1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity

The 1-cinnamoyl-3,11-dihydroxymeliacarpin (CDM), isolated from extracts of Melia azedarach L., displays antiviral and immunomodulating properties. CDM is the first reported tetranortriterpenoid responsible for the alkalinization of intracellular compartments affecting both, viral endocytic and exocy...

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Autores principales: Bueno, C.A., Alché, L.E., Barquero, A.A.
Formato: JOUR
Materias:
Antiviral
Golgi apparatus
Medicinal plants
Secretory pathway
Transferrin receptor
1 cinnamoyl 3,11 dihydroxymeliacarpin
concanamycin A
glycoprotein
Melia azedarach extract
monensin
transferrin receptor
triterpenoid
unclassified drug
alkalinization
article
cell compartmentalization
cell membrane
controlled study
cytotoxicity
drug activity
drug inhibition
endosome
glycoprotein synthesis
Herpes simplex virus 1
human
human cell
immunomodulation
integument
Melia azedarach
membrane transport
nonhuman
priority journal
protein binding
protein localization
protein transport
virogenesis
virus capsid
Antiviral Agents
Cell Line
Glycoproteins
Herpesvirus 1, Human
Humans
Limonins
Macrolides
Monensin
Protein Transport
Receptors, Transferrin
Tumor Necrosis Factor-alpha
Viral Envelope Proteins
Virus Replication
Human herpesvirus 1
Miridae
Acceso en línea:http://hdl.handle.net/20.500.12110/paper_0006291X_v393_n1_p32_Bueno
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Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA) de Universidad de Buenos Aires
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spelling todo:paper_0006291X_v393_n1_p32_Bueno2023-10-03T14:03:56Z 1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity Bueno, C.A. Alché, L.E. Barquero, A.A. Antiviral Golgi apparatus Medicinal plants Secretory pathway Transferrin receptor 1 cinnamoyl 3,11 dihydroxymeliacarpin concanamycin A glycoprotein Melia azedarach extract monensin transferrin receptor triterpenoid unclassified drug alkalinization article cell compartmentalization cell membrane controlled study cytotoxicity drug activity drug inhibition endosome glycoprotein synthesis Herpes simplex virus 1 human human cell immunomodulation integument Melia azedarach membrane transport nonhuman priority journal protein binding protein localization protein transport virogenesis virus capsid Antiviral Agents Cell Line Glycoproteins Herpesvirus 1, Human Humans Limonins Macrolides Melia azedarach Monensin Protein Transport Receptors, Transferrin Tumor Necrosis Factor-alpha Viral Envelope Proteins Virus Replication Human herpesvirus 1 Melia azedarach Miridae The 1-cinnamoyl-3,11-dihydroxymeliacarpin (CDM), isolated from extracts of Melia azedarach L., displays antiviral and immunomodulating properties. CDM is the first reported tetranortriterpenoid responsible for the alkalinization of intracellular compartments affecting both, viral endocytic and exocytic pathways. Considering that viral glycoprotein synthesis is completely dependent upon cellular membrane trafficking, we questioned whether CDM might also interfere with the normal transport of cellular glycoproteins. This study demonstrates that CDM promoted a transient block in the transport of two cellular glycoproteins, the transferrin receptor (TfR) and TNF-α. Nevertheless, CDM did not affect the transferrin binding ability of TfR and did not impede the TNF-α secretion. On the other hand, CDM disturbed the intracellular localization of capsid, glycoprotein and tegument proteins simultaneously in the same HSV-1 infected cells. Besides, we show that concanamycin A and monensin provoke a permanent blockage of viral and cellular glycoproteins, in contrast to the delay observed after CDM treatment. Thus, the delay on glycoprotein transport caused by CDM would account for the strong inhibition on virus multiplication without interfering with the bioactivity of cellular glycoproteins. © 2010 Elsevier Inc. All rights reserved. Fil:Bueno, C.A. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales; Argentina. Fil:Alché, L.E. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales; Argentina. Fil:Barquero, A.A. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales; Argentina. JOUR info:eu-repo/semantics/openAccess http://creativecommons.org/licenses/by/2.5/ar http://hdl.handle.net/20.500.12110/paper_0006291X_v393_n1_p32_Bueno
institution Universidad de Buenos Aires
institution_str I-28
repository_str R-134
collection Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA)
topic Antiviral
Golgi apparatus
Medicinal plants
Secretory pathway
Transferrin receptor
1 cinnamoyl 3,11 dihydroxymeliacarpin
concanamycin A
glycoprotein
Melia azedarach extract
monensin
transferrin receptor
triterpenoid
unclassified drug
alkalinization
article
cell compartmentalization
