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聚酰亚胺绝缘微丝的肽修饰:通过减少胶质瘢痕形成提高生物相容性。

Peptide modification of polyimide-insulated microwires: Towards improved biocompatibility through reduced glial scarring.

作者信息

Sridar Sangita, Churchward Matthew A, Mushahwar Vivian K, Todd Kathryn G, Elias Anastasia L

机构信息

Chemical and Materials Engineering, University of Alberta, Edmonton, AB T6G 1H9, Canada; Alberta Innovates-Health Solutions Interdisciplinary Team in Smart Neural Prostheses (Project SMART), University of Alberta, AB, Canada.

Neurochemical Research Unit, Department of Psychiatry, University of Alberta, Edmonton, AB T6G 2G3, Canada; Neuroscience and Mental Health Institute, University of Alberta, Edmonton, AB T6G 2E1, Canada; Alberta Innovates-Health Solutions Interdisciplinary Team in Smart Neural Prostheses (Project SMART), University of Alberta, AB, Canada.

出版信息

Acta Biomater. 2017 Sep 15;60:154-166. doi: 10.1016/j.actbio.2017.07.026. Epub 2017 Jul 19.

Abstract

UNLABELLED

The goal of this study is to improve the integration of implanted microdevices with tissue in the central nervous system (CNS). The long-term utility of neuroprosthetic devices implanted in the CNS is affected by the formation of a scar by resident glial cells (astrocytes and microglia), limiting the viability and functional stability of the devices. Reduction in the proliferation of glial cells is expected to enhance the biocompatibility of devices. We demonstrate the modification of polyimide-insulated microelectrodes with a bioactive peptide KHIFSDDSSE. Microelectrode wires were functionalized with (3-aminopropyl) triethoxy silane (APTES); the peptide was then covalently bonded to the APTES. The soluble peptide was tested in 2D mixed cultures of astrocytes and microglia, and reduced the proliferation of both cell types. The interactions of glial cells with the peptide-modified wires was then examined in 3D cell-laden hydrogels by immunofluorescence microscopy. As expected for uncoated wires, the microglia were first attracted to the wire (7days) followed by astrocyte recruitment and hypertrophy (14days). For the peptide-treated wires, astrocytes coated the wires directly (24h), and formed a thin, stable coating without evidence of hypertrophy, and the attraction of microglia to the wire was significantly reduced. The results suggest a mechanism to improve tissue integration by promoting uniform coating of astrocytes on a foreign body while lessening the reactive response of microglia. We conclude that the bioactive peptide KHIFSDDSSE may be effective in improving the biocompatibility of neural interfaces by both reducing acute glial reactivity and generating stable integration with tissue.

STATEMENT OF SIGNIFICANCE

The peptide KHIFSDDSSE has previously been shown in vitro to both reduce the proliferation of astrocytes, and to increase the adhesion of astrocyte to glass substrates. Here, we demonstrate a method to apply uniform coatings of peptides to microwires, which could readily be generalized to other peptides and surfaces. We then show that when peptide-modified wires are inserted into 3D cell-laden hydrogels, the normal cellular reaction (microglial activation followed by astrocyte recruitment and hypertrophy) does not occur, rather astrocytes are attracted directly to the surface of the wire, forming a relatively thin and uniform coating. This suggests a method to improve tissue integration of implanted devices to reduce glial scarring and ultimately reduce failure of neural interfaces.

摘要

未标注

本研究的目标是改善植入式微型设备与中枢神经系统(CNS)组织的整合。植入中枢神经系统的神经假体装置的长期效用受到驻留神经胶质细胞(星形胶质细胞和小胶质细胞)形成瘢痕的影响,限制了装置的生存能力和功能稳定性。神经胶质细胞增殖的减少有望提高装置的生物相容性。我们展示了用生物活性肽KHIFSDDSSE对聚酰亚胺绝缘微电极进行修饰。微电极丝用(3-氨丙基)三乙氧基硅烷(APTES)进行功能化;然后将肽共价键合到APTES上。在星形胶质细胞和小胶质细胞的二维混合培养物中测试了可溶性肽,其减少了两种细胞类型的增殖。然后通过免疫荧光显微镜在三维载细胞水凝胶中检查神经胶质细胞与肽修饰丝的相互作用。正如未涂层丝所预期的那样,小胶质细胞首先被丝吸引(7天),随后是星形胶质细胞的募集和肥大(14天)。对于肽处理的丝,星形胶质细胞直接覆盖在丝上(24小时),并形成薄而稳定的涂层,没有肥大的迹象,并且小胶质细胞对丝的吸引力显著降低。结果表明了一种通过促进星形胶质细胞在异物上均匀覆盖同时减少小胶质细胞的反应性反应来改善组织整合的机制。我们得出结论,生物活性肽KHIFSDDSSE可能通过减少急性神经胶质反应性和与组织产生稳定整合来有效改善神经界面的生物相容性。

重要性声明

肽KHIFSDDSSE先前已在体外显示既能减少星形胶质细胞的增殖,又能增加星形胶质细胞对玻璃基质的粘附。在此,我们展示了一种将肽均匀涂层应用于微丝的方法,该方法可以很容易地推广到其他肽和表面。然后我们表明,当将肽修饰的丝插入三维载细胞水凝胶中时,正常的细胞反应(小胶质细胞激活,随后是星形胶质细胞募集和肥大)不会发生,相反,星形胶质细胞直接被吸引到丝的表面,形成相对薄且均匀的涂层。这表明了一种改善植入装置的组织整合以减少神经胶质瘢痕形成并最终减少神经界面失败的方法。

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