首页|期刊导航|中国中药杂志|无忧汤通过抑制神经炎症及保护血脑屏障改善慢性睡眠剥夺模型大鼠海马损伤的机制研究

无忧汤通过抑制神经炎症及保护血脑屏障改善慢性睡眠剥夺模型大鼠海马损伤的机制研究OA

Mechanism of Wuyou Decoction in improving hippocampal injury in chronic sleep deprivation model rats by inhibiting neuroinflammation and protecting blood-brain barrier

中文摘要英文摘要

探讨无忧汤通过抑制神经炎症及保护血脑屏障改善慢性睡眠剥夺模型大鼠海马损伤的机制.将 50 只 2 月龄SD雄性大鼠随机分为正常组、模型组、无忧汤低剂量组、无忧汤中剂量组、无忧汤高剂量组.除正常组外,其余各组大鼠首先接受7 d的水平台睡眠剥夺适应性造模,随后进行 21 d的正式睡眠剥夺造模;并于正式造模开始时,无忧汤高、中、低剂量组大鼠给予相应剂量药物灌胃,持续28 d.造模及灌胃结束后,利用Morris水迷宫检测大鼠的学习记忆水平;尼氏染色检测尼氏小体的数量;免疫组化检测海马神经元标志物特异性核蛋白(NeuN)的形态与数量;ELISA检测β-淀粉样蛋白(Aβ)1-40 和Aβ1-42 的水平;免疫荧光法检测离子钙结合衔接分子 1(IBA1)和胶质纤维酸性蛋白(GFAP)的荧光强度;Western blot法检测大鼠海马组织中与血脑屏障及炎症因子相关的蛋白:基质金属蛋白酶 2(MMP2)、基质金属蛋白酶 9(MMP9)、胞质紧密黏连蛋白 1(ZO-1)、claudin 5、occludin、白细胞介素(IL)-1β、IL-6、肿瘤坏死因子-α(TNF-α).结果显示,与正常组相比,模型组大鼠逃避潜伏期增加,穿越平台次数和目标象限停留时间降低;尼氏小体数量减少,神经元阳性细胞数减少,排列不齐;Aβ1-40 和Aβ1-42 的水平升高;IBA1 和GFAP荧光强度增强;炎症因子IL-1β、IL-6、TNF-α蛋白表达升高,MMP9、MMP2 蛋白表达上调,ZO-1、occludin、claudin 5 蛋白表达降低.与模型组相比,大鼠在中剂量无忧汤干预后,逃避潜伏期缩短,穿越平台次数和目标象限停留时间增加;尼氏小体及神经元排列整齐,数量增加;Aβ1-40 和Aβ1-42 的水平降低;IBA1 和GFAP 荧光强度减弱;炎症因子IL-1β、IL-6、TNF-α蛋白表达降低,MMP9、MMP2 蛋白表达下降,ZO-1、occludin、claudin 5 蛋白表达升高.以上结果表明无忧汤通过抑制促炎因子的释放,保护血脑屏障的完整性,进而提高了慢性睡眠剥夺大鼠的认知水平.

This study explored the mechanism by which Wuyou Decoction(WYD)ameliorated hippocampal injury in a chronic sleep deprivation model rat by suppressing neuroinflammation and protecting the blood-brain barrier(BBB).Fifty 2-month-old male SD rats were randomly divided into five groups:normal,model,low-dose WYD,medium-dose WYD,and high-dose WYD.Except for the normal group,all rats underwent a 7-day adaptation period for the water platform sleep deprivation model,which was followed by 21 days of formal sleep deprivation modeling.Concurrently with the start of formal modeling,rats in the low-,medium-,and high-dose WYD groups received corresponding doses of WYD via intragastric administration for 28 consecutive days.After modeling and drug administration,learning and memory were assessed using the Morris water maze.Nissl staining was used to quantify Nissl bodies.Immunohistochemistry evaluated the morphology and quantity of the neuronal marker neuron specific nuclear protein(NeuN)in the hippocampus.Enzyme-linked immunosorbent assay(ELISA)measured levels of amyloid β-protein(Aβ)1-40 and Aβ1-42.Immunofluorescence assessed the fluorescence intensity of ionized calcium-binding adapter molecule 1(IBA1)and glial fibrillary acidic protein(GFAP).Western blot analyzed the expression of matrix metalloproteinase 2(MMP2),matrix metalloproteinase 9(MMP9),zona occludens 1(ZO-1),claudin 5,occludin,interleukin(IL)-1β,IL-6,tumor necrosis factor(TNF)-α in hippocampal tissue,which were proteins related to BBB and inflammatory factors.Compared with the normal group,the model group exhibited significantly prolonged escape latency and decreased platform-crossing times and target quadrant residence time.Nissl body count and NeuN-positive neurons were reduced with disorganized neuronal arrangement.Aβ1-40 and Aβ1-42 levels were elevated.Fluorescence intensity of IBA1 and GFAP was increased.Expression of inflammatory factors IL-1β,IL-6,and TNF-α was enhanced,and expression of MMP9 and MMP2 was upregulated,while expression of ZO-1,occludin,and claudin 5 was downregulated.Compared to the model group,medium-dose WYD intervention shortened escape latency and increased platform-crossing times and target quadrant residence time.Nissl bodies and neurons were more numerous and were orderly arranged.Aβ1-40 and Aβ1-42 levels were reduced.Fluorescence intensity of IBA1 and GFAP was attenuated.Levels of IL-1β,IL-6,and TNF-α were decreased.Expression of MMP9 and MMP2 was downregulated,while expression of ZO-1,occludin,and claudin 5 was upregulated.The above results suggest that WYD improves cognitive function in the chronic sleep deprivation model rats by inhibiting the release of pro-inflammatory cytokines and protecting the integrity of BBB.

王政喻;高建红;吴丹;赖碧璇;蔡元钦;王曦;龙清华

湖北民族大学 医学部,湖北 恩施 445000||湖北民族大学 风湿病发生与干预湖北省重点实验室,湖北 恩施 445000湖北民族大学 医学部,湖北 恩施 445000||安徽中医药大学,安徽 合肥 230000湖北民族大学 医学部,湖北 恩施 445000||湖北民族大学 风湿病发生与干预湖北省重点实验室,湖北 恩施 445000湖北民族大学 医学部,湖北 恩施 445000||湖北民族大学 风湿病发生与干预湖北省重点实验室,湖北 恩施 445000湖北民族大学 医学部,湖北 恩施 445000||湖北民族大学 风湿病发生与干预湖北省重点实验室,湖北 恩施 445000||云南中医药大学,云南 昆明 650000湖北民族大学 医学部,湖北 恩施 445000||湖北民族大学 风湿病发生与干预湖北省重点实验室,湖北 恩施 445000湖北民族大学 医学部,湖北 恩施 445000||湖北民族大学 风湿病发生与干预湖北省重点实验室,湖北 恩施 445000

无忧汤慢性睡眠剥夺血脑屏障神经炎症机制研究

Wuyou Decoctionchronic sleep deprivationblood-brain barrierneuroinflammationmechanism study

《中国中药杂志》 2026 (4)

1064-1071,8

国家自然科学基金项目(82204964)中国博士后科学基金面上项目(2025M773957)湖北民族大学研究生创新项目(MYK2023060)

10.19540/j.cnki.cjcmm.20250723.401

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