Plumieribetin, a fish lectin homologous to mannose-binding B-type lectins, inhibits the collagen-binding alpha1beta1 integrin

Recently, a few fish proteins have been described with a high homology to B-type lectins of monocotyledonous plants. Because of their mannose binding activity, they have been ascribed a role in innate immunity. By screening various fish venoms for their integrin inhibitory activity, we isolated a ho...

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Bibliographic Details
Published in:The Journal of biological chemistry 2009-12, Vol.284 (50), p.34747
Main Authors: de Santana Evangelista, Karla, Andrich, Filipe, Figueiredo de Rezende, Flávia, Niland, Stephan, Cordeiro, Marta N, Horlacher, Tim, Castelli, Riccardo, Schmidt-Hederich, Alletta, Seeberger, Peter H, Sanchez, Eladio F, Richardson, Michael, Gomes de Figueiredo, Suely, Eble, Johannes A
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Animals
Carbohydrate Conformation
Carbohydrate Sequence
Cell Adhesion - physiology
Cell Line
Collagen Type IV - metabolism
Fishes
Humans
Integrin alpha1beta1 - metabolism
Lectins - chemistry
Lectins - genetics
Lectins - metabolism
Microarray Analysis
Molecular Sequence Data
Protein Conformation
Sequence Alignment
Venoms - chemistry
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Summary:Recently, a few fish proteins have been described with a high homology to B-type lectins of monocotyledonous plants. Because of their mannose binding activity, they have been ascribed a role in innate immunity. By screening various fish venoms for their integrin inhibitory activity, we isolated a homologous protein from the fin stings and skin mucus of the scorpionfish (Scorpaena plumieri). This protein inhibits alpha1beta1 integrin binding to basement membrane collagen IV. By protein chemical and spectroscopic means, we demonstrated that this fish protein, called plumieribetin, is a homotetramer and contains a high content of anti-parallel beta strands, similar to the mannose-binding monocot B-lectins. It lacks both N-linked glycoconjugates and common O-glycan motifs. Despite its B-lectin-like structure, plumieribetin binds to alpha1beta1 integrin irrespective of N-glycosylation, suggesting a direct protein-protein interaction. This interaction is independent of divalent cations. On the cellular level, plumieribetin failed to completely detach hepatocarcinoma HepG2 cells and primary arterial smooth muscle cells from the collagen IV fragment CB3. However, plumieribetin weakened the cell-collagen contacts, reduced cell spreading, and altered the actin cytoskeleton, after the compensating alpha2beta1 integrin was blocked. The integrin inhibiting effect of plumieribetin adds a new function to the B-lectin family, which is known for pathogen defense.
ISSN:1083-351X
DOI:10.1074/jbc.M109.002873