Agonist Action of Adenosine Triphosphates at the Human P2Y1 Receptor

Overview

Journal Mol Pharmacol

Specialties Molecular Biology
Pharmacology

Date 1998 Dec 18

PMID 9855642

Citations 57

Authors

R K Palmer

J L Boyer

J B Schachter

R A Nicholas

T K Harden

Affiliations

Soon will be listed here.

Abstract

The agonist selectivity for adenosine di- and triphosphates was determined for the human P2Y1 receptor stably expressed in human 1321N1 astrocytoma cells and was studied under conditions in which nucleotide metabolism was both minimized and assessed. Cells were grown at low density on glass coverslips, encased in a flow-through chamber, and continuously superfused with medium, and Ca2+ responses to nucleotides were quantified. Superfusion with high performance liquid chromatographically purified ADP, ATP, 2-methylthio-ADP, and 2-methylthio-ATP resulted in rapid Ca2+ responses, with EC50 values of 10 +/- 5, 304 +/- 51, 2 +/- 1, and 116 +/- 50 nM, respectively. Similar peak responses were observed with maximal concentrations of these four agonists and with the hydrolysis-resistant adenine nucleoside triphosphate adenosine-5'-O-(3-thiotriphosphate). No conversion of [3H]ATP to [3H]ADP occurred under these conditions. Similar full agonist activities of ATP, 2-methylthio-ATP, and ADP were observed in human embryonic kidney 293 cells, which natively express the P2Y1 receptor. In contrast to these results, Leon et al. [FEBS Lett 403:26-30 (1997)] and Hechler et al. [Mol Pharmacol 53:727-733 (1998)] recently reported that, whereas ADP and 2-methylthio-ADP were agonists, ATP and 2-methylthio-ATP were weak antagonists in studies of the human P2Y1 receptor expressed in human Jurkat cells. To assess whether differences in the degree of receptor reserve might explain this discrepancy of results, P2Y1 receptor-expressing 1321N1 cells were incubated for 24 hr with adenosine-5'-O-(2-thiodiphosphate), with the goal of down-regulating the level of functional receptors. Pretreatment with adenosine-5'-O-(2-thiodiphosphate) resulted in a 10-fold rightward shift in the concentration-effect curve for ADP; in contrast, the agonist activity of ATP was completely abolished. Taken together, our results indicate that adenosine di- and triphosphates are agonists at the human P2Y1 receptor. However, the intrinsic efficacy of ATP is less than that of ADP, and the capacity of ATP to activate second messenger responses through this receptor apparently depends on the degree of P2Y1 receptor reserve.

Citing Articles

G-Protein-Coupled Receptor (GPCR) Signaling and Pharmacology in Metabolism: Physiology, Mechanisms, and Therapeutic Potential.

Cho Y, Kim S, Kim P, Jo M, Park S, Choi Y Biomolecules. 2025; 15(2).

PMID: 40001594 PMC: 11852853. DOI: 10.3390/biom15020291.

How selective antagonists and genetic modification have helped characterise the expression and functions of vascular P2Y receptors.

Dales M, Drummond R, Kennedy C Purinergic Signal. 2024; .

PMID: 38740733 DOI: 10.1007/s11302-024-10016-z.

Systematic P2Y receptor survey identifies P2Y11 as modulator of immune responses and virus replication in macrophages.

Andersen L, Huang Y, Urban C, Oubraham L, Winheim E, Stafford C EMBO J. 2023; 42(23):e113279.

PMID: 37881155 PMC: 10690470. DOI: 10.15252/embj.2022113279.

Migraine signaling pathways: purine metabolites that regulate migraine and predispose migraineurs to headache.

Biringer R Mol Cell Biochem. 2023; 478(12):2813-2848.

PMID: 36947357 DOI: 10.1007/s11010-023-04701-7.

Characterisation of P2Y receptor subtypes mediating vasodilation and vasoconstriction of rat pulmonary artery using selective antagonists.

Dales M, Mitchell C, Gurney A, Drummond R, Kennedy C Purinergic Signal. 2022; 18(4):515-528.

PMID: 36018534 PMC: 9832182. DOI: 10.1007/s11302-022-09895-x.