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Cellular vacuolization and apoptosis induced by hepatitis B virus large surface protein

โœ Scribed by Ngee-Chih Foo; Byung Y. Ahn; Xiaohong Ma; William Hyun; T. S. Benedict Yen


Book ID
102849018
Publisher
John Wiley and Sons
Year
2002
Tongue
English
Weight
1006 KB
Volume
36
Category
Article
ISSN
0270-9139

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โœฆ Synopsis


Fibrosing cholestatic hepatitis (FCH) is a rapidly progressive form of viral hepatitis B that occurs in severely immunosuppressed patients. Pathologically, the liver in FCH is characterized by widespread hepatocyte vacuolization and apoptosis, which, in contrast to more common forms of hepatitis B, is only rarely associated with significant inflammation. Therefore, it has been proposed that, in FCH, hepatocytes may be injured by a direct cytopathic effect of the virus rather than by the host immune response. In support of this hypothesis, we present evidence that cultured hepatoma cells that had been transfected with a plasmid selectively expressing the viral large surface protein form numerous large vacuoles and undergo apoptosis. The similarity of the cytopathology in FCH in vivo and in these transfected cells in vitro strongly implicates the large surface protein as the direct cause of this acute liver disease. This conclusion is further supported by the published demonstration that hepatocytes tend to accumulate large surface protein in FCH, which may reflect its overexpression by the virus. In conclusion, our data implicate the large surface protein as a major cause of hepatocyte injury in fibrosing cholestatic hepatitis.


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Hepatitis B virus X protein induces apop
โœ Hye Jin Kim; Sang Yong Kim; Jinchul Kim; Heemin Lee; Misun Choi; Jeong Ki Kim; J ๐Ÿ“‚ Article ๐Ÿ“… 2008 ๐Ÿ› John Wiley and Sons ๐ŸŒ English โš– 408 KB

## Abstract Hepatitis B virus X protein (HBx) is essential for viral replication and plays an important role in viral pathogenesis. HBx transactivates many viral and cellular genes and participates in cellular signal transduction pathways, proliferation, and apoptosis. In the present study, we repo