Abstract
Glutamate plays a crucial role in the treatment of depression by interacting with the metabotropic glutamate receptor subtype 5 (mGluR5), whose negative allosteric modulators (NAMs) are thus promising antidepressants. At present, to explore the structural features of 106 newly synthesized aryl benzamide series molecules as mGluR5 NAMs, a set of ligand-based three-dimensional quantitative structure-activity relationship (3D-QSAR) analyses were firstly carried out applying comparative molecular field analysis (CoMFA) and comparative molecular similarity indices analysis (CoMSIA) methods. In addition, receptor-based analysis, namely molecular docking and molecular dynamics (MD) simulations, were performed to further elucidate the binding modes of mGluR5 NAMs. As a result, the optimal CoMSIA model obtained shows that cross-validated correlation coefficient Q2 = 0.70, non-cross-validated correlation coefficient R2ncv = 0.89, predicted correlation coefficient R2pre = 0.87. Moreover, we found that aryl benzamide series molecules bind as mGluR5 NAMs at Site 1, which consists of amino acids Pro655, Tyr659, Ile625, Ile651, Ile944, Ser658, Ser654, Ser969, Ser965, Ala970, Ala973, Trp945, Phe948, Pro903, Asn907, Val966, Leu904, and Met962. This site is the same as that of other types of NAMs; mGluR5 NAMs are stabilized in the “linear” and “arc” configurations mainly through the H-bonds interactions, π–π stacking interaction with Trp945, and hydrophobic contacts. We hope that the models and information obtained will help understand the interaction mechanism of NAMs and design and optimize NAMs as new types of antidepressants.
Highlights
Depression has a clinical manifestation of low mood, anhedonia and low energy levels, cognitive impairment, sleep disorders, sexual dysfunction, and gastrointestinal diseases, amongst other symptoms [1]
According to statistical analysis results of partial least squares (PLS), in all comparative molecular field analysis (CoMFA) and comparative molecular similarity indices analysis (CoMSIA) models, both alignment-II and -III methods lead to statistically unacceptable models with Q2 < 0.5, but alignment-I
In the early development stage of metabotropic glutamate receptor subtype 5 (mGluR5) negative allosteric modulators (NAMs), the alkyne subunit in antagonists is regarded as a key structural motif for the molecules to possess a high affinity to mGluR5 [18]
Summary
Depression has a clinical manifestation of low mood, anhedonia and low energy levels, cognitive impairment, sleep disorders, sexual dysfunction, and gastrointestinal diseases, amongst other symptoms [1]. The combination of the primary and the secondary disabilities of chronic medical disease caused by depression makes it one of the most costly medical burdens in the world [2]. WHO has predicted that depression will become the second leading cause of disability worldwide by the year 2030 [3]. The study of depression has received widespread attention from the whole world. Depression involves the influence of psychological, genetic, social environment, culture, and physiology [4]. Its etiology and pathogenesis are still unclear, and various mechanisms are still at the stage of hypothesis.
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