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一种三维组织工程化的吻侧迁移流作为室下区来源细胞迁移的平台。

A three-dimensional tissue-engineered rostral migratory stream as an platform for subventricular zone-derived cell migration.

作者信息

Purvis Erin M, Garcia-Epelboim Andrés D, Krizman Elizabeth N, O'Donnell John C, Cullen D Kacy

机构信息

Center for Brain Injury and Repair, Department of Neurosurgery, Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, United States.

Center for Neurotrauma, Neurodegeneration and Restoration, Corporal Michael J. Crescenz Veterans Affairs Medical Center, Philadelphia, PA, United States.

出版信息

Front Bioeng Biotechnol. 2024 Jun 12;12:1410717. doi: 10.3389/fbioe.2024.1410717. eCollection 2024.

Abstract

In the brains of most adult mammals, neural precursor cells (NPCs) from the subventricular zone (SVZ) migrate through the rostral migratory stream (RMS) to replace olfactory bulb interneurons. Following brain injury, published studies have shown that NPCs can divert from the SVZ-RMS-OB route and migrate toward injured brain regions, but the quantity of arriving cells, the lack of survival and terminal differentiation of neuroblasts into neurons, and their limited capacity to re-connect into circuitry are insufficient to promote functional recovery in the absence of therapeutic intervention. Our lab has fabricated a biomimetic tissue-engineered rostral migratory stream (TE-RMS) that replicates some notable structural and functional components of the endogenous rat RMS. Based on the design attributes for the TE-RMS platform, it may serve as a regenerative medicine strategy to facilitate sustained neuronal replacement into an injured brain region or an tool to investigate cell-cell communication and neuroblast migration. Previous work has demonstrated that the TE-RMS replicates the basic structure, unique nuclear shape, cytoskeletal arrangement, and surface protein expression of the endogenous rat RMS. Here, we developed an enhanced TE-RMS fabrication method in hydrogel microchannels that allowed more robust and high-throughput TE-RMS assembly. We report unique astrocyte behavior, including astrocyte bundling into the TE-RMS, the presence of multiple TE-RMS bundles, and observations of discontinuities in TE-RMS bundles, when microtissues are fabricated in agarose microchannels containing different critical curved or straight geometric features. We also demonstrate that we can harvest NPCs from the SVZ of adult rat brains and that EGFP+ cells migrate in chain formation from SVZ neurospheres through the TE-RMS . Overall, the TE-RMS can be utilized as an platform to investigate the pivotal cell-cell signaling mechanisms underlying the synergy of molecular cues involved in immature neuronal migration and differentiation.

摘要

在大多数成年哺乳动物的大脑中,来自脑室下区(SVZ)的神经前体细胞(NPCs)通过吻侧迁移流(RMS)迁移,以替代嗅球中间神经元。脑损伤后,已发表的研究表明,NPCs可以从SVZ-RMS-OB途径转向并向损伤的脑区迁移,但到达的细胞数量、神经母细胞存活和终末分化为神经元的缺乏,以及它们重新连接到神经回路的能力有限,在没有治疗干预的情况下不足以促进功能恢复。我们实验室制造了一种仿生组织工程吻侧迁移流(TE-RMS),它复制了内源性大鼠RMS的一些显著结构和功能成分。基于TE-RMS平台的设计属性,它可以作为一种再生医学策略,以促进持续的神经元替代进入损伤的脑区,或者作为一种工具来研究细胞间通讯和神经母细胞迁移。先前的工作已经证明,TE-RMS复制了内源性大鼠RMS的基本结构、独特的核形状、细胞骨架排列和表面蛋白表达。在这里,我们开发了一种在水凝胶微通道中增强的TE-RMS制造方法,该方法允许更强大和高通量的TE-RMS组装。我们报告了独特的星形胶质细胞行为,包括星形胶质细胞聚集到TE-RMS中、多个TE-RMS束的存在,以及当在含有不同关键弯曲或直线几何特征的琼脂糖微通道中制造微组织时,观察到TE-RMS束中的不连续性。我们还证明,我们可以从成年大鼠大脑的SVZ中收获NPCs,并且EGFP+细胞以链状形式从SVZ神经球通过TE-RMS迁移。总体而言,TE-RMS可以用作一个平台,来研究未成熟神经元迁移和分化中涉及的分子线索协同作用的关键细胞间信号机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6213/11199690/3398afe10c5d/fbioe-12-1410717-g001.jpg

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