Mechanism of interactions of dsDNA binding with quercetin and its two novel sulfonate derivatives using multispectroscopic, voltammetric, and molecular docking studies

Büşra Bekar-Yıldırmaz; Pelin Şenel; Taner Erdoğan; Filiz Altay; Ayşegül Gölcü

doi:10.1016/j.molstruc.2022.134718

Mechanism of interactions of dsDNA binding with quercetin and its two novel sulfonate derivatives using multispectroscopic, voltammetric, and molecular docking studies

Büşra Bekar-Yıldırmaz, Pelin Şenel, Taner Erdoğan, Filiz Altay, Ayşegül Gölcü^*

^*Corresponding author for this work

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

1 Citation (Scopus)

Abstract

Flavonoids have an important place in chemistry and pharmacology. Several flavonoids, especially Quercetin, have the potential to form molecular complexes with nucleic acid structure and have recently attracted attention due to their prospective clinical and pharmacological uses. DNA is the main target for a wide variety of therapeutic agents. Therefore, there is great interest in studies of binding small molecules with DNA. The interaction of small molecules with DNA provides a structural guide in rational drug design and the synthesis of new and improved drugs with enhanced selective activity and higher clinical efficacy. Even if newly synthesized candidate drug molecules with small molecular weight are capable of indirectly interacting with DNA, the mechanisms that accomplish this need to be clearly known. In this study, the mechanism of fish sperm double strain deoxyribonucleic acid (dsDNA) binding with Quercetin (QCR) and its two novel sulfonate derivatives (quercetin mesylate (QMS) and quercetin tosylate-A (QTS-A)) were researched. For investigating the interaction between the molecules and dsDNA was studied by analytical (spectrophotometric, viscosimetric, and electrochemical) methods. The interaction of dsDNA and two quercetin sulfonate derivatives were compared with the interaction of the QCR standard after all experimental studies. Moreover, the DNA binding constants K_b were determined using each method. The K_b constants calculated for QCR, QMS, and QTS-A are in harmony for all techniques. The results showed that QCR binds to dsDNA via intercalation mode, while QMS and QTS-A bind through minor groove binding mode. In addition to experimental studies, theoretical studies were conducted at room temperature under physiological conditions (pH 7.4). Molecular docking calculations and molecular dynamics (MD) simulations have been found to be compatible with experimental studies.

Original language	English
Article number	134718
Journal	Journal of Molecular Structure
Volume	1276
DOIs	https://doi.org/10.1016/j.molstruc.2022.134718
Publication status	Published - 15 Mar 2023

Bibliographical note

Publisher Copyright:
© 2022

Funding

We are grateful to Prof. Omowunmi Sadik (New Jersey Institute of Technology, University Heights, USA) for sending us the materials they synthesized in her laboratories to be used in our studies upon request. The authors would like to thank the support of the grant of Istanbul Technical University (Scientific Research Projects Unit) under the TYL-2019-42132 project and for all experimental conditions (Lab L-105 belonging to Prof. Gölcü). We deeply thank Assoc. Prof. Bunyamin Karagoz for the fluorescence experiments and Assoc. Prof. Altug Mert Sevim for the FTIR experiments that were done in their laboratories. The computational studies reported in this paper were partially performed at TUBITAK ULAKBIM, High Performance and Grid Computing Center (TRUBA resources) and Kocaeli University.

Funders	Funder number
TUBITAK ULAKBIM
Kocaeli Üniversitesi
Istanbul Teknik Üniversitesi	TYL-2019-42132

Keywords

dsDNA
Flavonoids
Molecular Docking
Quercetin
Spectroscopy
Sulfonate
Voltammetry

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@article{65491e300bc7416680de0566853c712d,

title = "Mechanism of interactions of dsDNA binding with quercetin and its two novel sulfonate derivatives using multispectroscopic, voltammetric, and molecular docking studies",

abstract = "Flavonoids have an important place in chemistry and pharmacology. Several flavonoids, especially Quercetin, have the potential to form molecular complexes with nucleic acid structure and have recently attracted attention due to their prospective clinical and pharmacological uses. DNA is the main target for a wide variety of therapeutic agents. Therefore, there is great interest in studies of binding small molecules with DNA. The interaction of small molecules with DNA provides a structural guide in rational drug design and the synthesis of new and improved drugs with enhanced selective activity and higher clinical efficacy. Even if newly synthesized candidate drug molecules with small molecular weight are capable of indirectly interacting with DNA, the mechanisms that accomplish this need to be clearly known. In this study, the mechanism of fish sperm double strain deoxyribonucleic acid (dsDNA) binding with Quercetin (QCR) and its two novel sulfonate derivatives (quercetin mesylate (QMS) and quercetin tosylate-A (QTS-A)) were researched. For investigating the interaction between the molecules and dsDNA was studied by analytical (spectrophotometric, viscosimetric, and electrochemical) methods. The interaction of dsDNA and two quercetin sulfonate derivatives were compared with the interaction of the QCR standard after all experimental studies. Moreover, the DNA binding constants Kb were determined using each method. The Kb constants calculated for QCR, QMS, and QTS-A are in harmony for all techniques. The results showed that QCR binds to dsDNA via intercalation mode, while QMS and QTS-A bind through minor groove binding mode. In addition to experimental studies, theoretical studies were conducted at room temperature under physiological conditions (pH 7.4). Molecular docking calculations and molecular dynamics (MD) simulations have been found to be compatible with experimental studies.",

