2017
DOI: 10.3389/fnins.2017.00658
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Targeting Adenosine Signaling in Parkinson's Disease: From Pharmacological to Non-pharmacological Approaches

Abstract: Parkinson's disease (PD) is one of the most prevalent neurodegenerative disease displaying negative impacts on both the health and social ability of patients and considerable economical costs. The classical anti-parkinsonian drugs based in dopaminergic replacement are the standard treatment, but several motor side effects emerge during long-term use. This mini-review presents the rationale to several efforts from pre-clinical and clinical studies using adenosine receptor antagonists as a non-dopaminergic thera… Show more

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Cited by 38 publications
(26 citation statements)
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“…Activation of the A 2A R by adenosine or appropriate agonists results in the inhibition of the D 2 R and, thus, in reduced dopamine binding [2,4,5]. Pharmacological inhibition of the A 2A R amplifies the D 2 R-dependent signaling cascade and improves motor symptoms [2,3,5,6]. Since the A 2A R modulates the dopamine binding affinity of the D 2 R, selective A 2A R antagonists have great potential as appropriate non-dopaminergic PD therapeutics [2,3,6].…”
Section: Introductionmentioning
confidence: 99%
See 1 more Smart Citation
“…Activation of the A 2A R by adenosine or appropriate agonists results in the inhibition of the D 2 R and, thus, in reduced dopamine binding [2,4,5]. Pharmacological inhibition of the A 2A R amplifies the D 2 R-dependent signaling cascade and improves motor symptoms [2,3,5,6]. Since the A 2A R modulates the dopamine binding affinity of the D 2 R, selective A 2A R antagonists have great potential as appropriate non-dopaminergic PD therapeutics [2,3,6].…”
Section: Introductionmentioning
confidence: 99%
“…Pharmacological inhibition of the A 2A R amplifies the D 2 R-dependent signaling cascade and improves motor symptoms [2,3,5,6]. Since the A 2A R modulates the dopamine binding affinity of the D 2 R, selective A 2A R antagonists have great potential as appropriate non-dopaminergic PD therapeutics [2,3,6]. In clinical phase II and III trials, the A 2A R antagonists istradefylline, preladenant, and tozadenant improved motor symptoms in PD patients [7][8][9].…”
Section: Introductionmentioning
confidence: 99%
“…Stroke NNC-21-0136 [123] Sleep CPA [155] Anxiety and depression MRS5474 [151] TRR469 [150] Cognition and memory ASP5854 [159] Alzheimer's disease Sleep CGS21680 [133] Anxiety and depression Istradefylline [208] Cognition and memory ASP5854 [159] Alzheimer's disease MSX-3 [212] Huntington's diseases ZM241385 [220] Parkinson's diseases Tozadenant/SYN115, DT1133, ZM241385, ST1535, and istradefylline [61] Preladenant, ASP5854, vipadenant (DC) [61] SCH900800, and BIIB014 [221] KW-6002 [134] Schizophrenia APEC, CGS21680, NECA, CV-1808, and DPMA [210] MSX-3, DMPX, SCH58261, and ZM241385 [210] Pain CGS21680 [155] Spongosine (DC) [204] Epilepsy ZM241385 [202] Drug addiction CGS21680 and NECA [215] A 3 AR Stroke IB-MECA [222] CI-IB-MECA [223] LJ-1251 [72] Epilepsy ANR235 [224] A 2B AR mediates anti-inflammatory effects in neutrophils by inhibiting adhesion to endothelial cells [23], preventing the production of TNF-α and IL-1β, as well as macrophage proliferation, and stimulating IL-10 secretion from macrophages [216]. Interestingly, A 2B AR has proinflammatory and anti-inflammatory actions in mouse bone marrow-derived mast cells (BMMCs) [225].…”
Section: Selective Full Agonist Antagonist/partial Agonist Allostericmentioning
confidence: 99%
“…Apart from the elevated oxidative stress, activated microglial cells and the subsequent release of the inflammatory mediators have also been shown to play a prominent role in the execution of neuronal cell loss in PD [141]. The pharmacological inhibition of A2AR activates dopamine receptor-2, suppresses neuroinflammation by regulating the level of dopamine, and relieves the symptoms of PD [142]. The elevated oxidative stress and reduced level of dopamine due to the activation of A2AR in the substantia nigra and striatum of PD patients induce overall neuroinflammation and PD symptoms [143].…”
Section: Pathophysiology Of Parkinson's Disease (Pd)mentioning
confidence: 99%