Your search keyword '"Sun, Cheng-Peng"' showing total 13 results

1. Discovery of New Iridoids as Farnesoid X Receptor Agonists from Morinda officinalis: Agonistic Potentials and Molecular Stimulation.

Author

Luan, Zhi‐Lin Please confirm that given names (blue) and surnames/family names (vermilion) have been identified correctly. -->, Qiao, Fei, Zhao, Wen‐Yu, Ming, Wen‐Hua, Yu, Zhen‐Long, Liu, Jie, Dai, Sheng‐Yun, Jiang, Shuang‐Hui, Lian, Chao‐Jie, Sun, Cheng‐Peng, Zhang, Bao‐Jing, Zheng, Jian, Ma, Shuang‐Cheng, and Ma, Xiao‐Chi

Subjects

FARNESOID X receptor, IRIDOIDS, AMINO acid residues, MOLECULAR docking, MOLECULAR dynamics, GLYCOSIDES, QUANTUM wells

Abstract

Main observation and conclusion: The investigation of Morinda officinalis led to the isolation of twelve compounds (1—12), including three new iridoid glycosides morindalins A—C (1—3) and nine known compounds (4—12). Their structural identifications were conducted using HRMS, 1D and 2D NMR, and electronic circular dichroism (ECD) spectra as well as quantum chemical computations. Compound 6 displayed the most significantly agonistic activity against farnesoid X receptor (FXR) with an EC50 value of 7.18 μM, and its agonistic effect was verified through the investigation of FXR downstream target genes including small heterodimer partner 1 (SHP1), bile salt export pump (BSEP), and organic solute transporter subunit alpha and beta (OSTα and OSTβ). The potential interaction of compound 6 with FXR was analyzed by molecular docking and molecular dynamics stimulation, revealing that amino acid residues Leu287, Thr288, and Ser332 played a crucial role in the activation of compound 6 towards FXR. These findings suggested that compound 6 could be regarded as a potential candidate for the development of FXR agonists. [ABSTRACT FROM AUTHOR]

Published

2021

2. Uncarialins J—M from Uncaria rhynchophylla and Their Anti‐depression Mechanism in Unpredictable Chronic Mild Stress‐Induced Mice via Activating 5‐HT1A Receptor.

Author

Yu, Zhen‐Long Please verify that the linked ORCID identifiers are correct for each author., Bai, Rong, Zhou, Jun‐Jun, Huang, Hui‐Lian, Zhao, Wen‐Yu, Huo, Xiao‐Kui, Yang, Ya‐Hui, Luan, Zhi‐Lin, Zhang, Bao‐Jing, Sun, Cheng‐Peng, and Ma, Xiao‐Chi

Subjects

MONOTERPENES, INDOLE alkaloids, CENTRAL nervous system diseases, AMINO acid residues, QUANTUM computing, PSYCHOLOGICAL stress

Abstract

Main observation and conclusion: Uncaria rhynchophylla has been widely used to treat central nervous system diseases for a long history. After investigation of U. rhynchophylla, eleven monoterpene indole alkaloids, including four new compounds uncarialins J—M (1—4) and seven known analogues (5—11), were isolated and identified. Their structural characterization was conducted using HRESIMS, 1D and 2D NMR, electronic circular dichroism (ECD) spectra, and quantum chemical computations. Compounds 1, 2, 7, and 9—11 displayed significant agonistic effects towards 5‐HT1A receptor, and their EC50 values were 7.86, 7.32, 2.24, 1.18, 1.52, and 3.75 μmol/L, respectively. Furthermore, in vivo experimental results fully revealed that hirsuteine (7) displayed a significant antidepression effect in unpredictable chronic mild stress (UCMS)‐induced depression mice mainly via regulating 5‐HT1A signaling pathway. Molecular docking and site‐directed amino acid mutation verified that amino acid residues Asp116 and Asn386 were the binding sites of hirsuteine (7) with 5‐HT1A receptor. In addition, pre‐treatment of mice with WAY 100635 also blocked the anti‐depression effect of hirsuteine (7), which further demonstrated that 5‐HT1A receptor was a potential target of hirsuteine (7) to effectively treat depression. These findings indicated the therapeutic material basis of U. rhynchophylla and the anti‐depression underlying mechanism of hirsuteine (7), and further provided the useful guidance for the development of hirsuteine (7) as a potential antidepressant candidate. [ABSTRACT FROM AUTHOR]

