The Effects of Standardized Ginkgo Biloba Extracts (GBE) on Subjective Cognitive Decline (SCD) in Middle-Aged Adults: A Review

Subjective cognitive decline (SCD) is defined as the presence of self-reported cognitive complaints with unimpaired performance in neuropsychological cognitive tests. SCD has been identified as a precursor of mild cognitive impairment (MCI) and potentially represents the earliest clinical sign of Alzheimer’s disease (AD). Standardized extracts of Ginkgo biloba (GBE) are widely used as a treatment for cognitive impairment. Nonetheless, most of the available review articles focus on the effects of GBE in MCI and dementia but not in SCD and its specific cognitive effects. Thus, this review collects and discusses the available published clinical data for the effects of standardized GBE on the early stages of cognitive decline among an age group where SCD becomes a topic—the middle-aged adults. Randomized clinical trials (RCTs), systematic reviews and meta-analyses of standardized GBEs in cognitive decline subjects were searched using PubMed/MEDLINE, Science direct, Cochrane, and Google Scholar until January 2019. Data from relevant RCT were critically evaluated to determine the potential effects of GBE on SCD. The results showed that the number of available GBE studies on SCD is small. Eight studies were selected in which subjects reported memory impairment, in some cases with concerns (worries), and with an average age at onset SCD of 60 years. Six studies gave a proof of efficacy for GBE for the treatment of SCD in at least one cognitive parameter. One study is inconclusive, however, a post-hoc analysis demonstrates efficacy in preventing AD with intake >4 years. The most common GBE dosage used was 240 mg GBE/day over a minimum period of 8 weeks. Hence, there might be beneficial effects of GBE to prevent, improve or delay SCD in the generation of 50 years or older. However, larger, well-defined RCTs using SCD criteria are necessary to further substantiate this effect in SCD subjects.

Experimental Study on Inhibition of Neuronal Toxical Effect of Levodopa by Ginkgo Biloba Extract on Parkinson Disease in Rats

In order to observe neuronal toxical effect of Levodopa and investigate if using Levodopa together with Ginkgo Bilobar Extract (EGb) would be an workable method to treat Parkinson disease, rat models of Parkinson disease (PD) were made by injecting 6-OHDA stereotaxically to right side of the mesencephic ventral tegmental area (VTA) and substantia nigra pars compacta (SNc). Rotational behavioral observation, TUNEL, immunocytochemistry, Nissl's body staining were performed to measure the difference between group treated by Levodopa (50 mg/kg every day for 3 days, 5 days, 7 days, L-dopa group) and group treated by Levodopa combined with EGb (100 mg/ kg every day, E-D group). The results showed that in the L-dopa group, the numbers of apoptosis of substantial nigra, rings of rotational behavior were more than those in the E-D group (P<0. 05). The numbers of Nissl's cells in L-dopa group were fewer than in E-D group (P<0. 05). The results suggested that Levodopa had neur toxic effect and EGb may decrease the toxicity of levodopa. The combined use of EGb with Levodopa may be a workable method to treat PD and may be better than using Levodopa alone.

Extraction Process and Content Determination of Total Flavonoids in Ginkgo( Ginkgo biloba L. ) Leaves

[Objectives]This study was conducted to study the extraction process and the content determination of flavonoids in ginkgo( Ginkgo biloba L.) leaves.[Methods]Ethanol extraction and methanol extraction of total flavonoids in ginkgo leaves were studied,and the optimal extraction conditions for flavonoids were determined by orthogonal test; and with quercetin as reference substance,total flavonoid content in ginkgo leaves was determined by UV spectrophotometry.[Results]The optimal extraction process was 4 h of Soxhlet extraction with methanol; and the total flavonoid contents had a good linear relation in the range of 0. 006 5-0. 039 mg/ml( R^2= 0. 999 9),the average content was stabilized at 1. 135%,and the average recovery of the method was 102. 0%. [Conclusions]This study selected the optimal extraction process for total flavonoids in ginkgo leaves. The test method is simple with high accuracy and precision,and is suitable for the extraction and determination of total flavonoids in ginkgo leaves.

