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RNA Binding Antagonizes Neurotoxic Phase Transitions of TDP-43.

Neuron. 2019-04; 
MannJacob R,GleixnerAmanda M,MaunaJocelyn C,GomesEdward,DeChellis-MarksMichael R,NeedhamPatrick G,CopleyKatie E,HurtleBryan,PortzBede,PylesNoah J,GuoLin,CalderChristopher B,WillsZachary P,PandeyUdai B,KoflerJulia K,BrodskyJeffrey L,ThathiahAmantha,ShorterJames,DonnellyChristoph
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Gene Synthesis 2’-OMe-RNA bait oligonucleotides, see Table S2 for sequences was from GenScript...RNA oligonucleotides with 2'OMe modifications were synthesized by GenScript (see Table S2 for sequence details). Get A Quote

摘要

TDP-43 proteinopathy is a pathological hallmark of amyotrophic lateral sclerosis and frontotemporal dementia where cytoplasmic TDP-43 inclusions are observed within degenerating regions of patient postmortem tissue. The mechanism by which TDP-43 aggregates has remained elusive due to technological limitations, which prevent the analysis of specific TDP-43 interactions in live cells. We present an optogenetic approach to reliably induce TDP-43 proteinopathy under spatiotemporal control. We show that the formation of pathologically relevant inclusions is driven by aberrant interactions between low-complexity domains of TDP-43 that are antagonized by RNA binding. Although stress granules are hypothesized to be a... More

关键词

ALS,FTD,LLPS,RBP,RNA binding protein,TDP-43,bait oligonucleotide,liquid-liquid phase separation,neurodegeneration,optoTDP43,proteinopathy,stress gra