Design, synthesis, and biological evaluation of crenatoside analogues as novel influenza neuraminidase inhibitors.
Identifieur interne : 001050 ( Main/Exploration ); précédent : 001049; suivant : 001051Design, synthesis, and biological evaluation of crenatoside analogues as novel influenza neuraminidase inhibitors.
Auteurs : Bao-Long Chen [République populaire de Chine] ; Ya-Jing Wang [République populaire de Chine] ; Hong Guo [République populaire de Chine] ; Guang-Yao Zeng [République populaire de Chine]Source :
- European journal of medicinal chemistry [ 1768-3254 ] ; 2016.
Descripteurs français
- KwdFr :
- Acides caféiques (), Acides caféiques (pharmacologie), Antienzymes (), Antienzymes (pharmacologie), Antiviraux (), Antiviraux (pharmacologie), Conception de médicament, Glucosides (), Glucosides (pharmacologie), Grippe humaine (traitement médicamenteux), Grippe humaine (virologie), Humains, Modèles moléculaires, Relation structure-activité, Sialidase (antagonistes et inhibiteurs), Sialidase (métabolisme), Sous-type H1N1 du virus de la grippe A (), Sous-type H1N1 du virus de la grippe A (enzymologie), Virus de la grippe A (), Virus de la grippe A (enzymologie).
- MESH :
- antagonistes et inhibiteurs : Sialidase.
- enzymologie : Sous-type H1N1 du virus de la grippe A, Virus de la grippe A.
- métabolisme : Sialidase.
- pharmacologie : Acides caféiques, Antienzymes, Antiviraux, Glucosides.
- traitement médicamenteux : Grippe humaine.
- virologie : Grippe humaine.
- Acides caféiques, Antienzymes, Antiviraux, Conception de médicament, Glucosides, Humains, Modèles moléculaires, Relation structure-activité, Sous-type H1N1 du virus de la grippe A, Virus de la grippe A.
English descriptors
- KwdEn :
- Antiviral Agents (chemistry), Antiviral Agents (pharmacology), Caffeic Acids (chemistry), Caffeic Acids (pharmacology), Drug Design, Enzyme Inhibitors (chemistry), Enzyme Inhibitors (pharmacology), Glucosides (chemistry), Glucosides (pharmacology), Humans, Influenza A Virus, H1N1 Subtype (drug effects), Influenza A Virus, H1N1 Subtype (enzymology), Influenza A virus (drug effects), Influenza A virus (enzymology), Influenza, Human (drug therapy), Influenza, Human (virology), Models, Molecular, Neuraminidase (antagonists & inhibitors), Neuraminidase (metabolism), Structure-Activity Relationship.
- MESH :
- chemical , antagonists & inhibitors : Neuraminidase.
- chemical , chemistry : Antiviral Agents, Caffeic Acids, Enzyme Inhibitors, Glucosides.
- chemical , metabolism : Neuraminidase.
- chemical , pharmacology : Antiviral Agents, Caffeic Acids, Enzyme Inhibitors, Glucosides.
- drug effects : Influenza A Virus, H1N1 Subtype, Influenza A virus.
- drug therapy : Influenza, Human.
- enzymology : Influenza A Virus, H1N1 Subtype, Influenza A virus.
- virology : Influenza, Human.
- Drug Design, Humans, Models, Molecular, Structure-Activity Relationship.
Abstract
Natural products, especially derived from TCMH, have been found to exert antiviral effects against influenza virus. Crenatoside, a phenylethanoid glycoside from Pogostemon cablin Benth, which has been shown as a novel effective NA inhibitor previously, is considered as the leading compound for our further SARs studies. This work presented design, synthesis of novel crenatoside analogues from readily available d-Glucose and l-rhamnose in a convergent manner. Furthermore, their biological activities and SARs were also investigated. Especially, compound 2 h showed impressive IC50 = 27.77 μg/mL against NAs, which is 3 folds more potent than the leading compound crenatoside (IC50 = 89.81 μg/mL). These results would promise their therapeutic potential for influenza disease.
DOI: 10.1016/j.ejmech.2015.12.031
PubMed: 26774928
Affiliations:
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Le document en format XML
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<front><div type="abstract" xml:lang="en">Natural products, especially derived from TCMH, have been found to exert antiviral effects against influenza virus. Crenatoside, a phenylethanoid glycoside from Pogostemon cablin Benth, which has been shown as a novel effective NA inhibitor previously, is considered as the leading compound for our further SARs studies. This work presented design, synthesis of novel crenatoside analogues from readily available d-Glucose and l-rhamnose in a convergent manner. Furthermore, their biological activities and SARs were also investigated. Especially, compound 2 h showed impressive IC50 = 27.77 μg/mL against NAs, which is 3 folds more potent than the leading compound crenatoside (IC50 = 89.81 μg/mL). These results would promise their therapeutic potential for influenza disease. </div>
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