淫羊藿苷通过调控骨钙素改善AD模型小鼠认知损害及降低相关亢进内分泌激素水平OA
Icariin ameliorates cognitive impairment and decreases hyperactive endocrine hormone levels in Alzheimer's disease mice by regulating osteocalcin secretion
目的 探索淫羊藿苷(icariin,ICA)通过调节骨钙素(osteocalcin,OCN)分泌改善阿尔茨海默病(Alzheimer's disease,AD)模型小鼠认知损害及影响相关内分泌激素变化情况.方法 通过侧脑室注射冈田酸(okadaic acid,OA)制备AD小鼠模型.使用分层设计方法将4周龄,体质量18~22 g的雄性SPF级小鼠分为8组(n=6):野生对照(wild type,WT)组:小鼠60 mg/kg生理盐水灌胃;野生模型(WT-AD)组:WT小鼠+左侧脑室注射1 µL OA;野生加药(WT+ICA)组:每日60 mg/kg ICA;野生模型加药(WT-AD+ICA)组:WT-AD小鼠+每日60 mg/kg ICA.敲除对照(OCN-/-)组:OCN-/-小鼠60 mg/kg生理盐水灌胃;敲除模型(OCN-/--AD)组:OCN-/-小鼠+左侧脑室注射1 µL OA.敲除加药(OCN-/-+ICA)组:OCN-/-小鼠+每日60 mg/kg ICA;敲除模型加药(OCN-/--AD+ICA)组:OCN-/--AD小鼠+每日60 mg/kg ICA.Morris水迷宫实验检测小鼠学习记忆能力,旷场实验评估其焦虑水平;HE染色、镀银染色观察各组小鼠海马组织病理学变化,尼氏染色检测小鼠海马神经元尼氏小体表达情况;免疫组化检测β-淀粉样蛋白(amyloid β-protein,Aβ)、OCN阳性表达,Western blot检测Aβ、OCN的表达水平.ELISA检测促肾上腺皮质激素释放激素(corticotropin releasing hormone,CRH)、葡萄糖(glucose,GLU)、糖皮质激素(glucocorticoid,GC)、皮质醇(cortisol,COR)表达水平.结果 Morris水迷宫实验结果显示,WT-AD+ICA组与WT-AD组相比,OCN-/--AD+ICA组与OCN-/--AD组相比,小鼠潜伏期缩短和目标象限停留时间延长,穿越平台次数增加(均P<0.05);旷场实验结果显示,WT-AD+ICA与WT-AD组相比,OCN-/--AD+ICA组与OCN-/--AD组相比,小鼠的运动总距离、中央场运动距离及停留时间显著增加,活动意愿增强,周边区域停留时间和运动距离显著降低(均P<0.05);染色结果显示,经ICA干预后的海马病理减轻,海马形态结构趋于正常、神经纤维缠结(neurofibrillary tangles,NFTs)减少、尼氏小体呈逐渐恢复状态,但OCN-/-组小鼠仍未恢复到正常水平;免疫组化结果显示,WT-AD+ICA组与WT-AD组相比,OCN-/--AD+ICA组与OCN-/--AD组相比,Aβ水平下降,OCN水平上升(均P<0.05).Western blot结果显示,WT-AD+ICA组与WT-AD组相比,OCN-/--AD+ICA组与OCN-/--AD组相比,Aβ水平下降,OCN水平上升(均P<0.05).ELISA结果显示,WT-AD+ICA组与WT-AD组相比,OCN-/--AD+ICA组与OCN-/--AD相比,CRH、GLU、GC、COR水平明显降低(均P<0.05).结论 ICA可通过调节OCN分泌改善AD模型小鼠认知损害并降低相关亢进内分泌激素水平.