银杏提取物GBE50对紫外线C辐射诱导大鼠氧化应激的保护作用

目的:建立紫外线C辐射(UV-C)在SD大鼠体内诱导产生氧化应激的模型,并观察银杏提取物GBE50(Ginkgo biloba extract 50)对其保护及治疗作用。方法:采用253.7nm紫外灯进行辐照,连续7d,每天2h,辐照密度2.381mW/(cm2·h),每日辐射量为18W/cm2,建立UV-C在SD大鼠体内诱导产生氧化应激的模型,通过对各脏器组织还原型谷胱甘肽水平、超氧化物歧化酶(SOD)活性以及丙二醛水平进行检测,评价标准治疗量[100mg/(kg·d)]的GBE50的保护及治疗作用。结果:GBE50对UV-C辐射诱导的氧化应激模型有一定的保护治疗作用,可以提高肝脏、心脏和脑组织中SOD活性和肝脏及脑组织中谷胱甘肽还原酶活性,并降低心脏和脑组织中丙二醛水平。结论:GBE50应用于氧化应激的保护具有良好前景。

GBE50对高脂大鼠脑缺血再灌注损伤的保护作用

目的 研究新型银杏叶提取物制剂GBE5 0对高脂血症大鼠脑缺血再灌注损伤的保护作用。方法 在高脂血症大鼠上 ,建立大脑中动脉栓塞 (MCAO)再灌注损伤模型 ,观察灌胃给予GBE5 0 (5 0、10 0、2 0 0mg/kg) 2周 ,对大鼠脑梗死体积、神经行为学、血液流变学等指标的影响。结果 高脂MCAO模型组大鼠脑梗死体积为(31± 5 ) % ,神经行为评分为 2 .7± 0 .8;给予GBE5 0小、中、大剂量三组的高脂MCAO大鼠的脑梗死体积分别为(13± 4 ) %、(14± 4 ) %和 (13.0± 2 .6 ) % ,与模型组比较差异有显著意义 (P <0 .0 1) ;神经行为学评分分别为 1.7± 0 .5、1.5± 0 .6和 1.3± 0 .5 ,大剂量组与模型组比较差别有显著意义 (P <0 .0 5 ) ,并使全血黏度和还原黏度有不同程度的改善。结论 GBE5 0可降低高脂MCAO大鼠的脑梗死体积 ,改善神经行为障碍和血液流变学 。

Simultaneous quantification of flavonol glycosides, terpene lactones, polyphenols and carboxylic acids in Ginkgo biloba leaf extract by UPLC-QTOF-MS^E based metabolomic approach

Abstract： In the present study, we established an ultra performance liquid chromatography coupled with time-of-flight mass spectrometry （UPLC-QTOF-MSE） method to simultaneously quantify 33 components in Ginkgo biloba leaf extracts （GBEs）, including 17 flavonol glycosides, five terpene trilactones （TTLs）, four polyphenols and seven carboxylic acids. This optimized method was successfully applied to analyze the explicit compositions of GBE samples collected from different places. Furthermore, the data were processed through unsupervised principal component analysis （PCA） and supervised orthogonal partial least squared discrimination analysis （OPLS-DA） to evaluate the quality and compare the differences between the samples according to the contents of the 33 chemical constituents. Bilobalide, protocatechuic acid, shikimic acid, quinic acid, ginkgolide B, ginkgolide J, kaempferol-3-O-rutinoside, isorhamnetin-3-O-rutinoside, quercetin-3-O-ct-L-rhamnopyranocyl-2＂-（6＇＂-p-coumaroyl）-β-D-glucoside and rutin were recognized as characteristic chemical markers that contributed most to control the quality of GBEs. Based on the fact that GBEs should be standardized with the characteristic components as quality control chemical markers, it is most important to maintain the quality of GBEs stable and reliable, and this method also provided a good strategy to further rectify and standardize the GBEs market.

