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About:
Glycopeptide Antibiotics Potently Inhibit Cathepsin L in the Late Endosome/Lysosome and Block the Entry of Ebola Virus, Middle East Respiratory Syndrome Coronavirus (MERS-CoV), and Severe Acute Respiratory Syndrome Coronavirus (SARS-CoV)
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An Entity of Type :
schema:ScholarlyArticle
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wasabi.inria.fr
associated with source
document(s)
Type:
Academic Article
research paper
schema:ScholarlyArticle
New Facet based on Instances of this Class
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type
Academic Article
research paper
schema:ScholarlyArticle
isDefinedBy
Covid-on-the-Web dataset
has title
Glycopeptide Antibiotics Potently Inhibit Cathepsin L in the Late Endosome/Lysosome and Block the Entry of Ebola Virus, Middle East Respiratory Syndrome Coronavirus (MERS-CoV), and Severe Acute Respiratory Syndrome Coronavirus (SARS-CoV)
Creator
Zhang, Xue
Zhang, Hui
Huang, Feng
Li, Qianwen
Pan, Ting
Zhang, Junsong
Bai, Chuan
Liu, Chao
Peng, Tao
Tao, Liang
Zhang, Jianhua
Zhou, Nan
Source
Medline; PMC
abstract
Ebola virus infection can cause severe hemorrhagic fever with a high mortality in humans. The outbreaks of Ebola viruses in 2014 represented the most serious Ebola epidemics in history and greatly threatened public health worldwide. The development of additional effective anti-Ebola therapeutic agents is therefore quite urgent. In this study, via high throughput screening of Food and Drug Administration-approved drugs, we identified that teicoplanin, a glycopeptide antibiotic, potently prevents the entry of Ebola envelope pseudotyped viruses into the cytoplasm. Furthermore, teicoplanin also has an inhibitory effect on transcription- and replication-competent virus-like particles, with an IC(50) as low as 330 nm. Comparative analysis further demonstrated that teicoplanin is able to block the entry of Middle East respiratory syndrome (MERS) and severe acute respiratory syndrome (SARS) envelope pseudotyped viruses as well. Teicoplanin derivatives such as dalbavancin, oritavancin, and telavancin can also inhibit the entry of Ebola, MERS, and SARS viruses. Mechanistic studies showed that teicoplanin blocks Ebola virus entry by specifically inhibiting the activity of cathepsin L, opening a novel avenue for the development of additional glycopeptides as potential inhibitors of cathepsin L-dependent viruses. Notably, given that teicoplanin has routinely been used in the clinic with low toxicity, our work provides a promising prospect for the prophylaxis and treatment of Ebola, MERS, and SARS virus infection.
has issue date
2016-03-07
(
xsd:dateTime
)
bibo:doi
10.1074/jbc.m116.716100
bibo:pmid
26953343
has license
bronze-oa
sha1sum (hex)
ebdc99b03d47e9b235e6b3f71a5032e5a4c221f0
schema:url
https://doi.org/10.1074/jbc.m116.716100
resource representing a document's title
Glycopeptide Antibiotics Potently Inhibit Cathepsin L in the Late Endosome/Lysosome and Block the Entry of Ebola Virus, Middle East Respiratory Syndrome Coronavirus (MERS-CoV), and Severe Acute Respiratory Syndrome Coronavirus (SARS-CoV)
has PubMed Central identifier
PMC4861487
has PubMed identifier
26953343
schema:publication
Journal of Biological Chemistry
resource representing a document's body
covid:ebdc99b03d47e9b235e6b3f71a5032e5a4c221f0#body_text
is
schema:about
of
named entity 'severe acute respiratory syndrome (SARS)'
named entity 'inhibiting'
named entity 'severe'
named entity 'high'
named entity 'outbreaks'
named entity 'study'
named entity 'MERS'
named entity 'telavancin'
named entity 'Mechanistic'
named entity 'GLYCOPEPTIDE ANTIBIOTICS'
named entity 'EBOLA VIRUS'
named entity 'VIRUS INFECTION'
named entity 'MORTALITY'
named entity 'TEICOPLANIN'
named entity 'PREVENTS'
named entity 'CAUSE'
named entity 'MERS'
named entity 'COMPARATIVE ANALYSIS'
named entity 'GLYCOPEPTIDE ANTIBIOTIC'
named entity 'EFFECTIVE'
named entity 'INHIBITING'
named entity 'SARS'
named entity 'DRUGS'
named entity 'STUDY'
named entity 'VIRUS ENTRY'
named entity 'APPROVED'
named entity 'ENTRY'
named entity 'SEVERE'
named entity 'IDENTIFIED'
named entity 'MIDDLE EAST RESPIRATORY SYNDROME CORONAVIRUS'
named entity 'ENTRY'
named entity 'EBOLA VIRUS'
named entity 'BLOCK'
named entity 'CATHEPSIN L'
named entity 'LATE ENDOSOME'
named entity 'COMPETENT'
named entity 'INHIBITORY EFFECT'
named entity '330'
named entity 'OUTBREAKS'
named entity 'BLOCKS'
named entity 'USED'
named entity 'GREATLY'
named entity 'HEMORRHAGIC FEVER'
named entity 'SEVERE ACUTE RESPIRATORY SYNDROME CORONAVIRUS'
named entity 'PROSPECT'
named entity 'TREATMENT'
named entity 'PROPHYLAXIS'
named entity 'ADDITIONAL'
named entity 'BLOCK'
named entity 'EFFECT ON TRANSCRIPTION'
named entity 'AVENUE'
named entity 'VIRUS-LIKE PARTICLES'
named entity 'EBOLA VIRUS INFECTION'
named entity 'HUMANS'
named entity 'NOVEL'
named entity 'FOOD AND DRUG ADMINISTRATION'
named entity 'MECHANISTIC STUDIES'
named entity 'TELAVANCIN'
named entity 'HIGH THROUGHPUT SCREENING'
named entity 'VIRUSES'
named entity 'OPENING'
named entity 'EBOLA'
named entity 'OUR'
named entity 'THERAPEUTIC AGENTS'
named entity 'CLINIC'
named entity 'ORITAVANCIN'
named entity 'ACTIVITY'
named entity 'CATHEPSIN L'
named entity 'HISTORY'
named entity 'LOW'
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