Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap)

Sui Lin Mo; Wei Feng Liu; Yuling Chen; Hai Bin Luo; Lai Bao Sun; Xiao Wu Chen; Zhi Wei Zhou; Kevin B. Sneed; Chun Guang Li; Yao Min Du; Jun Liang; Shu Feng Zhou

doi:10.2174/138620712798280826

Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap)

Sui Lin Mo, Wei Feng Liu, Yuling Chen, Hai Bin Luo, Lai Bao Sun, Xiao Wu Chen, Zhi Wei Zhou, Kevin B. Sneed, Chun Guang Li, Yao Min Du, Jun Liang, Shu Feng Zhou

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

21 Scopus citations

Abstract

We have previously examined the binding patterns of various substrates to human cytochrome P450 2D6 (CYP2D6) using a series of molecular modeling methods. In this study, we further explored the binding modes of various types of inhibitors to CYP2D6 using a combination of ligand- and protein-based modeling approaches. Firstly, we developed and validated a pharmacophore model for CYP2D6 inhibitors, which consisted of two hydrophobic features and one hydrogen bond acceptor feature. Secondly, we constructed and validated a quantitative structure-activity relationship (QSAR) model for CYP2D6 inhibitors which gave a poor to moderate prediction accuracy. Thirdly, a panel of CYP2D6 inhibitors were subject to molecular docking into the active site of wild-type and mutated CYP2D6 enzyme. We demonstrated that 8 residues in the active site (Leu213, Glu216, Ser217, Gln244, Asp301, Ser304, Ala305, and Phe483) played an important role in the binding to the inhibitors via hydrogen bond formation and/or π-π stacking interaction. Apparent changes in the binding modes of the inhibitors have been observed with Phe120Ile, Glu216Asp, Asp301Glu mutations in CYP2D6. Finally, we screened for potential binders/inhibitors from the Chinese herbal medicine Scutellaria baicalensis (Huangqin, Baikal Skullcap) using the established pharmacophore model for CYP2D6 inhibitors and molecular docking approach. Overall, 18 out of 40 compounds from S. baicalensis were mapped to the pharmacophore model of CYP2D6 inhibitors and most herbal compounds from S. baicalensis could be docked into the active site of CYP2D6. Our study has provided insights into the molecular mechanisms of interaction of synthetic and herbal compounds with human CYP2D6 and further benchmarking studies are needed to validate our modeling and virtual screening results.

Original language	English (US)
Pages (from-to)	36-80
Number of pages	45
Journal	Combinatorial Chemistry and High Throughput Screening
Volume	15
Issue number	1
DOIs	https://doi.org/10.2174/138620712798280826
State	Published - Jan 2012
Externally published	Yes

Keywords

CYP2D6
Chinese herbal medicine
Inhibitor
Molecular docking
Pharmacophore
QSAR
Virtual screening

ASJC Scopus subject areas

Drug Discovery
Computer Science Applications
Organic Chemistry

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Mo, S. L., Liu, W. F., Chen, Y., Luo, H. B., Sun, L. B., Chen, X. W., Zhou, Z. W., Sneed, K. B., Li, C. G., Du, Y. M., Liang, J., & Zhou, S. F. (2012). Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap). Combinatorial Chemistry and High Throughput Screening, 15(1), 36-80. https://doi.org/10.2174/138620712798280826

Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap). / Mo, Sui Lin; Liu, Wei Feng; Chen, Yuling et al.
In: Combinatorial Chemistry and High Throughput Screening, Vol. 15, No. 1, 01.2012, p. 36-80.

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

Mo, SL, Liu, WF, Chen, Y, Luo, HB, Sun, LB, Chen, XW, Zhou, ZW, Sneed, KB, Li, CG, Du, YM, Liang, J & Zhou, SF 2012, 'Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap)', Combinatorial Chemistry and High Throughput Screening, vol. 15, no. 1, pp. 36-80. https://doi.org/10.2174/138620712798280826

Mo SL, Liu WF, Chen Y, Luo HB, Sun LB, Chen XW et al. Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap). Combinatorial Chemistry and High Throughput Screening. 2012 Jan;15(1):36-80. doi: 10.2174/138620712798280826

Mo, Sui Lin ; Liu, Wei Feng ; Chen, Yuling et al. / Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap). In: Combinatorial Chemistry and High Throughput Screening. 2012 ; Vol. 15, No. 1. pp. 36-80.

