Integrated In Silico Fragment-Based Drug Design: Case Study with Allosteric Modulators on Metabotropic Glutamate Receptor 5

Bian, Yuemin; Feng, Zhiwei; Yang, Peng; Xie, Xiang‐Qun

doi:10.1208/s12248-017-0093-5

Cited by 27 publications

(26 citation statements)

References 61 publications

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“…SYBYL-X 1.3 was used for the preparation of the crystal structure, including energy minimization and residue repair. SYBYL-X 1.3 and PyMol (http:// www.pymol.org) were used for molecular visualization, structural superimposition, and data analysis following our usual operation routine [33].…”

Section: Methodsmentioning

confidence: 99%

“…A conserved orthosteric binding pocket among rhodopsin-like GPCRs was defined by selecting corresponding surrounding residues. The Kollman all atom approach was used to calculate atomic charges for the protein [34] and the Gasteiger-Hückel approach for the ligand [35] following our usual operation routine [33]. The hydrogen atoms of the protein were allowed to move.…”

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Computational systems pharmacology analysis of cannabidiol: a combination of chemogenomics-knowledgebase network analysis and integrated in silico modeling and simulation

Bian

Jing

et al. 2018

Acta Pharmacol Sin

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With treatment benefits in both the central nervous system and the peripheral system, the medical use of cannabidiol (CBD) has gained increasing popularity. Given that the therapeutic mechanisms of CBD are still vague, the systematic identification of its potential targets, signaling pathways, and their associations with corresponding diseases is of great interest for researchers. In the present work, chemogenomics-knowledgebase systems pharmacology analysis was applied for systematic network studies to generate CBD-target, target-pathway, and target-disease networks by combining both the results from the in silico analysis and the reported experimental validations. Based on the network analysis, three human neuro-related rhodopsin-like GPCRs, i.e., 5-hydroxytryptamine receptor 1 A (5HT), delta-type opioid receptor (OPRD) and G protein-coupled receptor 55 (GPR55), were selected for close evaluation. Integrated computational methodologies, including homology modeling, molecular docking, and molecular dynamics simulation, were used to evaluate the protein-CBD binding modes. A CBD-preferred pocket consisting of a hydrophobic cavity and backbone hinges was proposed and tested for CBD-class A GPCR binding. Finally, the neurophysiological effects of CBD were illustrated at the molecular level, and dopamine receptor 3 (DRD3) was further predicted to be an active target for CBD.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Computational systems pharmacology analysis of cannabidiol: a combination of chemogenomics-knowledgebase network analysis and integrated in silico modeling and simulation

Bian

Jing

et al. 2018

Acta Pharmacol Sin

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“…Christopher et al [22] Up to now, two mGluR5 receptor binding regions (the orthosteric binding region in the VFT and the allosteric binding region in the 7TM) have been reported [24]. In fact, we find that the studies on the NAM site almost all focus on the transmembrane allosteric binding region [8,[19][20][21][22], which can be explained by the fact that the allosteric binding pocket is less conserved compared to the orthosteric binding region, thus helping the identification of selective ligands [9]. In structure, the 8 antagonists belong to the acetylenic chemotype and non-acetylenic chemotype, as shown in Figure 8.…”

Section: Discussionmentioning

confidence: 77%

“…Therefore, two structural motifs, i.e., amide and urea functional groups, are proposed as the replacements of alkyne linkages in mGluR5 NAMs [18]. So far, altogether eight known mGluR5 NAMs have entered and/or are about to enter clinical trials, i.e., Mavoglurant [19][20][21], Basimglurant [8,21], MTEP [8], HTL14242 [20], Dipraglurant [21], Fenobam [21,22], Thiazole-2-carboxamides (6bc, 6bj) [18]. It is worth mentioning that, for a long time, the important structural information on mGluR5 NAMs was to combine mutation studies with homology modeling and/or a series of ligand analogs.…”

Section: Discussionmentioning

confidence: 99%

Profiling the Structural Determinants of Aryl Benzamide Derivatives as Negative Allosteric Modulators of mGluR5 by In Silico Study

et al. 2020

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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.

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“…Nevertheless, RMSD is still widely used for comparing non-identical molecules such as in virtual screening programs. [14][15][16][17][18] Thus, it is unclear which metric is best at quantifying the degree of binding mode conservation, especially in cases where a smaller ligand and its elaborated counterpart are compared. Previous studies have discussed the pitfalls of certain metrics and hence use multiple metrics alongside one another.…”

Section: Introductionmentioning

confidence: 99%

SuCOS is Better than RMSD for Evaluating Fragment Elaboration and Docking Poses

Leung¹,

Bodkin²,

Delft³

et al. 2019

Preprint

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One of the fundamental assumptions of fragment-based drug discovery is that the fragment’s binding mode will be conserved upon elaboration into larger compounds. The most common way of quantifying binding mode similarity is Root Mean Square Deviation (RMSD), but Protein Ligand Interaction Fingerprint (PLIF) similarity and shape-based metrics are sometimes used. We introduce SuCOS, an open-source shape and chemical feature overlap metric. We explore the strengths and weaknesses of RMSD, PLIF similarity, and SuCOS on a dataset of X-ray crystal structures of paired elaborated larger and smaller molecules bound to the same protein. Our redocking and cross-docking studies show that SuCOS is superior to RMSD and PLIF similarity. When redocking, SuCOS produces fewer false positives and false negatives than RMSD and PLIF similarity; and in cross-docking, SuCOS is better at differentiating experimentally-observed binding modes of an elaborated molecule given the pose of its non-elaborated counterpart. Finally we show that SuCOS performs better than AutoDock Vina at differentiating actives from decoy ligands using the DUD-E dataset. SuCOS is available at https://github.com/susanhleung/SuCOS . <br>

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Integrated In Silico Fragment-Based Drug Design: Case Study with Allosteric Modulators on Metabotropic Glutamate Receptor 5

Cited by 27 publications

References 61 publications

Computational systems pharmacology analysis of cannabidiol: a combination of chemogenomics-knowledgebase network analysis and integrated in silico modeling and simulation

Computational systems pharmacology analysis of cannabidiol: a combination of chemogenomics-knowledgebase network analysis and integrated in silico modeling and simulation

Profiling the Structural Determinants of Aryl Benzamide Derivatives as Negative Allosteric Modulators of mGluR5 by In Silico Study

SuCOS is Better than RMSD for Evaluating Fragment Elaboration and Docking Poses

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