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Biophysical and computational characterization of vandetanib–lysozyme interaction

Interaction of an anticancer drug, vandetanib (VDB) with a ligand transporter, lysozyme (LYZ) was explored using multispectroscopic techniques, such as fluorescence, absorption and circular dichroism along with computational analysis. Fluorescence data and absorption results confirmed VDB–LYZ comple...

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Main Authors: Kabir, Md Zahirul, Hamzah, Nur Aziean, Ghani, Hamidah, Mohamad, Saharuddin, Alias, Zazali, Tayyab, Saad
Format: Article
Published: Elsevier 2018
Subjects:
Q Science (General)
QH Natural history
Online Access:http://eprints.um.edu.my/21726/
https://doi.org/10.1016/j.saa.2017.08.051
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spelling my.um.eprints.217262019-07-31T03:33:08Z http://eprints.um.edu.my/21726/ Biophysical and computational characterization of vandetanib–lysozyme interaction Kabir, Md Zahirul Hamzah, Nur Aziean Ghani, Hamidah Mohamad, Saharuddin Alias, Zazali Tayyab, Saad Q Science (General) QH Natural history Interaction of an anticancer drug, vandetanib (VDB) with a ligand transporter, lysozyme (LYZ) was explored using multispectroscopic techniques, such as fluorescence, absorption and circular dichroism along with computational analysis. Fluorescence data and absorption results confirmed VDB–LYZ complexation. VDB-induced quenching was characterized as static quenching based on inverse correlation of KSV with temperature as well as kq values. The complex was characterized by the weak binding constant (Ka = 4.96–3.14 × 103 M−1). Thermodynamic data (ΔS = + 12.82 J mol−1 K−1; ΔH = − 16.73 kJ mol−1) of VDB–LYZ interaction revealed participation of hydrophobic and van der Waals forces along with hydrogen bonds in VDB–LYZ complexation. Microenvironmental perturbations around tryptophan and tyrosine residues as well as secondary and tertiary structural alterations in LYZ upon addition of VDB were evident from the 3-D fluorescence, far- and near-UV CD spectral analyses, respectively. Interestingly, addition of VDB to LYZ significantly increased protein's thermostability. Molecular docking results suggested the location of VDB binding site near the LYZ active site while molecular dynamics simulation results suggested stability of VDB–LYZ complex. Presence of Mg2+, Ba2+ and Zn2+ was found to interfere with VDB–LYZ interaction. Elsevier 2018 Article PeerReviewed Kabir, Md Zahirul and Hamzah, Nur Aziean and Ghani, Hamidah and Mohamad, Saharuddin and Alias, Zazali and Tayyab, Saad (2018) Biophysical and computational characterization of vandetanib–lysozyme interaction. Spectrochimica Acta Part A: Molecular and Biomolecular Spectroscopy, 189. pp. 485-494. ISSN 1386-1425 https://doi.org/10.1016/j.saa.2017.08.051 doi:10.1016/j.saa.2017.08.051
institution Universiti Malaya
building UM Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Malaya
content_source UM Research Repository
url_provider http://eprints.um.edu.my/
topic Q Science (General)
QH Natural history
spellingShingle Q Science (General)
QH Natural history
Kabir, Md Zahirul
Hamzah, Nur Aziean
Ghani, Hamidah
Mohamad, Saharuddin
Alias, Zazali
Tayyab, Saad
Biophysical and computational characterization of vandetanib–lysozyme interaction
description Interaction of an anticancer drug, vandetanib (VDB) with a ligand transporter, lysozyme (LYZ) was explored using multispectroscopic techniques, such as fluorescence, absorption and circular dichroism along with computational analysis. Fluorescence data and absorption results confirmed VDB–LYZ complexation. VDB-induced quenching was characterized as static quenching based on inverse correlation of KSV with temperature as well as kq values. The complex was characterized by the weak binding constant (Ka = 4.96–3.14 × 103 M−1). Thermodynamic data (ΔS = + 12.82 J mol−1 K−1; ΔH = − 16.73 kJ mol−1) of VDB–LYZ interaction revealed participation of hydrophobic and van der Waals forces along with hydrogen bonds in VDB–LYZ complexation. Microenvironmental perturbations around tryptophan and tyrosine residues as well as secondary and tertiary structural alterations in LYZ upon addition of VDB were evident from the 3-D fluorescence, far- and near-UV CD spectral analyses, respectively. Interestingly, addition of VDB to LYZ significantly increased protein's thermostability. Molecular docking results suggested the location of VDB binding site near the LYZ active site while molecular dynamics simulation results suggested stability of VDB–LYZ complex. Presence of Mg2+, Ba2+ and Zn2+ was found to interfere with VDB–LYZ interaction.
format Article
author Kabir, Md Zahirul
Hamzah, Nur Aziean
Ghani, Hamidah
Mohamad, Saharuddin
Alias, Zazali
Tayyab, Saad
author_facet Kabir, Md Zahirul
Hamzah, Nur Aziean
Ghani, Hamidah
Mohamad, Saharuddin
Alias, Zazali
Tayyab, Saad
author_sort Kabir, Md Zahirul
title Biophysical and computational characterization of vandetanib–lysozyme interaction
title_short Biophysical and computational characterization of vandetanib–lysozyme interaction
title_full Biophysical and computational characterization of vandetanib–lysozyme interaction
title_fullStr Biophysical and computational characterization of vandetanib–lysozyme interaction
title_full_unstemmed Biophysical and computational characterization of vandetanib–lysozyme interaction
title_sort biophysical and computational characterization of vandetanib–lysozyme interaction
publisher Elsevier
publishDate 2018
url http://eprints.um.edu.my/21726/
https://doi.org/10.1016/j.saa.2017.08.051
_version_ 1643691643046461440
score 13.214268

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