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Stability Analysis of an Inline Peptide-based Conjugate for Metal Delivery: Nickel(II)-claMP Tag Epidermal Growth Factor as a Model System

机译:内联肽基共轭物用于金属传递的稳定性分析:镍(II)-claMP标签表皮生长因子作为模型系统

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摘要

Metals are a key component of many diagnostic imaging and biotechnology applications, and the majority of cancer patients receive a platinum-based drug as part of their treatment. Significant effort has been devoted to developing tight binding synthetic chelators to enable effective targeted delivery of metal-based conjugates, with most successes involving lanthanides rather than transition metals for diagnostic imaging. Chemical conjugation modifies the protein’s properties and generates a heterogeneous mixture of products. Chelator attachment is typically done by converting the amino group on lysines to an amide, which can impact the stability and solubility of the targeting protein and these properties vary among the set of individual conjugate species. Site-specific attachment is sought to reduce complexity and control stability. Here, the metal abstraction peptide (MAP) technology was applied to create the claMP Tag, an inline platform for generating site-specific conjugates involving transition metals. The claMP Tag was genetically encoded into epidermal growth factor (EGF) and loaded with nickel(II) as a model system to demonstrate that the tag within the homogeneous inline conjugate presents sufficient solution stability to enable biotechnology applications. The structure and disulfide network of the protein and chemical stability of the claMP Tag and EGF components were characterized.
机译:金属是许多诊断成像和生物技术应用程序的关键组成部分,大多数癌症患者将铂类药物作为治疗的一部分。已经投入大量努力来开发紧密结合的合成螯合剂,以实现金属基结合物的有效靶向递送,大多数成功涉及镧系元素而不是过渡金属来进行诊断成像。化学共轭改变了蛋白质的特性,并产生了产物的异质混合物。螯合剂的附着通常是通过将赖氨酸上的氨基转化为酰胺来完成的,这会影响靶向蛋白的稳定性和溶解性,并且这些性质在一组单独的缀合物中有所不同。寻求特定于站点的附件以减少复杂性和控制稳定性。在这里,金属提取肽(MAP)技术被用于创建claMP Tag,这是一个在线平台,用于生成涉及过渡金属的位点特异性结合物。 claMP标签已被遗传编码到表皮生长因子(EGF)中,并以镍(II)加载为模型系统,以证明均质串联缀合物中的标签具有足够的溶液稳定性,可实现生物技术应用。表征了蛋白质的结构和二硫键网络以及claMP Tag和EGF成分的化学稳定性。

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