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基质刚度调节三维水凝胶包裹的人诱导多能干细胞来源内皮祖细胞的机械转导和血管网络形成。

Matrix Stiffness Regulates Mechanotransduction and Vascular Network Formation of hiPSC-Derived Endothelial Progenitors Encapsulated in 3D Hydrogels.

作者信息

Han Jiwan, Halwachs Kathleen, West Toni, Larsen Bryce, Sacks Michael S, Rosales Adrianne M, Zoldan Janet

出版信息

bioRxiv. 2025 Apr 30:2025.04.11.648340. doi: 10.1101/2025.04.11.648340.

Abstract

The mechanical properties of the extracellular matrix (ECM), particularly stiffness, regulate endothelial progenitor responses during vascular development, yet their behavior in physiologically compliant matrices (<1 kPa) remains underexplored. Using norbornene-modified hyaluronic acid (NorHA) hydrogels with tunable stiffness (190-884 Pa), we investigated how hydrogel stiffness influences cell morphology, endothelial maturation, mechanotransduction, and microvascular network formation in human induced pluripotent stem cell-derived endothelial progenitors (hiPSC-EPs). Our findings reveal a stiffness-dependent tradeoff between mechanotransduction and vascular network formation. At intermediate stiffness (551 Pa), cells exhibited the greatest increase in endothelial marker CD31 expression and Yes-associated protein (YAP)/ transcriptional coactivator with PDZ-binding motif (TAZ) nuclear translocation, indicating enhanced mechanotransduction and endothelial maturation. However, this did not translate to superior plexus formation. Instead, the most compliant matrix (190 Pa) supported greater vascular connectivity, characterized by longer branches (∼0.03/volume vs. 0.015 at 551 Pa) and enhanced actin remodeling. 3D cell contraction measurements revealed a 15.6-fold higher basal displacement in compliant hydrogels, suggesting that cell-generated forces and matrix deformability collectively drive vascular morphogenesis. Unlike prior studies focusing on pathological stiffness ranges (>10 kPa), our results emphasize that vascularization is not solely driven by the most mechanotransductive environment but rather by a balance of compliance, contractility, and cell-induced remodeling. These findings underscore the need to design hydrogels that provide sufficient mechanotransduction for endothelial maturation while maintaining compliance to support dynamic vascular morphogenesis. This work provides a mechanically tuned framework for optimizing microenvironments to balance endothelial differentiation and vascular network formation in tissue engineering and regenerative medicine.

摘要

细胞外基质(ECM)的力学特性,尤其是硬度,在血管发育过程中调节内皮祖细胞的反应,然而它们在生理顺应性基质(<1 kPa)中的行为仍未得到充分研究。我们使用具有可调硬度(190 - 884 Pa)的降冰片烯修饰的透明质酸(NorHA)水凝胶,研究了水凝胶硬度如何影响人诱导多能干细胞衍生的内皮祖细胞(hiPSC - EPs)的细胞形态、内皮成熟、机械转导和微血管网络形成。我们的研究结果揭示了机械转导和血管网络形成之间的硬度依赖性权衡。在中等硬度(551 Pa)下,细胞在内皮标志物CD31表达和Yes相关蛋白(YAP)/具有PDZ结合基序的转录共激活因子(TAZ)核转位方面表现出最大增加,表明机械转导和内皮成熟增强。然而,这并未转化为更优的丛状结构形成。相反,最顺应的基质(190 Pa)支持更大的血管连通性,其特征是分支更长(~0.03/体积,而在551 Pa时为0.015)和肌动蛋白重塑增强。三维细胞收缩测量显示,顺应性水凝胶中的基础位移高15.6倍,这表明细胞产生的力和基质可变形性共同驱动血管形态发生。与之前关注病理硬度范围(>10 kPa)的研究不同,我们的结果强调血管生成并非仅由机械转导性最强的环境驱动,而是由顺应性、收缩性和细胞诱导重塑之间的平衡驱动。这些发现强调了设计水凝胶的必要性,这种水凝胶要为内皮成熟提供足够的机械转导,同时保持顺应性以支持动态血管形态发生。这项工作提供了一个机械调节的框架,用于优化微环境,以平衡组织工程和再生医学中的内皮分化和血管网络形成。

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