[1]胡波,盛蓉,宋艳华,等.RHDV VLPs对口蹄疫病毒B细胞表位的展示效果[J].江苏农业学报,2015,(06):1362-1370.[doi:doi:10.3969/j.issn.1000-4440.2015.06.026]
 HU Bo,SHENG Rong,SONG Yan-hua,et al.Presentation of B-cell epitope of foot-and-mouth disease virus in rabbit hemorrhagic disease virus-like particles[J].,2015,(06):1362-1370.[doi:doi:10.3969/j.issn.1000-4440.2015.06.026]
点击复制

RHDV VLPs对口蹄疫病毒B细胞表位的展示效果()
分享到:

江苏农业学报[ISSN:1006-6977/CN:61-1281/TN]

卷:
期数:
2015年06期
页码:
1362-1370
栏目:
畜牧兽医·水产养殖
出版日期:
2015-12-31

文章信息/Info

Title:
Presentation of B-cell epitope of foot-and-mouth disease virus in rabbit hemorrhagic disease virus-like particles
作者:
胡波1盛蓉12宋艳华1范志宇1魏后军1薛家宾1王芳1
(1.江苏省农业科学院兽医研究所/农业部兽用生物制品工程技术重点实验室/国家兽用生物制品工程技术研究中心,江苏南京210014;2.南京农业大学动物医学院,江苏南京210095)
Author(s):
HU Bo1SHENG Rong12SONG Yan-hua1FAN Zhi-yu1WEI Hou-jun1XUE Jia-bin1WANG Fang1
(1.Institute of Veterinary Medicine, Jiangsu Academy of Agricultural Sciences/Key Laboratory of Veterinary Biological Engineering and Technology,Ministry of Agriculture/National Center for Engineering Research of Veterinary Bio-products, Nanjing 210014, China;2.College of Veterinary Medicine, Nanjing Agricultural University, Nanjing 210095, China)
关键词:
兔出血症病毒病毒样颗粒口蹄疫病毒B细胞表位载体
Keywords:
RHDVvirus-like particlefoot-and-mouth disease virusB cell epitopevector
分类号:
Q78
DOI:
doi:10.3969/j.issn.1000-4440.2015.06.026
文献标志码:
A
摘要:
为研究兔出血症病毒(RHDV)病毒样颗粒(VLPs)携带外源表位的能力及其免疫原性,以兔出血症病毒(RHDV)衣壳蛋白VP60为载体,分别在RHDV VP60蛋白质的C端、N端和306位插入FMDV VP1双串联B细胞表位[GS-(200~213 aa)-GS-(141~160 aa)],得到嵌合蛋白质,分别命名为VP60-2FB、VP60-306FB和VP60-578FB。经IFA、SDS-PAGE和Western blot鉴定,嵌合VP60蛋白质在杆状病毒表达系统中均得到有效表达;通过电镜观察发现嵌合蛋白质可自聚成病毒样颗粒。将嵌合蛋白质免疫小鼠,检测产生的免疫应答情况,结果显示,嵌合蛋白质可以产生针对VP60特异的免疫应答,且在插入长度为42 aa外源氨基酸片段的情况下,嵌合蛋白质免疫的小鼠仍能诱导产生较高水平的针对外源表位的特异性应答。在进一步扩展了载体的容纳性后,序列的增加不影响VLPs的形成以及对外源表位的递呈效果,说明VP60-VLPs作为外源B细胞表位展示载体是可行性的。
Abstract:
To explore the capacity of antigen presentation of the foreign B cell epitopes by virus-like particles (VLPs) of rabbit hemorrhagic disease virus (RHDV), the sequences of multi-copy B-cell epitopes of foot-and-mouth disease virus (FMDV) [FMDV VP1 GS-(200-213 aa)-GS-(141-160 aa)] were fused to N-terminal and C-terminal and inserted between 306th and 307th amino acid of capsid protein of RHDV. The fused genes were cloned into the donor vector pFastBacTMHTA and three recombinant baculoviruses (rAc-VP60-2FB, rAc-VP60-306FB, rAc-VP60-578FB) were obtained using Bac-to-Bac baculovirus expression system. These chimeric proteins were expressed effectively in insect cells as confirmed by IFA, SDS-PAGE and Western blot. The immunogenicity of all chimeric proteins was evaluated in mice. The results showed that the chimeric proteins could react with both anti-VP60 monoclonal antibody and anti-FMDV polyclonal antibody. And all recombinant proteins could self-assemble into VLPs under electron microscopy, and were able to induce VP60-specific antibodies responses. The peptide-specific antibody maintained a high level when the inserted foreign fragments were up to 126 bp. The length of the foreign genes carried by VP60-VLPs was extended in this study, which demonstrated the feasibility of VP60-VLPs serving as a presentation carrier for foreign B-cell epitope.

