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.

银杏叶提取物联合多奈哌齐对阿尔茨海默病模型大鼠的协同作用及其机制

目的探讨银杏叶提取物(EGb 761)联合多奈哌齐对阿尔茨海默病(AD)模型大鼠的协同作用及其机制。方法取雄性SD大鼠72只,随机分为正常组(等体积生理盐水)、假手术组(等体积生理盐水)、模型组(等体积生理盐水)、多奈哌齐组(25 mg/kg)、EGb 761组(50 mg/kg)和联合组(多奈哌齐25 mg/kg+EGb 76150 mg/kg),各12只。腹膜内注射水合氯醛300 mg/kg麻醉,将聚集的Aβ25-35(10μL)以1μL/min的速率注入大鼠双侧海马,以复制AD大鼠模型。建模成功后,各组大鼠均灌胃相应药物或生理盐水,每天1次,共2个疗程(每个疗程10 d,间隔3 d)。采用Morris水迷宫实验评估大鼠的认知和记忆能力;采用TUNEL染色法,观察大鼠海马神经细胞凋亡情况,并计算凋亡指数;采用酶联免疫吸附法检测大鼠血清乙酰胆碱酯酶(AChE)、丙二醛(MDA)、超氧化物歧化酶(SOD)水平;采用Western blot法检测大鼠海马组织中核因子(NF)-κB通路相关蛋白p-IKKα,p-IκBα,p-NF-κB表达水平。结果与模型组比较,各给药组大鼠Morris水迷宫实验第6天逃避潜伏期均大幅缩短,第7天各给药组大鼠在象限Ⅰ中穿越平台的次数及耗时百分比均显著增加;各给药组大鼠海马神经细胞阳性数量均显著减少,凋亡指数均显著降低(P<0.05);各给药组大鼠AChE和MDA水平均显著降低,SOD水平显著升高(P<0.05);各给药组大鼠NF-κB通路相关蛋白p-IKKα,p-IκBα,p-NF-κB的表达水平均显著升高(P<0.05);且联合组上述指标变化均更显著(P<0.05)。结论EGb 761联合多奈哌齐可协同改善AD模型大鼠的记忆能力,其机制可能与减少海马神经细胞NF-κB通路激活后的细胞凋亡有关。

A ginkgo biloba extract promotes proliferation of endogenous neural stem cells in vascular dementia rats

The ginkgo biloba extract EGb761 improves memory loss and cognitive impairments in patients with senile dementia. It also promotes proliferation of neural stem cells in the subventricular zone in Parkinson＇s disease model mice and in the hippocampal zone of young epileptic rats. However, it remains unclear whether EGb761 enhances proliferation of endogenous neural stem cells in the brain of rats with vascular dementia. In this study, a vascular dementia model was established by repeatedly clipping and reperfusing the bilateral common carotid arteries of rats in combination with an intraperitoneal injection of a sodium nitroprusside solution. Seven days after establishing the model, rats were intragastrically given EGb761 at 50 mg/kg per day. Learning and memory abilities were assessed using the Morris water maze and proliferation of endogenous neural stem cells in the subventricular zone and dentate gyrus were labeled by 5-bromo-2-deoxyuridine immunofluorescence in all rats at 15 days, and 1, 2, and 4 months after model establishment. The escape latencies in Morris water maze tests of rats with vascular dementia after EGb761 treatment were significantly shorter than the model group. Immunofluorescence staining showed that the number and proliferation of 5-bromo-2-deoxyuridine-positive cells in the subventricular zone and dentate gyrus of the EGb761-treated group were significantly higher than in the model group. These experimental findings suggest that EGb761 enhances proliferation of neural stem cells in the subventricular zone and dentate gyrus, and significantly improves learning and memory in rats with vascular dementia.

