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A rare genetic variant in the cleavage site of prepro-orexin is associated with idiopathic hypersomnia.

Taku MiyagawaSusumu TanakaMihoko ShimadaNoriaki SakaiKotomi TanidaNozomu KotoriiTatayu KotoriiYu AriyoshiYuji HashizumeKimihiro OgiHiroshi HiejimaTakashi KanbayashiAya ImanishiAzusa IkegamiYuichi KameiAkiko HidaYamato WadaMasayuki MiyamotoMasanori TakamiHideaki KondoYoshiyuki TamuraYukari TaniyamaNaoto OmataTomoyuki MizunoShunpei MoriyaHirokazu FuruyaMitsuhiro KatoKayoko KatoJun IshigookaKazuhito TsurutaShigeru ChibaNaoto YamadaMasako OkawaKoichi HirataKenji KurodaKazuhiko KumeNaohisa UchimuraMasaaki KitadaTohru KodamaYuichi InoueSeiji NishinoKazuo MishimaKatsushi TokunagaMakoto Honda
Published in: NPJ genomic medicine (2022)
Idiopathic hypersomnia (IH) is a rare, heterogeneous sleep disorder characterized by excessive daytime sleepiness. In contrast to narcolepsy type 1, which is a well-defined type of central disorders of hypersomnolence, the etiology of IH is poorly understood. No susceptibility loci associated with IH have been clearly identified, despite the tendency for familial aggregation of IH. We performed a variation screening of the prepro-orexin/hypocretin and orexin receptors genes and an association study for IH in a Japanese population, with replication (598 patients and 9826 controls). We identified a rare missense variant (g.42184347T>C; p.Lys68Arg; rs537376938) in the cleavage site of prepro-orexin that was associated with IH (minor allele frequency of 1.67% in cases versus 0.32% in controls, P = 2.7 × 10 -8 , odds ratio = 5.36). Two forms of orexin (orexin-A and -B) are generated from cleavage of one precursor peptide, prepro-orexin. The difference in cleavage efficiency between wild-type (Gly-Lys-Arg; GKR) and mutant (Gly-Arg-Arg; GRR) peptides was examined by assays using proprotein convertase subtilisin/kexin (PCSK) type 1 and PCSK type 2. In both PCSK1 and PCSK2 assays, the cleavage efficiency of the mutant peptide was lower than that of the wild-type peptide. We also confirmed that the prepro-orexin peptides themselves transmitted less signaling through orexin receptors than mature orexin-A and orexin-B peptides. These results indicate that a subgroup of IH is associated with decreased orexin signaling, which is believed to be a hallmark of narcolepsy type 1.
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