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The mechanism of a high-affinity allosteric inhibitor of the serotonin transporter.


ABSTRACT: The serotonin transporter (SERT) terminates serotonin signaling by rapid presynaptic reuptake. SERT activity is modulated by antidepressants, e.g., S-citalopram and imipramine, to alleviate symptoms of depression and anxiety. SERT crystal structures reveal two S-citalopram binding pockets in the central binding (S1) site and the extracellular vestibule (S2 site). In this study, our combined in vitro and in silico analysis indicates that the bound S-citalopram or imipramine in S1 is allosterically coupled to the ligand binding to S2 through altering protein conformations. Remarkably, SERT inhibitor Lu AF60097, the first high-affinity S2-ligand reported and characterized here, allosterically couples the ligand binding to S1 through a similar mechanism. The SERT inhibition by Lu AF60097 is demonstrated by the potentiated imipramine binding and increased hippocampal serotonin level in rats. Together, we reveal a S1-S2 coupling mechanism that will facilitate rational design of high-affinity SERT allosteric inhibitors.

SUBMITTER: Plenge P 

PROVIDER: S-EPMC7083837 | biostudies-literature | 2020 Mar

REPOSITORIES: biostudies-literature

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The mechanism of a high-affinity allosteric inhibitor of the serotonin transporter.

Plenge Per P   Abramyan Ara M AM   Sørensen Gunnar G   Mørk Arne A   Weikop Pia P   Gether Ulrik U   Bang-Andersen Benny B   Shi Lei L   Loland Claus J CJ  

Nature communications 20200320 1


The serotonin transporter (SERT) terminates serotonin signaling by rapid presynaptic reuptake. SERT activity is modulated by antidepressants, e.g., S-citalopram and imipramine, to alleviate symptoms of depression and anxiety. SERT crystal structures reveal two S-citalopram binding pockets in the central binding (S1) site and the extracellular vestibule (S2 site). In this study, our combined in vitro and in silico analysis indicates that the bound S-citalopram or imipramine in S1 is allostericall  ...[more]

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