Published

2021

3. Bisfischoids A and B, dimeric ent-abietane-type diterpenoids with anti-inflammatory potential from Euphorbia fischeriana Steud.

Author

Sun, Cheng-Peng, Chang, Yi-Bo, Wang, Chao, Lv, Xia, Zhou, Wei-Yu, Tian, Xiang-Ge, Zhao, Wen-Yu, and Ma, Xiao-Chi

Subjects

*MOLECULAR kinetics, *EPOXIDE hydrolase, *MOLECULAR dynamics, *EUPHORBIA, *AMINO acid residues

Abstract

[Display omitted] • Rare diterpenoid dimers with nonacyclic skeleton were obtained from E. fischeriana. • Novel dimers 1 and 2 exhibited inhibitory activities against soluble epoxide hydrolase. • The inhibition kinetics and molecular dynamics of 1 and 2 with sEH were studied. Two undescribed ent -abietane-type diterpenoid dimers with nonacyclic backbone formed by intermolecular [4 + 2] cycloaddition into a spirocyclic skeleton, bisfischoids A (1) and B (2), along with a known one fischdiabietane A (3), were identified from Euphorbia fischeriana Steud. Their structures were elucidated by extensive spectroscopic analysis, ECD and NMR calculation combined with DP4+ probability analysis, as well as X-ray diffraction. The anti-inflammatory potential of dimers 1 – 3 were examined using their inhibitory effects on soluble epoxide hydrolase (sEH), which revealed that 1 and 2 exhibited promising activities with inhibition constant (K i) of 3.20 and 1.95 μM, respectively. Further studies of molecular docking and molecular dynamics indicated that amino acid residue Tyr343 in the catalytic cavity of sEH was the key site for their inhibitory function. [ABSTRACT FROM AUTHOR]

Published

2021

4. Protostane-type triterpenoids as natural soluble epoxide hydrolase inhibitors: Inhibition potentials and molecular dynamics.

Author

Sun, Cheng-Peng, Zhang, Juan, Zhao, Wen-Yu, Yi, Jing, Yan, Jian-Kun, Wang, Ya-Li, Morisseau, Christophe, Liu, Zhong-Bo, Hammock, Bruce D., and Ma, Xiao-Chi

Subjects

*EPOXIDE hydrolase, *MOLECULAR dynamics, *AMINO acid residues, *CHINESE medicine, *MOLECULAR docking

Abstract

• A small library of protostane-type triterpenoids (1 – 25) were isolated from A. orientale. • Compounds 1 , 4 , 5 , and 15 showed potential inhibitory activities against sEH. • The interaction of compound 5 with sEH were investigated by molecular docking and dynamics. • The Ki value of compound 5 was 3.48 μM. The inhibition of soluble epoxide hydrolase (sEH) is a promising therapeutic approach to treat inflammation and other disorders. In our present investigation on searching for sEH inhibitors from traditional Chinese medicines, we found that Alisma orientale displayed inhibition of sEH. We constructed a small library of protostane-type triterpenoids (1 – 25) isolated from A. orientale , and screened their inhibitory activities. Alismanin B (1), 11-deoxy-25-anhydro alisol E (4), 11-deoxy alisol B (5), and 25- O -ethyl alisol A (15) displayed concentration-dependently inhibitory activities against sEH with IC 50 values from 3.40 ± 0.57 μM to 9.57 ± 0.88 μM. 11-Deoxy-25-anhydro alisol E (4) and 11-deoxy alisol B (5) were defined as mixed-type competitive inhibitors with Ki values of 12.6 and 3.48 μM, respectively, based on the result of inhibition kinetics. The potential interaction mechanism of 11-deoxy alisol B (5) with sEH was analyzed by molecular docking and molecular dynamics, revealing that amino acid residues Trp336 and Tyr466 were vital for its inhibitory activity. [ABSTRACT FROM AUTHOR]

Published

2020

5. Amentoflavone from Selaginella tamariscina as a potent inhibitor of gut bacterial β-glucuronidase: Inhibition kinetics and molecular dynamics stimulation.

