| Literature DB >> 27052971 |
Marisela E Dy1, Florence C F Chang2, Sol De Jesus3, Irina Anselm4, Neil Mahant2, Pamela Zeilman3, Lance H Rodan5, Kelly D Foote6, Wen-Hann Tan5, Emad Eskandar7, Nutan Sharma8, Michael S Okun9, Victor S C Fung2, Jeff L Waugh8.
Abstract
ADCY5 mutations have been reported as a cause of early onset hyperkinetic movements associated with delayed motor milestones, hypotonia, and exacerbation during sleep. The movement disorder may be continuous or episodic, and can vary considerably in severity within families and in individuals. The authors report a case series of 3 patients with ADCY5 mutations treated with deep brain stimulation after unsuccessful medication trials. All had extensive imaging, metabolic, and genetic testing prior to confirmation of their ADCY5 mutation. Two of the patients had the c.1252C>T; p.R418W mutation, while the youngest and most severely affected had a de novo c.2080_2088del; p.K694_M696 mutation. All had variable and incomplete, but positive responses to deep brain stimulation. The authors conclude that deep brain stimulation may provide benefit in ADCY5-related movement disorders. Long-term efficacy remains to be confirmed by longitudinal observation. ADCY5 should be considered in the differential diagnosis of early onset hyperkinetic movement disorders, and may respond to deep brain stimulation.Entities:
Keywords: ADCY5; chorea; deep brain stimulation; hyperkinetic movements; whole-exome sequencing
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Year: 2016 PMID: 27052971 DOI: 10.1177/0883073816635749
Source DB: PubMed Journal: J Child Neurol ISSN: 0883-0738 Impact factor: 1.987