Computational analysis of bevacizumab binding with protein receptors for its potential anticancer activity

Nada Alsakhen; Enas S. Radwan; Imran Zafer; Husam Abed alfattah; Israa M. Shamkh; Md Tabish Rehman; Moayad Shahwan; Khalid Ali Khan; Shimaa A. Ahmed

doi:10.1080/07391102.2024.2307445

Computational analysis of bevacizumab binding with protein receptors for its potential anticancer activity

Nada Alsakhen
, Enas S. Radwan
, Imran Zafer
, Husam Abed alfattah
, Israa M. Shamkh
, Md Tabish Rehman
, Moayad Shahwan
, Khalid Ali Khan
, Shimaa A. Ahmed

Hashemite University
Zarqa University
Virtual University of Pakistan
Cairo University
King Saud University
King Khalid University
Faculty of Sciences

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

Breast cancer poses a significant global challenge, prompting researchers to explore novel approaches for potential treatments. In this study, we investigated the binding free energy (ΔG) of bevacizumab, an anti-cancer therapy targeting angiogenesis through the inhibition of vascular endothelial growth factor (VEGF), with various proto-oncogenes including CDK4, EGFR, frizzled, IGFR, OmoMYC, and KIT. Our in-silico investigation revealed that hydrogen bonding is pivotal in inducing conformational changes within the DNA structure, impeding its replication and preventing cell death. Molecular docking results revealed the presence of crucial hydrogen bonds and supported the formation of stable bevacizumab complexes. The molecular docking scores for the tested complexes were CDK4 (Score = −7.2 kcal/mol), EGFR (Score = −8.5 kcal/mol), frizzled (Score = −6.9 kcal/mol), IGFR (Score = −7.8 kcal/mol), KIT (Score = −6.5 kcal/mol), and MYC (Score = −8.3 kcal/mol). The binding mode demonstrated vital hydrogen bonds correlated with the observed energy gap. Notably, the calculated binding free energies of the tested compounds are as follows: CDK4 (ΔG = 24275.195 ± 6411.293 kJ/mol), EGFR (ΔG = 363273.625 ± 8731.466 kJ/mol), frizzled (ΔG = 181751.990 ± 28438.515 kJ/mol), IGFR (ΔG = 162414.725 ± 10728.367 kJ/mol), KIT (ΔG = 40162.585 ± 4331.017 kJ/mol), and MYC (ΔG = 434783.463 ± 53989.676 kJ/mol). Furthermore, through extensive 100 ns MD simulations, we observed the formation of a stable bevacizumab complex structure. The simulations confirmed the stability of the bevacizumab complex with the proto-oncogenes. The results of this study highlight the potential of bevacizumab complex as a promising candidate for anticancer treatment. The identification of hydrogen bonding, along with the calculated binding free energies and molecular docking scores, provides valuable insights into the molecular interactions and stability of the bevacizumab complexes. These findings and the extensive MD simulations open new avenues for future research and development of bevacizumab as a targeted therapy for breast cancer and other related malignancies.

Original language	English
Pages (from-to)	4814-4834
Number of pages	21
Journal	Journal of Biomolecular Structure and Dynamics
Volume	43
Issue number	9
DOIs	https://doi.org/10.1080/07391102.2024.2307445
State	Published - 2025

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Breast cancer
bevacizumab
molecular docking
molecular dynamic simulation

Access to Document

10.1080/07391102.2024.2307445

Cite this

@article{dd37ed581e134feca29d400c5fc3a685,

title = "Computational analysis of bevacizumab binding with protein receptors for its potential anticancer activity",

