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功能性嵌合小鼠/人抗体的产生。

Production of functional chimaeric mouse/human antibody.

作者信息

Boulianne G L, Hozumi N, Shulman M J

出版信息

Nature. 1984;312(5995):643-6. doi: 10.1038/312643a0.

Abstract

The availability of monoclonal antibodies has revived interest in immunotherapy. The ability to influence an individual's immune state by administering immunoglobulin of the appropriate specificity may provide a powerful approach to disease control and prevention. Compared with immunoglobulin from other species, human immunoglobulin (Ig) might be best for such therapeutic intervention; it might function better with the recipient's effector cells and should itself be less immunogenic. The success of the mouse hybridoma system suggests that immunoglobulin of virtually any specificity can be obtained from a properly immunized animal. In the human system, however, immunization protocols are restricted by ethical considerations, and it is not yet clear whether human antibody-producing cell lines of the required specificity can be obtained from adventitiously immunized individuals or from in vitro immunized cells. A method which might circumvent these difficulties is to produce antibodies consisting of mouse variable regions joined to human constant regions. Therefore, we have constructed immunoglobulin genes in which the DNA segments encoding mouse variable regions specific for the hapten trinitrophenyl (TNP) are joined to segments encoding human mu and kappa constant regions. These 'chimaeric' genes are expressed as functional TNP-binding chimaeric IgM. We report here some of the properties of this novel IgM.

摘要

单克隆抗体的出现重新唤起了人们对免疫疗法的兴趣。通过给予具有适当特异性的免疫球蛋白来影响个体免疫状态的能力,可能为疾病控制和预防提供一种强有力的方法。与来自其他物种的免疫球蛋白相比,人免疫球蛋白(Ig)可能最适合这种治疗干预;它可能与受体的效应细胞更好地发挥作用,并且其自身的免疫原性应该更低。小鼠杂交瘤系统的成功表明,几乎任何特异性的免疫球蛋白都可以从经过适当免疫的动物中获得。然而,在人类系统中,免疫方案受到伦理考量的限制,目前尚不清楚是否可以从偶然免疫的个体或体外免疫的细胞中获得具有所需特异性的人抗体产生细胞系。一种可能规避这些困难的方法是生产由与人类恒定区连接的小鼠可变区组成的抗体。因此,我们构建了免疫球蛋白基因,其中编码对三硝基苯(TNP)特异性的小鼠可变区的DNA片段与编码人μ和κ恒定区的片段连接。这些“嵌合”基因表达为具有功能的TNP结合嵌合IgM。我们在此报告这种新型IgM的一些特性。

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