Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening

Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening

Adlay (Coix larchryma-jobi L.) was the commonly used Traditional Chinese Medicine (TCM) with high content of seed storage protein. The hydrolyzed bioactive oligopeptides of adlay have been proven to be anti-hypertensive effective components. However, the structures and anti-hypertensive mechanism of...

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Main Authors: Liansheng Qiao, Bin Li, Yankun Chen, Lingling Li, Xi Chen, Lingzhi Wang, Fang Lu, Ganggang Luo, Gongyu Li, Yanling Zhang
Format: Article
Language:English
Published: MDPI AG 2016-12-01
Series:International Journal of Molecular Sciences
Subjects:
adlay
hypertension
oligopeptides
angiotensin-I converting enzyme (ACE)
in silico proteolysis
molecular dynamics (MD)
Online Access:http://www.mdpi.com/1422-0067/17/12/2099
id doaj-4af08b4a0d1a4ab58c629edef7355f26
record_format Article
collection DOAJ
language English
format Article
sources DOAJ
author Liansheng Qiao
Bin Li
Yankun Chen
Lingling Li
Xi Chen
Lingzhi Wang
Fang Lu
Ganggang Luo
Gongyu Li
Yanling Zhang
spellingShingle Liansheng Qiao
Bin Li
Yankun Chen
Lingling Li
Xi Chen
Lingzhi Wang
Fang Lu
Ganggang Luo
Gongyu Li
Yanling Zhang
Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening
International Journal of Molecular Sciences
adlay
hypertension
oligopeptides
angiotensin-I converting enzyme (ACE)
in silico proteolysis
molecular dynamics (MD)
author_facet Liansheng Qiao
Bin Li
Yankun Chen
Lingling Li
Xi Chen
Lingzhi Wang
Fang Lu
Ganggang Luo
Gongyu Li
Yanling Zhang
author_sort Liansheng Qiao
title Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening
title_short Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening
title_full Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening
title_fullStr Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening
title_full_unstemmed Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual Screening
title_sort discovery of anti-hypertensive oligopeptides from adlay based on in silico proteolysis and virtual screening
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2016-12-01
description Adlay (Coix larchryma-jobi L.) was the commonly used Traditional Chinese Medicine (TCM) with high content of seed storage protein. The hydrolyzed bioactive oligopeptides of adlay have been proven to be anti-hypertensive effective components. However, the structures and anti-hypertensive mechanism of bioactive oligopeptides from adlay were not clear. To discover the definite anti-hypertensive oligopeptides from adlay, in silico proteolysis and virtual screening were implemented to obtain potential oligopeptides, which were further identified by biochemistry assay and molecular dynamics simulation. In this paper, ten sequences of adlay prolamins were collected and in silico hydrolyzed to construct the oligopeptide library with 134 oligopeptides. This library was reverse screened by anti-hypertensive pharmacophore database, which was constructed by our research team and contained ten anti-hypertensive targets. Angiotensin-I converting enzyme (ACE) was identified as the main potential target for the anti-hypertensive activity of adlay oligopeptides. Three crystal structures of ACE were utilized for docking studies and 19 oligopeptides were finally identified with potential ACE inhibitory activity. According to mapping features and evaluation indexes of pharmacophore and docking, three oligopeptides were selected for biochemistry assay. An oligopeptide sequence, NPATY (IC50 = 61.88 ± 2.77 µM), was identified as the ACE inhibitor by reverse-phase high performance liquid chromatography (RP-HPLC) assay. Molecular dynamics simulation of NPATY was further utilized to analyze interactive bonds and key residues. ALA354 was identified as a key residue of ACE inhibitors. Hydrophobic effect of VAL518 and electrostatic effects of HIS383, HIS387, HIS513 and Zn2+ were also regarded as playing a key role in inhibiting ACE activities. This study provides a research strategy to explore the pharmacological mechanism of Traditional Chinese Medicine (TCM) proteins based on in silico proteolysis and virtual screening, which could be beneficial to reveal the pharmacological action of TCM proteins and provide new lead compounds for peptides-based drug design.
topic adlay
hypertension
oligopeptides
angiotensin-I converting enzyme (ACE)
in silico proteolysis
molecular dynamics (MD)
url http://www.mdpi.com/1422-0067/17/12/2099
work_keys_str_mv AT lianshengqiao discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
AT binli discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
AT yankunchen discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
AT linglingli discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
AT xichen discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
AT lingzhiwang discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
AT fanglu discoveryofantihypertensiveoligopeptidesfromadlaybasedoninsilicoproteolysisandvirtualscreening
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spelling doaj-4af08b4a0d1a4ab58c629edef7355f262020-11-24T22:23:50ZengMDPI AGInternational Journal of Molecular Sciences1422-00672016-12-011712209910.3390/ijms17122099ijms17122099Discovery of Anti-Hypertensive Oligopeptides from Adlay Based on In Silico Proteolysis and Virtual ScreeningLiansheng Qiao0Bin Li1Yankun Chen2Lingling Li3Xi Chen4Lingzhi Wang5Fang Lu6Ganggang Luo7Gongyu Li8Yanling Zhang9Key Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaKey Laboratory of TCM Foundation and New Drug Research, School of Chinese Material Medica, University of Chinese Medicine, Beijing 100102, ChinaAdlay (Coix larchryma-jobi L.) was the commonly used Traditional Chinese Medicine (TCM) with high content of seed storage protein. The hydrolyzed bioactive oligopeptides of adlay have been proven to be anti-hypertensive effective components. However, the structures and anti-hypertensive mechanism of bioactive oligopeptides from adlay were not clear. To discover the definite anti-hypertensive oligopeptides from adlay, in silico proteolysis and virtual screening were implemented to obtain potential oligopeptides, which were further identified by biochemistry assay and molecular dynamics simulation. In this paper, ten sequences of adlay prolamins were collected and in silico hydrolyzed to construct the oligopeptide library with 134 oligopeptides. This library was reverse screened by anti-hypertensive pharmacophore database, which was constructed by our research team and contained ten anti-hypertensive targets. Angiotensin-I converting enzyme (ACE) was identified as the main potential target for the anti-hypertensive activity of adlay oligopeptides. Three crystal structures of ACE were utilized for docking studies and 19 oligopeptides were finally identified with potential ACE inhibitory activity. According to mapping features and evaluation indexes of pharmacophore and docking, three oligopeptides were selected for biochemistry assay. An oligopeptide sequence, NPATY (IC50 = 61.88 ± 2.77 µM), was identified as the ACE inhibitor by reverse-phase high performance liquid chromatography (RP-HPLC) assay. Molecular dynamics simulation of NPATY was further utilized to analyze interactive bonds and key residues. ALA354 was identified as a key residue of ACE inhibitors. Hydrophobic effect of VAL518 and electrostatic effects of HIS383, HIS387, HIS513 and Zn2+ were also regarded as playing a key role in inhibiting ACE activities. This study provides a research strategy to explore the pharmacological mechanism of Traditional Chinese Medicine (TCM) proteins based on in silico proteolysis and virtual screening, which could be beneficial to reveal the pharmacological action of TCM proteins and provide new lead compounds for peptides-based drug design.http://www.mdpi.com/1422-0067/17/12/2099adlayhypertensionoligopeptidesangiotensin-I converting enzyme (ACE)in silico proteolysismolecular dynamics (MD)

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