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细胞外基质硬度的增加会抑制轴突的延伸、生长锥的面积和 F-肌动蛋白在胶原 I 三维培养物中的水平。

Extracellular matrix stiffness negatively affects axon elongation, growth cone area and F-actin levels in a collagen type I 3D culture.

机构信息

Departamento de Neurofarmacología Experimental, Instituto de Investigaciones Biológicas Clemente Estable (IIBCE), Montevideo, Uruguay.

Laboratorio de Biología Celular, Departamento de Neurofarmacología Experimental, Instituto de Investigaciones Biológicas Clemente Estable (IIBCE), Montevideo, Uruguay.

出版信息

J Tissue Eng Regen Med. 2022 Feb;16(2):151-162. doi: 10.1002/term.3269. Epub 2021 Nov 29.

Abstract

Three dimensional (3D) in vitro neuronal cultures can better reproduce physiologically relevant phenotypes compared to 2D-cultures, because in vivo neurons reside in a 3D microenvironment. Interest in neuronal 3D cultures is emerging, with special attention to the mechanical forces that regulate axon elongation and sprouting in three dimensions. Type I collagen (Col-I) is a native substrate since it is present in the extracellular matrix and hence emulates an in vivo environment to study axon growth. The impact of its mechanical properties needs to be further investigated. Here, we generated Col-I 3D matrices of different mechanical stiffness and evaluated axon growth in three dimensions. Superior cervical ganglion (SCG) explants from neonatal rats were cultured in soft and stiff Col-I 3D matrices and neurite outgrowth was assessed by measuring: maximum neuritic extent; neuritic halo area and fasciculation. Axonal cytoskeletal proteins were examined. Axon elongation in stiff Col-I 3D matrices was reduced (31%) following 24 h in culture compared to soft matrices. In stiff matrices, neurites fasciculated and formed less dense halos. Consistently, almost no F-actin rich growth cones were recognized, and F-actin staining was strongly reduced in the axonal compartment. This study shows that stiffness negatively affects 3D neurite outgrowth and adds insights on the cytoskeletal responses upon mechanic interactions of axons with a 3D environment. Our data will serve to facilitate the development of model systems that are mechanically well-behaved but still mimic key physiologic properties observed in vivo.

摘要

三维(3D)体外神经元培养物可以比 2D 培养更好地再现生理相关表型,因为体内神经元存在于 3D 微环境中。人们对神经元 3D 培养的兴趣正在兴起,特别关注调节轴突伸长和 3D 中发芽的机械力。I 型胶原蛋白(Col-I)是一种天然基质,因为它存在于细胞外基质中,因此可以模拟体内环境来研究轴突生长。需要进一步研究其机械性能的影响。在这里,我们生成了不同机械刚度的 Col-I 3D 基质,并在 3D 中评估了轴突生长。从新生大鼠的颈上神经节(SCG)外植体在软和硬 Col-I 3D 基质中培养,并通过测量最大神经突延伸度;神经突晕面积和聚集来评估神经突生长。检查了轴突细胞骨架蛋白。与软基质相比,在硬 Col-I 3D 基质中培养 24 小时后,轴突伸长减少了(31%)。在硬基质中,神经突聚集并形成不那么密集的晕圈。一致地,几乎没有识别到富含 F-肌动蛋白的生长锥,并且在轴突区中 F-肌动蛋白染色明显减少。这项研究表明,刚度会对 3D 神经突生长产生负面影响,并为轴突与 3D 环境的力学相互作用引起的细胞骨架反应提供了新的见解。我们的数据将有助于开发机械性能良好但仍能模拟体内观察到的关键生理特性的模型系统。

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