Your search keyword '"GB virus B"' showing total 7 results

1. GB Virus B and Hepatitis C Virus, Distantly Related Hepaciviruses, Share an Entry Factor, Claudin-1.

Author

Toon, Kamilla, Kalemera, Mphatso D., Palor, Machaela, Rose, Nicola J., Takeuchi, Yasuhiro, Grove, Joe, and Mattiuzzo, Giada

Subjects

*HEPATITIS C virus, *HEPATITIS B virus, *CLAUDINS, *TIGHT junctions, *NUMBERS of species

Abstract

Due to increased and broadened screening efforts, the last decade has seen a rapid expansion in the number of viral species classified into the Hepacivirus genus. Conserved genetic features of hepaciviruses suggest that they have undergone specific adaptation and have evolved to hijack similar host proteins for efficient propagation in the liver. Here, we developed pseudotyped viruses to elucidate the entry factors of GB virus B (GBV-B), the first hepacivirus described in an animal after hepatitis C virus (HCV). GBV-B-pseudotyped viral particles (GBVBpp) were shown to be uniquely sensitive to the sera of tamarins infected with GBV-B, validating their usefulness as a surrogate for GBV-B entry studies. We screened GBVBpp infection of human hepatoma cell lines that were CRISPR/Cas9 engineered to ablate the expression of individual HCV receptors/entry factors and found that claudin-1 is essential for GBV-B infection, indicating the GBV-B and HCV share an entry factor. Our data suggest that claudin-1 facilitates HCV and GBV-B entry through distinct mechanisms since the former requires the first extracellular loop and the latter is reliant on a C-terminal region containing the second extracellular loop. The observation that claudin- 1 is an entry factor shared between these two hepaciviruses suggests that the tight junction protein is of fundamental mechanistic importance during cell entry. [ABSTRACT FROM AUTHOR]

Published

2023

2. A comparative analysis of the substrate permissiveness of HCV and GBV-B NS3/4A proteases reveals genetic evidence for an interaction with NS4B protein during genome replication

Author

Benureau, Yann, Warter, Lucile, Malcolm, Bruce A., and Martin, Annette

Subjects

*HEPATITIS C virus, *COMPARATIVE studies, *PROTEOLYTIC enzymes, *VIRAL replication, *MUTAGENESIS, *ANTIVIRAL agents

Abstract

Abstract: The hepatitis C virus (HCV) serine protease (NS3/4A) processes the NS3–NS5B segment of the viral polyprotein and also cleaves host proteins involved in interferon signaling, making it an important target for antiviral drug discovery and suggesting a wide breadth of substrate specificity. We compared substrate specificities of the HCV protease with that of the GB virus B (GBV-B), a distantly related nonhuman primate hepacivirus, by exchanging amino acid sequences at the NS4B/5A and/or NS5A/5B cleavage junctions between these viruses within the backbone of subgenomic replicons. This mutagenesis study demonstrated that the GBV-B protease had a broader substrate tolerance, a feature corroborated by structural homology modeling. However, despite efficient polyprotein processing, GBV-B RNAs containing HCV sequences at the C-terminus of NS4B had a pseudo-lethal replication phenotype. Replication-competent revertants contained second-site substitutions within the NS3 protease or NS4B N-terminus, providing genetic evidence for an essential interaction between NS3 and NS4B during genome replication. [ABSTRACT FROM AUTHOR]

Published

2010

3. Chimeric GB virus B genomes containing hepatitis C virus p7 are infectious in vivo

Author

Griffin, Stephen, Trowbridge, Rachel, Thommes, Pia, Parry, Nigel, Rowlands, David, Harris, Mark, and Bright, Helen

Subjects

*HEPATITIS C virus, *VIRAL disease treatment, *VIRAL genomes, *DNA replication, *EFFECT of drugs on ion channels, *AMANTADINE, *MOSAICISM

Abstract

Background/Aims: The development of new therapies for hepatitis C virus (HCV) infection has been hampered by the lack of a small animal model. GB virus B (GBV-B), which infects new world monkeys, has been proposed as a surrogate system for HCV replication. Despite their short genetic distance, however, difficulties exist when extrapolating results from GBV-B to the HCV system. One way of addressing this is the creation of chimeric GBV-B containing HCV elements. Methods: Construction and analysis of GBV-B chimeras in which the p13 ion channel was replaced by its HCV counterpart, p7. Results: Replacing all, or part of, the GBV-B p13 protein with HCV p7 resulted in viable chimeras which replicated at wild-type levels in marmosets following intra-hepatic RNA injection. Serum from one animal injected with chimeric RNA was infectious in three naïve recipients, indicating that chimeras formed fully infectious virions. Amantadine, which blocks the ion channel activity of both HCV and GBV-B proteins in vitro, also inhibited GBV-B replication in primary hepatocytes. Conclusions: These viruses highlight the potential for chimeric GBV-B in the development of HCV-specific therapies and will provide a means of developing HCV p7 as a therapeutic target. [Copyright &y& Elsevier]

Published

2008

4. Restricted quasispecies variation following infection with the GB virus B

Author

McGarvey, Michael Joseph, Iqbal, Mohammed, Nastos, Theodoros, and Karayiannis, Peter

