MAOI

MAOI
  • 文章类型: Journal Article
    关于药物与迷幻药相互作用的数据是有限的。在这里,我们介绍了将psilocybin蘑菇与单胺氧化酶抑制剂(MAOI)联合使用后,可能是首次发表的高血压紧急情况报告。一名42岁患有难治性抑郁症的男性服用了1克Psilocybecubensis蘑菇,而开了tranylcypromine,缓释右旋苯丙胺-苯丙胺,和其他药物。大约半小时后,他出现了严重的高血压和胸痛,心悸,和头痛。在医院介绍时,心电图显示ST段抬高.病人被诊断为心肌梗塞,并接受劳拉西泮治疗,硝酸甘油,还有阿司匹林.他随后接受了紧急心导管检查,显示没有明显的心脏异常。住院过夜后,他出院回家,没有持久的身体后遗症。虽然数据很少,过去的研究表明,经典的5-羟色胺能迷幻药(5HT-2A受体激动剂),如二甲基色胺(DMT),麦角酸(LSD),与MAOIs联合使用时,合成的psilocybin不应产生高血压急症。我们怀疑苯乙胺,在裸盖菇和其他种类的裸盖菇中发现,与tranylcypromine和右旋苯丙胺-苯丙胺相互作用产生这种高血压急症。在服用psilocybin蘑菇时,应警告服用MAOIs的患者可能会发生高血压急症,特别是当还处方去甲肾上腺素释放剂,如右苯丙胺-苯丙胺。
    Data on medication interactions with psychedelics are limited. Here we present what may be the first published report of a hypertensive emergency following the combination of psilocybin mushrooms with a monoamine oxidase inhibitor (MAOI). A 42-year-old man with treatment-resistant major depressive disorder took 1 g of Psilocybe cubensis mushrooms, while prescribed tranylcypromine, extended-release dextroamphetamine-amphetamine, and other medications. Approximately half an hour later, he developed severe hypertension with chest pain, palpitations, and headache. Upon hospital presentation, the electrocardiogram demonstrated ST-elevation. The patient was diagnosed with a myocardial infarction and treated with lorazepam, nitroglycerin, and aspirin. He subsequently underwent emergency cardiac catheterization, which revealed no significant cardiac abnormalities. Following overnight hospitalization, he was discharged home with no lasting physical sequelae. Though data are few, past studies suggest that classic serotonergic psychedelics (5HT-2A receptor agonists) such as dimethyltryptamine (DMT), lysergic acid (LSD), and synthetic psilocybin should not produce hypertensive emergency when combined with MAOIs. We suspect phenylethylamine, found in Psilocybe cubensis and other species of psilocybin mushrooms, interacted with tranylcypromine and dextroamphetamine-amphetamine to produce this hypertensive emergency. Patients prescribed MAOIs should be warned of the potential for hypertensive emergency when consuming psilocybin mushrooms, particularly when also prescribed norepinephrine releasers such as dextroamphetamine-amphetamine.
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  • 文章类型: Systematic Review
    背景:与精神药物相关的水肿会带来相当大的负担,导致发病率和成本增加。外周性水肿有时与抗抑郁药的使用有关,这是处方最多的精神药物之一。我们回顾了抗抑郁药相关水肿的报告病例,以了解其危险因素。病因学和结果。
    方法:我们搜索了Medline,WebofScience和Embase数据库,以确定报告的与抗抑郁药使用相关的外周水肿病例。我们包括以英语发表的研究和具有全文可用性的研究。对这些报告进行了系统评价,以确定与水肿相关的抗抑郁药,探索可能的危险因素,调查潜在的机制,并评估结果。
    结果:我们确定了总共45例(27例病例报告和5例系列)报告与抗抑郁药使用相关的水肿。发现几乎所有主要类型的抗抑郁药都与水肿有关。在这些药物中,曲唑酮,米氮平,艾司西酞普兰的牵连最严重.年龄较大和女性更常见于水肿。病因学上,α1肾上腺素能受体和5HT2A受体的拮抗作用,导致血管舒张和水肿,成为最普遍的机制。在大多数情况下,停用抗抑郁药后水肿消退。
    结论:与抗抑郁药使用相关的外周性水肿可代表涉及各类抗抑郁药的显著药物不良反应。为了确保及时识别和正确管理水肿,定期监测至关重要。
    BACKGROUND: Oedema associated with psychotropics can impose a considerable burden, leading to increased morbidity and cost. Peripheral oedema is sometimes related to the use of antidepressants, which are among the most prescribed psychotropic medications. We reviewed the reported cases of antidepressant-associated oedema to understand the risk factors, aetiology and outcome.
