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中风后向大脑注射水凝胶生物材料支架。

Injection of Hydrogel Biomaterial Scaffolds to The Brain After Stroke.

作者信息

Wilson Katrina L, Carmichael S Thomas, Segura Tatiana

机构信息

Department of Biomedical Engineering, Duke University.

Department of Neurology, University of California Los Angeles.

出版信息

J Vis Exp. 2020 Oct 1(164). doi: 10.3791/61450.

Abstract

Stroke is the leading cause of disability and the fifth-leading cause of death in the United States. Approximately 87% of all strokes are ischemic strokes and are defined as the sudden blockage of a vessel supplying blood to the brain. Within minutes of the blockage, cells begin to die and result in irreparable tissue damage. Current therapeutic treatments focus on clot removal or lysis to allow for the reperfusion and prevent more severe brain damage. Although transient brain plasticity may salvage some of the damaged tissue over time, significant fractions of patients are left with neurological deficits that will never resolve. There is a lack of therapeutic options to treat neurological deficits caused by stroke, emphasizing the need to develop new strategies to treat this growing patient population. Injectable biomaterials are currently being designed to enhance brain plasticity and improve endogenous repair through the delivery of active agents or stem cells. One method to test these approaches is to utilize a rodent stroke model, inject the biomaterial into the stroke core, and assess repair. Knowing the precise location of the stroke core is imperative for the accurate treatment after stroke, therefore, a stroke model that results in a predictable stroke location is preferable to avoid the need for imaging prior to injection. The following protocol will cover how to induce a photothrombotic stroke, how to inject a hydrogel in a controlled and precise manner, and how to extract and cryosection the brain while keeping the biomaterial intact. In addition, we will highlight how these same hydrogel materials can be used for the co-delivery of stem cells. This protocol can be generalized to the use of other injectable biomaterials into the stroke core.

摘要

中风是美国导致残疾的首要原因,也是第五大死因。在美国,约87%的中风为缺血性中风,其定义为供应大脑血液的血管突然堵塞。堵塞发生后的几分钟内,细胞开始死亡,导致无法修复的组织损伤。目前的治疗方法主要集中在清除血栓或溶栓,以实现再灌注并防止更严重的脑损伤。尽管随着时间的推移,短暂的脑可塑性可能会挽救一些受损组织,但仍有相当一部分患者会留下无法恢复的神经功能缺损。目前缺乏治疗中风所致神经功能缺损的有效方法,这凸显了开发新策略来治疗这一不断增长的患者群体的必要性。目前正在设计可注射生物材料,通过递送活性剂或干细胞来增强脑可塑性并促进内源性修复。测试这些方法的一种方式是利用啮齿动物中风模型,将生物材料注射到中风核心区域,并评估修复情况。了解中风核心的精确位置对于中风后的准确治疗至关重要,因此,一种能导致可预测中风位置的中风模型更可取,这样可以避免在注射前进行成像。以下方案将涵盖如何诱导光血栓性中风、如何以可控且精确的方式注射水凝胶,以及如何在保持生物材料完整的情况下提取大脑并进行冷冻切片。此外,我们将重点介绍这些相同的水凝胶材料如何用于干细胞的共递送。该方案可推广至将其他可注射生物材料用于中风核心区域的情况。

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