Interaction of a pseudosubstrate peptide of protein kinase C and its myristoylated form with lipid vesicles: only the myristoylated form translocates into the lipid bilayer

Harishchandran, Avaronnan ; Nagaraj, Ramakrishnan (2005) Interaction of a pseudosubstrate peptide of protein kinase C and its myristoylated form with lipid vesicles: only the myristoylated form translocates into the lipid bilayer Biochimica et Biophysica Acta: Biomembranes, 1713 (2). pp. 73-82. ISSN 0005-2736

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Official URL: http://linkinghub.elsevier.com/retrieve/pii/S00052...

Related URL: http://dx.doi.org/10.1016/j.bbamem.2005.05.008

Abstract

Lipopeptides derived from protein kinase C (PKC) pseudosubstrates have the ability to cross the plasma membrane in cells and modulate the activity of PKC in the cytoplasm. Myristoylation or palmitoylation appears to promote translocation across membranes, as the non-acylated peptides are membrane impermeant. We have investigated, by fluorescence spectroscopy, how myristoylation modulates the interaction of the PKC pseudosubstrate peptide KSIYRRGARRWRKL with lipid vesicles and translocation across the lipid bilayer. Our results indicate that myristoylated peptides are intimately associated with lipid vesicles and are not peripherally bound. When visualized under a microscope, myristoylation does appear to facilitate translocation across the lipid bilayer in multilamellar lipid vesicles. Translocation does not involve large-scale destabilization of the bilayer structure. Myristoylation promotes translocation into the hydrophobic interior of the lipid bilayer even when the non-acylated peptide has only weak affinity for membranes and is also only peripherally associated with lipid vesicles.

Item Type:Article
Source:Copyright of this article belongs to Elsevier Science.
Keywords:Fatty Acylated Peptide; Lipid Vesicle; Fluorescence Spectroscopy; Translocation across Membrane; Membrane Binding; Membrane Perturbation
ID Code:24047
Deposited On:01 Dec 2010 12:41
Last Modified:23 Jan 2011 17:40

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