参考文献/References:

[1]FERREIRA P G,COSTA-E-SILVA A,MONTEIRO E,et al. Transient decrease in blood heterophils and sustained liver damage caused by calicivirus infection of young rabbits that are naturally resistant to rabbit haemorrhagic disease [J]. Res Vet Sci,2004,76(1):83-94.
[2]XU Z J,CHEN W X. Viral haemorrhagic disease in rabbits:a review [J]. Vet Res Commun,1989,13(3):205-212.
[3]ABRANTES J,VAN DER LOO W,LE PENDU J,et al. Rabbit haemorrhagic disease (RHD) and rabbit haemorrhagic disease virus (RHDV):a review[J]. Vet Res,2012,10(43):12.
[4]COOKE B D. Rabbit haemorrhagic disease:field epidemiology and the management of wild rabbit populations[J]. Rev Sci Tech,2002,21(2):347-358.
[5]CHEN M,SONG Y,FAN Z,et al. Immunogenicity of different recombinant rabbit hemorrhagic disease virus-like particles carrying CD8+T cell epitope from chicken ovalbumin (OVA)[J]. Virus Res,2014,183:15-22.
[6]CRISCI E,ALMANZA H,MENA I,et al. Chimeric calicivirus-like particles elicit protective anti-viral cytotoxic responses without adjuvant[J]. Virology,2009,387(2):303-312.
[7]VALICEK L, SMID B, RODAK L,et al. Electron and immunoelectron microscopy of rabbit haemorrhagic disease virus (RHDV)[J]. Arch Virol,1990,112(3-4):271-275.
[8]金明兰,侯继波,郑其升,等. 兔出血症病毒 VP60 蛋白 T 细胞表位优势区的筛选[J]. 江苏农业科学,2013,41(4): 186-188.
[9]王芳,胡波,任雪枫,等. 兔出血症病毒衣壳蛋白在昆虫细胞中的表达及对家兔的免疫保护效果[J]. 畜牧兽医学报,2008,39(10):1382-1387.
[10]PLANA-DURAN J, BASTONS M, RODRIGUEZ M J, et al. Oral immunization of rabbits with VP60 particles confers protection against rabbit hemorrhagic disease[J]. Arch Virol,1996,141(8):1423-1436.
[11]FARNOS O, RODRIGUEZ M, CHIONG M, et al. The recombinant rabbit hemorrhagic disease virus VP60 protein obtained from Pichia pastoris induces a strong humoral and cell-mediated immune response following intranasal immunization in mice[J]. Vet Microbiol,2006,114(3-4):187-195.
[12]FERNANDEZ-FERNANDEZ M R, MOURINO M, RIVERA J, et al. Protection of rabbits against rabbit hemorrhagic disease virus by immunization with the VP60 protein expressed in plants with a potyvirus-based vector[J]. Virology,2001,280(2):283-291.
[13]LAURENT S, KUT E, REMY-DELAUNAY S, et al. Folding of the rabbit hemorrhagic disease virus capsid protein and delineation of N-terminal domains dispensable for assembly[J]. Arch Virol,2002,147(8):1559-1571.
[14]BARCENA J, VERDAGUER N, ROCA R, et al. The coat protein of rabbit hemorrhagic disease virus contains a molecular switch at the N-terminal region facing the inner surface of the capsid[J]. Virology,2004,322(1):118-134.