Effects of Ginkgo biloba extract on expression of biomarkers during aflatoxin B_1-induced hepatocarcinogenesis in Wistar rats

Objective： The aim of this study was to study the effect of Ginkgo biloba extract （EGb761） on metabolism of afiatoxin B1 （AFB1） in Wistar rats. Methods： Seventy one Wistar rats were assigned at random to groups A, B and C. Rats in groups A, B were injected with AFB1 （intraperitoneal, 100-200 ug/kg body weight, 1-3 times/week）. Group C was normal control. Rats in group B were fed in food with EGb761, while rats in groups A, C were given normal food. Blood samples were collected and liver biopsies were performed on the 14th, 28th and 42nd week. All the rats were sacrificed on the 64th week. The incidence of hepatocarcinoma was investigated. The hepatic phase I drug-metabolizing enzyme Cytochrome-P450 （CYP450） and phase II metabolizing enzyme glutathione S-transferase （GST） were analyzed with spectrometry. Serum AFB1- lysine adduct levels were assessed with high performance liquid chromatography （HPLC）. The expression of 8-hydroxydeoxy- guanosine （8-OHdG） was measured with immunohistochemistry. Results： The incidence of hepatocellular carcinoma （HCC） in group B was significantly lower than that in group A （26.92% vs 76.00%, P 〈 0.001）. No HCC developed in group C. EGb761 showed no effects on the activities of CYP450 and GST in rat liver tissues. The level of AFB1-lysine adduct reached the peak （4356.01 pg/mg albumin） at the 14th week in group A. EGb761 significantly inhibited the formation of AFB1-lysine adduct in serum by 13.07% at the 14th week （P = 0.033）, and 73.63% at the 42nd week （P = 0.002）. The expression of 8-OHdG protein in rat liver tissues in group B was significantly lower than that in group A at the 28th, 42nd, and 64th week （P 〈 0.05）. Conclusion： The main mechanism underlying the effect of EGb761 in blocking hepatocarcinogenesis induced by AFB1 may not be fully attributable to its influence on the activity of liver phase I and phase II metabolizing enzymes. EGb761 inhibits the production of AFB1-lysine adducts, decreases the expression of 8-OHdG protein, and finally alleviates the DNA oxidative injury, which may be one of the mechanisms for the effects of EGb761 in inhibiting or delaying AFB1-induced hepatocarcinogenesis.

Ginkgo biloba Extract EGb 761® Improves Central Vestibular Vertigo in Patients Undergoing Vestibular Exercises: A Randomised Placebo-Controlled Trial

Background: Ginkgo biloba extract EGb 761® is widely used to treat various types of vertigo. Aims: An exploratory trial was conducted to evaluate the efficacy of EGb 761® in addition to vestibular exercises in central vestibular vertigo caused by vertebro-basilar ischaemia. Subjects and Methods: In this randomised, placebo-controlled, double-blind trial, 40 patients were enrolled in the vertigo clinic of a neurological university hospital and treated with daily doses of 240 mg EGb 761® or placebo for a period of 180 days. All patients regularly performed vestibular exercises in addition. Efficacy was assessed using: a visual analogue scale for the patients to rate the overall intensity of vertigo;a numeric scale for physician-rated change;a vertigo score based on intensity, duration, and frequency of vertigo;and electronystagmography. Results: Until day 180, the mean patient-rated intensity of vertigo decreased by 46% during EGb 761® treatment and by 19% with placebo (p ® group compared to the placebo group. Nystagmus or other eye movement disorders were present only in small subgroups of patients without sufficient statistical power to detect differences between treatment groups. Conclusions: EGb 761® alleviated vertigo caused by ischaemic lesions in the brainstem or cerebellum in patients undergoing vestibular exercises.

银杏叶提取物预防在体心肌缺血再灌注损伤

目的 :探讨中药成份银杏叶提取物 ( ginkgo biloba extract,EGb 761)在体心肌缺血再灌注损伤中的作用及其机制。方法 :以在体大鼠心肌缺血再灌注为模型 ,分别于再灌注前 10 min静脉给予生理盐水或不同剂量的 EGb 761,检测缺血再灌区心肌组织丙二醛 ( MDA )、一氧化氮 ( NO)含量。结果 :缺血再灌注使相应区域心肌 MDA、NO含量上升 ,EGb 761治疗组心肌MDA、NO含量下降 ,但下降程度与 EGb 761剂量不呈量效关系。结论 :EGb 761通过抗氧自由基和清除一氧化氮能预防在体心肌缺血再灌注损伤。

