Stereochemical Studies on Medicinal Agents. 15. Absolute Configurations and Analgetic Potencies of Enantiomeric Diastereomers of 3-Allyl-1-methyl-4-phenyl-4-propionoxypipendine

Kevin H. Bell; Philip S. Portoghese

doi:10.1021/jm00264a001

Stereochemical Studies on Medicinal Agents. 15. Absolute Configurations and Analgetic Potencies of Enantiomeric Diastereomers of 3-Allyl-1-methyl-4-phenyl-4-propionoxypipendine

Kevin H. Bell, Philip S. Portoghese

Medicinal Chemistry

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Abstract

Enantiomeric diastereomers of the title compound la, b were prepared and their absolute configurations determined by chemically relating them to (3R,4S)- and (3S,4R)-1,3-dimethyl-4-phenylpiperidin-4-ol. The analgetic potency of (3R,4S)-la (8a) is 40 times that of morphine and 260 times that of its enanti-omer 10a. Enantiomers of lb (8b and 10b) exhibited no stereoselectivity and possessed a relatively low order of potency (~ 1/12 that of morphine). The fact that this is in marked contrast to the reported high antipodal stereoselectivity for β-prodine suggests that the mode of interaction of lb with analgetic receptors differs from that of β-prodine. Possible reasons for the change of stereoselectivity are discussed.

Original language	English (US)
Pages (from-to)	589-591
Number of pages	3
Journal	Journal of medicinal chemistry
Volume	16
Issue number	6
DOIs	https://doi.org/10.1021/jm00264a001
State	Published - Jun 1 1973

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N2 - Enantiomeric diastereomers of the title compound la, b were prepared and their absolute configurations determined by chemically relating them to (3R,4S)- and (3S,4R)-1,3-dimethyl-4-phenylpiperidin-4-ol. The analgetic potency of (3R,4S)-la (8a) is 40 times that of morphine and 260 times that of its enanti-omer 10a. Enantiomers of lb (8b and 10b) exhibited no stereoselectivity and possessed a relatively low order of potency (~ 1/12 that of morphine). The fact that this is in marked contrast to the reported high antipodal stereoselectivity for β-prodine suggests that the mode of interaction of lb with analgetic receptors differs from that of β-prodine. Possible reasons for the change of stereoselectivity are discussed.

AB - Enantiomeric diastereomers of the title compound la, b were prepared and their absolute configurations determined by chemically relating them to (3R,4S)- and (3S,4R)-1,3-dimethyl-4-phenylpiperidin-4-ol. The analgetic potency of (3R,4S)-la (8a) is 40 times that of morphine and 260 times that of its enanti-omer 10a. Enantiomers of lb (8b and 10b) exhibited no stereoselectivity and possessed a relatively low order of potency (~ 1/12 that of morphine). The fact that this is in marked contrast to the reported high antipodal stereoselectivity for β-prodine suggests that the mode of interaction of lb with analgetic receptors differs from that of β-prodine. Possible reasons for the change of stereoselectivity are discussed.

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Stereochemical Studies on Medicinal Agents. 15. Absolute Configurations and Analgetic Potencies of Enantiomeric Diastereomers of 3-Allyl-1-methyl-4-phenyl-4-propionoxypipendine

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