Identification of two flavivirus-like genomes in the GB hepatitis agent.

Simons, John N.; Pilot‐Matias, Tami; Leary, Thomas P.; Dawson, George J.; Desai, Suresh M.; Schlauder, George G.; Muerhoff, A. Scott; Erker, James C.; Buijk, Sheri L.; Chalmers, Michelle L.

doi:10.1073/pnas.92.8.3401

Cited by 518 publications

(353 citation statements)

References 29 publications

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“…All C termini are arbitrary, but reflect an appropriate region where the alignment is maintained across all the groups of viruses before the similarity drops too low. Sequences used in the analyses : dengue virus (type 1 - Fu et al, 1992 ;type 2 -Hahn et al, 1988 ;type 3 -Osatomi & Sumiyoshi, 1990 ;type 4 -Mackow et al, 1987) ; Japanese encephalitis virus (Sumiyoshi et al, 1987) ; Kunjin virus (Coia et al, 1988) ; Murray Valley encephalitis virus (MVEV -Dalgarno et al, 1986) ; tick-borne encephalitis virus (TBEV -Pletnev et al, 1990) ; West Nile virus (WNV Castle et al, 1986) ; yellow fever virus (YVF - Rice et al, 1985) ; hepatitis G virus (strain GB-A, B - Simons et al, 1995 ;C -Leary et al, 1995) ; hepatitis C virus (HCV strain 1a -Choo et al, 1991 ;1b -Kato et al, 1990 ;1c -Okamoto et al, 1994 ;2a -Okamoto et al, 1991 ;2b -Okamoto et al, 1992 ;2c -Nakao et al, 1996 ;3a -Sakamoto et al, 1994 ;3b -Chayama et al, 1994 ;4a -Chamberlain et al, 1997 a ;5a -Chamberlain et al, 1997 b ;6a -Adams et al, 1997) ; bovine viral diarrhoea virus (BVDV strain Osloss - Renard et al, 1987 ;De Moerlooze et al, 1993 ;NADL -Collet et al, 1988 b ;SD1 -Deng & Brock, 1992 ;NCP7 -Meyers et al, 1996 ;ILLC -Roath & Berry, unpublished ;IIRidpath & Bolin, 1995) ; classical swine fever virus (CSFV strain Alfort -Meyers et al, 1989 ;Brescia -Moorman et al, 1990 . Sequence similarities between NS3 proteolytic domains of the Flaviviridae.…”

Section: Ns3 Proteinase (I) Identification Of the Ns3 Proteolytic Domainmentioning

confidence: 99%

Virus-encoded proteinases of the Flaviviridae.

Ryan¹,

Monaghan²,

Flint³

1998

Journal of General Virology

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Section: Ns3 Proteinase (I) Identification Of the Ns3 Proteolytic Domainmentioning

confidence: 99%

Virus-encoded proteinases of the Flaviviridae.

Ryan¹,

Monaghan²,

Flint³

1998

Journal of General Virology

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“…We have, therefore, examined whether a p7-like protein is expressed by GB virus B (GBV-B), the most closely related of all animal viruses to HCV. GBV-B was iden-tified in 1995 in a tamarin (Saguinus species) that developed acute hepatitis after inoculation with serum from the 11th tamarin passage of the original, human GB inoculum (16,17). GBV-B infection is typically self-limited and associated with acute hepatitis (18,19), although persistent infection can lead to chronic hepatitis in tamarins (20).…”

mentioning

confidence: 99%

Characterization of GB Virus B Polyprotein Processing Reveals the Existence of a Novel 13-kDa Protein with Partial Homology to Hepatitis C Virus p7 Protein

Ghibaudo

Cohen

Pénin

et al. 2004

Journal of Biological Chemistry

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Although responsible for a major health problem worldwide, hepatitis C virus is difficult to study because of the absence of fully permissive cell cultures or experimental animal models other than the chimpanzee. GB virus B (GBV-B), a closely related hepatotropic virus that infects small New World primates and replicates efficiently in primary hepatocyte cultures, is an attractive surrogate model system. However, little is known about processing of the GBV-B polyprotein. Because an understanding of these events is critical to further development of model GBV-B systems, we characterized signal peptidase processing of the polyprotein segment containing the putative structural proteins. We identified the exact N termini of the mature GBV-B envelope proteins, E1 and E2, and the first nonstructural protein, NS2, by direct amino acid sequencing. Interestingly, these studies document the existence of a previously unrecognized 13-kDa protein (p13) located between E2 and NS2 within the polyprotein. We compared the sequence of the p13 protein to that of hepatitis C virus p7, a small membrane-spanning protein with a similar location in the polyprotein and recently identified ion channel activity. The C-terminal half of p13 shows clear homology with p7, suggesting a common function, but the substantially larger size of p13, with 4 rather than 2 predicted transmembrane segments, indicates a different structural organization and/or additional functions. The identification of p13 in the GBV-B polyprotein provides strong support for the hypothesis that ion channel-forming proteins are essential for the life cycle of flaviviruses, possibly playing a role in virion morphogenesis and/or virus entry into cells.

