Molecular Design and Immunogenicity of a Multiple-epitope FMDV Antigen and DNA Vaccination 被引量：1

Molecular Design and Immunogenicity of a Multiple-epitope FMDV Antigen and DNA Vaccination

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摘要 This article reports the design and construction of a multiple-epitope foot and mouth disease virus （FMDV） antigen, designated as OAAT. This recombinant antigen consists of the structural protein VP1 genes from serotypes A and O FMDV, five major VP1 immunodominant epitopes from two genotypes of Asial serotype, and three Th2 epitopes originating from the nonstructural protein, three ABC gene and structural protein VP4 gene. Expressions of target gene from these plasmids in HeLa cells were verified by Western-blot. BALB/c mice were immunized intramuscularly with the DNA vaccines thrice every two weeks. We found that pA could induce simultaneously specific antibodies against serotypes A, Asial, and O FMDV. Compared to those of the controls, the spots of FMDV-specific IFN-7 and cytotoxic activity from mice immunized with pA were significantly increased, pA provided full protection in 2/4 guinea pigs from challenge with FMDV O/NY00 and Asial/YNBS/58, respectively. The results show that although pA did not give full protection in 100% immunized guinea pigs from challenge with type O and Asial FMDV, respectively, OAAT may be potential immunogen against FMDV and pA may be potential DNA vaccines against FMDV. This article reports the design and construction of a multiple-epitope foot and mouth disease virus （FMDV） antigen, designated as OAAT. This recombinant antigen consists of the structural protein VP1 genes from serotypes A and O FMDV, five major VP1 immunodominant epitopes from two genotypes of Asial serotype, and three Th2 epitopes originating from the nonstructural protein, three ABC gene and structural protein VP4 gene. Expressions of target gene from these plasmids in HeLa cells were verified by Western-blot. BALB/c mice were immunized intramuscularly with the DNA vaccines thrice every two weeks. We found that pA could induce simultaneously specific antibodies against serotypes A, Asial, and O FMDV. Compared to those of the controls, the spots of FMDV-specific IFN-7 and cytotoxic activity from mice immunized with pA were significantly increased, pA provided full protection in 2/4 guinea pigs from challenge with FMDV O/NY00 and Asial/YNBS/58, respectively. The results show that although pA did not give full protection in 100% immunized guinea pigs from challenge with type O and Asial FMDV, respectively, OAAT may be potential immunogen against FMDV and pA may be potential DNA vaccines against FMDV.

作者 MA Ming-xiao JIN Ning-yi LIU Hui-juan ZHENG Mini YIN Ge-fen TIAN Ming-yao JIN Ming-lan LU Hui-jun SHEN Guo-shun ZHU Guang-ze JIN Hong-tao JIN Kuo-shi ZHANG Ying-jiu

机构地区 Genetic Engineering Laboratory College of Animal Seienee and Veterinary Medieine College of Animal Seienee and Veterinary Medieine Key Laboratory for Moleeular Enzymology and Engineering of Ministry of Edueation

出处《Chemical Research in Chinese Universities》 SCIE CAS CSCD 2008年第1期69-74,共6页 高等学校化学研究（英文版）

基金 National High Technology Research and Development Program of China(No.2006AA10A204) Educa-tional Department of Liaoning Province (No.20060527)

关键词 Multiple-epitope Foot and mouth disease virus DNA vaccine Multiple-epitope Foot and mouth disease virus DNA vaccine

分类号 Q523 [生物学—生物化学] O62 [理学—有机化学]

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Molecular Design and Immunogenicity of a Multiple-epitope FMDV Antigen and DNA Vaccination 被引量：1

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