首页> 外文期刊>Acta biomaterialia >Improving bacterial cellulose for blood vessel replacement: Functionalization with a chimeric protein containing a cellulose-binding module and an adhesion peptide.
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Improving bacterial cellulose for blood vessel replacement: Functionalization with a chimeric protein containing a cellulose-binding module and an adhesion peptide.

机译:改善细菌纤维素以替代血管:用含有纤维素结合模块和粘附肽的嵌合蛋白进行功能化。

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摘要

Chimeric proteins containing a cellulose-binding module (CBM) and an adhesion peptide (RGD or GRGDY) were produced and used to improve the adhesion of human microvascular endothelial cells (HMEC) to bacterial cellulose (BC). The effect of these proteins on the HMEC-BC interaction was studied. The results obtained demonstrated that recombinant proteins containing adhesion sequences were able to significantly increase the attachment of HMEC to BC surfaces, especially the RGD sequence. The images obtained by scanning electron microscopy showed that the cells on the RGD-treated BC present a more elongated morphology 48h after cell seeding. The results also showed that RGD decreased the in-growth of HMEC cells through the BC and stimulated the early formation of cord-like structures by these endothelial cells. Thus, the use of recombinant proteins containing a CBM domain, with high affinity and specificity for cellulose surfaces allows control of the interaction of this material with cells. CBM may be combined with virtually any biologically active protein for the modification of cellulose-based materials, for in vitro or in vivo applications.
机译:产生了包含纤维素结合模块(CBM)和粘附肽(RGD或GRGDY)的嵌合蛋白,并用于改善人微血管内皮细胞(HMEC)对细菌纤维素(BC)的粘附。研究了这些蛋白质对HMEC-BC相互作用的影响。获得的结果证明,含有粘附序列的重组蛋白能够显着增加HMEC对BC表面的附着,特别是RGD序列。通过扫描电子显微镜获得的图像显示,RGD处理的BC上的细胞在接种细胞后48小时呈现出更长的形态。结果还表明,RGD降低了HMEC细胞通过BC的向内生长,并刺激了这些内皮细胞早期形成绳状结构。因此,使用对纤维素表面具有高亲和力和特异性的,含有CBM结构域的重组蛋白可以控制该材料与细胞的相互作用。 CBM可以与几乎任何生物活性蛋白结合使用,以修饰纤维素材料,用于体外或体内应用。

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