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Novel TNF receptor-1 inhibitors identified as potential therapeutic candidates for traumatic brain injury

机译:新型TNF受体1抑制剂被确定为颅脑外伤的潜在治疗候选药物

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摘要

BackgroundTraumatic brain injury (TBI) begins with the application of mechanical force to the head or brain, which initiates systemic and cellular processes that are hallmarks of the disease. The pathological cascade of secondary injury processes, including inflammation, can exacerbate brain injury-induced morbidities and thus represents a plausible target for pharmaceutical therapies. We have pioneered research on post-traumatic sleep, identifying that injury-induced sleep lasting for 6 h in brain-injured mice coincides with increased cortical levels of inflammatory cytokines, including tumor necrosis factor (TNF). Here, we apply post-traumatic sleep as a physiological bio-indicator of inflammation. We hypothesized the efficacy of novel TNF receptor (TNF-R) inhibitors could be screened using post-traumatic sleep and that these novel compounds would improve functional recovery following diffuse TBI in the mouse.
机译:背景颅脑外伤(TBI)始于向头部或大脑施加机械力,这引发了疾病的标志性系统性和细胞性过程。继发性损伤过程(包括炎症)的病理级联可加剧脑损伤诱导的发病率,因此代表了药物治疗的合理目标。我们在创伤后睡眠方面进行了开创性的研究,确定在脑损伤的小鼠中持续6小时的损伤诱导的睡眠与包括肿瘤坏死因子(TNF)在内的炎症细胞因子的皮质水平升高相吻合。在这里,我们将创伤后睡眠作为炎症的生理生物指标。我们假设可以使用创伤后睡眠来筛选新型TNF受体(TNF-R)抑制剂的功效,并且这些新型化合物将改善小鼠弥漫性TBI后的功能恢复。

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