Induction of raft‐like domains by a myristoylated NAP‐22 peptide and its Tyr mutant

Epand, Richard M.; Sayer, Brian G.

doi:10.1111/j.1742-4658.2005.04612.x

Cited by 23 publications

(29 citation statements)

References 48 publications

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“…The ability of NAP-22 to influence the distribution of PtdIns(4,5)P 2 and cholesterol in membranes provides a mechanism by which this protein can influence the actin cytoskeleton (Epand et al, 2003a(Epand et al, ,b, 2001(Epand et al, , 2004. Since NAP-22 sequesters both cholesterol and PtdIns(4,5)P 2 into domains, it has been suggested that the protein recruits PtdIns(4,5)P 2 into raft-like domains and increases cytoskeleton/plasma membrane interactions through rafts that induce spatial rearrangements of the cytoskeleton (Epand et al, 2005a). In a bilayer that phase-segregates into l o (enriched in Chol and SM) and DOPC-enriched (l d ) domains, it was found that the fulllength NAP-22 inserts almost exclusively into the l o domain (Khan et al, 2003).…”

Section: Discussionmentioning

confidence: 97%

“…Inset: corresponding section analyses along A-A 0 . PtdIns(4,5)P 2 (Epand et al, 2005a(Epand et al, ,c, 2004. As the NAP-22 peptide concentration increases in the l d domain, it is likely that the peptide would start to recruit more cholesterol from the SM/Chol domain.…”

Section: Discussionmentioning

confidence: 97%

“…Corresponding to the amino terminus of the NAP-22 protein, the smaller NAP-22 peptide has a weaker ability to sequester cholesterol from a mixture of SOPC and cholesterol (Epand et al, 2005a), and thus may be less able to selectively partition into l o versus l d domains. This peptide has also been shown to sequester PtdIns(4,5)P 2 into domains in a cholesteroldependent manner in an SOPC/cholesterol mixture (Epand et al, 2004).…”

Section: Discussionmentioning

confidence: 99%

“…Recently, it was demonstrated that NAP-22 peptide inserts into membranes, sequesters PtdIns(4,5)P 2 in a cholesteroldependent manner, and induces formation of a cholesterol-depleted domain (Epand et al, 2004(Epand et al, , 2005a. The formation of membrane domains containing both cholesterol and PtdIns(4,5)P 2 is also promoted by a peptide segment of caveolin (Wanaski et al, 2003).…”

Section: Introductionmentioning

confidence: 97%

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Tracking peptide–membrane interactions: Insights from in situ coupled confocal-atomic force microscopy imaging of NAP-22 peptide insertion and assembly

Shaw

Epand

Sinnathamby

et al. 2006

Journal of Structural Biology

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Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 97%

See 2 more Smart Citations

Tracking peptide–membrane interactions: Insights from in situ coupled confocal-atomic force microscopy imaging of NAP-22 peptide insertion and assembly

Shaw

Epand

Sinnathamby

et al. 2006

Journal of Structural Biology

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“…Myristate inserts hydrophobically into the lipid bilayer whereas basic amino acids form electrostatic interactions with the headgroups of acidic membrane phospholipids including PI (4,5)P 2 . There is evidence that in resting cells PI (4,5)P 2 is sequestered in cholesterol-rich domains by interaction with the hydrophobic/ basic motif of myristoylated proteins such as MARCKS, NAP-22, CAP-23, GAP-43 (Laux et al, 2000;Epand et al, 2005;McLaughlin & Murray, 2005). The modulation of availability of free PI (4,5)P 2 by these proteins regulates a number of cell signaling cascades in cells.…”

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confidence: 99%

Peptides modified by myristoylation activate eNOS in endothelial cells through Akt phosphorylation

Krotova

Hao

Xia

et al. 2006

British J Pharmacology

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1 Myristoylated pseudosubstrate of PKCz (mPS) -a synthetic myristoylated peptide with a sequence (13 amino acids) mimicking the endogenous PKCz pseudosubstrate region -is considered a selective cell-permeable inhibitor of PKCz. We present strong evidence that in endothelial cells the action of mPS is not limited to inhibition of PKC activity and that myristoylation of certain peptides can activate eNOS (endothelial nitric oxide synthase) through Akt phosphorylation. 2 mPS at micromolar concentrations (1-10 mM) induced profound phosphorylation of eNOS, Akt, ERK 1/2, and p38 MAPK in cultured pulmonary artery endothelial cells (PAEC). The same changes were observed after treatment of PAEC with a myristoylated scrambled version of mPS (mScr), whereas a cell-permeable version of PKCz pseudosubstrate fused to the HIV-TAT membranetranslocating peptide did not induce analogous changes, suggesting that myristoylation confers new properties on the peptides consisting of activation of different signaling pathways in endothelial cells. 3 In addition to mPS and mScr, a number of other myristoylated peptides induced phosphorylation of eNOS suggesting that myristoylation of peptides can activate eNOS by mechanisms unrelated to inhibition of PKC. All active myristoylated peptides contained basic amino acids motif and were longer than six amino acids. 4 Activation of eNOS by myristoylated peptides was dependent on the PI3K/Akt pathway and the rise of intracellular calcium and was associated with an elevation of cGMP levels in PAEC and with relaxation of precontracted isolated pulmonary artery segments. 5 Myristoylated peptides can be considered a new class of activators of NO production in endothelial cells and that using mPS as a specific inhibitor of PKCz should be done with caution, especially in endothelial cells.

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Lipid Domains, Chemistry of

Epand

2008

Wiley Encyclopedia of Chemical Biology

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Biological membranes are composed largely of proteins and lipids. A wide range of molecular structures exists among these molecules. It is therefore not surprising that biological membranes are not uniform but rather cluster certain molecules in specific regions or domains. This behavior can be mimicked in model systems comprising a limited number of components to study in more detail the molecular nature of this domain formation. Two types of domains exist that have been more extensively studied. One is a membrane domain enriched in polyanionic lipids, such as phosphatidylinositol diphosphate. Such domains are formed by the presence of proteins with segments containing several cationic amino acid residues. Such proteins have been termed “pipmodulins.” Another kind of domain is formed as a consequence of the nonuniform distribution of cholesterol in the membrane. Caveolae represent one type of cholesterol‐rich domain that is well characterized. Other cholesterol‐rich domains are termed “rafts.” Characterization of rafts in model membranes is well documented, but the nature of cholesterol‐rich domains in biological membranes remains a subject of controversy. Several imaging and fluorescence methods are being employed to further characterize the size and lifetime of small raft domains in biological membranes.

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Induction of raft‐like domains by a myristoylated NAP‐22 peptide and its Tyr mutant

Cited by 23 publications

References 48 publications

Tracking peptide–membrane interactions: Insights from in situ coupled confocal-atomic force microscopy imaging of NAP-22 peptide insertion and assembly

Tracking peptide–membrane interactions: Insights from in situ coupled confocal-atomic force microscopy imaging of NAP-22 peptide insertion and assembly

Peptides modified by myristoylation activate eNOS in endothelial cells through Akt phosphorylation

Lipid Domains, Chemistry of

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