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应用于视网膜假体的组织工程:释放神经营养因子的聚合物水凝胶涂层

Tissue Engineering Applied to the Retinal Prosthesis: Neurotrophin-Eluting Polymeric Hydrogel Coatings.

作者信息

Winter Jessica O, Gokhale Mrudula, Jensen Ralph J, Cogan Stuart F, Rizzo Joseph F

机构信息

Center for Innovative Visual Rehabilitation, VA Medical Center, Boston, MA.

出版信息

Mater Sci Eng C Mater Biol Appl. 2008 Apr 1;28(3):448-453. doi: 10.1016/j.msec.2007.04.011.

Abstract

Several groups are developing visual prostheses to aid patients with vision loss. While these devices have shown some success in the clinic, they are severely limited by poor resolution, and in many cases have as few as 15 electrodes. Pixel density is poor because high stimulation thresholds require large electrodes to minimize charge density that would otherwise damage the electrode and tissue. A significant contributor to high stimulation threshold requirements is poor biocompatibility. We investigated the application of one system popular in tissue engineering, drug-releasing hydrogels, as a mechanism to improve the tissue-electrode interface. Hydrogels studied (i.e., PEGPLA photocrosslinkable polymers) released neurotrophic factors (i.e., BDNF) known to promote neuron survival and neurite extension in the retina. Hydrogels were examined in co-culture with retinal explants for 7 and 14 days, at which time neurite extension and neurite density was measured. Neurite extension was enhanced in samples exposed to BDNF-releasing hydrogels at 7 days; however, these increases were absent by day 14 suggesting declining drug release. Thus, PEGPLA hydrogels are excellent candidates for short-term (< 14 day) acute release of therapeutic factors in the retina, but will require additional modifications for application with neural prostheses. Additionally, these results suggest that the effects of neurotrophic factors are short-lived in the absence of additional support cues, and tissue engineering systems employing such factors may only produce transient benefits to the patient.

摘要

几个研究小组正在研发视觉假体,以帮助视力受损患者。虽然这些设备在临床上已显示出一定成效,但它们因分辨率低而受到严重限制,而且在许多情况下电极数量少至15个。像素密度低是因为高刺激阈值需要大电极来最小化电荷密度,否则会损坏电极和组织。高刺激阈值要求的一个重要因素是生物相容性差。我们研究了组织工程中一种常用系统——药物释放水凝胶的应用,作为改善组织-电极界面的一种机制。所研究的水凝胶(即聚乙二醇-聚乳酸光交联聚合物)释放已知能促进视网膜神经元存活和神经突延伸的神经营养因子(即脑源性神经营养因子)。将水凝胶与视网膜外植体共培养7天和14天,然后测量神经突延伸和神经突密度。在第7天,暴露于释放脑源性神经营养因子水凝胶的样本中神经突延伸增强;然而,到第14天这些增加消失,表明药物释放减少。因此,聚乙二醇-聚乳酸水凝胶是视网膜治疗因子短期(<14天)急性释放的极佳候选材料,但与神经假体一起应用时需要进行额外修饰。此外,这些结果表明,在没有额外支持线索的情况下,神经营养因子的作用是短暂的,采用这些因子的组织工程系统可能只会给患者带来短暂的益处。

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本文引用的文献

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Retinal prostheses: current challenges and future outlook.视网膜假体:当前挑战与未来展望。
J Biomater Sci Polym Ed. 2007;18(8):1031-55. doi: 10.1163/156856207781494403.

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