Redirecting host preexisting influenza A virus immunity for cancer immunotherapy

被引:0
|
作者
Bharat K. R. Chaganty
Songbo Qiu
Yang Lu
Gabriel Lopez-Berestein
Bulent Ozpolat
Zhen Fan
机构
[1] The University of Texas MD Anderson Cancer Center,Department of Experimental Therapeutics
[2] MD Anderson Cancer Center UTHealth Graduate School of Biomedical Sciences,undefined
来源
Cancer Immunology, Immunotherapy | 2022年 / 71卷
关键词
Influenza A virus; Preexisting immunity; Human epidermal growth factor receptor-2; Single-lipid nanoparticle; Cancer immunotherapy;
D O I
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中图分类号
学科分类号
摘要
We tested the concept that host preexisting influenza A virus immunity can be redirected to inhibit tumor growth and metastasis through systemic administration of influenza A virus–related peptides to targeted tumors. Mice infected with influenza A virus strain A/Puerto Rico/8/34 (PR8) were used as a model of a host with preexisting viral immunity. The extent to which preexisting influenza A immunity in PR8-immunized mice can be redirected to inhibit tumor growth and metastasis was first examined by ectopic expression of influenza A nucleoprotein (NP) and hemagglutinin (HA) in syngeneic mammary tumor cells via lentiviral transduction. Then, the feasibility of implementing this strategy using a systemic therapy approach was assessed by systemic delivery of major histocompatibility complex class I (MHC-I)-compatible peptides to targeted mammary tumors overexpressing human epidermal growth factor receptor-2 (HER2) in mice using a novel HER2-targeting single-lipid nanoparticle (SLNP). Our results show that preexisting influenza A immunity in PR8-immunized mice could be quickly redirected to syngeneic tumors expressing influenza A NP and HA, leading to strong inhibition of tumor growth and metastasis and improvement of survival compared to the findings in antigen-naïve control mice. MHC-I-compatible peptides could be delivered to targeted mammary tumors in mice using the HER2-targeting SLNP for antigen presentation, which subsequently redirected preexisting influenza A immunity to the tumors to exert antitumor activities. In conclusion, preexisting influenza A immunity can be repurposed for cancer immunotherapy through systemic delivery of influenza A–related peptides to targeted tumors. Further development of the strategy for clinical translation is warranted.
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页码:1611 / 1623
页数:12
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