Literature DB >> 30237168

Membrane curvature allosterically regulates the phosphatidylinositol cycle, controlling its rate and acyl-chain composition of its lipid intermediates.

José Carlos Bozelli1, William Jennings1, Stephanie Black1, Yu Heng Hou1, Darius Lameire1, Preet Chatha1, Tomohiro Kimura1, Bob Berno2, Adree Khondker3, Maikel C Rheinstädter3, Richard M Epand4.   

Abstract

Signaling events at membranes are often mediated by membrane lipid composition or membrane physical properties. These membrane properties could act either by favoring the membrane binding of downstream effectors or by modulating their activity. Several proteins can sense/generate membrane physical curvature (i.e. shape). However, the modulation of the activity of enzymes by a membrane's shape has not yet been reported. Here, using a cell-free assay with purified diacylglycerol kinase ϵ (DGKϵ) and liposomes, we studied the activity and acyl-chain specificity of an enzyme of the phosphatidylinositol (PI) cycle, DGKϵ. By systematically varying the model membrane lipid composition and physical properties, we found that DGKϵ has low activity and lacks acyl-chain specificity in locally flat membranes, regardless of the lipid composition. On the other hand, these enzyme properties were greatly enhanced in membrane structures with a negative Gaussian curvature. We also found that this is not a consequence of preferential binding of the enzyme to those structures, but rather is due to a curvature-mediated allosteric regulation of DGKϵ activity and acyl-chain specificity. Moreover, in a fine-tuned interplay between the enzyme and the membrane, DGKϵ favored the formation of structures with greater Gaussian curvature. DGKϵ does not bear a regulatory domain, and these findings reveal the importance of membrane curvature in regulating DGKϵ activity and acyl-chain specificity. Hence, this study highlights that a hierarchic coupling of membrane physical property and lipid composition synergistically regulates membrane signaling events. We propose that this regulatory mechanism of membrane-associated enzyme activity is likely more common than is currently appreciated.
© 2018 Bozelli et al.

Entities:  

Keywords:  PM-ER junctions; allostery; contact sites; diacylglycerol; diacylglycerol kinase (DGK, DAGK); endoplasmic reticulum (ER); lipid signaling; lipid trafficking; membrane biophysics; membrane enzyme; membrane lipid; membrane protein; membrane shape; membrane trafficking; negative Gaussian curvature; phosphatidylinositol cycle; phosphatidylinositol signaling; plasma membrane; regulation of enzyme by membrane curvature

Mesh:

Substances:

Year:  2018        PMID: 30237168      PMCID: PMC6240852          DOI: 10.1074/jbc.RA118.005293

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.486


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