DNAzyme Cleavage of CAG Repeat RNA in Polyglutamine Diseases

被引:0
|
作者
Nan Zhang
Brittani Bewick
Jason Schultz
Anjana Tiwari
Robert Krencik
Aijun Zhang
Kaho Adachi
Guangbin Xia
Kyuson Yun
Partha Sarkar
Tetsuo Ashizawa
机构
[1] Neuroscience Program,Department of Neurology
[2] Houston Methodist Research Institute,Center for Neuroregeneration, Department of Neurosurgery
[3] Houston Methodist Research Institute,Center for Bioenergetics, Department of Neurosurgery
[4] Houston Methodist Research Institute,Department of Molecular and Cell Biology
[5] UC-Berkeley,Department of Neurology and Department of Neuroscience, Cell Biology and Anatomy
[6] Indiana University School of Medicine-Fort Wayne,undefined
[7] UTMB Health,undefined
来源
Neurotherapeutics | 2021年 / 18卷
关键词
DNAzyme; Polyglutamine; CAG repeats; Huntington’s disease; Spinocerebellar ataxia; Microsatellite expansion;
D O I
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中图分类号
学科分类号
摘要
CAG repeat expansion is the genetic cause of nine incurable polyglutamine (polyQ) diseases with neurodegenerative features. Silencing repeat RNA holds great therapeutic value. Here, we developed a repeat-based RNA-cleaving DNAzyme that catalyzes the destruction of expanded CAG repeat RNA of six polyQ diseases with high potency. DNAzyme preferentially cleaved the expanded allele in spinocerebellar ataxia type 1 (SCA1) cells. While cleavage was non-allele-specific for spinocerebellar ataxia type 3 (SCA3) cells, treatment of DNAzyme leads to improved cell viability without affecting mitochondrial metabolism or p62-dependent aggresome formation. DNAzyme appears to be stable in mouse brain for at least 1 month, and an intermediate dosage of DNAzyme in a SCA3 mouse model leads to a significant reduction of high molecular weight ATXN3 proteins. Our data suggest that DNAzyme is an effective RNA silencing molecule for potential treatment of multiple polyQ diseases.
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页码:1710 / 1728
页数:18
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