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.

A Strategy to Employ Clitoria ternatea as a Prospective Brain Drug Confronting Monoamine Oxidase (MAO) Against Neurodegenerative Diseases and Depression

Ayurveda is a renowned traditional medicine practiced in India from ancient times and Clitoria ternatea is one such prospective medicinal herb incorporated as an essential constituent in a brain tonic called as medhya rasayan for treating neurological disorders.This work emphasises the significance of the plant as a brain drug there by upholding Indian medicine.The phytochemicals from the root extract were extricated using gas chromatography–mass spectrometry assay and molecular docking against the protein Monoamine oxidase was performed with four potential compounds along with four reference compounds of the plant.This persuades the prospect of C.ternatea as a remedy for neurodegenerative diseases and depression.The in silico assay enumerates that a major compound(Z)-9,17-octadecadienal obtained from the chromatogram with a elevated retention time of 32.99 furnished a minimum binding affinity energy value of-6.5 kcal/mol against monoamine oxidase(MAO-A).The interactions with the amino acid residues ALA 68,TYR 60 and TYR 69 were analogous to the reference compound kaempferol-3-monoglucoside with a least score of-13.90/-12.95 kcal/mol against the isoforms(MAO)A and B.This study fortifies the phytocompounds of C.ternatea as MAO-inhibitors and to acquire a pharmaceutical approach in rejuvenating Ayurvedic medicine.

A novel fluorogenic probe for monoamine oxidase assays

Monoamine oxidase is flavoenzymes, widely distributed in mammals. It is well recognized that MAOs serve an important role in metabolism that they have close relationship with health .Along with the discoveries between MAOs and neurotic disease, more and more studies have been jumped in .In this paper, we design a new probe for assaying the activities of MAOs. The results showed that the probe [7-（3-aminopropoxy）coumarin] is simple, effective and sensitive for MAOB.

Preliminary in vitro evaluation of neuroprotective and monoamine oxidase type B inhibitory effects of newly synthesized 8-aminocaffeines

The expected growth of the elderly population at highest risk for Parkinson’s disease(PD)in the next decades makes the identification of factors that promote or prevent the disease an important goal.In addition,new therapies-aiming to delay the progression of PD are also needed(Prediger,2010).However,there have been few clinical trials designed to investigate neuroprotection.Thus the application of an appropriate in vitro model such as the neuroblastoma SH-SY5Y cell line is extremely helpful.These cells were selected due to its human origin,catecholaminergic neuronal properties,and ease of maintenance(Xicoy et al.,2017).

DNA methylation of the Monoamine Oxidases A and B genes in postmortem brains of subjects with schizophrenia

Aims: We focused on DNA methylation of the promoter regions of the Monoamine Oxidase (MAO) A and B genes from postmortem brains of subjects with schizophrenia. Methods: We determined levels of DNA methylation using genomic DNA samples purified from four brain areas: prefrontal cortex (PFC), hippocampus, occipital cortex and nucleus accumbens (NAc), by a bisulfite sequencing method from seven normal subjects and six subjects with schizophrenia. Results: Although very few methylated CpGs of the MAOA and MAOB genes were detected in male samples, various DNA methylation patterns were present in female samples, and some differences were found in such patterns between normal subjects and subjects with schizophrenia. In the PFC, the average level of methylation of both genes was significantly higher in subjects with schizophrenia than in normal subjects. The content of highly methylated alleles of the MAOA gene in the NAc was significantly associated with schizophrenia, with similar results obtained for the MAOB gene in both the NAc and PFC. Some CpG sites showed higher levels of methylation in schizophrenia than in normal subjects. Conclusions: Levels of methylation were quite high in NAc and PFC in female subjects with schizophrenia compared with those in female normal subjects.

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.

Tyramine in Malt Beverages Interfering with Monoamine Oxidase Inhibitor Drugs

The objective of this review is the determination of tyramine in 13 nonalcoholic beers (Maoshaieer) of Tehran market and survey of it’s probably interaction with monoamine oxidase inhibitor drugs (MAOIs) has been investigated. Tyramine was at the highest levels in Baltika (111.34 ± 8.19 μg/ml) and at the lowest level in Bitmalt (8.01 ± 2.09 μg/ml). Comparing different flavors of malt drinks, the highest tyramine content was shown for classic or normal flavor (average 72.99 ± 30.87 μg/ml), while the lowest value belonged to cantaloupe flavored drinks (average 10.55 ± 1.29 μg/ml). In our study, it is seen that there is a significant difference between import and Iranian non-alcoholic beers, the import ones has more tyramine than Iranians. A number of 10 kinds of 13 samples interact whit MAOIs in one serving (250 ml) usage 18.50 mg. The highest tyramine content of Iranian ones is 17.74 mg/250ml and for import ones is 27.83 mg/250ml.