    METHODS: We searched the Medline, Web of Science and Embase databases to identify reported cases of peripheral oedema associated with antidepressant use. We included studies published in English and those with full-text availability. A systematic review of the reports was done to identify the antidepressants associated with oedema, explore possible risk factors, investigate potential mechanisms, and assess the outcome.
    RESULTS: We identified a total of 45 cases (27 case reports and five case series) that reported oedema associated with antidepressant use. Almost all major classes of antidepressants were found to be associated with oedema. Among these drugs, trazodone, mirtazapine, and escitalopram were the most implicated. Older age and female gender were more commonly associated with oedema. Etiologically, antagonism of α1 adrenergic receptors and 5HT2A receptors, leading to vasodilation and oedema, emerged as the most prevalent mechanisms. In most cases, the oedema subsided following the discontinuation of the antidepressants.
    CONCLUSIONS: Peripheral oedema associated with antidepressant use can represent a significant adverse drug reaction involving various classes of antidepressants. To ensure timely identification and proper management of oedema, regular monitoring is crucial.
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  • DOI:
    文章类型: Journal Article
    1950-60年代用于治疗抑郁症的第一种单胺氧化酶抑制剂(MAOIs)被认为可以成功治疗严重的忧郁抑郁症(MeD),并大大减少了电惊厥治疗(ECT)的需求。在由当时不了解的奶酪反应引起的中断之后,MAOI的使用仅限于非典型和抗治疗性抑郁症,基于来自不足的调查研究的数据,表明它们在MeD中的有效性相对较低。具有不同机制的新型“更好”药物的警笛吸引力放大了这一趋势。在重新评估数据后,我们建议MAOIs在MeD中有效。此外,DSM模型中对重度抑郁症(MDD)的广泛统一概念化减少了对不同抗抑郁药(AD)(如SSRIs)的独特反应的机会,TCA,和MAOIs,从而进一步降低对MAOIs的兴趣。更可靠的MeD分类区分,把它从MDD中解开,如果更灵敏的测量仪器(CORE,使用SMPI)。Wesuggesttheseissueswillbenefitfromre-appraisementviaan归纳推理processwithinabinary(ratherthanunit)modelfordefiningthedifferentdepressingdisords,特别是允许对MeD使用更可靠的诊断标准。我们得出结论,MAOIs仍然是必不可少的,除其他外,抗TCA药物,并且通常应在ECT之前使用;此外,在接受ECT(和氯胺酮/艾氯胺酮)治疗的病例中,它们在维持缓解中起作用。我们建议在治疗算法中更早地使用MAOI,并且比目前的情况具有更大的规律性。
    The first monoamine oxidase inhibitors (MAOIs) used for the treatment of depression in the 1950-60s were credited with treating severe melancholic depression (MeD) successfully and greatly reducing the need for electroconvulsive therapy (ECT). Following the hiatus caused by the then ill-understood cheese reaction, MAOI use was relegated to atypical and treatment-resistant depressions only, based on data from insufficiently probing research studies suggesting their comparatively lesser effectiveness in MeD. The siren attraction of new \'better\' drugs with different mechanisms amplified this trend. Following a re-evaluation of the data, we suggest that MAOIs are effective in MeD. Additionally, the broad unitary conceptualisation of major depressive disorder (MDD) in the DSM model diminished the chance of demonstrating distinctive responses to different antidepressant drugs (ADs) such as SSRIs, TCAs, and MAOIs, thereby further reducing the interest in MAOIs. More reliable categorical distinction of MeD, disentangling it from MDD, may be possible if more sensitive measuring instruments (CORE, SMPI) are used. We suggest these issues will benefit from re-appraisement via an inductive reasoning process within a binary (rather than a unitary) model for defining the different depressive disorders, allowing for the use of more reliable diagnostic criteria for MeD in particular. We conclude that MAOIs remain essential for, inter alia, TCA-resistant MeD, and should typically be used prior to ECT; additionally, they have a role in maintaining remission in cases treated with ECT (and ketamine/esketamine). We suggest that MAOIs should be utilized earlier in treatment algorithms and with greater regularity than is presently the case.