Objective To investigate whether icariin(ICA)ameliorates cognitive impairment and modulates relevant endocrine hormone alterations in Alzheimer's disease(AD)model mice by regulating osteocalcin(OCN)secretion.Methods An AD mouse model was established by intraventricular injection of okadaic acid(OA).Using a stratified design,4-week-old male SPF mice(weighing 18 to 22 g)were randomly divided into 8 groups(n=6):wild-type(WT)control group(intragastric administration of 60 mg/kg normal saline);WT-AD group(WT mice with left intracerebroventricular injection of 1 µL OA);WT+ICA group(60 mg/kg ICA daily);WT-AD+ICA group(WT-AD mice with daily 60 mg/kg ICA);OCN-/-control group(OCN-/-mice with 60 mg/kg normal saline);OCN-/--AD group(OCN-/-mice with left intracerebroventricular injection of 1 µL OA);OCN-/-+ICA group(OCN-/-mice with 60 mg/kg ICA daily);and OCN-/--AD+ICA group(OCN-/--AD mice with 60 mg/kg ICA daily).The Morris water maze test was conducted to assess learning and memory abilities,while open field test was performed to evaluate anxiety levels.Hippocampal histopathological changes were observed with HE staining and silver impregnation staining;Nissl bodies in hippocampal neurons were detected with Nissl staining.Immunohistochemistry assay was employed to determine the expression of amyloid β-protein(Aβ)and OCN,and Western blotting was used to measure the protein levels of Aβ and OCN.ELISA was applied to detect the expression levels of corticotropin-releasing hormone(CRH),glucose(GLU),glucocorticoid(GC),and cortisol(COR).Results Morris water maze test demonstrated that compared with the WT-AD group,the WT-AD+ICA group exhibited significantly shortened escape latency,prolonged time spent in the target quadrant,and increased platform crossing frequency(all P<0.05);similarly,the OCN-/--AD+ICA group showed improvements than the OCN-/--AD group(all P<0.05).Open field test results indicated that compared with the WT-AD group,the WT-AD+ICA group displayed significantly increased total exploration distance,distance in the center,and time in the center,enhanced activity willingness,and reduced time in peripheral zone and distance in peripheral zone(all P<0.05);similar improvements were observed in the OCN-/--AD+ICA group compared with the OCN-/--AD group(all P<0.05).Staining results revealed that ICA intervention attenuated hippocampal pathology,restored hippocampal morphological architecture,reduced neurofibrillary tangles(NFTs),and promoted gradual recovery of Nissl bodies;however,the OCN-/-mice failed to achieve complete normalization.Immunohistochemistry assay showed that compared with the WT-AD group,the WT-AD+ICA group exhibited decreased Aβ levels and increased OCN levels(all P<0.05);similar trends were observed in the OCN-/--AD+ICA group relative to the OCN-/--AD group(all P<0.05).Western blotting demonstrated that compared with the WT-AD group,the WT-AD+ICA group showed reduced Aβ expression and elevated OCN expression(both P<0.05);comparable changes were found in the OCN-/--AD+ICA group compared with the OCN-/--AD group(both P<0.05).ELISA indicated that compared with the WT-AD group,the WT-AD+ICA group exhibited significantly decreased levels of CRH,GLU,GC,and COR(all P<0.05);similar reductions were observed in the OCN-/--AD+ICA group compared with the OCN-/--AD group(all P<0.05).Conclusion ICA ameliorates cognitive impairment and reduces levels of related hyperactive endocrine hormones in AD model mice through regulating OCN secretion.
崔曼;朱其凤;方兴;古联;闫雨;方俪霖;张明达;陈星宇
广西中医药大学研究生院,广西南宁广西中医药大学附属瑞康医院神经内科,广西南宁广西中医药大学附属瑞康医院神经内科,广西南宁广西中医药大学附属瑞康医院神经内科,广西南宁合江县中医医院心脑病科,四川泸州平南县中医院脑病科,广西贵港广西中医药大学附属瑞康医院空港院区神经内科,广西崇左广西中医药大学研究生院,广西南宁
医药卫生
阿尔茨海默病淫羊藿苷骨钙素神经内分泌
Alzheimer's diseaseicariinosteocalcinneuroendocrine
《陆军军医大学学报》 2026 (5)
551-562,12
广西自然科学基金一般项目(2023GXNSFAA026458)国家自然科学基金地区科学基金项目(82260944) Supported by the General Project of Natural Science Foundation of Guangxi Zhuang Autonomous Region(2023GXNSFAA026458)and the Regional Science Fund Program of National Natural Science Foundation of China(82260944).
评论