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P 物质可减少缺血性脑卒中后的梗死面积和死亡率,可能是通过缺血性大鼠大脑中小胶质细胞/巨噬细胞的 M2 极化和神经保护作用。

Substance P Reduces Infarct Size and Mortality After Ischemic Stroke, Possibly Through the M2 Polarization of Microglia/Macrophages and Neuroprotection in the Ischemic Rat Brain.

机构信息

Department of Genetics and Biotechnology, College of Life Science and Graduate School of Biotechnology, Kyung Hee University, Seocheon-dong, Kiheung-gu 446-701, Yongin-Si, Republic of Korea.

出版信息

Cell Mol Neurobiol. 2023 Jul;43(5):2035-2052. doi: 10.1007/s10571-022-01284-7. Epub 2022 Sep 16.

Abstract

Substance-P (SP) is an 11 amino acid neuropeptide that is known to stimulate the peripheral mobilization of bone marrow mesenchymal stem cells and M2 polarization in monocytes/macrophages in a variety of acute and chronic tissue injuries. To examine the role of SP in protection and recovery from acute ischemic brain injury, experimental ischemic stroke was induced by transient middle cerebral artery occlusion (tMCAo) in rats for 1 h with subsequent reperfusion. Two injections of SP, immediately and one day post-tMCAo, resulted in approximately threefold lower mortality and 40% less infarct volume than those of saline-treated rats at seven days post-tMCAo. At 4.5 h, SP markedly increased CD11b/cCD163/CD 206 cells in the blood, which were concomitantly decreased in the bone marrow, suggesting that SP preferentially mobilized M2-polarized monocytes. After two days, SP increased the expression of neuroprotective and anti-inflammatory genes in the ischemic brain and induced neuronal survival in the brain penumbra. Additionally, SP markedly increased CD68CD163 and CD68CD206 M2 microglia/macrophages in the ischemic brain during seven days post-tMCAo. Furthermore, SP preserved the blood‒brain barrier in the ischemic brain, which was confirmed by the abundant levels of SMI71 brain endothelial cells that colocalized with α-SMA pericytes. The beneficial effects of SP on functional recovery and tissue preservation were maintained for six weeks. Collectively, SP treatment in the early phase of ischemic stroke markedly suppressed the destructive inflammatory response and improved the microenvironment for tissue protection and repair.

摘要

P 物质(SP)是一种由 11 个氨基酸组成的神经肽,已知它能刺激骨髓间充质干细胞在多种急性和慢性组织损伤中的外周动员,并使单核细胞/巨噬细胞向 M2 极化。为了研究 P 物质在急性缺血性脑损伤中的保护和恢复作用,我们通过短暂性大脑中动脉闭塞(tMCAo)在大鼠中诱导 1 小时的实验性缺血性中风,随后再进行再灌注。SP 进行两次注射,即在 tMCAo 后立即和一天后进行注射,与生理盐水处理的大鼠相比,在 tMCAo 后 7 天,SP 组的死亡率降低了约三分之二,梗死体积减少了 40%。在 4.5 小时时,SP 明显增加了血液中的 CD11b/cCD163/CD206 细胞,同时骨髓中的这些细胞减少,表明 SP 优先动员 M2 极化的单核细胞。两天后,SP 增加了缺血性大脑中神经保护和抗炎基因的表达,并诱导了脑半影区的神经元存活。此外,SP 在 tMCAo 后 7 天内明显增加了缺血性大脑中 CD68CD163 和 CD68CD206 M2 小胶质细胞/巨噬细胞的表达。此外,SP 还保留了缺血性大脑中的血脑屏障,这通过与α-SMA 周细胞共定位的 SMI71 脑内皮细胞的丰富水平得到证实。SP 在功能恢复和组织保存方面的有益作用持续了 6 周。总的来说,在缺血性中风的早期阶段进行 SP 治疗,可显著抑制破坏性炎症反应,并改善组织保护和修复的微环境。

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