Literature DB >> 22453138

Activation of the orexin 1 receptor is a critical component of CO2-mediated anxiety and hypertension but not bradycardia.

Philip L Johnson1, Brian C Samuels, Stephanie D Fitz, Stafford L Lightman, Christopher A Lowry, Anantha Shekhar.   

Abstract

Acute hypercapnia (elevated arterial CO(2)/H(+)) is a suffocation signal that is life threatening and rapidly mobilizes adaptive changes in breathing and behavioral arousal in order to restore acid-base homeostasis. Severe hypercapnia, seen in respiratory disorders (eg, asthma or bronchitis, chronic obstructive pulmonary disease (COPD)), also results in high anxiety and autonomic activation. Recent evidence has demonstrated that wake-promoting hypothalamic orexin (ORX: also known as hypocretin) neurons are highly sensitive to local changes in CO(2)/H(+), and mice lacking prepro-ORX have blunted respiratory responses to hypercapnia. Furthermore, in a recent clinical study, ORX-A, which crosses blood-brain barrier easily, was dramatically increased in the plasma of patients with COPD and hypercapnic respiratory failure. This is consistent with a rodent model of COPD where chronic exposure to cigarette smoke led to a threefold increase in hypothalamic ORX-A expression. In the present study, we determined the role of ORX in the anxiety-like behavior and cardiorespiratory responses to acute exposure to a threshold panic challenge (ie, 20% CO(2)/normoxic gas). Exposing conscious rats to such hypercapnic, but not atmospheric air, resulted in respiratory, pressor, and bradycardic responses, as well as anxiety-like behavior and increased cellular c-Fos responses in ORX neurons. Systemically, pre-treating rats with a centrally active ORX1 receptor antagonist (30 mg/kg SB334867) attenuated hypercapnic gas-induced pressor and anxiety responses, without altering the robust bradycardia response, and only attenuated breathing responses at offset of the CO(2) challenge. Our results show that the ORX system has an important role in anxiety and sympathetic mobilization during hypercapnia. Furthermore, ORX1 receptor antagonists may be a therapeutic option rapidly treating increased anxiety and sympathetic drive seen during panic attacks and in hypercapnic states such as COPD.

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Year:  2012        PMID: 22453138      PMCID: PMC3376323          DOI: 10.1038/npp.2012.38

Source DB:  PubMed          Journal:  Neuropsychopharmacology        ISSN: 0893-133X            Impact factor:   7.853


  61 in total

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  42 in total

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Journal:  Neuroscience       Date:  2017-01-11       Impact factor: 3.590

2.  The brain orexin system and almorexant in fear-conditioned startle reactions in the rat.

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Review 3.  Role of orexin in the pathophysiology of depression: potential for pharmacological intervention.

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Journal:  CNS Drugs       Date:  2013-06       Impact factor: 5.749

Review 4.  Drug Addiction: Hyperkatifeia/Negative Reinforcement as a Framework for Medications Development.

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5.  5-HT2A receptor activation is necessary for CO2-induced arousal.

Authors:  Gordon F Buchanan; Haleigh R Smith; Amanda MacAskill; George B Richerson
Journal:  J Neurophysiol       Date:  2015-04-29       Impact factor: 2.714

Review 6.  Orexin, stress, and anxiety/panic states.

Authors:  Philip L Johnson; Andrei Molosh; Stephanie D Fitz; William A Truitt; Anantha Shekhar
Journal:  Prog Brain Res       Date:  2012       Impact factor: 2.453

7.  Orexin neuropeptides contribute to the development and persistence of generalized avoidance behavior in the rat.

Authors:  Daniele Viviani; Patrizia Haegler; Francois Jenck; Michel A Steiner
Journal:  Psychopharmacology (Berl)       Date:  2014-10-16       Impact factor: 4.530

8.  First-in-human study with ACT-539313, a novel selective orexin-1 receptor antagonist.

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Journal:  Br J Clin Pharmacol       Date:  2020-03-06       Impact factor: 4.335

9.  Anxiogenic CO2 stimulus elicits exacerbated hot flash-like responses in a rat menopause model and hot flashes in postmenopausal women.

Authors:  Lauren M Federici; Sarah Dorsey Roth; Connie Krier; Stephanie D Fitz; Todd Skaar; Anantha Shekhar; Janet S Carpenter; Philip L Johnson
Journal:  Menopause       Date:  2016-11       Impact factor: 2.953

10.  Dorsal Raphe Serotonin Neurons Mediate CO2-Induced Arousal from Sleep.

Authors:  Haleigh R Smith; Nicole K Leibold; Daniel A Rappoport; Callie M Ginapp; Benton S Purnell; Nicole M Bode; Stephanie L Alberico; Young-Cho Kim; Enrica Audero; Cornelius T Gross; Gordon F Buchanan
Journal:  J Neurosci       Date:  2018-01-29       Impact factor: 6.167

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