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Cited 22 time in webofscience Cited 24 time in scopus
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Upregulation of ATG7 attenuates motor neuron dysfunction associated with depletion of TARDBP/TDP-43

Authors
Donde, AneeshSun, MingkuanJeong, Yun HaWen, XinruiLing, JonathanLin, SophieBraunstein, KerstinNie, ShukeWang, ShengChen, LiamWong, Philip C.
Issue Date
Apr-2020
Publisher
TAYLOR & FRANCIS INC
Keywords
ALS; ATG7; autophagy; Drosophila; frontotemporal dementia; mouse; SQSTM1; p62; TARDBP; TDP-43
Citation
AUTOPHAGY, v.16, no.4, pp.672 - 682
Journal Title
AUTOPHAGY
Volume
16
Number
4
Start Page
672
End Page
682
URI
http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/630
DOI
10.1080/15548627.2019.1635379
ISSN
1554-8627
Abstract
A shared neuropathological hallmark in amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) is nuclear clearance and cytoplasmic aggregation of TARDBP/TDP-43 (TAR DNA binding protein). We previously showed that the ability of TARDBP to repress nonconserved cryptic exons was impaired in brains of patients with ALS and FTD, suggesting that its nuclear depletion contributes to neurodegeneration. However, the critical pathways impacted by the failure to repress cryptic exons that may contribute to neurodegeneration remain undefined. Here, we report that transcriptome analysis of TARDBP-deficient neurons revealed downregulation of ATG7, a critical gene required for macroautophagy/autophagy. Mouse and Drosophila models lacking TARDBP/TBPH in motor neurons exhibiting age-dependent neurodegeneration and motor deficits showed reduction of ATG7 and accumulation of SQSTM1/p62 inclusions. Importantly, genetic upregulation of the autophagy pathway improved motor function and survival in TBPH-deficient flies. Together with our observation that ATG7 is reduced in ALS-FTD brain tissues, these findings identify the autophagy pathway as one key effector of nuclear depletion of TARDBP that contributes to neurodegeneration. We thus suggest that the autophagy pathway is a therapeutic target for ALS-FTD and other disorders exhibiting TARDBP pathology.
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연구본부 (퇴행성뇌질환 연구그룹)
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