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Incensole acetate: a novel neuroprotective agent isolated from Boswellia carterii.

机译:醋酸茵那索:一种从乳香中分离出来的新型神经保护剂。

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摘要

Boswellia resin has been used as a major anti-inflammatory agent and for the healing of wounds for centuries. Incensole acetate (IA), isolated from this resin, was shown to inhibit the activation of nuclear factor-kappaB, a key transcription factor in the inflammatory response. We now show that IA inhibits the production of inflammatory mediators in an in vitro model system of C6 glioma and human peripheral monocytes. Given the involvement of postinjury inflammation in the pathophysiology and outcome of traumatic brain injury, we examined the effect of IA on the inflammatory process and on the recovery of neurobehavioral and cognitive functions in a mouse model of closed head injury (CHI). In the brains of post-CHI mice, IA reduced glial activation, inhibited the expression of interleukin-1beta, and tumor necrosis factor-alpha mRNAs, and induced cell death in macrophages at the area of trauma. A mild hypothermic effect was also noted. Subsequently, IA inhibited hippocampal neurodegeneration and exerteda beneficial effect on functional outcome after CHI, indicated by reduced neurological severity scores and improved cognitive ability in an object recognition test. This study attributes the anti-inflammatory activity of Boswellia resin to IA and related cembranoid diterpenes and suggests that they may serve as novel neuroprotective agents.
机译:乳香树脂已被用作主要的消炎药,并且已经治愈了多个世纪的伤口。从该树脂中分离出的乙酸烯那洛酯(IA)被证明可抑制核因子-κB的激活,核因子-κB是炎症反应中的关键转录因子。我们现在显示,IA在C6胶质瘤和人类外周血单核细胞的体外模型系统中抑制炎症介质的产生。考虑到损伤后炎症参与了创伤性脑损伤的病理生理和预后,我们在闭式颅脑损伤(CHI)小鼠模型中研究了IA对炎症过程以及神经行为和认知功能恢复的影响。在CHI后小鼠的大脑中,IA减少了神经胶质的激活,抑制了白介素1β和肿瘤坏死因子αmRNA的表达,并在创伤部位的巨噬细胞中诱导了细胞死亡。还注意到了轻微的低温作用。随后,IA抑制了CHI后海马神经退行性变,并对功能结局发挥了有益作用,这在对象识别测试中表现为神经系统严重程度评分降低和认知能力提高。这项研究将乳香树脂的抗炎活性归因于IA和相关的双萜类二萜,并建议它们可以作为新型神经保护剂。

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