New insights into the responder/nonresponder divide in rectal cancer: Damage-induced Type I IFNs dictate treatment efficacy and can be targeted to enhance radiotherapy

Author:

Gerber Scott1,Uccello Taylor1,Lesch Maggie1,Kintzel Sarah1,Gradzewicz Lauren1,Lamrous Lillia1,Murphy Shawn1,Fleming Fergal1,Mills Bradley2,Murphy Joseph1,Hughson Angela1,Garrett-Larsen Jesse1,Qiu Haoming1,Drage Michael1,Ye Jian1,Gavras Nicholas1,Keeley David1,Love Tanzy1,Repasky Elizabeth3,Lord Edith4,Linehan David4

Affiliation:

1. University of Rochester School of Medicine and Dentistry

2. University of Rochester Medical Center

3. Roswell Park Comprehensive Cancer Center

4. University of Rochester

Abstract

Abstract Rectal cancer ranks as the second leading cause of cancer-related deaths. Neoadjuvant therapy for rectal cancer patients often results in individuals that respond well to therapy and those that respond poorly, requiring life-altering excision surgery. It is inadequately understood what dictates this responder/nonresponder divide. Our major aim is to identify what factors in the tumor microenvironment drive a fraction of rectal cancer patients to respond to radiotherapy. We also sought to distinguish potential biomarkers that would indicate a positive response to therapy and design combinatorial therapeutics to enhance radiotherapy efficacy. To address this, we developed an orthotopic murine model of rectal cancer treated with short course radiotherapy that recapitulates the bimodal response observed in the clinic. We utilized a robust combination of transcriptomics and protein analysis to identify differences between responding and nonresponding tumors. Our mouse model recapitulates human disease in which a fraction of tumors respond to radiotherapy (responders) while the majority are nonresponsive. We determined that responding tumors had increased damage-induced cell death, and a unique immune-activation signature associated with tumor-associated macrophages, cancer-associated fibroblasts, and CD8+ T cells. This signature was dependent on radiation-induced increases of Type I interferons (IFNs). We investigated a therapeutic approach targeting the cGAS/STING pathway and demonstrated improved response rate following radiotherapy. These results suggest that modulating the Type I IFN pathway has the potential to improve radiation therapy efficacy in RC.

Publisher

Research Square Platform LLC

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