Subjects

*VIRUS diseases, *HEPATITIS C virus, *HEPATITIS, *HYPERVARIABLE regions

Abstract

Abstract: The extent of genetic variability following acute infection of tamarins with GB virus B (GBV-B) is not known. In this study we attempted to define the quasispecies variation of GBV-B 17 days post-infection, by PCR amplification of GBV-B RNA extracted from serum and liver. Cloning followed by sequencing revealed a small number of changes in the three regions studied, namely the 5′ untranslated region, E2 and NS3. Moreover, there was no region of high amino acid variability in E2, akin to hypervariable region 1 of hepatitis C virus. This was further confirmed by analysing sequences from two additional animals obtained at a similar time point post-infection. Nevertheless, it was apparent that different variants with one or two amino acid substitutions in the region studied had been selected when comparing the sequences from the three animals. This restricted sequence variation of GBV-B during acute hepatitis may explain the infrequent progression of the infection to a chronic stage. [Copyright &y& Elsevier]

Published

2008

5. Efficient regulation of viral replication by siRNA in a non-human primate surrogate model for hepatitis C

Author

Yokota, Takanori, Iijima, Sayuki, Kubodera, Takayuki, Ishii, Koji, Katakai, Yuko, Ageyama, Naohide, Chen, Yingwei, Lee, Young-Jung, Unno, Toshinori, Nishina, Kazutaka, Iwasaki, Yuki, Maki, Noboru, Mizusawa, Hidehiro, and Akari, Hirofumi

Subjects

*HEPATITIS C, *SERUM, *HEPATITIS C virus, *BIOCHEMICAL research

Abstract

Abstract: RNA interference (RNAi) represents a new technology which could offer potential applications for the therapeutics of human diseases. RNAi-mediated therapy has recently been shown to be effective toward infectious diseases in in vitro and rodent models, however, it remains unclear whether RNAi therapy with systemic application could be effective in primates. In this study, we examined if RNAi therapy could be effective toward infectious diseases by using a non-human primate surrogate model for hepatitis C. Administration into marmosets of cationic liposome-encapsulated siRNA (CL-siRNA) for GB virus B (GBV-B), which is most closely related to hepatitis C virus, repressed GBV-B replication in a dose-dependent manner. Especially, 5mg/kg of the CL-siRNA completely inhibited the viral replication. Since the serum interferons (IFNs) were induced by CL-siRNA in vivo, inhibition of viral regulation by anti-GBV-B CL-siRNA may include an antiviral effect of IFN. However, contribution of induced IFN may be partial, since the control CL-siRNA which induced a stronger IFN response than GBV-B CL-siRNA could only delay the viral replication. Our results suggest the feasibility of systemic administration of CL-siRNA as an antiviral strategy. [Copyright &y& Elsevier]

Published

2007

6. GBV-B as a pleiotropic virus: distribution of GBV-B in extrahepatic tissues in vivo

Author

Ishii, Koji, Iijima, Sayuki, Kimura, Nobuyuki, Lee, Young-Jung, Ageyama, Naohide, Yagi, Shintaro, Yamaguchi, Kenjiro, Maki, Noboru, Mori, Ken-ichi, Yoshizaki, Sayaka, Machida, Sanae, Suzuki, Tetsuro, Iwata, Naoko, Sata, Tetsutaro, Terao, Keiji, Miyamura, Tatsuo, and Akari, Hirofumi

Subjects

*NEW World monkeys, *HEPATITIS C virus, *TAMARINS, *HEPATITIS

Abstract

Abstract: GB virus B (GBV-B) infection of New World monkeys is considered to be a useful surrogate model for hepatitis C virus (HCV) infection. GBV-B replicates in the liver and induces acute resolving hepatitis but little is known whether the other organs could be permissive for the virus. We investigated the viral tropism of GBV-B in tamarins in the acute stage of viral infection and found that the viral genomic RNA could be detected in a variety of tissues. Notably, a GBV-B-infected tamarin with marked acute viremia scarcely showed a sign of hepatitis, due to preferential infection in lymphoid tissues such as lymph nodes and spleen. These results indicate that GBV-B as well as HCV is a pleiotropic virus in vivo. [Copyright &y& Elsevier]

Published

2007

7. Investigation into the ability of GB virus B to replicate in various immortalized cell lines

Author

Buckwold, Victor E., Collins, Barbara, Hogan, Priscilla, Rippeon, Sherry, and Wei, Jiayi

Subjects

*HEPATITIS C virus, *ANTIVIRAL agents, *DRUG development, *NUCLEIC acids

Abstract

Abstract: GB virus B (GBV-B) is the most closely related virus to the hepatitis C virus (HCV) and is an attractive surrogate model system for HCV drug development efforts. Unfortunately, GBV-B can only be grown in the primary hepatocytes of certain non-human primates. We grew GBV-B in tamarins and marmosets and then used this virus in the absence and presence of lipofection reagents to try to infect 20 different cell lines including human primary hepatocytes and marmoset primary hepatocytes. GBV-B only replicated in marmoset primary hepatocytes. We isolated primary hepatocytes from GBV-B-positive and negative tamarins and marmosets and tried to immortalize the cells using SV40 large T-antigen or cell fusion. GBV-B stable cell lines were constructed in Huh7 and HepG2 cell lines, but there was no evidence for viral replication or a response to antiviral agents in these lines. Infectious full-length GBV-B RNA could be transfected into Vero, Huh7 and HepG2 at high efficiency, however there was no evidence for GBV-B replication or a response to antiviral agents. None of these approaches were successful and an in vitro model of GBV-B replication using immortalized cell lines was not produced. We hypothesize that these immortalized cell lines lack liver-specific factors that are required for GBV-B replication. [Copyright &y& Elsevier]

Published

2005