Type-B monoamine oxidase inhibitors in neurological diseases:clinical applications based on preclinical findings

Type-B monoamine oxidase inhibitors,encompassing selegiline,rasagiline,and safinamide,are available to treat Parkinson's disease.These drugs ameliorate motor symptoms and improve motor fluctuation in the advanced stages of the disease.There is also evidence suppo rting the benefit of type-B monoamine oxidase inhibitors on non-motor symptoms of Parkinson's disease,such as mood deflection,cognitive impairment,sleep disturbances,and fatigue.Preclinical studies indicate that type-B monoamine oxidase inhibitors hold a strong neuroprotective potential in Parkinson's disease and other neurodegenerative diseases for reducing oxidative stress and stimulating the production and release of neurotrophic factors,particularly glial cell line-derived neurotrophic factor,which suppo rt dopaminergic neurons.Besides,safinamide may interfere with neurodegenerative mechanisms,countera cting excessive glutamate overdrive in basal ganglia motor circuit and reducing death from excitotoxicity.Due to the dual mechanism of action,the new generation of type-B monoamine oxidase inhibitors,including safinamide,is gaining interest in other neurological pathologies,and many supporting preclinical studies are now available.The potential fields of application concern epilepsy,Duchenne muscular dystrophy,multiple scle rosis,and above all,ischemic brain injury.The purpose of this review is to investigate the preclinical and clinical pharmacology of selegiline,rasagiline,and safinamide in Parkinson's disease and beyond,focusing on possible future therapeutic applications.

Monoamine Oxidase-B Inhibitor Rasagiline Effects on Motor and Non-Motor Symptoms in Individuals with Parkinson’s Disease: A Systematic Review and Meta-Analysis

Objective: In the manuscript titled Monoamine Oxidase-B Inhibitor Rasagiline Effects on Motor and Non-Motor Symptoms in Individuals with Parkinsons Disease: A Systematic Review and Meta-Analysis, the objective was to conduct a systematic review with meta-analysis to investigate the effects that Rasagiline has on motor and non-motor symptoms in individuals with PD. Introduction: Rasagiline is a second-generation monoamine oxidase-B (MAO-B) inhibitor used both as monotherapy and adjunctive therapy for Parkinsons Disease (PD). Methods: A systematic literature search and meta-analysis were performed with randomized control trials that investigated the effects of Rasagiline on motor and non-motor symptoms in individuals with PD. The systematic search was conducted in PubMed, Cochrane, and EBSCO databases. Methodological quality was assessed using the Cochrane Grading Recommendations Assessment, Development and Evaluation approach. Results: Fourteen studies were included in our review. There were trivial to small and statistically significant improvements in motor symptoms for individuals with PD treated with Rasagiline compared to placebo. Non-motor symptoms showed no significant improvement with Rasagiline compared to placebo in five of six meta-analyses. Results were based on very low to moderate certainty of evidence. Conclusion: 1 mg/day Rasagiline significantly improved Parkinsonian motor symptoms in individuals with PD compared with placebo. For all outcomes, the 1 mg/day Rasagiline group was favored over the placebo group.

Association of adverse effects with monoamine oxidase type B inhibitor and catechol-o-methyl transferase inhibitor combination therapy in Parkinson’s disease patients

Currently, levodopa is the most effective and commonly used medication to control motor symptoms in Parkinson’s disease (PD). However, its long-term use is associated with adverse effects (AEs). Combination therapy of a monoamine oxidase type B inhibitor (MAOBI) with levodopa or a catechol-O-methyl transferase inhibitor (COMTI) with levodopa provides benefits to PD patients. Direct comparison of efficacy and side effect profiles is complex. The aim of this study is to investigate the different AE profiles of MAOBI and COMTI combination therapies. Data used to analyze the AEs of different PD medications were retrieved from “The Boston University Medical Center’s Parkinson’s Disease and Movement Disorder Database”. Ten categories of AEs were compared between patients receiving MAOBI and COMTI combination treatment. In total, 87 subjects were included in the analysis. Out of ten AEs, the presence of dementia was signifi- cantly different between the MAOBI and COMTI groups with an OR of 6.9 (COMTI vs MAOBI, 95% CI 1.3 - 37.0). Motor fluctuations were also found to be differently distributed in the two medication groups with an OR of 3.1 (COMTI vs MAOBI, 95% CI 1.0 - 9.8). In this retrospective database analysis of patients treated with combination treatment for PD, combination therapy of a COMTI with levodopa was more likely to be associated with dementia and motor fluctuations than a MAOBI with levodopa.

