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Adenosine is a ubiquitous homeostatic substance released fro
Adenosine is a ubiquitous homeostatic substance released from most cells, including neurons and glias. Endogenous adenosine acts at four principal G-protein-associated receptor subtypes: A1, A2a, A2b and A3 (Ralevic and Burnstock, 1998). The stimulation of adenosine receptors by extracellular adenosine and the adenosine receptor activation following modest increases in extracellular adenosine concentrations play important roles in the modulation of many AL 8810 functions, most notably the regulation of sleep and arousal, locomotion, anxiety, cognition and memory (Hasko et al., 2005). All adenosine receptor subtypes are expressed in the brain; however, their expression is localized in specific sites and cell types. The A1 adenosine receptor is highly expressed in the brain cortex, cerebellum, and hippocampus. The A2a adenosine receptor is highly expressed in the neurons and olfactory bulb. The A2b adenosine receptor has low levels of expression in the brain. Meanwhile, the A3 adenosine receptor appears to have intermediate levels of expression in the human cerebellum and hippocampus and low levels in most of the brain (Ribeiro et al., 2002). Adenosine acts in parallel as a neuromodulator and as a homeostatic modulator in the central nervous system (Cunha, 2001). Adenosine is apparently involved in many functions with consequences in the pathology of the nervous system. Adenosine and its receptors play important roles in a number of brain disorders, such as ischemia, epilepsy, and Alzheimer’s disease (AD) (Gomes et al., 2011, Sebastiao and Ribeiro, 2009).
In this study, we demonstrated that activation of adenosine receptors affects the proliferation of NPCs using a 96-well-based screening system. The A1 adenosine receptor agonist cyclopentyladenosine (CPA) and A2a adenosine receptor agonist CGS-21680 were able to increase proliferation of NPCs. The A1 adenosine receptor agonist-induced cell proliferation was attenuated by A1 adenosine receptor antagonist DPCPA. Accordingly, the A2a adenosine receptor agonist-induced cell proliferation was attenuated by A2a adenosine receptor antagonist SCH-58261. Further study indicated that CPA and CGS-21680 also induced phosphorylation of ERK and Akt. In addition, CPA-induced or CGS-21680-induced cell proliferation was inhibited by ERK and Akt inhibitors. These results suggested that the activation of A1 and A2a adenosine receptors stimulated the proliferation of NPCs via the ERK and Akt signaling pathways.
Results
Discussion
Adenosine is a ubiquitous homeostatic substance released from most cells, including neurons and glias. In this study, A1 adenosine receptor showed high expression in NPCs isolated from the cerebral cortex, while A2a and A2b adenosine receptors had low expression in NPCs (Fig. 3A-B). Stimulation of adenosine receptors by extracellular adenosine and adenosine receptor activation following modest increases in extracellular adenosine concentrations play important roles in the modulation of many brain functions, most notably the regulation of sleep and arousal, locomotion, anxiety, cognition and memory (Ribeiro et al., 2002). Many studies using adenosine receptor agonists and antagonists have also shown them to provide a neuroprotective effect in various models of neurodegenerative diseases such as stroke and Alzheimer’s disease through the reduction of excitatory neurotransmitter release, apoptosis and inflammatory responses (Rivera-Oliver and Diaz-Rios, 2014). A recent study found that the activation of A1 adenosine receptor provided neuroprotection after transient middle cerebral artery occlusion and that blocking this receptor with DPCPX eliminated the neuroprotective effects (Hu et al., 2012). In other studies, the activation of the A2a adenosine receptor has also been shown to have a potential therapeutic effect against stroke. The A2a adenosine receptor is highly sensitive to neuromodulation after brain insults and related inflammatory responses (Rivera-Oliver and Diaz-Rios, 2014). A2a adenosine receptor agonists have been found to be protective in the global ischemia model in the gerbil, and an A2a adenosine receptor knockout neonatal mouse model showed aggravated hypoxic ischemic injury in comparison to wild-type mice (Aden et al., 2003, Von Lubitz et al., 1995).