New PPARα/γ/δ Optimal Activator Rationally Designed by Computational Methods

Padilha, Elias Carvalho; Serafim, Rodolfo Bortolozo; Sarmiento, Deisy Y. R.; Santos, César F.; Santos, Cleydson Breno Rodrigues dos; Silva, Carlos Henrique Tomich de Paula da

doi:10.5935/0103-5053.20160043

Cited by 16 publications

(20 citation statements)

References 29 publications

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“…Pharmacophore perception for the compounds was carried out using PharmaGist, and the top-ranked pre-alignment of the compounds had a score of 64.605 (see Figure 2), wherein Silva [22] and Padilha [23] independently reported similar score values in their studies, using the same the PharmaGist algorithm. The aligned compounds shared six spatial characteristics: two aromatic (AR) groups and four hydrogen acceptor (HA) groups, where the coordinates and the radius of the spatial characteristics are shown in Table 1.…”

Section: Pharmacophore Perception Using the Pharmagist And Discovery mentioning

confidence: 99%

“…The other models were unsatisfactory in the recovery of the known bioactive ligands, since many hypotheses did not obtain the necessary characteristics for interaction at the A2AAR receptor site [26]. Pharmacophore hypothese was classified according to the number of ligands aligned or that combined in order to generate a pharmacophore model that was satisfactory based on score, according to literature data [22,23,26]. The pharmacophore model chosen in pre-alignment via PharmaGist was used as input in the Discovery Studio, in order to refine the initial pharmacophore model.…”

Section: Pharmacophore Model Evaluationmentioning

confidence: 99%

“…The QSAR model was built with n samples of 16 structures (1, 6, 7, 9-21), since 5 structures were outliers (2-5 and 8-randomic errors contaminated the observations) and they were identified and subsequently removed in order to obtain models with greater predictive power, without impairing the statistical quality that was evaluated by the correlation coefficient (r), squared correlation coefficient (r 2 ), explained variance (r 2 A , i.e., r 2 adjusted), standard error of estimate (SEE), and variance ratio (F). The best regression models were selected based on the higher values of r and F and smaller values of SEE [23]. This was proven through the application of the models to the compounds for verifying the variation between the experimental and theoretical values, calculated through the quantitative structure-activity relationship (QSAR) model.…”

Section: Qsar Modeling Using Multiple Linear Regressions (Mlr)mentioning

confidence: 99%

“…After evaluating the parameters and the statistical quality, the parametric models (tetra-, pentaand hexaparametric) were applied to the set of seven compounds (22)(23)(24)(25)(26)(27)(28) in this study, called the test set (totaling 43.75% in relation to the number of compounds used in the training set; n = 16). Compounds were selected from the Pubchem database based on their respective EC 50 values, which were converted to pEC 50 .…”

Section: Quantitative Structure-activity Relationship (Qsar) Modelingmentioning

confidence: 99%

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Identification of Novel Chemical Entities for Adenosine Receptor Type 2A Using Molecular Modeling Approaches

et al. 2020

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Adenosine Receptor Type 2A (A2AAR) plays a role in important processes, such as anti-inflammatory ones. In this way, the present work aimed to search for compounds by pharmacophore-based virtual screening. The pharmacokinetic/toxicological profiles of the compounds, as well as a robust QSAR, predicted the binding modes via molecular docking. Finally, we used molecular dynamics to investigate the stability of interactions from ligand-A2AAR. For the search for A2AAR agonists, the UK-432097 and a set of 20 compounds available in the BindingDB database were studied. These compounds were used to generate pharmacophore models. Molecular properties were used for construction of the QSAR model by multiple linear regression for the prediction of biological activity. The best pharmacophore model was used by searching for commercial compounds in databases and the resulting compounds from the pharmacophore-based virtual screening were applied to the QSAR. Two compounds had promising activity due to their satisfactory pharmacokinetic/toxicological profiles and predictions via QSAR (Diverset 10002403 pEC50 = 7.54407; ZINC04257548 pEC50 = 7.38310). Moreover, they had satisfactory docking and molecular dynamics results compared to those obtained for Regadenoson (Lexiscan®), used as the positive control. These compounds can be used in biological assays (in vitro and in vivo) in order to confirm the potential activity agonist to A2AAR.

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Section: Pharmacophore Perception Using the Pharmagist And Discovery mentioning

confidence: 99%

Section: Pharmacophore Model Evaluationmentioning

confidence: 99%

Section: Qsar Modeling Using Multiple Linear Regressions (Mlr)mentioning

confidence: 99%

Section: Quantitative Structure-activity Relationship (Qsar) Modelingmentioning

confidence: 99%

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Identification of Novel Chemical Entities for Adenosine Receptor Type 2A Using Molecular Modeling Approaches

et al. 2020

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“…By the use of a computational approach, research has studied protein-ligand interactions at the PPAR receptor that have successfully provided experimentally verified detailed structural information at the molecular level and identified a large number PPAR agonists [8,22,36,38,63,[68][69][70][71][72][73][74][75][76][77][78][79][80]. These include a number studies combining virtual screening with molecular modeling [64,69], molecular docking [36], molecular dynamics (MD) simulations [81], and in vitro assays [38,68] for further validation.…”

Section: Introductionmentioning

confidence: 99%

To Probe Full and Partial Activation of Human Peroxisome Proliferator-Activated Receptors by Pan-Agonist Chiglitazar Using Molecular Dynamics Simulations

et al. 2020

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Chiglitazar is a promising new-generation insulin sensitizer with low reverse effects for the treatment of type II diabetes mellitus (T2DM) and has shown activity as a nonselective pan-agonist to the human peroxisome proliferator-activated receptors (PPARs) (i.e., full activation of PPARγ and a partial activation of PPARα and PPARβ/δ). Yet, it has no high-resolution complex structure with PPARs and its detailed interactions and activation mechanism remain unclear. In this study, we docked chiglitazar into three experimentally resolved crystal structures of hPPAR subtypes, PPARα, PPARβ/δ, and PPARγ, followed by 3 μs molecular dynamics simulations for each system. Our MM-GBSA binding energy calculation revealed that chiglitazar most favorably bound to hPPARγ (-144.6 kcal/mol), followed by hPPARα (-138.0 kcal/mol) and hPPARβ (-135.9 kcal/mol), and the order is consistent with the experimental data. Through the decomposition of the MM-GBSA binding energy by residue and the use of two-dimensional interaction diagrams, key residues involved in the binding of chiglitazar were identified and characterized for each complex system. Additionally, our detailed dynamics analyses support that the conformation and dynamics of helix 12 play a critical role in determining the activities of the different types of ligands (e.g., full agonist vs. partial agonist). Rather than being bent fully in the direction of the agonist versus antagonist conformation, a partial agonist can adopt a more linear conformation and have a lower degree of flexibility. Our finding may aid in further development of this new generation of medication.

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Virtual screening, ADME/Tox predictions and the drug repurposing concept for future use of old drugs against the COVID-19

et al. 2020

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New PPARα/γ/δ Optimal Activator Rationally Designed by Computational Methods

Cited by 16 publications

References 29 publications

Identification of Novel Chemical Entities for Adenosine Receptor Type 2A Using Molecular Modeling Approaches

Identification of Novel Chemical Entities for Adenosine Receptor Type 2A Using Molecular Modeling Approaches

To Probe Full and Partial Activation of Human Peroxisome Proliferator-Activated Receptors by Pan-Agonist Chiglitazar Using Molecular Dynamics Simulations

Virtual screening, ADME/Tox predictions and the drug repurposing concept for future use of old drugs against the COVID-19

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