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VPS35 and DNAJC13 disease-causing variants in essential tremor

机译:VPS35和DNAJC13导致原发性震颤的疾病

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Exome-sequencing analyses have identified vacuolar protein sorting 35 homolog (VPS35) and DnaJ (Hsp40) homolog, subfamily C, member 13 (DNAJC13) harboring disease-causing variants for Parkinson disease (PD). Owing to the suggested clinical, pathological and genetic overlap between PD and essential tremor (ET) we assessed the presence of two VPS35 and DNAJC13 disease-causing variants in ET patients. TaqMan probes were used to genotype VPS35 c.1858G > A (p.(D620N)) (rs188286943) and DNAJC13 c.2564A > G (p.(N855S)) (rs387907571) in 571 ET patients of European descent, and microsatellite markers were used to define the disease haplotype in variant carriers. Genotyping of DNAJC13 identified two ET patients harboring the c.2564A > G (p.( N855S)) variant previously identified in PD patients. Both patients appear to share the disease haplotype previously reported. ET patients with the VPS35 c.1858G > A (p.(D620N)) variants were not observed. Although a genetic link between PD and ET has been suggested, DNAJC13 c.2564A > G (p.(N855S)) represents the first disease-causing variant identified in both, and suggests the regulation of clathrin dynamics and endosomal trafficking in the pathophysiology of a subset of ET patients.
机译:外显子组测序分析已鉴定出空泡蛋白分选的35个同源物(VPS35)和DnaJ(Hsp40)同源物,亚家族C,成员13(DNAJC13),具有帕金森病(PD)的致病变体。由于PD和原发性震颤(ET)之间存在临床,病理和遗传上的重叠,我们评估了ET患者中存在两种导致VPS35和DNAJC13疾病的变异体。使用TaqMan探针对571名欧洲血统的ET患者的VPS35 c.1858G> A(p。(D620N))(rs188286943)和DNAJC13 c.2564A> G(p。(N855S))(rs387907571)进行基因分型,并使用微卫星标记用来定义变异携带者中的疾病单倍型。 DNAJC13的基因分型确定了两名ET患者,这些患者先前曾在PD患者中发现了c.2564A> G(p。(N855S))变异。两名患者似乎共享先前报道的疾病单倍型。未观察到VPS35 c.1858G> A(p。(D620N))变异的ET患者。尽管已经提出了PD和ET之间的遗传联系,但DNAJC13 c.2564A> G(p。(N855S))代表了两者中鉴定出的第一个致病变体,并暗示了网格蛋白动力学的调控和内体运输在病理生理中的作用。一部分ET患者。

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