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首页> 外文期刊>European Archives of Psychiatry and Clinical Neuroscience >The role of ceramide in major depressive disorder
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The role of ceramide in major depressive disorder

机译:神经酰胺在重度抑郁症中的作用

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Major depression is a severe mood disorder with a lifetime prevalence of more than 10%. The pharmacokinetic hypothesis claims that a slow accumulation of antidepressant drugs by acid trapping mainly into lysosomes is responsible for the therapeutic latency and that a lysosomal target mediates the antidepressant effects. The lysosomal lipid metabolizing enzyme acid sphingomyelinase (ASM) cleaves sphingomyelin into ceramide and phosphorylcholine. In a pilot study, the activity of this enzyme was increased in peripheral blood cells of patients with major depressive disorder (MDD), making the ASM an interesting molecular target of antidepressant drugs. Indeed, several antidepressant drugs functionally inhibit ASM. The ASM/ceramide pathway might be a missing link unifying independent findings in neurobiology and the treatment of MDD such as therapeutic latency, oxidative stress, immune activation and increased risk of cardiovascular disease.
机译:重度抑郁症是一种严重的情绪障碍,终生患病率超过10%。药代动力学假说声称,主要通过将酸捕获到溶酶体中来使抗抑郁药缓慢积累,这是治疗潜伏期的原因,而溶酶体靶标则介导了抗抑郁作用。溶酶体脂质代谢酶酸性鞘磷脂酶(ASM)将鞘磷脂裂解为神经酰胺和磷酸胆碱。在一项前期研究中,这种酶的活性在患有重度抑郁症(MDD)的患者的外周血细胞中增加,使ASM成为抗抑郁药的有趣分子靶标。实际上,几种抗抑郁药在功能上抑制ASM。 ASM /神经酰胺途径可能是一个缺失的环节,无法统一神经生物学和MDD治疗(例如治疗潜伏期,氧化应激,免疫激活和心血管疾病风险增加)的独立发现。

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