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  • 文章类型: Letter
    暂无摘要。
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  • 文章类型: Journal Article
    单胺氧化酶(MAOA/MAOB)是已知在中枢神经系统(CNS)中神经递质调节中的作用的酶。不可逆和非选择性MAO抑制剂(MAOi)是第一类抗抑郁药,因此,关于选择性MAOA抑制剂clorgyline等药物的后续工作集中在选择性和增加CNS渗透上.MAOA在高级别和转移性前列腺癌中高表达,对前列腺癌的生长具有预期的影响,复发,和抗药性。II期临床试验已经证明了不可逆的非选择性MAOi苯乙嗪对前列腺癌的治疗效果。然而,在纳入的患者人群中,有25%的患者出现了神经系统不良反应导致患者提前戒断.在这项工作中,我们修改了Clorgyline支架,目的是减少CNS渗透,以最大限度地减少CNS相关副作用,同时保留或增强MAOA抑制效力和选择性.使用已知的与hMAOA活性位点中的FAD辅因子结合的Clorgyline的共晶体结构作为参考,我们设计并合成了一系列预测具有较低CNS渗透(logBB)的化合物。所有合成的衍生物都表现出良好的药物样特征,例如预测的Caco-2渗透性和人类口服吸收,并表现出高度选择性的hMAOA结合相互作用。在苯环clorgyline的5位引入HBD基团(NH2或OH)导致3倍更有效的hMAOA抑制,具有同等或更好的hMAOB选择性,和类似的前列腺癌细胞毒性。相比之下,在该位置或末端胺引入较大的取代基显著降低了hMAOA抑制效力,部分归因于MAOA活性位点的结合袋内的空间冲突。用极性更大的N-甲基取代,但较大的2-羟乙基并不能增强药效.然而,在丙基链中引入极性2-羟基保留了高选择性MAOA抑制和Clorgyline的癌细胞细胞毒性,同时将其CNS评分从2降低到0。我们相信,这些结果鉴定了一类新的外周定向的MAOI,其可以允许针对多种抗癌和抗炎适应症的MAOA的更安全的治疗靶向。
    Monoamine oxidases (MAOA/MAOB) are enzymes known for their role in neurotransmitter regulation in the central nervous system (CNS). Irreversible and non-selective MAO inhibitors (MAOi\'s) were the first class of antidepressants, thus subsequent work on drugs such as the selective MAOA inhibitor clorgyline has focussed on selectivity and increased CNS penetration. MAOA is highly expressed in high grade and metastatic prostate cancer with a proposed effect on prostate cancer growth, recurrence, and drug resistance. A Phase II Clinical Trial has demonstrated the therapeutic effects of the irreversible nonselective MAOi phenelzine for prostate cancer. However, neurologic adverse effects led to early withdrawal in 25% of the enrolled patient-population. In this work, we revised the clorgyline scaffold with the goal of decreasing CNS penetration to minimize CNS-related side effects while retaining or enhancing MAOA inhibition potency and selectivity. Using the known co-crystal structure of clorgyline bound with FAD co-factor in the hMAOA active site as a reference, we designed and synthesized a series of compounds predicted to have lower CNS penetration (logBB). All synthesized derivatives displayed favorable drug-like characteristics such as predicted Caco-2 permeability and human oral absorption, and exhibited highly selective hMAOA binding interactions. Introduction of an HBD group (NH2 or OH) at position 5 of the phenyl ring clorgyline resulted in 3x more potent hMAOA inhibition with equivalent or better hMAOB selectivity, and similar prostate cancer cell cytotoxicity. In contrast, introduction of larger substituents at this position or at the terminal amine significantly reduced the hMAOA inhibition potency, attributed in part to a steric clash within the binding pocket of the MAOA active site. Replacement of the N-methyl group by a more polar, but larger 2-hydroxyethyl group did not enhance potency. However, introduction of a polar 2-hydroxy in the propyl chain retained the highly selective MAOA inhibition and cancer cell cytotoxicity of clorgyline while reducing its CNS score from 2 to 0. We believe that these results identify a new class of peripherally directed MAOIs that may allow safer therapeutic targeting of MAOA for a variety of anti-cancer and anti-inflammatory indications.
