Everything about Hepatitis C Virus totally explained
» This page is for the virus. For the disease, see Hepatitis C.
Hepatitis C virus (
HCV) is a small (50
nm in size), enveloped,
positive sense single strand
RNA virus in the family
Flaviviridae. Although
Hepatitis A virus,
Hepatitis B virus, and Hepatitis C virus have similar names (because they all cause
liver inflammation), these are distinctly different viruses both genetically and clinically.
Structure
The structure of the hepatitis C virus consists of a core of genetic material (RNA), surrounded by an
icosahedral protective shell of
protein, and further encased in a lipid (fatty) envelope of cellular origin. Two viral envelope
glycoproteins, E1 and E2, are embedded in the lipid envelope.
Genome
Hepatitis C virus has a positive sense
RNA genome that consists of a single
open reading frame of 9600
nucleoside bases. At the 5’ and 3’ ends of the RNA there are regions, (UTR), that are not translated into proteins but are important to translation and replication of the viral RNA. The 5’ UTR has a
ribosome binding site (IRES - Internal Ribosomal Entry Site) that starts the translation of a 3000 amino acid containing protein that's later cut by cellular and viral
proteases into 10 active structural and non-structural smaller proteins.
Replication
Replication of HCV involves several steps. The viruses need a certain environment to be able to replicate, and must therefore first move to such areas.
HCV has a high rate of replication with approximately one trillion particles produced each day in an infected individual. Due to lack of proofreading by the HCV RNA polymerase, HCV also has an exceptionally high mutation rate, a factor that may help it elude the host's immune response.
HCV mainly replicates within
hepatocytes in the liver, although there's controversial evidence for replication in
lymphocytes or
monocytes. By mechanisms of
host tropism, the viruses reach these proper locations. Circulating HCV particles bind to
receptors on the surfaces of hepatocytes and subsequently enter the cells. Two putative HCV receptors are
CD81 and human
scavenger receptor class B1 (SR-BI). However, these receptors are found throughout the body. The identification of hepatocyte-specific cofactors that determine observed HCV liver
tropism are currently under investigation.
Once inside the hepatocyte, HCV initiates the
lytic cycle. It utilizes the intracellular machinery necessary to accomplish its own replication.
Specifically, the HCV genome is
translated to produce a single protein of around 3011 amino acids. This "polyprotein" is then proteolytically processed by viral and cellular
proteases to produce three structural (virion-associated) and seven nonstructural (NS) proteins. Alternatively, a frameshift may occur in the Core region to produce an Alternate Reading Frame Protein (ARFP). HCV encodes two proteases, the NS2 cysteine autoprotease and the NS3-4A serine protease. The NS proteins then recruit the viral genome into an RNA replication complex, which is associated with rearranged cytoplasmic membranes. RNA replication takes places via the viral RNA-dependent
RNA polymerase of NS5B, which produces a negative-strand RNA intermediate. The negative strand RNA then serves as a template for the production of new positive-strand viral genomes. Nascent genomes can then be translated, further replicated, or packaged within new virus particles. New virus particles presumably bud into the secretory pathway and are released at the cell surface.
Genotypes
Based on genetic differences between HCV isolates, the hepatitis C virus species is classified into six
genotypes (1-6) with several subtypes within each genotype (represented by letters). Subtypes are further broken down into quasispecies based on their genetic diversity. The preponderance and distribution of HCV genotypes varies globally. For example, in
North America, genotype 1a predominates followed by 1b, 2a, 2b, and 3a. In
Europe, genotype 1b is predominant followed by 2a, 2b, 2c, and 3a. Genotypes 4 and 5 are found almost exclusively in
Africa. Genotype is clinically important in determining potential response to
interferon-based therapy and the required duration of such therapy. Genotypes 1 and 4 are less responsive to
interferon-based treatment than are the other genotypes (2, 3, 5 and 6).
Duration of standard interferon-based therapy for genotypes 1 and 4 is 48 weeks, whereas treatment for genotypes 2 and 3 is completed in 24 weeks.
Vaccination
Unlike hepatitis A and B, there's currently no
vaccine to prevent hepatitis C infection.
In a 2006 study, 60 patients received four different doses of an experimental hepatitis C vaccine. All the patients produced
antibodies that the researchers believe could protect them from the virus.
Current Research
In 2007 the World Community Grid launched a project where, by computer modeling of the Hepatitis C Virus (and related viruses), thousands of small molecules are screened for their potential anti-viral properties in fighting the Hepatitis C Virus. This is the first project to seek out medicines to directly attack the virus once a person is infected. This is a distributed process project similar to
SETI@Home where the general public downloads the World Community Grid agent and the program (along with thousands of other users) screens thousands of molecules while their computer would be otherwise idle. If the user needs to use the computer the program sleeps. There are several different projects running, including a similar one screening for anti-AIDS drugs. The project covering the Hepatitis C Virus is called "Discovering Dengue Drugs – Together." (
Dengue virus and HCV belong to the same familly, together with
West Nile and
Yellow fever viruses
(External Link
)). The software and information about the project can be found at the World Community Grid web site.
(External Link)
Current research is focused in virus'
protease inhibitors, with drugs such as
Telaprevir. Barriers to the study of HCV include that fact that HCV has a very narrow host range. Hence the only animal model viable for HCV study is the
chimpanzee. The use of
replicons has been very successful as well but has only been recently discovered. Finally, HCV, as with most all
RNA viruses, exists as a
viral quasispecies, making it very difficult to isolate a single strain or receptor type for study.
Further Information
Get more info on 'Hepatitis C Virus'.
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