期刊
CLINICAL CANCER RESEARCH
卷 13, 期 22, 页码 6779-6787出版社
AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1078-0432.CCR-07-1587
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Purpose: Previous studies indicated that humoral or cellular immunity against murine vascular endothelial growth factor 2 (mFIk-1) was elicited to inhibit tumor growth. Here we describe a genetic fusion vaccine, pMBD2-mFIk-1, based on the targeting of a modified mFlk-1 to antigen-presenting cells by a murine p-defensin 2 (MBD2) protein to induce both humoral and cellular immunity against mFlk-1, with the targeting especially focused on immature dendritic cells. Experimental Design: The protective and therapeutic antitumor immunity of the fusion vaccine was investigated in mouse models. Antiangiogenesis effect was detected by immunohistochemical staining and alginate-encapsulate tumor cell assay. The mechanisms of the fusion vaccine were primarily explored by detection of autoantibodies and CTL activity and confirmed by the deletion of immune cell subsets. Results: The fusion vaccine elicited a strong protective and therapeutic antitumor immunity through antiangiogenesis in mouse models, and this worked through stimulation of an antigenspecific CD8(+) T-cell response as well as a specific B-cell response against mFlk-1 The findings were confirmed by depletion of immune cell subsets and in knockout mice. Conclusion: Our study showed that a fusion vaccine based on self immune peptide (MBD2) and self antigen (mFIk-1) induced autoimmunity against endothelial cells, resulting in inhibition of tumor growth, and could be further exploited in clinical applications of cancer immunotherapy.
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