Isoquinoline and quinazoline urea analogues as antagonists for the human adenosine A(3) receptor

Isoquinoline and quinazoline urea analogues as antagonists for the human adenosine A(3) receptor

Isoquinoline and quinazoline urea derivatives were found to bind to human adenosine A(3) receptors. Series of N-phenyl-N'-quinazolin-4-ylurea derivatives and N-phenyl-N'-isoquinolin-1-ylurea derivatives were synthesized and tested in radioligand binding assays on their adenosine receptor a...

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Veröffentlicht in:Journal of medicinal chemistry 2000-06, Vol.43 (11), p.2227-2238
Hauptverfasser: van Muijlwijk-Koezen, J E, Timmerman, H, van der Goot, H, Menge, W M, Frijtag Von Drabbe Künzel, J, de Groote, M, IJzerman, A P
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Binding Sites
Cells, Cultured
Cerebral Cortex - cytology
CHO Cells
Cricetinae
Humans
Isoquinolines - chemical synthesis
Isoquinolines - chemistry
Isoquinolines - pharmacology
Models, Molecular
Purinergic P1 Receptor Antagonists
Quinazolines - chemical synthesis
Quinazolines - chemistry
Quinazolines - pharmacology
Rats
Receptor, Adenosine A3
Receptors, Purinergic P1 - metabolism
Structure-Activity Relationship
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Zusammenfassung:Isoquinoline and quinazoline urea derivatives were found to bind to human adenosine A(3) receptors. Series of N-phenyl-N'-quinazolin-4-ylurea derivatives and N-phenyl-N'-isoquinolin-1-ylurea derivatives were synthesized and tested in radioligand binding assays on their adenosine receptor affinities. A structure-affinity analysis indicated that on the 2-position of the quinazoline ring or the equivalent 3-position of the isoquinoline ring a phenyl or heteroaryl substituent increased the adenosine A(3) receptor affinity in comparison to unsubstituted or aliphatic derivatives. Furthermore, the structure-affinity relationship of substituted phenylurea analogues was investigated. Substituents such as electron-withdrawing or electron-donating groups were introduced at different positions of the benzene ring to probe electronic and positional effects of substitution. Substitution on the 3- or 4-position of the phenyl ring decreased the adenosine A(3) receptor affinity. Substitution at position 2 with an electron-donating substituent, such as methyl or methoxy, increased human adenosine A(3) receptor affinity, whereas substitution on the 2-position with an electron-withdrawing substituent did not influence affinity. Combination of the optimal substituents in the two series had an additive effect, which led to the potent human adenosine A(3) receptor antagonist N-(2-methoxyphenyl)-N'-(2-(3-pyridyl)quinazolin-4-yl)urea (VUF5574, 10a) showing a K(i) value of 4 nM and being at least 2500-fold selective vs A(1) and A(2A) receptors. Compound 10a competitively antagonized the effect of an agonist in a functional A(3) receptor assay, i.e., inhibition of cAMP production in cells expressing the human adenosine A(3) receptor; a pA(2) value of 8.1 was derived from a Schild plot. In conclusion, compound 10a is a potent and selective human adenosine A(3) receptor antagonist and might be a useful tool in further characterization of the human A(3) receptor.
ISSN:0022-2623
DOI:10.1021/jm000002u