Structure- and Cation-Dependent Mechanism of Interaction of Tricyclic Antidepressants with NMDA Receptor According to Molecular Modeling Data

Daria A Belinskaia; Natalia N Shestakova

doi:10.1134/S0006297924030106

Structure- and Cation-Dependent Mechanism of Interaction of Tricyclic Antidepressants with NMDA Receptor According to Molecular Modeling Data

Biochemistry (Mosc). 2024 Mar;89(3):507-522. doi: 10.1134/S0006297924030106.

Authors

Daria A Belinskaia¹, Natalia N Shestakova²

Affiliations

¹ Sechenov Institute of Evolutionary Physiology and Biochemistry, Russian Academy of Sciences, St. Petersburg, 194223, Russia. d_belinskaya@mail.ru.
² Sechenov Institute of Evolutionary Physiology and Biochemistry, Russian Academy of Sciences, St. Petersburg, 194223, Russia.

PMID: 38648769
DOI: 10.1134/S0006297924030106

Abstract

Some tricyclic antidepressants (TCAs), including amitriptyline (ATL), clomipramine (CLO), and desipramine (DES), are known to be effective for management of neuropathic pain. It was previously determined that ATL, CLO, and DES are capable of voltage-dependent blocking of NMDA receptors of glutamate (NMDAR), which play a key role in pathogenesis of neuropathic pain. Despite the similar structure of ATL, CLO, and DES, efficacy of their interaction with NMDAR varies significantly. In the study presented here, we applied molecular modeling methods to investigate the mechanism of binding of ATL, CLO, and DES to NMDAR and to identify structural features of the drugs that determine their inhibitory activity against NMDAR. Molecular docking of the studied TCAs into the NMDAR channel was performed. Conformational behavior of the obtained complexes in the lipid bilayer was simulated by the method of molecular dynamics (MD). A single binding site (upper) for the tertiary amines ATL and CLO and two binding sites (upper and lower) for the secondary amine DES were identified inside the NMDAR channel. The upper and lower binding sites are located along the channel axis at different distances from the extracellular side of the plasma membrane. MD simulation revealed that the position of DES in the lower site is stabilized only in the presence of sodium cation inside the NMDAR channel. DES binds more strongly to NMDAR compared to ATL and CLO due to simultaneous interaction of two hydrogen atoms of its cationic group with the asparagine residues of the ion pore of the receptor. This feature may be responsible for the stronger side effects of DES. It has been hypothesized that ATL binds to NMDAR less efficiently compared to DES and CLO due to its lower conformational mobility. The identified features of the structure- and cation-dependent mechanism of interaction between TCAs and NMDAR will help in the further development of effective and safe analgesic therapy.

Keywords: NMDA receptor; molecular docking; molecular dynamics; neuropathic pain; tricyclic antidepressants.

MeSH terms

Amitriptyline / chemistry
Amitriptyline / metabolism
Amitriptyline / pharmacology
Antidepressive Agents, Tricyclic* / chemistry
Antidepressive Agents, Tricyclic* / metabolism
Antidepressive Agents, Tricyclic* / pharmacology
Binding Sites
Cations / chemistry
Cations / metabolism
Clomipramine / chemistry
Clomipramine / metabolism
Clomipramine / pharmacology
Desipramine / pharmacology
Humans
Molecular Docking Simulation*
Molecular Dynamics Simulation*
Protein Binding
Receptors, N-Methyl-D-Aspartate* / chemistry
Receptors, N-Methyl-D-Aspartate* / metabolism

Substances

Receptors, N-Methyl-D-Aspartate
Antidepressive Agents, Tricyclic
Amitriptyline
Clomipramine
Cations
Desipramine