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免疫识别、抗原设计与催化抗体的产生。

Immune recognition, antigen design, and catalytic antibody production.

作者信息

Tramontano A

机构信息

IGEN Research Institute, Seattle, WA 98109.

出版信息

Appl Biochem Biotechnol. 1994 May-Jun;47(2-3):257-73; discussion 273-5. doi: 10.1007/BF02787939.

Abstract

Catalytic antibodies have been developed by experimental approaches exploiting the analogy between antibody-antigen and enzyme-substrate interaction. Haptens have been prepared to model the electrostatic or geometric attributes of a reaction's transition state and to induce combining sites having appropriate catalytic residues. The relative merits of these design strategies may be gleaned from the apparent activities and efficiencies of the respective catalysts. The implications of screening strategies on the kinetic characteristics of the resulting abzymes are also considered. Combining-site hypermutation provides the variation in the antibody repertoire from which high-affinity clones are selected. The same mechanism can also lead to a subset of antibodies with reduced hapten affinity, but improved catalytic activity. This possibility has not been adequately characterized, but is suggested by a number of considerations. These include the unexplained efficiency and diversity of mechanisms utilized by various antibody catalysts, and the observed catalytic activity of antibodies found in autoimmune serum. This article attempts to assess critically the evidence for rational design of catalytic activity in antibodies. Correlations among abzymes and their relevant models could lead to revised or novel strategies for producing better catalysts.

摘要

催化抗体是通过利用抗体 - 抗原与酶 - 底物相互作用之间的相似性的实验方法开发出来的。已制备半抗原以模拟反应过渡态的静电或几何属性,并诱导具有适当催化残基的结合位点。这些设计策略的相对优点可以从各自催化剂的表观活性和效率中收集。还考虑了筛选策略对所得抗体酶动力学特性的影响。结合位点超突变提供了抗体库中的变异,从中选择高亲和力克隆。相同的机制也可能导致一部分对半抗原亲和力降低但催化活性提高的抗体。这种可能性尚未得到充分表征,但从一些考虑因素中可以看出。这些因素包括各种抗体催化剂所利用机制的无法解释的效率和多样性,以及在自身免疫血清中发现的抗体的催化活性。本文试图批判性地评估抗体催化活性合理设计的证据。抗体酶与其相关模型之间的相关性可能会导致产生更好催化剂的修订或新策略。

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