Endogenous oxytocin inhibits hypothalamic corticotrophin‐releasing hormone neurones following acute hypernatraemia

Pati, Dipanwita; Harden, Scott W; Sheng, Wanhui; Kelly, Kyle B.; Kloet, Annette D. de; Krause, Eric G.; Frazier, Charles J.

doi:10.1111/jne.12839

Cited by 20 publications

(16 citation statements)

References 49 publications

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“…P. Li and Pan, 2005). Crosstalk among the neuronal phenotypes residing within the PVN may also contribute to the increased blood pressure that accompanies activation of AT1aR(s), and recent reports demonstrate paracrine signaling within the PVN resulting from dendritic release of neuropeptides (Son et al, 2013;Stern, 2015;Brown et al, 2020;Pati et al, 2020). Finally, it is likely that neurons in the MnPO/OVLT that express AT1aRs make connections beyond the PVN that mediate the autonomic and behavioral effects of Ang-II.…”

Section: Discussionmentioning

confidence: 99%

“…While completing these studies, we also tested for optogenetic stimulation evoked EPSCs in parvocellular PVN neurons (n = 11) that lacked and I A but exhibited a low threshold spike, a common characteristic of preautonomic neurons with direct projections to the RVLM that control sympathetic outflow to cardiovascular tissues (Luther and Tasker, 2000;Luther et al, 2002). We also recorded from an additional 18 PVN neurons that lacked both I A and low threshold spike, a phenotype observed in corticotrophin-releasing hormone neurosecretory neurons (Wamsteeker Cusulin et Pati et al, 2020). Notably, none of these 29 neurons exhibited an EPSC in response to blue light.…”

Section: Optogenetic Stimulation Of At1ar-containing Neurons Of the Mnpo/ovlt Potently Influences Sbp And Fluid Intakementioning

confidence: 99%

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An Angiotensin-Responsive Connection from the Lamina Terminalis to the Paraventricular Nucleus of the Hypothalamus Evokes Vasopressin Secretion to Increase Blood Pressure in Mice

et al. 2020

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Blood pressure is controlled by endocrine, autonomic, and behavioral responses that maintain blood volume and perfusion pressure at levels optimal for survival. Although it is clear that central angiotensin type 1a receptors (AT1aR; encoded by the Agtr1a gene) influence these processes, the neuronal circuits mediating these effects are incompletely understood. The present studies characterize the structure and function of AT1aR neurons in the lamina terminalis (containing the median preoptic nucleus and organum vasculosum of the lamina terminalis), thereby evaluating their roles in blood pressure control. Using male Agtr1a-Cre mice, neuroanatomical studies reveal that AT1aR neurons in the area are largely glutamatergic and send projections to the paraventricular nucleus of the hypothalamus (PVN) that appear to synapse onto vasopressin-synthesizing neurons. To evaluate the functionality of these lamina terminalis AT1aR neurons, we virally delivered light-sensitive opsins and then optogenetically excited or inhibited the neurons while evaluating cardiovascular parameters or fluid intake. Optogenetic excitation robustly elevated blood pressure, water intake, and sodium intake, while optogenetic inhibition produced the opposite effects. Intriguingly, optogenetic excitation of these AT1aR neurons of the lamina terminalis also resulted in Fos induction in vasopressin neurons within the PVN and supraoptic nucleus. Further, within the PVN, selective optogenetic stimulation of afferents that arise from these lamina terminalis AT1aR neurons induced glutamate release onto magnocellular neurons and was sufficient to increase blood pressure. These cardiovascular effects were attenuated by systemic pretreatment with a vasopressin-1a-receptor antagonist. Collectively, these data indicate that excitation of lamina terminalis AT1aR neurons induces neuroendocrine and behavioral responses that increase blood pressure.

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Section: Discussionmentioning

confidence: 99%

Section: Optogenetic Stimulation Of At1ar-containing Neurons Of the Mnpo/ovlt Potently Influences Sbp And Fluid Intakementioning

confidence: 99%

An Angiotensin-Responsive Connection from the Lamina Terminalis to the Paraventricular Nucleus of the Hypothalamus Evokes Vasopressin Secretion to Increase Blood Pressure in Mice

et al. 2020

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“…Oxytocin has also been reported to decrease the activity of corticotrophin-releasing hormone (CRH) neurons in the PVN following stress in voles [ 118 ]. The oxytocin receptor is expressed in CRH neurons of the PVN, and oxytocin released by acute salt loading has been suggested to tonically inhibit PVN CRH neurons via the oxytocin receptor [ 119 ].…”

