| Literature DB >> 31612321 |
Claire Guissart1, Alexander N Harrison2, Mehdi Benkirane3, Ibrahim Oncel4, Elif Acar Arslan5, Anna K Chassevent6, Kristin Baraῆano6, Lise Larrieu3, Maria Iascone7, Romano Tenconi8, Mireille Claustres3, Nesibe Eroglu-Ertugrul4, Patrick Calvas9, Haluk Topaloglu4, Robert S Molday2, Michel Koenig3.
Abstract
ATP8A2-related disorders are autosomal recessive conditions that associate encephalopathy with or without hypotonia, psychomotor delay, abnormal movements, chorea, tremor, optic atrophy and cerebellar atrophy (CARMQ4). Through a multi-centric collaboration, we identified six point mutations (one splice site and five missense mutations) involving ATP8A2 in six individuals from five families. Two patients from one family with the homozygous p.Gly585Val mutation had a milder presentation without encephalopathy. Expression and functional studies of the missense mutations demonstrated that protein levels of four of the five missense variants were very low and lacked phosphatidylserine-activated ATPase activity. One variant p.Ile215Leu, however, expressed at normal levels and displayed phospholipid-activated ATPase activity similar to the non-mutated protein. We therefore expand for the first time the phenotype related to ATP8A2 mutations to less severe forms characterized by cerebellar ataxia without encephalopathy and suggest that ATP8A2 should be analyzed for all cases of syndromic or non-syndromic recessive or sporadic ataxia.Entities:
Keywords: ATP8A2; Ataxia; CAMRQ; P4-ATPase; Psychomotor delay
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Year: 2019 PMID: 31612321 DOI: 10.1007/s00415-019-09579-4
Source DB: PubMed Journal: J Neurol ISSN: 0340-5354 Impact factor: 4.849