Repurposing rotavirus vaccines for intratumoral immunotherapy can overcome resistance to immune checkpoint blockade

免疫检查点 免疫疗法 医学 溶瘤病毒 轮状病毒 免疫系统 免疫原性 癌症研究 免疫学 病毒学 病毒
作者
Tala Shekarian,Éva Sivadó,Anne-Catherine Jallas,Stéphane Depil,Janice Kielbassa,Isabelle Janoueix‐Lerosey,Gregor Hütter,Nadège Goutagny,Christophe Bergeron,Alain Viari,Sandrine Valsesia‐Wittmann,Christophe Caux,Aurélien Marabelle
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:11 (515) 被引量:58
标识
DOI:10.1126/scitranslmed.aat5025
摘要

Although immune checkpoint-targeted therapies are currently revolutionizing cancer care, only a minority of patients develop durable objective responses to anti-PD-1, PD-L1, and CTLA-4 therapy. Therefore, new therapeutic interventions are needed to increase the immunogenicity of tumors and overcome the resistance to these immunotherapies. Oncolytic properties of common viruses can be exploited for the priming of antitumor immunity, and such oncolytic viruses are currently in active clinical development in combination with immune checkpoint-targeted therapies. However, the routine implementation of these therapies is limited by their manufacturing constraints, the risk of exposure of clinical staff, and the ongoing regulations on genetically modified organisms. We sought to determine whether anti-infectious disease vaccines could be used as a commercially available source of immunostimulatory agents for cancer immunotherapy. We found that rotavirus vaccines have both immunostimulatory and oncolytic properties. In vitro, they can directly kill cancer cells with features of immunogenic cell death. In vivo, intratumoral rotavirus therapy has antitumor effects that are dependent on the immune system. In several immunocompetent murine tumor models, intratumoral rotavirus overcomes resistance to and synergizes with immune checkpoint-targeted therapy. Heat- and UV-inactivated rotavirus lost their oncolytic activity but kept their synergy with immune checkpoint-targeted antibodies through the up-regulation of the double-stranded RNA receptor retinoic acid-induced gene 1 (RIG-I). Rotavirus vaccines are clinical-grade products used in pediatric and adult populations. Therefore, in situ immunization strategies with intratumoral-attenuated rotavirus could be implemented quickly in the clinic.
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