Domain 3 of hepatitis C virus core protein is sufficient for intracellular lipid accumulation.
BACKGROUND: Hepatitis C virus (HCV) is a major cause of liver disease worldwide, with steatosis, or "fatty liver," being a frequent histologic finding. In previous work, we identified sequence polymorphisms within domain 3 (d3) of genotype 3 HCV core protein that correlated with steatosis and in vitro lipid accumulation. In this study, we investigated the sufficiency of d3 to promote lipid accumulation, the role of HCV genotype in d3 lipid accumulation, and the subcellular distribution of d3. METHODS: Stable cell lines expressing green fluorescent protein (GFP) fusions with isolates of HCV genotype 3 core steatosis-associated d3 (d3S), non-steatosis-associated d3 (d3NS), and genotype 1 d3 (d3G1) were analyzed by means of immunofluorescence, oil red O (ORO) staining, and triglyceride quantitation. RESULTS: Cells that expressed d3S had statistically significantly more ORO than did cells expressing d3NS or d3G1 (P=.02 and <.001, respectively), as well as higher triglyceride levels P =.03 and .003, respectively). Immunofluorescence analysis showed that d3 does not colocalize to lipid droplets but partially colocalizes to the Golgi apparatus. CONCLUSIONS: Our results suggest that HCV core d3 is sufficient to mediate the accumulation of lipid by means of a mechanism that is independent of domains 1 and 2. Our results also suggest that altered lipid trafficking may be involved.
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Related Subject Headings
- Viral Core Proteins
- Triglycerides
- Stress, Physiological
- Reproducibility of Results
- Recombinant Fusion Proteins
- Rats
- Protein Structure, Tertiary
- Molecular Sequence Data
- Microscopy, Fluorescence
- Microbiology
Citation
Published In
DOI
EISSN
Publication Date
Volume
Issue
Start / End Page
Location
Related Subject Headings
- Viral Core Proteins
- Triglycerides
- Stress, Physiological
- Reproducibility of Results
- Recombinant Fusion Proteins
- Rats
- Protein Structure, Tertiary
- Molecular Sequence Data
- Microscopy, Fluorescence
- Microbiology