1991
DOI: 10.1002/chir.530030207
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Stereoselectivity of (R)‐ and (S)‐hexahydro‐difenidol binding to neuroblastoma M1, cardiac M2, pancreatic M3, and striatum M4 muscarinic receptors

Abstract: ABSTRACT(R)-Hexahydro-difenidol has a higher affinity for M 1 receptors in NB-OK 1 cells, pancreas M 3 and striatum M 4 receptors (pKi 7.9 to 8.3) than for cardiac M 2 receptors (pKi 7 .0). (8)-Hexahydro-difenidol, by contrast, is nonselective (pKi 5.8 to 6.1). Our goal in the present study was to evaluate the importance ofthe hydrophobic phenyl, and cyclohexyl rings of hexahydro-difenidol for the stereoselectivity and reeeptor selectivity of hexahydro-difenidol binding to the four muscarinic receptors. Our re… Show more

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Cited by 19 publications
(12 citation statements)
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“…In this study, and in contrast with the procyclidine and hexahydro-diphenidol distomers (Waelbroeck et al, 1990a;, we obtained evidence that most distomers did not recognize…”
Section: Allosteric Effect Of Distomers On [3h]-nms Bindingmentioning
confidence: 42%
See 1 more Smart Citation
“…In this study, and in contrast with the procyclidine and hexahydro-diphenidol distomers (Waelbroeck et al, 1990a;, we obtained evidence that most distomers did not recognize…”
Section: Allosteric Effect Of Distomers On [3h]-nms Bindingmentioning
confidence: 42%
“…As shown in Tables I and 3, this modification resulted ina 6 to 60 fold affinity decrease. Further experiments are needed to determine whether the affinity decrease is due to steric hindrance or to the loss of a strong hydrogen bond between one of the two possible enol-like hydroxy groups and the receptor (Waelbroeck et al, 1990a;. Structure-activity relationships: distomers As previously stated in the Results section, we are confident that we measured the intrinsic affinity of most distomers, rather than the effect of a (very small) contamination by the eutomer.…”
Section: Pharmacological Studiesmentioning
confidence: 83%
“…Comparison of the enantioselectivity ratio for the two enantiomers of HHD in RAM [ Table 2; (R)/(S) = 288] with data obtained in radioligand binding studies at native M 1 to M 4 receptors (M 1 = 158, M 2 = 16, M 3 = 158, M 4 = 100; Waelbroeck et al 1991b) clearly excludes the M 2 subtype for mediating contraction in RAM (see below). In addition, the stereoselectivity ratio for HHD in RAM [(R)/(S) = 288] is in very good agreement with that obtained in functional experiments at M 3 receptors in guinea-pig ileum longitudinal smooth muscle (= 191;Feifel et al 1990) and submucosal arterioles (= 229-275; Bungardt et al 1992) as well as in rat duodenum longitudinal smooth muscle (= 186;Pfaff et al 1995a).…”
Section: Discussionmentioning
confidence: 99%
“…In addition, muscarinic receptors may be differentiated on the basis of their stereoselective recognition of chiral antagonists such as hexahydrodifenidol (Feifel et al 1990;Dörje et al 1991;Waelbroeck et al 1992Waelbroeck et al , 1996Pfaff et al 1995b). In the present study, all of the above mentioned key antagonists, including the (R)-and (S)-enantiomers of hexahydro-difenidol [(R)-and (S)-HHD] (Waelbroeck et al 1991b), were used to identify the muscarinic receptor subtype mediating contraction in RAM.…”
Section: Introductionmentioning
confidence: 99%
“…The reaction pathways used to synthesize compounds 1-26 are reported in Scheme 1. n-Butyl (la), n-pentyl(5-10), and n-hexyl (12)(13)(14)(15)(16) analogs of the lead compounds were obtained from the corresponding thioacids (3%35), synthesized according to ref. [l].…”
Section: Chemistrymentioning
confidence: 99%