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Aptamers targeting protein-specific glycosylation in tumor biomarkers: general selection, characterization and structural modeling

机译:靶向肿瘤生物标志物中蛋白质特异性糖基化的适体:一般选择,表征和结构建模

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Detecting specific protein glycoforms is attracting particular attention due to its potential to improve the performance of current cancer biomarkers. Although natural receptors such as lectins and antibodies have served as powerful tools for the detection of protein-bound glycans, the development of effective receptors able to integrate in the recognition both the glycan and peptide moieties is still challenging. Here we report a method for selecting aptamers toward the glycosylation site of a protein. It allows identification of an aptamer that binds with nM affinity to prostate-specific antigen, discriminating it from proteins with a similar glycosylation pattern. We also computationally predict the structure of the selected aptamer and characterize its complex with the glycoprotein by docking and molecular dynamics calculations, further supporting the binary recognition event. This study opens a new route for the identification of aptamers for the binary recognition of glycoproteins, useful for diagnostic and therapeutic applications.
机译:检测特定的蛋白质糖族是由于其提高目前癌症生物标志物的性能而受到特别关注。虽然凝集素和抗体等天然受体作为检测蛋白质结合的聚糖的强大工具,但是能够在识别中融入甘草和肽部分的有效受体的发展仍然具有挑战性。在这里,我们报告了一种方法,用于向蛋白质的糖基化位点选择适体。它允许鉴定与NM亲和力与前列腺特异性抗原结合的适体,将其与具有相似糖基化图案的蛋白质区分离。我们还通过对接和分子动力学计算来计算地预测所选适体的结构,并用糖蛋白表征其与糖蛋白的复合物,进一步支持二进制识别事件。本研究开启了用于鉴定适体的新途径,用于糖蛋白的二进制识别,可用于诊断和治疗应用。

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