创伤性脑损伤小鼠模型中,伤后给予一种新型小分子可抑制急性促炎细胞因子和趋化因子上调,改善长期神经功能结局。
Suppression of acute proinflammatory cytokine and chemokine upregulation by post-injury administration of a novel small molecule improves long-term neurologic outcome in a mouse model of traumatic brain injury.
作者信息
Lloyd Eric, Somera-Molina Kathleen, Van Eldik Linda J, Watterson D Martin, Wainwright Mark S
机构信息
Division of Critical Care, Department of Pediatrics, Children's Memorial Hospital, 2300 Children's Plaza, Chicago, IL 60614, USA.
出版信息
J Neuroinflammation. 2008 Jun 30;5:28. doi: 10.1186/1742-2094-5-28.
BACKGROUND
Traumatic brain injury (TBI) with its associated morbidity is a major area of unmet medical need that lacks effective therapies. TBI initiates a neuroinflammatory cascade characterized by activation of astrocytes and microglia, and increased production of immune mediators including proinflammatory cytokines and chemokines. This inflammatory response contributes both to the acute pathologic processes following TBI including cerebral edema, in addition to longer-term neuronal damage and cognitive impairment. However, activated glia also play a neuroprotective and reparative role in recovery from injury. Thus, potential therapeutic strategies targeting the neuroinflammatory cascade must use careful dosing considerations, such as amount of drug and timing of administration post injury, in order not to interfere with the reparative contribution of activated glia.
METHODS
We tested the hypothesis that attenuation of the acute increase in proinflammatory cytokines and chemokines following TBI would decrease neurologic injury and improve functional neurologic outcome. We used the small molecule experimental therapeutic, Minozac (Mzc), to suppress TBI-induced up-regulation of glial activation and proinflammatory cytokines back towards basal levels. Mzc was administered in a clinically relevant time window post-injury in a murine closed-skull, cortical impact model of TBI. Mzc effects on the acute increase in brain cytokine and chemokine levels were measured as well as the effect on neuronal injury and neurobehavioral function.
RESULTS
Administration of Mzc (5 mg/kg) at 3 h and 9 h post-TBI attenuates the acute increase in proinflammatory cytokine and chemokine levels, reduces astrocyte activation, and the longer term neurologic injury, and neurobehavioral deficits measured by Y maze performance over a 28-day recovery period. Mzc-treated animals also have no significant increase in brain water content (edema), a major cause of the neurologic morbidity associated with TBI.
CONCLUSION
These results support the hypothesis that proinflammatory cytokines contribute to a glial activation cycle that produces neuronal dysfunction or injury following TBI. The improvement in long-term functional neurologic outcome following suppression of cytokine upregulation in a clinically relevant therapeutic window indicates that selective targeting of neuroinflammation may lead to novel therapies for the major neurologic morbidities resulting from head injury, and indicates the potential of Mzc as a future therapeutic for TBI.
背景
创伤性脑损伤(TBI)及其相关的发病率是医学需求未得到满足的一个主要领域,目前缺乏有效的治疗方法。TBI引发了一种神经炎症级联反应,其特征是星形胶质细胞和小胶质细胞的激活,以及包括促炎细胞因子和趋化因子在内的免疫介质产生增加。这种炎症反应不仅导致TBI后的急性病理过程,如脑水肿,还会导致长期的神经元损伤和认知障碍。然而,活化的胶质细胞在损伤恢复过程中也发挥着神经保护和修复作用。因此,针对神经炎症级联反应的潜在治疗策略必须谨慎考虑给药剂量,如药物用量和伤后给药时间,以免干扰活化胶质细胞的修复作用。
方法
我们检验了这样一个假设,即减轻TBI后促炎细胞因子和趋化因子的急性增加会减少神经损伤并改善神经功能结局。我们使用小分子实验性治疗药物米诺扎克(Mzc),将TBI诱导的胶质细胞活化和促炎细胞因子的上调抑制至基础水平。在小鼠闭合性颅骨皮质撞击TBI模型中,在伤后的临床相关时间窗内给予Mzc。检测Mzc对脑内细胞因子和趋化因子水平急性增加的影响,以及对神经元损伤和神经行为功能的影响。
结果
在TBI后3小时和9小时给予Mzc(5毫克/千克)可减轻促炎细胞因子和趋化因子水平的急性增加,减少星形胶质细胞活化,以及在28天恢复期内通过Y迷宫测试所测量的长期神经损伤和神经行为缺陷。接受Mzc治疗的动物脑含水量(水肿)也没有显著增加,而水肿是与TBI相关的神经发病率的一个主要原因。
结论
这些结果支持了这样一个假设,即促炎细胞因子促成了一个胶质细胞活化循环,该循环在TBI后导致神经元功能障碍或损伤。在临床相关治疗窗内抑制细胞因子上调后长期神经功能结局得到改善,这表明选择性靶向神经炎症可能会带来针对头部损伤所致主要神经疾病的新疗法,并表明Mzc作为TBI未来治疗药物的潜力。
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