Stromal reprogramming by FAK inhibition overcomes radiation resistance to allow for immune priming and response to checkpoint blockade

Varintra E Lander, Jad I Belle, Natalie L Kingston, John M Herndon, Graham D Hogg, Xiuting Liu, Liang-I Kang, Brett L Knolhoff, Savannah J Bogner, John M Baer, Chong Zuo, Nick Borcherding, Daniel P Lander, Cedric Mpoy, Jalen Scott, Michael Zahner, Buck E Rogers, Julie K Schwarz, Hyun Kim, David G DeNardo
December 2022
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Abstract

The effects of radiotherapy (RT) on tumor immunity in pancreatic ductal adenocarcinoma (PDAC) are not well understood. To better understand if RT can prime antigen-specific T-cell responses, we analyzed human PDAC tissues and mouse models. In both settings, there was little evidence of RT-induced T-cell priming. Using in vitro systems, we found that tumor-stromal components, including fibroblasts and collagen, cooperate to blunt RT efficacy and impair RT-induced interferon signaling. Focal adhesion kinase (FAK) inhibition rescued RT efficacy in vitro and in vivo, leading to tumor regression, T-cell priming, and enhanced long-term survival in PDAC mouse models. Based on these data, we initiated a clinical trial of defactinib in combination with stereotactic body RT in patients with PDAC (NCT04331041). Analysis of PDAC tissues from these patients showed stromal reprogramming mirroring our findings in genetically engineered mouse models. Finally, the addition of checkpoint immunotherapy to RT and FAK inhibition in animal models led to complete tumor regression and long-term survival.

Type
Journal article
Publication
In Cancer Discovery
cancer microenvironment Single-Cell
Nick Borcherding
Nick Borcherding
Assistant Professor

My research includes systems immunology, single-cell sequencing technology, and computational frameworks.

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