Binding of DEP domain to phospholipid membranes: More than just electrostatics

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Authors

FALGINELLA Francesco Luca KRAVEC Marek DRABINOVÁ Martina PACLÍKOVÁ Petra BRYJA Vítězslav VÁCHA Robert

Year of publication 2022
Type Article in Periodical
Magazine / Source Biochimica et Biophysica Acta (BBA) - Biomembranes
MU Faculty or unit

Central European Institute of Technology

Citation
web https://doi.org/10.1016/j.bbamem.2022.183983
Doi http://dx.doi.org/10.1016/j.bbamem.2022.183983
Keywords DVL protein; DEP domain; Lipid membrane; Molecular dynamics; Flow cytometry; QCM-D; Lipid preference; Phosphatidylserine; Phosphatidic acid; Phosphatidylinositol
Attached files
Description Over the past decades an extensive effort has been made to provide a more comprehensive understanding of Wnt signaling, yet many regulatory and structural aspects remain elusive. Among these, the ability of Dishevelled (DVL) protein to relocalize at the plasma membrane is a crucial step in the activation of all Wnt pathways. The membrane binding of DVL was suggested to be mediated by the preferential interaction of its C-terminal DEP domain with phosphatidic acid (PA). However, due to the scarcity and fast turnover of PA, we investigated the role on the membrane association of other more abundant phospholipids. The combined results from computational simulations and experimental measurements with various model phospholipid membranes, demonstrate that the membrane binding of DEP/DVL constructs is governed by the concerted action of generic electrostatics and finely-tuned intermolecular interactions with individual lipid species. In particular, while we confirmed the strong preference for PA lipid, we also observed a weak but non-negligible affinity for phosphatidylserine, the most abundant anionic phospholipid in the plasma membrane, and phosphatidylinositol 4,5-bisphosphate. The obtained molecular insight into DEP-membrane interaction helps to elucidate the relation between changes in the local membrane composition and the spatiotemporal localization of DVL and, possibly, other DEP-containing proteins.
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