A Novel Protein Glycan–Derived Inflammation Biomarker Independently Predicts Cardiovascular Disease and Modifies the Association of HDL Subclasses with Mortality-Reference-Cited by-同舟云学术

A Novel Protein Glycan–Derived Inflammation Biomarker Independently Predicts Cardiovascular Disease and Modifies the Association of HDL Subclasses with Mortality

Published:2017-01-01 Issue:1 Volume:63 Page:288-296
ISSN:0009-9147
Container-title:Clinical Chemistry
language:en
Short-container-title:

Author:

McGarrah Robert W¹²,Kelly Jacob P¹²³,Craig Damian M²,Haynes Carol²,Jessee Ryan C⁴,Huffman Kim M²⁴,Kraus William E¹²,Shah Svati H¹²³

Affiliation:

1. Division of Cardiology, Department of Medicine, Duke University School of Medicine, Durham, NC

2. Duke Molecular Physiology Institute, Duke University School of Medicine, Durham, NC

3. Duke Clinical Research Institute, Duke University, Durham, NC

4. Division of Rheumatology, Department of Medicine, Duke University School of Medicine, Durham, NC

Abstract

Abstract BACKGROUND Evidence suggests that systemic inflammation may adversely impact HDL function. In this study we sought to evaluate the independent and incremental predictive performance of GlycA—a novel serum inflammatory biomarker that is an aggregate measure of enzymatically glycosylated acute phase proteins—and HDL subclasses on adverse events in a retrospective observational study of a secondary prevention population and to understand a priori defined potential interactions between GlycA and HDL subclasses. METHODS GlycA and HDL subclasses were measured using proton nuclear magnetic resonance spectroscopy in 7617 individuals in the CATHGEN (CATHeterization GENetics) cardiac catheterization biorepository. RESULTS GlycA was associated with presence [odds ratio (OR) 1.07 (1.02–1.13), P = 0.01] and extent [OR 1.08 (1.03, 1.12) P < 0.0005] of coronary artery disease and with all-cause mortality [hazard ratio (HR) 1.34 (1.29–1.39), P < 0.0001], cardiovascular mortality [1.37 (1.30–1.45), P < 0.0001] and noncardiovascular mortality [1.46 (1.39–1.54) P < 0.0001] in models adjusted for 10 cardiovascular risk factors. GlycA and smaller HDL subclasses had independent but opposite effects on mortality risk prediction, with smaller HDL subclasses being protective [HR 0.69 (0.66–0.72), P < 0.0001]. There was an interaction between GlycA and smaller HDL subclasses—increasing GlycA concentrations attenuated the inverse association of smaller HDL subclasses with mortality. Adding GlycA and smaller HDL subclasses into the GRACE (Global Registry of Acute Coronary Events) and Framingham Heart Study Risk Scores improved mortality risk prediction, discrimination and reclassification. CONCLUSIONS These findings highlight the interaction of systemic inflammation and HDL with clinical outcomes and may increase precision for clinical risk assessment in secondary prevention populations.

Funder

National Institutes of Health

Institutional support from Liposcience, Incorporated

Sponsored research agreement between BMS and Duke

Publisher

Oxford University Press (OUP)

Subject

Biochemistry (medical),Clinical Biochemistry

Link

http://academic.oup.com/clinchem/article-pdf/63/1/288/32647539/clinchem0288.pdf

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