keywords = "dsDNA, Flavonoids, Molecular Docking, Quercetin, Spectroscopy, Sulfonate, Voltammetry",

author = "B{\"u}{\c s}ra Bekar-Yıldırmaz and Pelin {\c S}enel and Taner Erdoğan and Filiz Altay and Ay{\c s}eg{\"u}l G{\"o}lc{\"u}",

note = "Publisher Copyright: {\textcopyright} 2022",

year = "2023",

month = mar,

day = "15",

doi = "10.1016/j.molstruc.2022.134718",

language = "English",

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Mechanism of interactions of dsDNA binding with quercetin and its two novel sulfonate derivatives using multispectroscopic, voltammetric, and molecular docking studies. / Bekar-Yıldırmaz, Büşra; Şenel, Pelin; Erdoğan, Taner et al.
In: Journal of Molecular Structure, Vol. 1276, 134718, 15.03.2023.

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

TY - JOUR

T1 - Mechanism of interactions of dsDNA binding with quercetin and its two novel sulfonate derivatives using multispectroscopic, voltammetric, and molecular docking studies

AU - Bekar-Yıldırmaz, Büşra

AU - Şenel, Pelin

AU - Erdoğan, Taner

AU - Altay, Filiz

AU - Gölcü, Ayşegül

PY - 2023/3/15

Y1 - 2023/3/15

N2 - Flavonoids have an important place in chemistry and pharmacology. Several flavonoids, especially Quercetin, have the potential to form molecular complexes with nucleic acid structure and have recently attracted attention due to their prospective clinical and pharmacological uses. DNA is the main target for a wide variety of therapeutic agents. Therefore, there is great interest in studies of binding small molecules with DNA. The interaction of small molecules with DNA provides a structural guide in rational drug design and the synthesis of new and improved drugs with enhanced selective activity and higher clinical efficacy. Even if newly synthesized candidate drug molecules with small molecular weight are capable of indirectly interacting with DNA, the mechanisms that accomplish this need to be clearly known. In this study, the mechanism of fish sperm double strain deoxyribonucleic acid (dsDNA) binding with Quercetin (QCR) and its two novel sulfonate derivatives (quercetin mesylate (QMS) and quercetin tosylate-A (QTS-A)) were researched. For investigating the interaction between the molecules and dsDNA was studied by analytical (spectrophotometric, viscosimetric, and electrochemical) methods. The interaction of dsDNA and two quercetin sulfonate derivatives were compared with the interaction of the QCR standard after all experimental studies. Moreover, the DNA binding constants Kb were determined using each method. The Kb constants calculated for QCR, QMS, and QTS-A are in harmony for all techniques. The results showed that QCR binds to dsDNA via intercalation mode, while QMS and QTS-A bind through minor groove binding mode. In addition to experimental studies, theoretical studies were conducted at room temperature under physiological conditions (pH 7.4). Molecular docking calculations and molecular dynamics (MD) simulations have been found to be compatible with experimental studies.

AB - Flavonoids have an important place in chemistry and pharmacology. Several flavonoids, especially Quercetin, have the potential to form molecular complexes with nucleic acid structure and have recently attracted attention due to their prospective clinical and pharmacological uses. DNA is the main target for a wide variety of therapeutic agents. Therefore, there is great interest in studies of binding small molecules with DNA. The interaction of small molecules with DNA provides a structural guide in rational drug design and the synthesis of new and improved drugs with enhanced selective activity and higher clinical efficacy. Even if newly synthesized candidate drug molecules with small molecular weight are capable of indirectly interacting with DNA, the mechanisms that accomplish this need to be clearly known. In this study, the mechanism of fish sperm double strain deoxyribonucleic acid (dsDNA) binding with Quercetin (QCR) and its two novel sulfonate derivatives (quercetin mesylate (QMS) and quercetin tosylate-A (QTS-A)) were researched. For investigating the interaction between the molecules and dsDNA was studied by analytical (spectrophotometric, viscosimetric, and electrochemical) methods. The interaction of dsDNA and two quercetin sulfonate derivatives were compared with the interaction of the QCR standard after all experimental studies. Moreover, the DNA binding constants Kb were determined using each method. The Kb constants calculated for QCR, QMS, and QTS-A are in harmony for all techniques. The results showed that QCR binds to dsDNA via intercalation mode, while QMS and QTS-A bind through minor groove binding mode. In addition to experimental studies, theoretical studies were conducted at room temperature under physiological conditions (pH 7.4). Molecular docking calculations and molecular dynamics (MD) simulations have been found to be compatible with experimental studies.

KW - dsDNA

KW - Flavonoids

KW - Molecular Docking

KW - Quercetin

KW - Spectroscopy

KW - Sulfonate

KW - Voltammetry

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DO - 10.1016/j.molstruc.2022.134718

M3 - Article

AN - SCOPUS:85145584532

SN - 0022-2860

VL - 1276

JO - Journal of Molecular Structure

JF - Journal of Molecular Structure

M1 - 134718

ER -

Mechanism of interactions of dsDNA binding with quercetin and its two novel sulfonate derivatives using multispectroscopic, voltammetric, and molecular docking studies

Abstract

Bibliographical note

Funding

Keywords

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