Enhanced Vaccine Immunogenicity Enabled by Targeted Cytosolic Delivery of Tumor Antigens into Dendritic Cells

被引:5
|
作者
Truex, Nicholas L. [1 ,2 ]
Rondon, Aureïlie [1 ]
Ro''ssler, Simon L. [1 ]
Hanna, Cameron C. [1 ]
Cho, Yehlin [3 ]
Wang, Bin-You [1 ]
Backlund, Coralie M. [4 ]
Lutz, Emi A. [4 ,6 ]
Irvine, Darrell J. [3 ,4 ,5 ,6 ,7 ,8 ,9 ]
Pentelute, Bradley L. [1 ,4 ,10 ,11 ]
机构
[1] MIT, Dept Chem, Cambridge, MA 02139 USA
[2] Univ South Carolina, Dept Chem & Biochem, Columbia, SC 29208 USA
[3] MIT, Dept Mat Sci & Engn, Cambridge, MA 02139 USA
[4] MIT, Koch Inst Integrat Canc Res, Cambridge, MA 02139 USA
[5] MIT, Dept Biol Engn, Cambridge, MA 02139 USA
[6] MIT, Dept Biol Engn, Cambridge, MA 02139 USA
[7] MIT, Koch Inst Integrat Canc Res, Cambridge, MA 02139 USA
[8] MIT, Ragon Inst Massachusetts Gen Hosp, 400 Technol Sq, Cambridge, MA 02139 USA
[9] Howard Hughes Med Inst, Chevy Chase, MD 20815 USA
[10] MIT, Ctr Environm Hlth Sci, Cambridge, MA 02139 USA
[11] Broad Inst MIT & Harvard, Cambridge, MA 02142 USA
基金
美国国家卫生研究院;
关键词
ANTHRAX PROTECTIVE ANTIGEN; TOXIN-MEDIATED DELIVERY; PEPTIDE VACCINE; ELISPOT ASSAY; IN-VIVO; MELANOMA; GAMMA; MUTATIONS; RECEPTOR; MURINE;
D O I
10.1021/acscentsci.3c00625
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Molecular vaccines comprising antigen peptides and inflammatory cues make up a class of therapeutics that promote immunity against cancer and pathogenic diseases but often exhibit limited efficacy. Here, we engineered an antigen peptide delivery system to enhance vaccine efficacy by targeting dendritic cells and mediating cytosolic delivery. The delivery system consists of the nontoxic anthrax protein, protective antigen (PA), and a single-chain variable fragment (scFv) that recognizes the XCR1 receptor on dendritic cells (DCs). Combining these proteins enabled selective delivery of the N-terminus of lethal factor (LFN) into XCR1-positive cross-presenting DCs. Incorporating immunogenic epitope sequences into LFN showed selective protein translocation in vitro and enhanced the priming of antigen-specific T cells in vivo. Administering DC-targeted constructs with tumor antigens (Trp1/gp100) into mice bearing aggressive B16-F10 melanomas improved mouse outcomes when compared to free antigen, including suppressed tumor growth up to 58% at 16 days post tumor induction (P < 0.0001) and increased survival (P = 0.03). These studies demonstrate that harnessing DC-targeting anthrax proteins for cytosolic antigen delivery significantly enhances the immunogenicity and antitumor efficacy of cancer vaccines.
引用
收藏
页码:1835 / 1845
页数:11
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