cell membrane
controlled study
cytotoxicity
drug activity
drug inhibition
endosome
glycoprotein synthesis
Herpes simplex virus 1
human
human cell
immunomodulation
integument
Melia azedarach
membrane transport
nonhuman
priority journal
protein binding
protein localization
protein transport
virogenesis
virus capsid
Antiviral Agents
Cell Line
Glycoproteins
Herpesvirus 1, Human
Humans
Limonins
Macrolides
Melia azedarach
Monensin
Protein Transport
Receptors, Transferrin
Tumor Necrosis Factor-alpha
Viral Envelope Proteins
Virus Replication
Human herpesvirus 1
Melia azedarach
Miridae
spellingShingle Antiviral
Golgi apparatus
Medicinal plants
Secretory pathway
Transferrin receptor
1 cinnamoyl 3,11 dihydroxymeliacarpin
concanamycin A
glycoprotein
Melia azedarach extract
monensin
transferrin receptor
triterpenoid
unclassified drug
alkalinization
article
cell compartmentalization
cell membrane
controlled study
cytotoxicity
drug activity
drug inhibition
endosome
glycoprotein synthesis
Herpes simplex virus 1
human
human cell
immunomodulation
integument
Melia azedarach
membrane transport
nonhuman
priority journal
protein binding
protein localization
protein transport
virogenesis
virus capsid
Antiviral Agents
Cell Line
Glycoproteins
Herpesvirus 1, Human
Humans
Limonins
Macrolides
Melia azedarach
Monensin
Protein Transport
Receptors, Transferrin
Tumor Necrosis Factor-alpha
Viral Envelope Proteins
Virus Replication
Human herpesvirus 1
Melia azedarach
Miridae
Bueno, C.A.
Alché, L.E.
Barquero, A.A.
1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
topic_facet Antiviral
Golgi apparatus
Medicinal plants
Secretory pathway
Transferrin receptor
1 cinnamoyl 3,11 dihydroxymeliacarpin
concanamycin A
glycoprotein
Melia azedarach extract
monensin
transferrin receptor
triterpenoid
unclassified drug
alkalinization
article
cell compartmentalization
cell membrane
controlled study
cytotoxicity
drug activity
drug inhibition
endosome
glycoprotein synthesis
Herpes simplex virus 1
human
human cell
immunomodulation
integument
Melia azedarach
membrane transport
nonhuman
priority journal
protein binding
protein localization
protein transport
virogenesis
virus capsid
Antiviral Agents
Cell Line
Glycoproteins
Herpesvirus 1, Human
Humans
Limonins
Macrolides
Melia azedarach
Monensin
Protein Transport
Receptors, Transferrin
Tumor Necrosis Factor-alpha
Viral Envelope Proteins
Virus Replication
Human herpesvirus 1
Melia azedarach
Miridae
description The 1-cinnamoyl-3,11-dihydroxymeliacarpin (CDM), isolated from extracts of Melia azedarach L., displays antiviral and immunomodulating properties. CDM is the first reported tetranortriterpenoid responsible for the alkalinization of intracellular compartments affecting both, viral endocytic and exocytic pathways. Considering that viral glycoprotein synthesis is completely dependent upon cellular membrane trafficking, we questioned whether CDM might also interfere with the normal transport of cellular glycoproteins. This study demonstrates that CDM promoted a transient block in the transport of two cellular glycoproteins, the transferrin receptor (TfR) and TNF-α. Nevertheless, CDM did not affect the transferrin binding ability of TfR and did not impede the TNF-α secretion. On the other hand, CDM disturbed the intracellular localization of capsid, glycoprotein and tegument proteins simultaneously in the same HSV-1 infected cells. Besides, we show that concanamycin A and monensin provoke a permanent blockage of viral and cellular glycoproteins, in contrast to the delay observed after CDM treatment. Thus, the delay on glycoprotein transport caused by CDM would account for the strong inhibition on virus multiplication without interfering with the bioactivity of cellular glycoproteins. © 2010 Elsevier Inc. All rights reserved.
format JOUR
author Bueno, C.A.
Alché, L.E.
Barquero, A.A.
author_facet Bueno, C.A.
Alché, L.E.
Barquero, A.A.
author_sort Bueno, C.A.
title 1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
title_short 1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
title_full 1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
title_fullStr 1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
title_full_unstemmed 1-Cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
title_sort 1-cinnamoyl-3,11-dihydroxymeliacarpin delays glycoprotein transport restraining virus multiplication without cytotoxicity
url http://hdl.handle.net/20.500.12110/paper_0006291X_v393_n1_p32_Bueno
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AT alchele 1cinnamoyl311dihydroxymeliacarpindelaysglycoproteintransportrestrainingvirusmultiplicationwithoutcytotoxicity
AT barqueroaa 1cinnamoyl311dihydroxymeliacarpindelaysglycoproteintransportrestrainingvirusmultiplicationwithoutcytotoxicity
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