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免疫毒素:单克隆抗体与毒素亚基的杂交分子可特异性杀死肿瘤细胞。

Immunotoxins: hybrid molecules of monoclonal antibodies and a toxin subunit specifically kill tumour cells.

作者信息

Blythman H E, Casellas P, Gros O, Gros P, Jansen F K, Paolucci F, Pau B, Vidal H

出版信息

Nature. 1981 Mar 12;290(5802):145-6. doi: 10.1038/290145a0.

Abstract

Several attempts to attack tumours in experimental systems have been made using conjugates of chemotherapeutic agents or potent toxins with antibodies (immunotoxins). In vitro studies have been highly successful, showing target specificity of a high order in some cases. However, so far, such conjugates have been inadequate in vivo, probably for two main reasons. First, conventional heteroclonal antibodies are perhaps inappropriate, because purification by biochemical methods leaves a large amount of non-antibody gamma-globulins. The use of monoclonal antibodies may overcome this problem. Second, when whole toxins have been conjugated to antibodies there has been a strong residual nonspecific cytotoxicity due to the binding capacity of a subunit, the B-piece of the toxin. (Diphtheria toxin or ricin consist of two polypeptide subunits. The A-piece is responsible for inhibition of protein synthesis on ribosomes, and the B-piece binds to galactose residues on the cell membrane and facilitates the transmembrane passage of the A-piece.) In the present work the problem of nonspecific binding by the B-piece has been circumvented by using the A-piece only as the toxin component of immunotoxins; these immunotoxins are active both in vitro and in vivo.

摘要

人们已经尝试了多种方法,利用化疗药物或强效毒素与抗体的偶联物(免疫毒素)来攻击实验系统中的肿瘤。体外研究取得了巨大成功,在某些情况下显示出高度的靶向特异性。然而,到目前为止,这类偶联物在体内的效果并不理想,可能主要有两个原因。首先,传统的异源单克隆抗体可能不合适,因为通过生化方法纯化会留下大量非抗体γ球蛋白。使用单克隆抗体可能会克服这个问题。其次,当完整的毒素与抗体偶联时,由于毒素的一个亚基(B片段)的结合能力,会产生强烈的残余非特异性细胞毒性。(白喉毒素或蓖麻毒素由两个多肽亚基组成。A片段负责抑制核糖体上的蛋白质合成,B片段与细胞膜上的半乳糖残基结合,并促进A片段的跨膜转运。)在本研究中,通过仅使用A片段作为免疫毒素的毒素成分,规避了B片段的非特异性结合问题;这些免疫毒素在体外和体内均具有活性。

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