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Brain neurotoxic amyloid-beta peptides: their potential role in the pathophysiology of depression and as molecular therapeutic targets

机译:脑神经毒性淀粉样β肽:它们在抑郁症的病理生理中的潜在作用,并作为分子治疗靶标

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摘要

The monoamine hypothesis ascribes an important role to the underactivity of brain monoamines such as 5-HT, noradrenaline and dopamine to the pathophysiology of depression. This view emerged more than 50 years ago and has guided development of most medications currently used for the treatment of this disorder. However, large numbers of depressed individuals treated with currently available antidepressant agents, or even with various combinations, do not respond. Residual symptoms, relapses and recurrences are common while receiving adequate doses of these medications. In a recent issue of the BJP, Colaianna et al. describe results suggesting that a new neurobiological mechanism with treatment implications should be considered for the development of depression in humans, namely, elevations in potentially neurotoxic brain amyloid-β peptides.
机译:单胺假说归因于脑单胺(如5-HT,去甲肾上腺素和多巴胺)的活性不足对抑郁症的病理生理作用。这种观点在50多年前就出现了,并指导了目前用于治疗这种疾病的大多数药物的开发。但是,用目前可用的抗抑郁药或什至以各种组合治疗的大量抑郁症患者没有反应。残余症状,复发和复发在接受足够剂量的这些药物时很常见。在BJP的最新一期中,Colaianna等人。描述的结果表明,对于抑郁症的发展,应该考虑具有治疗意义的新的神经生物学机制,即潜在的神经毒性脑淀粉样蛋白β肽的升高。

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