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Protein engineering approaches for antibody fragments: directed evolution and rational design approaches

机译:抗体片段的蛋白质工程方法:定向进化和合理设计方法

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摘要

The number of therapeutic antibodies in preclinical, clinical, or approved phases has been increasing exponentially, mostly due to their known successes. Development of antibody engineering methods has substantially hastened the development of therapeutic antibodies. A variety of protein engineering techniques can be applied to antibodies to improve their afinity and/or biophysical properties such as solubility and stability. Antibody fragments (where all or some parts of constant regions are eliminated while the essential antigen binding region is preserved) are more suitable for protein engineering techniques because there are many in vitro screening technologies available for antibody fragments but not full-length antibodies. Improvement of biophysical characteristics is important in the early development phase because most antibodies fail at the later stage of development and this leads to loss of resources and time. Here, we review directed evolution and rational design methods to improve antibody properties. Recent developments in rational design approaches and antibody display technologies, and especially phage display, which was recently awarded the 2018 Nobel Prize, are discussed to be used in antibody research and development.
机译:临床前,临床或批准阶段的治疗性抗体数量呈指数增长,这主要是由于其已知的成功。抗体工程方法的发展大大加快了治疗性抗体的发展。可以将多种蛋白质工程技术应用于抗体以改善其亲和力和/或生物物理特性,例如溶解性和稳定性。抗体片段(恒定区的全部或部分部分被消除,而必需的抗原结合区被保留)更适合蛋白质工程技术,因为有许多体外筛选技术可用于抗体片段,但不能用于全长抗体。生物物理特性的改进在早期开发阶段很重要,因为大多数抗体在开发的后期都会失败,这会导致资源和时间的损失。在这里,我们审查定向进化和合理的设计方法,以提高抗体性能。讨论了合理设计方法和抗体展示技术的最新发展,特别是最近被授予2018年诺贝尔奖的噬菌体展示技术,它们将用于抗体研发。

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