Author

Tian, Xiang-Ge, Yan, Jian-Kun, Sun, Cheng-Peng, Li, Jing-Xin, Ning, Jing, Wang, Chao, Huo, Xiao-Kui, Zhao, Wen-Yu, Yu, Zhen-Long, Feng, Lei, Lv, Xia, and Ma, Xiao-Chi

Subjects

*MOLECULAR kinetics, *XENOBIOTICS, *SELAGINELLA, *MOLECULAR docking, *FLUORESCENT probes, *AMINO acid residues, *MOLECULAR dynamics

Abstract

Gut bacterial β -glucuronidase (GUS) plays a pivotal role in the metabolism and reactivation of a vast of glucuronide conjugates of both endogenous and xenobiotic compounds in the gastrointestinal tract of human, which has been implicated in certain drug-induced gastrointestinal tract (GI) toxicity in clinic. Inhibitors of gut microbial GUS exhibited great potentials in relieving the drug-induced GI toxicity. In this study, Selaginella tamariscina and its major biflavonoid amentoflavone (AMF) were evaluated for their inhibitory activity against Escherichia coli GUS. Two selective probe substrates for GUS (a specific fluorescent probe substrate for GUS, DDAOG and a classical drug substrate for GUS, SN38G) were used in parallel for charactering the inhibition behaviors. Both the extract of S. tamariscina and its major biflavonoid AMF displayed evident inhibitory effects on GUS, and the IC 50 values of AMF against GUS mediated DDAOG and SN-38G hydrolysis were 0.62 and 0.49 μM, respectively. Inhibition kinetics studies indicated that AMF showed mixed type inhibition for GUS-mediated DDAOG hydrolysis, while displayed competitive type inhibition against GUS-mediated SN-38G hydrolysis, with the K i values of 0.24 and 1.25 μM, respectively. Molecular docking studies and molecular dynamics stimulation results clarified the role of amino acid residues Leu361, Ile363, and Glu413 in the inhibition of AMF on GUS. These results provided some foundations for the potential clinical utility of S. tamariscina and its major biflavonoid AMF for treating drug-induced enteropathy. [Display omitted] • Selaginell a tamariscina extract displayed strong inhibitory effects on GUS. •.►Amentoflavone was identified as the key inhibitory component in S. tamariscina. •.►The inhibition constant and the inhibition mechanism were well-characterized. [ABSTRACT FROM AUTHOR]

Published

2021

6. Natural soluble epoxide hydrolase inhibitors from Alisma orientale and their potential mechanism with soluble epoxide hydrolase.

Author

Zhao, Wen-Yu, Zhang, Xin-Yue, Zhou, Mei-Rong, Tian, Xiang-Ge, Lv, Xia, Zhang, Hou-Li, Deng, Sa, Zhang, Bao-Jing, Sun, Cheng-Peng, and Ma, Xiao-Chi

Subjects

*EPOXIDE hydrolase, *MOLECULAR dynamics, *AMINO acid residues, *SMALL molecules, *MOLECULAR docking

Abstract

Inhibition of soluble epoxide hydrolase (sEH) is considered to be an effective treatment for inflammation-related diseases, and small molecules origin from natural products show promising activity against sEH. Two undescribed protostanes, 3 β -hydroxy-25-anhydro-alisol F (1) and 3 β -hydroxy-alisol G (2) were isolated from Alisma orientale and identified as new sEH inhibitors with IC 50 values of 10.06 and 30.45 μM, respectively. Potential lead compound 1 was determined as an uncompetitive inhibitor against sEH, which had a K i value of 5.13 μM. In-depth molecular docking and molecular dynamics simulations revealed that amino acid residue Ser374 plays an important role in the inhibition of 1 , which also provides an idea for the development of sEH inhibitors based on protostane-type triterpenoids. [ABSTRACT FROM AUTHOR]

Published

2021

7. Investigation of the inhibitory effect of protostanes on human carboxylesterase 2 and their interaction: Inhibition kinetics and molecular stimulations.

