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首页> 外文期刊>New biotechnology >Combination of ribosome display and next generation sequencing as a powerful method for identification of affibody binders against beta-lactamase CTX-M15
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Combination of ribosome display and next generation sequencing as a powerful method for identification of affibody binders against beta-lactamase CTX-M15

机译:核糖体显示和下一代测序的组合作为针对β-内酰胺酶CTX-M15鉴定隐语粘合剂的强大方法

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摘要

CTX-M15 is one of the most widespread, extended spectrum beta-lactamases, a major determinant of antibiotic resistance representing urgent public health threats, among enterobacterial strains infecting humans and animals. Here we describe the selection of binders to CTX-M15 from a combinatorial affibody library displayed on ribosomes. Upon three increasingly selective ribosome display iterations, selected variants were identified by next generation sequencing (NGS). Nine affibody variants with high relative abundance bearing QRP and QLH amino acid motifs at residues 9-11 were produced and characterized in terms of stability, affinity and specificity. All affibodies were correctly folded, with affinities ranging from 0.04 to 2 mu M towards CTX-M15, and successfully recognized CTX-M15 in bacterial lysates, culture supernatants and on whole bacteria. It was further demonstrated that the binding of affibody molecules to CTX-M15 modulated the enzyme's kinetic parameters. This work provides an approach using ribosome display coupled to NGS for the rapid generation of protein ligands of interest in diagnostic and research applications.
机译:CTX-M15是最普遍的扩展谱β-内酰胺酶之一,是一种在感染人类和动物的肠杆菌菌株中代表紧急公共卫生威胁的抗生素抗性的主要决定因素。在这里,我们将粘合剂的选择从核糖体上显示的组合粘合文库中选择粘合剂到CTX-M15。在三个越来越多的选择性核糖体显示迭代中,通过下一代测序(NGS)鉴定出选定的变体。在稳定性,亲和力和特异性方面产生九个具有高相对丰度QRP和QLH氨基酸基序的含有高相对丰度的QRP和QLH氨基酸基序。所有辅助物都是正确折叠的,亲和力从0.04〜2 mu m朝向CTX-M15,并在细菌裂解物,培养上清液和整个细菌上成功地认识到CTX-M15。进一步证明了隐语分子与CTX-M15的结合调节了酶的动力学参数。这项工作提供了一种方法,使用核糖体显示器耦合到NGS,用于快速产生诊断和研究应用的蛋白质配体的快速产生。

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