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探索一种溶剂依赖的策略来控制基于层粘连蛋白模拟短肽的超分子水凝胶的自组装行为和细胞相互作用。

Exploring a Solvent Dependent Strategy to Control Self-Assembling Behavior and Cellular Interaction in Laminin-Mimetic Short Peptide based Supramolecular Hydrogels.

机构信息

Chemical Biology Unit, Institute of Nano Science and Technology, Sector-81, Knowledge City Mohali, Punjab,140306, India.

出版信息

Chembiochem. 2024 Apr 16;25(8):e202300835. doi: 10.1002/cbic.202300835. Epub 2024 Mar 25.

Abstract

Self-assembled hydrogels, fabricated through diverse non-covalent interactions, have been extensively studied in regenerative medicines. Inspired from bioactive functional motifs of ECM protein, short peptide sequences have shown remarkable abilities to replicate the intrinsic features of the natural extracellular milieu. In this direction, we have fabricated two short hydrophobic bioactive sequences derived from the laminin protein i. e., IKVAV and YIGSR. Based on the substantial hydrophobicity of these peptides, we selected a co-solvent approach as a suitable gelation technique that included different concentrations of DMSO as an organic phase along with an aqueous solution containing 0.1 % TFA. These hydrophobic laminin-based bioactive peptides with limited solubility in aqueous physiological environment showed significantly enhanced solubility with higher DMSO content in water. The enhanced solubility resulted in extensive intermolecular interactions that led to the formation of hydrogels with a higher-order entangled network along with improved mechanical properties. Interestingly, by simply modulating DMSO content, highly tunable gels were accessed in the same gelator domain that displayed differential physicochemical properties. Further, the cellular studies substantiated the potential of these laminin-derived hydrogels in enhancing cell-matrix interactions, thereby reinforcing their applications in tissue engineering.

摘要

自组装水凝胶通过多种非共价相互作用制备,在再生医学中得到了广泛研究。受 ECM 蛋白生物活性功能基序的启发,短肽序列显示出显著的能力,可以复制天然细胞外环境的固有特征。在这个方向上,我们制备了两种源自层粘连蛋白的短疏水性生物活性序列,即 IKVAV 和 YIGSR。基于这些肽的显著疏水性,我们选择共溶剂方法作为合适的凝胶化技术,该方法包括不同浓度的 DMSO 作为有机相,以及含有 0.1%TFA 的水溶液。这些疏水性层粘连蛋白基生物活性肽在生理环境中的水中溶解度有限,随着 DMSO 含量的增加,其溶解度显著提高。增强的溶解度导致形成具有更高阶缠结网络的水凝胶,以及改善的机械性能。有趣的是,通过简单地调节 DMSO 含量,在同一凝胶剂域中可以获得高度可调的凝胶,这些凝胶表现出不同的物理化学性质。此外,细胞研究证实了这些源自层粘连蛋白的水凝胶在增强细胞-基质相互作用方面的潜力,从而加强了它们在组织工程中的应用。

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