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用于设计 ECM 模拟生物材料的组织特异性参数。

Tissue-specific parameters for the design of ECM-mimetic biomaterials.

机构信息

Paul M. Rady Department of Mechanical Engineering, University of Colorado - Boulder, 1111 Engineering Center, 427 UCB, Boulder, CO 80309, United States.

Paul M. Rady Department of Mechanical Engineering, University of Colorado - Boulder, 1111 Engineering Center, 427 UCB, Boulder, CO 80309, United States.

出版信息

Acta Biomater. 2021 Sep 15;132:83-102. doi: 10.1016/j.actbio.2021.04.017. Epub 2021 Apr 18.

Abstract

The extracellular matrix (ECM) is a complex network of biomolecules that mechanically and biochemically directs cell behavior and is crucial for maintaining tissue function and health. The heterogeneous organization and composition of the ECM varies within and between tissue types, directing mechanics, aiding in cell-cell communication, and facilitating tissue assembly and reassembly during development, injury and disease. As technologies like 3D printing rapidly advance, researchers are better able to recapitulate in vivo tissue properties in vitro; however, tissue-specific variations in ECM composition and organization are not given enough consideration. This is in part due to a lack of information regarding how the ECM of many tissues varies in both homeostatic and diseased states. To address this gap, we describe the components and organization of the ECM, and provide examples for different tissues at various states of disease. While many aspects of ECM biology remain unknown, our goal is to highlight the complexity of various tissues and inspire engineers to incorporate unique components of the native ECM into in vitro platform design and fabrication. Ultimately, we anticipate that the use of biomaterials that incorporate key tissue-specific ECM will lead to in vitro models that better emulate human pathologies. STATEMENT OF SIGNIFICANCE: Biomaterial development primarily emphasizes the engineering of new materials and therapies at the expense of identifying key parameters of the tissue that is being emulated. This can be partially attributed to the difficulty in defining the 3D composition, organization, and mechanics of the ECM within different tissues and how these material properties vary as a function of homeostasis and disease. In this review, we highlight a range of tissues throughout the body and describe how ECM content, cell diversity, and mechanical properties change in diseased tissues and influence cellular behavior. Accurately mimicking the tissue of interest in vitro by using ECM specific to the appropriate state of homeostasis or pathology in vivo will yield results more translatable to humans.

摘要

细胞外基质 (ECM) 是一种生物分子的复杂网络,它在机械和生化方面指导细胞行为,对于维持组织功能和健康至关重要。ECM 的异质组织和组成在组织类型内和之间变化,指导力学、辅助细胞间通讯,并在发育、损伤和疾病过程中促进组织组装和重新组装。随着 3D 打印等技术的快速发展,研究人员能够更好地在体外重现体内组织特性;然而,ECM 组成和组织的组织特异性变化并没有得到足够的考虑。部分原因是缺乏有关许多组织的 ECM 在稳态和患病状态下如何变化的信息。为了解决这一差距,我们描述了 ECM 的组成部分和组织,并提供了不同组织在不同疾病状态下的示例。虽然 ECM 生物学的许多方面仍然未知,但我们的目标是强调各种组织的复杂性,并激励工程师将天然 ECM 的独特成分纳入体外平台设计和制造中。最终,我们预计使用包含关键组织特异性 ECM 的生物材料将导致更好地模拟人类病理学的体外模型。

意义陈述

生物材料的发展主要侧重于新材料和疗法的工程,而忽略了确定被模拟组织的关键参数。这在一定程度上归因于难以定义不同组织内 ECM 的 3D 组成、组织和力学特性,以及这些材料特性如何随稳态和疾病而变化。在这篇综述中,我们突出了身体各个部位的一系列组织,并描述了 ECM 含量、细胞多样性和机械特性如何在患病组织中发生变化以及如何影响细胞行为。通过使用体内适当稳态或病理状态特有的 ECM 来准确模拟体外感兴趣的组织,将产生更适合人类的可翻译结果。

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