Dysregulated MiRNA Biogenesis Downstream of Cellular Stress and ALS-causing Mutations: a New Mechanism for ALS

Overview

Journal EMBO J

Specialties Biotechnology
Molecular Biology

Date 2015 Sep 3

PMID 26330466

Citations 112

Authors

Anna Emde

Chen Eitan

Lee-Loung Liou

Ryan T Libby

Natali Rivkin

Iddo Magen

Irit Reichenstein

Hagar Oppenheim

Raya Eilam

Aurelio Silvestroni

Betty Alajajian

Iddo Z Ben-Dov

Julianne Aebischer

Alon Savidor

Yishai Levin

Robert Sons

Scott M Hammond

John M Ravits

Thomas Moller

Eran Hornstein

Affiliations

Soon will be listed here.

Abstract

Interest in RNA dysfunction in amyotrophic lateral sclerosis (ALS) recently aroused upon discovering causative mutations in RNA-binding protein genes. Here, we show that extensive down-regulation of miRNA levels is a common molecular denominator for multiple forms of human ALS. We further demonstrate that pathogenic ALS-causing mutations are sufficient to inhibit miRNA biogenesis at the Dicing step. Abnormalities of the stress response are involved in the pathogenesis of neurodegeneration, including ALS. Accordingly, we describe a novel mechanism for modulating microRNA biogenesis under stress, involving stress granule formation and re-organization of DICER and AGO2 protein interactions with their partners. In line with this observation, enhancing DICER activity by a small molecule, enoxacin, is beneficial for neuromuscular function in two independent ALS mouse models. Characterizing miRNA biogenesis downstream of the stress response ties seemingly disparate pathways in neurodegeneration and further suggests that DICER and miRNAs affect neuronal integrity and are possible therapeutic targets.

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