Three-dimensional structure of poliovirus receptor bound to poliovirus

摘要

Poliovirus initiates infection by binding to its cellular receptor (Pvr). We have studied this interaction by using cryoelectron microscopy to determine the structure. at 21-A resolution, of poIiovirus com- plexed with a soluble form of its receptor (sPvr). This density map aided construction of a homology-based model of sPvr and, in conjunction with the known crystal structure of the virus. allowed delineation of the binding site. The virion does not change signif- icantly in structure on binding sPvr in short incubations at 4℃. We infer that the binding configuration visualized represents the initial interaction that is followed by structural changes in the virion as infection proceeds. sPvr is segmented into three well- defined lg-like domains. The two domains closest to the virion (domains 1 and 2) are aligned and rigidly connected, whereas domain 3 diverges at an angle of ≈60°. Two nodules of density on domain 2 are identified as glycosylation sites. Domain 1 penetrates the "canyon" that surrounds the 5-fold protrusion on the capsid Surface, and its binding site involves all three major capsid pro- teins. The inferred pattern of virus--sPvr interactions accounts for most mutations that affect the binding of Pvr to poliovirus.