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Publication : TAp73 loss favors Smad-independent TGF-β signaling that drives EMT in pancreatic ductal adenocarcinoma.

First Author  Thakur AK Year  2016
Journal  Cell Death Differ Volume  23
Issue  8 Pages  1358-70
PubMed ID  26943320 Mgi Jnum  J:259266
Mgi Id  MGI:6140776 Doi  10.1038/cdd.2016.18
Citation  Thakur AK, et al. (2016) TAp73 loss favors Smad-independent TGF-beta signaling that drives EMT in pancreatic ductal adenocarcinoma. Cell Death Differ 23(8):1358-70
abstractText  Advances made in pancreatic cancer therapy have been far from sufficient and have allowed only a slight improvement in global survival of patients with pancreatic ductal adenocarcinoma (PDA). Recent progresses in chemotherapy have offered some hope for an otherwise gloomy outlook, however, only a limited number of patients are eligible because of important cytotoxicity. In this context, enhancing our knowledge on PDA initiation and evolution is crucial to highlight certain weaknesses on which to specifically target therapy. We found that loss of transcriptionally active p73 (TAp73), a p53 family member, impacted PDA development. In two relevant and specific engineered pancreatic cancer mouse models, we observed that TAp73 deficiency reduced survival and enhanced epithelial-to-mesenchymal transition (EMT). Through proteomic analysis of conditioned media from TAp73 wild-type (WT) and deficient pancreatic tumor cells, we identified a secreted protein, biglycan (BGN), which is necessary and sufficient to mediate this pro-EMT effect. Interestingly, BGN is modulated by and modulates the transforming growth factor-beta (TGF-beta) pathway, a key regulator of the EMT process. We further examined this link and revealed that TAp73 impacts the TGF-beta pathway by direct regulation of BGN expression and Sma and Mad-related proteins (SMADs) expression/activity. Absence of TAp73 leads to activation of TGF-beta signaling through a SMAD-independent pathway, favoring oncogenic TGF-beta effects and EMT. Altogether, our data highlight the implication of TAp73 in the aggressiveness of pancreatic carcinogenesis through modulation of the TGF-beta signaling. By suggesting TAp73 as a predictive marker for response to TGF-beta inhibitors, our study could improve the classification of PDA patients with a view to offering combined therapy involving TGF-beta inhibitors.
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