<link file:4038 download file>Dr. Laurence Cocquerel,
<link file:4038 download file>Center for Infection and Immunity of Lille (CIIL), Pasteur Institute of Lille, University of Lille, France,
<link file:4038 download file>Title: New insights into the understanding of Hepatitis E Virus lifecycle,
<link file:4038 download file>Time: 5 pm,
Location: TWINCORE Lecture Hall (0.02)
Abstract
Hepatitis E virus (HEV) is a major cause of enterically transmitted hepatitis worldwide. It is responsible for over 50% of acute viral hepatitis cases and approximately 2 billion people live in areas endemic for HEV and thus are at risk of infection. HEV is a small non-enveloped virus whose genome is a positive-strand RNA that encodes three open reading frames (ORFs) called ORF1, ORF2 and ORF3. Detailed analyses of HEV lifecycle have been for a long time hampered by the lack of an efficient viral culture system. Here, we describe a robust HEV cell culture system for which RNA, infectious viral particles and expression of ORF2/ORF3 proteins were detected very early in time-course experiments. Purification on iodixanol gradient of infectious supernatant led to the isolation of cell culture produced HEV particles that were infectious in vitro and in human liver chimeric mice. Importantly, for the first time, we defined the ultrastructure of cell culture-produced HEV particles by transmission electron microscopy and analyzed the sequence of infectious particle-associated ORF2 capsid protein by nanoscale liquid chromatography coupled to tandem mass spectrometry. Strikingly, our analyses also revealed that, in cell culture and in infected patients, HEV produces three forms of the ORF2 capsid protein named ORF2i, ORF2g and ORF2c. The ORF2i protein is associated with infectious particles whereas ORF2g and ORF2c proteins are massively produced glycoproteins that are not associated with infectious particles and are the major antigens present in HEV-infected patient sera.
Who is Laurence Cocquerel?
Laurence Cocquerel received her Ph. D degree in 2001 from the University of Paris VII. During her thesis, she characterized the transmembrane domains of the hepatitis C virus (HCV) envelope glycoproteins and, received a Ph. D Thesis award from the TransHepat Association. She did a post-doctoral training from 2001 to 2003 at the Stanford University in the United States. She worked on the interaction of HCV glycoproteins with the tetraspanin CD81. In 2003, she came back to Jean Dubuisson’s laboratory as a CNRS scientist. Currently, she works on cellular aspects of the HCV entry
Contact: <link internal link in current>Dr. Gisa Gerold