Orexin/hypocretin receptor modulation of anxiolytic and antidepressive responses during social stress and decision-making: Potential for therapy
•Orexin/hypocretins innervate limbic regions associated with anxiety and depression.•Orexins are reciprocally innervated with CRF.•Orexin 1 receptors promote anxious and pro-depressive behavior.•Orexin 2 receptor knockdown promotes anxious and depressive behaviors.•Orexin 2 agonists are anxiolytic a...
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Published in | Brain research Vol. 1731; p. 146085 |
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Main Authors | , , , , |
Format | Journal Article |
Language | English |
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Elsevier B.V
15.03.2020
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Abstract | •Orexin/hypocretins innervate limbic regions associated with anxiety and depression.•Orexins are reciprocally innervated with CRF.•Orexin 1 receptors promote anxious and pro-depressive behavior.•Orexin 2 receptor knockdown promotes anxious and depressive behaviors.•Orexin 2 agonists are anxiolytic and anti-depressive.
Hypothalmic orexin/hypocretin (Orx) neurons in the lateral and dorsomedial perifornical region (LH-DMH/PeF) innervate broadly throughout the brain, and receive similar inputs. This wide distribution, as well as two Orx peptides (OrxA and OrxB) and two Orx receptors (Orx1 and Orx2) allow for functionally related but distinctive behavioral outcomes, that include arousal, sleep-wake regulation, food seeking, metabolism, feeding, reward, addiction, and learning. These are all motivational functions, and tie the orexin systems to anxiety and depression as well. We present evidence, that for affective behavior, Orx1 and Orx2 receptors appear to have opposing functions. The majority of research on anxiety- and depression-related outcomes has focused on Orx1 receptors, which appear to have primarily anxiogenic and pro-depressive actions. Although there is significant research suggesting contrary findings, the primary potential for pharmacotherapies linked to the Orx1 receptor is via antagonists to block anxious and depressive behavior. Dual orexin receptor antagonists have been approved for treatment of sleep disorders, and are likely candidates for adaptation for affect disorder treatments. However, we present evidence here that demonstrates the Orx2 receptors are anxiolytic and antidepressive. Using a new experimental pre-clinical model of anxious and depressive behavior stimulated by social stress and decision-making that produces two stable behavioral phenotypes, Escape/Resilient and Stay/Susceptible, we tested the effects of intracerebroventricular injections of Orx2 agonist and antagonist drugs. Over ten behavioral measures, we have demonstrated that Orx2 agonists promote resilience, as well as anxiolytic and antidepressive behavior. In contrast, Orx2 antagonists or knockdown kindle anxious and pro-depressive behavior plus increase susceptibility. The results suggest that the Orx2 receptor may be a useful target for pharmacotherapies to treat anxiety and depression. |
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AbstractList | •Orexin/hypocretins innervate limbic regions associated with anxiety and depression.•Orexins are reciprocally innervated with CRF.•Orexin 1 receptors promote anxious and pro-depressive behavior.•Orexin 2 receptor knockdown promotes anxious and depressive behaviors.•Orexin 2 agonists are anxiolytic and anti-depressive.
Hypothalmic orexin/hypocretin (Orx) neurons in the lateral and dorsomedial perifornical region (LH-DMH/PeF) innervate broadly throughout the brain, and receive similar inputs. This wide distribution, as well as two Orx peptides (OrxA and OrxB) and two Orx receptors (Orx1 and Orx2) allow for functionally related but distinctive behavioral outcomes, that include arousal, sleep-wake regulation, food seeking, metabolism, feeding, reward, addiction, and learning. These are all motivational functions, and tie the orexin systems to anxiety and depression as well. We present evidence, that for affective behavior, Orx1 and Orx2 receptors appear to have opposing functions. The majority of research on anxiety- and depression-related outcomes has focused on Orx1 receptors, which appear to have primarily anxiogenic and pro-depressive actions. Although there is significant research suggesting contrary findings, the primary potential for pharmacotherapies linked to the Orx1 receptor is via antagonists to block anxious and depressive behavior. Dual orexin receptor antagonists have been approved for treatment of sleep disorders, and are likely candidates for adaptation for affect disorder treatments. However, we present evidence here that demonstrates the Orx2 receptors are anxiolytic and antidepressive. Using a new experimental pre-clinical model of anxious and depressive behavior stimulated by social stress and decision-making that produces two stable behavioral phenotypes, Escape/Resilient and Stay/Susceptible, we tested the effects of intracerebroventricular injections of Orx2 agonist and antagonist drugs. Over ten behavioral measures, we have demonstrated that Orx2 agonists promote resilience, as well as anxiolytic and antidepressive behavior. In contrast, Orx2 antagonists or knockdown kindle anxious and pro-depressive behavior plus increase susceptibility. The results suggest that the Orx2 receptor may be a useful target for pharmacotherapies to treat anxiety and depression. Hypothalmic orexin/hypocretin (Orx) neurons in the lateral and dorsomedial perifornical region (LH-DMH/PeF) innervate broadly throughout the brain, and receive similar inputs. This wide distribution, as well as two Orx peptides (Orx A and Orx B ) and two Orx receptors (Orx 1 and Orx 2 ) allow for functionally related but distinctive behavioral outcomes, that include arousal, sleep-wake