Litcius/Paper detail

RNA editing of microtubule-associated protein tau circular RNAs promotes their translation and tau tangle formation

Justin R. Welden, Giorgi Margvelani, Karol Andrea Arizaca Maquera, Bhavani Gudlavalleti, Sandra C. Miranda Sardón, Alexandre Rosa Campos, Noémie Robil, Daniel C. Lee, Alvaro G. Hernandez, Wang‐Xia Wang, Jing Di, Pierre de la Grange, Peter T. Nelson, Stefan Stamm

2022Nucleic Acids Research43 citationsDOIOpen Access PDF

Abstract

Aggregation of the microtubule-associated protein tau characterizes tauopathies, including Alzheimer's disease and frontotemporal lobar degeneration (FTLD-Tau). Gene expression regulation of tau is complex and incompletely understood. Here we report that the human tau gene (MAPT) generates two circular RNAs (circRNAs) through backsplicing of exon 12 to either exon 7 (12→7 circRNA) or exon 10 (12→10 circRNA). Both circRNAs lack stop codons. The 12→7 circRNA contains one start codon and is translated in a rolling circle, generating a protein consisting of multimers of the microtubule-binding repeats R1-R4. For the 12→10 circRNA, a start codon can be introduced by two FTLD-Tau mutations, generating a protein consisting of multimers of the microtubule-binding repeats R2-R4, suggesting that mutations causing FTLD may act in part through tau circRNAs. Adenosine to inosine RNA editing dramatically increases translation of circRNAs and, in the 12→10 circRNA, RNA editing generates a translational start codon by changing AUA to AUI. Circular tau proteins self-aggregate and promote aggregation of linear tau proteins. Our data indicate that adenosine to inosine RNA editing initiates translation of human circular tau RNAs, which may contribute to tauopathies.

Topics & Concepts

BiologyExonCircular RNATranslation (biology)RNAMicrotubuleGeneticsRNA-binding proteinTau proteinRNA editingGeneRNA splicingCell biologyMessenger RNAAlzheimer's diseaseMedicineDiseasePathologyRNA regulation and diseaseRNA Research and SplicingCircular RNAs in diseases