posted on 2019-03-28, 00:00authored byMinetaro Arita, Joëlle Bigay
Phosphatidylinositol-4 kinase III
β (PI4KB) and oxysterol-binding protein (OSBP) family I provide
a conserved host pathway required for enterovirus replication. Here,
we analyze the role and essentiality of this pathway in enterovirus
replication. Phosphatidylinositol 4-phosphate (PI4P) production and
cholesterol accumulation in the replication organelle (RO) are severely
suppressed in cells infected with a poliovirus (PV) mutant isolated
from a PI4KB-knockout cell line (RD[ΔPI4KB]). Major determinants of the mutant for infectivity
in RD(ΔPI4KB) cells map to the A5270U(3A-R54W)
and U3881C(2B-F17L) mutations. The 3A mutation is required for PI4KB-independent
development of RO. The 2B mutation rather sensitizes PV to PI4KB/OSBP
inhibitors by itself but confers substantially complete resistance
to the inhibitors with the 3A mutation. The 2B mutation also confers
hypersensitivity to interferon alpha treatment on PV. These suggest
that the PI4KB/OSBP pathway is not necessarily essential for enterovirus
replication in vitro. This work supports a two-step
resistance model of enterovirus to PI4KB/OSBP inhibitors involving
unique recessive epistasis of 3A and 2B and offers insights into a
potential evolutionary pathway of enterovirus toward independence
from the PI4KB/OSBP pathway.