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NogoA 中和促进皮质下卒中后白质损伤的轴突修复。

NogoA Neutralization Promotes Axonal Restoration After White Matter Injury In Subcortical Stroke.

机构信息

Neuroscience and Cerebrovascular Research Laboratory, Department of Neurology and Stroke Center, La Paz University Hospital, Neuroscience Area of IdiPAZ Health Research Institute, Autonomous University of Madrid, Madrid, Spain.

出版信息

Sci Rep. 2017 Aug 25;7(1):9431. doi: 10.1038/s41598-017-09705-0.

Abstract

Blocking axonal growth inhibitor NogoA has been of great interest for promoting axonal recovery from neurological diseases. The present study investigates the therapeutic effects of blocking NogoA, inducing functional recovery and promoting white matter repair in an experimental animal model of stroke. Adult male rats were subjected to white matter injury by subcortical ischemic stroke. Twenty-four hours after surgery, 250 ug of anti-NogoA or anti-IgG-1 were administered through the tail vein. The quantity of NogoA protein was determined by immunohistochemistry in the brain and peripheral organs. In addition, functional status, lesion size, fiber tract integrity, axonal sprouting and white matter repair markers were analyzed. Moreover, an in vitro study was performed in order to strengthen the results obtained in vivo. A lower quantity of NogoA protein was found in the brain and peripheral organs of the animals that received anti-NogoA treatment. The animals receiving anti-NogoA treatment showed significantly better results in terms of functional recovery, fiber tract integrity, axonal sprouting and white matter repair markers compared with the control group at 28 days. White matter integrity was in part restored by antibody-mediated inhibition of NogoA administration in those animals that were subjected to an axonal injury by subcortical stroke. This white matter restoration triggered functional recovery.

摘要

阻断轴突生长抑制剂 NogoA 一直是促进神经疾病轴突恢复的研究热点。本研究旨在探讨阻断 NogoA 对皮质下缺血性卒中动物模型的治疗作用,以诱导功能恢复和促进白质修复。成年雄性大鼠通过皮质下缺血性卒中造成白质损伤。术后 24 小时,通过尾静脉给予 250μg 的抗 NogoA 或抗 IgG-1。通过免疫组化测定脑组织和外周器官中 NogoA 蛋白的含量。此外,还分析了功能状态、病变大小、纤维束完整性、轴突发芽和白质修复标志物。此外,还进行了一项体外研究以加强体内获得的结果。接受抗 NogoA 治疗的动物的脑组织和外周器官中 NogoA 蛋白的含量较低。与对照组相比,在 28 天时,接受抗 NogoA 治疗的动物在功能恢复、纤维束完整性、轴突发芽和白质修复标志物方面的结果明显更好。在皮质下卒中导致轴突损伤的动物中,通过抗体介导的 NogoA 抑制给药,部分恢复了白质完整性,进而触发了功能恢复。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6137/5573364/3b710aa304bc/41598_2017_9705_Fig1_HTML.jpg

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