regulation, food seeking, metabolism, feeding, reward, addiction, and learning. These are all motivational functions, and tie the orexin systems to anxiety and depression as well. We present evidence, that for affective behavior, Orx 1 and Orx 2 receptors appear to have opposing functions. The majority of research on anxiety- and depression-related outcomes has focused on Orx 1 receptors, which appear to have primarily anxiogenic and pro-depressive actions. Although there is significant research suggesting contrary findings, the primary potential for pharmacotherapies linked to the Orx 1 receptor is via antagonists to block anxious and depressive behavior. Dual orexin receptor antagonists have been approved for treatment of sleep disorders, and are likely candidates for adaptation for affect disorder treatments. However, we present evidence here that demonstrates the Orx 2 receptors are anxiolytic and antidepressive. Using a new experimental pre-clinical model of anxious and depressive behavior stimulated by social stress and decision-making that produces two stable behavioral phenotypes, Escape/Resilient and Stay/Susceptible, we tested the effects of intracerebroventricular injections of Orx 2 agonist and antagonist drugs. Over ten behavioral measures, we have demonstrated that Orx 2 agonists promote resilience, as well as anxiolytic and antidepressive behavior. In contrast, Orx 2 antagonists or knockdown kindle anxious and pro-depressive behavior plus increase susceptibility. The results suggest that the Orx 2 receptor may be a useful target for pharmacotherapies to treat anxiety and depression. Hypothalmic orexin/hypocretin (Orx) neurons in the lateral and dorsomedial perifornical region (LH-DMH/PeF) innervate broadly throughout the brain, and receive similar inputs. This wide distribution, as well as two Orx peptides (Orx and Orx ) and two Orx receptors (Orx and Orx ) allow for functionally related but distinctive behavioral outcomes, that include arousal, sleep-wake regulation, food seeking, metabolism, feeding, reward, addiction, and learning. These are all motivational functions, and tie the orexin systems to anxiety and depression as well. We present evidence, that for affective behavior, Orx and Orx receptors appear to have opposing functions. The majority of research on anxiety- and depression-related outcomes has focused on Orx receptors, which appear to have primarily anxiogenic and pro-depressive actions. Although there is significant research suggesting contrary findings, the primary potential for pharmacotherapies linked to the Orx receptor is via antagonists to block anxious and depressive behavior. Dual orexin receptor antagonists have been approved for treatment of sleep disorders, and are likely candidates for adaptation for affect disorder treatments. However, we present evidence here that demonstrates the Orx receptors are anxiolytic and antidepressive. Using a new experimental pre-clinical model of anxious and depressive behavior stimulated by social stress and decision-making that produces two stable behavioral phenotypes, Escape/Resilient and Stay/Susceptible, we tested the effects of intracerebroventricular injections of Orx agonist and antagonist drugs. Over ten behavioral measures, we have demonstrated that Orx agonists promote resilience, as well as anxiolytic and antidepressive behavior. In contrast, Orx antagonists or knockdown kindle anxious and pro-depressive behavior plus increase susceptibility. The results suggest that the Orx receptor may be a useful target for pharmacotherapies to treat anxiety and depression. |
ArticleNumber | 146085 |
Author | Yaeger, Jazmine D.W. Arendt, David H. Summers, Cliff H. Summers, Tangi R. Staton, Clarissa D. |
AuthorAffiliation | c Veterans Affairs Research Service, Sioux Falls VA Health Care System, Sioux Falls, SD 57105 USA b Neuroscience Group, Division of Basic Biomedical Sciences, Sanford School of Medicine, University of South Dakota, Vermillion, SD 57069 USA a Department of Biology, University of South Dakota, Vermillion, SD 57069 USA |
AuthorAffiliation_xml | – name: b Neuroscience Group, Division of Basic Biomedical Sciences, Sanford School of Medicine, University of South Dakota, Vermillion, SD 57069 USA – name: a Department of Biology, University of South Dakota, Vermillion, SD 57069 USA – name: c Veterans Affairs Research Service, Sioux Falls VA Health Care System, Sioux Falls, SD 57105 USA |
Author_xml | – sequence: 1 givenname: Cliff H. surname: Summers fullname: Summers, Cliff H. email: cliff@usd.edu organization: Department of Biology, University of South Dakota, Vermillion, SD 57069 USA – sequence: 2 givenname: Jazmine D.W. surname: Yaeger fullname: Yaeger, Jazmine D.W. organization: Department of Biology, University of South Dakota, Vermillion, SD 57069 USA – sequence: 3 givenname: Clarissa D. surname: Staton fullname: Staton, Clarissa D. organization: Department of Biology, University of South Dakota, Vermillion, SD 57069 USA – sequence: 4 givenname: David H. surname: Arendt fullname: Arendt, David H. organization: Neuroscience Group, Division of Basic Biomedical Sciences, Sanford School of Medicine, University of South Dakota, Vermillion, SD 57069 USA – sequence: 5 givenname: Tangi R. surname: Summers fullname: Summers, Tangi R. organization: Department of Biology, University of South Dakota, Vermillion, SD 57069 USA |
BackLink | https://www.ncbi.nlm.nih.gov/pubmed/30590027$$D View this record in MEDLINE/PubMed |
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Keywords | Depression Anxiety Orexin 2 receptor Stress-Alternatives Model Social defeat Fear conditioning |
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Title | Orexin/hypocretin receptor modulation of anxiolytic and antidepressive responses during social stress and decision-making: Potential for therapy |
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