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一种外毒素A变体,可形成强效且特异性的化学偶联免疫毒素。

A variant of exotoxin A that forms potent and specific chemically conjugated immunotoxins.

作者信息

Chaudry G J, Fulton R J, Draper R K

机构信息

Molecular and Cell Biology Program, University of Texas at Dallas, Richardson 75083.

出版信息

J Biol Chem. 1993 May 5;268(13):9437-41.

PMID:8486636
Abstract

To introduce a free sulfhydryl into Pseudomonas aeruginosa exotoxin A (ETA), methionine 161 in domain I of the toxin was changed to cysteine by site-directed mutagenesis. The free sulfhydryl provides a convenient site for covalent attachment of ETA to other proteins in the production of chimeric toxins. The mutation was then introduced into a variant of ETA that is impaired in receptor binding, termed ETA-60EF61, that has the dipeptide Glu-Phe inserted between residues 60 and 61. The resulting double mutant, ETA-60EF61 Cys161, was conjugated to three different monoclonal antibodies via a thioether linkage, and the immunotoxins were tested for cytotoxicity with cells in culture. Each immunotoxin was extremely potent against cells that expressed surface determinants for the monoclonal antibodies but had little cytotoxicity for cells that did not bind the antibodies. For comparison, we also conjugated ricin A chain to each of the three monoclonal antibodies and found that the resulting immunotoxins were at least two-orders of magnitude less potent than the corresponding immunotoxins made with ETA-60EF61Cys161. This study demonstrates that ETA-60EF61Cys161 makes potent and specific immunotoxins and may potentially be useful in selectively eliminating subpopulations of cells in vitro and in vivo.

摘要

为了将一个游离巯基引入铜绿假单胞菌外毒素A(ETA),通过定点诱变将毒素I结构域中的甲硫氨酸161替换为半胱氨酸。该游离巯基为在嵌合毒素生产过程中将ETA共价连接到其他蛋白质提供了一个便利位点。然后将该突变引入到一种受体结合受损的ETA变体中,该变体称为ETA-60EF61,其在60和61位残基之间插入了二肽Glu-Phe。所得的双突变体ETA-60EF61 Cys161通过硫醚键与三种不同的单克隆抗体偶联,并在细胞培养中测试了这些免疫毒素的细胞毒性。每种免疫毒素对表达针对单克隆抗体的表面决定簇的细胞具有极强的毒性,但对不结合抗体的细胞几乎没有细胞毒性。作为比较,我们还将蓖麻毒素A链与这三种单克隆抗体中的每一种偶联,发现所得的免疫毒素的效力比用ETA-60EF61Cys161制备的相应免疫毒素至少低两个数量级。这项研究表明,ETA-60EF61Cys161可制成强效且特异性的免疫毒素,可能在体外和体内选择性清除细胞亚群方面具有潜在用途。

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