Binding Mechanism and Molecular Design of Benzimidazole/Benzothiazole Derivatives as Potent Abl T315I Mutant Inhibitors

Lin, Weicong; Tan, Shepei; Zhou, Shengfu; Zheng, Xiaojie; Wu, Wenjuan; Zheng, Kang‐Cheng

doi:10.1063/1674-0068/30/cjcp1704066

Chinese Journal of Chemical Physics

2017

DOI: 10.1063/1674-0068/30/cjcp1704066

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Binding Mechanism and Molecular Design of Benzimidazole/Benzothiazole Derivatives as Potent Abl T315I Mutant Inhibitors

Weicong Lin

Shepei Tan

Shengfu Zhou

et al.

Abstract: Despite the efficacy of imatinib therapy in chronic myelogenous leukemia, the development of drug-resistant Abl mutants, especially the most difficult overcoming T315I mutant, makes the search for new Abl T315I inhibitors a very interesting challenge in medicinal chemistry. In this work, a multistep computational framework combining the three dimensional quantitative structure-activity relationship (3D-QSAR), molecular docking, molecular dynamics (MD) simulation and binding free energy calculation, was perform… Show more

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Cited by 3 publications

References 28 publications

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Advances in enhanced sampling molecular dynamics simulations for biomolecules

Wang

Zhang

2019

Chinese Journal of Chemical Physics

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Molecular dynamics simulation has emerged as a powerful computational tool for studying biomolecules as it can provide atomic insights into the conformational transitions involved in biological functions. However, when applied to complex biological macromolecules, the conformational sampling ability of conventional molecular dynamics is limited by the rugged free energy landscapes, leading to inherent timescale gaps between molecular dynamics simulations and real biological processes. To address this issue, several advanced enhanced sampling methods have been proposed to improve the sampling efficiency in molecular dynamics. In this review, the theoretical basis, practical applications, and recent improvements of both constraint and unconstrained enhanced sampling methods are summarized. Furthermore, the combined utilizations of different enhanced sampling methods that take advantage of both approaches are also briefly discussed.

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Advances in enhanced sampling molecular dynamics simulations for biomolecules

Wang

Zhang

2019

Chinese Journal of Chemical Physics

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Effect of protein dimerization on ion conductivity of gramicidin a channel studied using polarizable force field

Weng

Liao

et al. 2021

Chinese Journal of Chemical Physics

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In studies of ion channel systems, due to the huge computational cost of polarizable force fields, classical force fields remain the most widely used for a long time. In this work, we used the AMOEBA polarizable atomic multipole force field in enhanced sampling simulations of single-channel gramicidin A (gA) and double-channel gA systems and investigated its reliability in characterizing ion-transport properties of the gA ion channel under dimerization. The influence of gA dimerization on the permeation of potassium and sodium ions through the channel was described in terms of conductance, diffusion coefficient, and free energy profile. Results from the polarizable force field simulations show that the conductance of potassium and sodium ions passing through the single- and double-channel agrees well with experimental values. Further data analysis reveals that the molecular mechanism of protein dimerization affects the ion-transport properties of gA channels, i.e., protein dimerization accelerates the permeation of potassium and sodium ions passing through the double-channel by adjusting the environment around gA protein (the distribution of phospholipid head groups, ions outside the channel, and bulk water), rather than directly adjusting the conformation of gA protein.

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Identification of Potent ABL Inhibitors from Coumestrol: An Integrative In Silico Approach

Raghi¹,

Sherin²,

Archana³

et al. 2022

J. Comput. Biophys. Chem.

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Chronic Myeloid Leukemia (CML) is known as clonal myeloproliferative disorder resulted by the proliferative and deregulated expression of the BCR-ABL gene. Although targeting the BCR-ABL gene is an effective treatment for CML, the development of drug intolerance and drug resistance is still an issue for BCR-ABL targeted therapy. With an aim to develop novel BCR-ABL inhibitors with fewer side effects, we started with the anti-cancerous natural compound coumestrol as the lead. Chalcone and pyrazole are the well-exploited scaffolds in the anticancer domain; hence, in this work, we designed novel coumestrol derivatives with these structures. In order to quantify the structural changes, we employed in silico methods. The new drug leads were compared with the FDA-approved CML drug bosutinib. The molecular orbital analysis of the selected lead compounds was assessed by Density Functional Theory (DFT) approach. Molecular Dynamic (MD) computations were performed on the most promising leads to find the stability. Following which, the pharmacokinetics parameters of the screened compounds were also analyzed to check the drug-like property.

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Binding Mechanism and Molecular Design of Benzimidazole/Benzothiazole Derivatives as Potent Abl T315I Mutant Inhibitors

Cited by 3 publications

References 28 publications

Advances in enhanced sampling molecular dynamics simulations for biomolecules

Advances in enhanced sampling molecular dynamics simulations for biomolecules

Effect of protein dimerization on ion conductivity of gramicidin a channel studied using polarizable force field

Identification of Potent ABL Inhibitors from Coumestrol: An Integrative In Silico Approach

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