Literature DB >> 9573243

Initiation of hepatitis delta virus genome replication.

K Dingle1, V Bichko, H Zuccola, J Hogle, J Taylor.   

Abstract

The small, 195-amino-acid form of the hepatitis delta virus (HDV) antigen (deltaAg-S) is essential for genome replication, i.e., for the transcription, processing, and accumulation of HDV RNAs. To better understand this requirement, we used purified recombinant deltaAg-S and HDV RNA synthesized in vitro to assemble high-molecular-weight ribonucleoprotein (RNP) structures. After transfection of these RNPs into human cells, we detected HDV genome replication, as assayed by Northern analysis or immunofluorescence microscopy. Our interpretation is that the input deltaAg-S is necessary for the RNA to undergo limited amounts of RNA-directed RNA synthesis, RNA processing, and mRNA formation, leading to de novo translation of deltaAg-S. It is this second source of deltaAg-S which then goes on to support genome replication. This assay made it possible to manipulate in vitro the composition of the RNP and then test in vivo the ability of the complex to initiate RNA-directed RNA synthesis and go on to achieve genome replication. For example, both genomic and antigenomic linear RNAs were acceptable. Substitution for deltaAg-S with truncated or modified forms of the deltaAg, and even with HIV nucleocapsid protein and polylysine, was unacceptable; the exception was a form of deltaAg-S with six histidines added at the C terminus. We expect that further in vitro modifications of these RNP complexes should help define the in vivo requirements for what we define as the initiation of HDV genome replication.

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Year:  1998        PMID: 9573243      PMCID: PMC110015          DOI: 10.1128/JVI.72.6.4783-4788.1998

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  27 in total

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2.  A specific base transition occurs on replicating hepatitis delta virus RNA.

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Journal:  J Virol       Date:  1990-03       Impact factor: 5.103

3.  In vitro-synthesized hepatitis delta virus RNA initiates genome replication in cultured cells.

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4.  Cleavage of structural proteins during the assembly of the head of bacteriophage T4.

Authors:  U K Laemmli
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5.  Role of two forms of hepatitis delta virus antigen: evidence for a mechanism of self-limiting genome replication.

Authors:  M Chao; S Y Hsieh; J Taylor
Journal:  J Virol       Date:  1990-10       Impact factor: 5.103

6.  Redistribution of the delta antigens in cells replicating the genome of hepatitis delta virus.

Authors:  V V Bichko; J M Taylor
Journal:  J Virol       Date:  1996-11       Impact factor: 5.103

7.  Tissue culture system for infection with human hepatitis delta virus.

Authors:  C Sureau; J R Jacob; J W Eichberg; R E Lanford
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8.  Replication of human hepatitis delta virus in primary cultures of woodchuck hepatocytes.

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  13 in total

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Authors:  G Moraleda; S Seeholzer; V Bichko; R Dunbrack; J Otto; J Taylor
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3.  RNA-Dependent replication and transcription of hepatitis delta virus RNA involve distinct cellular RNA polymerases.

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5.  Novel nuclear export signal-interacting protein, NESI, critical for the assembly of hepatitis delta virus.

Authors:  Yun-Hsin Wang; Shin C Chang; Cheng Huang; Ya-Ping Li; Chia-Huei Lee; Ming-Fu Chang
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6.  Parameters of human hepatitis delta virus genome replication: the quantity, quality, and intracellular distribution of viral proteins and RNA.

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8.  In vivo RNA-directed transcription, with template switching, by a mammalian RNA polymerase.

Authors:  Jinhong Chang; John Taylor
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9.  Intrinsic disorder and oligomerization of the hepatitis delta virus antigen.

Authors:  Carolina Alves; Hong Cheng; Heinrich Roder; John Taylor
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10.  Hepatitis delta antigen requires a minimum length of the hepatitis delta virus unbranched rod RNA structure for binding.

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