内源性MAO-B抑制因子-靛红预防MPTP对多巴胺神经递质的耗竭作用(英文)

研究内源性单胺氧化酶B抑制因子 靛红 (2 ,3 吲哚醌 ,isatin)对MPTP引起的小鼠纹状体DA含量降低的影响。用高效液相色谱配电化学检测器测定纹状体DA ,DOPAC和HVA水平。MPTP 30mg/kgip使纹状体DA ,DOPAC和HVA含量与各自对照组比较显著降低 (P <0 .0 1) ,预先靛红 (2 0 0mg/kg·d ,× 4d ,ig)几乎完全抑制了上述效应 ,并减少了MPTP对DA更新率的升高 ,说明靛红有预防MPTP对中枢DA能神经元的毒性。

尼莫地平对铝损伤大鼠脑组织MAO-B表达的影响

目的观察铝负荷大鼠脑组织单胺氧化酶B(MAO-B)的活性与表达改变,并探讨尼莫地平对该动物模型的影响。方法采用三氯化铝(AlCl3)(400mg/kg)灌胃大鼠,1次/d,5d/w,持续3个月,建立铝负荷致大鼠慢性脑损伤的动物模型,尼莫地平(80mg/kg)在每次铝给予4h后灌胃,观察行为学、生化酶学、MAO-B mRNA及蛋白表达水平等指标的变化。结果铝负荷能明显导致大鼠被动回避性学习记忆能力和空间识别能力障碍,使其脑组织乙酰胆碱转移酶(ChAT)活性显著降低(P<0.01),而胆碱酯酶(AchE)活性显著升高(P<0.01),超氧化物歧化酶(SOD)活性显著降低(P<0.01),而丙二醛(MDA)含量显著升高(P<0.01),MAO-B活性与MAO-B mRNA及蛋白表达水平显著增加(P<0.01);NMDP能明显改善铝负荷大鼠的学习记忆能力障碍,明显阻遏铝负荷大鼠海马组织ChAT与SOD活性的降低,AchE活性与MDA含量的增高,MAO-B活性及其mRNA与蛋白表达的增加。结论铝负荷致大鼠脑损伤涉及脑组织的MAO-B活性与表达改变;NMDP可能降低铝负荷大鼠脑组织MAO-B表达和活性,并增加SOD活性,减少自由基而保护大鼠慢性脑损伤。

单胺氧化酶B在神经元退行性变模型中的意义研究

目的:研究不同神经元退行性变动物模型中单胺氧化酶B(MAO B)活性变化,并探讨其意义。方法:NIH雄性小鼠,分别建立脑缺血再灌注、铝过负荷及一氧化碳中毒神经元退行性变模型。采用Morris水迷宫和跳台实验进行学习记忆能力测试,HE切片染色光镜下观察海马病理变化和以市售标准试剂盒测定脑匀浆MAO B活性。结果:各模型组小鼠较相应对照组学习记忆能力显著降低,海马切片可见神经元核固缩和细胞丢失等退行性改变。脑缺血再灌注模型组MAO B活性与对照组相比无显著变化,但铝中毒和一氧化碳中毒模型小鼠MAO B活性较对照组显著升高。结论:MAO B活性异常升高在各种神经元退行性变动物模型中不具有普遍性意义。脑缺血再灌注模型可能适用于痴呆研究,而一氧化碳中毒和铝过负荷模型可能适用于痴呆和锥体外系疾病研究。

β-淀粉样肽损伤后小鼠脑单胺氧化酶B、白细胞介素6的变化及中药的干预作用

目的观察β-淀粉样肽(Aβ)25-35致痴呆小鼠模型脑单胺氧化酶B(MAO-B)、白细胞介素-6(IL-6)的改变及中药脑复聪的干预作用.方法脑室内注射Aβ25-35造成痴呆模型小鼠,用Morris水迷宫测空间学习记忆功能;用比色法测MAO-B活性;免疫组化检测IL-6.结果模型小鼠的Morris水迷宫潜伏期(81.3±13.4)s,比对照组(34.2±10.9)s延长(P<0.05);大脑皮层和海马的MAO-B活性(120.12±10.15)、(83.60±5.29)均较对照组(93.09±10.54)、(50.39±9.16)升高(P<0.05～0.01),海马齿状回有大量IL-6免疫荧光阳性细胞.经脑复聪治疗后,水迷宫潜伏期(43.7±12.7)s缩短(P<0.05);海马的MAO-B活性(47.11±6.57)回降(P<0.01);IL-6免疫阳性神经细胞减少.结论抑制海马MAO-B的过度激活,减少自由基的产生,减少氧化应激反应,抑制小胶质细胞产生炎性因子IL-6,缓解Aβ的损伤作用,阻断AD发病的重要环节,是中药脑复聪治疗AD的重要机理之一.

