These observations, as well as the

These observations, as well as the low density of HCV viral particles and their association with
apolipoproteins like apoB, apoE, apoC1 [20,22,31] led to the idea that HCV particle morphogenesis
intersects the VLDL secretion pathway. VLDL formation begins with cotranslational association of
apoB with the nascent lipoprotein formed by MTP mediated lipid accumulation between ER leaflets.
Several reports showed that apoB and MTP are essential for HCV assembly [21,207]. Thus, one may
imagine that the pushing force of lipid accumulation between ER leaflets during pre-VLDL biogenesis
would lead to virion budding resulting in the formation of a LVP (Figure 3). This hybrid particle should
be associated to apoB which was reported for both patient-derived and HCVcc virions [31]. On the other
hand, later reports showed that while apoB is dispensable for HCV secretion, apoE and MTP are not [41].
Moreover, the mere presence of apoE can lead to the production of infectious particles in non-hepatic
cells, suggesting the crucial role of this protein in HCV infectivity [208,209]. Interestingly, Hueging et al.
showed that the role of apoE in HCV infectivity is in a post-envelopment step [209]. This would imply
an apoE-HCV particle interaction in a post-budding step possibly by direct envelope-apoE interaction
as it was recently reported [31,32]. A LVP as depicted in Figure 3 might be imagined as the interaction
between intraluminal LD harboring apoE and an immature HCV particle. The nascent particle matures
further in a post-ER step to get to the low density of an infectious particle [21]. HCV particle takes the
secretory pathway and its secretion depends on classical host factors of the secretory pathway [188].