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The role of protein phosphatase 2A tau axis in traumatic brain injury therapy

机译:蛋白磷酸酶2A tau轴在创伤性脑损伤治疗中的作用

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Background Traumatic brain injury (TBI) is a debilitating disorder due to trauma caused by an external mechanical force eventually leading to disruption in the normal function of the brain, with possible outcomes including permanent or temporary dysfunction of cognitive, physical, and psychosocial abilities. There have been several studies focusing on the search and innovation of neuroprotective agents that could have therapeutic relevance in TBI management. Due to its complexity, TBI is divided into two major components. The first initial event is known as the primary injury; it is a result of the mechanical insult itself and is known to be irreversible and resistant to a vast variety of therapeutics. The secondary event or secondary brain injury is viewed as a cellular injury that does not manifest immediately after the trauma but evolved after a delay period of hours or several days. This category of injury is known to respond favorably to different pharmacological treatment approaches. Main body Due to the complexity in the pathophysiology of the secondary injury, the therapeutic strategy needs to be in a multi-facets model and to have the ability to simultaneously regulate different cellular changes. Several studies have investigated in deep the possible approaches relying on natural compounds as an alternative therapeutic strategy for the management of TBI. In addition, many natural compounds have the potential to target numerous different components of the secondary injury including neuroinflammation, apoptosis, PP2A, tau, and A beta among others. Here, we review past and current strategies in the therapeutic management of TBI, focusing on the PP2A-tau axis both in animal and human subjects. This review uncovers, in addition, a variety of compounds used in TBI therapy. Conclusion Despite beneficial therapeutic effects observed in animals for many compounds, studies are still needed to be conducted on human subjects to validate their therapeutic virtues. Furthermore, potential therapeutic virtues observed among studies might likely be dependent on the TBI animal model used and the type of induced injury. In addition, specificity and side effects are challenges in TBI therapy specifically which site of PP2A dysfunction to be targeted.
机译:背景 创伤性脑损伤 (TBI) 是一种使人衰弱的疾病,由外部机械力引起的创伤,最终导致大脑正常功能的破坏,可能的结果包括认知、身体和社会心理能力的永久性或暂时性功能障碍。已经有几项研究专注于寻找和创新可能在 TBI 管理中具有治疗相关性的神经保护剂。由于其复杂性,TBI 分为两个主要部分。第一个初始事件称为原发性损伤;它是机械损伤本身的结果,已知是不可逆的,并且对多种治疗方法具有抗药性。继发性事件或继发性脑损伤被视为一种细胞损伤,不会在创伤后立即表现出来,而是在数小时或数天的延迟期后演变。已知此类损伤对不同的药物治疗方法反应良好。主体 由于继发性损伤病理生理学的复杂性,治疗策略需要处于多方面模型中,并具有同时调节不同细胞变化的能力。几项研究深入研究了依靠天然化合物作为治疗 TBI 的替代治疗策略的可能方法。此外,许多天然化合物有可能靶向继发性损伤的许多不同成分,包括神经炎症、细胞凋亡、PP2A、tau 和 A β 等。在这里,我们回顾了过去和现在 TBI 治疗管理的策略,重点关注动物和人类受试者的 PP2A-tau 轴。此外,本综述还揭示了TBI治疗中使用的各种化合物。结论 尽管在动物身上观察到许多化合物的有益治疗效果,但仍需要对人类受试者进行研究以验证其治疗效果。此外,在研究中观察到的潜在治疗价值可能取决于所使用的 TBI 动物模型和诱导损伤的类型。此外,特异性和副作用是 TBI 治疗的挑战,特别是针对 PP2A 功能障碍的哪个部位。

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