Abstract

Project 3 Abstract Immunotherapy has emerged as an exciting new strategy in cancer treatment. The development of antibodies that can block negative immune regulatory pathways have resulted in clinical improvements in cancer patients that was not seen previously. Because of this success, there has been strong research and clinical interest in developing strategies to further improve cancer immunotherapy. One key strategy has been to utilize radiotherapy to enhance immunotherapy effects. Radiotherapy is thought to increase the antigen exposure to the immune system. There is also growing preclinical data demonstrating that nanoparticles (NPs) can enhance immunotherapy by improving antigen presentation. We hypothesize that we can engineer NPs that can capture the antigens released by radiotherapy and such NPs can enhance the effects of immunotherapy. We have preliminary data demonstrating that NPs can indeed capture tumor antigens released from radiotherapy. We have termed these NPs antigen-capturing NPs or AC- NP. Using a mouse model of melanoma, we have demonstrated AC-NPs, when given in conjunction with ?CTLA-4 antibody, can improve immunotherapy efficacy. The therapeutic efficacy of AC-NPs are dependent on the NPs' surface properties. We have also demonstrated that AC-NPs, when injected into tumors after radiotherapy, can generate systemic immune response against tumor cells in mice. The central goal of this application is to develop NPs that can effectively capture tumor antigens released by radiotherapy and evaluate these NPs in cancer immunotherapy. Our application has 3 specific aims:
Aim 1 : To optimize the size and surface chemistry of AC-NPs for capturing tumor antigen released from radiotherapy Aim 2: To determine whether AC-NPs can enhance the abscopal effect by radiotherapy.
Aim 3 : To determine whether AC-NPs' efficacy in enhancing the radiation therapy abscopal effect can be further improved by the addition of tumor microenvironment modifiers. To accomplish this goal, we plan to engineer biocompatible and biodegradable NPs with various size and surface properties. Melanoma will be used as a model disease for our work since it is a disease that has clearly benefited from immunotherapy. Furthermore, there are well-established mouse melanoma models for immunotherapy and extensive research using these tumor models. Our application combines concepts from several disciplines: nanotechnology, immune therapy and radiotherapy, in developing a novel strategy to improve cancer immunotherapy. Our work can increase the response rates of cancer immunotherapy which will directly translate into increased cure and survival in patients. While our work is focused on melanoma as a model, our results may be broadly applied to other cancers.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
1U54CA198999-01
Application #
8960622
Study Section
Special Emphasis Panel (ZCA1-TCRB-Q (M1))
Project Start
2015-09-01
Project End
2020-07-31
Budget Start
2015-09-01
Budget End
2016-07-31
Support Year
1
Fiscal Year
2015
Total Cost
$239,178
Indirect Cost
$81,824

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
DUNS #
608195277
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Song, Wantong; Shen, Limei; Wang, Ying et al. (2018) Synergistic and low adverse effect cancer immunotherapy by immunogenic chemotherapy and locally expressed PD-L1 trap. Nat Commun 9:2237
Hou, Lin; Liu, Qi; Shen, Limei et al. (2018) Nano-delivery of fraxinellone remodels tumor microenvironment and facilitates therapeutic vaccination in desmoplastic melanoma. Theranostics 8:3781-3796
Liu, Qi; Zhu, Hongda; Liu, Yun et al. (2018) BRAF peptide vaccine facilitates therapy of murine BRAF-mutant melanoma. Cancer Immunol Immunother 67:299-310
Mi, Yu; Smith, Christof C; Yang, Feifei et al. (2018) A Dual Immunotherapy Nanoparticle Improves T-Cell Activation and Cancer Immunotherapy. Adv Mater 30:e1706098
Zhou, Jingying; Liu, Man; Sun, Hanyong et al. (2018) Hepatoma-intrinsic CCRK inhibition diminishes myeloid-derived suppressor cell immunosuppression and enhances immune-checkpoint blockade efficacy. Gut 67:931-944
Wan, Xiaomeng; Beaudoin, James J; Vinod, Natasha et al. (2018) Co-delivery of paclitaxel and cisplatin in poly(2-oxazoline) polymeric micelles: Implications for drug loading, release, pharmacokinetics and outcome of ovarian and breast cancer treatments. Biomaterials 192:1-14
Collier, Michael A; Junkins, Robert D; Gallovic, Matthew D et al. (2018) Acetalated Dextran Microparticles for Codelivery of STING and TLR7/8 Agonists. Mol Pharm 15:4933-4946
Liu, Lina; Wang, Yuhua; Miao, Lei et al. (2018) Combination Immunotherapy of MUC1 mRNA Nano-vaccine and CTLA-4 Blockade Effectively Inhibits Growth of Triple Negative Breast Cancer. Mol Ther 26:45-55
Cheng, Ning; Watkins-Schulz, Rebekah; Junkins, Robert D et al. (2018) A nanoparticle-incorporated STING activator enhances antitumor immunity in PD-L1-insensitive models of triple-negative breast cancer. JCI Insight 3:
Liu, Qi; Chen, Fengqian; Hou, Lin et al. (2018) Nanocarrier-Mediated Chemo-Immunotherapy Arrested Cancer Progression and Induced Tumor Dormancy in Desmoplastic Melanoma. ACS Nano 12:7812-7825

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