SOX9 triggers different epithelial to mesenchymal transition states to promote pancreatic cancer progression

Background: Pancreatic ductal adenocarcinoma (PDAC) is one of the most lethal cancers mainly due to spatial obstacles to complete resection, early metastasis and therapy resistance. The molecular events accompanying PDAC progression remain poorly understood. SOX9 is required for maintaining the panc...

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Autores: Carrasco-Garcia, E. (Estefania)|||/items/ba45a153-c596-454a-9ed5-a85db319c200, Lopez-Serra, L. (Lidia)|||/items/68c2b4fa-baba-41c0-8c42-d7ca93647d40, Moncho-Amor, V. (Veronica)|||/items/a6a9757a-0135-4ffe-8b9b-c4af8b7bddcb, Carazo-Melo, F.(Fernando)|||/items/23abbe07-938d-434d-9483-864ef915f6b5, Aldaz, P. (Paula)|||/items/b9c0f230-0f8e-46a0-94e8-b85079ff62d9, Collado, M. (Manuel)|||/items/162d4146-4fa1-4f12-b63d-d4cd694a53ac, Bell, D. (Donald)|||/items/962fa51f-6f79-4ff9-a611-8585c695b9df, Gaafar, A. (Ayman)|||/items/8f807755-ad47-46f9-84b3-62d8ea4923f4, Karamitopoulou, E. (Eva)|||/items/209982f5-e411-4379-9574-1b31a27eaaa6, Tzankov, A. (Alexandar)|||/items/ceb514e7-d807-42da-a3de-52ae27771b52, Hidalgo, M. (Manuel)|||/items/82c25e37-ac17-42a8-89b6-9314a92a4b74, Rubio-Díaz-Cordovés, A. (Ángel)|||/items/7d740e1e-38db-46ea-9834-8c61aa6eedee, Serrano, M. (Manuel)|||/items/eab5ede4-df61-4fcb-ac7f-4c22d34c4030, Lawrie, C.H. (Charles H.)|||/items/30e8e5fb-0147-456d-8aa0-5bd189b30229, Lovell-Badge, R. (Robin)|||/items/c0ce18f2-245e-4e49-9835-0785934bce20, Matheu, A. (Ander)|||/items/79d399df-1789-495b-af31-49af2b5ea9e0
Tipo de recurso: artículo
Fecha de publicación:2022
País:España
Institución:Consejo Superior de Investigaciones Científicas (CSIC)
Repositorio:Dadun. Depósito Académico Digital de la Universidad de Navarra
Idioma:inglés
OAI Identifier:oai:dadun.unav.edu:10171/123732
Acceso en línea:https://hdl.handle.net/10171/123732
Access Level:acceso abierto
Palabra clave:EMT
SOX9
Chemoresistance
Metastasis
Pancreatic cancer
Plasticity
Descripción
Sumario:Background: Pancreatic ductal adenocarcinoma (PDAC) is one of the most lethal cancers mainly due to spatial obstacles to complete resection, early metastasis and therapy resistance. The molecular events accompanying PDAC progression remain poorly understood. SOX9 is required for maintaining the pancreatic ductal identity and it is involved in the initiation of pancreatic cancer. In addition, SOX9 is a transcription factor linked to stem cell activity and is commonly overexpressed in solid cancers. It cooperates with Snail/Slug to induce epithelial-mesenchymal transition (EMT) during neural development and in diseases such as organ fibrosis or different types of cancer. Methods: We investigated the roles of SOX9 in pancreatic tumor cell plasticity, metastatic dissemination and chemoresistance using pancreatic cancer cell lines as well as mouse embryo fibroblasts. In addition, we characterized the clinical relevance of SOX9 in pancreatic cancer using human biopsies. Results: Gain- and loss-of-function of SOX9 in PDAC cells revealed that high levels of SOX9 increased migration and invasion, and promoted EMT and metastatic dissemination, whilst SOX9 silencing resulted in metastasis inhibition, along with a phenotypic reversion to epithelial features and loss of stemness potential. In both contexts, EMT factors were not altered. Moreover, high levels of SOX9 promoted resistance to gemcitabine. In contrast, overexpression of SOX9 was sufficient to promote metastatic potential in K-Ras transformed MEFs, triggering EMT associated with Snail/Slug activity. In clinical samples, SOX9 expression was analyzed in 198 PDAC cases by immunohistochemistry and in 53 patient derived xenografts (PDXs). SOX9 was overexpressed in primary adenocarcinomas and particularly in metastases. Notably, SOX9 expression correlated with high vimentin and low E-cadherin expression. Conclusions: Our results indicate that SOX9 facilitates PDAC progression and metastasis by triggering stemness and EMT.