Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations

Although it is known crocin, a hydrophilic compound from the herbal plant Crocus sativus L., has promising antitumor activity, the detailed mechanism of its antitumor activity was not well understood. Recent experiments suggested tubulin as the primary target for the antitumor activity of crocin. Ho...

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Autores principales: Wang, Ze, Ren, Juan, Jin, Nengzhi, Liu, Xingyi, Li, Xiaofei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Molecular Biosciences
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7674667/
https://www.ncbi.nlm.nih.gov/pubmed/33251248
http://dx.doi.org/10.3389/fmolb.2020.586970
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author Wang, Ze
Ren, Juan
Jin, Nengzhi
Liu, Xingyi
Li, Xiaofei
author_facet Wang, Ze
Ren, Juan
Jin, Nengzhi
Liu, Xingyi
Li, Xiaofei
author_sort Wang, Ze
collection PubMed
description Although it is known crocin, a hydrophilic compound from the herbal plant Crocus sativus L., has promising antitumor activity, the detailed mechanism of its antitumor activity was not well understood. Recent experiments suggested tubulin as the primary target for the antitumor activity of crocin. However, due to a lack of crystal structure of tubulin bound with crocin, the exact binding mode and interaction between crocin and tubulin remains exclusive. In the present work, a computational study by integrating multiple conformation docking, molecular dynamics simulation as well as residue interaction network analysis was performed to investigate the molecular mechanism of crocin-tubulin interaction. By comparing the docking score, the most likely binding mode CRO_E1 were identified from 20 different binding modes of crocin in the vinca binding pockets. Further molecular dynamics simulation of CRO_E1 complex showed the binding of crocin is more stable than the inhibitor soblidotin and vinblastine. During the simulation course, an excessive number of hydrogen bonds were observed for the ligand crocin. The binding free energy of crocin-tubulin complex was calculated as −79.25 ± 7.24 kcal/mol, which is almost twice of the ligand soblidotin and vinblastine. By using energy decomposition, hot residues for CRO_E1 were identified as Gln(11), Gln(15), Thr(72), Ser(75), Pro(173)-Lys(174)-Val(175)-Ser(176)-Asp(177), Tyr(222), and Asn(226) in the β-chain, and Asp(245), Ala(247)-Leu(248), Val(250), Asn(329), and Ile(332) in the α-chain. Residue interaction network analysis also showed the importance of these hot residues in the interaction network of crocin-tubulin complex. In addition, a common residue motif Val(175)-Xxx(176)-Asp(177) was discovered for all three bindings, suggesting its importance in future drug design. The study could provide valuable insights into the interaction between crocin and tubulin, and give suggestive clues for further experimental studies.
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spelling pubmed-76746672020-11-27 Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations Wang, Ze Ren, Juan Jin, Nengzhi Liu, Xingyi Li, Xiaofei Front Mol Biosci Molecular Biosciences Although it is known crocin, a hydrophilic compound from the herbal plant Crocus sativus L., has promising antitumor activity, the detailed mechanism of its antitumor activity was not well understood. Recent experiments suggested tubulin as the primary target for the antitumor activity of crocin. However, due to a lack of crystal structure of tubulin bound with crocin, the exact binding mode and interaction between crocin and tubulin remains exclusive. In the present work, a computational study by integrating multiple conformation docking, molecular dynamics simulation as well as residue interaction network analysis was performed to investigate the molecular mechanism of crocin-tubulin interaction. By comparing the docking score, the most likely binding mode CRO_E1 were identified from 20 different binding modes of crocin in the vinca binding pockets. Further molecular dynamics simulation of CRO_E1 complex showed the binding of crocin is more stable than the inhibitor soblidotin and vinblastine. During the simulation course, an excessive number of hydrogen bonds were observed for the ligand crocin. The binding free energy of crocin-tubulin complex was calculated as −79.25 ± 7.24 kcal/mol, which is almost twice of the ligand soblidotin and vinblastine. By using energy decomposition, hot residues for CRO_E1 were identified as Gln(11), Gln(15), Thr(72), Ser(75), Pro(173)-Lys(174)-Val(175)-Ser(176)-Asp(177), Tyr(222), and Asn(226) in the β-chain, and Asp(245), Ala(247)-Leu(248), Val(250), Asn(329), and Ile(332) in the α-chain. Residue interaction network analysis also showed the importance of these hot residues in the interaction network of crocin-tubulin complex. In addition, a common residue motif Val(175)-Xxx(176)-Asp(177) was discovered for all three bindings, suggesting its importance in future drug design. The study could provide valuable insights into the interaction between crocin and tubulin, and give suggestive clues for further experimental studies. Frontiers Media S.A. 2020-11-05 /pmc/articles/PMC7674667/ /pubmed/33251248 http://dx.doi.org/10.3389/fmolb.2020.586970 Text en Copyright © 2020 Wang, Ren, Jin, Liu and Li. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Molecular Biosciences
Wang, Ze
Ren, Juan
Jin, Nengzhi
Liu, Xingyi
Li, Xiaofei
Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations
title Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations
title_full Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations
title_fullStr Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations
title_full_unstemmed Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations
title_short Is Crocin a Potential Anti-tumor Candidate Targeting Microtubules? Computational Insights From Molecular Docking and Dynamics Simulations
title_sort is crocin a potential anti-tumor candidate targeting microtubules? computational insights from molecular docking and dynamics simulations
topic Molecular Biosciences
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7674667/
https://www.ncbi.nlm.nih.gov/pubmed/33251248
http://dx.doi.org/10.3389/fmolb.2020.586970
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