Author

Lv, Xia, Bai, Rong, Yan, Jian-Kun, Huang, Hui-Lian, Huo, Xiao-Kui, Tian, Xiang-Ge, Zhao, Xin-Yu, Zhang, Bao-Jing, Zhao, Wen-Yu, and Sun, Cheng-Peng

Subjects

*MOLECULAR kinetics, *AMINO acid residues, *XENOBIOTICS, *MOLECULAR biology, *MOLECULAR docking, *FLUORESCENT probes

Abstract

Carboxylesterase 2 (CES 2), plays a pivotal role in endobiotic homeostasis and xenobiotic metabolism. Protostanes, the major constituents of the genus Alisma , display a series of pharmacological activities. Despite the extensive studies of pharmacological activities, the investigation on inhibitory effects of protostanes against CES 2 is rarely reported. In this study, the inhibitory activities of a library of protostanes (1–25) against human CES 2 were investigated for the first time, using 6,8-dichloro-9,9-dimethyl-7-oxo-7,9-dihydroacridin-2-yl benzoate (DDAB) as the specific fluorescent probe for human CES 2. Compounds 1 , 2 , 7 , 8 , 12 , 13 , 18 , 19 , and 25 showed strong inhibitory effects towards CES 2. For the most potent compounds 1 , 7 , 13 , and 25 , the inhibition kinetics were further investigated, and these four protostanes were all uncompetitive inhibitors against human CES 2 with the inhibition constant (K i) values ranging from 0.89 μM to 2.83 μM. In addition, molecular docking and molecular dynamics stimulation were employed to analyze the potential interactions between these protostanes and CES 2, and amino acid residue Gln422 was identified to play a crucial role in the strong inhibition of protostanes towards CES 2. [ABSTRACT FROM AUTHOR]

Published

2021

8. The inhibition effect of uncarialin A on voltage-dependent L-type calcium channel subunit alpha-1C: Inhibition potential and molecular stimulation.

Author

Yun, Wei-Jing, Zhang, Xin-Yue, Liu, Tian-Tian, Liang, Jia-Hao, Sun, Cheng-Peng, Yan, Jian-Kun, Huo, Xiao-Kui, Tian, Xiang-Ge, Zhang, Bao-Jing, Huang, Hui-Lian, and Ma, Xiao-Chi

Subjects

*CALCIUM channels, *VASCULAR smooth muscle, *AMINO acid residues, *MOLECULAR dynamics, *MESENTERIC artery, *CHINESE medicine, *BLOOD pressure

Abstract

Cardiovascular diseases, such as hypertension and cardiac failure, have become the most major and global cause for threatening human health in recent years. Uncaria rhynchophylla as a traditional Chinese medicine is widely used to treat hypertension for a long history, whereas its medicinal effective components and potential action mechanism are uncertain. Therefore, twenty-four alkaloids (1–24) isolated from U. rhynchophylla were assayed for their relaxant effects against phenylephrine (Phe)-induced contraction of rat mesenteric arteries. Among them, we surprisingly found that uncarialin A (21) exhibited most potent relaxation effect against Phe-induced contraction (IC 50 = 0.18 μM) in the manner of independent on endothelium-derived vasorelaxing factors and endothelium. All the experiments including measurement of Ca2+ in vascular smooth muscle cells (VSMCs) by fluorescence microscopy, whole-cell path clamp, molecular docking, and molecular dynamics, demonstrated that uncarialin A (21) could significantly inhibit L-type calcium channel subunit alpha-1C (Cav1.2) via the hydrogen bond interaction with amino acid residue Met1186, allowing the inhibition of Ca2+ inward current. Our results suggested that uncarialin A (21) could be served as a potential L-type Cav1.2 blocker in the effective treatment of cardiovascular diseases. [ABSTRACT FROM AUTHOR]

Published

2020

9. Natural soluble epoxide hydrolase inhibitors from Inula helenium and their interactions with soluble epoxide hydrolase.

