Loss of aly/ALYREF suppresses toxicity in both tau and TDP-43 models of neurodegeneration

被引:0
|
作者
Rebecca L. Kow
Aristide H. Black
Aleen D. Saxton
Nicole F. Liachko
Brian C. Kraemer
机构
[1] Veterans Affairs Puget Sound Health Care System,Geriatrics Research Education and Clinical Center
[2] University of Washington,Division of Gerontology and Geriatric Medicine, Department of Medicine
[3] University of Washington,Department of Psychiatry and Behavioral Sciences
[4] University of Washington,Department of Laboratory Medicine and Pathology
来源
GeroScience | 2022年 / 44卷
关键词
Tau; TAR DNA-binding protein 43; TDP-43; ALYREF; MSUT2; Neurodegeneration;
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中图分类号
学科分类号
摘要
Neurodegenerative diseases with tau pathology, or tauopathies, include Alzheimer’s disease and related dementia disorders. Previous work has shown that loss of the poly(A) RNA-binding protein gene sut-2/MSUT2 strongly suppressed tauopathy in Caenorhabditis elegans, human cell culture, and mouse models of tauopathy. However, the mechanism of suppression is still unclear. Recent work has shown that MSUT2 protein interacts with the THO complex and ALYREF, which are components of the mRNA nuclear export complex. Additionally, previous work showed ALYREF homolog Ref1 modulates TDP-43 and G4C2 toxicity in Drosophila melanogaster models. We used transgenic C. elegans models of tau or TDP-43 toxicity to investigate the effects of loss of ALYREF function on tau and TDP-43 toxicity. In C. elegans, three genes are homologous to human ALYREF: aly-1, aly-2, and aly-3. We found that loss of C. elegans aly gene function, especially loss of both aly-2 and aly-3, suppressed tau-induced toxic phenotypes. Loss of aly-2 and aly-3 was also able to suppress TDP-43-induced locomotor behavior deficits. However, loss of aly-2 and aly-3 had divergent effects on mRNA and protein levels as total tau protein levels were reduced while mRNA levels were increased, but no significant effects were seen on total TDP-43 protein or mRNA levels. Our results suggest that although aly genes modulate both tau and TDP-43-induced toxicity phenotypes, the molecular mechanisms of suppression are different and separated from impacts on mRNA and protein levels. Altogether, this study highlights the importance of elucidating RNA-related mechanisms in both tau and TDP-43-induced toxicity.
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页码:747 / 761
页数:14
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