Section: Stress Responses and Oxytocinmentioning

confidence: 99%

Roles of Oxytocin in Stress Responses, Allostasis and Resilience

Takayanagi

Onaka

2021

IJMS

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Oxytocin has been revealed to work for anxiety suppression and anti-stress as well as for psychosocial behavior and reproductive functions. Oxytocin neurons are activated by various stressful stimuli. The oxytocin receptor is widely distributed within the brain, and oxytocin that is released or diffused affects behavioral and neuroendocrine stress responses. On the other hand, there has been an increasing number of reports on the role of oxytocin in allostasis and resilience. It has been shown that oxytocin maintains homeostasis, shifts the set point for adaptation to a changing environment (allostasis) and contributes to recovery from the shifted set point by inducing active coping responses to stressful stimuli (resilience). Recent studies have suggested that oxytocin is also involved in stress-related disorders, and it has been shown in clinical trials that oxytocin provides therapeutic benefits for patients diagnosed with stress-related disorders. This review includes the latest information on the role of oxytocin in stress responses and adaptation.

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“…It is complicated by the fact that there are both magnocellular and parvocellular hypothalamic OT synthesizing neurons 67 (OT-MCNs, OT-PCNs), and by the fact that OT-MCNs can release peptide both from their axon terminals and from their dendrites. The current study focuses on dendritic physiology of PVN OT-MCNs because 1) OT-MCNs substantially outnumber OT-PCNs (Althammer and Grinevich, 2017), 2) most axons of OT-MCNs project through the median eminence to the posterior pituitary 71 where activity (action potential) dependent release into the vasculature increases peripheral (and 72 not central) OT concentration (Guzek, 1987;Robinson et al, 1989;Falke, 1991), 3) a large portion of 73 OT available for release into the CNS exists in dendritic rather than axonal vesicles that are subject 74 to activity, and calcium, dependent exocytosis (Pow and Morris, 1989;Ludwig et al, 2002;Ludwig 75 and Leng, 2006), 4) such exocytosis supports functionally important peptide mediated paracrine 76 signaling within the hypothalamus (Son et al, 2013;Smith et al, 2015;Pati et al, 2020), and 5) 77 likely also drives volume transmission to increase functional activation of OTRs in a variety of extrahypothalamic cortical and limbic areas (Veening et al, 2010;Fuxe et al, 2012;Ludwig and 79 Stern, 2015;Brown et al, 2020). Indeed, this mechanism seems likely to work in concert with 80 limited/targeted release from centrally projecting axon collaterals of OT neurons, as has been 81…”

Section: Introductionmentioning

confidence: 99%

Dendritic osmosensors modulate activity-induced calcium influx in oxytocinergic magnocellular neurons of the mouse PVN

Sheng

Harden

Tan

et al. 2021

eLife

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Hypothalamic oxytocinergic magnocellular neurons have a fascinating ability to release peptide from both their axon terminals and from their dendrites. Existing data indicates that the relationship between somatic activity and dendritic release is not constant, but the mechanisms through which this relationship can be modulated are not completely understood. Here we use a combination of electrical and optical recording techniques to quantify activity-induced calcium influx in proximal vs. distal dendrites of oxytocinergic magnocellular neurons located in the paraventricular nucleus of the hypothalamus (OT-MCNs). Results reveal that the dendrites of OT-MCNs are weak conductors of somatic voltage changes, however activity-induced dendritic calcium influx can be robustly regulated by both osmosensitive and non-osmosensitive ion channels located along the dendritic membrane. Overall, this study reveals that dendritic conductivity is a dynamic and endogenously regulated feature of OT-MCNs that is likely to have substantial functional impact on central oxytocin release.

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Endogenous oxytocin inhibits hypothalamic corticotrophin‐releasing hormone neurones following acute hypernatraemia

Cited by 20 publications

References 49 publications

An Angiotensin-Responsive Connection from the Lamina Terminalis to the Paraventricular Nucleus of the Hypothalamus Evokes Vasopressin Secretion to Increase Blood Pressure in Mice

An Angiotensin-Responsive Connection from the Lamina Terminalis to the Paraventricular Nucleus of the Hypothalamus Evokes Vasopressin Secretion to Increase Blood Pressure in Mice

Roles of Oxytocin in Stress Responses, Allostasis and Resilience

Dendritic osmosensors modulate activity-induced calcium influx in oxytocinergic magnocellular neurons of the mouse PVN

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