草问荆总生物碱对小鼠脑单胺氧化酶-B活性的影响

目的 研究草问荆总生物碱 (TAEP)对小鼠脑单胺氧化酶 -B(MAO-B)活性的影响 ,揭示 TAEP对中枢神经系统抑制作用的机制。方法 采用紫外分光光度法测定 MAO-B的活性。结果 TAEP对小鼠脑 MAO-B具有明显的激活作用 ,并具有对抗烟肼酰胺抑制小鼠脑 MAO-B活性的作用。结论 TAEP是 MAO-B的激动药 ,有单胺代谢作用 ,这可能是

单胺氧化酶活性分析在HBV感染者中的应用

目的分析乙肝病毒(HBV)感染者血清单胺氧化酶活性,研究其临床应用价值.方法应用终点比色法检测血清单胺氧化酶(MAO)活性;ELISA法检测乙肝病毒标志物;PCR法检测HBv DNA;常规方法检测ALT.结果 ALT异常组,大三阳HBsAg(+),HBeAg(+),Anti-HBc(+)和小三阳HBsAg(+),Anti-HBe(+),Anti-HBc(+)合并HBV DNA阳性的HBV感染者MAO显著升高,而小三阳并HBV DNA阴性者MAO升高不明显;ALT正常组仅40例大三阳患者MAO升高明显,其他各组MAO大多在正常范围内.结论 HBV感染后,只要有病毒复制,就会破坏肝细胞,引起MAO升高.MAO活性分析对肝脏病情的判断有重要价值.

老年大鼠耳蜗酪氨酸羟化酶及单胺氧化酶-B基因的表达

目的 检测老年大鼠耳蜗多巴胺(dopamine,DA)合成和降解过程中的关键酶——酪氨酸羟化酶(tyroxinehydroxylase,TH)及单胺氧化酶-B(monoamine oxidase-B,MAO-B)基因的mRNA水平变化,以便更好地理解听觉系统老化的机制。方法 采用半定量逆转录聚合酶链反应(reverse transcription polymerase chain reaction,RTPCR)的方法检测耳蜗组织TH及MAO-B基因mRNA的含量。结果 耳蜗组织TH及MAO-B基因mRNAR的水平,老年组均高于成年组,差异均有非常显著性意义(tTH=9.634,tMA0-B=8.108,P<0.01)。结论 在基因转录水平证明了老年大鼠耳蜗多巴胺系统合成和降解过程发生了紊乱,推测耳蜗多巴胺代谢的变化在老年性聋的发生机制中可能起一定的作用。

铝过负荷致小鼠脑神经元退变与脑单胺氧化酶B的关系

目的:采用铝负荷致小鼠脑损伤模型,探讨铝致神经元退行性变与脑单胺氧化酶B代谢失衡的关系。方法:每鼠侧脑室内分别注射浓度为0.125%、0.25%、0.5%的AlCl3 3μl,连续给药5天,建立不同量铝过负荷致脑损伤小鼠模型。于给药后第10天、第20天和第30天测定小鼠学习记忆功能、海马病理形态学改变、单胺氧化酶B(Monoamine oxidase B,MAO-B)活性。结果:铝过负荷致小鼠脑内MAO-B活力显著升高和CA1区出现明显神经元丢失及核固缩;上述指标均呈剂量依赖性和时间依赖性改变。结论:铝过负荷致神经元退变可能与其干扰脑单胺氧化酶B代谢有关。

