结蛋白
中间灯丝
损失函数
线粒体
热休克蛋白
细胞生物学
生物
突变
基因
遗传学
表型
细胞骨架
免疫学
免疫组织化学
细胞
波形蛋白
作者
Maike Stentenbach,Laetitia A. Hughes,Samuel V. Fagan,Blake Payne,Danielle L. Rudler,Stefan J. Siira,Tim McCubbin,A Chopin,Kara L. Perks,Judith A. Ermer,J.H. Hendry,Tze‐Kiong Er,Shanti Balasubramaniam,Joel A. Eliades,Livia C. Hool,Nicolle H. Packer,Edward S. X. Moh,Benjamin Scott Padman,Oliver Rackham,Aleksandra Filipovska
标识
DOI:10.1038/s41467-025-60563-1
摘要
Mutations in the TANGO2 gene cause an autosomal recessive disorder characterised by developmental delay, stress-induced episodic rhabdomyolysis, and cardiac arrhythmias along with severe metabolic crises. Although TANGO2 mutations result in a well characterised disease pathology, the function of TANGO2 is still unknown. To investigate the function of TANGO2, we knocked out the TANGO2 gene in human cells and mice. We identify that loss of TANGO2 impairs intermediate filament structure, resulting in fragmented mitochondrial networks and formation of cup-like mitochondria. In male mice, loss of TANGO2 caused heart defects, reduced muscle function and glucose intolerance by remodelling of intermediate filaments, which altered the mitochondrial and cytoplasmic proteomes, N-glycosylation and nucleocytoplasmic O-GlcNAcylation. We identify that TANGO2 binds the small heat shock protein crystallin alpha B (CRYAB) to prevent the aggregation of the intermediate filament desmin and in the absence of TANGO2, mice develop desminopathy, which is consistent with features found in patients carrying mutations in either desmin or CRYAB.
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