Literature DB >> 17684232

Nuclear factors are involved in hepatitis C virus RNA replication.

Olaf Isken1, Martina Baroth, Claus W Grassmann, Susan Weinlich, Dirk H Ostareck, Antje Ostareck-Lederer, Sven-Erik Behrens.   

Abstract

Unraveling the molecular basis of the life cycle of hepatitis C virus (HCV), a prevalent agent of human liver disease, entails the identification of cell-encoded factors that participate in the replication of the viral RNA genome. This study provides evidence that the so-called NF/NFAR proteins, namely, NF90/NFAR-1, NF110/NFAR-2, NF45, and RNA helicase A (RHA), which mostly belong to the dsRBM protein family, are involved in the HCV RNA replication process. NF/NFAR proteins were shown to specifically bind to replication signals in the HCV genomic 5' and 3' termini and to promote the formation of a looplike structure of the viral RNA. In cells containing replicating HCV RNA, the generally nuclear NF/NFAR proteins accumulate in the cytoplasmic viral replication complexes, and the prototype NFAR protein, NF90/NFAR-1, stably interacts with a viral protein. HCV replication was inhibited in cells where RNAi depleted RHA from the cytoplasm. Likewise, HCV replication was hindered in cells that contained another NF/NFAR protein recruiting virus. The recruitment of NF/NFAR proteins by HCV is assumed to serve two major purposes: to support 5'-3' interactions of the viral RNA for the coordination of viral protein and RNA synthesis and to weaken host-defense mechanisms.

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Year:  2007        PMID: 17684232      PMCID: PMC1986813          DOI: 10.1261/rna.594207

Source DB:  PubMed          Journal:  RNA        ISSN: 1355-8382            Impact factor:   4.942


  58 in total

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  89 in total

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6.  In vitro and in vivo analysis of the interaction between RNA helicase A and HIV-1 RNA.

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7.  Up-regulation of NF45 correlates with Schwann cell proliferation after sciatic nerve crush.

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8.  Poxviral protein E3-altered cytokine production reveals that DExD/H-box helicase 9 controls Toll-like receptor-stimulated immune responses.

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