| Literature DB >> 34516822 |
Ulrike B S Hedrich1, Stephan Lauxmann1, Markus Wolff2,3, Matthis Synofzik4,5, Thomas Bast6,7, Adrian Binelli8, José M Serratosa9,10, Pedro Martínez-Ulloa9, Nicholas M Allen11, Mary D King12,13, Kathleen M Gorman12,13, Bruria Ben Zeev14,15, Michal Tzadok14,15, Lily Wong-Kisiel16, Dragan Marjanovic17, Guido Rubboli17,18, Sanjay M Sisodiya19,20, Florian Lutz1, Harshad Pannikkaveettil Ashraf1, Kirsten Torge1, Pu Yan1, Christian Bosselmann1, Niklas Schwarz1, Monika Fudali21, Holger Lerche1.
Abstract
Developmental and epileptic encephalopathies are devastating disorders characterized by epilepsy, intellectual disability, and other neuropsychiatric symptoms, for which available treatments are largely ineffective. Following a precision medicine approach, we show for KCNA2-encephalopathy that the K+ channel blocker 4-aminopyridine can antagonize gain-of-function defects caused by variants in the KV1.2 subunit in vitro, by reducing current amplitudes and negative shifts of steady-state activation and increasing the firing rate of transfected neurons. In n-of-1 trials carried out in nine different centers, 9 of 11 patients carrying such variants benefitted from treatment with 4-aminopyridine. All six patients experiencing daily absence, myoclonic, or atonic seizures became seizure-free (except some remaining provoked seizures). Two of six patients experiencing generalized tonic-clonic seizures showed marked improvement, three showed no effect, and one worsening. Nine patients showed improved gait, ataxia, alertness, cognition, or speech. 4-Aminopyridine was well tolerated up to 2.6 mg/kg per day. We suggest 4-aminopyridine as a promising tailored treatment in KCNA2-(gain-of-function)–encephalopathy and provide an online tool assisting physicians to select patients with gain-of-function mutations suited to this treatment.Entities:
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Year: 2021 PMID: 34516822 DOI: 10.1126/scitranslmed.aaz4957
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956