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新型工程化曲妥珠单抗构象表位显示出针对HER-2/neu的体内外抗肿瘤特性。

Novel engineered trastuzumab conformational epitopes demonstrate in vitro and in vivo antitumor properties against HER-2/neu.

作者信息

Garrett Joan T, Rawale Sharad, Allen Stephanie D, Phillips Gary, Forni Guido, Morris John C, Kaumaya Pravin T P

机构信息

Departments of Obstetrics and Gynecology, Arthur G. James Comprehensive Cancer Center, Ohio State University, Columbus, OH 43210, USA.

出版信息

J Immunol. 2007 Jun 1;178(11):7120-31. doi: 10.4049/jimmunol.178.11.7120.

DOI:10.4049/jimmunol.178.11.7120
PMID:17513761
Abstract

Trastuzumab is a growth-inhibitory humanized Ab targeting the oncogenic protein HER-2/neu. Although trastuzumab is approved for treatment of advanced breast cancer, a number of concerns exist with passive immunotherapy. Treatment is expensive and has a limited duration of action, necessitating repeated administrations of the mAb. Active immunotherapy with conformational B cell epitopes affords the possibility of generating an enduring immune response, eliciting protein-reactive high-affinity anti-peptide Abs. The three-dimensional structure of human HER-2 in complex with trastuzumab reveals that the Ag-binding region of HER-2 spans residues 563-626 that comprises an extensive disulfide-bonding pattern. To delineate the binding region of HER-2, we have designed four synthetic peptides with different levels of conformational flexibility. Chimeric peptides incorporating the measles virus fusion "promiscuous" T cell epitope via a four-residue linker sequence were synthesized, purified, and characterized. All conformational peptides were recognized by trastuzumab and prevented the function of trastuzumab inhibiting tumor cell proliferation, with 563-598 and 597-626 showing greater reactivity. All epitopes were immunogenic in FVB/N mice with Abs against 597-626 and 613-626 recognizing HER-2. The 597-626 epitope was immunogenic in outbred rabbits eliciting Abs which recognized HER-2, competed with trastuzumab for the same epitope, inhibited proliferation of HER-2-expressing breast cancer cells in vitro and caused their Ab-dependent cell-mediated cytotoxicity. Moreover, immunization with the 597-626 epitope significantly reduced tumor burden in transgenic BALB-neuT mice. These results suggest the peptide B cell immunogen is appropriate as a vaccine for HER-2-overexpressing cancers because the resulting Abs show analogous biological properties to trastuzumab.

摘要

曲妥珠单抗是一种靶向致癌蛋白HER-2/neu的生长抑制性人源化抗体。尽管曲妥珠单抗已被批准用于治疗晚期乳腺癌,但被动免疫疗法仍存在一些问题。治疗费用昂贵且作用持续时间有限,需要反复注射单克隆抗体。用构象性B细胞表位进行主动免疫疗法有可能产生持久的免疫反应,引发蛋白反应性高亲和力抗肽抗体。人HER-2与曲妥珠单抗复合物的三维结构显示,HER-2的抗原结合区域跨越残基563 - 626,该区域包含广泛的二硫键模式。为了确定HER-2的结合区域,我们设计了四种具有不同构象灵活性的合成肽。通过四残基连接序列掺入麻疹病毒融合“混杂”T细胞表位的嵌合肽被合成、纯化和表征。所有构象肽均能被曲妥珠单抗识别,并阻止曲妥珠单抗抑制肿瘤细胞增殖的功能,其中563 - 598和597 - 626表现出更高的反应性。所有表位在FVB/N小鼠中具有免疫原性,针对597 - 626和613 - 626的抗体可识别HER-2。597 - 626表位在远交兔中具有免疫原性,可引发识别HER-2的抗体,与曲妥珠单抗竞争相同表位,在体外抑制HER-2表达的乳腺癌细胞增殖并引起其抗体依赖性细胞介导的细胞毒性。此外,用597 - 626表位免疫可显著减轻转基因BALB-neuT小鼠的肿瘤负担。这些结果表明,肽B细胞免疫原适合作为HER-2过表达癌症的疫苗,因为产生的抗体表现出与曲妥珠单抗类似的生物学特性。

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