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定制胶原蛋白以构建细胞微环境。

Tailoring Collagen to Engineer the Cellular Microenvironment.

机构信息

Department of Biomedical Engineering, University of California, Irvine, CA, 92697, USA.

Department of Chemical and Biomolecular Engineering, University of California, Irvine, CA, 92697, USA.

出版信息

Biotechnol J. 2018 Dec;13(12):e1800140. doi: 10.1002/biot.201800140. Epub 2018 Sep 21.

Abstract

Collagen is the most abundant protein in the extracellular matrix (ECM), and it can direct the behavior of the neighboring cells. By customizing properties of collagen, it is possible to control the cells that interact with it. Utilizing a bottom-up strategy, modular gene fragments are assembled and recombinantly processed to create collagen-mimetic variants that modulate proteolytic degradation, cell adhesion, and mechanical characteristics. The removal of the native MMP cleavage site results in MMP-1 resistant collagen. By introducing additional MMP-susceptible sequences, the degradation characteristics of collagen molecules are modified. Additional non-native functionality is also introduced into the collagen, including the IKVAV sequence, which has been implicated in neurite outgrowth. This mutation, which disrupts the Gly-X-Y tripeptide repeat of collagen, does not prevent the formation of triple-helical collagen. Non-native cysteines and the integrin binding sequence GFOGER are combined in the collagen, and encapsulation of normal human lung fibroblasts within collagen hydrogels are tested. Cells remain spherical, when encapsulated within hydrogels of collagen variants in which the native integrin binding sites are removed, but cell adhesion is restored with the introduction of non-native GFOGER binding sequences. This modular collagen system allows for the combination of multiple functionalities, and it enables the production of biomimetic scaffolds with customizable characteristics to modulate cellular microenvironments.

摘要

胶原蛋白是细胞外基质(ECM)中含量最丰富的蛋白质,它可以指导相邻细胞的行为。通过定制胶原蛋白的特性,可以控制与之相互作用的细胞。利用自下而上的策略,将模块化的基因片段进行组装和重组处理,以创建模拟胶原蛋白的变体,从而调节蛋白水解降解、细胞黏附和机械特性。去除天然的 MMP 切割位点可产生 MMP-1 抗性胶原蛋白。通过引入额外的 MMP 易感性序列,可以改变胶原蛋白分子的降解特性。还可以向胶原蛋白中引入额外的非天然功能,包括 IKVAV 序列,该序列与神经突生长有关。这种突变破坏了胶原蛋白的 Gly-X-Y 三肽重复序列,但不会阻止三螺旋胶原蛋白的形成。非天然半胱氨酸和整合素结合序列 GFOGER 被组合在胶原蛋白中,并测试了正常的人肺成纤维细胞在胶原蛋白水凝胶中的包封。当包封在去除天然整合素结合位点的胶原蛋白变体的水凝胶中时,细胞保持球形,但通过引入非天然 GFOGER 结合序列可以恢复细胞黏附。这种模块化的胶原蛋白系统允许多种功能的组合,并能够生产具有可定制特性的仿生支架,以调节细胞微环境。

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