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Rational design of a peptide capture agent for CXCL8 based on a model of the CXCL8CXCR1 complex

机译:基于CXCL8CXCR1复合物模型的CXCL8肽捕获剂的合理设计

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Protein-capture agents are widely used for the detection, immobilization and isolation of proteins and are the foundation for the development of in vitro diagnostic chips. The chemokine CXCL8 is an interesting protein target due to its involvement in the human inflammatory response. We constructed a novel structural model of CXCL8 interaction with its G-protein coupled receptor CXCR1, taking into account previously reported experimental data. From this CXCL8:CXCR1 model complex, the interaction of CXCL8 with residues near the extracellular domains 3 and 4 of CXCR1 were used as a scaffold for the rational design of a peptide capture agent called ‘IL8RPLoops’. A molecular dynamics simulation of IL8RPLoops indicates a stable helical conformation consistent with the CXCR1 structure from which it was derived. CXCL8 capture in fluorescence-based assays on beads and on glass demonstrates that IL8RPLoops is an effective capture agent for CXCL8. Additionally, we found IL8RPLoops to be a potent inhibitor of CXCL8-induced neutrophil migration and CXCL8:CXCR1 association. A theoretical binding model for IL8RPLoops:CXCL8 is proposed, which shows the peptide predominantly interacting with CXCL8 via electrostatic contacts with the ELR motif at the CXCL8 N-terminus.
机译:蛋白质捕获剂广泛用于蛋白质的检测,固定和分离,是体外诊断芯片的发育的基础。由于其参与人炎症反应,趋化因子CXCL8是一种有趣的蛋白质目标。我们构建了一种与其G蛋白偶联受体CXCR1的CXCL8相互作用的新颖结构模型,考虑到先前报道的实验数据。从该CXCL8:CXCR1模型复合物中,CXCL8与CXCR1细胞外结构域3和4附近残留物的相互作用用作称为“IL8RPLOOPA”的肽捕获剂的合理设计的支架。 IL8RPLOOPOP的分子动力学模拟表明,与其衍生的CXCR1结构一致的稳定螺旋构象。 CXCL8在珠粒和玻璃上基于荧光的测定捕获表明IL8RPLOOPS是CXCL8的有效捕获剂。另外,我们发现IL8RPLOOPS是CXCL8诱导的中性粒细胞迁移和CXCL8:CXCR1关联的有效抑制剂。提出了IL8RPLOOPOPS的理论结合模型:CXCL8,其显示了主要通过与CXCL8 N-末端的ELR基序的静电触点与CXCL8相互作用的肽。

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