Cholesterol Efflux Capacity, High-Density Lipoprotein Function, and Atherosclerosis

Khera, Amit; Cuchel, Marina; Llera-Moya, Margarita de la; Rodrigues, Amrith; Burke, Megan F.; Jafri, Kashif; French, Benjamin; Phillips, Julie A.; Mucksavage, Megan; Wilensky, Robert L.; Mohler, Emile R.; Rothblat, George H.; Rader, Daniel J.

doi:10.1056/nejmoa1001689

Cited by 1,667 publications

(1,293 citation statements)

References 38 publications

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“…Using unsupervised hierarchical clustering, we noted that the BHK‐stimulated assay clustered with the J774‐basal model in controls, but with the J774‐stimulated and J774‐ABCA1–dependent measures in cases (Figure 1). Finally, we confirmed that CECs were associated with reduced prevalent CAD events, thus replicating previous observations3 and validating our data set (Table 1). …”

Section: Resultssupporting

confidence: 91%

“…Background cholesterol efflux (obtained in the absence of apolipoprotein B–depleted plasma) was subtracted from individual cholesterol efflux values. To correct for interassay variability, CEC was measured with the same pool of 40 healthy volunteers’ serum in each assay, and individual percentage CEC values were divided (normalized) by percentage CEC of control serum in each assay, as described previously 3, 5. Control serum CEC values were required to be within the limits defined by the historical mean of CEC for each model, plus or minus 2 SDs, to allow batch qualification.…”

Section: Methodsmentioning

confidence: 99%

“…Cholesterol efflux from macrophages occurs mainly toward HDL particles through multiple pathways, including passive diffusion, as well as facilitated ABCG1‐ and SR‐BI–dependent transport and active ABCA1‐dependent transport 2. CEC of HDL represents the fraction of radiolabeled cholesterol exiting macrophages typically after 4 hours of incubation, and higher CEC values have been shown to be associated with reductions of both prevalent and incident cardiovascular disease,3, 4, 5 although conflicting reports have been published 6…”

Section: Introductionmentioning

confidence: 99%

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Variants at the APOE/C1/C2/C4 Locus Modulate Cholesterol Efflux Capacity Independently of High‐Density Lipoprotein Cholesterol

Low‐Kam

Rhainds

et al. 2018

JAHA

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BackgroundMacrophage cholesterol efflux to high‐density lipoproteins (HDLs) is the first step of reverse cholesterol transport. The cholesterol efflux capacity (CEC) of HDL particles is a protective risk factor for coronary artery disease independent of HDL cholesterol levels. Using a genome‐wide association study approach, we aimed to identify pathways that regulate CEC in humans.Methods and ResultsWe measured CEC in 5293 French Canadians. We tested the genetic association between 4 CEC measures and genotypes at >9 million common autosomal DNA sequence variants. These analyses yielded 10 genome‐wide significant signals (P<6.25×10−9) representing 7 loci. Five of these loci harbor genes with important roles in lipid biology (CETP,LIPC,LPL,APOA1/C3/A4/A5, and APOE /C1/C2/C4). Except for the APOE/C1/C2/C4 variant (rs141622900, P nonadjusted=1.0×10−11; P adjusted=8.8×10−9), the association signals disappear when correcting for HDL cholesterol and triglyceride levels. The additional 2 significant signals were near the PPP1CB/PLB1 and RBFOX3/ENPP7 genes. In secondary analyses, we considered candidate functional variants for 58 genes implicated in HDL biology, as well as 239 variants associated with blood lipid levels and/or coronary artery disease risk by genome‐wide association study. These analyses identified 27 significant CEC associations, implicating 5 additional loci (GCKR,LIPG,PLTP,PPARA, and TRIB1).ConclusionsOur genome‐wide association study identified common genetic variation at the APOE/C1/C2/C4 locus as a major determinant of CEC that acts largely independently of HDL cholesterol. We predict that HDL‐based therapies aiming at increasing CEC will be modulated by changes in the expression of apolipoproteins in this gene cluster.

