Literature DB >> 29773713

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

Allison L Cooke1, Jamie Morris1, John T Melchior1, Scott E Street1, W Gray Jerome2, Rong Huang1, Andrew B Herr3, Loren E Smith4, Jere P Segrest5, Alan T Remaley6, Amy S Shah7, Thomas B Thompson8, W Sean Davidson9.   

Abstract

APOA1 is the most abundant protein in HDL. It modulates interactions that affect HDL's cardioprotective functions, in part via its activation of the enzyme, LCAT. On nascent discoidal HDL, APOA1 comprises 10 α-helical repeats arranged in an anti-parallel stacked-ring structure that encapsulates a lipid bilayer. Previous chemical cross-linking studies suggested that these APOA1 rings can adopt at least two different orientations, or registries, with respect to each other; however, the functional impact of these structural changes is unknown. Here, we placed cysteine residues at locations predicted to form disulfide bonds in each orientation and then measured APOA1's ability to adopt the two registries during HDL particle formation. We found that most APOA1 oriented with the fifth helix of one molecule across from fifth helix of the other (5/5 helical registry), but a fraction adopted a 5/2 registry. Engineered HDLs that were locked in 5/5 or 5/2 registries by disulfide bonds equally promoted cholesterol efflux from macrophages, indicating functional particles. However, unlike the 5/5 registry or the WT, the 5/2 registry impaired LCAT cholesteryl esterification activity (P < 0.001), despite LCAT binding equally to all particles. Chemical cross-linking studies suggest that full LCAT activity requires a hybrid epitope composed of helices 5-7 on one APOA1 molecule and helices 3-4 on the other. Thus, APOA1 may use a reciprocating thumbwheel-like mechanism to activate HDL-remodeling proteins.

Entities:  

Keywords:  apolipoprotein A1; apolipoproteins; cholesterol metabolism; cholesterol/efflux; electron microscopy; high density lipoprotein; high density lipoprotein metabolism; lecithin:cholesterol acyltransferase; proteomics; surface plasmon resonance

Mesh:

Substances:

Year:  2018        PMID: 29773713      PMCID: PMC6027914          DOI: 10.1194/jlr.M085332

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


  63 in total

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3.  Glycation of HDL blunts its anti-inflammatory and cholesterol efflux capacities in vitro, but has no effect in poorly controlled type 1 diabetes subjects.

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5.  Large-scale analysis reveals a novel risk score to predict overall survival in hepatocellular carcinoma.

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Review 6.  Impact of cholesterol-pathways on breast cancer development, a metabolic landscape.

Authors:  Alina González-Ortiz; Octavio Galindo-Hernández; Gerson N Hernández-Acevedo; Gustavo Hurtado-Ureta; Victor García-González
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7.  Integrated analysis of methylation-driven genes and pretreatment prognostic factors in patients with hepatocellular carcinoma.

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Journal:  BMC Cancer       Date:  2021-05-25       Impact factor: 4.430

8.  Modified sites and functional consequences of 4-oxo-2-nonenal adducts in HDL that are elevated in familial hypercholesterolemia.

Authors:  Linda S May-Zhang; Valery Yermalitsky; John T Melchior; Jamie Morris; Keri A Tallman; Mark S Borja; Tiffany Pleasent; Venkataraman Amarnath; Wenliang Song; Patricia G Yancey; W Sean Davidson; MacRae F Linton; Sean S Davies
Journal:  J Biol Chem       Date:  2019-10-30       Impact factor: 5.486

9.  A robust twelve-gene signature for prognosis prediction of hepatocellular carcinoma.

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Journal:  Cancer Cell Int       Date:  2020-06-03       Impact factor: 5.722

10.  Sterically stabilized recombined HDL composed of modified apolipoprotein A-I for efficient targeting toward glioma cells.

Authors:  Jin Li; Mengmeng Han; Jianfei Li; Zhiming Ge; Qianqian Wang; Kai Zhou; Xiaoxing Yin
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