RNA Interference and Single Particle Tracking Analysis of Hepatitis C Virus Endocytosis

Coller, Kelly E.; Berger, Kristi L.; Heaton, Nicholas S.; Cooper, Jacob D.; Yoon, Rosa; Randall, Glenn

doi:10.1371/journal.ppat.1000702

Cited by 160 publications

(210 citation statements)

References 73 publications

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“…To this end, cell lines deficient for individual key factors (8) or expressing functionally relevant variants may be very useful, especially when combined with innovative approaches that make the HCV cell entry process directly observable (10). A better understanding of the entry process may inform both the development of antiviral approaches and the development of better smallanimal models.…”

Section: Discussionmentioning

confidence: 99%

Impact of Intra- and Interspecies Variation of Occludin on Its Function as Coreceptor for Authentic Hepatitis C Virus Particles

Ciesek

Westhaus

Wicht

et al. 2011

J Virol

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Hepatitis C virus (HCV) is characterized by a narrow host range and high interindividual variability in the clinical course of infection. Both of these traits are thought to be largely due to genetic variation between species and between individual hosts. The tight junction component occludin (OCLN) is essential for HCV entry into host cells, and the differences between human and murine OCLN are thought to account in part for the inability of HCV to infect mice and hence preclude their use as a convenient small-animal model. This study assesses the impact of genetic variation in OCLN on cell culture-grown HCV (HCVcc) using a newly generated and characterized OCLN low subclone of the Huh-7.5 cell line (Huh-7.5 subclone in which endogenous OCLN expression has been downregulated by a short hairpin RNA). We report the frequency of coding nonsynonymous single nucleotide polymorphisms, i.e., polymorphisms resulting in amino acid exchanges, present in the human population and determine their ability to function as HCV (co)receptors. Moreover, we show that murine OCLN can sustain HCVcc entry, albeit with about 5-fold reduced efficiency compared to that of human OCLN. This reduction in efficiency is due solely to two amino acid residues previously identified by others using an HCV pseudoparticle approach. Finally, we use the Huh-7.5/OCLN low cell line to show that HCV spread between neighboring cells is strictly dependent on OCLN.The hepatitis C virus (HCV) is a small enveloped viral pathogen of the Flaviviridae family with a single plus-strand RNA genome (26). About 130 million individuals worldwide are currently chronically HCV infected and thus at risk for the development of cirrhosis, end-stage liver disease, and hepatocellular carcinoma (34).HCV primarily infects and replicates in hepatocytes. All stages of its replication cycle are dependent on various hostencoded factors. Completion of the earliest stage of the replication cycle, HCV cell entry, requires at least four host factors on the hepatocyte surface. These include the tetraspanin CD81 (30), scavenger receptor class B type I (SR-BI) (32), and more recently described, the tight junction components claudin 1 (CLDN1) (13) and occludin (OCLN) (27,31). It is thought that the viral envelope glycoproteins E1 and E2 interact with these four (co)receptors sequentially and that these interactions are orchestrated by cell signaling processes (6,14,28). SR-BI may act early and the tight junction components may act later in this process (11,13,21,24,42). The exact mechanisms and sequence of the interactions remain to be determined, but the result is known to be the uptake of the virion or a virion-coreceptor complex into an endosomal compartment. Acidification then triggers fusion of the viral envelope with the endosomal membrane (20,24,40). This releases the nucleocapsid into the cytosol, completing the cell entry process.Only humans and chimpanzees are natural hosts of HCV. This is thought to be because HCV is unable to utilize other species' homologues of several esse...

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Section: Discussionmentioning

confidence: 99%

Impact of Intra- and Interspecies Variation of Occludin on Its Function as Coreceptor for Authentic Hepatitis C Virus Particles

Ciesek

Westhaus

Wicht

et al. 2011

J Virol

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“…The most intuitive but work-intensive approach is to directly look at virus entry with live-cell microscopy. To this end, Coller et al labelled HCVcc with the DiD or DiI lipophilic dyes and monitored entry of single particles into target cells [154]. The main difficulties to overcome seem to be the low HCV titers and specific infectivity, making the distinction between infectious and non-infectious particles difficult.…”

Section: Dynamics Of Hcv Entrymentioning

confidence: 99%

“…Clathrin-dependent endocytosis -Internalization assay [146] -Inhibition by drugs and dominant-negative mutants -Live cell microscopy with labelled HCV [154] Low pH-mediated fusion in early endosomes -Inhibitors of endosomal acidi cation -Di erent fusion assays (see main text) Attachment and receptor interaction -Cell binding assays (CHO-SR-BI, CHO-CD81, etc) [118] -Pull-down assays [152] or ELISAs [132,153] with soluble CD81 or with heparin -Cell lines for receptor complementation (see Table 1) -Lentiviral expression vectors for the 4 speci c receptors and their homologs [104,116] H + Concanamycin A, Bafilomycin A1, Chloroquine, NH 4 Cl [69,146,147] Rab5 dominant negative mutant [145,146] Eps15 dominant negative mutant, Clathrin heavy chain siRNAs, Chlorpromazine [78,[145][146][147] Abs, Ezetimibe [32] NPC1L1 EGFR…”

Section: Highly Specific Receptors Initial Attachment Factorsmentioning

confidence: 99%

Entry and replication of recombinant hepatitis C viruses in cell culture

Vièyres

Pietschmann

2013

Methods

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“…The HCV particle finally enters the cell via clathrin-mediated endocytosis [61]. The HCV-receptor complexes then migrate to endosomal compartments [62,63] where acidification occurs to induce membrane fusion, which allows the release of viral RNA into the host cytosol.…”

Section: Overview Of Hcv Entrymentioning

confidence: 99%

Strategies to Preclude Hepatitis C Virus Entry

Burnouf¹,

Lin²

2017

Advances in Treatment of Hepatitis C and B

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Without a preventive vaccine, hepatitis C virus (HCV) remains an important pathogen worldwide with millions of carriers at risk of end-stage liver diseases. Despite the introduction of novel direct-acting antivirals (DAAs), resistance problems, challenges with the difficult-to-treat populations and high costs limit the widespread application of these drugs. Antivirals with alternative mechanism(s) of action, such as by restricting viral entry or cell-to-cell spread, could help expand the scope of antiviral strategies for the management of hepatitis C. Transfusion-associated HCV infection remains another issue in endemic and resource-limited areas around the world. This chapter describes some of the latest developments in antiviral strategies to preclude HCV entry, such as through monoclonal antibodies and small molecules, as well as measures to enhance the safety of therapeutic plasma products in blood transfusion.

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RNA Interference and Single Particle Tracking Analysis of Hepatitis C Virus Endocytosis

Cited by 160 publications

References 73 publications

Impact of Intra- and Interspecies Variation of Occludin on Its Function as Coreceptor for Authentic Hepatitis C Virus Particles

Impact of Intra- and Interspecies Variation of Occludin on Its Function as Coreceptor for Authentic Hepatitis C Virus Particles

Entry and replication of recombinant hepatitis C viruses in cell culture

Strategies to Preclude Hepatitis C Virus Entry

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