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Enhancement of DNA vaccine potency by antigen linkage to IFN-gamma-inducible protein-10

Authors
Kang, Tae HeungKim, Keon WooBae, Hyun CheolSeong, Seung-YongKim, Tae Woo
Issue Date
1-Feb-2011
Publisher
WILEY
Keywords
DNA vaccines; chemokines; IP-10; HPV-16 E7; CD4(+) Th1 T-cells; CD8(+) T-cells
Citation
INTERNATIONAL JOURNAL OF CANCER, v.128, no.3, pp.702 - 714
Indexed
SCIE
SCOPUS
Journal Title
INTERNATIONAL JOURNAL OF CANCER
Volume
128
Number
3
Start Page
702
End Page
714
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/113093
DOI
10.1002/ijc.25391
ISSN
0020-7136
Abstract
DNA vaccines have emerged as an attractive approach to generate antigen-specific T-cell immune response. Nevertheless, the potency of DNA vaccines still needs to be improved for cancer immunotherapy. In this study, we explored whether functional linkage of a Th1-polarizing chemokine, IP-10, to a model tumor antigen, human papillomavirus type 16 (HPV-16) E7, enhanced DNA vaccine potency. IP-10 linkage changed the location of E7 from the nucleus to the endoplasmic reticulum and led to the secretion of functionally chemoattractive chimeric IP-10/E7 protein. In addition, this linkage drastically enhanced the endogenous processing of E7 antigen through MHC class I. More importantly, we found that C57BL/6 mice intradermally vaccinated with IP-10/E7 DNA exhibited a dramatic increase in the number of E7-specific CD4(+) Th1 T-cells and CD8(+) T-cells and, consequently, were strongly resistant over the long term to E7-expressing tumors compared to mice vaccinated with wild-type E7 DNA. Thus, because of the increase in tumor antigen-specific T-cell immune responses obtained through both enhanced antigen presentation and chemoattraction, vaccination with DNA encoding IP-10 linked to a tumor antigen holds great promise for treating tumors.
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