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免疫毒素合成的一种新方法:核糖体失活蛋白与单克隆抗体非共价结合。

A new approach in the synthesis of immunotoxins: ribosome inactivating protein noncovalently bound to monoclonal antibody.

作者信息

Dosio F, Brusa P, Delprino L, Grosa G, Ceruti M, Cattel L

机构信息

Istituto di Chimica Farmaceutica Applicata, Torino, Italy.

出版信息

J Pharm Sci. 1994 Feb;83(2):206-11. doi: 10.1002/jps.2600830218.

Abstract

This study describes the synthesis of a new generation of immunotoxins made by a noncovalent interaction between a monoclonal antibody derivatized with a dichlorotriazinic dye and the ribosomal inhibitor protein gelonin. The scheme of preparation has several advantages with respect to the traditional methods, which used heterobifunctional cross-linkers, such as a higher overall yield of production and the homogeneity of the obtained conjugate. Moreover, because no chemical derivatization of the gelonin was required, the unconjugated ribosome inactivating protein was recovered unaltered and therefore can be reused in other synthetic processes. This immunoconjugate was stable when tested in mouse serum and showed an interesting slow elimination rate when administered intravenously in mice. Although a high dye derivatization degree induced a modification of the specificity of the monoclonal antibody, the native specificity was restored after conjugation with gelonin. Furthermore the noncovalent linkage did not affect the gelonin inhibitory activity; in fact, the specific cytotoxic activity seemed to be similar to that of other disulfide-linked immunotoxins previously prepared in our laboratories.

摘要

本研究描述了一种新一代免疫毒素的合成方法,该免疫毒素通过用二氯三嗪染料衍生化的单克隆抗体与核糖体抑制蛋白相思豆毒素A之间的非共价相互作用制备而成。与使用异双功能交联剂的传统方法相比,该制备方案具有几个优点,如总体产率更高以及所获得的缀合物具有均一性。此外,由于不需要对相思豆毒素A进行化学衍生化,未结合的核糖体失活蛋白得以完整回收,因此可在其他合成过程中重复使用。该免疫缀合物在小鼠血清中测试时很稳定,静脉注射到小鼠体内时显示出有趣的缓慢消除速率。尽管高染料衍生化程度会导致单克隆抗体特异性发生改变,但与相思豆毒素A缀合后可恢复其天然特异性。此外,非共价连接并不影响相思豆毒素A的抑制活性;事实上,其特异性细胞毒性活性似乎与我们实验室之前制备的其他二硫键连接的免疫毒素相似。

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