Familial hemiplegic migraine type 2 results from pathogenic variants in the ATP1A2 gene, which encodes for a catalytic subunit of sodium/potassium ATPase. This extremely rare autosomal dominant disorder manifests with a spectrum of symptoms, most commonly pure hemiplegic phenotype, epilepsy, and/or intellectual disability. In this study, we detail the clinical features and genetic analysis of nine patients from a large family spanning four generations, with all carrying a previously unreported likely pathogenic variant, p.Gly615Glu, in ATP1A2, compatible with a diagnosis of familial hemiplegic migraine type 2, fully penetrant with variable expressivity. This newly identified likely pathogenic variant primarily presented with psychiatric disturbances and a non-hemiplegic phenotype. Only one patient presented hemiplegic attacks, while seven were diagnosed with migraine with aura, including visual, sensory, and speech/language aura, and one with migraine without aura. The identification of the genes responsible for the more common forms of migraine, both with and without aura, remains a significant challenge in migraine genetics and is critical for advancing personalized medicine.Romozzi et al. describe a family of nine members with familial hemiplegic migraine Type 2 caused by a novel likely pathogenic variant (p.Gly615Glu) in the ATP1A2 gene. The variant demonstrated full penetrance with variable expressivity, predominantly presenting with psychiatric disturbances and migraine with aura instead of hemiplegic attacks.
Romozzi, M., Spartano, S., L'Erario, F. F., Iannone, L. F., Trigila, V., Gentile, A., Sanginario, P., Calabresi, P., Tiziano, F. D., Vollono, C., Clinical characterization of a novel ATP1A2 p.Gly615Glu mutation in nine family members with familial hemiplegic migraine, <<BRAIN COMMUNICATIONS>>, 2024; 7 (1): N/A-N/A. [doi:10.1093/braincomms/fcae447] [https://hdl.handle.net/10807/302061]
Clinical characterization of a novel ATP1A2 p.Gly615Glu mutation in nine family members with familial hemiplegic migraine
Romozzi, Marina;Spartano, Serena;L'Erario, Federica Francesca;Sanginario, Pasquale;Calabresi, Paolo;Tiziano, Francesco Danilo;Vollono, Catello
2024
Abstract
Familial hemiplegic migraine type 2 results from pathogenic variants in the ATP1A2 gene, which encodes for a catalytic subunit of sodium/potassium ATPase. This extremely rare autosomal dominant disorder manifests with a spectrum of symptoms, most commonly pure hemiplegic phenotype, epilepsy, and/or intellectual disability. In this study, we detail the clinical features and genetic analysis of nine patients from a large family spanning four generations, with all carrying a previously unreported likely pathogenic variant, p.Gly615Glu, in ATP1A2, compatible with a diagnosis of familial hemiplegic migraine type 2, fully penetrant with variable expressivity. This newly identified likely pathogenic variant primarily presented with psychiatric disturbances and a non-hemiplegic phenotype. Only one patient presented hemiplegic attacks, while seven were diagnosed with migraine with aura, including visual, sensory, and speech/language aura, and one with migraine without aura. The identification of the genes responsible for the more common forms of migraine, both with and without aura, remains a significant challenge in migraine genetics and is critical for advancing personalized medicine.Romozzi et al. describe a family of nine members with familial hemiplegic migraine Type 2 caused by a novel likely pathogenic variant (p.Gly615Glu) in the ATP1A2 gene. The variant demonstrated full penetrance with variable expressivity, predominantly presenting with psychiatric disturbances and migraine with aura instead of hemiplegic attacks.
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