Bioinspired Hyaluronic Acid-Based Hydrogel Fuels Bi-Directional Lung Organoid Maturation via PIEZO1 and ITGB1 Mediated Mechanosensation

IF 4.3 3区 材料科学 Q2 CHEMISTRY, MULTIDISCIPLINARY Advanced Materials Interfaces Pub Date : 2024-09-03 DOI:10.1002/admi.202400194
Junyao Zhang, Daniele Marciano, Lei Wang, Weiwei Wang, Manfred Gossen, Mengting Yang, Tingying Peng, Julien Gautrot, Xun Xu, Nan Ma
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Abstract

Lung diseases are one of the leading causes of global mortality. Advances in induced pluripotent stem cell (iPSC) differentiation have enabled the creation of bronchiolar and alveolar lung organoids, advancing research on lung conditions. Traditional Matrigel encapsulation, reliant on the spontaneous assembly and propagation of cells with limited external intervention, often results in variability and low reproducibility. The absence of hyaluronic acid (HA) in Matrigel, a key lung extracellular matrix component, limits bronchiolar and alveolar cell differentiation, reducing the efficacy and reproducibility of iPSC-derived organoid generation. To address this, a novel hybrid hydrogel combining HA and 23% Matrigel, inspired by the natural lung environment, is developed. This hydrogel offers improved biochemical support and viscoelastic properties, significantly accelerating organoid development. Within eight days, the hydrogel produces uniformly sized organoids containing both bronchiolar and alveolar epithelial cells. Increased levels of active mechanosensors and transducers, including PIEZO1, Integrin, and Myosin, suggest that the hydrogel's altered viscoelasticity triggers a mechanotransduction cascade. This bioinspired hydrogel provides a robust, fast model for biomedical research, facilitating rapid drug screening, respiratory disease treatment studies, and surfactant trafficking investigations. Furthermore, it enables the exploration of underlying biomechanical mechanisms to enhance the controllability of organoid generation and maturation.

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基于生物启发的透明质酸水凝胶通过 PIEZO1 和 ITGB1 介导的机械感觉促进双向肺器官样体成熟
肺部疾病是导致全球死亡的主要原因之一。诱导多能干细胞(iPSC)分化技术的进步使得支气管和肺泡肺器官组织得以创建,从而推动了肺部疾病的研究。传统的 Matrigel 包裹法依赖于细胞在有限的外部干预下自发组装和繁殖,但往往导致变异和可重复性低。透明质酸(HA)是肺细胞外基质的关键成分,Matrigel 中透明质酸的缺失限制了支气管和肺泡细胞的分化,降低了 iPSC 衍生类器官生成的有效性和可重复性。为了解决这个问题,我们开发了一种新型混合水凝胶,它结合了 HA 和 23% Matrigel,其灵感来源于自然肺环境。这种水凝胶提供了更好的生化支持和粘弹性能,大大加快了类器官的发育。在八天内,这种水凝胶就能产生大小一致的类器官,其中包含支气管和肺泡上皮细胞。活性机械传感器和换能器(包括 PIEZO1、整合素和肌球蛋白)水平的提高表明,水凝胶粘弹性的改变触发了机械传导级联。这种生物启发水凝胶为生物医学研究提供了一个稳健、快速的模型,有助于快速筛选药物、呼吸系统疾病治疗研究和表面活性物质贩运研究。此外,它还有助于探索潜在的生物力学机制,从而提高类器官生成和成熟的可控性。
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来源期刊
Advanced Materials Interfaces
Advanced Materials Interfaces CHEMISTRY, MULTIDISCIPLINARY-MATERIALS SCIENCE, MULTIDISCIPLINARY
CiteScore
8.40
自引率
5.60%
发文量
1174
审稿时长
1.3 months
期刊介绍: Advanced Materials Interfaces publishes top-level research on interface technologies and effects. Considering any interface formed between solids, liquids, and gases, the journal ensures an interdisciplinary blend of physics, chemistry, materials science, and life sciences. Advanced Materials Interfaces was launched in 2014 and received an Impact Factor of 4.834 in 2018. The scope of Advanced Materials Interfaces is dedicated to interfaces and surfaces that play an essential role in virtually all materials and devices. Physics, chemistry, materials science and life sciences blend to encourage new, cross-pollinating ideas, which will drive forward our understanding of the processes at the interface. Advanced Materials Interfaces covers all topics in interface-related research: Oil / water separation, Applications of nanostructured materials, 2D materials and heterostructures, Surfaces and interfaces in organic electronic devices, Catalysis and membranes, Self-assembly and nanopatterned surfaces, Composite and coating materials, Biointerfaces for technical and medical applications. Advanced Materials Interfaces provides a forum for topics on surface and interface science with a wide choice of formats: Reviews, Full Papers, and Communications, as well as Progress Reports and Research News.
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