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p72 DEAD box RNA helicase is required for optimal function of the zinc-finger antiviral protein

by Gao, Guangxia , Chen, Guifang , Lv, Fengxiang , Guo, Xuemin , Xu, Yihui

in Antibodies / antiviral proteins / Antivirals / Binding Sites / Biological Sciences / Cell Line / Cell lines / DEAD-box RNA helicases / DEAD-box RNA Helicases - genetics / DEAD-box RNA Helicases - metabolism / Enzymes / Exosomes / Gene Deletion / Gene expression / HEK293 cells / Humans / Messenger RNA / Mutation - genetics / Plasmids / Protein Binding / Proteins / Ribonucleic acid / RNA / RNA Interference / RNA stability / RNA-Binding Proteins - genetics / RNA-Binding Proteins - metabolism / Viruses / Zinc Fingers

2008

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p72 DEAD box RNA helicase is required for optimal function of the zinc-finger antiviral protein

by Gao, Guangxia , Chen, Guifang , Lv, Fengxiang , Guo, Xuemin , Xu, Yihui

2008

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p72 DEAD box RNA helicase is required for optimal function of the zinc-finger antiviral protein

by Gao, Guangxia , Chen, Guifang , Lv, Fengxiang , Guo, Xuemin , Xu, Yihui

2008

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Journal Article

p72 DEAD box RNA helicase is required for optimal function of the zinc-finger antiviral protein

Gao, Guangxia,

Chen, Guifang,

Lv, Fengxiang,

Guo, Xuemin,

Xu, Yihui

2008

Overview

The zinc-finger antiviral protein (ZAP) specifically inhibits the replication of many viruses by preventing the accumulation of viral mRNAs in the cytoplasm. ZAP directly binds to the viral mRNAs and recruits the RNA exosome to degrade the target RNA. In the present study, we identified the p72 DEAD box RNA helicase, but not the highly similar RNA helicase p68, as a ZAP-interacting protein. The binding domain of ZAP was mapped to its N-terminal portion, whereas both the N- and C-terminal domains of p72 bound to ZAP. Overexpression of the C-terminal domain of p72 reduced ZAP's activity, whereas overexpression of the full-length p72 enhanced ZAP's activity. The RNA helicase activity was required for p72 to promote ZAP-mediated RNA degradation. Depletion of p72 by RNAi also reduced ZAP's activity but did not affect tristetraprolin-mediated RNA degradation. We conclude that p72 is required for the optimal activity of ZAP, and we propose that p72 helps to restructure the ZAP-bound target mRNA for efficient degradation.

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Publisher

National Academy of Sciences,National Acad Sciences

Subject

/ Biological Sciences

/ Cell Line

/ Cell lines