Continuous human cell lines inducibly expressing hepatitis C virus structural and nonstructural proteins

“…Cell lines. Tetracycline-regulated cell lines were generated as described previously (38,40). In brief, the constitutively tetracycline-controlled-transactivatorexpressing U-2 OS human osteosarcoma-derived founder cell line UTA-6 (20) was cotransfected with pUHD-BVDV-5A-HA or pUHD-BVDV-5A⌬N28-HA and pBabepuro (42), followed by selection with G418 and puromycin.…”

Section: Methodsmentioning

confidence: 99%

“…Immunofluorescence staining was performed as described previously (38,40). In brief, cells grown as monolayers on glass coverslips were fixed with 2% paraformaldehyde, permeabilized with 0.1% saponin, blocked with phosphate-buffered saline containing 3% bovine serum albumin and 0.05% saponin, and incubated with primary antibodies in phosphate-buffered saline containing 3% bovine serum albumin and 0.05% saponin.…”

Section: Methodsmentioning

confidence: 99%

Conserved Determinants for Membrane Association of Nonstructural Protein 5A fromHepatitis C Virus and Related Viruses

Brass

Pál

Sapay

et al. 2007

J Virol

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Nonstructural protein 5A (NS5A) is a membrane-associated essential component of the hepatitis C virus (HCV) replication complex. An N-terminal amphipathic alpha helix mediates in-plane membrane association of HCV NS5A and at the same time is likely involved in specific protein-protein interactions required for the assembly of a functional replication complex. The aim of this study was to identify the determinants for membrane association of NS5A from the related GB viruses and pestiviruses. Although primary amino acid sequences differed considerably, putative membrane anchor domains with amphipathic features were predicted in the N-terminal domains of NS5A proteins from these viruses. Confocal laser scanning microscopy, as well as membrane flotation analyses, demonstrated that NS5As from GB virus B (GBV-B), GBV-C, and bovine viral diarrhea virus, the prototype pestivirus, display membrane association characteristics very similar to those of HCV NS5A. The N-terminal 27 to 33 amino acid residues of these NS5A proteins were sufficient for membrane association. Circular dichroism analyses confirmed the capacity of these segments to fold into alpha helices upon association with lipid-like molecules. Despite structural conservation, only very limited exchanges with sequences from related viruses were tolerated in the context of functional HCV RNA replication, suggesting virus-specific interactions of these segments. In conclusion, membrane association of NS5A by an N-terminal amphipathic alpha helix is a feature shared by HCV and related members of the family Flaviviridae. This observation points to conserved roles of the N-terminal amphipathic alpha helices of NS5A in replication complex formation.The family Flaviviridae comprises the genera Flavirus, Hepacivirus, and Pestivirus, as well as the as-yet-unassigned GB virus A (GBV-A), GBV-B, and GBV-C. These enveloped positivestrand RNA viruses express their structural and nonstructural proteins via translation of a single long open reading frame (30). Hepatitis C virus (HCV) is the sole member of the genus Hepacivirus and a major cause of chronic hepatitis, liver cirrhosis, and hepatocellular carcinoma, affecting an estimated 3% of the world's population (44). GB viruses and pestiviruses are more closely related to HCV than the classical flaviviruses. The availability of efficient cell culture systems and animal models makes these related viruses attractive in vitro and in vivo models for HCV. GBV-B, the closest relative of HCV, was recovered from a tamarin inoculated with blood from a surgeon suffering from acute hepatitis (16, 54) and causes acute and chronic hepatitis in New World monkeys, which are believed to represent the natural hosts (10). Subsequent attempts to isolate GBV-B sequences from humans have failed. By contrast, GBV-C persistently infects humans. However, the pathogenic relevance of GBV-C, if any, remains unclear. It does not cause hepatitis but has been associated with prolonged survival in human immunodeficiency virus-infected individuals (62-64). ...

