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A computational and experimental study to develop E-selectin targeted peptides for molecular imaging applications

机译:用于开发用于分子成像应用的E-Selectin靶向肽的计算和实验研究

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摘要

Aim: E-selectin is overexpressed on angiogenic and inflamed endothelium. Molecules binding to E-selectin with high affinity and specificity enable its use as a molecular imaging biomarker. Material & methods: The interactions of four different peptides (i.e., Ac-P1 [Acetyl-IELLQAR-CONH2], H2N-P2 [H2N-DITWDQLWDLMK-CONH2], H2N-P3A5 [H2N-YRNWAGRW-CONH2], and Ac-P4 [Acetyl-YRNWDGRW-CONH2]) with E-selectin were analyzed by computational methodologies, surface plasmon resonance and in vitro using activated human umbilical vein endothelial cells. Poly(butyl cyanoacrylate) microbubbles were functionalized with the best candidates and evaluated as molecular ultrasound probes in cultured cells and explanted carotid arteries. Results: H2N-P3A5 and Ac-P4 peptides bound stronger to E-selectin than Ac-P1 and H2N-P2, but with lower specificity. H2N-P2 bound with higher specificity and affinity than Ac-P1. Conclusion: H2N-P2 is a good candidate for designing E-selectin-targeted molecular imaging agents.
机译:目的:E-Selectin在血管生成和发炎内皮上过表达。具有高亲和力和特异性的E-选择素结合的分子使其能够用作分子成像生物标志物。材料和方法:四种不同肽的相互作用(即AC-P1 [乙酰​​-IellQar-Conh2],H2N-P2 [H2N-DITWDLMK-CONH2],H2N-P3A5 [H2N-YRNWAGRW-CONH2]和AC-P4通过使用活化的人脐静脉内皮细胞,通过计算方法,表面等离子体共振和体外分析具有E-SELITEN的α-乙酰-YRNWDGRW-CONH2])。聚(氰基丙烯酸丁酯)微泡用最佳候选物官能化,并在培养细胞中评价为分子超声探针,并分析颈动脉。结果:H 2N-P3A5和AC-P4肽比AC-P1和H 2N-P2更强,但具有较低的特异性。 H2N-P2比AC-P1更高的特异性和亲和力。结论:H2N-P2是用于设计E-选择蛋白靶向分子成像剂的良好候选者。

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