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“…HCV infection in humans frequently results in persistent infection with associated disease sequelae, while GBV-B-infected tamarins appear to clear the viral infection with no long-lasting ill effects. However, relatively few animals have been followed long term by reverse transcription-PCR (RT-PCR) since the virus was identified in 1995 (28), and so the potential for a low percentage of chronic infections exists. The acute nature of GBV-B infections in tamarins distinguishes this hepatitis from HCV infections in humans, although the viruses share many characteristics.…”

mentioning

confidence: 99%

Development of a Primary Tamarin Hepatocyte Culture System for GB Virus-B: a Surrogate Model for Hepatitis C Virus

Beames¹,

Chavez²,

Guerra³

et al. 2000

J Virol

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GB virus-B (GBV-B)causes an acute hepatitis in tamarins characterized by increased alanine transaminase levels that quickly return to normal as the virus is cleared. Phylogenetically, GBV-B is the closest relative to hepatitis C virus (HCV), and thus GBV-B infection of tamarins represents a powerful surrogate model system for the study of HCV. In this study, the course of infection of GBV-B in tamarins was followed using a real-time 5 exonuclease (TaqMan) reverse transcription-PCR assay to determine the level of GBV-B in the serum. Peak viremia levels exceeded 10 9 genome equivalents/ml, followed by viral clearance within 14 to 16 weeks. Rechallenge of animals that had cleared infection resulted in viremia that was limited to 1 week, suggestive of a strong protective immune response. A robust tissue culture system for GBV-B was developed using primary cultures of tamarin hepatocytes. Hepatocytes obtained from a GBV-B-infected animal maintained high levels of cellassociated viral RNA and virion secretion for 42 days of culture. In vitro infection of normal hepatocytes resulted in rapid amplification of cell-associated viral RNA and secretion of up to 10 7 genome equivalents/ml of culture supernatant. In addition, infection could be monitored by immunofluorescence staining for GBV-B nonstructural NS3 protein. This model system overcomes many of the current obstacles to HCV research, including low levels of viral replication, lack of a small primate animal model, and lack of a reproducible tissue culture system. Hepatitis C virus (HCV) is a major worldwide health problem, with an estimated 2% of the population chronically infected with this virus. Chronic HCV infection can cause significant liver disease and cirrhosis of the liver and, in some patients, lead eventually to liver cancer. The current animal model for the study of HCV is the chimpanzee. However, this model system suffers from the limited availability of chimpanzees and the high cost associated with conducting studies on large nonhuman primates. A smaller, less expensive model system would be desirable.One alternative model is the hepatitis GB virus-B (GBV-B) in Saguinus species (tamarins). The GB agents, GBV-A, -B, and -C, are members of Flaviviridae (21); GBV-B is the virus most closely related to HCV (22). GBV-A and GBV-B were isolated from tamarins inoculated with a blood sample from a surgeon (GB) suffering from acute hepatitis (10). Although GBV-A and GBV-B were isolated from a tamarin inoculated with human serum believed to contain a human hepatitis virus, GBV-A and GBV-B are considered tamarin viruses. While GBV-A has been isolated from a number of tamarins (5), GBV-B has been isolated only once, and its origins are unclear. A third GB agent, GBV-C (27), also known as hepatitis G virus (19), was isolated from human serum samples in attempts to isolate new hepatitis viruses; however its association with hepatitis is tenuous (1).GBV-A causes no recognized disease in tamarins, while GBV-B causes an acute, self-limited hepatitis, as evidenced by a r...

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Identification of two flavivirus-like genomes in the GB hepatitis agent.

Cited by 518 publications

References 29 publications

Virus-encoded proteinases of the Flaviviridae.

Virus-encoded proteinases of the Flaviviridae.

Characterization of GB Virus B Polyprotein Processing Reveals the Existence of a Novel 13-kDa Protein with Partial Homology to Hepatitis C Virus p7 Protein

Development of a Primary Tamarin Hepatocyte Culture System for GB Virus-B: a Surrogate Model for Hepatitis C Virus

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