Stabilization and improved functionality of three-dimensional perfusable microvascular networks in microfluidic devices under macromolecular crowding.

IF 11.3 1区 医学 Q1 Medicine
Ho-Ying Wan, Jack Chun Hin Chen, Qinru Xiao, Christy Wingtung Wong, Boguang Yang, Benjamin Cao, Rocky S Tuan, Susan K Nilsson, Yi-Ping Ho, Michael Raghunath, Roger D Kamm, Anna Blocki
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引用次数: 3

Abstract

Background: There is great interest to engineer in vitro models that allow the study of complex biological processes of the microvasculature with high spatiotemporal resolution. Microfluidic systems are currently used to engineer microvasculature in vitro, which consists of perfusable microvascular networks (MVNs). These are formed through spontaneous vasculogenesis and exhibit the closest resemblance to physiological microvasculature. Unfortunately, under standard culture conditions and in the absence of co-culture with auxiliary cells as well as protease inhibitors, pure MVNs suffer from a short-lived stability.

Methods: Herein, we introduce a strategy for stabilization of MVNs through macromolecular crowding (MMC) based on a previously established mixture of Ficoll macromolecules. The biophysical principle of MMC is based on macromolecules occupying space, thus increasing the effective concentration of other components and thereby accelerating various biological processes, such as extracellular matrix deposition. We thus hypothesized that MMC will promote the accumulation of vascular ECM (basement membrane) components and lead to a stabilization of MVN with improved functionality.

Results: MMC promoted the enrichment of cellular junctions and basement membrane components, while reducing cellular contractility. The resulting advantageous balance of adhesive forces over cellular tension resulted in a significant stabilization of MVNs over time, as well as improved vascular barrier function, closely resembling that of in vivo microvasculature.

Conclusion: Application of MMC to MVNs in microfluidic devices provides a reliable, flexible and versatile approach to stabilize engineered microvessels under simulated physiological conditions.

Abstract Image

Abstract Image

Abstract Image

大分子拥挤条件下微流控装置中三维可灌注微血管网络的稳定性和功能改善。
背景:有很大的兴趣设计体外模型,允许研究微血管复杂的生物过程与高时空分辨率。微流体系统目前被用于体外微血管工程,它由可灌注微血管网络(MVNs)组成。它们是通过自发血管发生形成的,表现出与生理微血管最相似的特征。不幸的是,在标准培养条件下,在没有辅助细胞和蛋白酶抑制剂共同培养的情况下,纯MVNs的稳定性很短。方法:在此,我们介绍了一种基于先前建立的Ficoll大分子混合物的大分子拥挤(MMC)稳定MVNs的策略。MMC的生物物理原理是基于大分子占据空间,从而增加其他成分的有效浓度,从而加速各种生物过程,如细胞外基质沉积。因此,我们假设MMC会促进血管ECM(基底膜)成分的积累,并导致MVN的稳定和功能的改善。结果:MMC促进了细胞连接和基底膜成分的富集,同时降低了细胞的收缩性。随着时间的推移,粘附力与细胞张力之间的有利平衡导致了MVNs的显著稳定,并改善了血管屏障功能,与体内微血管非常相似。结论:将MMC应用于微流控装置的MVNs提供了一种可靠、灵活和通用的方法来稳定模拟生理条件下的工程微血管。
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来源期刊
Biomaterials Research
Biomaterials Research Medicine-Medicine (miscellaneous)
CiteScore
10.20
自引率
3.50%
发文量
63
审稿时长
30 days
期刊介绍: Biomaterials Research, the official journal of the Korean Society for Biomaterials, is an open-access interdisciplinary publication that focuses on all aspects of biomaterials research. The journal covers a wide range of topics including novel biomaterials, advanced techniques for biomaterial synthesis and fabrication, and their application in biomedical fields. Specific areas of interest include functional biomaterials, drug and gene delivery systems, tissue engineering, nanomedicine, nano/micro-biotechnology, bio-imaging, regenerative medicine, medical devices, 3D printing, and stem cell research. By exploring these research areas, Biomaterials Research aims to provide valuable insights and promote advancements in the biomaterials field.
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