abstract = "Breast cancer poses a significant global challenge, prompting researchers to explore novel approaches for potential treatments. In this study, we investigated the binding free energy (ΔG) of bevacizumab, an anti-cancer therapy targeting angiogenesis through the inhibition of vascular endothelial growth factor (VEGF), with various proto-oncogenes including CDK4, EGFR, frizzled, IGFR, OmoMYC, and KIT. Our in-silico investigation revealed that hydrogen bonding is pivotal in inducing conformational changes within the DNA structure, impeding its replication and preventing cell death. Molecular docking results revealed the presence of crucial hydrogen bonds and supported the formation of stable bevacizumab complexes. The molecular docking scores for the tested complexes were CDK4 (Score = −7.2 kcal/mol), EGFR (Score = −8.5 kcal/mol), frizzled (Score = −6.9 kcal/mol), IGFR (Score = −7.8 kcal/mol), KIT (Score = −6.5 kcal/mol), and MYC (Score = −8.3 kcal/mol). The binding mode demonstrated vital hydrogen bonds correlated with the observed energy gap. Notably, the calculated binding free energies of the tested compounds are as follows: CDK4 (ΔG = 24275.195 ± 6411.293 kJ/mol), EGFR (ΔG = 363273.625 ± 8731.466 kJ/mol), frizzled (ΔG = 181751.990 ± 28438.515 kJ/mol), IGFR (ΔG = 162414.725 ± 10728.367 kJ/mol), KIT (ΔG = 40162.585 ± 4331.017 kJ/mol), and MYC (ΔG = 434783.463 ± 53989.676 kJ/mol). Furthermore, through extensive 100 ns MD simulations, we observed the formation of a stable bevacizumab complex structure. The simulations confirmed the stability of the bevacizumab complex with the proto-oncogenes. The results of this study highlight the potential of bevacizumab complex as a promising candidate for anticancer treatment. The identification of hydrogen bonding, along with the calculated binding free energies and molecular docking scores, provides valuable insights into the molecular interactions and stability of the bevacizumab complexes. These findings and the extensive MD simulations open new avenues for future research and development of bevacizumab as a targeted therapy for breast cancer and other related malignancies.",

keywords = "Breast cancer, bevacizumab, molecular docking, molecular dynamic simulation",

author = "Nada Alsakhen and Radwan, \{Enas S.\} and Imran Zafer and \{Abed alfattah\}, Husam and Shamkh, \{Israa M.\} and Rehman, \{Md Tabish\} and Moayad Shahwan and Khan, \{Khalid Ali\} and Ahmed, \{Shimaa A.\}",

note = "Publisher Copyright: {\textcopyright} 2024 Informa UK Limited, trading as Taylor \& Francis Group.",

year = "2025",

doi = "10.1080/07391102.2024.2307445",

language = "English",

volume = "43",

pages = "4814--4834",

journal = "Journal of Biomolecular Structure and Dynamics",

issn = "0739-1102",

publisher = "Taylor and Francis Ltd.",

number = "9",

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TY - JOUR

T1 - Computational analysis of bevacizumab binding with protein receptors for its potential anticancer activity

AU - Alsakhen, Nada

AU - Radwan, Enas S.

AU - Zafer, Imran

AU - Abed alfattah, Husam

AU - Shamkh, Israa M.

AU - Rehman, Md Tabish

AU - Shahwan, Moayad

AU - Khan, Khalid Ali

AU - Ahmed, Shimaa A.

