Literature DB >> 21159667

Sequence conservation of apolipoprotein A-I affords novel insights into HDL structure-function.

Denys Bashtovyy1, Martin K Jones, G M Anantharamaiah, Jere P Segrest.   

Abstract

We performed alignment of apolipoprotein A-I (apoA-I) sequences from 31 species of animals. We found there is specific conservation of salt bridge-forming residues in the first 30 residues of apoA-I and general conservation of a variety of residue types in the central domain, helix 2/3 to helix 7/8. In the lipid-associating domain, helix 7 and helix 10 are the most and least conserved helixes, respectively. Furthermore, eight residues are completely conserved: P66, R83, P121, E191, and P220, and three of seven Tyr residues in human apoA-I, Y18, Y115, and Y192, are conserved. Residue Y18 appears to be important for assembly of HDL. E191-Y192 represents the only completely conserved pair of adjacent residues in apoA-I; Y192 is a preferred target for site-specific oxidative modification within atheroma, and molecular dynamic simulations suggest that the conserved pair E191-Y192 is in a solvent-exposed loop-helix-loop. Molecular dynamics testing of human apoA-I showed that M112 and M148 interact with Y115, a microenvironment unique to human apoA-I. Finally, conservation of Arg residues in the α11/3 helical wheel position 7 supports several possibilities: interactions with adjacent phospholipid molecules and/or oxidized lipids and/or binding of antioxidant enzymes through cation-π orbital interactions. We conclude that sequence alignment of apoA-I provides unique insights into apoA-I structure-function relationship.

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Year:  2010        PMID: 21159667      PMCID: PMC3035680          DOI: 10.1194/jlr.R012658

Source DB:  PubMed          Journal:  J Lipid Res        ISSN: 0022-2275            Impact factor:   5.922


  84 in total

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Authors:  Baohai Shao; Jay W Heinecke
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5.  Structure of spheroidal HDL particles revealed by combined atomistic and coarse-grained simulations.

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4.  "Sticky" and "promiscuous", the yin and yang of apolipoprotein A-I termini in discoidal high-density lipoproteins: a combined computational-experimental approach.

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6.  Solution structure of discoidal high-density lipoprotein particles with a shortened apolipoprotein A-I.

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7.  A thumbwheel mechanism for APOA1 activation of LCAT activity in HDL.

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8.  Sidedness of interfacial arginine residues and anti-atherogenicity of apolipoprotein A-I mimetic peptides.

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9.  Molecular dynamics simulations of lipid nanodiscs.

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10.  Proteolysis of apolipoprotein A-I by secretory phospholipase A₂: a new link between inflammation and atherosclerosis.

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