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Neuroimaging markers of cellular function in major depressive disorder: implications for therapeutics, personalized medicine, and prevention.

机译:严重抑郁症患者细胞功能的神经影像标记物:对治疗方法,个性化药物和预防的意义。

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It is estimated that 15% of all individuals will experience a major depressive episode (MDE) during their lifetime and that treatment response is inadequate in 40% of these cases. To address this, neuroimaging is being used to identify MDE subtypes and mechanisms of onset as well as to optimize target occupancy of novel treatments. Neuroimaging of monoamine oxidase-A (MAO-A) binding; glutamate levels; indexes of 5-HT(2A), 5-HTT, 5-HT(1A), and 5-HT(1B) receptors; levels of dopamine transporters D(1) and D(2); and hippocampal volume are described here. Three themes emerge. First, symptoms such as pessimism, motor retardation, anxiety disorder, and verbal memory deficits best indicate the subtype of depression. Second, measures related to mechanisms of monoamine loss, particularly elevated MAO-A binding in prefrontal and anterior cingulate cortex, are present in MDE and in high-risk states for MDE. Third, clinical trials show a consistent 80% 5-HTT occupancy of selective serotonin reuptake inhibitors at doses sufficient to distinguish from placebo in clinical trials (although in vitro affinities vary 100-fold), thereby supporting the need for further occupancy studies to accelerate therapeutic development.
机译:据估计,所有个体中有15%在其一生中会经历严重的抑郁发作(MDE),并且在这些病例中有40%的治疗反应不足。为了解决这个问题,神经影像学被用于识别MDE亚型和发病机制,并优化新疗法的靶标占有率。单胺氧化酶-A(MAO-A)结合的神经成像;谷氨酸水平; 5-HT(2A),5-HTT,5-HT(1A)和5-HT(1B)受体的指标;多巴胺转运蛋白D(1)和D(2)的水平;和海马体积在这里描述。出现了三个主题。首先,悲观,运动迟缓,焦虑症和言语记忆障碍等症状最能说明抑郁症的亚型。其次,在MDE和MDE的高危状态中,存在与单胺丢失机制有关的措施,特别是额叶前额扣带和前扣带回皮质中MAO-A的结合增加。第三,临床试验表明选择性5-羟色胺再摄取抑制剂在5-HTT的使用率始终保持在临床试验中足以区别于安慰剂的剂量(尽管体外亲和力相差100倍),从而支持进行进一步的占用率研究以加速治疗的需要发展。

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