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A Cell Culture Model for Producing High Titer Hepatitis E Virus Stocks

Toni Luise Meister, Mara Klöhn, Eike Steinmann, Daniel Tödt

2020Journal of Visualized Experiments17 citationsDOIOpen Access PDF

Abstract

Hepatitis E virus is the leading cause of liver cirrhosis and liver failure with increasing prevalence worldwide. The single-stranded RNA virus is predominantly transmitted by blood transfusions, inadequate sanitary conditions and contaminated food products. To date the off-label drug ribavirin (RBV) is the treatment of choice for many patients. Nonetheless, a specific HEV treatment remains to be identified. So far, the knowledge about the HEV life cycle and pathogenesis has been severely hampered because of the lack of an efficient HEV cell culture system. A robust cell culture system is essential for the study of the viral life cycle which also includes the viral pathogenesis. With the method described here one can produce viral titers of up to 3 x 106 focus forming unit/mL (FFU/mL) of non-enveloped HEV and up to 5 x 104 FFU/mL of enveloped HEV. Using these particles, it is possible to infect a variety of cells of diverse origins including primary cells and human, as well as animal cell lines. The production of infectious HEV particles from plasmids poses an infinite source, which makes this protocol exceedingly efficient.

Topics & Concepts

VirologyHepatitis E virusVirusViral life cycleBiologyTiterViral hepatitisCell cultureRibavirinPathogenesisMedicineImmunologyMicrobiologyHepatitis C virusViral replicationGeneBiochemistryGenotypeGeneticsHepatitis Viruses Studies and EpidemiologyViral gastroenteritis research and epidemiologyHepatitis C virus research