Bi-allelic variants in CHKA cause a neurodevelopmental disorder with epilepsy and microcephaly.
Chiara KlöcknerJ Pedro Fernández-MurrayMahtab TavasoliHeinrich StichtGisela Stoltenburg-DidingerLeila Motlagh ScholleSomayeh BakhtiariMichael C KruerHossein DarvishSaghar Ghasemi FirouzabadiAlex PagnozziAnju ShuklaKatta Mohan GirishaDhanya Lakshmi NarayananParneet KaurReza MaroofianMaha Saad ZakiMahmoud M NoureldeenAndreas MerkenschlagerJanina Gburek-AugustatElisa CaliSelina BanuKamrun NaharStephanie EfthymiouHenry HouldenRami Abou JamraJason WilliamsChristopher R McMasterKonrad PlatzerPublished in: Brain : a journal of neurology (2022)
The Kennedy pathways catalyse the de novo synthesis of phosphatidylcholine and phosphatidylethanolamine, the most abundant components of eukaryotic cell membranes. In recent years, these pathways have moved into clinical focus because four of ten genes involved have been associated with a range of autosomal recessive rare diseases such as a neurodevelopmental disorder with muscular dystrophy (CHKB), bone abnormalities and cone-rod dystrophy (PCYT1A) and spastic paraplegia (PCYT2, SELENOI). We identified six individuals from five families with bi-allelic variants in CHKA presenting with severe global developmental delay, epilepsy, movement disorders and microcephaly. Using structural molecular modelling and functional testing of the variants in a cell-based Saccharomyces cerevisiae model, we determined that these variants reduce the enzymatic activity of CHKA and confer a significant impairment of the first enzymatic step of the Kennedy pathway. In summary, we present CHKA as a novel autosomal recessive gene for a neurodevelopmental disorder with epilepsy and microcephaly.