作者
Tiffany Y-T Hsu, Lukas M Simon, Nicholas J Neill, Richard Marcotte, Azin Sayad, Christopher S Bland, Gloria V Echeverria, Tingting Sun, Sarah J Kurley, Siddhartha Tyagi, Kristen L Karlin, Rocio Dominguez-Vidaña, Jessica D Hartman, Alexander Renwick, Kathleen Scorsone, Ronald J Bernardi, Samuel O Skinner, Antrix Jain, Mayra Orellana, Chandraiah Lagisetti, Ido Golding, Sung Y Jung, Joel R Neilson, Xiang H-F Zhang, Thomas A Cooper, Thomas R Webb, Benjamin G Neel, Chad A Shaw, Thomas F Westbrook
发表日期
2015/9/17
期刊
Nature
卷号
525
期号
7569
页码范围
384-388
出版商
Nature Publishing Group UK
简介
MYC (also known as c-MYC) overexpression or hyperactivation is one of the most common drivers of human cancer. Despite intensive study, the MYC oncogene remains recalcitrant to therapeutic inhibition. MYC is a transcription factor, and many of its pro-tumorigenic functions have been attributed to its ability to regulate gene expression programs,,. Notably, oncogenic MYC activation has also been shown to increase total RNA and protein production in many tissue and disease contexts,,,. While such increases in RNA and protein production may endow cancer cells with pro-tumour hallmarks, this increase in synthesis may also generate new or heightened burden on MYC-driven cancer cells to process these macromolecules properly. Here we discover that the spliceosome is a new target of oncogenic stress in MYC-driven cancers. We identify BUD31 as a MYC-synthetic lethal gene in human mammary epithelial …
学术搜索中的文章
TYT Hsu, LM Simon, NJ Neill, R Marcotte, A Sayad… - Nature, 2015