Litcius/Paper detail

Ribosome profiling reveals novel regulation of <i>C9ORF72</i> GGGGCC repeat-containing RNA translation

Heleen M. van ‘t Spijker, Emily E. Stackpole, Sandra Almeida, Olga Katsara, Botao Liu, Kuang Shen, Robert J. Schneider, Fen‐Biao Gao, Joel D. Richter

2021RNA29 citationsDOIOpen Access PDF

Abstract

GGGGCC (G 4 C 2 ) repeat expansion in the first intron of C9ORF72 causes amyotrophic lateral sclerosis and frontotemporal dementia. Repeat-containing RNA is translated into dipeptide repeat (DPR) proteins, some of which are neurotoxic. Using dynamic ribosome profiling, we identified three translation initiation sites in the intron upstream of ( G 4 C 2 ) repeats; these sites are detected irrespective of the presence or absence of the repeats. During translocation, ribosomes appear to be stalled on the repeats. An AUG in the preceding C9ORF72 exon initiates a uORF that inhibits downstream translation. Polysome isolation indicates that unspliced ( G 4 C 2 ) repeat-containing RNA is a substrate for DPR protein synthesis. ( G 4 C 2 ) repeat-containing RNA translation is 5′ cap-independent but inhibited by the initiation factor DAP5, suggesting an interplay with uORF function. These results define novel translational mechanisms of expanded ( G 4 C 2 ) repeat-containing RNA in disease.

Topics & Concepts

BiologyRibosome profilingTranslation (biology)RNAComputational biologyGeneticsRibosomeProfiling (computer programming)C9orf72Molecular biologyMessenger RNAGeneTrinucleotide repeat expansionAlleleOperating systemComputer scienceAmyotrophic Lateral Sclerosis ResearchRNA and protein synthesis mechanismsRNA Research and Splicing