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针对HLA - A2.1转基因兔中CRPV诱导的乳头瘤的长肽治疗性疫苗接种。

Long-peptide therapeutic vaccination against CRPV-induced papillomas in HLA-A2.1 transgenic rabbits.

作者信息

Hu Jiafen, Budgeon Lynn R, Balogh Karla K, Peng Xuwen, Cladel Nancy M, Christensen Neil D

机构信息

Jake Gittlen Cancer Research Foundation, Pennsylvania State University college of medicine, Hershey, PA 17033, USA ; Department of Pathology, Pennsylvania State University college of medicine, Hershey, PA 17033, USA.

Department of Comparative Medicine, Pennsylvania State University college of medicine, Hershey, PA 17033, USA.

出版信息

Trials Vaccinol. 2014;3:134-142. doi: 10.1016/j.trivac.2014.06.002.

Abstract

Long peptide immunization is a promising strategy to clear established tumors. In the current study, we investigated the therapeutic effect of a naturally existing long peptide that contained two HLA-A2.1 restricted epitopes (CRPVE1/149-157 and CRPVE1/161-169) from cottontail rabbit papillomavirus (CRPV) E1 using our CRPV/HLA-A2.1 transgenic rabbit model. A universal Tetanus Toxin helper motif (TT helper) was tagged at either the N-terminus or the carboxyl-terminus of this long peptide and designated as TT-E1 peptide and E1 peptide-TT respectively. Four groups of HLA-A2.1 transgenic rabbits were infected with wild type CRPV DNA. Three weeks post-infection, the rabbits were immunized four times with TT-E1 peptide, E1peptide only, E1 peptide -TT or TT-control peptide with two-week intervals between immunizations. Tumor outgrowth was monitored and recorded weekly. After the third booster immunization, tumors on two of the four E1 peptide-TT immunized rabbits began to shrink. One animal from this group was free of tumors at the termination of the study. The mean papilloma size of E1 peptide-TT immunized rabbits was significantly smaller when compared with that of the three other groups (P<0.05, one way ANOVA analysis). It is interesting that E1 peptide-TT vaccination not only stimulated stronger T cell mediate immune responses but also stronger antibody generations. We conclude that the location of a TT helper motif tagged at the long peptide vaccine is critical for the outcome of therapeutic responses to persistent tumors in our HLA-A2.1 transgenic rabbit model.

摘要

长肽免疫是清除已形成肿瘤的一种有前景的策略。在本研究中,我们使用我们的棉尾兔乳头瘤病毒(CRPV)/HLA - A2.1转基因兔模型,研究了一种天然存在的长肽的治疗效果,该长肽包含来自棉尾兔乳头瘤病毒(CRPV)E1的两个HLA - A2.1限制性表位(CRPVE1/149 - 157和CRPVE1/161 - 169)。一个通用的破伤风毒素辅助基序(TT辅助基序)被标记在该长肽的N端或C端,分别命名为TT - E1肽和E1肽 - TT。四组HLA - A2.1转基因兔被野生型CRPV DNA感染。感染后三周,兔子分别用TT - E1肽、仅E1肽、E1肽 - TT或TT - 对照肽免疫四次,每次免疫间隔两周。每周监测并记录肿瘤生长情况。在第三次加强免疫后,四只接受E1肽 - TT免疫的兔子中有两只的肿瘤开始缩小。该组中有一只动物在研究结束时无肿瘤。与其他三组相比,E1肽 - TT免疫的兔子的平均乳头瘤大小显著更小(P<0.0

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