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In Situ Tumor Vaccination with Nanoparticle Co‐Delivering CpG and STAT3 siRNA to Effectively Induce Whole‐Body Antitumor Immune Response

Worapol NgamcherdtrakulPDX Pharmaceuticals, Inc. Portland OR 97239 USAMoataz RedaPDX Pharmaceuticals, Inc. Portland OR 97239 USAMolly A. NelsonPDX Pharmaceuticals, Inc. Portland OR 97239 USARuijie WangPDX Pharmaceuticals, Inc. Portland OR 97239 USAHusam Y. ZaidanPDX Pharmaceuticals, Inc. Portland OR 97239 USADaniel S. BejanPDX Pharmaceuticals, Inc. Portland OR 97239 USANgoc Ha HoangDepartment of Biomedical Engineering Oregon Health and Science University Portland OR 97239 USARyan S. LaneDepartment of Cell, Developmental and Cancer Biology Oregon Health and Science University Portland OR 97239 USAShiuh‐Wen LuohKnight Cancer Institute Oregon Health and Science University Portland OR 97239 USASancy A. LeachmanDepartment of Dermatology Oregon Health and Science University Portland OR 97239 USAGordon B. MillsDepartment of Cell, Developmental and Cancer Biology Oregon Health and Science University Portland OR 97239 USAJoe W. GrayDepartment of Biomedical Engineering Oregon Health and Science University Portland OR 97239 USAAmanda W. LundDepartment of Cell, Developmental and Cancer Biology Oregon Health and Science University Portland OR 97239 USAWassana YantaseeDepartment of Biomedical Engineering Oregon Health and Science University Portland OR 97239 USA
2021en
ABI

Abstract

The success of immunotherapy with immune checkpoint inhibitors (ICIs) in a subset of individuals has been very exciting. However, in many cancers, responses to current ICIs are modest and are seen only in a small subsets of patients. Herein, a widely applicable approach that increases the benefit of ICIs is reported. Intratumoral administration of augmenting immune response and inhibiting suppressive environment of tumors-AIRISE-02 nanotherapeutic that co-delivers CpG and STAT3 siRNA-results in not only regression of the injected tumor, but also tumors at distant sites in multiple tumor model systems. In particular, three doses of AIRISE-02 in combination with systemic ICIs completely cure both treated and untreated aggressive melanoma tumors in 63% of mice, while ICIs alone do not cure any mice. A long-term memory immune effect is also reported. AIRISE-02 is effective in breast and colon tumor models as well. Lastly, AIRISE-02 is well tolerated in mice and nonhuman primates. This approach combines multiple therapeutic agents into a single nanoconstruct to create whole-body immune responses across multiple cancer types. Being a local therapeutic, AIRISE-02 circumvents regulatory challenges of systemic nanoparticle delivery, facilitating rapid translation to the clinic. AIRISE-02 is under investigational new drug (IND)-enabling studies, and clinical trials will soon follow.

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