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Interactions of taurine and structurally related analogues with GABAergic system and taurine binding sites of rabbit brain.

Academic Article
Publication Date:
2003
abstract:
The aim of this studywas to find taurinergic compounds that do not interact with brain GABA ergic systems. Washed synaptic membranes (SM) from whole rabbit brain were able to bind [3H]muscimol. Saturation experiments of the binding of [3H]GABA to GABAB receptors showed that SM possess two binding components; twice Triton X-100-treated SM contained 0.048 mmol endogenous taurine/ kg protein and bound [3H]taurine in a saturable manner (Kd¼249.076.3 nm and Bmax3.471.0 pmol mg_1 prot). Among the 19 structural analogues of taurine, 6-aminomethyl-3-methyl-4H-1,2,4-benzothiadiazine 1,1-dioxide (TAG), 2-aminoethylarsonic (AEA), 2-hydroxyethanesulfonic (ISE) and (7)cis-2- aminocyclohexane sulfonic acids (CAHS) displaced [3H]taurine binding (K0.13, 0.13, 13.5 and 4.0 mm, respectively). These analogues did not interact with GABAA and GABAB receptors and did not affect taurine- and GABA-uptake systems and GABA-transaminase activity. 3-Aminopropanesulfonic acid (OMO), b-alanine, pyridine-3-sulfonic acid, N,N,N-trimethyltaurine (TMT), 2-(guanidino)ethanesulfonic acid (GES), ethanolamine-O-sulphate, N,N-dimethyltaurine (DMT), taurine and (7)piperidine-3-sulfonic acid (PSA) inhibited [3H]muscimol binding to GABAA receptors with different affinities (Ki¼0.013, 7.9, 24.6, 47.5, 52.0, 91.0, 47.5, 118.1 and 166.3 mm, respectively). Taurine, 2-aminoethylphosphonic acid, DMT, TMT and OMO inhibited the binding of [3H]GABA to GABAB receptors with Ki’s in the mm range (0.8, 3.5, 4.4, 11.3 and 5.0, respectively). GES inhibited taurine uptake (IC50 3.72 mm) and PSA GABA transaminase activity(IC50103.0 mm). In conclusion, AEA, TAG, ISE and CAHS fulfill the criteria for taurinergic agents.
Iris type:
01.01 Articolo in rivista
Keywords:
GABA receptors; Taurine; Taurine binding site; Taurine derivatives
List of contributors:
Machetti, Fabrizio
Authors of the University:
MACHETTI FABRIZIO
Handle:
https://iris.cnr.it/handle/20.500.14243/167062
Published in:
BRITISH JOURNAL OF PHARMACOLOGY
Journal
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URL

http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1573748/
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