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  • 文章类型: English Abstract
    The history of studying the effectiveness of therapy of patients with depression by irreversible non-selective monoamine oxidase inhibitors (MAOIs) is analyzed and systematized. Authors describe the stages of the appearance of the first data on the effectiveness of treatment by the first representatives (the 50s of the XX century), the targeted study of the effectiveness of the use of numerous «new» representatives and the emergence of disagreements in assessing the power of therapy (the end of the 50s-60s of the XX century), continuing to study the effectiveness of treatment by representatives who remained in clinical practice, and establishing its clinical predictors (80s-90s of the XX century), the appearance of the first data on the effectiveness of therapy for «atypical depression» (1959-1960) and further development of this issue (80s-90s of the XX century). The stage of formation and development of the idea of the effectiveness of treatment for resistant depression (late 70s-90s of the XX century) is characterized. Separately, the history of studying the effectiveness of application in the USSR and Russia (late 50s- 90s of the XX century) is outlined. The current state of the issue of assessing the effectiveness of therapy (the end of the 90s of the XX century - 2022) is shown.
    В статье проанализирована и систематизирована история изучения эффективности терапии больных депрессией необратимыми неселективными ингибиторами моноаминоксидазы. Описаны этапы появления первых данных об эффективности лечения первыми представителями (50-е годы XX века), прицельного исследования эффективности применения многочисленных «новых» представителей и возникновения разногласий в оценке мощности терапии (конец 50-х — 60-е года XX века), продолжения изучения эффективности лечения представителями, оставшимися в клинической практике, и установления ее клинических предикторов (80—90-е годы XX века), появления первых данных об эффективности терапии при «атипичной депрессии» (1959—1960 гг.) и дальнейшего развития этого вопроса (80—90-е годы XX века). Охарактеризован этап становления и развития представления об эффективности лечения при резистентной депрессии (конец 70-х — 90-е годы XX века). Отдельно обрисована история изучения эффективности применения в СССР и России (конец 50-х — 90-е годы XX века). Показано современное состояние вопроса оценки эффективности терапии (конец 90-х годов XX века — 2022 г.).
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  • 文章类型: Journal Article
    本文是一份临床指南,讨论了经典单胺氧化酶抑制剂(MAOI)抗抑郁药(苯乙嗪,tranylcypromine,和异卡波肼)在现代精神病学实践中。该指南适用于所有临床医生,包括那些可能没有经验的MAOI处方者。它讨论了适应症,药物-药物相互作用,副作用管理,以及各种增强策略的安全性。达成了明确和广泛的共识(70多位国际专家代言人),根据60年的经验,对于此处披露的建议。它们基于经验证据和专家意见-该指南作为新的专家共识标准提出。指南提供实用的临床建议,是合理使用这些药物的基础,特别是因为它改进和更新了知识,纠正了迄今为止文献中突出的各种误解,部分原因是药理学知识不足。该指南建议,在难治性抑郁症(包括性质上的忧郁症)的情况下,应始终考虑MAOIs,并且在电惊厥治疗之前-同时考虑到患者的偏好。在某些情况下,在治疗算法中,它们可能比以前习惯的更早被考虑,并且不应该被视为万不得已的药物;当许多其他治疗失败时,它们可能被证明是决定性的有效。该指南阐明了伴随使用不正确的违禁药物如哌醋甲酯和一些三环抗抑郁药的要点。它还说明了直接的“桥接”方法,可用于简单安全地从其他抗抑郁药过渡到MAOIs。
