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Neural Cell Interactions with a Surgical Grade Biomaterial Using a Simulated Injury in Brain Organotypic Slices

机译:使用大脑器官型切片中的模拟损伤的神经细胞与手术级生物材料的相互作用

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Tissue engineering research for neurological applications has demonstrated that biomaterial-based structural bridges present a promising approach for promoting regeneration. This is particularly relevant for penetrating traumatic brain injuries, where the clinical prognosis is typically poor, with no available regeneration-enhancing therapies. Specifically, repurposing clinically approved biomaterials offers many advantages (reduced approval time and achieving commercial scaleup for clinical applications), highlighting the need for detailed screening of potential neuromaterials. A major challenge in experimental testing is the limited availability of neuromimetic, technically accessible, cost-effective, and humane models of neurological injury for efficient biomaterial testing in injury-simulated environments. Three dimensional (3D) organotypic brain slices bridge the gap between live animal models and simplified co-cultures and are a versatile tool for studies on neural development, neurodegenerative disease and in drug testing. Despite this, their utility for investigation of neural cell responses to biomaterial implantation is poorly investigated. We demonstrate that murine brain organotypic slices can be used to develop a model of penetrating traumatic brain injury, wherein a surgical-grade biomaterial scaffold can be implanted into the lesion cavity. Critically, the model allowed for examination of key cellular responses involved in CNS injury pathology/biomaterial handling: astrogliosis, microglial activation and axonal sprouting. The approach offers a technically simple and versatile methodology to study biomaterial interventions as a regenerative therapy for neurological injuries.
机译:用于神经学应用的组织工程研究表明,基于生物材料的结构桥为促进再生提供了一种很有前途的方法。这与穿透性创伤性脑损伤尤其相关,因为临床预后通常很差,没有可用的再生增强疗法。具体来说,重新利用临床批准的生物材料具有许多优势(减少审批时间并实现临床应用的商业放大),突出了对潜在神经材料进行详细筛选的必要性。实验测试的一个主要挑战是神经模拟、技术可及、经济高效和人道的神经损伤模型的可用性有限,无法在损伤模拟环境中进行有效的生物材料测试。三维 (3D) 器官型脑切片弥合了活体动物模型和简化的共培养之间的差距,是研究神经发育、神经退行性疾病和药物测试的通用工具。尽管如此,它们在研究神经细胞对生物材料植入反应方面的效用研究不足。我们证明小鼠脑器官型切片可用于开发穿透性创伤性脑损伤模型,其中手术级生物材料支架可以植入病变腔。至关重要的是,该模型允许检查涉及 CNS 损伤病理学/生物材料处理的关键细胞反应:星形胶质细胞增生、小胶质细胞活化和轴突发芽。该方法提供了一种技术简单且用途广泛的方法来研究生物材料干预作为神经损伤的再生疗法。

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