一种白僵菌中MAO抑制剂的分离纯化和结构鉴定

本研究对前期筛选出的一株具有较强的单胺氧化酶(MAO)抑制活性的白僵菌菌株Ba02进行了液体培养;通过不同提取剂的提取效果比较,发现乙酸乙酯能较好地提取出该发酵液中单胺氧化酶抑制剂。通过活性指导下的色谱分离,从乙酸乙酯提取物中得到了一种深红色粉末状化合物。活性测定结果显示该化合物在15μg.mL-1时对MAO-A和MAO-B的抑制率分别为97.50%和95.34%。MS和NMR的鉴定结果表明该化合物为卵孢菌素(Oosporein)。虽然该化合物是一已知化合物,但其对单胺氧化酶的抑制活性尚属首次发现。

次黄嘌呤－内源性单胺氧化酶（MAO）抑制剂样活性的研究

体外实验证明，嘌呤类化合物对Ｂ－型ＭＡＯ活性有不同程度的抑制作用，其抑制强度为：次黄嘌呤＞鸟便嘌呤＞腺嘌呤＞嘌呤＞黄嘌呤＞尿酸。老龄小鼠（１８月龄）的血、脑及肝组织ＭＡＯ活性较年青小鼠（１月龄）显著升高，而上述组织中嘌呤类化合物的含量却随年龄增加而降低。老龄小鼠肝线粒体外膜ＭＡＯ提取物中次黄嘌呤含量明显低于年青小鼠，但两组ＭＡＯ中腺嘌呤含量却无明显差异。离体温孵实验证明［３Ｈ］次黄嘌呤与老龄小鼠脑和肝ＭＡＯ结合量明显高于年青小鼠。体内结合实验结果亦表明［３Ｈ］次黄嘌呤与老龄小鼠肝ＭＡＯ结合量高于年青小鼠外，并证明［３Ｈ］次黄嘌呤的结合部位是在ＭＡＯ酶蛋白上，而非在辅基上。此外，多次灌服次黄嘌呤２００ｍｇ／ｋｇ可明显抑制老龄小鼠脑ＭＡＯ－Ｂ活性，并使单胺类物质（５－ＨＴ、ＤＡ）含量明显增加。

CUS致大鼠抑郁行为涉及TPH2、DDC及MAO-A异常表达的实验研究

目的探讨慢性不可预见刺激(chronically unpredicted stress,CUS)致大鼠抑郁行为与端脑和海马色氨酸羟化酶2(tryptophan hydroxylase-2,TPH2)、多巴脱羧酶(dopa-decarboxylase,DDC)及单胺氧化酶A(monoamine oxidase-A,MAOA)mRNA及蛋白表达的关系。方法 30只♂SD大鼠随机分为模型组(MG)与对照组(CG),每组15只。采用孤养结合CUS连续刺激28 d建立大鼠抑郁模型;以开场实验和强迫游泳实验评价大鼠抑郁行为;采用实时荧光定量PCR与Western blot方法分别检测大鼠端脑和海马TPH2、DDC、MAO-A mRNA及蛋白表达。结果与对照组大鼠相比,模型组大鼠开场实验运动得分明显降低(P<0.01)、强迫游泳不动时间明显延长(P<0.01);端脑和海马TPH2和DDC mRNA及蛋白表达明显下降(P<0.01,P<0.05)、MAO-A mRNA及蛋白表达明显升高(P<0.01,P<0.05)。结论CUS诱导大鼠产生抑郁症样行为,其机制可能与TPH2、DDC及MAO-A异常表达有关。

V_A与V_E对梭曼(GD)染毒大鼠MDA和MAO的影响

目的 研究梭曼染毒大鼠丙二醛 (MDA)含量和单胺氧化酶 (MAO)活性的变化 ,探讨抗氧化剂 VA,VE对梭曼染毒大鼠自由基损伤的保护作用 .方法 雄性大鼠 40只 ,按体质量随机分为 4组 :阴性对照组 ,阳性对照组 ,VA 和 VE实验组 .观察染毒大鼠血清、大脑、肝、肾组织 MDA含量和 MAO活性的变化 .结果 梭曼 (GD)染毒大鼠阳性对照组 5阴性 5对照组相比较 ,脑组织 MDA含量和 MAO活性有显著性增加 (P<0 .0 5 ) ;血清蛋白有显著减少 (P<0 .0 5 ) ,肝蛋白有显著增加(P<0 .0 5 ) .VA 实验组与阳性对照组比较 ,脑组织 MDA有显著增加 (P <0 .0 1) ,肝组织 MDA有显著降低 (P<0 .0 1) ;脑组织 MAO活性增加 ,但差异不显著 .VE实验组与阳性对照组相比 ,肾脏 MDA有显著减少 (P<0 .0 1) ;脑组织 MAO活性有非常显著的降低 (P<0 .0 1) .施加 VA,VE抗氧化剂后 ,与阳性对照组比较 ,血清和肝蛋白有非常显著减少 (P<0 .0 1) ,脑蛋白有显著减少 (P<0 .0 5 ) .结论 梭曼 (GD)染毒引起明显脂质过氧化损伤 ,VE具有抗氧化保护作用 ,而 VA 有协同促进

