Local Delivery of SBRT and IL12 by mRNA Technology Overcomes Immunosuppressive Barriers to Eliminate Pancreatic Cancer

Author:

Hughson Angela L.,Hannon GaryORCID,Salama Noah A.,Vrooman Tara G.,Stockwell Caroline A.,Mills Bradley N.,Garrett-Larsen Jesse,Qiu Haoming,Katerji Roula,Benoodt Lauren,Johnston Carl J.,Murphy Joseph D.,Kruger Emma,Ye Jian,Gavras Nicholas W.,Keeley David C.,Qin Shuyang S.,Lesch Maggie L.,Muhitch Jason B.,Love Tanzy M.T.,Calvi Laura M.ORCID,Lord Edith M.,Luheshi Nadia,Elyes Jim,Linehan David C.,Gerber Scott A.

Abstract

AbstractThe immunosuppressive milieu in pancreatic cancer (PC) is a significant hurdle to treatments, resulting in survival statistics that have barely changed in 5 decades. Here we present a combination treatment consisting of stereotactic body radiation therapy (SBRT) and IL-12 mRNA lipid nanoparticles delivered directly to pancreatic murine tumors. This treatment was effective against primary and metastatic models, achieving cures in both settings. IL-12 protein concentrations were transient and localized primarily to the tumor. Depleting CD4 and CD8 T cells abrogated treatment efficacy, confirming they were essential to treatment response. Single cell RNA sequencing from SBRT/IL-12 mRNA treated tumors demonstrated not only a complete loss of T cell exhaustion, but also an abundance of highly proliferative and effector T cell subtypes. SBRT elicited T cell receptor clonal expansion, whereas IL-12 licensed these cells with effector function. This is the first report demonstrating the utility of SBRT and IL-12 mRNA in PC.Statement of significanceThis study demonstrates the use of a novel combination treatment consisting of radiation and immunotherapy in murine pancreatic tumors. This treatment could effectively treat local and metastatic disease, suggesting it may have the potential to treat a cancer that has not seen a meaningful increase in survival in 5 decades.

Publisher

Cold Spring Harbor Laboratory

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