Author:
Ohtsuka Junpei,Fukumura Masayuki,Furuyama Wakako,Wang Shujie,Hara Kenichiro,Maeda Mitsuyo,Tsurudome Masato,Miyamoto Hiroko,Kaito Aika,Tsuda Nobuyuki,Kataoka Yosky,Mizoguchi Akira,Takada Ayato,Nosaka Tetsuya
Abstract
Abstract
Ectopic protein with proper steric structure was efficiently loaded onto the envelope of the F gene-defective BC-PIV vector derived from human parainfluenza virus type 2 (hPIV2) by a reverse genetics method of recombinant virus production. Further, ectopic antigenic peptide was successfully loaded either outside, inside, or at both sides of the envelope of the vector. The BC-PIV vector harboring the Ebola virus GP gene was able to elicit neutralizing antibodies in mice. In addition, BC-PIV with antigenic epitopes of both melanoma gp100 and WT1 tumor antigen induced a CD8+ T-cell-mediated response in tumor-transplanted syngeneic mice. Considering the low pathogenicity and recurrent infections of parental hPIV2, BC-PIV can be used as a versatile vector with high safety for recombinant vaccine development, addressing unmet medical needs.
Publisher
Springer Science and Business Media LLC
Cited by
4 articles.
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