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A polyepitope DNA vaccine targeted to Her-2/ErbB-2 elicits a broad range of human and murine CTL effectors to protect against tumor challenge.

机译:靶向Her-2 / ErbB-2的多表位DNA疫苗引发了广泛的人类和鼠类CTL效应子,以抵抗肿瘤攻击。

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摘要

A cDNA vaccine (pVax1/pet-neu) was designed to encode 12 different Her-2/ErbB-2-derived, HLA-A*0201-restricted dominant and high-affinity heteroclitic cryptic epitopes. Vaccination with pVax1/pet-neu triggered multiple and ErbB-2-specific CTL responses in HLA-A*0201 transgenic HHD mice and in HLA-A*0201 healthy donors in vitro. Human and murine CTL specific for each one of the 12 ErbB-2 peptides recognized in vitro both human and murine tumor cells overexpressing endogenous ErbB-2. Furthermore, vaccination of HHD mice with pVax1/pet-neu significantly delayed the in vivo growth of challenged ErbB-2-expressing tumor (EL4/HHD/neu murine thymoma) more actively when compared with vaccination with the empty vector (pVax1) or vehicle alone. These data indicate that the pVax1/pet-neu cDNA vaccine coding for a poly-ErbB-2 epitope is able to generate simultaneous ErbB-2-specific antitumor responses against dominant and cryptic multiple epitopes.
机译:设计了一种cDNA疫苗(pVax1 / pet-neu),以编码12种不同的Her-2 / ErbB-2衍生的HLA-A * 0201限制性显性和高亲和力异质隐表位。在体外对HLA-A * 0201转基因HHD小鼠和HLA-A * 0201健康供体进行pVax1 / pet-neu疫苗接种后,会触发多种和ErbB-2特异性CTL反应。对12种ErbB-2肽中的每一种具有特异性的人和鼠CTL在体外都识别了过表达内源性ErbB-2的人和鼠肿瘤细胞。此外,与用空载体(pVax1)或载体接种疫苗相比,用pVax1 / pet-neu疫苗接种HHD小鼠显着更有效地延缓了表达ErbB-2表达的挑战性肿瘤(EL4 / HHD /中性鼠胸腺瘤)的体内生长单独。这些数据表明,编码poly-ErbB-2表位的pVax1 / pet-neu cDNA疫苗能够同时产生针对显性和隐性多个表位的ErbB-2特异性抗肿瘤反应。

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