    This article is a clinical guide which discusses the \"state-of-the-art\" usage of the classic monoamine oxidase inhibitor (MAOI) antidepressants (phenelzine, tranylcypromine, and isocarboxazid) in modern psychiatric practice. The guide is for all clinicians, including those who may not be experienced MAOI prescribers. It discusses indications, drug-drug interactions, side-effect management, and the safety of various augmentation strategies. There is a clear and broad consensus (more than 70 international expert endorsers), based on 6 decades of experience, for the recommendations herein exposited. They are based on empirical evidence and expert opinion-this guide is presented as a new specialist-consensus standard. The guide provides practical clinical advice, and is the basis for the rational use of these drugs, particularly because it improves and updates knowledge, and corrects the various misconceptions that have hitherto been prominent in the literature, partly due to insufficient knowledge of pharmacology. The guide suggests that MAOIs should always be considered in cases of treatment-resistant depression (including those melancholic in nature), and prior to electroconvulsive therapy-while taking into account of patient preference. In selected cases, they may be considered earlier in the treatment algorithm than has previously been customary, and should not be regarded as drugs of last resort; they may prove decisively effective when many other treatments have failed. The guide clarifies key points on the concomitant use of incorrectly proscribed drugs such as methylphenidate and some tricyclic antidepressants. It also illustrates the straightforward \"bridging\" methods that may be used to transition simply and safely from other antidepressants to MAOIs.
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  • DOI:
    文章类型: Journal Article
    这篇综述文章全面讨论了对服用经典单胺氧化酶抑制剂(苯乙嗪,tranylcypromine,异卡波肼),或高剂量(口服或经皮)司来吉兰。它使医生掌握了向患者解释哪些饮食预防措施是必要的知识,为什么会这样:MAOI改变了代谢某些单胺的能力,像酪胺,导致剂量相关的血压升高。现代食品生产和卫生标准导致大多数食品和饮料中酪胺浓度大幅下降,包括许多奶酪。因此,因此引起的血压升高的风险大大降低,但仍需谨慎.其他相关生物胺(组胺,多巴胺),还讨论了氨基酸L-多巴和L-色氨酸。通常在MAOI饮食指南中提供的酪胺数据表本质上是无益和不精确的,因为在同一类别的食物中,酪胺的含量差异很大。出于这个原因,医生必须理解本指南中概述的一般原则;这样,他们可以为个人定制他们的指导和建议,他/她的生活方式和情况。这是重要的,因为升压响应的特征在于显著的患者间变异性。当所有因素都经过权衡和平衡时,结论是MAOI饮食并不是那么困难。尽量减少少量危险食物的摄入量是所需要的。许多患者可能几乎不需要改变他们的饮食。
    This review article features comprehensive discussions on the dietary restrictions issued to patients taking a classic monoamine oxidase inhibitor (phenelzine, tranylcypromine, isocarboxazid), or high-dose (oral or transdermal) selegiline. It equips doctors with the knowledge to explain to their patients which dietary precautions are necessary, and why that is so: MAOIs alter the capacity to metabolize certain monoamines, like tyramine, which causes dose-related blood pressure elevations. Modern food production and hygiene standards have resulted in large reductions of tyramine concentrations in most foodstuffs and beverages, including many cheeses. Thus, the risk of consequential blood pressure increases is considerably reduced-but some caution remains warranted. The effects of other relevant biogenic amines (histamine, dopamine), and of the amino acids L-dopa and L-tryptophan are also discussed. The tables of tyramine data usually presented in MAOI diet guides are by nature unhelpful and imprecise, because tyramine levels vary widely within foods of the same category. For this reason, it is vital that doctors understand the general principles outlined in this guide; that way, they can tailor their instructions and advice to the individual, to his/her lifestyle and situation. This is important because the pressor response is characterized by significant interpatient variability. When all factors are weighed and balanced, the conclusion is that the MAOI diet is not all that difficult. Minimizing the intake of the small number of risky foods is all that is required. Many patients may hardly need to change their diet at all.
