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硫酸化糖肽纳米结构用于多能蛋白激活。

Sulfated glycopeptide nanostructures for multipotent protein activation.

机构信息

Simpson Querrey Institute for BioNanotechnology, Northwestern University, Chicago, Illinois 60611, USA.

Department of Materials Science and Engineering, Northwestern University, Evanston, Illinois 60208, USA.

出版信息

Nat Nanotechnol. 2017 Aug;12(8):821-829. doi: 10.1038/nnano.2017.109. Epub 2017 Jun 19.

Abstract

Biological systems have evolved to utilize numerous proteins with capacity to bind polysaccharides for the purpose of optimizing their function. A well-known subset of these proteins with binding domains for the highly diverse sulfated polysaccharides are important growth factors involved in biological development and tissue repair. We report here on supramolecular sulfated glycopeptide nanostructures, which display a trisulfated monosaccharide on their surfaces and bind five critical proteins with different polysaccharide-binding domains. Binding does not disrupt the filamentous shape of the nanostructures or their internal β-sheet backbone, but must involve accessible adaptive configurations to interact with such different proteins. The glycopeptide nanostructures amplified signalling of bone morphogenetic protein 2 significantly more than the natural sulfated polysaccharide heparin, and promoted regeneration of bone in the spine with a protein dose that is 100-fold lower than that required in the animal model. These highly bioactive nanostructures may enable many therapies in the future involving proteins.

摘要

生物系统已经进化到利用许多具有结合多糖能力的蛋白质,以优化其功能。这些蛋白质的一个众所周知的子集具有结合高度多样化硫酸多糖的结合域,是参与生物发育和组织修复的重要生长因子。我们在这里报告了超分子硫酸糖肽纳米结构,其表面显示出一个三硫酸化单糖,并结合了五个具有不同多糖结合域的关键蛋白质。结合不会破坏纳米结构的丝状形状或其内部β-折叠骨架,但必须涉及可访问的自适应构象才能与如此不同的蛋白质相互作用。糖肽纳米结构显著增强了骨形态发生蛋白 2 的信号转导,比天然硫酸多糖肝素强得多,并以比动物模型低 100 倍的蛋白剂量促进脊柱的骨再生。这些高生物活性的纳米结构可能会在未来涉及蛋白质的许多治疗中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/760f/5553550/6d07f46e75be/nihms872469f2.jpg

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