Increased hippocampal excitability in miR-324-null mice

Author:

Hayman Dan J.,Modebadze Tamara,Charlton Sarah,Cheung Kat,Soul Jamie,Lin Hua,Hao Yao,Miles Colin G.,Tsompani Dimitra,Jackson Robert M.,Briggs Michael D.,Piróg Katarzyna A.,Clark Ian M.,Barter Matt J.,Clowry Gavin J.,LeBeau Fiona E. N.,Young David A.

Abstract

AbstractMicroRNAs are non-coding RNAs that act to downregulate the expression of target genes by translational repression and degradation of messenger RNA molecules. Individual microRNAs have the ability to specifically target a wide array of gene transcripts, therefore allowing each microRNA to play key roles in multiple biological pathways. miR-324 is a microRNA predicted to target thousands of RNA transcripts and is expressed far more highly in the brain than in any other tissue, suggesting that it may play a role in one or multiple neurological pathways. Here we present data from the first global miR-324-null mice, in which increased excitability and interictal discharges were identified in vitro in the hippocampus. RNA sequencing was used to identify differentially expressed genes in miR-324-null mice which may contribute to this increased hippocampal excitability, and 3′UTR luciferase assays and western blotting revealed that two of these, Suox and Cd300lf, are novel direct targets of miR-324. Characterisation of microRNAs that produce an effect on neurological activity, such as miR-324, and identification of the pathways they regulate will allow a better understanding of the processes involved in normal neurological function and in turn may present novel pharmaceutical targets in treating neurological disease.

Funder

Medical Research Council

Dunhill Medical Trust

Versus Arthritis

JGW Patterson Foundation

NIHR Newcastle Biomedical Research Centre

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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