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Mechanism of STMN2 cryptic splice-polyadenylation and its correction for TDP-43 proteinopathies.

Author: Acks Eitan
Agra de Almeida Quadros Ana
Artates Jonathan
Baughn Michael
Beccari Melinda
Bennett C
Bravo-Hernández Mariana
Chaturvedi Som
Cleveland Don
Gonzalo-Gil Elena
Jafar-Nejad Paayman
Lagier-Tourenne Clotilde
Ling Karen
Lutz Cathleen
López-Erauskin Jone
Maimon Roy
Melamed Zeev
Moore Stephen
Ndayambaje I
Presa Maximilliano
Rigo Frank
Taupin Vanessa
Vazquez-Sanchez Sonia
Zuberi Aamir
Publication venue: eScholarship, University of California
Publication date: 17/03/2023
Field of study

Loss of nuclear TDP-43 is a hallmark of neurodegeneration in TDP-43 proteinopathies, including amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). TDP-43 mislocalization results in cryptic splicing and polyadenylation of pre-messenger RNAs (pre-mRNAs) encoding stathmin-2 (also known as SCG10), a protein that is required for axonal regeneration. We found that TDP-43 binding to a GU-rich region sterically blocked recognition of the cryptic 3 splice site in STMN2 pre-mRNA. Targeting dCasRx or antisense oligonucleotides (ASOs) suppressed cryptic splicing, which restored axonal regeneration and stathmin-2-dependent lysosome trafficking in TDP-43-deficient human motor neurons. In mice that were gene-edited to contain human STMN2 cryptic splice-polyadenylation sequences, ASO injection into cerebral spinal fluid successfully corrected Stmn2 pre-mRNA misprocessing and restored stathmin-2 expression levels independently of TDP-43 binding

eScholarship - University of California

Mechanism of STMN2 cryptic splice-polyadenylation and its correction for TDP-43 proteinopathies

Author: Acks Eitan
Agra de Almeida Quadros Ana R
Artates Jonathan W
Baughn Michael W
Beccari Melinda S
Bennett C Frank
Bravo-Hernández Mariana
Chaturvedi Som
Cleveland Don W
Gonzalo-Gil Elena
Jafar-Nejad Paayman
Lagier-Tourenne Clotilde
Ling Karen
Lutz Cathleen
López-Erauskin Jone
Maimon Roy
Melamed Ze\u27ev
Moore Stephen
Ndayambaje I Sandra
Presa Maximiliano
Rigo Frank
Taupin Vanessa
Vazquez-Sanchez Sonia
Zuberi Aamir
Publication venue: The Mouseion at the JAXlibrary
Publication date: 17/03/2023
Field of study

Loss of nuclear TDP-43 is a hallmark of neurodegeneration in TDP-43 proteinopathies, including amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). TDP-43 mislocalization results in cryptic splicing and polyadenylation of pre–messenger RNAs (pre-mRNAs) encoding stathmin-2 (also known as SCG10), a protein that is required for axonal regeneration. We found that TDP-43 binding to a GU-rich region sterically blocked recognition of the cryptic 3′ splice site in STMN2 pre-mRNA. Targeting dCasRx or antisense oligonucleotides (ASOs) suppressed cryptic splicing, which restored axonal regeneration and stathmin-2–dependent lysosome trafficking in TDP-43–deficient human motor neurons. In mice that were gene-edited to contain human STMN2 cryptic splice-polyadenylation sequences, ASO injection into cerebral spinal fluid successfully corrected Stmn2 pre-mRNA misprocessing and restored stathmin-2 expression levels independently of TDP-43 binding

The Jackson Laboratory: The Mouseion at the JAXlibrary

eScholarship - University of California