银杏叶提取物对豚鼠心室肌细胞动作电位及L型钙离子通道的影响

目的 :观察银杏叶提取物 (EGB)对豚鼠心室肌细胞动作电位和L 型钙通道的影响。方法 :采用全细胞膜片钳技术的电流钳记录动作电位和电压钳记录L 型钙离子通道电流 (ICa L)。结果 :银杏叶提取物 (原液含银杏黄酮甙 0 .80 4g·L-1,银杏内酯0 .0 6g·L-1)明显缩短心室肌细胞动作电位时程(APD) ,1 80 0稀释液致APD90 缩短 13% (P <0 .0 5 ) ,1 2 0 0稀释液致APD90 缩短 2 3% (P <0 .0 5 ) ;银杏叶提取物对心肌细胞L 型钙离子通道的开放有抑制作用 ,在 1 80 0时ICa L 峰值降低 15 % (P <0 .0 5 ) ,1 2 0 0时ICa L峰值降低 4 2 % (P <0 .0 5 ) ,均呈浓度依赖性 ,随着药物浓度的增加 ,I V关系曲线逐渐上移 ,但出现电流峰值的电压不变。结论 :银杏叶提取物能明显缩短APD ,抑制心肌细胞钙离子通道的开放 ,具有明显的浓度依赖关系 ,可能是其抗心律失常的分子基础。

银杏叶提取物对慢性阻塞性肺疾病患者诱导痰炎症细胞计数及IL-8水平的影响

目的:观察银杏叶提取物(GBE)对慢性阻塞性肺疾病(COPD)患者诱导痰IL-8的影响,研究GBE治疗COPD的疗效,并初步探讨其作用机制。方法:36例COPD缓解期患者随机分为GBE治疗组和安慰剂治疗组,分别于治疗前后行诱导痰炎性细胞计数、ELISA法测诱导痰上清中IL-8含量以及肺功能检查。并与18例健康人比较。结果:COPD患者治疗前后各指标与健康人比较差异均有显著性(P<0.01);GBE治疗组治疗后诱导痰中性粒细胞百分比(PMN%)、IL-8水平均显著性下降(P<0.05),FEV1占预计值百分比显著性升高(P<0.05)。而安慰剂组治疗前后各指标差异无显著性(P>0.05)。结论:GBE可减轻COPD患者气道炎症反应,改善肺功能而发挥治疗作用。

银杏外种皮提取物有效部位GBEE-2对胃癌SGC-7901细胞凋亡及其通路的影响

目的研究银杏外种皮提取物有效部位GBEE-2体外对人胃癌细胞凋亡及其凋亡通路的影响。方法体外培养人胃癌SGC-7901细胞,应用MTT法检测细胞增殖;应用流式细胞术检测凋亡率和细胞周期;应用ELISA法检测培养上清中基因蛋白Caspase-9、Fas及Survivin的含量。结果 GBEE-2(5～160μg.mL-1)对SGC-7901细胞的体外增殖具有抑制作用,并具有浓度依耐性,IC50为83μg.mL-1;在10～160μg.mL-1浓度下体外培养,GBEE-2可提高SGC-7901细胞的凋亡率,可使Caspase-9、Fas蛋白表达量增加(P<0.05或0.01),而Survivin蛋白的表达则减少(P<0.05或0.01)。结论 GBEE-2抑制人胃癌SGC-7901细胞的作用机制与诱导细胞凋亡有关,其凋亡通路涉及Caspase途径。

银杏酮酯对缺血豚鼠心室肌细胞Ⅰ_(Ca-L)和游离钙的影响

目的观察银杏酮酯GBE50对模拟缺血游离豚鼠心室肌细胞L型钙电流和游离钙浓度的影响,探讨GBE50抗心肌缺血的作用机制。方法应用单酶酶解法分离游离单个豚鼠心室肌细胞,采用膜片钳全细胞记录心室肌细胞L型钙电流,通过激光共聚焦显微镜扫描测定细胞内游离钙浓度的动态变化。结果缺血抑制豚鼠心室肌细胞的ICa-L(n=9,P<0.01),使豚鼠心室肌细胞内游离钙增加(n=10,P<0.01),而50mg·mL-1GBE50减轻缺血对ICa-L的抑制效应(n=6,P>0.05),减少缺血后心室肌细胞内游离钙浓度的增加(n=10,P>0.05)。结论GBE50可减轻心肌缺血区域与非缺血区域电生理的异质性,维持缺血后豚鼠心肌细胞电生理的稳定性,并减轻缺血后心肌细胞内钙超载介导的心肌损伤。

