- Liu, Chen;
- Karam, Rachid;
- Zhou, YingQi;
- Su, Fang;
- Ji, Yuan;
- Li, Gang;
- Xu, GuoTong;
- Lu, LiXia;
- Wang, ChongRen;
- Song, MeiYi;
- Zhu, JingPing;
- Wang, YiRan;
- Zhao, YiFan;
- Foo, Wai Chin;
- Zuo, MingXin;
- Valasek, Mark A;
- Javle, Milind;
- Wilkinson, Miles F;
- Lu, YanJun
Pancreatic adenosquamous carcinoma (ASC) is an enigmatic and aggressive tumor that has a worse prognosis and higher metastatic potential than its adenocarcinoma counterpart. Here we report that ASC tumors frequently harbor somatically acquired mutations in the UPF1 gene, which encodes the core component of the nonsense-mediated RNA decay (NMD) pathway. These tumor-specific mutations alter UPF1 RNA splicing and perturb NMD, leading to upregulated levels of NMD substrate mRNAs. UPF1 mutations are, to our knowledge, the first known unique molecular signatures of pancreatic ASC.