Genoepidemiology and Pathogenicity of Hepatitis G Virus in Japan

A recently discovered non-A non-B hepatitis virus has been designated hepatitis G virus (HGV). Blood contamination has been proposed as its mode of transmission. We studied the genoprevalence of HGV in Japanese people at high risk. HGV was identified in serum by a reverse-transcription polymerase ch...

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Published inThe Tohoku Journal of Experimental Medicine Vol. 183; no. 2; pp. 101 - 112
Main Authors Gama, Hiroko, Toyota, Takayoshi, Kobayashi, Koji, Niitsuma, Hirofumi, Ishii, Motoyasu, Ueno, Yoshiyuki, Kobayashi, Tomoo, Kikuchi, Kumiko, Suzuki, Chiaki
Format Journal Article
LanguageEnglish
Published Japan Tohoku University Medical Press 1997
Subjects
Adult
Base Sequence
Female
Flaviviridae - genetics
Flaviviridae - pathogenicity
Genome, Viral
genotype
hepatitis
hepatitis G virus
Hepatitis, Viral, Human - epidemiology
Hepatitis, Viral, Human - genetics
Hepatitis, Viral, Human - virology
Humans
Japan - epidemiology
Male
Middle Aged
Molecular Sequence Data
polymerase chain reaction
Virulence - genetics
Japan
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ISSN0040-8727
1349-3329
DOI10.1620/tjem.183.101

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Summary:A recently discovered non-A non-B hepatitis virus has been designated hepatitis G virus (HGV). Blood contamination has been proposed as its mode of transmission. We studied the genoprevalence of HGV in Japanese people at high risk. HGV was identified in serum by a reverse-transcription polymerase chain reaction. HGV was detected in 16.0% of intravenous drug users (IDUs) (n=25), 16.2% of those with tattoos (n=37), 10.9% of IDUs with tattoos (n=55), 5.7% of chronic hepatitis (CH)-C patients (n=87), and in none of the CH-B (n=50) or CH non-B non-C (n=46) patients. Serum alanine aminotransferase (ALT) levels of those infected with HGV alone (n=3) were all within normal range. In the patients with CH-C, serum ALT levels of those coinfected with HGV were similar to serum ALT levels of those without HGV infection. A phylogenetic tree of isolated HGV clones showed that the HGVs of these subjects bore only a distant-resemblance to clones reported from Africa and North America, and that variation in the phylogenetic index of HGV clones was small. These results suggest that HGV clones from different areas have genetic heterogeneity and that HGV causes no or mild hepatitis.
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ISSN:0040-8727
1349-3329
DOI:10.1620/tjem.183.101