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Supplementary Material for: A Novel de novo Frameshift Mutation in the BCL11A Gene in a Patient with Intellectual Disability Syndrome and Epilepsy

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DataCite Commons2020-08-25 更新2024-07-28 收录
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https://karger.figshare.com/articles/Supplementary_Material_for_A_Novel_de_novo_Frameshift_Mutation_in_the_BCL11A_Gene_in_a_Patient_with_Intellectual_Disability_Syndrome_and_Epilepsy/12533309
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Intellectual disability syndrome (IDS) associated with a hereditary persistence of fetal haemoglobin (HbF), also known as Dias-Logan syndrome, is commonly characterised by psychomotor developmental delay, intelectual disability, language delay, strabismus, thin upper lip, abnormalities of external ears, microcephaly, downslanting palpebral fissures. Sporadically, autism spectrum disorders and blue sclerae in infancy have been reported in IDS. Rarely, IDS-affected patients present with epilepsy and/or epileptic syndromes. It has been shown that a haploinsufficiency of the B cell leukaemia/lymphoma 11A gene (<i>BCL11A</i>) is responsible for IDS. Herein, we identified a novel de novo frameshift deletion (c.271delG; p.E91Afs*2) in the <i>BCL11A</i> gene in a boy affected with IDS. Interestingly, this heterozygous loss-of-function <i>BCL11A</i> mutation was also associated with a generalised idiopathic epilepsy and severe language delay observed in the patient. Moreover, our study showed that the combination of molecular genetic analyses with the monitoring of HbF was essential to make the final diagnosis of Dias-Logan syndrome. Because our patient suffered from well-controlled epilepsy, we propose to include the <i>BCL11A</i> gene in routinely used molecular genetic epilepsy-related gene panels. Additionally, many of the clinical features of IDS overlap with symptoms observed in patients with suspected alcohol spectrum disorders. Therefore, we also suggest monitoring HbF levels in patients with these syndromes to further facilitate clinical diagnosis.
提供机构:
Karger Publishers
创建时间:
2020-06-22
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