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  • 文章类型: Journal Article
    Ayahuasca,盖丘亚语灵魂的葡萄树,是一种迷幻的啤酒,有几种配方,最常见的配方包括Malpighiaceae家族(Banisteriopsiscaapi)中藤本植物的树皮,用咖啡科茜草科(Psychotriaviridis)的灌木叶子。与水混合并煮沸数小时或数天,它产生一种棕色的液体,具有强烈和特征性的味道。Ayahuasca含有迷幻色胺N,N-二甲基色胺(DMT),和单胺氧化酶抑制剂(MAOi),在过去的几年里,它已经过测试。近年来,它的抗抑郁特性已得到测试。来自开放和随机安慰剂对照临床试验的证据显示出令人鼓舞的结果,表明显著和快速的抗抑郁作用,早在ayahuasca干预后1天开始。此外,我们已经使用多变量措施探索了这些影响的性质。在这篇文章中,我们将回顾历史,药理学,临床试验,以及与ayahuasca抗抑郁作用相关的临床和行为标志物。
    Ayahuasca, the vine of the souls in Quechua, is a psychedelic brew with a few formulations that most often include the bark of a liana in the Malpighiaceae family (Banisteriopsis caapi), with leaves from a shrub in the coffee family Rubiaceae (Psychotria viridis). Mixed with water and boiled for hours or days, it produces a brownish-colored liquid with a strong and characteristic taste. Ayahuasca contains the psychedelic tryptamine N,N-Dimethyltryptamine (DMT), and Monoamine Oxidase Inhibitors (MAOi), and in the past few years, it has been tested. In recent years its antidepressant properties have been put to the test. Evidence from open and randomized placebo-controlled clinical trials has shown encouraging results, indicating significant and rapid antidepressant effects, starting as early as 1 day after the ayahuasca intervention. In addition, we have explored the nature of these effects using multivariate measures. In this article, we will review the history, pharmacology, clinical trials, and clinical and behavioral markers associated with the antidepressant effects of ayahuasca.
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  • 文章类型: Journal Article
    单胺氧化酶抑制剂(MAOIs)是第一类现代抗抑郁药;然而,与较新的抗抑郁药相比,它们的利用率不足。
    在这篇系统综述中,采用网络荟萃分析研究MAOIs对抑郁障碍的比较疗效和可接受性.总的来说,网络荟萃分析包括52名双盲,比较14种抗抑郁药或安慰剂的随机对照试验(RCT)。在整个研究中,在总共N=6462例(5309种活性药物;1153种安慰剂)中,平均手臂大小为n=58例.
    除了氟伏沙明,所有抗抑郁药均表现出比安慰剂更好的疗效,没有人表现出明显更好或更坏的全因辍学率。与所有其他治疗方法相比,苯乙嗪表现出更好的疗效证据,与所有其他治疗方法相比,氯米帕明和氯米帕明表现出更好的可接受性证据。
    该研究主要受到低估计精度的限制,这是由于对一些所包括的治疗条件的研究相对缺乏。需要进一步的证据来研究MAOIs对新型抗抑郁药的相对功效。
    该分析的结果在很大程度上支持了对MAOIs作为抗抑郁药在抑郁症治疗方案中使用的重新评估。
    Monoamine oxidase inhibitors (MAOIs) were the first class of modern antidepressants; however, they are under-utilized as compared to the newer antidepressants.
    In this systematic review, network meta-analysis was used to investigate the comparative efficacy and acceptability of MAOIs for depressive disorders. Overall, the network meta-analysis included 52 double-blind, randomized controlled trials (RCTs) that compared 14 antidepressants or placebo. Across studies, the mean arm size was n = 58 participants from a total N = 6462 (5309 active drug; 1153 placebo).
    Except fluvoxamine, all antidepressants demonstrated superior efficacy to placebo, and none demonstrated substantially better or worse all-cause dropout rates. Phenelzine demonstrated superior evidence for efficacy compared to all other treatments, and clomipramine demonstrated superior evidence for acceptability compared to all other treatments.
    The study is primarily limited by low estimate precision due to a relative paucity of studies for some of the included treatment conditions. Further evidence is required to study the relative efficacy of MAOIs against newer antidepressants.
    The results of this analysis largely support the re-evaluation of the use of MAOIs as antidepressant agents in the treatment algorithm of depression.
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