| Title : Syntheses, resolution, and structure-activity relationships of potent acetylcholinesterase inhibitors: 8-carbaphysostigmine analogues - Chen_1992_J.Med.Chem_35_1429 |
| Author(s) : Chen YL , Nielsen J , Hedberg K , Dunaiskis A , Jones S , Russo L , Johnson J , Ives J , Liston D |
| Ref : Journal of Medicinal Chemistry , 35 :1429 , 1992 |
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Abstract :
The synthesis of a series of 1,2,3,3a,8,8a-hexahydroindeno[2,1-b]pyrrole 5-alkylcarbamates and their resolution are reported. These compounds are structurally related to physostigmine with substitution of a methylene group in place of the NMe group at position 8 of physostigmine. Many of these 8-carbaphysostigmine analogues are more potent acetylcholinesterase inhibitors in vitro and less toxic in vivo than physostigmine. The (-)-enantiomer (e.g., 1d and 1g) possessing the same absolute configuration at C3a and C8a as that of physostigmine, is about 6 to 12-fold more potent at inhibiting acetylcholinesterase than the corresponding (+)-enantiomer (e.g., 1e and 1h). |
| PubMedSearch : Chen_1992_J.Med.Chem_35_1429 |
| PubMedID: 1573636 |
Chen YL, Nielsen J, Hedberg K, Dunaiskis A, Jones S, Russo L, Johnson J, Ives J, Liston D (1992)
Syntheses, resolution, and structure-activity relationships of potent acetylcholinesterase inhibitors: 8-carbaphysostigmine analogues
Journal of Medicinal Chemistry
35 :1429
Chen YL, Nielsen J, Hedberg K, Dunaiskis A, Jones S, Russo L, Johnson J, Ives J, Liston D (1992)
Journal of Medicinal Chemistry
35 :1429