Author

He, Xin, Zhao, Wen-Yu, Shao, Bo, Zhang, Bao-Jing, Liu, Tian-Tian, Sun, Cheng-Peng, Huang, Hui-Lian, Wu, Jia-Rong, Liang, Jia-Hao, and Ma, Xiao-Chi

Subjects

*EPOXIDE hydrolase, *LINOLEIC acid, *AMINO acid residues, *HYDROLASES, *CHINESE medicine, *MOLECULAR docking

Abstract

The inhibition of soluble epoxide hydrolase (sEH) is regarded as a promising therapeutic approach to treat inflammation and its related disorders. In present work, we investigated inhibitory effects of forty-nine kinds of traditional Chinese medicines against sEH. Inula helenium showed significant inhibitory effect against sEH, and the extract of I. helenium was isolated to obtain eight compounds, including 4 H -tomentosin (1), xanthalongin (2), linoleic acid (3), 8-hydroxy-9-isobutyryloxy-10(2)-methylbutyrylthymol (4), dehydrocostus lactone (5), alantolactone (6), costunolide (7), and isoalantolactone (8). Among them, 4 H -tomentosin (1), xanthalongin (2), and linoleic acid (3) showed significantly inhibitory activities on sEH with half maximal inhibitory concentration (IC 50) from 5.88 ± 0.97 μM to 11.63 ± 0.58 μM. The inhibition kinetics suggested that 4 H -tomentosin (1) and xanthalongin (2) were mixed-competitive type inhibitors with inhibition constants (K i) of 7.02 and 6.57 μM, respectively, and linoleic acid (3) was a competitive type inhibitor with a K i values of 3.52 μM. The potential interactions of 4 H -tomentosin (1), xanthalongin (2), and linoleic acid (3) with sEH were analyzed by molecular docking, which indicated that these bioactive compounds had interactions with key amino acid residues Tyr343, Ile363, Tyr383, and His524. • Eight compounds were isolated from I. helenium. • Compounds 1-3 could inhibit sEH activity with IC 50 values from 5.88 ± 0.97 μM to 11.63 ± 0.58 μM. • They were all mixed-competitive type inhibitor with Ki values from 3.52 μM to 7.02 μM • Molecular docking revealed interaction of compounds 1-3 with sEH. [ABSTRACT FROM AUTHOR]

Published

2020

10. Degradation profile of environmental pollutant 17β-estradiol by human intestinal fungus Aspergillus niger RG13B1 and characterization of genes involved in its degradation.

Author

Zhu, Qi-Meng, Wang, Chao, Liu, Jing-Wen, Zhang, Rui, Xin, Xiu-Lan, Zhang, Juan, Sun, Cheng-Peng, and Ma, Xiao-Chi

Subjects

*ASPERGILLUS niger, *POLLUTANTS, *ENVIRONMENTAL degradation, *AMINO acid residues, *XENOESTROGENS, *ENVIRONMENTAL security

