De novo variants in EMC1 lead to neurodevelopmental delay and cerebellar degeneration and affect glial function in Drosophila.
Hyung-Lok ChungPatrick RumpDi LuMegan R GlassfordJung-Wan MokJawid FatihAdily BasalPaul C MarcoglieseOguz KancaMichele RappJohanna M FockErik-Jan KamsteegJames R LupskiAustin LarsonMark C HaninbalHugo BellenTamar HarelPublished in: Human molecular genetics (2022)
We establish de novo monoallelic EMC1 variants as causative of a neurological disease trait by providing functional evidence in a Drosophila model. The identified variants failed to rescue the lethality of a null allele. Variations in dosage of the wild-type EMC1, specifically in glia, lead to pupal lethality, which we hypothesize results from the altered stoichiometry of the multi-subunit protein complex EMC.