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Single-molecule selection and recovery of structure-specific antibodies using atomic force microscopy

机译:使用原子力显微镜单分子选择和恢复结构特异性抗体

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摘要

Protein misfolding and aggregation are a common thread in numerous diseases including Alzheimer's,Parkinson's,Huntington's,amyotrophic lateral sclerosis,diabetes,and prion-related diseases.Elucidation of the role played by the various protein forms in these diseases requires reagents that can target specific protein forms.Here we present a method to isolate antibodies that bind to a specific protein form.We combined the imaging and nanomanipulation capabilities of atomic force microscopy (AFM) with the protein diversity of phage display antibody libraries to develop a technology that allows us to recover a single antibody molecule that is bound to a single protein molecular target.The target protein-antibody complex is first imaged by AFM,the AFM tip is then manipulated by nanolithography over the target antibody to recover the associated phage,and the antibody gene is recovered from the single phage particle by polymerase chain reaction.
机译:蛋白质错折叠和聚集是包括阿尔茨海默氏病,帕金森氏病,亨廷顿氏病,肌萎缩性侧索硬化症,糖尿病和病毒相关疾病在内的多种疾病的共同点。我们提出了一种分离与特定蛋白质形式结合的抗体的方法,我们将原子力显微镜(AFM)的成像和纳米操作能力与噬菌体展示抗体库的蛋白质多样性相结合,从而开发了一种技术,使我们能够回收与单个蛋白分子靶标结合的单个抗体分子。首先通过AFM对靶蛋白-抗体复合物进行成像,然后通过对靶标抗体进行纳米光刻对AFM尖端进行操作,以回收相关的噬菌体,并回收抗体基因通过聚合酶链反应从单个噬菌体颗粒中分离。

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