Selectivity is species-dependent: Characterization of standard agonists and antagonists at human, rat, and mouse adenosine receptors

Alnouri, Mohamad Wessam; Jepards, Stephan; Casari, Alessandro; Schiedel, Anke C.; Hinz, Sonja; Müller, Christian

doi:10.1007/s11302-015-9460-9

Cited by 117 publications

(157 citation statements)

References 79 publications

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“…As shown in Figure 2a, the antiproliferative effect of adenosine was primarily mediated by A 2B AR, because it was abrogated by MRS. The opposing effects of the nonselective agonist NECA and the endogenous ligand adenosine are probably due to the higher affinity of NECA for the A 2A AR (see Supplementary Table S1) (Alnouri et al, 2015), thus explaining the previously reported divergences regarding the effect of AR activation on NHEK proliferation.…”

Section: Resultsmentioning

confidence: 93%

Adenosine A2A and A2B Receptors Differentially Modulate Keratinocyte Proliferation: Possible Deregulation in Psoriatic Epidermis

Andrés

Terencio

Arasa

et al. 2017

Journal of Investigative Dermatology

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Adenosine is a potent regulator of inflammation and immunity, but the role of adenosine receptors in keratinocytes remains controversial. We determined that in addition to A 2B receptors, human epidermal keratinocytes also express A 2A receptors, although to a lower extent. Through the use of selective adenosine receptor agonists and antagonists, we showed that physiological concentrations of adenosine activate A 2B receptors in normal human keratinocytes, inducing cell cycle arrest through the increase of intracellular calcium but not through cAMP signaling. In contrast, the selective activation of A 2A receptors by CGS-21680 induces keratinocyte proliferation via p38emitogen-activated protein kinase activation. Adenosine and selective A 2A and A 2B agonists presented anti-inflammatory profiles independent of adenosine receptors but mediated by membrane phosphatase activation. Finally, keratinocyte exposure to diverse inflammatory cytokines altered adenosine receptor expression by reducing A 2B and increasing A 2A , a pattern also observed in psoriatic epidermis. Because increased epidermal turnover and inflammatory response are characteristics of psoriatic disease, further studies are needed to assess the role and consequences of the altered adenosine receptor expression in lesional and nonlesional psoriatic keratinocytes.

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Section: Resultsmentioning

confidence: 93%

Adenosine A2A and A2B Receptors Differentially Modulate Keratinocyte Proliferation: Possible Deregulation in Psoriatic Epidermis

Andrés

Terencio

Arasa

et al. 2017

Journal of Investigative Dermatology

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“…Notably, preischemic exposure to a selective A1R agonist (CCPA) essentially mimicked preconditioning in the liver through a mitochondrial adaptation similar to ischemic preconditioning. The single used dose of CCPA is expected to engage A1R since CCPA is 32 times selective for A1R versus A3 receptors in rats [61]. The possible involvement of A3 receptors in the effects of CCPA cannot be fully ruled out, although the role of A3 receptors in the preconditioning process is far from clear, with opposite effects in different tissues [62,63].…”

Section: Discussionmentioning

confidence: 99%

Adenosine receptors: regulatory players in the preservation of mitochondrial function induced by ischemic preconditioning of rat liver

Duarte

Amorim

Varela

et al. 2016

Purinergic Signalling

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Although adenosine A 1 receptors (A1R) have been associated to ischemic preconditioning (IPC), direct evidence for their ability to preserve mitochondrial function upon hepatic preconditioning is still missing and could represent a novel strategy to boost the quality of liver transplants. We tested if the A1R antagonist 8-cyclopentyl-1,3-dipropylxanthine (DPCPX) prevented IPC in the liver and if the A1R agonist 2-chloro-N 6 -cyclopentyladenosine (CCPA) might afford a pharmacological preconditioning. Livers underwent a 120 min of 70% warm ischemia and 16 h of reperfusion (I/R), and the IPC group underwent a 5-min ischemic episode followed by a 10-min period of reperfusion before I/R. DPCPX or CCPA was administered intraperitoneally 2 h before IPC or I/R. The control of mitochondrial function emerged as the central element affected by IPC and controlled by endogenous A1R activation. Thus, livers from IPC-or CCPA-treated rats displayed an improved oxidative phosphorylation with higher state 3 respiratory rate, higher respiratory control ratio, increased ATP content, and decreased lag phase. IPC and CCPA also prevented the I/Rinduced susceptibility to calcium-induced mitochondrial permeability transition, the rate of reactive oxygen species (ROS) generation, and the decreased mitochondrial content of phospho-Ser 9 GSK-3β. DPCPX abrogated these effects of IPC. These implicate the control of GSK-3β activity by Aktmediated Ser 9 -GSK-3β phosphorylation preserving the efficiency of oxidative phosphorylation and ROS-mediated cell death in the ability of A1R activation to mimic IPC in the liver. In conclusion, the parallel between IPC and A1R-mediated preconditioning also paves the way to consider a putative therapeutic use of the later in liver transplants.

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“…Cl-ENBA (number 3 in Figure 2) is a more selective A 1 AR agonist for in vivo use than 1 and 2 (Carlin et al, 2017). CGS21680 (not shown) is an A 2A AR agonist in rat, but has substantial human (h) A 3 AR affinity (Alnouri et al, 2015). Potent A 2A AR agonist ATL-313 5 attenuates colitis in mice and reduces pro-inflammatory cytokines (Longhi et al, 2017).…”

Section: Medicinal Chemistry Of Purinergic Receptorsmentioning

confidence: 99%

Purinergic drug targets for gastrointestinal disorders

Burnstock

Christofi

2017

Current Opinion in Pharmacology

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Purinergic receptors are implicated in the pathogenesis of gastrointestinal disorders and are being explored as potential therapeutic targets. Gut inflammation releases ATP that acts on neuron, glial, epithelial and immune cells. Purinergic signalling in glia and neurons is implicated in enteric neuropathies. Inflammation activates glia to increase ATP release and alter purinergic signalling. ATP release causes neuronal death and gut motor dysfunction in colitis via a P2X7-dependent neural-glial pathway and a glial purinergic-connexin-43 pathway. The latter pathway also mediates morphine-induced constipation and gut inflammation that may differ from opioid-induced constipation (OIC). P2X7R antagonists are protective in inflammatory bowel disease (IBD) models, where as AZD9056 is questionable in CD, but is potentially beneficial for chronic abdominal pain. Drug targets under investigation for IBD, IBS and motility disorders include P2X7R, P2X3R, P2Y2R, A2A/A2BAR, enzymes and transporters.

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Selectivity is species-dependent: Characterization of standard agonists and antagonists at human, rat, and mouse adenosine receptors

Cited by 117 publications

References 79 publications

Adenosine A2A and A2B Receptors Differentially Modulate Keratinocyte Proliferation: Possible Deregulation in Psoriatic Epidermis

Adenosine A2A and A2B Receptors Differentially Modulate Keratinocyte Proliferation: Possible Deregulation in Psoriatic Epidermis

Adenosine receptors: regulatory players in the preservation of mitochondrial function induced by ischemic preconditioning of rat liver

Purinergic drug targets for gastrointestinal disorders

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