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Role of selective serotonin reuptake inhibitors in psychiatric disorders: a comprehensive review.

机译:选择性5-羟色胺再摄取抑制剂在精神疾病中的作用:全面综述。

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The selective serotonin reuptake inhibitors (SSRIs) have emerged as a major therapeutic advance in psychopharmacology. As a result, the discovery of these agents marks a milestone in neuropsychopharmacology and rational drug design, and has launched a new era in psychotropic drug development. Prior to the SSRIs, all psychotropic medications were the result of chance observation. In an attempt to develop a SSRI, researchers discovered a number of nontricyclic agents with amine-uptake inhibitory properties, acting on both noradrenergic and serotonergic neurons with considerable differences in potency. A given drug may affect one or more sites over its clinically relevant dosing range and may produce multiple and different clinical effects. The enhanced safety profile includes a reduced likelihood of pharmacodynamically mediated adverse drug-drug interactions by avoiding affects on sites that are not essential to the intended outcome. SSRIs were developed for inhibition of the neuronal uptake pump for serotonin (5-HT), a property shared with the TCAs, but without affecting the other various neuroreceptors or fast sodium channels. The therapeutic mechanism of action of SSRIs involves alteration in the 5-HT system. The plethora of biological substrates, receptors and pathways for 5-HT are candidates to mediate not only the therapeutic actions of SSRIs, but also their side effects. A hypothesis to explain these immediate side effects is that 5-HT is increased at specific 5-HT receptor subtypes in discrete regions of the body where the relevant physiologic processes are regulated. Marked differences exist between the SSRIs with regard to effects on specific cytochrome P450 (CYP) enzymes, and thus the likelihood of clinically important pharmacokinetic drug-drug interactions. Although no clear relationship exists between the clinical efficacy, plasma concentration of SSRIs, nor any threshold that defines toxic concentrations, but therapeutic drug monitoring (TDM) may be useful in special populations, such as in elderly patients, poor metabolizers (PM) of sparteine (CYP2D6) or mephenytoin (CYP2C19), and patients with liver and kidney impairment. Several meta-analyses have reviewed the comparative efficacy of TCAs and SSRIs, and concluded that both TCAs and SSRIs have similar efficacy in the treatment of depression. SSRIs have demonstrated better efficacy and tolerability in the treatment of obsessive compulsive disorder (OCD). They have also been found to be effective in the treatment for social anxiety disorder both in reducing total levels of social anxiety and in improving overall clinical condition. The benefit of SSRIs in anorexia nervosa (AN) is apparently short-term unless medication is given in the context of nutritional or behavioral therapy. No single antidepressant can ever be recommended for every patient, but in a vast majority of patients, SSRIs should be considered as one of the first-line drugs in the treatment of depression.
机译:选择性5-羟色胺再摄取抑制剂(SSRIs)已作为心理药理学的主要治疗方法出现。结果,这些药物的发现标志着神经心理药理学和合理药物设计的一个里程碑,并开创了精神药物开发的新时代。在SSRIs之前,所有精神药物都是偶然观察的结果。为了开发SSRI,研究人员发现了许多具有胺吸收抑制特性的非三环剂,它们作用于去甲肾上腺素能神经元和5-羟色胺能神经元,但效能却有很大差异。给定的药物可能会影响其临床相关剂量范围内的一个或多个部位,并可能产生多种不同的临床效果。通过避免对预期结果并非必不可少的部位的影响,增强的安全性可降低药效学介导的不良药物相互作用的可能性。开发了SSRIs来抑制5-羟色胺(5-HT)的神经元摄取泵,这是TCA共有的特性,但不影响其他各种神经受体或快速钠通道。 SSRIs的治疗机制涉及5-HT系统的改变。 5-HT的大量生物底物,受体和途径不仅可以介导SSRI的治疗作用,还可以介导其副作用。解释这些直接副作用的假设是,在调节相关生理过程的身体离散区域中,特定的5-HT受体亚型会增加5-HT。 SSRI之间在对特定细胞色素P450(CYP)酶的影响以及临床上重要的药代动力学药物-药物相互作用的可能性方面存在明显差异。尽管临床疗效,SSRIs的血浆浓度以及定义毒性浓度的任何阈值之间均不存在明确的关系,但是治疗药物监测(TDM)在特殊人群中可能有用,例如老年患者,斯巴地碱的弱代谢者(PM) (CYP2D6)或甲吩妥英(CYP2C19),以及肝肾功能不全的患者。几项荟萃分析综述了TCA和SSRI的比较功效,并得出结论,TCA和SSRI在抑郁症治疗中具有相似的功效。 SSRI在强迫症(OCD)的治疗中表现出更好的疗效和耐受性。还发现它们在减少社交焦虑症的总水平和改善整体临床状况方面均有效治疗社交焦虑症。 SSRIs在神经性厌食症(AN)中的益处显然是短期的,除非在营养或行为疗法的情况下给予药物治疗。永远不会为每个患者推荐任何一种抗抑郁药,但是在绝大多数患者中,SSRIs应该被视为治疗抑郁症的一线药物之一。

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