Abstract

Hypothalamic neuropeptide orexin has been implicated in the pathophysiology of psychiatric disorders and accumulating clinical evidence indicates a potential link between orexin and depression. However, the exact role of orexin in depression, particularly the underlying neural substrates and mechanisms, remains unknown. In this study, we reveal a direct projection from the hypothalamic orexinergic neurons to the ventral pallidum (VP), a structure that receives an increasing attention for its critical position in rewarding processing, stress responses, and depression. We find that orexin directly excites GABAergic VP neurons and prevents depressive-like behaviors in rats. Two orexin receptors, OX1R and OX2R, and their downstream Na+–Ca2+ exchanger and L-type Ca2+ channel co-mediate the effect of orexin. Furthermore, pharmacological blockade or genetic knockdown of orexin receptors in VP increases depressive-like behaviors in forced swim test and sucrose preference test. Intriguingly, blockage of orexinergic inputs in VP has no impact on social proximity in social interaction test between novel partners, but remarkably strengthens social avoidance under an acute psychosocial stress triggered by social rank. Notably, a significantly increased orexin level in VP is accompanied by an increase in serum corticosterone in animals exposed to acute stresses, including forced swimming, food/water deprivation and social rank stress, rather than non-stress situations. These results suggest that endogenous orexinergic modulation on VP is especially critical for protecting against depressive reactions to stressful events. The findings define an indispensable role for the central orexinergic system in preventing depression by promoting stress resilience.

Highlights

  • Depression is a prevalent and life-threatening psychiatric disorder and one of the leading causes of disease burden worldwide [1, 2]

  • We demonstrate that ventral pallidum (VP) receives direct innervation from the hypothalamic orexinergic neurons, and orexin directly excites GABAergic VP neurons via two orexin receptors, OX1R and OX2R

  • Given the findings that blockage of orexinergic inputs in VP by knocking down orexin receptors induces depressive-like behaviors in paradigms with, rather than without, acute stress, we attribute the protective role of the central orexinergic system against depression, partly but substantially, to promotion of stress resilience via its direct modulation on VP activity

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Summary

Introduction

Depression is a prevalent and life-threatening psychiatric disorder and one of the leading causes of disease burden worldwide [1, 2]. These authors contributed : Miao-Jin Ji, Xiao-Yang Zhang. Patients with narcolepsy-cataplexy manifest moderate to severe depressive symptoms [21, 22]. These clinical clues indicate an emerging role of the central orexinergic system in the pathophysiology of depression and prevention of depression. Given the findings that blockage of orexinergic inputs in VP by knocking down orexin receptors induces depressive-like behaviors in paradigms with, rather than without, acute stress, we attribute the protective role of the central orexinergic system against depression, partly but substantially, to promotion of stress resilience via its direct modulation on VP activity

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