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Literature DB >> 18831538

Conformational flexibility of the N-terminal domain of apolipoprotein a-I bound to spherical lipid particles.

Momoe Kono¹, Yusuke Okumura, Masafumi Tanaka, David Nguyen, Padmaja Dhanasekaran, Sissel Lund-Katz, Michael C Phillips, Hiroyuki Saito.

Abstract

Lipid binding of human apolipoprotein A-I (apoA-I) occurs initially through the C-terminal alpha-helices followed by conformational reorganization of the N-terminal helix bundle. This led us to hypothesize that apoA-I has multiple lipid-bound conformations, in which the N-terminal helix bundle adopts either open or closed conformations anchored by the C-terminal domain. To investigate such possible conformations of apoA-I at the surface of a spherical lipid particle, site-specific labeling of the N- and C-terminal helices in apoA-I by N-(1-pyrene)maleimide was employed after substitution of a Cys residue for Val-53 or Phe-229. Neither mutagenesis nor the pyrene labeling caused discernible changes in the lipid-free structure and lipid interaction of apoA-I. Taking advantage of a significant increase in fluorescence when a pyrene-labeled helix is in contact with the lipid surface, we monitored the behaviors of the N- and C-terminal helices upon binding of apoA-I to egg PC small unilamellar vesicles. Comparison of the binding isotherms for pyrene-labeled apoA-I as well as a C-terminal helical peptide suggests that an increase in surface concentration of apoA-I causes dissociation of the N-terminal helix from the surface leaving the C-terminal helix attached. Consistent with this, isothermal titration calorimetry measurements showed that the enthalpy of apoA-I binding to the lipid surface under near saturated conditions is much less exothermic than that for binding at a low surface concentration, indicating the N-terminal helix bundle is out of contact with lipid at high apoA-I surface concentrations. Interestingly, the presence of cholesterol significantly induces the open conformation of the helix bundle. These results provide insight into the multiple lipid-bound conformations that the N-terminal helix bundle of apoA-I can adopt on a lipid or lipoprotein particle, depending upon the availability of space on the surface and the surface composition.

Entities: Chemical Disease Gene Mutation Species

Mesh：

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Year: 2008 PMID： 18831538 PMCID： PMC2667695 DOI： 10.1021/bi801503r

Source DB: PubMed Journal: Biochemistry ISSN： 0006-2960 Impact factor: 3.162

62 in total

1. Two homologous apolipoprotein AI mimetic peptides. Relationship between membrane interactions and biological activity.

Authors: Richard M Epand; Raquel F Epand; Brian G Sayer; Geeta Datta; Manjula Chaddha; G M Anantharamaiah
Journal: J Biol Chem Date: 2004-09-08 Impact factor: 5.157

2. Apolipoprotein-mediated plasma membrane microsolubilization. Role of lipid affinity and membrane penetration in the efflux of cellular cholesterol and phospholipid.

Authors: K L Gillotte; M Zaiou; S Lund-Katz; G M Anantharamaiah; P Holvoet; A Dhoest; M N Palgunachari; J P Segrest; K H Weisgraber; G H Rothblat; M C Phillips
Journal: J Biol Chem Date: 1999-01-22 Impact factor: 5.157

3. Calorimetry of apolipoprotein-A1 binding to phosphatidylcholine-triolein-cholesterol emulsions.

Authors: A Derksen; D Gantz; D M Small
Journal: Biophys J Date: 1996-01 Impact factor: 4.033

Review 4. Structural models of human apolipoprotein A-I.