单胺氧化酶B单核苷酸基因多态性与犬旷场行为关联分析

采用旷场行为测试方法,测定204条德国牧羊犬、拉布拉多犬、史宾格犬二月龄幼犬在新异环境下的兴奋性和探索活动,同时应用RFLP-PCR方法检测单胺氧化酶B(Monoamine Oxidase B,MAOB)基因的多态性,分析MAOB基因的基因型和基因频率在品种间的分布差异以及基因多态性与旷场测验中行为参数的相互关系,发现MAOB基因型频率与基因频率在犬品种之间差异极显著(P<0．01),MAOB基因型与幼犬在旷场中的走动时间、趴卧时间、跨格次数、站立扒墙次数有关(P<0．01或P<0．05),对运动姿势改变次数也有一定影响(P=0．064)。其中,TT基因型犬的走动时间和跨格次数均高于TC型和CC型犬(P<0．05),运动姿势改变次数和站立扒墙次数高于CC型犬(P<0．05);而CC型个体的趴卧时间高于TT型个体(P<0．05)。MAOB基因对走动时间和跨格次数的加性遗传效应达极显著(P<0．01),对运动姿势改变次数、站立扒墙次数和趴卧时间有显著的加性效应(P<0．05)。实验结果表明,MAOB基因与幼犬在旷场测验中的运动、兴奋性和探索活动有关,TT基因型对运动、兴奋性和探索活动具有正遗传效应。

单胺氧化酶B——治疗神经元退行性变的可能靶点

单胺氧化酶B(MAOB)是一类黄素依赖性蛋白酶,由520个氨基酸构成,通过C端的跨膜螺旋结合于线粒体外膜。MAOB基因定位于X染色体,核心启动子位于-246/-99。MAOB基因表达受多种因素调控。MAOB在多巴胺代谢途径中发挥重要作用。可将多巴胺降解为二羟苯乙酸,并生成过氧化氢。MAOB基因敲除小鼠对神经毒素1-甲基-4-苯基-1,2,3,6-四羟嘧啶(MPTP)具有耐受性。MAOB分布于脑内特定脑区,在多种神经元退行性疾病中发现脑内MAOB活性升高。MAOB可能发挥着调节氧化应激、参与神经元退行性变等作用。

洋金花提取物对单胺氧化酶B的抑制作用研究

目的研究洋金花对单胺氧化酶B(MAO-B)的抑制效果及抑制类型。方法采用醇提水沉法对洋金花不同部位进行提取,获得提取物,并计算得率。利用分光光度法研究了洋金花不同部位提取物对MAO-B的抑制作用。对花提取物抑制数据进行分析,求得花提取物对MAO-B的半数抑制浓度IC_(50)值。进一步对花提取物抑制MAO-B的动力学进行考察,根据双倒数曲线结果判定抑制机制。结果洋金花提取物对MAO-B有抑制作用,花部位提取物抑制效果最强,浓度为1 mg/ml时,对MAO-B的抑制率为(55.74±1.5)%,半数抑制浓度IC_(50)为0.75 mg/ml。抑制动力学研究结果表明,洋金花提取物对MAO-B的抑制作用属于混合型抑制。结论洋金花提取物对MAO-B具有明显抑制作用,属于混合性抑制,这可能是洋金花对PD具治疗作用的机制之一。

单胺氧化酶B抑制剂对急性脑出血患者APACHE Ⅱ评分和GCS评分的影响

目的评价单胺氧化酶B抑制剂对急性脑出血(ICH)患者急性生理和慢性健康评分(APACHEⅡ)评分和格拉斯哥昏迷(GCS)评分的影响。方法共纳入ICH患者82例,随机分为对照组和观察组各41例,对照组采用常规内科治疗,必要时行外科手术;观察组联合应用单胺氧化酶B抑制剂5mg·d-1×14d。对比两组患者治疗前和治疗后1个月、3个月APACHEⅡ评分和GCS评分。结果治疗1个月和3个月后两组患者APACHEⅡ评分逐渐降低,GCS评分逐渐升高;且观察组改善程度显著高于对照组,差异有统计学意义(P<0.05)。3个月后两组患者昏迷程度均显著改善,且观察组正常患者比例显著高于对照组,差异有统计学意义(P<0.05)。结论单胺氧化酶B抑制剂可有效改善ICH患者APACHEⅡ、GCS评分与临床预后。

人参茎叶皂甙及其单体对大鼠脑内B型单胺氧化酶活性的影响

本文用体外法研究了人参茎叶皂甙(GSLS)及其单体Rg_1,Rg_2,Re和Rh_1大鼠脑内B型单胺氧化酶(MAO-B)活性的影响。结果表明,GSLS和Rh_1可加强MAO-B的活性。Rg_1和Rg_2可抑制MAO-B的活性,其抑制强度与3.3×10^(-5)mg/ml优降宁相当。抑制特征曲线表明Rg_1和Rg_2对MAO-B的抑制作用均属竞争性抑制。

