8-substituted adenosine and theophylline-7-riboside analogues as potential partial agonists for the adenosine A1 receptor

A series of 8-substituted adenosine and theophylline-7-riboside analogues (28 and 9 compounds, respectively) was tested on adenosine A1 and A2A receptors as an extensive exploration of the adenosine C8-region. Alkylamino substituents at the 8-position cause an affinity decrease for adenosine analogu...

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Veröffentlicht in:	European journal of pharmacology 1995-08, Vol.290 (3), p.189-199
Hauptverfasser:	Van der Wenden, E M, Hartog-Witte, H R, Roelen, H C, von Frijtag Drabbe Künzel, J K, Pirovano, I M, Mathôt, R A, Danhof, M, Van Aerschot, A, Lidaks, M J, IJzerman, A P
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Sprache:	eng
Schlagworte:	Adenosine - analogs & derivatives Adenosine - chemistry Adenosine - pharmacology Adenylyl Cyclases - metabolism Animals Cells, Cultured Heart Rate - drug effects In Vitro Techniques Kinetics Purinergic P1 Receptor Agonists Rats Theophylline - analogs & derivatives Theophylline - chemistry Theophylline - pharmacology Xanthines - pharmacology
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container_title	European journal of pharmacology
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creator	Van der Wenden, E M Hartog-Witte, H R Roelen, H C von Frijtag Drabbe Künzel, J K Pirovano, I M Mathôt, R A Danhof, M Van Aerschot, A Lidaks, M J IJzerman, A P
description	A series of 8-substituted adenosine and theophylline-7-riboside analogues (28 and 9 compounds, respectively) was tested on adenosine A1 and A2A receptors as an extensive exploration of the adenosine C8-region. Alkylamino substituents at the 8-position cause an affinity decrease for adenosine analogues, but an affinity increase for theophylline-7-riboside derivatives. The affinity decrease is probably due to a direct steric hindrance between the C8-substituent and the binding site as well as to electronic effects, not to a steric influence on the ribose moiety to adopt the anti conformation. The 8-substituents increase the affinity of theophylline-7-riboside analogues probably by binding to a lipophilic binding site. The intrinsic activity was tested in vitro for some 8-substituted adenosine analogues, by determining the GTP shift in receptor binding studies and the inhibition of adenylate cyclase in a culture of rat thyroid FRTL-5 cells, and in vivo in the rat cardiovascular system for 8-butylaminoadenosine. Thus, it was shown that 8-ethyl-, 8-butyl-, and 8-pentylamino substituted analogues of adenosine may be partial agonists in vitro, and that 8-butylaminoadenosine is a partial agonist for the rat cardiovascular A1 receptor in vivo.
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source	MEDLINE; Elsevier ScienceDirect Journals Complete
subjects	Adenosine - analogs & derivatives Adenosine - chemistry Adenosine - pharmacology Adenylyl Cyclases - metabolism Animals Cells, Cultured Heart Rate - drug effects In Vitro Techniques Kinetics Purinergic P1 Receptor Agonists Rats Theophylline - analogs & derivatives Theophylline - chemistry Theophylline - pharmacology Xanthines - pharmacology
title	8-substituted adenosine and theophylline-7-riboside analogues as potential partial agonists for the adenosine A1 receptor
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