乘方相似度法定性定量评价银杏叶提取物HPLC指纹图谱

目的:建立中药色谱指纹图谱乘方相似度和定量乘方相似度评价方法及其应用。方法:用乘方相似度和定量乘方相似度评价银杏叶提取物HPLC指纹图谱,并以夹角余弦SF、相关系数r和描述定量特征的指标即宏观含量相似度R%、平均质量百分数M%进行对比研究。结果:乘方相似度能够反映不同批次提取物的相似性变化,并具有定量描述功能:定量乘方相似度和加权定量乘方相似度能够较好地反映提取物不同成分含量的宏观变化。结论:乘方相似度和定量乘方相似度能够定性定量评价样品与对照指纹图谱间的相似程度,是一种新的相似度评价方法。

不同银杏叶提取物浓度对痴呆大鼠海马神经元L-型钙离子通道的影响

目的:探讨银杏叶提取物(Ginkgo biloba extract.EGB761)对痴呆大鼠海马神经元L-型钙离子通道的作用。方法:酶加机械分离方法获得痴呆大鼠海马神经元,用标准的全细胞膜片钳技术记录钙通道电流。结果:①细胞外给予EGB对正常的高电压激活钙通道电流(IHvA)没有影响。②使用β-淀粉肽(1-40)(β-amyloid peptideI-40,AβI-40)后分别使用1μmol/L,10μol/L,20μmol/L EGB,显示L型钙电流(ICa-L)/电压(I-V)曲线逐渐上移,但出现电流峰值的电压不变,这表明EGB可抵消Aβ对IHvA的增强作用。结论:银杏叶提取物可通过抑制钙离子内流对神经元起一定保护作用。

N-乙酰-L-半胱氨酸对失血性休克大鼠再灌注损伤的保护作用

目的 为临床应用抗氧化剂N 乙酰 L 半胱氨酸 (NAC)防治失血性休克提供实验基础。方法大鼠放血致休克 (失血量 4 9% ,血压 4～ 5 .3kPa) ,30min后 ,回输全血并再灌注 3h。回输全血的同时 ,分别给予NAC (15 0mg·kg- 1)和银杏叶提取物(Egb ,5 0mg·kg- 1) ,3h后检测血浆乳酸脱氢酶(LDH)、谷 草转氨酶 (GOT)活性和组织匀浆丙二醛(MDA)含量、髓过氧化物酶 (MPO)活性 ,并观察肾和肝组织病理变化。结果 给予NAC可明显降低缺血再灌注所致的血浆LDH、GOT活性及心、肝、肺和肾组织MPO活性和MDA含量增高 ,病理观察也显示组织损伤改善。Egb也有一定的改善作用 ,但不如NAC作用显著。结论 再灌早期给予NAC可抑制自由基的产生和脂质过氧化反应 。

银杏叶中黄酮的水提取及HPLC测定

本文运用水提法提取了银杏叶中的黄酮,提取物经酸水解后,用HPLC—UV法进行定量分析,测得黄酮用本法提取的产量为1.78%(W/W)。

银杏叶提取物对大鼠脑缺血再灌注后Bcl-2、Bax蛋白和Caspase-3表达的影响

目的探讨银杏叶提取物(ginkgo biloba extract,GBE)对脑缺血再灌注后Bcl-2、Bax蛋白和半胱氨酸蛋白酶-3(Caspase-3)表达的影响。方法将SD大鼠随机分为假手术组(A组)、缺血再灌注组(B组)和GBE治疗组(C组),建立大鼠大脑中动脉缺血1.5 h再灌注24 h的模型;C组于缺血前30 min及缺血再灌注后1 h腹腔内注射银杏叶提取物;采用免疫组化SP法检测脑缺血再灌注后Bcl-2、Bax蛋白的表达,采用四肽酶底物法检测Caspase-3活性水平。结果 GBE治疗组大鼠Bcl-2阳性细胞表达数目均高于缺血再灌注组,Bax少于缺血再灌注组(P<0.05);假手术组未检测到Caspase-3活性升高,缺血再灌注组Caspase-3活性明显高于GBE组,有统计学意义(P<0.05)。结论 GBE可通过上调Bcl-2蛋白表达而减少Caspase-3活性水平,下调Bax蛋白表达,来降低脑缺血再灌注后大鼠神经细胞凋亡。

