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星形胶质细胞的转录组分析和3D生物工程表明,ROCK抑制可产生营养性星形胶质细胞增生。

Transcriptomic analysis and 3D bioengineering of astrocytes indicate ROCK inhibition produces cytotrophic astrogliosis.

作者信息

O'Shea Ross D, Lau Chew L, Zulaziz Natasha, Maclean Francesca L, Nisbet David R, Horne Malcolm K, Beart Philip M

机构信息

Department of Physiology, Anatomy and Microbiology, La Trobe University Bundoora, VIC, Australia.

Florey Institute of Neuroscience and Mental Health, University of Melbourne Parkville, VIC, Australia.

出版信息

Front Neurosci. 2015 Feb 20;9:50. doi: 10.3389/fnins.2015.00050. eCollection 2015.

Abstract

Astrocytes provide trophic, structural and metabolic support to neurons, and are considered genuine targets in regenerative neurobiology, as their phenotype arbitrates brain integrity during injury. Inhibitors of Rho kinase (ROCK) cause stellation of cultured 2D astrocytes, increased L-glutamate transport, augmented G-actin, and elevated expression of BDNF and anti-oxidant genes. Here we further explored the signposts of a cytotrophic, "healthy" phenotype by data-mining of our astrocytic transcriptome in the presence of Fasudil. Gene expression profiles of motor and autophagic cellular cascades and inflammatory/angiogenic responses were all inhibited, favoring adoption of an anti-migratory phenotype. Like ROCK inhibition, tissue engineered bioscaffolds can influence the extracellular matrix. We built upon our evidence that astrocytes maintained on 3D poly-ε-caprolactone (PCL) electrospun scaffolds adopt a cytotrophic phenotype similar to that produced by Fasudil. Using these procedures, employing mature 3D cultured astrocytes, Fasudil (100 μM) or Y27632 (30 μM) added for the last 72 h of culture altered arborization, which featured numerous additional minor processes as shown by GFAP and AHNAK immunolabelling. Both ROCK inhibitors decreased F-actin, but increased G-actin labeling, indicative of disassembly of actin stress fibers. ROCK inhibitors provide additional beneficial effects for bioengineered 3D astrocytes, including enlargement of the overall arbor. Potentially, the combined strategy of bio-compatible scaffolds with ROCK inhibition offers unique advantages for the management of glial scarring. Overall these data emphasize that manipulation of the astrocyte phenotype to achieve a "healthy biology" offers new hope for the management of inflammation in neuropathologies.

摘要

星形胶质细胞为神经元提供营养、结构和代谢支持,并且被认为是再生神经生物学中的真正靶点,因为它们的表型在损伤期间对脑完整性起仲裁作用。Rho激酶(ROCK)抑制剂可导致培养的二维星形胶质细胞形成星状,增加L-谷氨酸转运,增强G-肌动蛋白,并提高脑源性神经营养因子(BDNF)和抗氧化基因的表达。在这里,我们通过在法舒地尔存在的情况下对我们的星形胶质细胞转录组进行数据挖掘,进一步探索了一种营养性“健康”表型的标志。运动和自噬细胞级联反应以及炎症/血管生成反应的基因表达谱均受到抑制,有利于采用抗迁移表型。与ROCK抑制一样,组织工程生物支架可以影响细胞外基质。我们基于以下证据:维持在三维聚ε-己内酯(PCL)电纺支架上的星形胶质细胞采用类似于法舒地尔产生的营养性表型。使用这些方法,采用成熟的三维培养星形胶质细胞,在培养的最后72小时添加法舒地尔(100μM)或Y27632(30μM)可改变树突分支,其特征是出现许多额外的小分支,如GFAP和AHNAK免疫标记所示。两种ROCK抑制剂均降低F-肌动蛋白,但增加G-肌动蛋白标记,表明肌动蛋白应力纤维的解聚。ROCK抑制剂为生物工程三维星形胶质细胞提供了额外的有益作用,包括整体树突分支的扩大。潜在地,生物相容性支架与ROCK抑制的联合策略为胶质瘢痕的管理提供了独特的优势。总体而言,这些数据强调,操纵星形胶质细胞表型以实现“健康生物学”为神经病理学炎症的管理带来了新的希望。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/83dc/4335181/1d66dc53fdae/fnins-09-00050-g0001.jpg

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