Despite important progress toward deciphering human hepatitis B virus (HBV) entry into host cells, many aspects of the early steps of the life cycle remained completely obscure. Following endocytosis, HBV must travel through the complex network of the endocytic pathway to reach the cell nucleus and initiate replication. In addition to guiding the viral particles to the replication site, the endosomal vesicles may play a crucial role in infection, providing the appropriate environment for virus uncoating and nucleocapsid release. In this work, we investigated the trafficking of HBV particles internalized in permissive cells. Expression of key Rab proteins, involved in specific pathways leading to different intracellular locations, was modulated in HepaRG cells, using a stable and inducible short hairpin RNA (shRNA) expression system. The trafficking properties of the newly developed cells were demonstrated by confocal microscopy and flow cytometry using specific markers. The results showed that HBV infection strongly depends on Rab5 and Rab7 expression, indicating that HBV transport from early to mature endosomes is required for a step in the viral life cycle. This may involve reduction of disulfide bond-linked envelope proteins, as alteration of the redox potential of the endocytic pathway resulted in inhibition of infection. Subcellular fractionation of HBV-infected cells showed that viral particles are further transported to lysosomes. Intriguingly, infection was not dependent on the lysosomal activity, suggesting that trafficking to this compartment is a "dead-end" route. Together, these data add to our understanding of the HBV-host cell interactions controlling the early stages of infection. C hronic hepatitis B virus (HBV) infections can lead to lifethreatening liver diseases, such as cirrhosis and hepatocellular carcinoma, the third cause of cancer deaths worldwide (1). Infectious viral particles consist of an icosahedral nucleocapsid made of the core protein and a lipid bilayer embedding the small (S), middle (M), and large (L) envelope proteins (2). The nucleocapsid surrounds the relaxed circular, partially double-stranded DNA genome, to which the viral polymerase is covalently attached (3). Apart from the crucial roles played in virus morphogenesis and infection, the envelope proteins bear the intriguing property to self-assemble into spherical and filamentous subviral particles (SVP), which are released from cells in vast excess over virions, accounting for more than 90% of the total particles in the serum of infected patients (4).Studies regarding the early events of the HBV life cycle have been particularly problematic, as human primary hepatocytes, the physiological host, are difficult to procure and maintain in tissue culture and are refractory to genetic manipulation. The development of alternative infectivity models for HBV, represented by proliferating liver-derived cell lines able to differentiate and support HBV infection in vitro, has considerably overcome many of these drawbacks (5-7). Moreo...
