Nuclear RNA foci from C9ORF72 expansion mutation form paraspeckle-like bodies

Abstract

The GGGGCC (G₄C₂) repeat expansion mutation in the C9ORF72 gene is the most common genetic cause of frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS). Transcription of the repeat and formation of nuclear RNA foci, which sequester specific RNA-binding proteins, is one of the possible pathological mechanisms. Here, we show that (G₄C₂) _n repeat RNA predominantly associates with essential paraspeckle proteins SFPQ, NONO, RBM14, FUS and hnRNPH and colocalizes with known paraspeckle-associated RNA hLinc-p21. As formation of paraspeckles in motor neurons has been associated with early phases of ALS, we investigated the extent of similarity between paraspeckles and (G₄C₂) _n RNA foci. Overexpression of (G₄C₂)₇₂ RNA results in their increased number and colocalization with SFPQ-stained nuclear bodies. These paraspeckle-like (G₄C₂)₇₂ RNA foci form independently of the known paraspeckle scaffold, the long non-coding RNA NEAT1 Moreover, the knockdown of SFPQ protein in C9ORF72 expansion mutation-positive fibroblasts significantly reduces the number of (G₄C₂) _n RNA foci. In conclusion, (G₄C₂) _n RNA foci have characteristics of paraspeckles, which suggests that both RNA foci and paraspeckles play roles in FTD and ALS, and implies approaches for regulation of their formation.

Keywords: C9ORF72; NEAT1; Paraspeckles; RNA foci; SFPQ.