Literature DB >> 16156664

Structural analysis of lipoprotein E particles.

Lumelle A Schneeweis1, Vishwanath Koppaka, Sissel Lund-Katz, Michael C Phillips, Paul H Axelsen.   

Abstract

Apolipoprotein E (apoE) is a key regulator of cholesterol homeostasis. Human apoE has three common isoforms, each with different risk implications for cardiovascular and neurodegenerative disease. Neither the structure of lipoprotein E particles nor the structural consequences of the isoform differences are known. In this investigation, synthetic lipoprotein particles were prepared by complexing phospholipids with full-length apoE isoforms, or with truncated N-terminal and C-terminal domains of apoE. These particles were examined with calorimetry, electron microscopy, circular dichroism spectroscopy, and internal reflection infrared spectroscopy. Results indicate that particles made with the three full-length apoE isoforms are discoidal in shape, and structurally indistinguishable. Thus, differences in their pathological consequences are not due to gross differences in particle structure. Although apoE is predominantly helical, and the axes of the helices are parallel to the flat surfaces of the particles, the orientational order of lipid acyl chains is low and inconsistent with the belt model of lipoprotein A-I structure. Instead, the data suggest that there are at least two different types of apoE-lipid interactions within lipoprotein E particles. One type occurs between apoE helices and the edge of the lipid bilayer as in the belt model, while a second type involves apoE helices that situate in the plane of the membrane and disturb acyl chain order. These interactions allow LpE particles to form with different protein/lipid ratios, and they account for the structure of LpE particles made with only the truncated domains.

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Year:  2005        PMID: 16156664     DOI: 10.1021/bi050872j

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


  12 in total

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4.  Dissociation of apolipoprotein E oligomers to monomer is required for high-affinity binding to phospholipid vesicles.

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Review 5.  Electron Tomography: A Three-Dimensional Analytic Tool for Hard and Soft Materials Research.

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Review 6.  Optimized negative-staining electron microscopy for lipoprotein studies.

Authors:  Lei Zhang; Huimin Tong; Mark Garewal; Gang Ren
Journal:  Biochim Biophys Acta       Date:  2012-09-29

7.  Role of the N- and C-terminal domains in binding of apolipoprotein E isoforms to heparan sulfate and dermatan sulfate: a surface plasmon resonance study.

Authors:  Yuko Yamauchi; Noriko Deguchi; Chika Takagi; Masafumi Tanaka; Padmaja Dhanasekaran; Minoru Nakano; Tetsurou Handa; Michael C Phillips; Sissel Lund-Katz; Hiroyuki Saito
Journal:  Biochemistry       Date:  2008-06-24       Impact factor: 3.162

8.  Morphology and structure of lipoproteins revealed by an optimized negative-staining protocol of electron microscopy.

Authors:  Lei Zhang; James Song; Giorgio Cavigiolio; Brian Y Ishida; Shengli Zhang; John P Kane; Karl H Weisgraber; Michael N Oda; Kerry-Anne Rye; Henry J Pownall; Gang Ren
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9.  Characterization and purification of polydisperse reconstituted lipoproteins and nanolipoprotein particles.

Authors:  Craig D Blanchette; Brent W Segelke; Nicholas Fischer; Michele H Corzett; Edward A Kuhn; Jenny A Cappuccio; William Henry Benner; Matthew A Coleman; Brett A Chromy; Graham Bench; Paul D Hoeprich; Todd A Sulchek
Journal:  Int J Mol Sci       Date:  2009-07-02       Impact factor: 6.208

10.  An optimized negative-staining protocol of electron microscopy for apoE4 POPC lipoprotein.

Authors:  Lei Zhang; James Song; Yvonne Newhouse; Shengli Zhang; Karl H Weisgraber; Gang Ren
Journal:  J Lipid Res       Date:  2009-11-16       Impact factor: 5.922

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