Saa3 is a key mediator of the protumorigenic properties of cancer-associated fibroblasts in pancreatic tumors

Al-Shahrour, Fátima; Barbacid, Mariano; Blasco, María Teresa; Burdiel, Miranda; Cabras, Lavinia; Djurec, Magdolna; Espinet, Elisa; Graña, Osvaldo; Guerra, Carmen; Lee, Albert; Li, Jing; Liu, Zhaoqi; Martín-Díaz, Laura; Navas, Carolina; Rabadan, Raúl; Sainz, Bruno Jr.; Sprick, Martin R.; Sánchez-Bueno, Francisco; Troulé, Kevin; Trumpp, Andreas; Vallespinós, Mireia

Saa3 is a key mediator of the protumorigenic properties of cancer-associated fibroblasts in pancreatic tumors

Authors: Fátima Al-Shahrour
Mariano Barbacid
María Teresa Blasco
Miranda Burdiel
Lavinia Cabras
Magdolna Djurec
Elisa Espinet
Osvaldo Graña
Carmen Guerra
Albert Lee
Jing Li
Zhaoqi Liu
Laura Martín-Díaz
Carolina Navas
Raúl Rabadan
Bruno Jr. Sainz
Martin R. Sprick
Francisco Sánchez-Bueno
Kevin Troulé
Andreas Trumpp
Mireia Vallespinós
Publication date: 25 January 2022
Publisher: 'Proceedings of the National Academy of Sciences'
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Abstract

Pancreatic ductal adenocarcinoma (PDAC) is characterized by the presence of abundant desmoplastic stroma primarily composed of cancer-associated fibroblasts (CAFs). It is generally accepted that CAFs stimulate tumor progression and might be implicated in drug resistance and immunosuppression. Here, we have compared the transcriptional profile of PDGFRα+ CAFs isolated from genetically engineered mouse PDAC tumors with that of normal pancreatic fibroblasts to identify genes potentially implicated in their protumorigenic properties. We report that the most differentially expressed gene, Saa3, a member of the serum amyloid A (SAA) apolipoprotein family, is a key mediator of the protumorigenic activity of PDGFRα+ CAFs. Whereas Saa3-competent CAFs stimulate the growth of tumor cells in an orthotopic model, Saa3-null CAFs inhibit tumor growth. Saa3 also plays a role in the cross talk between CAFs and tumor cells. Ablation of Saa3 in pancreatic tumor cells makes them insensitive to the inhibitory effect of Saa3-null CAFs. As a consequence, germline ablation of Saa3 does not prevent PDAC development in mice. The protumorigenic activity of Saa3 in CAFs is mediated by Mpp6, a member of the palmitoylated membrane protein subfamily of the peripheral membrane-associated guanylate kinases (MAGUK). Finally, we interrogated whether these observations could be translated to a human scenario. Indeed, SAA1, the ortholog of murine Saa3, is overexpressed in human CAFs. Moreover, high levels of SAA1 in the stromal component correlate with worse survival. These findings support the concept that selective inhibition of SAA1 in CAFs may provide potential therapeutic benefit to PDAC patients.This work was supported by European Research Council Grants ERC-AG/250297-RAS AHEAD and ERC-AG/695566-THERACAN, Spanish Ministry of Economy and Competitiveness Grant SAF2014-59864-R, and Asociación Española contra el Cáncer Grant GC16173694BARB (to M. Barbacid). M.D. was supported by a fellowship from La Caixa International Fellowship Program. M. Barbacid is the recipient of an Endowed Chair from the AXA Research Fund

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