细胞粘附配体呈递对五肽超分子组装和凝胶化的影响:模拟和实验。

IF 2.9 4区 生物学 Q1 ANATOMY & MORPHOLOGY Cells Tissues Organs Pub Date : 2023-01-01 Epub Date: 2023-09-26 DOI:10.1159/000534280
Andrew T Thede, James D Tang, Clare E Cocker, Liza J Harold, Connor D Amelung, Anna R Kittel, Phillip A Taylor, Kyle J Lampe
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引用次数: 0

摘要

细胞外基质(ECM)是一种复杂的、分级的物质,含有结构和生物活性成分。这种复杂性使得生物力学特性和细胞-基质相互作用的影响难以解耦,尤其是在3D环境中研究细胞过程时。基质力学和细胞粘附都是干细胞增殖和分化等特定细胞过程的已知调节因子。然而,还需要更多关于这些变量如何影响各种神经谱系的信息,这些神经谱系在移植后可以在治疗上改善中枢神经系统(CNS)损伤或疾病后的神经功能。用于注射递送的快速组装五肽(RAPID)水凝胶是实现这些目标的一种生物材料方法,由在生理介质中组装成物理水凝胶的肽序列家族组成。在这项研究中,我们研究了我们之前报道的用ECM衍生的细胞粘附肽配体RGD、IKVAV和YIGSR功能化的超分子组装RAPID水凝胶。使用分子动力学模拟和实验流变学,我们证明这些整合素结合配体在生理浓度(3-12mM)下不影响KYFIL肽系统的组装。在模拟中,组装的分子测量,如氢键和π-π相互作用,似乎不受细胞粘附序列或浓度的影响。聚类的可视化和溶剂可及表面积(SASA)的分析表明整合素结合结构域仍然暴露。含有3mM整合素结合结构域的KYFIL或AYFIL水凝胶产生与其非官能化等价物一致的机械性能。这种用细胞粘附序列掺杂RAPID凝胶的策略允许精确调节肽配体浓度,而与流变特性无关。RAPID水凝胶系统的可控性为研究整合素结合相互作用对封装的神经细胞的影响提供了机会,以了解水凝胶微环境如何影响生长、成熟或分化。
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Effects of Cell-Adhesive Ligand Presentation on Pentapeptide Supramolecular Assembly and Gelation: Simulations and Experiments.

The extracellular matrix (ECM) is a complex, hierarchical material containing structural and bioactive components. This complexity makes decoupling the effects of biomechanical properties and cell-matrix interactions difficult, especially when studying cellular processes in a 3D environment. Matrix mechanics and cell adhesion are both known regulators of specific cellular processes such as stem cell proliferation and differentiation. However, more information is required about how such variables impact various neural lineages that could, upon transplantation, therapeutically improve neural function after a central nervous system injury or disease. Rapidly Assembling Pentapeptides for Injectable Delivery (RAPID) hydrogels are one biomaterial approach to meet these goals, consisting of a family of peptide sequences that assemble into physical hydrogels in physiological media. In this study, we studied our previously reported supramolecularly-assembling RAPID hydrogels functionalized with the ECM-derived cell-adhesive peptide ligands RGD, IKVAV, and YIGSR. Using molecular dynamics simulations and experimental rheology, we demonstrated that these integrin-binding ligands at physiological concentrations (3-12 mm) did not impact the assembly of the KYFIL peptide system. In simulations, molecular measures of assembly such as hydrogen bonding and pi-pi interactions appeared unaffected by cell-adhesion sequence or concentration. Visualizations of clustering and analysis of solvent-accessible surface area indicated that the integrin-binding domains remained exposed. KYFIL or AYFIL hydrogels containing 3 mm of integrin-binding domains resulted in mechanical properties consistent with their non-functionalized equivalents. This strategy of doping RAPID gels with cell-adhesion sequences allows for the precise tuning of peptide ligand concentration, independent of the rheological properties. The controllability of the RAPID hydrogel system provides an opportunity to investigate the effect of integrin-binding interactions on encapsulated neural cells to discern how hydrogel microenvironment impacts growth, maturation, or differentiation.

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来源期刊
Cells Tissues Organs
Cells Tissues Organs 生物-发育生物学
CiteScore
4.90
自引率
3.70%
发文量
45
审稿时长
6-12 weeks
期刊介绍: ''Cells Tissues Organs'' aims at bridging the gap between cell biology and developmental biology and the emerging fields of regenerative medicine (stem cell biology, tissue engineering, artificial organs, in vitro systems and transplantation biology). CTO offers a rapid and fair peer-review and exquisite reproduction quality. Special topic issues, entire issues of the journal devoted to a single research topic within the range of interests of the journal, are published at irregular intervals.
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