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靶向膜蛋白的纳米抗体筛选与表征策略

Screening and Characterization Strategies for Nanobodies Targeting Membrane Proteins.

作者信息

Veugelen S, Dewilde M, De Strooper B, Chávez-Gutiérrez L

机构信息

University of Leuven, Leuven, Belgium; VIB Center for Brain and Disease, Leuven, Belgium.

University of Leuven, Leuven, Belgium; VIB Center for Brain and Disease, Leuven, Belgium; UCL Institute of Neurology, London, United Kingdom.

出版信息

Methods Enzymol. 2017;584:59-97. doi: 10.1016/bs.mie.2016.10.029. Epub 2016 Dec 12.

DOI:10.1016/bs.mie.2016.10.029
PMID:28065273
Abstract

The study of membrane protein function and structure requires their successful detection, expression, solubilization, and/or reconstitution, which poses a challenging task and relies on the availability of suitable tools. Several research groups have successfully applied Nanobodies in the purification, as well as the functional and structural characterization of membrane proteins. Nanobodies are small, single-chain antibody fragments originating from camelids presenting on average a longer CDR3 which enables them to bind in cavities and clefts (such as active and allosteric sites). Notably, Nanobodies generally bind conformational epitopes making them very interesting tools to stabilize, dissect, and characterize specific protein conformations. In the clinic, several Nanobodies are under evaluation either as potential drug candidates or as diagnostic tools. In recent years, we have successfully generated high-affinity, conformation-sensitive anti-γ-secretase Nanobodies. γ-Secretase is a multimeric membrane protease involved in processing of the amyloid precursor protein with high clinical relevance as mutations in its catalytic subunit (Presenilin) cause early-onset Alzheimer's disease. Advancing our knowledge on the mechanisms governing γ-secretase intramembrane proteolysis through various strategies may lead to novel therapeutic avenues for Alzheimer's disease. In this chapter, we present the strategies we have developed and applied for the screening and characterization of anti-γ-secretase Nanobodies. These protocols could be of help in the generation of Nanobodies targeting other membrane proteins.

摘要

对膜蛋白功能和结构的研究需要成功检测、表达、溶解和/或重组膜蛋白,这是一项具有挑战性的任务,并且依赖于合适工具的可用性。几个研究小组已成功将纳米抗体应用于膜蛋白的纯化及其功能和结构表征。纳米抗体是源自骆驼科动物的小型单链抗体片段,其互补决定区3(CDR3)平均较长,这使它们能够结合腔和裂缝(如活性位点和变构位点)。值得注意的是,纳米抗体通常结合构象表位,这使其成为稳定、剖析和表征特定蛋白质构象的非常有趣的工具。在临床上,几种纳米抗体正在作为潜在的候选药物或诊断工具进行评估。近年来,我们已成功产生了高亲和力、构象敏感的抗γ-分泌酶纳米抗体。γ-分泌酶是一种多聚体膜蛋白酶,参与淀粉样前体蛋白的加工,具有高度的临床相关性,因为其催化亚基(早老素)中的突变会导致早发性阿尔茨海默病。通过各种策略增进我们对γ-分泌酶膜内蛋白水解调控机制的了解,可能会为阿尔茨海默病带来新的治疗途径。在本章中,我们介绍了我们开发并应用于抗γ-分泌酶纳米抗体筛选和表征的策略。这些方案可能有助于生成靶向其他膜蛋白的纳米抗体。

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