作者
Vanessa Königs, Camila O Freitas Machado, Benjamin Arnold, Nicole Blümel, Anfisa Solovyeva, Sinah Löbbert, Michal Schafranek, Igor Ruiz de los Mozos, Ilka Wittig, François McNicoll, Michaela Schulz, Marcel H, Müller-McNicoll
发表日期
2020/3/2
期刊
Nature Structural and Molecular Biology
简介
SRSF7 is an essential RNA-binding protein whose misexpression promotes cancer. Here, we describe how SRSF7 maintains its protein homeostasis in murine P19 cells using an intricate negative feedback mechanism. SRSF7 binding to its premessenger RNA promotes inclusion of a poison cassette exon and transcript degradation via nonsense-mediated decay (NMD). However, elevated SRSF7 levels inhibit NMD and promote translation of two protein halves, termed Split-ORFs, from the bicistronic SRSF7-PCE transcript. The first half acts as dominant-negative isoform suppressing poison cassette exon inclusion and instead promoting the retention of flanking introns containing repeated SRSF7 binding sites. Massive SRSF7 binding to these sites and its oligomerization promote the assembly of large nuclear bodies, which sequester SRSF7 transcripts at their transcription site, preventing their export and restoring …
学术搜索中的文章
V Königs, C de Oliveira Freitas Machado, B Arnold… - Nature structural & molecular biology, 2020