作者
Manuel Irimia, Robert J Weatheritt, Jonathan D Ellis, Neelroop N Parikshak, Thomas Gonatopoulos-Pournatzis, Mariana Babor, Mathieu Quesnel-Vallières, Javier Tapial, Bushra Raj, Dave O’Hanlon, Miriam Barrios-Rodiles, Michael JE Sternberg, Sabine P Cordes, Frederick P Roth, Jeffrey L Wrana, Daniel H Geschwind, Benjamin J Blencowe
发表日期
2014/12/18
期刊
Cell
卷号
159
期号
7
页码范围
1511-1523
出版商
Elsevier
简介
Alternative splicing (AS) generates vast transcriptomic and proteomic complexity. However, which of the myriad of detected AS events provide important biological functions is not well understood. Here, we define the largest program of functionally coordinated, neural-regulated AS described to date in mammals. Relative to all other types of AS within this program, 3-15 nucleotide "microexons" display the most striking evolutionary conservation and switch-like regulation. These microexons modulate the function of interaction domains of proteins involved in neurogenesis. Most neural microexons are regulated by the neuronal-specific splicing factor nSR100/SRRM4, through its binding to adjacent intronic enhancer motifs. Neural microexons are frequently misregulated in the brains of individuals with autism spectrum disorder, and this misregulation is associated with reduced levels of nSR100. The results thus reveal …
学术搜索中的文章
M Irimia, RJ Weatheritt, JD Ellis, NN Parikshak… - Cell, 2014