Stonefish toxin defines an ancient branch of the perforin-like superfamily
Author(s) -
Andrew M. Ellisdon,
Cyril F. Reboul,
Santosh Panjikar,
Kitmun Huynh,
Christine A. Oellig,
Kelly L. Winter,
Michelle A. Dunstone,
Wayne C. Hodgson,
Jamie Seymour,
Peter K. Dearden,
Rodney K. Tweten,
James C. Whisstock,
Sheena McGowan
Publication year - 2015
Publication title -
proceedings of the national academy of sciences
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.011
H-Index - 771
eISSN - 1091-6490
pISSN - 0027-8424
DOI - 10.1073/pnas.1507622112
Subject(s) - perforin , biology , complement membrane attack complex , microbiology and biotechnology , protein domain , immune system , genetics , complement system , gene , cd8
The lethal factor in stonefish venom is stonustoxin (SNTX), a heterodimeric cytolytic protein that induces cardiovascular collapse in humans and native predators. Here, using X-ray crystallography, we make the unexpected finding that SNTX is a pore-forming member of an ancient branch of the Membrane Attack Complex-Perforin/Cholesterol-Dependent Cytolysin (MACPF/CDC) superfamily. SNTX comprises two homologous subunits (α and β), each of which comprises an N-terminal pore-forming MACPF/CDC domain, a central focal adhesion-targeting domain, a thioredoxin domain, and a C-terminal tripartite motif family-like PRY SPla and the RYanodine Receptor immune recognition domain. Crucially, the structure reveals that the two MACPF domains are in complex with one another and arranged into a stable early prepore-like assembly. These data provide long sought after near-atomic resolution insights into how MACPF/CDC proteins assemble into prepores on the surface of membranes. Furthermore, our analyses reveal that SNTX-like MACPF/CDCs are distributed throughout eukaryotic life and play a broader, possibly immune-related function outside venom.
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