Adenosine A<sub>2A</sub>receptors regulate the activity of sleep regulatory GABAergic neurons in the preoptic hypothalamus

Kumar, Sunil; Rai, Seema; Hsieh, Kung-Chiao; McGinty, Dennis; Alam, Md. Noor; Szymusiak, Ronald

doi:10.1152/ajpregu.00402.2012

Cited by 42 publications

(31 citation statements)

References 57 publications

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“…In A2A receptor knockout mice, caffeine (an A1 and A2A receptor antagonist) failed to promote wakefulness 106 and deprivation-induced NREM sleep rebound was reduced 107 . In vivo application of an A2A receptor agonist increased NREM sleep and enhanced c-Fos expression in the VLPO and MnPO 108,109 , whereas application of an antagonist in the VLPO attenuated sleep-deprivation-induced increases in the firing rates of sleep-active neurons 110 . In brain slices, VLPO neurons were shown to be activated directly or indirectly via A2A receptors 111,112 .…”

Section: Nrem Wake Remmentioning

confidence: 96%

Circuit-based interrogation of sleep control

Weber

Dan

2016

Nature

308

246

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Sleep is a fundamental biological process observed widely in the animal kingdom, but the neural circuits generating sleep remain poorly understood. Understanding the brain mechanisms controlling sleep requires the identification of key neurons in the control circuits and mapping of their synaptic connections. Technical innovations over the past decade have greatly facilitated dissection of the sleep circuits. This has set the stage for understanding how a variety of environmental and physiological factors influence sleep. The ability to initiate and terminate sleep on command will also help us to elucidate its functions within and beyond the brain.

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Section: Nrem Wake Remmentioning

confidence: 96%

Circuit-based interrogation of sleep control

Weber

Dan

2016

Nature

308

246

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“…Similarly, A 2A AR and A 1 AR of hippocampal CA1 have the opposite effect in spreading piriform cortex kindled seizures, in which A 2A AR tends to have a convulsive effect [201]. In fact, the A 2A AR antagonist ZM241385 had a potent anticonvulsant profile with few adverse effects [202] and suppressed subsequent recovery sleep [203]. Concerning sleep and arousal, the A 2A AR agonist CGS21680 promoted both rapid eye movement (REM) and NREM sleep [133].…”

Section: A 2a Ar In the Cnsmentioning

confidence: 99%

Focusing on Adenosine Receptors as a Potential Targeted Therapy in Human Diseases

Effendi

Nagano

Kobayashi

et al. 2020

Cells

102

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Adenosine is involved in a range of physiological and pathological effects through membrane-bound receptors linked to G proteins. There are four subtypes of adenosine receptors, described as A1AR, A2AAR, A2BAR, and A3AR, which are the center of cAMP signal pathway-based drug development. Several types of agonists, partial agonists or antagonists, and allosteric substances have been synthesized from these receptors as new therapeutic drug candidates. Research efforts surrounding A1AR and A2AAR are perhaps the most enticing because of their concentration and affinity; however, as a consequence of distressing conditions, both A2BAR and A3AR levels might accumulate. This review focuses on the biological features of each adenosine receptor as the basis of ligand production and describes clinical studies of adenosine receptor-associated pharmaceuticals in human diseases.

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“…5 Additionally, the VLPO and MnPN have been shown as sites of sensitivity to adenosine, an important mediator of homeostatic sleep pressure. 151 Further exploration of these molecular and neurological pathways could provide greater insight into precisely how E2 is affecting sleep need and behavior.…”

Section: Sleepmentioning

confidence: 99%

Estradiol Action at the Median Preoptic Nucleus is Necessary and Sufficient for Sleep Suppression in Female Rats

Smith

Cusmano

Phillips

et al. 2020

Preprint

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To further our understanding of how gonadal steroids impact sleep biology, we sought to address the mechanism by which proestrus levels of cycling ovarian steroids, particularly estradiol (E2), suppress sleep in female rats. We showed that steroid replacement of proestrus levels of E2 to ovariectomized female rats, suppressed sleep to similar levels as those reported by endogenous ovarian hormones. We further showed that this suppression is due to the high levels of E2 alone, and that progesterone did not have a significant impact on sleep behavior. We found that E2 action within the Median Preoptic Nucleus (MnPN), which contains estrogen receptors (ERs), is necessary for this effect; antagonism of ERs in the MnPN attenuated the E2-mediated suppression of both non-Rapid Eye Movement (NREM) and Rapid Eye Movement (REM) sleep. Finally, we found E2 action at the MnPN is also sufficient for sleep suppression, as direct infusion of E2 into the MnPN suppressed sleep. Based on our findings, we predict proestrus levels of E2 alone, acting at the MnPN, mediate sex-hormone driven suppression of sleep in female rats.

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Adenosine A_2Areceptors regulate the activity of sleep regulatory GABAergic neurons in the preoptic hypothalamus

Cited by 42 publications

References 57 publications

Circuit-based interrogation of sleep control

Circuit-based interrogation of sleep control

Focusing on Adenosine Receptors as a Potential Targeted Therapy in Human Diseases

Estradiol Action at the Median Preoptic Nucleus is Necessary and Sufficient for Sleep Suppression in Female Rats

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Adenosine A2Areceptors regulate the activity of sleep regulatory GABAergic neurons in the preoptic hypothalamus

Cited by 42 publications

References 57 publications

Circuit-based interrogation of sleep control

Circuit-based interrogation of sleep control

Focusing on Adenosine Receptors as a Potential Targeted Therapy in Human Diseases

Estradiol Action at the Median Preoptic Nucleus is Necessary and Sufficient for Sleep Suppression in Female Rats

Contact Info

Product

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Adenosine A_2Areceptors regulate the activity of sleep regulatory GABAergic neurons in the preoptic hypothalamus