绞股蓝总苷对老化小鼠脑中MAO和Na/K-ATP酶活性的影响

目的 研究绞股蓝总苷对老化小鼠脑中 MAO和 Na/ K- ATP酶活性的影响。方法 采用连续眼球后注射D-半乳糖 1个月 ,造成小鼠老化模型 ,观察绞股蓝总苷对老化鼠脑中单胺氧化酶 (MAO)和 Na/ K- ATP酶的活性影响。结果 老化小鼠可造成脑中 MAO活力的升高和 Na/ K - ATP活力的降低 ,而绞股蓝总苷在造模型同时 ig给药 ,每日剂量 75和 15 0 m g/ kg下 ,能逆转小鼠因老化而产生的上述二种酶活性的改变。结论 绞股蓝总苷能对抗老化小鼠因衰老引起的 MAO和 Na/ K- ATP酶的活性改变 ,从生化酶学角度 。

Aβ损伤后大鼠SYP和MAO的变化及加减地黄饮子的干预作用

目的:观察β-淀粉样蛋白1-40(Aβ1-40)大鼠海马双侧注射后大脑组织突触素(synaptophysin,SYP)表达和单胺氧化酶(monoamine oxidase,MAO)活性的变化及加减地黄饮子的干预作用。方法:采用大鼠海马立体定向注射凝聚态Aβ1-40诱导老年性痴呆(Alzheimer s disease,AD)动物模型。采用免疫印迹(western blotting)方法检测大脑组织SYP的表达,通过紫外分光光度法检测大鼠大脑组织MAO的活性。结果:模型组大鼠大脑组织SYP蛋白表达相对值(0.508±0.187)较假手术组(0.915±0.069,P<0.05)明显降低,而加减地黄饮子(0.833±0.077,P<0.05)可上调SYP的表达。模型组大鼠脑组织MAO活性(7.88±0.76U/h/mg/prot)较空白对照组(5.17±0.33U/h/mg/prot,P<0.05)明显升高,而这种升高可被加减地黄饮子(7.04±0.72U/h/mg/prot)抑制。结论:加减地黄饮子通过上调SYP蛋白的表达和抑制MAO活性而发挥保护Aβ对大鼠脑神经细胞的损伤。

血清MAO、5’-NT及SAA联合检测在肝脏疾病诊断中的应用价值

目的探讨血清单胺氧化酶(MAO)、5’-核苷酸酶(5’-NT)、淀粉样蛋白A(SAA)联合诊断肝脏疾病的价值。方法选择2017年3月至2019年12月我院门诊及住院治疗的110例肝病及100例健康成年人作为研究对象,所有受试者测定血清MAO、5’-NT、SAA水平。收集天冬氨酸氨基转移酶(AST)、丙氨酸氨基转移酶(ALT)等肝生化指标,比较两组受试者指标差异并分析诊断价值。结果肝脏疾病组患者血清MAO、5’-NT、SAA水平及肝生化指标AST、ALT水平均显著高于对照组,差异具统计学意义(P<0.05);Pearson相关性分析示,血清MAO、5’-NT水平与肝生化指标AST、ALT指标呈正相关关系(P<0.05);ROC曲线分析示,血清MAO、5’-NT、SAA水平单独诊断肝脏疾病的曲线下面积(AUC)分别为0.754、0.773、0.722,当截点值为9.26 U/L、23.77 U/L、7.26 mg/L时,约登指数最大;MAO+5’-NT、MAO+SAA、5’-NT+SAA、三者联合诊断的AUC分别为0.796、0.784、0.789、0.805,三者联合诊断价值最高。结论肝脏疾病患者伴有血清MAO、5’-NT、SAA水平的明显升高,临床可将其单独或联合检测用于诊断、评估肝脏病变。