Authors: C G Brouillette; G M Anantharamaiah
Journal: Biochim Biophys Acta Date: 1995-05-17

5. Effect of cholesterol on apolipoprotein A-I binding to lipid bilayers and emulsions.

Authors: H Saito; Y Miyako; T Handa; K Miyajima
Journal: J Lipid Res Date: 1997-02 Impact factor: 5.922

6. An apolipoprotein AI mimetic peptide: membrane interactions and the role of cholesterol.

Authors: Richard M Epand; Raquel F Epand; Brian G Sayer; Giuseppe Melacini; Mayakonda N Palgulachari; Jere P Segrest; G M Anantharamaiah
Journal: Biochemistry Date: 2004-05-04 Impact factor: 3.162

7. Potential involvement of dissociated apoA-I in the ABCA1-dependent cellular lipid release by HDL.

Authors: Kei-ichiro Okuhira; Maki Tsujita; Yoshio Yamauchi; Sumiko Abe-Dohmae; Koichi Kato; Tetsurou Handa; Shinji Yokoyama
Journal: J Lipid Res Date: 2004-01-16 Impact factor: 5.922

8. Only the two end helixes of eight tandem amphipathic helical domains of human apo A-I have significant lipid affinity. Implications for HDL assembly.

Authors: M N Palgunachari; V K Mishra; S Lund-Katz; M C Phillips; S O Adeyeye; S Alluri; G M Anantharamaiah; J P Segrest
Journal: Arterioscler Thromb Vasc Biol Date: 1996-02 Impact factor: 8.311

9. Hydrophobic amino acids in the hinge region of the 5A apolipoprotein mimetic peptide are essential for promoting cholesterol efflux by the ABCA1 transporter.

Authors: Denis O Sviridov; Alexander M Andrianov; Ivan V Anishchenko; John A Stonik; Marcelo J A Amar; Scott Turner; Alan T Remaley
Journal: J Pharmacol Exp Ther Date: 2012-10-05 Impact factor: 4.030

10. Crystal structure of Δ(185-243)ApoA-I suggests a mechanistic framework for the protein adaptation to the changing lipid load in good cholesterol: from flatland to sphereland via double belt, belt buckle, double hairpin and trefoil/tetrafoil.

Authors: Olga Gursky
Journal: J Mol Biol Date: 2012-10-04 Impact factor: 5.469

Conformational flexibility of the N-terminal domain of apolipoprotein a-I bound to spherical lipid particles.

1. Two homologous apolipoprotein AI mimetic peptides. Relationship between membrane interactions and biological activity.

2. Apolipoprotein-mediated plasma membrane microsolubilization. Role of lipid affinity and membrane penetration in the efflux of cellular cholesterol and phospholipid.

3. Calorimetry of apolipoprotein-A1 binding to phosphatidylcholine-triolein-cholesterol emulsions.

Review 4. Structural models of human apolipoprotein A-I.

5. Effect of cholesterol on apolipoprotein A-I binding to lipid bilayers and emulsions.

6. An apolipoprotein AI mimetic peptide: membrane interactions and the role of cholesterol.

7. Potential involvement of dissociated apoA-I in the ABCA1-dependent cellular lipid release by HDL.

8. Only the two end helixes of eight tandem amphipathic helical domains of human apo A-I have significant lipid affinity. Implications for HDL assembly.

9. Binding steps of apolipoprotein A-I with phospholipid monolayers: adsorption and penetration.

10. Alpha-helix formation is required for high affinity binding of human apolipoprotein A-I to lipids.

1. Fluorescence analysis of the lipid binding-induced conformational change of apolipoprotein E4.

2. Kinetics of lipid mixing between bicelles and nanolipoprotein particles.

3. Maturation of apolipoprotein A-I: unrecognized health benefit or a forgotten rudiment?

4. Effects of cholesterol on thermal stability of discoidal high density lipoproteins.

5. Surface pressure-dependent conformation change of apolipoprotein-derived amphipathic α-helices.

6. Direct detection of ABCA1-dependent HDL formation based on lipidation-induced hydrophobicity change in apoA-I.

7. Interaction between the N- and C-terminal domains modulates the stability and lipid binding of apolipoprotein A-I.

Review 8. The helix bundle: a reversible lipid binding motif.

9. Hydrophobic amino acids in the hinge region of the 5A apolipoprotein mimetic peptide are essential for promoting cholesterol efflux by the ABCA1 transporter.

10. Crystal structure of Δ(185-243)ApoA-I suggests a mechanistic framework for the protein adaptation to the changing lipid load in good cholesterol: from flatland to sphereland via double belt, belt buckle, double hairpin and trefoil/tetrafoil.