银杏叶提取物对急性肝衰竭大鼠肝脏Bcl-2及Bax表达的影响

为了观察银杏叶提取物(ginkgo biloba extract,GBE)对由硫代乙酰胺(TAA)所致肝损伤大鼠肝脏的作用及其对Bcl-2、Bax的影响,并探讨其作用机制,试验将大鼠分5组,其中GBE低、中、高剂量组(50,100,200 mg/kg)连续灌服GBE 30 d,1次/d,正常对照组和模型组分别给予等体积的生理盐水;模型组和GBE低、中、高剂量组在第28天用300 mg/kg的TAA腹腔注射,正常对照组腹腔注射等体积的生理盐水,连续3 d,于末次注射后24,48,72小时采血,用试剂盒检测血清中谷草转氨酶(AST)、谷丙转氨酶(ALT)的水平,并用RT-PCR和Western-blot方法检测各组肝脏Bcl-2、BaxmRNA和蛋白水平的表达情况。结果表明:与正常对照组相比,模型组血清中ALT、AST水平明显升高,在肝脏中Bcl-2 mRNA表达水平下调,Bcl-2蛋白水平在48小时时达到最低点,而Bax mRNA和蛋白水平均上调;与模型组相比,GBE组血清中ALT、AST水平明显降低,肝脏中Bcl-2 mRNA和蛋白水平均上调,Bax mRNA和蛋白水平均下调。

银杏叶提取物对三氯乙烯所致BALB/c裸鼠皮肤氧化损伤的保护作用

目的研究银杏叶提取物(ginkgo bilobaextract,GBE)对有机溶剂三氯乙烯(TCE)所致BALB/c裸鼠皮肤组织氧化损伤的保护作用。方法将BALB/c裸鼠随机分成空白对照组、橄榄油溶剂对照组、100%TCE处理组和0.1%、1%、10%GBE保护组,分别染毒1 d和14 d,取染毒背部皮肤进行MDA含量、SOD活性测定。结果用GBE保护后,皮肤组织中的MDA含量随GBE水平的增加呈明显下降趋势,皮肤组织匀浆中的SOD活性随GBE剂量的增加呈上升趋势。结论银杏叶提取物可能通过降低皮肤的氧化应激水平,对TCE所致的皮肤损伤发挥保护作用,从而有效保护三氯乙烯所致BALB/c裸鼠皮肤氧化损伤。

银杏叶提取物抑制人冠状动脉内皮细胞中NF-κB表达及VAP-1、IL-6生成的研究

目的检测银杏叶提取物(Ginkgo biloba extract,EGb)能否抑制由活化血小板刺激引起的人冠状动脉内皮细胞(human coronary artery ebditgekuak cells,HCAECs)中NF-κB的表达,并降低炎症因子血管黏附蛋白-1(vascalur adhesion protein l,VAP-1),白细胞介素6(interlenkin-6,IL-6)的生成。方法活化血小板刺激HCAECs建立氧化应激模型,使用银杏叶提取物(4、40、400μg/ml)进行干预后,通过Western Blot检测NF-κB(p65、PP65)的表达量,酶联免疫吸附试验检测VAP-1,IL-6的生成量。结果活化血小板刺激HCAECs可引起目的分子表达量的增加,检测结果显示治疗量的EGb能显著抑制p65,PP65的表达及VAP-1、IL-6的生成,并成剂量依赖性。结论银杏叶提取物能显著抑制活化血小板刺激的人冠状动脉内皮细胞中p65,PP65的表达,并降低VAP-1及IL-6的生成。

