BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. rs2300478, PRKCA, Response to oxidative stress, Inflammatory disorder, Neuron)
Bookmark Forward

Selectivity of (3)H-MADAM binding to 5-hydroxytryptamine transporters in vitro and in vivo in mice; correlation with behavioural effects.

A K Larsen, L T Brennum, J Egebjerg, C Sánchez, C Halldin, P H Andersen

Department of Disease Biology, H. Lundbeck A/S, 9 Ottiliavej, Valby, DK-2500 Denmark. stil@lundbeck.com

British journal of pharmacology 2004 Mar


filter terms:
  • 5 htp (3)
  • 5 hydroxytryptamine (3)
  • a 2C (1)
  • animals (1)
  • antidepressive agents (2)
  • antidepressive agents, tricyclic (2)
  • behavior animal (1)
  • benzylamine (2)
  • binding (9)
  • binding competitive (1)
  • cells (2)
  • cells cultured (1)
  • cerebral cortex (2)
  • CHO (2)
  • clomipramine (1)
  • cricetinae (1)
  • dopamine transport (1)
  • drug synergism (1)
  • in vitro (5)
  • ion channels (1)
  • male (1)
  • membrane glycoproteins (2)
  • membrane transport proteins (2)
  • membranes (1)
  • mice (2)
  • mice inbred strains (1)
  • n n- dimethyl- 2-( 2- amino- 4- methylphenylthi... (1)
  • nerve tissue proteins (2)
  • noradrenaline (2)
  • selective serotonin re- uptake inhibitors (3)
  • serotonin antagonists (2)
  • serotonin plasma membrane transport proteins (2)
  • serotonin uptake inhibitors (2)
  • SERT (6)
  • slc6a4 protein, mouse (1)
  • synaptosomes (1)
  • transport (2)
  • tritium (2)
    • Sizes of these terms reflect their relevance to your search.

    1. Binding of the novel radioligand (3)H-2-(2-dimethylaminomethyl-phenylsulphanyl)-5-methyl-phenylamine ((3)H-MADAM) to the serotonin transporter (SERT) was used to characterise a range of selective serotonin re-uptake inhibitors (SSRIs) in vitro and in vivo. 2. (3)H-MADAM bound with high affinity in a saturable manner to both human SERT expressed in CHO cells (K(d)=0.20 nm (pK(d)=9.74+/-0.12), B(max)=35+/-4 fmol mg(-1) protein) and mouse cerebral cortex membranes (K(d)=0.21 nm (pK(d)=9.66+/-0.10), B(max)=50+/-24 fmol mg(-1) protein). 3. Binding of (3)H-MADAM was highly selective for SERT in vitro as demonstrated by the in vitro profile of MADAM tested at 75 different receptors, ion channels and transporters. This was further substantiated by the pharmacological profile of the binding. Hence, the binding of (3)H-MADAM was potently inhibited by SSRIs but not by selective inhibitors of noradrenaline transport and dopamine transport. Likewise, a 5-HT(2A/2C) receptor antagonist did not inhibit (3)H-MADAM binding. 4. (3)H-MADAM binding in vivo was inhibited only by compounds which also inhibited the binding of (3)H-MADAM in vitro (the SSRIs, mixed SERT/noradrenaline transport inhibitors and clomipramine), confirming the selectivity of (3)H-MADAM for SERT also in vivo. Moreover, compounds effective in inhibiting (3)H-MADAM binding were the only ones found to be active in the mouse 5-HTP potentiation test confirming the model as a behavioural correlate to in vivo 5-HT uptake. 5. Finally, it was found that a SERT occupancy of 85-95% was necessary to produce 50% of the maximum behavioural response (ED(50)).

    Citation

    A K Larsen, L T Brennum, J Egebjerg, C Sánchez, C Halldin, P H Andersen. Selectivity of (3)H-MADAM binding to 5-hydroxytryptamine transporters in vitro and in vivo in mice; correlation with behavioural effects. British journal of pharmacology. 2004 Mar;141(6):1015-23

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 14993096

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.