GB virus C (GBV-C), formerly known as hepatitis G virus (HGV), is a virus in the Flaviviridae family which has not yet been assigned to a genus, is known to infect humans, but is not known to cause human disease. There have been reports that HIV patients coinfected with GBV-C can survive longer than those without GBV-C, but the patients may be different in other ways. There is current active research into the virus' effects on the immune system in patients coinfected with GBV-C and HIV.^[1][2]

History

Hepatitis G virus and GB virus C (GBV-C) are RNA viruses that were independently identified in 1995, and were subsequently found to be two isolates of the same virus.^[3][4][5][6] Although GBV-C was initially thought to be associated with chronic hepatitis, extensive investigation failed to identify any association between this virus and any clinical illness.^[7] GB Virus C (and indeed, GBV-A and GBV-B) is named after the surgeon, G. Barker, who fell ill in 1966 with a non-A non-B hepatitis which at the time was thought to have been caused by a new, infectious hepatic virus.^[8]

Taxonomy

GBV-C is a member of the Flaviviridae family and is phylogenetically related to hepatitis C virus but appears to replicate primarily in lymphocytes, and poorly if at all in hepatocytes.^[9][10] GBV-A and GBV-B are probably tamarin viruses, while GBV-C infects humans.^[11] The GB viruses have been tentatively assigned to a fourth genus within the Flavivirdae named "Pegivirus", but this has yet to be formally endorsed by The International Committee on Taxonomy of Viruses.^[12]

Another member of this clade GBV-D has been isolated from a bat (Pteropus giganteus).^[13] It appears that GBV-D is ancestral to GBV-A and GBV-C.

The mutation rate of the genome has been estimated at 10^-2 to 10^-3 substitutions/site/year.^[14]

Epidemiology

GBV-C infection has been found worldwide. High prevalence is observed among subjects with the risk of parenteral exposures including those with exposure to blood and blood products, those on hemodialysis, and intravenous drug users. Sexual contact and vertical transmission may occur. ~10–25% of hepatitis C infected patients and 14–36% of drug users who are seropositive for HIV-1 show the evidence of GBV-C infection.

It has been classified into six genotypes and many subtypes with distinct geographical distributions. A seventh has also been described.^[15]

Genotype 1 is predominant in Africa and is divided into five subtypes. Genotype 2 has three subtypes and is found in Europe and America. Genotype 3 is the most common in Asia including Japan and China. Genotype 4 is predominant in Southeast Asia and genotype 5 is only seen in South Africa. Genotype 6 has been described in Indonesia.

Virology

It has a single stranded positive RNA genome of about 9.3 kb and contains a single open reading frame (ORF) encoding two structural (E1 and E2) and five non-structural (NS2, NS3, NS4, NS5A, and NS5B) proteins.

Human infection

The majority of immune-competent individuals appear to clear GBV-C viraemia within the first few years following infection and although the time interval between GBV-C infection and clearance of viraemia (detection of GBV-C RNA in plasma) is not known, infection may persist for decades in some individuals.

Approximately 2% of healthy US blood donors are viraemic with GBV-C, and up to 13% of blood donors have antibodies to E2 protein, indicating prior infection.

Parenteral, sexual and vertical transmission of GBV-C have all been documented, and because of shared modes of transmission, individuals infected with HIV are commonly co-infected with GBV-C. Among people with HIV infection, the prevalence of GBV-C viraemia ranges from 14 to 43%.^[16]

Some studies have suggested that co-infection with GBV-C slows the progression of HIV disease.^[17]

References

External links

• GBV-C at the US National Library of Medicine Medical Subject Headings (MeSH)