银杏叶提取物EGb-761对乳腺癌肺转移型小鼠体内实体瘤的影响

目的:探讨银杏叶提取物EGb-761对乳腺癌肺转移型小鼠体内实体瘤的影响。方法:选取雌性BALB/c小鼠,使用小鼠乳腺癌4T1细胞系建立高转移性的肿瘤小鼠模型,随机分为五组,即正常组、模型组、EGb-761组[高剂量组(200 mg/kg)、中剂量组(100 mg/kg)、低剂量组(50 mg/kg)]。观察并测量各组小鼠原位灶实体瘤体积和小鼠体质量;观察并计算各组小鼠肺部转移灶结节数、转移率;采用RT-PCR法检测各组小鼠特异性标志物角蛋白-19(CK-19)mRNA表达。结果:随着EGb-761剂量的增加,小鼠原位灶实体瘤体积越来越小,而小鼠体质量越来越重(P<0.05);随着EGb-761剂量的增加,肺部结节数随之减少(P<0.05),肺部转移率随之降低(P<0.05);随着EGb-761剂量的增加,肺组织CK-19 mRNA表达量越低(P<0.05)。结论:银杏叶提取物(EGb-761)对乳腺癌肺转移型小鼠体内的实体瘤生长有抑制作用。

银杏叶提取物对实验性肝纤维化大鼠COX-2、TNF-α等表达的影响

研究银杏叶提取物(EGb)对CCl_4诱导的大鼠肝纤维化肝组织COX-2、TNF-α及TLR4mRNA表达的影响。采用皮下注射40%CCl_4植物油溶液制备大鼠肝纤维化模型。造模第4周后,开始给药。以高低两个剂量的EGb进行干预,同时设计正常组、秋水仙碱组。每天给药1次,给药期间大鼠仍皮下注射40%CCl_4植物油溶液。给药6周后处死大鼠,通过RT-PCR技术观察大鼠肝组织中COX-2、TNF-α及TLR4 mRNA的表达。RT-PCR结果显示,与正常组相比,模型组大鼠肝组织的COX-2、TNF-α及TLR4mRNA表达明显增加(P<0.01);银杏叶提取物(EGb)干预组(100,50 mg/kg)较模型组大鼠肝组织的COX-2、TNF-α及TLR4 mRNA表达明显下降(P<0.05)。结论银杏叶提取物(EGb)能够抑制大鼠肝纤维化肝组织COX-2、TNF-α及TLR4的表达。

银杏叶提取物防治心脑血管疾病的研究进展

银杏叶提取物(Ginkgo biloba extract)是目前国际上使用最为广泛的中药提取物之一,主要活性成分是银杏黄酮和银杏内酯类化合物。心脑血管疾病是全球主要的病死原因,对其防治具有重要的意义。近年来的研究表明,银杏叶提取物对心脑血管疾病的防治有多环节、多靶点、不良反应小的优势,应用前景良好。因此,本文综述了近年来银杏叶提取物对心脑血管疾病的防治作用和机制。

银杏叶提取物对衰老小鼠学习记忆障碍的改善作用

目的:探讨银杏叶提取物(extract of Gingko biloba leaves,EGB)对衰老小鼠学习、记忆障碍的改善作用及其作用机制。方法:将33只雄性小鼠分为3组,每组11只。即模型组:按300mg/kgBW剂量腹腔注射D-半乳糖,1次/d;治疗组:在按上述剂量注射D-半乳糖的同时,按15mg/kgBW剂量腹腔注射EGB,1次/d;对照组:按上述同样剂量注射生理盐水溶液,1次/d。所有实验处理进行6周后停止给药,用Y式迷宫、跳台法检测小鼠的学习记忆能力,同时测定肝、脑组织的单胺氧化酶(monoamine oxidase,MAO)活性。结果治疗组的学习、记忆成绩均显著高于模型组,差异都具有统计学意义(P<0.05或P<0.01)。结论:EGB对于衰老小鼠的学习、记忆障碍有明显的改善作用,在其作用机制中,MAO发挥了重要作用。