- 作者:Ralph Gruber1 ; Richard Panayiotou2 ; Emma Nye3 ; Bradley Spencer-Dene3 ; Gordon Stamp3 ; Axel Behrens1 ; 4 ; Axel.Behrens@crick.ac.uk" class="auth_mail" title="E-mail the corresponding author
- 关键词:PanINs ; Pancreatic Cancer Progression ; Mouse Model ; Inflammation
- 刊名:Gastroenterology
- 出版年:2016
- 出版时间:September 2016
- 年:2016
- 卷:151
- 期:3
- 页码:526-539
- 全文大小:6392 K
Methods
We generated mice carrying conditional alleles of Yap1 and Taz and disrupted Yap1 and Taz using a Cre-lox recombination strategy in adult mouse pancreatic acinar cells (Yap1fl/fl;Tazfl/fl;Ela1-CreERT2). We crossed these mice with LSL-KrasG12D mice, which express a constitutively active form of KRAS after Cre recombination. Pancreatic tumor initiation and progression were analyzed after chemically induced pancreatitis. We analyzed pancreatic tissues from patients with pancreatitis or PDAC by immunohistochemistry.
Results
Oncogenic activation of KRAS in normal, untransformed acinar cells in the pancreatic tissues of mice resulted in increased levels of pancreatitis-induced ADM. Expression of the constitutive active form of KRAS in this system led to activation of the transcriptional regulators YAP1 and TAZ; their function was required for pancreatitis-induced ADM in mice. The JAK–STAT3 pathway was a downstream effector of KRAS signaling via YAP1 and TAZ. YAP1 and TAZ directly mediated transcriptional activation of several genes in the JAK–STAT3 signaling pathway; this could be a mechanism by which acinar cells that express activated KRAS become susceptible to inflammation.
Conclusions
We identified a mechanism by which oncogenic KRAS facilitates ADM and thereby generates the cells that initiate neoplastic progression. This process involves activation of YAP1 and TAZ in acinar cells, which up-regulate JAK–STAT3 signaling to promote development of PDAC in mice.