An Exploratory Analysis of Criteria for the Metabolic Syndrome and Its Prediction of Long-term Cardiovascular Outcomes: The Hoorn Study

doi:10.1093/aje/kwi229

American Journal of Epidemiology Advance Access originally published online on August 2, 2005
American Journal of Epidemiology 2005 162(5):438-447; doi:10.1093/aje/kwi229

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American Journal of Epidemiology Copyright © 2005 by the Johns Hopkins Bloomberg School of Public Health All rights reserved

ORIGINAL CONTRIBUTIONS

An Exploratory Analysis of Criteria for the Metabolic Syndrome and Its Prediction of Long-term Cardiovascular Outcomes

The Hoorn Study

Cynthia J. Girman¹, Jacqueline M. Dekker², Thomas Rhodes¹, Giel Nijpels², Coen D. A. Stehouwer², Lex M. Bouter² and Robert J. Heine²

¹ Department of Epidemiology, Merck Research Laboratories, West Point, PA
² Institute for Research in Extramural Medicine, VU University Medical Center, Amsterdam, the Netherlands

Correspondence to Dr. Cynthia J. Girman, Department of Epidemiology, Merck Research Laboratories, P.O. Box 4, BL1-7, West Point, PA 19486 (e-mail: Cindy_Girman{at}merck.com).

Studies have shown an increased risk of cardiovascular outcomeswith the metabolic syndrome, but information on predictive propertiesof the National Cholesterol Education Program Adult TreatmentPanel 3 (NCEP) criteria is sparse. The authors used data fromthe Hoorn population-based study in the Netherlands including2,484 participants aged 50–75 years examined in 1989 andfollowed for cardiovascular morbidity and mortality through2000 to assess NCEP criteria, excluding known diabetes or cardiovasculardisease. Cluster analyses explored whether NCEP identifies amixture of heterogeneous groups. For each gender, participantsmeeting NCEP criteria seemed to be divided into clusters distinguishedprimarily by triglycerides or high density lipoprotein cholesterol.Cutpoints for components predicting cardiovascular events usingclassification and survival tree methodology varied by endpointand gender, but Cox model hazards ratios were relatively comparableregardless of cutpoints (range: 1.3–2.5). Clear gradationin risk of cardiovascular outcomes was evident with increasingnumber of components, with statistically elevated risk for $≥$ 3(NCEP) components in men but for $≥$ 2 components in women. Exploratoryanalyses of alternative metabolic syndrome criteria suggestcardiovascular risk estimates comparable to those derived byusing NCEP, but criteria evaluating risk on more of a continuumwould potentially allow consideration of alternative definitionsby gender or for patients with other risk factors.

cardiovascular diseases; metabolic syndrome X; morbidity; mortality

Abbreviations: CART, classification and regression tree; HDL, high density lipoprotein; NCEP, National Cholesterol Education Program Adult Treatment Panel 3; WHO, World Health Organization

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