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“…In the present study, we analysed the effect of HCV protein expression on host-cell chemokine gene expression in an osteosarcoma model cell system expressing HCV genes in a tetracycline-regulated fashion (Hugle et al, 2001;Moradpour et al, 1998;Wolk et al, 2000). We observed that, in the cell lines expressing NS3/4A or the full-length HCV polyprotein, Sendai virus (SeV)-induced chemokine gene expression was clearly reduced.…”

Section: Introductionmentioning

confidence: 99%

Hepatitis C virus proteins interfere with the activation of chemokine gene promoters and downregulate chemokine gene expression

Sillanpää

Kaukinen

Melén

et al. 2008

Journal of General Virology

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The hepatitis C virus (HCV) non-structural (NS) 3/4A protein complex inhibits the retinoic acid inducible gene I (RIG-I) pathway by proteolytically cleaving mitochondria-associated CARD-containing adaptor protein Cardif, and this leads to reduced production of beta interferon (IFN-b). This study examined the expression of CCL5 (regulated upon activation, normal T-cell expressed and secreted, or RANTES), CXCL8 (interleukin 8) and CXCL10 (IFN-c-activated protein 10, or IP-10) chemokine genes in osteosarcoma cell lines that inducibly expressed NS3/4A, NS4B, core-E1-E2-p7 and the entire HCV polyprotein. Sendai virus (SeV)-induced production of IFN-b, CCL5, CXCL8 and CXCL10 was downregulated by the NS3/4A protein complex and by the full-length HCV polyprotein. Expression of NS3/4A and the HCV polyprotein reduced the binding of interferon regulatory factors (IRFs) 1 and 3 and, to a lesser extent, nuclear factor (NF)-kB (p65/p50) to their respective binding elements on the CXCL10 promoter during SeV infection. Furthermore, binding of IRF1 and IRF3 to the interferon-stimulated response element-like element, and of c-Jun and phosphorylated c-Jun to the activator protein 1 element of the CXCL8 promoter, was reduced when NS3/4A and the HCV polyprotein were expressed. In cell lines expressing NS3/4A and the HCV polyprotein, the subcellular localization of mitochondria was changed, and this was kinetically associated with the partial degradation of endogenous Cardif. These results indicate that NS3/4A alone or as part of the HCV polyprotein disturbs the expression of IRF1-and IRF3-regulated genes, as well as affecting mitogen-activated protein kinase kinase-and NF-kB-regulated genes. INTRODUCTIONHepatitis C virus (HCV) belongs to the family Flaviviridae. Its single-stranded RNA genome is 9.6 kb and encodes a large polyprotein that is cleaved into 11 structural and non-structural (NS) proteins by cellular and viral-encoded proteases. The structural region of the HCV genome contains the core, E1, E2 and p7 proteins and an alternative reading frame protein (Moradpour et al., 2002). The core protein forms the viral nucleocapsid, E1 and E2 are viral envelope glycoproteins, and p7 functions as a cation channel (Griffin et al., 2003). The HCV genome also encodes six NS proteins. NS2 is a cysteine protease and NS3 a serine protease, and they are involved in processing of the HCV polyprotein. NS3 also functions as an RNA helicase. NS4A is an essential co-factor for NS3 protease activity. NS4B is a membrane-associated protein with no assigned functions, NS5A is a phosphoprotein and NS5B is an RNA-dependent RNA polymerase (Lindenbach & Rice, 2005;Moradpour et al., 2002).In the early stages of virus infection, the production of the antiviral cytokines alpha and beta interferon (IFN-a/b) and several proinflammatory chemokines such as CCL5 [regulated upon activation, normal T-cell expressed and secreted (RANTES)], CXCL8 [interleukin (IL) 8], and CXCL10 [IFNc-activated protein 10 (IP-10)] are activated. These chemokines are chemoattractive...

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Continuous human cell lines inducibly expressing hepatitis C virus structural and nonstructural proteins

Cited by 145 publications

References 52 publications

S‐adenosylmethionine and betaine correct hepatitis C virus induced inhibition of interferon signaling in vitro†

S‐adenosylmethionine and betaine correct hepatitis C virus induced inhibition of interferon signaling in vitro†

Conserved Determinants for Membrane Association of Nonstructural Protein 5A fromHepatitis C Virus and Related Viruses

Hepatitis C virus proteins interfere with the activation of chemokine gene promoters and downregulate chemokine gene expression

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