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Targeting the VCP-binding motif of ataxin-3 improves phenotypes in Drosophila models of Spinocerebellar Ataxia Type 3

Neurobiol Dis. 2021-09; 
Sean L Johnson, Kozeta Libohova, Jessica R Blount, Alyson L Sujkowski, Matthew V Prifti, Wei-Ling Tsou, Sokol V Todi
Products/Services Used Details Operation
Gene Synthesis We used the company Genscript (genscript.com) to synthesize the VCP N-terminus cDNA as well as full-length fly VCP Get A Quote

摘要

Of the family of polyglutamine (polyQ) neurodegenerative diseases, Spinocerebellar Ataxia Type 3 (SCA3) is the most common. Like other polyQ diseases, SCA3 stems from abnormal expansions in the CAG triplet repeat of its disease gene resulting in elongated polyQ repeats within its protein, ataxin-3. Various ataxin-3 protein domains contribute to its toxicity, including the valosin-containing protein (VCP)-binding motif (VBM). We previously reported that VCP, a homo-hexameric protein, enhances pathogenic ataxin-3 aggregation and exacerbates its toxicity. These findings led us to explore the impact of targeting the SCA3 protein by utilizing a decoy protein comprising the N-terminus of VCP (N-VCP) that binds ataxin... More

關鍵詞

AAA ATPase, Ataxia, Ataxin-3, Deubiquitinase, Drosophila, Machado-Joseph Disease, Neurodegeneration, Polyglutamine, Spinocerebellar Ataxia Type 3, VCP/p97
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