PY - 2025

Y1 - 2025

N2 - Breast cancer poses a significant global challenge, prompting researchers to explore novel approaches for potential treatments. In this study, we investigated the binding free energy (ΔG) of bevacizumab, an anti-cancer therapy targeting angiogenesis through the inhibition of vascular endothelial growth factor (VEGF), with various proto-oncogenes including CDK4, EGFR, frizzled, IGFR, OmoMYC, and KIT. Our in-silico investigation revealed that hydrogen bonding is pivotal in inducing conformational changes within the DNA structure, impeding its replication and preventing cell death. Molecular docking results revealed the presence of crucial hydrogen bonds and supported the formation of stable bevacizumab complexes. The molecular docking scores for the tested complexes were CDK4 (Score = −7.2 kcal/mol), EGFR (Score = −8.5 kcal/mol), frizzled (Score = −6.9 kcal/mol), IGFR (Score = −7.8 kcal/mol), KIT (Score = −6.5 kcal/mol), and MYC (Score = −8.3 kcal/mol). The binding mode demonstrated vital hydrogen bonds correlated with the observed energy gap. Notably, the calculated binding free energies of the tested compounds are as follows: CDK4 (ΔG = 24275.195 ± 6411.293 kJ/mol), EGFR (ΔG = 363273.625 ± 8731.466 kJ/mol), frizzled (ΔG = 181751.990 ± 28438.515 kJ/mol), IGFR (ΔG = 162414.725 ± 10728.367 kJ/mol), KIT (ΔG = 40162.585 ± 4331.017 kJ/mol), and MYC (ΔG = 434783.463 ± 53989.676 kJ/mol). Furthermore, through extensive 100 ns MD simulations, we observed the formation of a stable bevacizumab complex structure. The simulations confirmed the stability of the bevacizumab complex with the proto-oncogenes. The results of this study highlight the potential of bevacizumab complex as a promising candidate for anticancer treatment. The identification of hydrogen bonding, along with the calculated binding free energies and molecular docking scores, provides valuable insights into the molecular interactions and stability of the bevacizumab complexes. These findings and the extensive MD simulations open new avenues for future research and development of bevacizumab as a targeted therapy for breast cancer and other related malignancies.

AB - Breast cancer poses a significant global challenge, prompting researchers to explore novel approaches for potential treatments. In this study, we investigated the binding free energy (ΔG) of bevacizumab, an anti-cancer therapy targeting angiogenesis through the inhibition of vascular endothelial growth factor (VEGF), with various proto-oncogenes including CDK4, EGFR, frizzled, IGFR, OmoMYC, and KIT. Our in-silico investigation revealed that hydrogen bonding is pivotal in inducing conformational changes within the DNA structure, impeding its replication and preventing cell death. Molecular docking results revealed the presence of crucial hydrogen bonds and supported the formation of stable bevacizumab complexes. The molecular docking scores for the tested complexes were CDK4 (Score = −7.2 kcal/mol), EGFR (Score = −8.5 kcal/mol), frizzled (Score = −6.9 kcal/mol), IGFR (Score = −7.8 kcal/mol), KIT (Score = −6.5 kcal/mol), and MYC (Score = −8.3 kcal/mol). The binding mode demonstrated vital hydrogen bonds correlated with the observed energy gap. Notably, the calculated binding free energies of the tested compounds are as follows: CDK4 (ΔG = 24275.195 ± 6411.293 kJ/mol), EGFR (ΔG = 363273.625 ± 8731.466 kJ/mol), frizzled (ΔG = 181751.990 ± 28438.515 kJ/mol), IGFR (ΔG = 162414.725 ± 10728.367 kJ/mol), KIT (ΔG = 40162.585 ± 4331.017 kJ/mol), and MYC (ΔG = 434783.463 ± 53989.676 kJ/mol). Furthermore, through extensive 100 ns MD simulations, we observed the formation of a stable bevacizumab complex structure. The simulations confirmed the stability of the bevacizumab complex with the proto-oncogenes. The results of this study highlight the potential of bevacizumab complex as a promising candidate for anticancer treatment. The identification of hydrogen bonding, along with the calculated binding free energies and molecular docking scores, provides valuable insights into the molecular interactions and stability of the bevacizumab complexes. These findings and the extensive MD simulations open new avenues for future research and development of bevacizumab as a targeted therapy for breast cancer and other related malignancies.

KW - Breast cancer

KW - bevacizumab

KW - molecular docking

KW - molecular dynamic simulation

UR - https://www.scopus.com/pages/publications/85183642531

U2 - 10.1080/07391102.2024.2307445

DO - 10.1080/07391102.2024.2307445

M3 - Article

C2 - 38281913

AN - SCOPUS:85183642531

SN - 0739-1102

VL - 43

SP - 4814

EP - 4834

JO - Journal of Biomolecular Structure and Dynamics

JF - Journal of Biomolecular Structure and Dynamics

IS - 9

ER -

Computational analysis of bevacizumab binding with protein receptors for its potential anticancer activity

Abstract

UN SDGs

Keywords

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