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发现、工程改造并鉴定了一种高效的抗人白细胞介素 13 的 Fab 片段,该 Fab 片段设计用于吸入给药。

The discovery, engineering and characterisation of a highly potent anti-human IL-13 fab fragment designed for administration by inhalation.

机构信息

UCB Pharma, 216 Bath Road, Slough, Berkshire SL1 3WE, United Kingdom.

出版信息

J Mol Biol. 2013 Feb 8;425(3):577-93. doi: 10.1016/j.jmb.2012.11.036. Epub 2012 Dec 3.

Abstract

We describe the discovery, engineering and characterisation of a highly potent anti-human interleukin (IL)-13 Fab fragment designed for administration by inhalation. The lead candidate molecule was generated via a novel antibody discovery process, and the selected IgG variable region genes were successfully humanised and reformatted as a human IgG γ1 Fab fragment. Evaluation of the biophysical properties of a selection of humanised Fab fragments in a number of assays allowed us to select the molecule with the optimal stability profile. The resulting lead candidate, CA652.g2 Fab, was shown to have comparable activity to the parental IgG molecule in a range of in vitro assays and was highly stable. Following nebulisation using a mesh nebuliser, CA652.g2 Fab retained full binding affinity, functional neutralisation potency and structural integrity. Epitope mapping using solution nuclear magnetic resonance confirmed that the antibody bound to the region of human IL-13 implicated in the interaction with IL-13Rα1 and IL-13Rα2. The work described here resulted in the discovery and design of CA652.g2 human γ1 Fab, a highly stable and potent anti-IL-13 molecule suitable for delivery via inhalation.

摘要

我们描述了一种高效的抗人白细胞介素(IL)-13 Fab 片段的发现、工程设计和特性,该片段旨在通过吸入给药。该先导候选分子是通过一种新型抗体发现过程产生的,所选的 IgG 可变区基因成功地进行了人源化,并重新设计为 IgGγ1 Fab 片段。在多项测定中评估一系列人源化 Fab 片段的生物物理特性,使我们能够选择具有最佳稳定性特征的分子。由此产生的先导候选物 CA652.g2 Fab 在一系列体外测定中表现出与亲本 IgG 分子相当的活性,且具有高度稳定性。使用网孔雾化器雾化后,CA652.g2 Fab 保持完整的结合亲和力、功能中和效力和结构完整性。使用溶液核磁共振进行的表位作图证实,该抗体结合到与人 IL-13Rα1 和 IL-13Rα2 相互作用相关的 IL-13 区域。此处描述的工作导致发现和设计 CA652.g2 人 γ1 Fab,这是一种高度稳定且有效的抗 IL-13 分子,适合通过吸入给药。

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