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Section: Resultssupporting

confidence: 91%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Variants at the APOE/C1/C2/C4 Locus Modulate Cholesterol Efflux Capacity Independently of High‐Density Lipoprotein Cholesterol

Low‐Kam

Rhainds

et al. 2018

JAHA

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“…As HDL cholesterol concentrations were found predictive for HF exacerbations independent of HF aetiology,5 increasing research has focused on HDL. It has become apparent that quality and function of HDL may relate more to outcome in CV diseases than serum levels 6. Particularly, the anti‐oxidant capacity of HDL was found associated with HF and clinical outcome,7 emphasizing the pivotal role of oxidative stress in the pathogenesis of HF.…”

Section: Introductionmentioning

confidence: 99%

Polyunsaturated fatty acids supplementation impairs anti‐oxidant high‐density lipoprotein function in heart failure

Wurm

Schrutka

Hammer

et al. 2018

Eur J Clin Investigation

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BackgroundThe underlying reasons for the highly inconsistent clinical outcome data for omega‐3‐polyunsaturated fatty acids (n3‐PUFAs) supplementation in patients with cardiac disease have not been understood yet. The aim of this prospective, randomized, double‐blind, placebo controlled study was to determine the effects of oral treatment with n3‐PUFAs on the anti‐oxidant capacity of HDL in heart failure (HF) patients.MethodsA total of 40 patients with advanced HF of nonischaemic origin, defined by NT‐proBNP levels of >2000 pg/mL, NYHA class III or IV and a LVEF <35% who were on stable optimized medical therapy for ≥3 months, were consecutively enrolled into this prospective, double‐blind, placebo‐controlled trial and randomized in a 1:1:1 fashion to receive 1 g/day or 4 g/day of n3‐PUFA, or placebo, respectively, for 12 weeks.ResultsAfter 12 weeks of treatment, the anti‐oxidant function of HDL, measured by the HDL inflammatory index, was found significantly impaired in the treatment group in a dose‐dependent fashion with 0.67 [IQR 0.49‐1.04] for placebo vs 0.71 [IQR 0.55‐1.01] for 1 g/day n3‐PUFA vs 0.98 [IQR 0.73‐1.16] for 4 g/day n3‐PUFA (P for trend = 0.018).ConclusionWe provide evidence for an adverse effect of n3‐PUFA supplementation on anti‐oxidant function of HDL in nonischaemic heart failure patients, establishing a potential mechanistic link for the controversial outcome data on n3‐PUFA supplementation.

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“…Increasing our knowledge of this fundamental property of apoA-I has clinical significance because apoA-I plasma levels uniquely predict risk of cardiovascular disease (22)(23)(24). One pathway through which apoA-I exerts its beneficial lipid trafficking function involves the plasma membrane transporter ATP-* This work was supported by a new investigator award from the TobaccoRelated Disease Research Program of California (Grant 18KT-0021) and an International Atherosclerosis Society Visiting Fellowship Award.…”

mentioning

confidence: 99%

Impact of Self-association on Function of Apolipoprotein A-I

Jayaraman

Abe-Dohmae

Yokoyama

et al. 2011

Journal of Biological Chemistry

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Background: Self-association is an intrinsic property of exchangeable apolipoproteins but an under-explored feature of the major protein of good cholesterol, apolipoprotein A-I. Result: Different degrees of apolipoprotein A-I self-association exhibit distinct in vitro lipid remodeling and cellular lipid release efficiencies. Conclusion: Self-association of apolipoprotein A-I modulates the biogenesis of high density lipoprotein. Significance: This is the first study to demonstrate that self-association of apolipoprotein A-I attunes key steps in reverse cholesterol transport.

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Cholesterol Efflux Capacity, High-Density Lipoprotein Function, and Atherosclerosis

Cited by 1,667 publications

References 38 publications

Variants at the APOE/C1/C2/C4 Locus Modulate Cholesterol Efflux Capacity Independently of High‐Density Lipoprotein Cholesterol

Variants at the APOE/C1/C2/C4 Locus Modulate Cholesterol Efflux Capacity Independently of High‐Density Lipoprotein Cholesterol

Polyunsaturated fatty acids supplementation impairs anti‐oxidant high‐density lipoprotein function in heart failure

Impact of Self-association on Function of Apolipoprotein A-I

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