Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis

The Huashi Baidu Formula (HSBDF), a key Chinese medical drug, has a remarkable clinical efficacy in treating acute lung injury (ALI), and it has been officially approved by the National Medical Products Administration of China for drug clinical trials. Nevertheless, the regulated mechanisms of HSBDF...

Descripción completa

Detalles Bibliográficos
Autores principales: Wang, Yanru, Jin, Xiaojie, Fan, Qin, Li, Chenghao, Zhang, Min, Wang, Yongfeng, Wu, Qingfeng, Li, Jiawei, Liu, Xiuzhu, Wang, Siyu, Wang, Yu, Li, Ling, Ling, Jia, Li, Chaoxin, Wang, Qianqian, Liu, Yongqi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9201258/
https://www.ncbi.nlm.nih.gov/pubmed/35721141
http://dx.doi.org/10.3389/fphar.2022.879268
_version_ 1784728269061357568
author Wang, Yanru
Jin, Xiaojie
Fan, Qin
Li, Chenghao
Zhang, Min
Wang, Yongfeng
Wu, Qingfeng
Li, Jiawei
Liu, Xiuzhu
Wang, Siyu
Wang, Yu
Li, Ling
Ling, Jia
Li, Chaoxin
Wang, Qianqian
Liu, Yongqi
author_facet Wang, Yanru
Jin, Xiaojie
Fan, Qin
Li, Chenghao
Zhang, Min
Wang, Yongfeng
Wu, Qingfeng
Li, Jiawei
Liu, Xiuzhu
Wang, Siyu
Wang, Yu
Li, Ling
Ling, Jia
Li, Chaoxin
Wang, Qianqian
Liu, Yongqi
author_sort Wang, Yanru
collection PubMed
description The Huashi Baidu Formula (HSBDF), a key Chinese medical drug, has a remarkable clinical efficacy in treating acute lung injury (ALI), and it has been officially approved by the National Medical Products Administration of China for drug clinical trials. Nevertheless, the regulated mechanisms of HSBDF and its active compounds in plasma against ALI were rarely studied. Based on these considerations, the key anti-inflammatory compounds of HSBDF were screened by molecular docking and binding free energy. The key compounds were further identified in plasma by LC/MS. Network pharmacology was employed to identify the potential regulatory mechanism of the key compounds in plasma. Next, the network pharmacological prediction was validated by a series of experimental assays, including CCK-8, EdU staining, test of TNF-α, IL-6, MDA, and T-SOD, and flow cytometry, to identify active compounds. Molecular dynamic simulation and binding interaction patterns were used to evaluate the stability and affinity between active compounds and target. Finally, the active compounds were subjected to predict pharmacokinetic properties. Molecular docking revealed that HSBDF had potential effects of inhibiting inflammation by acting on IL-6R and TNF-α. Piceatannol, emodin, aloe-emodin, rhein, physcion, luteolin, and quercetin were key compounds that may ameliorate ALI, and among which, there were five compounds (emodin, aloe-emodin, rhein, luteolin, and quercetin) in plasma. Network pharmacology results suggested that five key compounds in plasma likely inhibited ALI by regulating inflammation and oxidative damage. Test performed in vitro suggested that HSBDF (0.03125 mg/ml), quercetin (1.5625 μM), emodin (3.125 μM), and rhein (1.5625 μM) have anti-inflammatory function against oxidative damage and decrease apoptosis in an inflammatory environment by LPS-stimulation. In addition, active compounds (quercetin, emodin, and rhein) had good development prospects, fine affinity, and stable conformations with the target protein. In summary, this study suggested that HSBDF and its key active components in plasma (quercetin, emodin, and rhein) can decrease levels of pro-inflammatory factors (IL-6 and TNF-α), decrease expression of MDA, increase expression of T-SOD, and decrease cell apoptosis in an inflammatory environment. These data suggest that HSBDF has significant effect on anti-inflammation and anti-oxidative stress and also can decrease cell apoptosis in treating ALI. These findings provided an important strategy for developing new agents and facilitated clinical use of HSBDF against ALI.
format Online
Article
Text
id pubmed-9201258
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-92012582022-06-17 Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis Wang, Yanru Jin, Xiaojie Fan, Qin Li, Chenghao Zhang, Min Wang, Yongfeng Wu, Qingfeng Li, Jiawei Liu, Xiuzhu Wang, Siyu Wang, Yu Li, Ling Ling, Jia Li, Chaoxin Wang, Qianqian Liu, Yongqi Front Pharmacol Pharmacology The Huashi Baidu Formula (HSBDF), a key Chinese medical drug, has a remarkable clinical efficacy in treating acute lung injury (ALI), and it has been officially approved by the National Medical Products Administration of China for drug clinical trials. Nevertheless, the regulated mechanisms of HSBDF and its active compounds in plasma against ALI were rarely studied. Based