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Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies

Multiple spectroscopic techniques, such as fluorescence, absorption, and circular dichroism along with in silico studies were used to characterize the binding of a potent inhibitor molecule, CCG1423 to the major transport protein, human serum albumin (HSA). Fluorescence and absorption spectroscopic...

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Main Authors: Kabir, Md Zahirul, Ghani, Hamidah, Mohamad, Saharuddin, Alias, Zazali, Tayyab, Saad
Format: Article
Published: Taylor & Francis 2018
Subjects:
Q Science (General)
QH Natural history
Online Access:http://eprints.um.edu.my/21725/
https://doi.org/10.1080/07391102.2017.1360207
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spelling my.um.eprints.217252019-07-31T03:27:45Z http://eprints.um.edu.my/21725/ Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies Kabir, Md Zahirul Ghani, Hamidah Mohamad, Saharuddin Alias, Zazali Tayyab, Saad Q Science (General) QH Natural history Multiple spectroscopic techniques, such as fluorescence, absorption, and circular dichroism along with in silico studies were used to characterize the binding of a potent inhibitor molecule, CCG1423 to the major transport protein, human serum albumin (HSA). Fluorescence and absorption spectroscopic results confirmed CCG1423–HSA complex formation. A strong binding affinity stabilized the CCG1423–HSA complex, as evident from the values of the binding constant (Ka = 1.35 × 106–5.43 × 105 M−1). The KSV values for CCG1423–HSA system were inversely correlated with temperature, suggesting the involvement of static quenching mechanism. Thermodynamic data anticipated that CCG1423–HSA complexation was mainly driven by hydrophobic and van der Waals forces as well as hydrogen bonds. In silico analysis also supported these results. Three-dimensional fluorescence and circular dichroism spectral analysis suggested microenvironmental perturbations around protein fluorophores and structural (secondary and tertiary) changes in the protein upon CCG1423 binding. CCG1423 binding to HSA also showed some protection against thermal denaturation. Site-specific marker-induced displacement results revealed CCG1423 binding to Sudlow’s site I of HSA, which was also confirmed by the computational results. A few common ions were also found to interfere with the CCG1423–HSA interaction. Taylor & Francis 2018 Article PeerReviewed Kabir, Md Zahirul and Ghani, Hamidah and Mohamad, Saharuddin and Alias, Zazali and Tayyab, Saad (2018) Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies. Journal of Biomolecular Structure and Dynamics, 36 (10). pp. 2495-2507. ISSN 0739-1102 https://doi.org/10.1080/07391102.2017.1360207 doi:10.1080/07391102.2017.1360207
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
Ghani, Hamidah
Mohamad, Saharuddin
Alias, Zazali
Tayyab, Saad
Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies
description Multiple spectroscopic techniques, such as fluorescence, absorption, and circular dichroism along with in silico studies were used to characterize the binding of a potent inhibitor molecule, CCG1423 to the major transport protein, human serum albumin (HSA). Fluorescence and absorption spectroscopic results confirmed CCG1423–HSA complex formation. A strong binding affinity stabilized the CCG1423–HSA complex, as evident from the values of the binding constant (Ka = 1.35 × 106–5.43 × 105 M−1). The KSV values for CCG1423–HSA system were inversely correlated with temperature, suggesting the involvement of static quenching mechanism. Thermodynamic data anticipated that CCG1423–HSA complexation was mainly driven by hydrophobic and van der Waals forces as well as hydrogen bonds. In silico analysis also supported these results. Three-dimensional fluorescence and circular dichroism spectral analysis suggested microenvironmental perturbations around protein fluorophores and structural (secondary and tertiary) changes in the protein upon CCG1423 binding. CCG1423 binding to HSA also showed some protection against thermal denaturation. Site-specific marker-induced displacement results revealed CCG1423 binding to Sudlow’s site I of HSA, which was also confirmed by the computational results. A few common ions were also found to interfere with the CCG1423–HSA interaction.
format Article
author Kabir, Md Zahirul
Ghani, Hamidah
Mohamad, Saharuddin
Alias, Zazali
Tayyab, Saad
author_facet Kabir, Md Zahirul
Ghani, Hamidah
Mohamad, Saharuddin
Alias, Zazali
Tayyab, Saad
author_sort Kabir, Md Zahirul
title Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies
title_short Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies
title_full Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies
title_fullStr Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies
title_full_unstemmed Interactive association between RhoA transcriptional signaling inhibitor, CCG1423 and human serum albumin: Biophysical and in silico studies
title_sort interactive association between rhoa transcriptional signaling inhibitor, ccg1423 and human serum albumin: biophysical and in silico studies
publisher Taylor & Francis
publishDate 2018
url http://eprints.um.edu.my/21725/
https://doi.org/10.1080/07391102.2017.1360207
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score 13.159267

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