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Generation of a high-fidelity antibody against nerve growth factor using library scanning mutagenesis and validation with structures of the initial and optimized Fab-antigen complexes

机译:使用文库扫描诱变生成抗神经生长因子的高保真抗体并通过初始和优化的Fab-抗原复合物的结构进行验证

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摘要

Nerve growth factor (NGF) is indispensable during normal embryonic development and critical for the amplification of pain signals in adults. Intervention in NGF signaling holds promise for the alleviation of pain resulting from human diseases such as osteoarthritis, cancer and chronic lower back disorders. We developed a fast, high-fidelity method to convert a hybridoma-derived NGF-targeted mouse antibody into a clinical candidate. This method, termed Library Scanning Mutagenesis (LSM), resulted in the ultra-high affinity antibody tanezumab, a first-in-class anti-hyperalgesic specific for an NGF epitope. Functional and structural comparisons between tanezumab and the mouse 911 precursor antibody using neurotrophin-specific cell survival assays and X-ray crystal structures of both Fab-antigen complexes illustrated high fidelity retention of the NGF epitope. These results suggest the potential for wide applicability of the LSM method for optimization of well-characterized antibodies during humanization.
机译:在正常胚胎发育过程中,神经生长因子(NGF)是必不可少的,对于成人疼痛信号的放大至关重要。 NGF信号传导的干预有望减轻由人类疾病(如骨关节炎,癌症和慢性下背部疾病)引起的疼痛。我们开发了一种快速,高保真的方法,可将杂交瘤来源的靶向NGF的小鼠抗体转化为临床候选药物。该方法称为文库扫描诱变(LSM),可产生超高亲和力抗体tanezumab,它是NGF表位特异的一流抗痛觉过敏药。使用神经营养蛋白特异性细胞存活测定法和两种Fab抗原复合物的X射线晶体结构,在tanezumab和小鼠911前体抗体之间的功能和结构比较表明,NGF表位具有高保真度。这些结果表明,LSM方法在人源化过程中优化表征良好的抗体方面具有广泛的应用潜力。

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