Immunological properties of a single-chain fragment of the anti-idiotypic antibody ACA125

被引:17
|
作者
Reinartz, S
Wagner, U
Giffels, P
Gruenn, U
Schlebusch, H
Wallwiener, D
机构
[1] Univ Tubingen, Ctr Obstet & Gynecol, D-72076 Tubingen, Germany
[2] Univ Bonn, Ctr Obstet & Gynecol, D-5300 Bonn, Germany
关键词
anti-idiotype vaccination; scFv; immune responses; ovarian cancer;
D O I
10.1007/s002620000126
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Vaccination with anti-idiotypic antibodies has been described as a promising concept for treatment of several malignant diseases. The murine monoclonal antiidiotypic antibody ACA125 imitates a specific epitope of the tumor-associated antigen CA125 expressed by 80% of ovarian carcinomas. In the first clinical trial it could be shown that mAb ACA125 is able to elicit anti-antiidiotypic antibodies (Ab3) with anti-CA125 specificity in patients with advanced ovarian cancer. In order to improve the capabilities of anti-idiotype vaccines we generated a genetically engineered single-chain fragment (scFv) ACA125 composed of heavy- and light-chain variable regions connected by a flexible linker. The antigenicity of scFv ACA125 was demonstrated by immunizing rats i.p, with scFv or complete mAb in complete/incomplete Freund's adjuvants (CFA/IFA) or precipitated by aluminium hydroxide. Negative control groups included applications of irrelevant mouse IgG or adjuvants alone. Anti-anti-idiotypic antibodies (Ab3) directed against the mAb ACA125 as well as specific anti-CA125 antibodies (Ab1') could be detected in all animals treated with scFv in CFA/IFA. Nevertheless, antibody titers were lower than when the complete mAb ACA125 was used. Surprisingly, an increase of specificity could not be observed in scFv-immunized animals, which had been expected because of the lack of heavy- and light-chain constant regions that could raise rather unspecific anti-isotypic and anti-allotypic rat anti(mouse Ig) antibodies (RAMA). In contrast, the RAMA responses detected in these rats were even stronger than those following immunization with complete mAb ACA125. In conclusion, the anti-idiotypic scFv ACA125 alone cannot improve the immunogenic features of the corresponding mAb, but provides a useful tool for the further development of genetic vaccines.
引用
收藏
页码:186 / 192
页数:7
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