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通过超分子多价支架与蛋白质表面结合。

Binding to protein surfaces by supramolecular multivalent scaffolds.

作者信息

Martos Vera, Castreño Pilar, Valero Julián, de Mendoza Javier

机构信息

Institute of Chemical Research of Catalonia (ICIQ), Avda. Països Catalans 16, 43007 Tarragona, Spain.

出版信息

Curr Opin Chem Biol. 2008 Dec;12(6):698-706. doi: 10.1016/j.cbpa.2008.08.024. Epub 2008 Sep 16.

Abstract

Multivalency plays a pivotal role in biological recognition, particularly at protein-protein and protein-carbohydrate interaction sites. Scaffolds of diverse structure, flexibility, and valency are gaining increasing biomedical importance in the development of artificial multivalent ligands for these interfaces. Relevant examples range from small C(4) symmetric calix[4]arenes and porphyrin ligands, which may achieve nanomolar affinity for protein surfaces of pharmaceutical interest, to large-sized dendrimers that provide promising adherence-inhibition for toxins and other relevant lectins. In addition, highly flexible supramolecular platforms like rotaxanes and polymers have been proposed as challenging alternatives to more rigid designs. Finally, nanoparticles are being exploited for this aim as they present important advantages from the biological and synthetic points of view.

摘要

多价性在生物识别中起着关键作用,尤其是在蛋白质 - 蛋白质和蛋白质 - 碳水化合物相互作用位点。具有不同结构、灵活性和价态的支架在开发用于这些界面的人工多价配体方面正日益获得重要的生物医学意义。相关例子从小的C(4)对称杯[4]芳烃和卟啉配体(它们对具有药物研究价值的蛋白质表面可实现纳摩尔亲和力)到为毒素和其他相关凝集素提供有前景的粘附抑制作用的大尺寸树枝状大分子。此外,像轮烷和聚合物这样高度灵活的超分子平台已被提议作为比更刚性设计更具挑战性的替代方案。最后,纳米颗粒正被用于此目的,因为从生物学和合成的角度来看它们具有重要优势。

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