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abstract = "We have previously examined the binding patterns of various substrates to human cytochrome P450 2D6 (CYP2D6) using a series of molecular modeling methods. In this study, we further explored the binding modes of various types of inhibitors to CYP2D6 using a combination of ligand- and protein-based modeling approaches. Firstly, we developed and validated a pharmacophore model for CYP2D6 inhibitors, which consisted of two hydrophobic features and one hydrogen bond acceptor feature. Secondly, we constructed and validated a quantitative structure-activity relationship (QSAR) model for CYP2D6 inhibitors which gave a poor to moderate prediction accuracy. Thirdly, a panel of CYP2D6 inhibitors were subject to molecular docking into the active site of wild-type and mutated CYP2D6 enzyme. We demonstrated that 8 residues in the active site (Leu213, Glu216, Ser217, Gln244, Asp301, Ser304, Ala305, and Phe483) played an important role in the binding to the inhibitors via hydrogen bond formation and/or π-π stacking interaction. Apparent changes in the binding modes of the inhibitors have been observed with Phe120Ile, Glu216Asp, Asp301Glu mutations in CYP2D6. Finally, we screened for potential binders/inhibitors from the Chinese herbal medicine Scutellaria baicalensis (Huangqin, Baikal Skullcap) using the established pharmacophore model for CYP2D6 inhibitors and molecular docking approach. Overall, 18 out of 40 compounds from S. baicalensis were mapped to the pharmacophore model of CYP2D6 inhibitors and most herbal compounds from S. baicalensis could be docked into the active site of CYP2D6. Our study has provided insights into the molecular mechanisms of interaction of synthetic and herbal compounds with human CYP2D6 and further benchmarking studies are needed to validate our modeling and virtual screening results.",

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author = "Mo, {Sui Lin} and Liu, {Wei Feng} and Yuling Chen and Luo, {Hai Bin} and Sun, {Lai Bao} and Chen, {Xiao Wu} and Zhou, {Zhi Wei} and Sneed, {Kevin B.} and Li, {Chun Guang} and Du, {Yao Min} and Jun Liang and Zhou, {Shu Feng}",

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AU - Mo, Sui Lin

AU - Liu, Wei Feng

AU - Chen, Yuling

AU - Luo, Hai Bin

AU - Sun, Lai Bao

AU - Chen, Xiao Wu

AU - Zhou, Zhi Wei

AU - Sneed, Kevin B.

AU - Li, Chun Guang

AU - Du, Yao Min

AU - Liang, Jun

AU - Zhou, Shu Feng

PY - 2012/1

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AB - We have previously examined the binding patterns of various substrates to human cytochrome P450 2D6 (CYP2D6) using a series of molecular modeling methods. In this study, we further explored the binding modes of various types of inhibitors to CYP2D6 using a combination of ligand- and protein-based modeling approaches. Firstly, we developed and validated a pharmacophore model for CYP2D6 inhibitors, which consisted of two hydrophobic features and one hydrogen bond acceptor feature. Secondly, we constructed and validated a quantitative structure-activity relationship (QSAR) model for CYP2D6 inhibitors which gave a poor to moderate prediction accuracy. Thirdly, a panel of CYP2D6 inhibitors were subject to molecular docking into the active site of wild-type and mutated CYP2D6 enzyme. We demonstrated that 8 residues in the active site (Leu213, Glu216, Ser217, Gln244, Asp301, Ser304, Ala305, and Phe483) played an important role in the binding to the inhibitors via hydrogen bond formation and/or π-π stacking interaction. Apparent changes in the binding modes of the inhibitors have been observed with Phe120Ile, Glu216Asp, Asp301Glu mutations in CYP2D6. Finally, we screened for potential binders/inhibitors from the Chinese herbal medicine Scutellaria baicalensis (Huangqin, Baikal Skullcap) using the established pharmacophore model for CYP2D6 inhibitors and molecular docking approach. Overall, 18 out of 40 compounds from S. baicalensis were mapped to the pharmacophore model of CYP2D6 inhibitors and most herbal compounds from S. baicalensis could be docked into the active site of CYP2D6. Our study has provided insights into the molecular mechanisms of interaction of synthetic and herbal compounds with human CYP2D6 and further benchmarking studies are needed to validate our modeling and virtual screening results.

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Ligand- and protein-based modeling studies of the inhibitors of human cytochrome P450 2D6 and a virtual screening for potential inhibitors from the Chinese herbal medicine, Scutellaria baicalensis (Huangqin, Baikal Skullcap)

Abstract

Keywords

ASJC Scopus subject areas

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