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Pharmacological actions of some cyclic analogues of choline
Author(s) -
Hemsworth B.A.,
Shreeve S.M.,
Veitch G.B.A.
Publication year - 1984
Publication title -
british journal of pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.432
H-Index - 211
eISSN - 1476-5381
pISSN - 0007-1188
DOI - 10.1111/j.1476-5381.1984.tb16135.x
Subject(s) - acetylcholine , choline , cholinergic , neuromuscular junction , physostigmine , chemistry , cholinesterase , choline acetyltransferase , biochemistry , acetylcholinesterase , stereochemistry , enzyme , pharmacology , biology , endocrinology , neuroscience
1 Two cyclic choline analogues (3‐hydroxy‐ N,N ‐dimethylpiperidinium and 2‐hydroxymethyl‐ N,N ‐dimethylpiperidinium) and two cyclic homocholine analogues (4‐hydroxy‐ N,N ‐dimethylpiperidinium and 3‐hydroxymethyl‐ N,N ‐dimethylpiperidinium) have been studied with regard to their actions at the cholinergic synapse. 2 All the analogues had some direct depolarizing activity on the frog rectus abdominis muscle but they were less potent in this respect than acetylcholine. Compared to physostigmine, the analogues were weak inhibitors of Cholinesterase enzymes. 3 All the analogues were found to have a presynaptic blocking action on the rat phrenic nerve‐hemidiaphragm preparation, which was reversed by choline. In addition, they all inhibited the high affinity transport of choline into synaptosomes but only the cyclic choline analogues were found to be acetylated by soluble choline acetyltransferase in vitro . 4 We conclude that the hydroxypiperidinium analogues caused the presynaptic block seen at the neuromuscular junction by inhibiting acetylcholine synthesis.