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Label-free optical detection of small-molecule compound microarraysimmobilized on solid support using macromolecular scaffolds andsubsequent protein binding reactions

机译:使用大分子支架和仲状蛋白结合反应的固体载体对固体载体的小分子化合物微arraysimmobilize的无标记光学检测

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Small-molecule microarrays composed of tens of thousands of distinct synthetic molecules, natural products, and their combinations/modifications provide a high-throughput platform for studying protein-ligand interactions. Immobilization of small molecule compounds on solid supports remains a challenge as widely varied small molecules generally lack unique chemical groups that readily react with singly or even multiply functionalized solid support. We explored two strategies for immobilizing small molecule compounds on epoxy-functionalized glass surface using primary-amine-containing macromolecular scaffolds: bovine serum albumin (BSA) and amine-modified poly-vinyl alcohol (PVA). Small molecules with N-hydroxysuccinimide (NHS) groups were conjugated to BSA or amine-modified PVA. Small-molecule-BSA conjugates and small-molecule-PVA conjugates were subsequently immobilized on epoxy-functionalized glass slides through amine-epoxy reactions. Using an oblique-incidence reflectivity difference (OI-RD) scanning microscope as a label-free detector, we performed a comparative study of the effectiveness of BSA and PVA as macromolecular scaffolds for anchoring small molecule compounds in terms of conjugation efficiency, surface immobilization efficiency, effect of the scaffold on end-point and kinetics of subsequent binding reactions with protein probes.
机译:由数万个不同的合成分子,天然产物组成的小分子微阵列,以及它们的组合/修饰提供了用于研究蛋白质 - 配体相互作用的高通量平台。在固体载体上固定小分子化合物仍然是广泛变化的小分子的挑战通常缺乏独特的化学基团,其容易与单独反应或甚至乘法官能化固体载体反应。我们探讨了使用含有含伯胺的大分子支架:牛血清白蛋白(BSA)和胺改性的聚乙烯醇(PVA)对环氧官能化玻璃表面固定在环氧官能化玻璃表面上的两种策略。具有N-羟基琥珀酰亚胺(NHS)基团的小分子与BSA或胺改性的PVA缀合。随后将小分子-BSA缀合物和小分子-PVA缀合物通过胺 - 环氧反应对环氧官能化玻璃载玻片固定。使用倾斜入射反射率差(OI-RD)扫描显微镜作为无标签探测器,我们对BSA和PVA的有效性进行了比较研究,作为用于锚定小分子化合物的缀合效率,表面固定效率的大分子支架,支架对随后与蛋白质探针的后续结合反应的终点和动力学的影响。

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