Abstract

Environmental hormones have attracted more attention because of their adverse impact on the health and ecological security of human. Biodegradation is still an efficient tactics to remove environmental hormones, but human intestinal microbes remain to be elucidated in the role of their degradation. In the present work, we intended to perform the in vitro experiment for investigating the degradation of 17 β -estradiol, the main environmental estrogen, by human intestinal microflora Aspergillus niger RG13B1. Its degradation led to the production of eighteen metabolites characterized by 1H, 13C, and 2D NMR, and HRMS spectra, including nine new (1–9) and nine known metabolites (10–18). Based on their structures, the degradation pathway of 17 β -estradiol mediated by A. niger RG13B1 involved hydroxylation, oxidation, methylation, acetylation, and dehydrogenation, especially infrequent lactylation, and the key degradation enzymes were found in the gene cluster of A. niger. In addition, we found that metabolite 12 interacted with amino acid residues Lys37, Gln39, Lys93, and Asn115 of NF-κB p65 to suppress expressions of inflammatory genes or proteins, exerting its anti-inflammatory effect. This study first illustrated the role of human gut microbe in 17 β -estradiol degradation and provided new insights into its degradation mechanism by A. niger RG13B1. [Display omitted] • 17 β -Estradiol was degraded by human intestinal fungus A. niger RG13B1. • Its degradation pathway mainly involved hydroxylation, and oxidation. • The key enzymes were characterized in A. niger RG13B1. • Some metabolites displayed anti-inflammatory effects. [ABSTRACT FROM AUTHOR]

Published

2024

11. Inhibition effect of 1-acetoxy-6α-(2-methylbutyryl)eriolanolide toward soluble epoxide hydrolase: Multispectral analysis, molecular dynamics simulation, biochemical, and in vitro cell-based studies.

Author

Zhang, Juan, Yang, Fang-Yu, Zhu, Qi-Meng, Zhang, Wen-Hao, Zhang, Min, Yi, Jing, Wang, Yan, Zhang, Hou-Li, Liang, Guo-Biao, Yan, Jian-Kun, and Sun, Cheng-Peng

Subjects

*MOLECULAR dynamics, *EPOXIDE hydrolase, *AMINO acid residues, *BINDING site assay, *IN vitro studies, *INFLAMMATORY mediators

Abstract

Soluble epoxide hydrolase (sEH) serves as a potential target in inflammation-related diseases. Based on the bioactivity-guided separation, a new sesquiterpenoid inulajaponoid A (1) was isolated from Inula japonica with a sEH inhibitory effect, together with five known compounds, such as 1- O -acetyl-6- O -isobutyrylbritannilactone (2), 6 β -hydroxytomentosin (3), 1 β ,8 β -dihydroxyeudesma-4(15),11(13)-dien-12,6 α -olide (4), (4 S ,6 S ,7 S ,8 R)-1- O -acetyl-6- O -(3-methylvaleryloxy)-britannilactone (5), and 1-acetoxy-6 α -(2-methylbutyryl)eriolanolide (6). Among them, compounds 1 and 6 were assigned as mixed and uncompetitive inhibitors, respectively. The result of immunoprecipitation (IP)-MS demonstrated the specific binding of compound 6 to sEH in the complex system, which was further confirmed by the fluorescence-based binding assay showing its equilibrium dissociation constant (K d = 2.43 μM). The detail molecular stimulation revealed the mechanism of action of compound 6 with sEH through the hydrogen bond of amino acid residue Gln384. Furthermore, this natural sEH inhibitor (6) could suppress the MAPK/NF-κB activation to regulate inflammatory mediators, such as NO, TNF-α, and IL-6, which confirmed the anti-inflammatory effect of inhibition of sEH by 6. These findings provided a useful insight to develop sEH inhibitors upon the sesquiterpenoids. [ABSTRACT FROM AUTHOR]

Published

2023

12. Natural soluble epoxide hydrolase inhibitors from Inula britanica and their potential interactions with soluble epoxide hydrolase: Insight from inhibition kinetics and molecular dynamics.

