2006
DOI: 10.2174/092986706775476052
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P2 Receptors Activated by Uracil Nucleotides - An Update

Abstract: Pyrimidine nucleotides, including UTP, UDP and UDP-glucose, are important signaling molecules which activate G protein-coupled membrane receptors (GPCRs) of the P2Y family. Four distinct pyrimidine nucleotide-sensitive P2Y receptor subtypes have been cloned, P2Y2, P2Y4, P2Y6 and P2Y14. P2Y2 and P2Y4 receptors are activated by UTP (the P2Y2, and the rat but not the human P2Y4 receptor are also activated by ATP), the P2Y6 receptor is activated by UDP, and the P2Y14 receptor by UDP-glucose. Furthermore, non-P2Y G… Show more

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Cited by 134 publications
(185 citation statements)
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References 182 publications
(302 reference statements)
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“…Suramin and RB-2 are potent inhibitors of all P2Y subtypes expressed in HUVECs (P2Y 1 , P2Y 2 , P2Y 4 , P2Y 6 and P2Y 11 ) with the exception of P2Y 4 that is insensitive to suramin (Brunschweiger and Muller, 2006). To further define the P2Y receptor involved, the selective antagonists of P2Y 1 , P2Y 6 and P2Y 11 (MRS2500, MRS2578 and NF157, respectively) were tested on LPS-induced neutrophil TEM.…”
Section: Endothelial P2y 2 Receptor Regulates Lps-induced Neutrophil Temmentioning
confidence: 99%
“…Suramin and RB-2 are potent inhibitors of all P2Y subtypes expressed in HUVECs (P2Y 1 , P2Y 2 , P2Y 4 , P2Y 6 and P2Y 11 ) with the exception of P2Y 4 that is insensitive to suramin (Brunschweiger and Muller, 2006). To further define the P2Y receptor involved, the selective antagonists of P2Y 1 , P2Y 6 and P2Y 11 (MRS2500, MRS2578 and NF157, respectively) were tested on LPS-induced neutrophil TEM.…”
Section: Endothelial P2y 2 Receptor Regulates Lps-induced Neutrophil Temmentioning
confidence: 99%
“…One of the most selective antagonists described to date is the thiouracil derivative 5- Fig. 1) [26,27], which has been developed by structural modifications of the physiological agonist UTP [28]. Replacement of the ribose triphosphate moiety and derivatization of the uracil ring in UTP (1b) eliminated agonist properties and improved potency and pharmacokinetic properties, respectively [28].…”
Section: Introductionmentioning
confidence: 99%
“…Purinoceptors Two families of purinergic receptors known as P1 and P2 (for ADO and ATP/ADP, respectively) were postulated almost 40 years ago (in 1978); however, it has been proposed the existence of another subfamily of receptors activated by the nucleobase adenine named P0 receptors [18].…”
mentioning
confidence: 99%
“…In addition, ADORA1 activation can directly activate K + channels and inhibit Q-, P-and N-type Ca 2+ channels [24]. The proposed P0 receptors are also GPCR, the first one was cloned in 2002 from rat tissue [25], recently has been cloned from, mouse and guinea pig [26,27], P0 receptor are mainly coupled to Gi protein and in consequence to the inhibition of adenylate cyclase [18,25,26], and are expressed in lung, ovaries, kidneys, and nervous system [25].…”
mentioning
confidence: 99%