Author:
Ning Yun-Jia,Deng Fei,Hu Zhihong,Wang Hualin
Abstract
AbstractEbolaviruses are highly dangerous pathogens exhibiting extreme virulence in humans
and nonhuman primates. The majority of ebolavirus species, most notably Zaire ebolavirus, can cause Ebola virus disease (EVD),
formerly known as Ebola hemorrhagic fever, in humans. EVD is associated with
case-fatality rates as high as 90%, and there is currently no specific treatment or
licensed vaccine available against EVD. Understanding the molecular biology and
pathogenesis of ebolaviruses is important for the development of antiviral
therapeutics. Ebolavirus encodes several forms of glycoproteins (GPs), which have
some interesting characteristics, including the transcriptional editing coding
strategy and extensive O-glycosylation modification, clustered in the mucin-like
domain of GP1, full-length GP (GP1,2), and shed GP. In
addition to the canonical role of the spike protein, GP1,2,
in viral entry, ebolavirus GPs appear to have multiple additional functions, likely
contributing to the complex pathogenesis of the virus. Here, we review the roles of
ebolavirus GPs in viral pathogenesis.
Subject
Virology,Molecular Medicine,Immunology
Cited by
16 articles.
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