on these considerations, the key anti-inflammatory compounds of HSBDF were screened by molecular docking and binding free energy. The key compounds were further identified in plasma by LC/MS. Network pharmacology was employed to identify the potential regulatory mechanism of the key compounds in plasma. Next, the network pharmacological prediction was validated by a series of experimental assays, including CCK-8, EdU staining, test of TNF-α, IL-6, MDA, and T-SOD, and flow cytometry, to identify active compounds. Molecular dynamic simulation and binding interaction patterns were used to evaluate the stability and affinity between active compounds and target. Finally, the active compounds were subjected to predict pharmacokinetic properties. Molecular docking revealed that HSBDF had potential effects of inhibiting inflammation by acting on IL-6R and TNF-α. Piceatannol, emodin, aloe-emodin, rhein, physcion, luteolin, and quercetin were key compounds that may ameliorate ALI, and among which, there were five compounds (emodin, aloe-emodin, rhein, luteolin, and quercetin) in plasma. Network pharmacology results suggested that five key compounds in plasma likely inhibited ALI by regulating inflammation and oxidative damage. Test performed in vitro suggested that HSBDF (0.03125 mg/ml), quercetin (1.5625 μM), emodin (3.125 μM), and rhein (1.5625 μM) have anti-inflammatory function against oxidative damage and decrease apoptosis in an inflammatory environment by LPS-stimulation. In addition, active compounds (quercetin, emodin, and rhein) had good development prospects, fine affinity, and stable conformations with the target protein. In summary, this study suggested that HSBDF and its key active components in plasma (quercetin, emodin, and rhein) can decrease levels of pro-inflammatory factors (IL-6 and TNF-α), decrease expression of MDA, increase expression of T-SOD, and decrease cell apoptosis in an inflammatory environment. These data suggest that HSBDF has significant effect on anti-inflammation and anti-oxidative stress and also can decrease cell apoptosis in treating ALI. These findings provided an important strategy for developing new agents and facilitated clinical use of HSBDF against ALI. Frontiers Media S.A. 2022-06-02 /pmc/articles/PMC9201258/ /pubmed/35721141 http://dx.doi.org/10.3389/fphar.2022.879268 Text en Copyright © 2022 Wang, Jin, Fan, Li, Zhang, Wang, Wu, Li, Liu, Wang, Wang, Li, Ling, Li, Wang and Liu. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Wang, Yanru
Jin, Xiaojie
Fan, Qin
Li, Chenghao
Zhang, Min
Wang, Yongfeng
Wu, Qingfeng
Li, Jiawei
Liu, Xiuzhu
Wang, Siyu
Wang, Yu
Li, Ling
Ling, Jia
Li, Chaoxin
Wang, Qianqian
Liu, Yongqi
Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis
title Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis
title_full Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis
title_fullStr Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis
title_full_unstemmed Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis
title_short Deciphering the Active Compounds and Mechanisms of HSBDF for Treating ALI via Integrating Chemical Bioinformatics Analysis
title_sort deciphering the active compounds and mechanisms of hsbdf for treating ali via integrating chemical bioinformatics analysis
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9201258/
https://www.ncbi.nlm.nih.gov/pubmed/35721141
http://dx.doi.org/10.3389/fphar.2022.879268
work_keys_str_mv AT wangyanru decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT jinxiaojie decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT fanqin decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT lichenghao decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT zhangmin decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT wangyongfeng decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT wuqingfeng decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT lijiawei decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT liuxiuzhu decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT wangsiyu decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT wangyu decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT liling decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT lingjia decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT lichaoxin decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT wangqianqian decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis
AT liuyongqi decipheringtheactivecompoundsandmechanismsofhsbdffortreatingaliviaintegratingchemicalbioinformaticsanalysis

Ejemplares similares