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。

抑郁症患者血清MAO、MDA、hs-CRP水平检测及其临床意义

目的检测抑郁症患者血清MAO、MDA、hs-CRP含量,探讨MAO、MDA、hs-CRP水平与抑郁症发病的相关性。方法采用化学比色法、硫代巴比妥酸法和散射免疫比浊法分别测定42例抑郁症患者血清MAO、MDA、hs-CRP含量,并与30名正常健康人做比较。结果抑郁症患者血清MAO、MDA、hs-CRP水平[分别为(32.24±2.32)U/ml,(3.63±0.75)nmol/ml,(5.05±0.92)mg/L]明显高于对照组[分别为(21.26±1.96)U/ml,(3.16±0.82)nmol/ml,(1.88±0.81)mg/L],差异均有统计学意义。结论抑郁症患者血清MAO、MDA、hs-CRP水平均显著升高,与抑郁症发病机制关系密切。

宁夏无果枸杞芽提取物对自然衰老小鼠学习记忆、MAO、GSH-Px及ChAT活性的影响

目的观察宁夏无果枸杞芽提取物(FLE)对自然衰老小鼠学习、记忆功能,脑组织中谷胱甘肽过氧化物酶(GSH-Px)、单胺氧化酶(MAO)、乙酰胆碱转移酶(ChAT)的活力的影响,探讨FLE抗衰老机制。方法将60只13月龄自然衰老昆明小鼠分为老年对照组和FLE低剂量组(FLE1组)、FLE中剂量组(FLE2组)、FLE高剂量组(FLE3组),每组15只;另将15只6月龄昆明小鼠做为成年对照组。FLE1组、FLE2组、FLE3组分别用质量/体积百分比为5%、10%、20%FLE灌胃,0.2mL·(10g·d)-1,老年对照组和成年对照组灌胃等量生理盐水,连续8周。用Morris水迷宫检测各组小鼠给药前后的学习记忆能力;分光光度法检测脑组织中GSH-Px、MAO和ChAT的活性;免疫组化方法检测小鼠大脑皮层和海马区的ChAT的表达。结果给药后,与成年对照组比较,老年对照组小鼠逃避潜伏期延长、目标象限停留时间百分比缩短(P<0.01),脑组织中MAO活力增高,GSH-Px、ChAT活性降低(P<0.01);与老年对照组比较,FLE2组、FLE3组小鼠逃避潜伏期缩短、目标象限停留时间百分比延长(P<0.01),FLE3组脑组织中MAO活性降低、GSH-Px活性明显升高(P<0.01),FLE2及FLE3组脑组织中ChAT活性增高(P<0.01);FLE各组间比较,FLE3组治疗效果较FLE1组及FLE2组好(P<0.01)。结论较高浓度的FLE能够改善自然衰老昆明小鼠的学习记忆能力,其机制可能与FLE提高GSH-Px活性,降低MAO活性,发挥抗氧化作用以及上调脑组织中ChAT的活性,提高脑组织中乙酰胆碱含量有关。

血清MAO、5’-NT、GGT检测在诊断原发性肝癌中的价值

目的探讨血清单胺氧化酶(MAO)、5′-核苷酸酶(5′-NT)、γ-谷氨酰基转移酶(GGT)检测在诊断原发性肝癌中的价值。方法选择43例原发性肝癌患者,52例良性肝病患者及35例健康体检者,比较各组血清MAO、5′-HT、GGT水平,并分析血清MAO、5′-HT、GGT水平在检测原发性肝癌中的价值。结果原发性肝癌组血清MAO、5′-HT、GGT水平高于良性肝病组,良性肝病组血清MAO、5′-HT及GGT水平高于健康对照组,差异有统计学意义(P<0.05)。血清MAO曲线下面积为0.718、敏感度和特异度分别为0.571和0.418;5′-NT曲线下面积为0.717、敏感度和特异度分别为0.558和0.476;GGT曲线下面积为0.714、敏感度和特异度分别为0.738和0.334;联合检测曲线下面积为0.884、敏感度和特异度分别为0.401和0.881,联合检测曲线下面积大于单个指标检测。结论血清MAO、5′-NT及GGT是反映肝功能损伤程度的敏感指标,联合检测可为原发性肝癌的诊断提供可靠依据。

结节性红斑患者血清总IgE和MAO水平测定

目的:检测结节性红斑患者血清总IgE和单胺氧化酶(MAO)含量。方法:选择结节性红斑患者115例及正常人36名,应用化学发光免疫分析仪和全自动生化分析仪分别检测其血清总IgE和MAO。结果:结节性红斑患者血清总IgE含量235.36±295.14 IU/mL高于健康对照组83.19±82.52IU/mL(P<0.05),血清MAO含量15.55±14.32 U/L高于健康对照组7.43±3.76 U/L(P<0.01)。结论:IgE和MAO可能参与了结节性红斑的发病过程。