Effect of linker substitution on the binding of butorphan univalent and bivalent ligands to opioid receptors

连接基团取代对丁丙诺啡单价和二价配体与阿片受体结合的影响

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Abstract

A series of bivalent hydroxy ether butorphan ligands were prepared and their binding affinities at the opioid receptors determined. Addition of a hydroxy group to a hydrocarbon chain can potentiate binding affinity up to 27- and 86-fold at the mu and kappa opioid receptors, respectively. Two bivalent ligands with sub-nanomolar binding affinity at the mu and kappa opioid receptors were discovered.

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