal epilepsy, with or without malformations of cortical development, with known decreased penetrance. : This work details the diagnostic odyssey of a neurotypical 10-year-old boy who presented at age 2 with unusual nocturnal episodes and a history of microcytic anemia, as well as a review of the existing literature on -related epilepsy, with an emphasis on individuals with deletions who also present with α-thalassemia trait. The proband's episodes were mistaken for gastroesophageal reflux disease for several years. He had molecular testing for his α-thalassemia trait and was noted to carry a deletion encompassing the regulatory region of the α-thalassemia gene cluster. Following the onset of overt focal motor seizures, genetic testing revealed a heterozygous loss of within a 106 kb microdeletion on chromosome 16p13.3, inherited from his mother. This deletion encompassed the entire gene, which overlaps the regulatory region of the α-globin gene cluster, giving him the dual diagnosis of -related epilepsy and α-thalassemia trait. Brain imaging postprocessing showed left hippocampal sclerosis and mid-posterior para-hippocampal focal cortical dysplasia, leading to the consideration of epilepsy surgery. : This case underscores the necessity of early and comprehensive genetic assessments in children with epilepsy accompanied by systemic features, even in the absence of a family history of epilepsy or a developmental delay. Recognizing phenotypic overlaps is crucial to avoid diagnostic delays. Our findings also highlight the impact of disruptions in regulatory regions in genetic disorders: any individual with full gene deletion of would have, at a minimum, α-thalassemia trait, due to the presence of the major regulatory element of α-globin genes overlapping the gene's introns.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11275569 | PMC |
| http://dx.doi.org/10.3390/genes15070836 | DOI Listing |
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