银杏酮酯(GBE50)抑制NLRP3炎症小体活性改善大鼠抑郁样行为

目的:本实验通过观察银杏酮酯(GBE50)对抑郁模型大鼠行为学及NLRP3炎症小体作用,探索GBE50抗抑郁的机制。方法:采用慢性不可预见性应激抑郁模型(CUMS)。将40只雄性SD大鼠随机分为4组(对照组、模型组、氟西汀组、GBE50组)。经3周应激刺激后,运用糖水偏爱实验、强迫游泳实验评价造模,并剔除造模不成功老鼠。然后对照组、模型组给予1%CMC灌胃,氟西汀组给予氟西汀(10mg/kg)灌胃,GBE50组给予GBE50(100mg/kg)灌胃,持续3周,最后对各实验组进行糖水偏爱实验、强迫游泳实验测试,并运用Western检测各组大鼠海马组织NLRP3炎症小体及其相关激活信号通路蛋白的表达含量。结果:糖水偏爱实验结果显示,与模型组相比,GBE50(100mg/kg)可以明显增加抑郁大鼠的糖水消耗量。强迫游泳实验结果显示,与模型组相比,GBE50(100mg/kg)可以明显增加抑郁大鼠强迫游泳的挣扎时间。Western结果显示:CUMS可以明显增加模型组NLRP3、ASC、Caspase-1、IL-1β、TLR4、P2X7、P-IKKα/β、P-NF-κB的蛋白表达,而GBE50(100mg/kg)治疗后NLRP3、ASC、Caspase-1、IL-1β、TLR4、P2X7、P-IKKα/β、P-NF-κB蛋白表达明显减少。结论:GBE50(100mg/kg)可以改善CUMS诱导的大鼠的抑郁样行为,而其作用机制与调控TLR4/NF-κB信号通路,抑制NLRP3炎症小体激活有关。

银杏酮酯对小胶质细胞炎症诱导的PC12细胞损伤的保护作用

目的探讨银杏酮酯(GBE50)通过抑制小胶质细胞的炎症反应对神经元突触损伤的影响。方法①采用格里斯(Griess)试剂检测不同浓度GBE50(25~400 mg·L^(-1))干预对经脂多糖(LPS)刺激后BV2小胶质细胞培养液中亚硝酸盐含量的影响。②不同浓度GBE50(25~400 mg·L^(-1))干预经LPS刺激的BV2小胶质细胞,收集上清液作为条件培养基(CM)处理PC12细胞,采用四甲基偶氮唑盐比色(MTT)法检测BV2小胶质细胞和PC12细胞活力。③将对数生长的BV2和PC12细胞以2×106个/孔铺板于6孔板中,分为空白对照组(Ctrl组,仅培养液培养),对照加药组(Ctrl+GBE50组,GBE50干预浓度为200 mg·L^(-1)),模型组(LPS组,LPS刺激浓度为100μg·L^(-1)),模型加药组(LPS+GBE50组,GBE50预处理1 h后,加入LPS),各组进行相应干预。采用Western blot、实时荧光定量逆转录聚合酶链式反应(RT-qPCR)法检测CM处理的PC12细胞N-甲基-D-天门冬氨酸受体(NMDAR)亚基蛋白及基因表达量。结果①Greiss法结果显示,GBE50干预可降低LPS刺激BV2细胞产生的一氧化氮(NO)水平(P<0.05)。②MTT法结果显示,GBE50对BV2细胞活力无影响;LPS刺激后的CM处理PC12细胞活力显著下降,该现象在GBE50干预的CM中有所改善,GBE50浓度在200 mg·L^(-1)时细胞活力已无明显下降(P<0.05)。③Western blot结果显示,与LPS组比较,LPS+GBE50组中NMDAR亚基NR1、NR2A和NR2B蛋白表达升高(P<0.05);RT-qPCR结果显示,与LPS组比较,LPS+GBE50组中NMDAR亚基基因表达量均增加(P<0.05)。结论GBE50可通过抑制激活小胶质细胞的炎症反应,减少NMDAR的损伤,对神经元突触起到保护作用。