RNA interaction and cleavage of poly(C)-binding protein 2 by hepatitis A virus protease

Bo Zhang; Simone Seitz; Yuri Kusov; Roland Zell; Verena Gauss-Müller

doi:10.1016/j.bbrc.2007.09.133

RNA interaction and cleavage of poly(C)-binding protein 2 by hepatitis A virus protease

Bo Zhang, Simone Seitz, Yuri Kusov, Roland Zell, Verena Gauss-Müller^*

^*Corresponding author for this work

Institute of Virology and Cell Biology

Friedrich Schiller University Jena

29 Citations (Scopus)

Abstract

The poly(rC)-binding protein PCBP2 has multiple functions in post-transcriptional control of host and viral gene expression. Since it interacts with picornaviral RNA structures, it was proposed that PCBP2 regulates viral genome translation and replication. The hepatitis A virus (HAV), an atypical picornavirus, contains an unusual pyrimidine-rich tract (pY1) with unknown functions. Using in vivo and in vitro assays, we provide direct evidence that PCBP2 interacts with pY1 and that binding is mediated by KH domains 1 and 3. Proteolytic cleavage by the viral protease 3C generates a C-terminally truncated polypeptide with highly reduced RNA affinity. The results suggest that during HAV infection PCBP2 cleavage might specifically down-regulate viral protein synthesis, thereby giving way to viral RNA synthesis.

Original language	English
Journal	Biochemical and Biophysical Research Communications
Volume	364
Issue number	4
Pages (from-to)	725-730
Number of pages	6
ISSN	0006-291X
DOIs	https://doi.org/10.1016/j.bbrc.2007.09.133
Publication status	Published - 28.12.2007

Funding

We thank Drs. E. Ehrenfeld, M. Görlach, R. Lloyd, and B. Semler for material used in this study. The help of Ms. A. Klingenschmidt, B. Andresen, and K. Thiele-Bössel is highly appreciated. Work in the laboratories is funded by the Deutsche Forschungsgemeinschaft (DFG, projects Ga304/7-1 and Ze 446/3, 4). Appendix A

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Research Areas and Centers

Academic Focus: Center for Infection and Inflammation Research (ZIEL)

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10.1016/j.bbrc.2007.09.133

Cite this

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title = "RNA interaction and cleavage of poly(C)-binding protein 2 by hepatitis A virus protease",

abstract = "The poly(rC)-binding protein PCBP2 has multiple functions in post-transcriptional control of host and viral gene expression. Since it interacts with picornaviral RNA structures, it was proposed that PCBP2 regulates viral genome translation and replication. The hepatitis A virus (HAV), an atypical picornavirus, contains an unusual pyrimidine-rich tract (pY1) with unknown functions. Using in vivo and in vitro assays, we provide direct evidence that PCBP2 interacts with pY1 and that binding is mediated by KH domains 1 and 3. Proteolytic cleavage by the viral protease 3C generates a C-terminally truncated polypeptide with highly reduced RNA affinity. The results suggest that during HAV infection PCBP2 cleavage might specifically down-regulate viral protein synthesis, thereby giving way to viral RNA synthesis.",

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T1 - RNA interaction and cleavage of poly(C)-binding protein 2 by hepatitis A virus protease

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AU - Seitz, Simone

AU - Kusov, Yuri

AU - Zell, Roland

AU - Gauss-Müller, Verena

PY - 2007/12/28

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N2 - The poly(rC)-binding protein PCBP2 has multiple functions in post-transcriptional control of host and viral gene expression. Since it interacts with picornaviral RNA structures, it was proposed that PCBP2 regulates viral genome translation and replication. The hepatitis A virus (HAV), an atypical picornavirus, contains an unusual pyrimidine-rich tract (pY1) with unknown functions. Using in vivo and in vitro assays, we provide direct evidence that PCBP2 interacts with pY1 and that binding is mediated by KH domains 1 and 3. Proteolytic cleavage by the viral protease 3C generates a C-terminally truncated polypeptide with highly reduced RNA affinity. The results suggest that during HAV infection PCBP2 cleavage might specifically down-regulate viral protein synthesis, thereby giving way to viral RNA synthesis.

AB - The poly(rC)-binding protein PCBP2 has multiple functions in post-transcriptional control of host and viral gene expression. Since it interacts with picornaviral RNA structures, it was proposed that PCBP2 regulates viral genome translation and replication. The hepatitis A virus (HAV), an atypical picornavirus, contains an unusual pyrimidine-rich tract (pY1) with unknown functions. Using in vivo and in vitro assays, we provide direct evidence that PCBP2 interacts with pY1 and that binding is mediated by KH domains 1 and 3. Proteolytic cleavage by the viral protease 3C generates a C-terminally truncated polypeptide with highly reduced RNA affinity. The results suggest that during HAV infection PCBP2 cleavage might specifically down-regulate viral protein synthesis, thereby giving way to viral RNA synthesis.

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RNA interaction and cleavage of poly(C)-binding protein 2 by hepatitis A virus protease

Abstract

Funding

UN SDGs

Research Areas and Centers

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The switch from translation to replication in the life cycle of the hepatitis A virus (HAV): A cell-virus interplay

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RNA interaction and cleavage of poly(C)-binding protein 2 by hepatitis A virus protease

Abstract

Funding

UN SDGs

Research Areas and Centers

Access to Document

Other files and links

Fingerprint

Projects

The switch from translation to replication in the life cycle of the hepatitis A virus (HAV): A cell-virus interplay

Cite this