经前舒颗粒对经前期综合征肝气郁证模型大鼠海马单胺氧化酶A、B表达的影响

目的:研究经前舒颗粒对经前期综合征(PMS)肝气郁证大鼠海马单胺氧化酶A/B(MAOA/B)表达水平的影响。方法:雌性未孕SD大鼠48只,随机分为3组:正常对照组、模型组、经前舒治疗组,束缚造模法复制PMS肝气郁证大鼠模型,旷场实验对模型进行评价,治疗组采用经前舒颗粒治疗,RT-PCR和Western blot方法分别检测各组大鼠海马MAOA/B的mRNA及蛋白的表达。结果:模型大鼠海马MAOA mRNA及蛋白表达显著升高,经前舒颗粒治疗后,MAOA mRNA和蛋白表达均显著降低,而MAOB mRNA和蛋白表达各组间没有显著性变化。结论:PMS肝气郁证大鼠海马MAOA表达出现异常,经前舒颗粒的作用机制可能是通过调节海马MAOA的表达而发挥作用。

High-throughput discovery of highly selective reversible hMAO-B inhibitors based on at-line nanofractionation

Human monoamine oxidase B(hMAO-B)has emerged as a pivotal therapeutic target for Parkinson's disease.Due to adverse effects and shortage of commercial drugs,there is a need for novel,highly selective,and reversible hMAO-B inhibitors with good blood-brain barrier permeability.In this study,a high-throughput at-line nanofractionation screening platform was established with extracts from Chuanxiong Rhizoma,which resulted in the discovery of 75 active compounds,including phenolic acids,volatile oils,and phthalides,two of which were highly selective novel natural phthalide hMAO-B inhibitors that were potent,selective,reversible and had good blood‒brain permeability.Molecular docking and molecular dynamics simulations elucidated the inhibition mechanism.Sedanolide(IC_(50)=103 nmol/L;SI=645)and neocnidilide(IC_(50)=131 nmol/L;SI=207)demonstrated their excellent potential as hMAO-B inhibitors.They offset the limitations of deactivating enzymes associated with irreversible hMAO-B inhibitors such as rasagiline.In SH-SY5Y cell assays,sedanolide(EC_(50)=0.962μmol/L)and neocnidilide(EC_(50)=1.161μmol/L)exhibited significant neuroprotective effects,comparable to the positive drugs rasagiline(EC_(50)=0.896μmol/L)and safinamide(EC_(50)=1.079μmol/L).These findings underscore the potential of sedanolide as a novel natural hMAO-B inhibitor that warrants further development as a promising drug candidate.

单胺氧化酶B单核苷酸多态性与幼犬工作行为性状的关联分析

测定了204条德国牧羊犬、拉布拉多犬、史宾格犬二月龄幼犬对人依恋性和服从性、衔取、争夺游戏和胆量等行为性状,同时用PCR-RFLP方法检测各犬单胺氧化酶B(MAOB)基因型。用2χ检验MAOB基因多态性的基因型和基因频率在品种间的分布,发现基因型和基因频率在犬品种之间差异极显著(P<0.01)。构建一般线性模型分析MAOB基因型与行为性状的关系,发现MAOB基因型对幼犬的衔取行为有显著影响(P<0.05)。TC基因型犬的衔取得分值均高于TT型(P<0.01)。这些结果表明,MAOB基因可能是影响犬衔取行为的主效基因或与主效基因紧密连锁的标记基因,可用于建立选择犬衔取性状的基因标记辅助选择方法。

HBV感染者单胺氧化酶活性分析的临床价值

目的分析乙型肝炎病毒(HBV)感染者的血清单胺氧化酶(MAO)活性,探讨MAO活性分析在HBV感染者的临床应用价值。方法回顾分析了284例HBV感染者及123例正常对照者的血清MAO活性水平。结果与正常对照组比较,A组(ALT升高,大三阳者)、B组(ALT升高,小三阳、HBV-DNA阳性者)、D组(ALT正常,大三阳)MAO均呈明显升高(P<0.01);C组(ALT升高,小三阳、HBV-DNA阴性者)、E组(ALT正常,小三阳、HBV-DNA阳性者)、F组(ALT正常,小三阳、HBV-DNA阴性者)MAO水平无显著性变化(P>0.05)。结论对HBV感染者进行血清MAO活性分析,有助于了解肝细胞损害情况,预测肝纤维化的发生,对病情判断有重要意义。