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用于可控胶原蛋白结合和生物矿化的蜘蛛丝融合蛋白。

Spider Silk Fusion Proteins for Controlled Collagen Binding and Biomineralization.

作者信息

Neubauer Vanessa J, Scheibel Thomas

机构信息

Lehrstuhl Biomaterialien, Fakultät für Ingenieurwissenschaften, Universität Bayreuth, Prof.-Rüdiger-Bormann-Straße 1, 95447 Bayreuth, Germany.

Bayreuther Zentrum für Kolloide und Grenzflächen (BZKG), Universität Bayreuth, Universitätsstraße 30, 95440 Bayreuth, Germany.

出版信息

ACS Biomater Sci Eng. 2020 Oct 12;6(10):5599-5608. doi: 10.1021/acsbiomaterials.0c00818. Epub 2020 Sep 4.

Abstract

The development of biomaterials for the interface between tendon and bone is important for realizing functional tendon replacements. Toward the development of new materials for such applications, engineered recombinant spider silk proteins were modified with peptide tag sequences derived from noncollagenous proteins in bone, so-called SIBLING proteins, such as osteopontin and sialoprotein, which are known to interact with collagen and to initiate mineralization. Materials made of these spider silk-SIBLING hybrids were analyzed concerning mineralization and interaction with cells. They showed enhanced calcium phosphate formation upon incubation in mineralization agents. In gradient films, MC3T3-E1 mouse preosteoblasts adhered preferentially along the gradient toward the variant with a collagen binding motif.

摘要

开发用于肌腱与骨界面的生物材料对于实现功能性肌腱替代至关重要。为了开发适用于此类应用的新材料,工程重组蜘蛛丝蛋白用源自骨中非胶原蛋白(即所谓的SIBLING蛋白,如骨桥蛋白和唾液蛋白)的肽标签序列进行了修饰,已知这些蛋白可与胶原蛋白相互作用并启动矿化。对由这些蜘蛛丝-SIBLING杂化物制成的材料进行了矿化及与细胞相互作用方面的分析。它们在矿化剂中孵育后显示出增强的磷酸钙形成。在梯度膜中,MC3T3-E1小鼠前成骨细胞优先沿着梯度朝着具有胶原蛋白结合基序的变体方向粘附。

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