The parkin V380L variant is a genetic modifier of Machado–Joseph disease with impact on mitophagy

IF 9.3 1区 医学 Q1 CLINICAL NEUROLOGY
Jonasz J. Weber, Leah Czisch, Priscila Pereira Sena, Florian Fath, Chrisovalantou Huridou, Natasa Schwarz, Rana D. Incebacak Eltemur, Anna Würth, Daniel Weishäupl, Miriam Döcker, Gunnar Blumenstock, Sandra Martins, Jorge Sequeiros, Guy A. Rouleau, Laura Bannach Jardim, Maria-Luiza Saraiva-Pereira, Marcondes C. França Jr., Carlos R. Gordon, Roy Zaltzman, Mario R. Cornejo-Olivas, Bart P. C. van de Warrenburg, Alexandra Durr, Alexis Brice, Peter Bauer, Thomas Klockgether, Ludger Schöls, Olaf Riess, The EUROSCA Network, Thorsten Schmidt
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Abstract

Machado–Joseph disease (MJD) is an autosomal dominant neurodegenerative spinocerebellar ataxia caused by a polyglutamine-coding CAG repeat expansion in the ATXN3 gene. While the CAG length correlates negatively with the age at onset, it accounts for approximately 50% of its variability only. Despite larger efforts in identifying contributing genetic factors, candidate genes with a robust and plausible impact on the molecular pathogenesis of MJD are scarce. Therefore, we analysed missense single nucleotide polymorphism variants in the PRKN gene encoding the Parkinson's disease-associated E3 ubiquitin ligase parkin, which is a well-described interaction partner of the MJD protein ataxin-3, a deubiquitinase. By performing a correlation analysis in the to-date largest MJD cohort of more than 900 individuals, we identified the V380L variant as a relevant factor, decreasing the age at onset by 3 years in homozygous carriers. Functional analysis in an MJD cell model demonstrated that parkin V380L did not modulate soluble or aggregate levels of ataxin-3 but reduced the interaction of the two proteins. Moreover, the presence of parkin V380L interfered with the execution of mitophagy—the autophagic removal of surplus or damaged mitochondria—thereby compromising cell viability. In summary, we identified the V380L variant in parkin as a genetic modifier of MJD, with negative repercussions on its molecular pathogenesis and disease age at onset.

Abstract Image

Parkin V380L 变体是马查多-约瑟夫病的遗传修饰因子,对有丝分裂有影响。
马查多-约瑟夫病(MJD)是一种常染色体显性神经退行性脊髓小脑共济失调症,由 ATXN3 基因中多聚谷氨酰胺编码的 CAG 重复扩增引起。虽然CAG长度与发病年龄呈负相关,但只占其变异性的约50%。尽管在确定遗传因素方面做了大量工作,但对 MJD 分子发病机制具有可靠和可信影响的候选基因仍然很少。因此,我们分析了编码帕金森病相关 E3 泛素连接酶 parkin 的 PRKN 基因中的错义单核苷酸多态性变异。通过对迄今为止最大的由 900 多人组成的 MJD 群体进行相关性分析,我们发现 V380L 变异是一个相关因素,它使同卵携带者的发病年龄降低了 3 岁。在一个 MJD 细胞模型中进行的功能分析表明,parkin V380L 不会调节共济失调蛋白-3 的可溶性或聚集水平,但会降低这两种蛋白的相互作用。此外,parkin V380L 的存在干扰了有丝分裂--自噬清除多余或受损线粒体--的执行,从而损害了细胞的活力。总之,我们发现 Parkin V380L 变体是 MJD 的遗传修饰因子,对其分子发病机制和发病年龄有负面影响。
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来源期刊
Acta Neuropathologica
Acta Neuropathologica 医学-病理学
CiteScore
23.70
自引率
3.90%
发文量
118
审稿时长
4-8 weeks
期刊介绍: Acta Neuropathologica publishes top-quality papers on the pathology of neurological diseases and experimental studies on molecular and cellular mechanisms using in vitro and in vivo models, ideally validated by analysis of human tissues. The journal accepts Original Papers, Review Articles, Case Reports, and Scientific Correspondence (Letters). Manuscripts must adhere to ethical standards, including review by appropriate ethics committees for human studies and compliance with principles of laboratory animal care for animal experiments. Failure to comply may result in rejection of the manuscript, and authors are responsible for ensuring accuracy and adherence to these requirements.
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