[15]DIMARCHI R, BROOKE G, GALE C, et al. Protection of cattle against foot-and-mouth disease by a synthetic peptide[J]. Science,1986,232(4750):639-641.
[16]BAXTER R, CRAIGMILE S C, HALEY C, et al. BoLA-DR peptide binding pockets are fundamental for foot-and-mouth disease virus vaccine design in cattle[J]. Vaccine,2009,28(1):28-37.
[17]ZHANG H Y, SUN S H, GUO Y J, et al. Immune response in mice inoculated with plasmid DNAs containing multiple-epitopes of foot-and-mouth disease virus[J]. Vaccine,2003,21(32):4704-4707.
[18]WONG H T, CHENG S C, CHAN E W, et al. Plasmids encoding foot-and-mouth disease virus VP1 epitopes elicited immune responses in mice and swine and protected swine against viral infection [J]. Virology,2000,278(1):27-35.
[19]蔡少平,王芳,贾华敏,等.兔出血症病毒胶体金免疫层析试纸条诊断方法的建立及初步应用[J]. 畜牧兽医学报,2012,43 (11):1795-1801.
[20]杨廷亚,王芳,姜平,等.应用噬菌体展示技术筛选兔出血症病毒抗原模拟表位[J]. 畜牧兽医学报,2012,43(8):1281-1286.
[21]李超美,王芳,蔡少平,等. 检测兔出血症病毒抗体间接ELISA方法的建立[J]. 江苏农业学报,2010,26(3):546-550.
[22]DI MARTINO B, MARSILIO F, ROY P. Assembly of feline calicivirus-like particle and its immunogenicity[J]. Vet Microbiol,2007,120(1-2):173-178.
[23]NICOLLIER-JAMOT B, OGIER A, PIROTH L, et al. Recombinant virus-like particles of a norovirus (genogroup II strain) administered intranasally and orally with mucosal adjuvants LT and LT(R192G) in BALB/c mice induce specific humoral and cellular Th1/Th2-like immune responses[J]. Vaccine,2004,22(9-10):1079-1086.
[24]HAN M G, CHEETHAM S, AZEVEDO M, et al. Immune responses to bovine norovirus-like particles with various adjuvants and analysis of protection in gnotobiotic calves[J]. Vaccine,2006,24(3):317-326.
[25]SOUZA M, COSTANTINI V, AZEVEDO M S, et al. A human norovirus-like particle vaccine adjuvanted with ISCOM or mLT induces cytokine and antibody responses and protection to the homologous GII.4 human norovirus in a gnotobiotic pig disease model[J]. Vaccine,2007,25(50):8448-8459.
[26]PEREZ-FILGUEIRA D M, RESINO-TALAVAN P, CUBILLOS C, et al. Development of a low-cost, insect larvae-derived recombinant subunit vaccine against RHDV[J]. Virology,2007,364(2):422-430.

相似文献/References:

[1]蒙正群,周丽军,罗怡琳,等.2株兔出血症病毒全基因测定与遗传进化分析[J].江苏农业学报,2018,(04):854.[doi:doi:10.3969/j.issn.1000-4440.2018.04.020]
 MENG Zheng-qun,ZHOU Li-jun,LUO Yi-lin,et al.Full genetic sequence determination and genetic evolution analysis of two rabbit hemorrhagic disease viruses[J].,2018,(06):854.[doi:doi:10.3969/j.issn.1000-4440.2018.04.020]

备注/Memo

备注/Memo:
收稿日期:2015-03-19 基金项目:甘肃省农业生物技术研究与应用开发项目(GNSW-2011-22);甘肃省高等学校基本科研业务费项目 作者简介:张欣(1988-),女,山东诸城人,硕士研究生,研究方向为动物免疫与抗病。(E-mail)zhangxinfreedom@163.com 通讯作者:张小丽,(E-mail)zhxl228@163.com
更新日期/Last Update: 2015-12-31