Author

Zhao, Wen-Yu, Yan, Juan-Juan, Zhang, Min, Wang, Chao, Feng, Lei, Lv, Xia, Huo, Xiao-Kui, Sun, Cheng-Peng, Chen, Li-Xia, and Ma, Xiao-Chi

Subjects

*EPOXIDE hydrolase, *MOLECULAR dynamics, *MOLECULAR kinetics, *AMINO acid residues, *DRUG target, *ENANTIOMERS, *LIGNANS

Abstract

Soluble epoxide hydrolase (sEH) is a potential drug target to treat inflammation and neurodegenerative diseases. In this study, we found that the extract of Inula britanica exhibited significantly inhibitory effects against sEH, therefore, we investigated its phytochemical constituents to obtain seven new compounds together with sixteen known ones (1-20), including two pairs of novel enantiomers, (2S,3S)-britanicafanin A (1a), (2R,3R)-britanicafanin A (1b), (2R,3S)-britanicafanin B (2a), and (2S,3R)-britanicafanin B (2b), and three new lignans britanicafanins C-E (3–5). Their structures were determined by HRESIMS, 1D and 2D NMR, and electronic circular dichroism (ECD) spectra as well as quantum chemical computations. All the isolates were evaluated for their inhibitory effects against sEH, compounds 1 – 3 , 5 – 7 , 9 , 10 , 13 , 14 , and 17 – 20 showed significant inhibitory effects against sEH with IC 50 values from 3.56 μM to 26.93 μM. The inhibition kinetics results indicated that compounds 9 , 10 , 13 , and 19 were all uncompetitive inhibitors, and their inhibition constants (K i) values were 7.11, 1.99, 4.06, and 8.78 μM, respectively. Their potential interactions were analyzed by molecular docking and molecular dynamics (MD), which suggested that amino acid residues Asp335 and Asn359, especially Gln384, played an important role in the inhibition of compounds 10 and 13 on sEH, and compounds 10 and 13 could be considered as the potential candidates for the development of sEH inhibitors. • Seven new lignans together with 16 known ones were obtained from I. britanica. • Some of the isolates showed inhibitory effects against sEH with potential. • The inhibition kinetics and molecular dynamics of active compounds with sEH were studied. [ABSTRACT FROM AUTHOR]

Published

2021

13. Demethylbellidifolin isolated from Swertia bimaculate against human carboxylesterase 2: Kinetics and interaction mechanism merged with docking simulations.

Author

Liu, Tian-Tian, Huo, Xiao-Kui, Tian, Xiang-Ge, Liang, Jia-Hao, Yi, Jing, Zhang, Xin-Yue, Zhang, Song, Feng, Lei, Ning, Jing, Zhang, Bao-Jing, Sun, Cheng-Peng, and Ma, Xiao-Chi

Subjects

*SWERTIA, *AMINO acid residues, *CHINESE medicine, *MOLECULAR docking, *CELL imaging

Abstract

• Swertia bimaculata showed significant inhibition on HCE 2 at 10 μg/mL. • The extract of Swertia bimaculata was separated to afford demethylbellidifolin (1). • The inhibition kinetics of compound 1 against HCE 2 has been studied. • Molecular docking revealed interaction of compound 1 with HCE 2. In this study, forty-nine kinds of traditional Chinese medicines (TCMs) were evaluated for their inhibitory activities against human carboxylesterase 2 (HCE 2) using a human liver microsome (HLM) system. Swertia bimaculata showed significant inhibition on HCE 2 at 10 μg/mL among forty-nine kinds of TCMs. The extract of Swertia bimaculata was separated by preparative HPLC to afford demethylbellidifolin (1) identified by MS, 1H NMR, and 13C NMR spectra. Demethylbellidifolin (1) was assayed for its inhibitory HCE 2 effect by HCE 2-mediated DDAB hydrolysis, and its potential IC 50 value was 3.12 ± 0.64 μM. Demethylbellidifolin (1) was assigned as a mixed-type competitive inhibitor with the inhibiton constant Ki value of 6.87 µM by Lineweaver-Burk and slope plots. Living cell imaging was conducted to corroborate its inhibitory HCE 2 activity. Molecular docking indicated potential interactions of demethylbellidifolin (1) with HCE 2 through two hydrogen bonds of the C-3 and C-5 hydroxy groups with amino acid residues Glu227 and Ser228 in the catalytic cavity, respectively. [ABSTRACT FROM AUTHOR]

Published

2019