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神经酰胺与抑郁症:一项系统综述。

Ceramides and depression: A systematic review.

作者信息

Dinoff Adam, Herrmann Nathan, Lanctôt Krista L

机构信息

Neuropsychopharmacology Research Group, Hurvitz Brain Sciences Program, Sunnybrook Research Institute, Toronto, Ontario, Canada; Department of Pharmacology and Toxicology, Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada.

Neuropsychopharmacology Research Group, Hurvitz Brain Sciences Program, Sunnybrook Research Institute, Toronto, Ontario, Canada; Department of Psychiatry, Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada.

出版信息

J Affect Disord. 2017 Apr 15;213:35-43. doi: 10.1016/j.jad.2017.02.008. Epub 2017 Feb 7.

Abstract

BACKGROUND

Major depressive disorder is a significant contributor to global disability and mortality. The mechanisms of depression are vast and not fully understood, and as a result current treatment of depression is suboptimal. Aberrant sphingolipid metabolism has been observed in some cases of depression, specifically alterations in ceramide concentrations. The role of ceramides and other sphingolipids in depression is a novel concept. This review summarizes and evaluates the current state of evidence for a role of ceramides in depression pathophysiology and the potential for novel depression pharmacotherapies targeting ceramide metabolism.

METHODS

Medline, Embase, and PsycINFO databases were searched through October 2016 for English-language studies using combinations of the search terms: ceramide, depression, sphingolipid, and depressive symptoms.

RESULTS

Of the 489 articles screened, 14 were included in the qualitative synthesis of this review article. Pre-clinical and clinical evidence suggest that ceramide species may contribute to depression pathophysiology. In human studies, ceramides C18:0 and C20:0 are the species most strongly linked to depression. Evidence for altered ceramide metabolism in depression is present, but data for a causal role of ceramides in depression are lacking.

LIMITATIONS

This review was limited by potential reporting bias. Furthermore, a lack of specificity of which ceramides were altered in depression was common.

CONCLUSIONS

Pharmacotherapy targeting ceramide metabolism may be a novel treatment option for depression. A number of pharmacological targets exists for ceramide reduction and a number of currently approved medications inhibit ceramide production. More evidence, pre-clinical and clinical, is warranted to determine the extent and consistency of the role of ceramides in depression.

摘要

背景

重度抑郁症是导致全球残疾和死亡的重要因素。抑郁症的发病机制广泛且尚未完全明确,因此目前对抑郁症的治疗效果欠佳。在一些抑郁症病例中观察到鞘脂代谢异常,特别是神经酰胺浓度的改变。神经酰胺和其他鞘脂在抑郁症中的作用是一个新概念。本综述总结并评估了目前关于神经酰胺在抑郁症病理生理学中的作用以及针对神经酰胺代谢的新型抑郁症药物治疗潜力的证据状况。

方法

通过检索Medline、Embase和PsycINFO数据库,查找截至2016年10月的英文研究,检索词组合为:神经酰胺、抑郁症、鞘脂和抑郁症状。

结果

在筛选的489篇文章中,有14篇纳入了本综述文章的定性分析。临床前和临床证据表明,神经酰胺可能与抑郁症病理生理学有关。在人体研究中,神经酰胺C18:0和C20:0与抑郁症关联最为紧密。抑郁症中存在神经酰胺代谢改变的证据,但缺乏神经酰胺在抑郁症中起因果作用的数据。

局限性

本综述受到潜在报告偏倚的限制。此外,抑郁症中哪些神经酰胺发生改变缺乏特异性是常见现象。

结论

针对神经酰胺代谢的药物治疗可能是抑郁症的一种新型治疗选择。存在多种降低神经酰胺的药理学靶点,并且一些目前已获批的药物可抑制神经酰胺的产生。需要更多的临床前和临床证据来确定神经酰胺在抑郁症中的作用程度和一致性。

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