A Recurrent Missense Variant in AP2M1 Impairs Clathrin-Mediated Endocytosis and Causes Developmental and Epileptic Encephalopathy

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Helbig, Ingo | Lopez-Hernandez, Tania | Shor, Oded | Galer, Peter | Ganesan, Shiva | Pendziwiat, Manuela | Rademacher, Annika | Ellis, Colin | Hümpfer, Nadja | Schwarz, Niklas | Seiffert, Simone | Peeden, Joseph | Shen, Joseph | Štěrbová, Katalin | Hammer, Trine Bjørg | Møller, Rikke | Shinde, Deepali | Tang, Sha | Smith, Lacey | Poduri, Annapurna | Krause, Roland | Benninger, Felix | Helbig, Katherine | Haucke, Volker | Weber, Yvonne | Balling, Rudi | Barisic, Nina | Baulac, Stéphanie | Caglayan, Hande | Craiu, Dana | de Jonghe, Peter | Depienne, Christel | Guerrini, Renzo | Hjalgrim, Helle | Hoffman-Zacharska, Dorota | Jähn, Johanna | Klein, Karl Martin | Koeleman, Bobby P.C. | Komarek, Vladimir | Leguern, Eric | Lehesjoki, Anna-Elina | Lemke, Johannes | Lerche, Holger | Linnankivi, Tarja | Marini, Carla | May, Patrick | Muhle, Hiltrud | Pal, Deb | Palotie, Aarno | Rosenow, Felix | Schubert-Bast, Susanne | Selmer, Kaja | Serratosa, Jose | Sisodiya, Sanjay | Stephani, Ulrich | Striano, Pasquale | Suls, Arvid | Talvik, Tiina | von Spiczak, Sarah | Weckhuysen, Sarah | Zara, Federico | Avillach, Paul | Bartels, Anna | Biswas, Sawona | Bourgeois, Florence | Devkota, Batsal | Glauser, Tracy | Hallinan, Barbara | Heath, Allison | Hirschhorn, Joel | Kilbourn, Judson | Kong, Sek Won | Krantz, Ian | Lee, In-Hee | Mandl, Kenneth | Marsh, Eric | Sund, Kristen | Taylor, Deanne | White, Peter | Jonghe, Peter De | Lemke, Johannes R. | Pal, Deb K. | Serratosa, Jose M. | Spiczak, Sarah Von | Mandl, Kenneth D.

Edité par CCSD ; Elsevier (Cell Press) -

International audience. The developmental and epileptic encephalopathies (DEEs) are heterogeneous disorders with a strong genetic contribution, but the underlying genetic etiology remains unknown in a significant proportion of individuals. To explore whether statistical support for genetic etiologies can be generated on the basis of phenotypic features, we analyzed whole-exome sequencing data and phenotypic similarities by using Human Phenotype Ontology (HPO) in 314 individuals with DEEs. We identified a de novo c.508C>T (p.Arg170Trp) variant in AP2M1 in two individuals with a phenotypic similarity that was higher than expected by chance (p = 0.003) and a phenotype related to epilepsy with myoclonic-atonic seizures. We subsequently found the same de novo variant in two individuals with neurodevelopmental disorders and generalized epilepsy in a cohort of 2,310 individuals who underwent diagnostic whole-exome sequencing. AP2M1 encodes the μ-subunit of the adaptor protein complex 2 (AP-2), which is involved in clathrin-mediated endocytosis (CME) and synaptic vesicle recycling. Modeling of protein dynamics indicated that the p.Arg170Trp variant impairs the conformational activation and thermodynamic entropy of the AP-2 complex. Functional complementation of both the μ-subunit carrying the p.Arg170Trp variant in human cells and astrocytes derived from AP-2μ conditional knockout mice revealed a significant impairment of CME of transferrin. In contrast, stability, expression levels, membrane recruitment, and localization were not impaired, suggesting a functional alteration of the AP-2 complex as the underlying disease mechanism. We establish a recurrent pathogenic variant in AP2M1 as a cause of DEEs with distinct phenotypic features, and we implicate dysfunction of the early steps of endocytosis as a disease mechanism in epilepsy.

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