Structures of perforin-2 in solution and on a membrane reveal mechanisms for pore formation

Abstract

AbstractPerforin-2 (PFN2, MPEG1) is a key pore-forming protein in mammalian innate immunity restricting intracellular bacteria proliferation. It forms a membrane-bound pre-pore complex that converts to a pore-forming structure upon acidification; but its mechanism of conformational transition has been debated. Here we used cryo-electron microscopy, tomography and subtomogram averaging to determine structures of PFN2 in pre-pore and pore conformations in isolation and bound to liposomes. In isolation and upon acidification, the pre-assembled complete pre-pore rings convert to pores in both flat ring and twisted conformations. The twisted pore structure suggests an intermediate or alternative state to the flat conformation, and a capacity to distort the underlying membrane during membrane insertion. On membranes, in situ assembled PFN2 pre-pores display various degrees of completeness; whereas PFN2 pores are mainly incomplete arc structures that follow the same subunit packing arrangements as found in isolation. Both assemblies on membranes use their P2 β-hairpin for binding to the lipid membrane surface. These structural snapshots in different states reveal a molecular mechanism for PFN2 pre-pore to pore transition on a targeted membrane.