Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds

Ying Zhang; Alan A. Simpson; Rebecca M. Ledford; Carol M. Bator; Sugoto Chakravarty; Gregory A. Skochko; Tina M. Demenczuk; Adiba Watanyar; Daniel C. Pevear; Michael G. Rossmann

doi:10.1128/JVI.78.20.11061-11069.2004

Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds

Ying Zhang, Alan A. Simpson, Rebecca M. Ledford, Carol M. Bator, Sugoto Chakravarty, Gregory A. Skochko, Tina M. Demenczuk, Adiba Watanyar, Daniel C. Pevear, Michael G. Rossmann

Research output: Contribution to journal › Article › peer-review

60 Scopus citations

Abstract

Pleconaril is a broad-spectrum antirhinovirus and antienterovirus compound that binds into a hydrophobic pocket within viral protein 1, stabilizing the capsid and resulting in the inhibition of cell attachment and RNA uncoating. When crystals of human rhinovirus 16 (HRV16) and HRV14 are incubated with pleconaril, drug occupancy in the binding pocket is lower than when pleconaril is introduced during assembly prior to crystallization. This effect is far more marked in HRV16 than in HRV14 and is more marked with pleconaril than with other compounds. These observations are consistent with virus yield inhibition studies and radio-labeled drug binding studies showing that the antiviral effect of pleconaril against HRV16 is greater on the infectivity of progeny virions than the parent input viruses. These data suggest that drug integration into the binding pocket during assembly, or at some other late stage in virus replication, may contribute to the antiviral activity of capsid binding compounds.

Original language	English (US)
Pages (from-to)	11061-11069
Number of pages	9
Journal	Journal of virology
Volume	78
Issue number	20
DOIs	https://doi.org/10.1128/JVI.78.20.11061-11069.2004
State	Published - Oct 2004
Externally published	Yes

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Zhang, Y., Simpson, A. A., Ledford, R. M., Bator, C. M., Chakravarty, S., Skochko, G. A., Demenczuk, T. M., Watanyar, A., Pevear, D. C., & Rossmann, M. G. (2004). Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds. Journal of virology, 78(20), 11061-11069. https://doi.org/10.1128/JVI.78.20.11061-11069.2004

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title = "Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds",

abstract = "Pleconaril is a broad-spectrum antirhinovirus and antienterovirus compound that binds into a hydrophobic pocket within viral protein 1, stabilizing the capsid and resulting in the inhibition of cell attachment and RNA uncoating. When crystals of human rhinovirus 16 (HRV16) and HRV14 are incubated with pleconaril, drug occupancy in the binding pocket is lower than when pleconaril is introduced during assembly prior to crystallization. This effect is far more marked in HRV16 than in HRV14 and is more marked with pleconaril than with other compounds. These observations are consistent with virus yield inhibition studies and radio-labeled drug binding studies showing that the antiviral effect of pleconaril against HRV16 is greater on the infectivity of progeny virions than the parent input viruses. These data suggest that drug integration into the binding pocket during assembly, or at some other late stage in virus replication, may contribute to the antiviral activity of capsid binding compounds.",

author = "Ying Zhang and Simpson, \{Alan A.\} and Ledford, \{Rebecca M.\} and Bator, \{Carol M.\} and Sugoto Chakravarty and Skochko, \{Gregory A.\} and Demenczuk, \{Tina M.\} and Adiba Watanyar and Pevear, \{Daniel C.\} and Rossmann, \{Michael G.\}",

year = "2004",

month = oct,

doi = "10.1128/JVI.78.20.11061-11069.2004",

language = "English (US)",

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T1 - Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds

AU - Zhang, Ying

AU - Simpson, Alan A.

AU - Ledford, Rebecca M.

AU - Bator, Carol M.

AU - Chakravarty, Sugoto

AU - Skochko, Gregory A.

AU - Demenczuk, Tina M.

AU - Watanyar, Adiba

AU - Pevear, Daniel C.

AU - Rossmann, Michael G.

PY - 2004/10

Y1 - 2004/10

N2 - Pleconaril is a broad-spectrum antirhinovirus and antienterovirus compound that binds into a hydrophobic pocket within viral protein 1, stabilizing the capsid and resulting in the inhibition of cell attachment and RNA uncoating. When crystals of human rhinovirus 16 (HRV16) and HRV14 are incubated with pleconaril, drug occupancy in the binding pocket is lower than when pleconaril is introduced during assembly prior to crystallization. This effect is far more marked in HRV16 than in HRV14 and is more marked with pleconaril than with other compounds. These observations are consistent with virus yield inhibition studies and radio-labeled drug binding studies showing that the antiviral effect of pleconaril against HRV16 is greater on the infectivity of progeny virions than the parent input viruses. These data suggest that drug integration into the binding pocket during assembly, or at some other late stage in virus replication, may contribute to the antiviral activity of capsid binding compounds.

AB - Pleconaril is a broad-spectrum antirhinovirus and antienterovirus compound that binds into a hydrophobic pocket within viral protein 1, stabilizing the capsid and resulting in the inhibition of cell attachment and RNA uncoating. When crystals of human rhinovirus 16 (HRV16) and HRV14 are incubated with pleconaril, drug occupancy in the binding pocket is lower than when pleconaril is introduced during assembly prior to crystallization. This effect is far more marked in HRV16 than in HRV14 and is more marked with pleconaril than with other compounds. These observations are consistent with virus yield inhibition studies and radio-labeled drug binding studies showing that the antiviral effect of pleconaril against HRV16 is greater on the infectivity of progeny virions than the parent input viruses. These data suggest that drug integration into the binding pocket during assembly, or at some other late stage in virus replication, may contribute to the antiviral activity of capsid binding compounds.

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Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds

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