Defining the Metabolic Syndrome Construct: Multi-Ethnic Study of Atherosclerosis (MESA) cross-sectional analysis

doi:10.2337/dc07-0147

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Cardiovascular and Metabolic Risk
Original Article

Defining the Metabolic Syndrome Construct

Multi-Ethnic Study of Atherosclerosis (MESA) cross-sectional analysis

Dhananjay Vaidya, MBBS, PHD, MPH¹, Moyses Szklo, MD, DRPH¹, Kiang Liu, PHD², Pamela J. Schreiner, PHD³, Alain G. Bertoni, MD, PHD⁴ and Pamela Ouyang, MD¹

¹ Johns Hopkins University, Baltimore, Maryland
² Northwestern University, Chicago, Illinois
³ University of Minnesota, Minneapolis, Minnesota
⁴ Wake Forest University, Winston-Salem, North Carolina

Address correspondence and reprint requests to Dhananjay Vaidya, PhD, Johns Hopkins Medical Institutions, 1830 E. Monument St., Suite 8028-A, Baltimore, MD 21287. E-mail: dvaidya1{at}jhmi.edu

ABSTRACT

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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS--
RESULTS--
CONCLUSIONS--
APPENDIX
References

OBJECTIVE—It is controversial whether the clustering ofcertain metabolic abnormalities should be separately designatedas the metabolic syndrome. We operationalized the "syndrome"concept and tested whether the metabolic syndrome was compatiblewith these operational constructs.

RESEARCH DESIGN AND METHODS—The baseline cross-sectionof the Multi-Ethnic Study of Atherosclerosis recruited a population-basedcohort of 6,781 individuals, aged 45–84 years, from sixcommunities in the U.S. Metabolic syndrome components (waistcircumference, blood pressure, fasting serum HDL cholesterol,triglycerides, and plasma glucose), homeostasis model assessment(HOMA) of insulin resistance (fasting glucose x insulin), andintimal-medial thickness (IMT) in the common and internal carotidarteries by B-mode ultrasound were measured.

RESULTS—Higher syndrome component count is associatedwith higher HOMA levels (trend P < 0.001). Given the prevalenceof individual components, the nonprevalence of any componentor the co-prevalence of four or five components is greater thanexpected ( ${chi}$ ² P < 0.001). After accounting for the additiveassociation of each component, the current definition of metabolicsyndrome (co-prevalence of three or more components) does nothave supra-additive association with thicker IMT in the commoncarotid (men: P = 0.075, women: P = 0.949) or internal carotidartery (men: P = 0.106, women: P = 0.121).

CONCLUSIONS—The metabolic syndrome did not have supra-additiveassociation with IMT, but its components clustered greater thanchance expectation and a higher component count was associatedwith greater insulin resistance. The metabolic syndrome wascompatible with two of three "syndrome" constructs tested.

Abbreviations: CIMT, common carotid artery intimal-medial thickness • HOMA, homeostasis model assessment • IIMT, internal carotid artery intimal-medial thickness • IMT, intimal-medial thickness • MESA, Multi-Ethnic Study of Atherosclerosis

INTRODUCTION

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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS--
RESULTS--
CONCLUSIONS--
APPENDIX
References

A recent joint statement by the American Diabetes Associationand European Association for the Study of Diabetes (1) questionedthe designation of the clustering of certain metabolic factorsas a "syndrome," igniting a debate (2,3). The commonly useddescription of "syndrome" as a "cluster of abnormalities" doesnot lend to straightforward operationalization. Factor analysishas been previously used to evaluate whether the metabolic syndromeabnormalities (obesity, dyslipidemia, hypertension, and impairedfasting glucose) load factors as a group (4,5). However, withoutbiological insight, factor loadings are opaque and depend onthe model parameterization (6).

We propose three different ways to operationalize the notionof "syndrome," with different signification, as follows:

Construct1: Each component of the metabolic syndrome is additivelydiagnosticof insulin resistance, the putative etiology (4,7,8).ProposedMetric: A graded association of individual componentsand componentcount with insulin resistance, e.g., as measuredby the homeostasismodel assessment (HOMA) (9). Practical significance:The componentcount may be used to diagnose underlying insulinresistance,which is not routinely assayed.
Construct 2: "Unusual" clusteringof components may manifestan unknown underlying etiology. Proposedmetric: Observed componentco-prevalence compared with thatexpected by their individualprevalences. Practical significance:Research effort is neededin identifying the underlying etiology.
Construct 3: Co-prevalence of components implies greater pathologythan the summation of the independent associations of each component.Proposed metric: Supra-additive association of component co-prevalencewith pathology. Practical significance: Aggressive treatmentof any risk factors would also reduce the supra-additive clusterrisk.

We used baseline data from the Multi-Ethnic Study of Atherosclerosis(MESA) to explore whether the National Cholesterol EducationProgram Adult Treatment Panel III definition of the metabolicsyndrome (10,11) is compatible with any of the above syndromeconstructs.

RESEARCH DESIGN AND METHODS—

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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS--
RESULTS--
CONCLUSIONS--
APPENDIX
References

The design of MESA has been previously described (12). The studywas approved by institutional review boards of all participatingcenters. At baseline (2000–2002), 6,814 white, African-American,Chinese, or Hispanic men and women who were free of clinicalcardiovascular disease were recruited. The majority (3,199 men,3,581 women) had complete data required for classification bythe modified National Cholesterol Education Program Adult TreatmentPanel III definition (10,11) for these analyses. Subjects completedstandardized medical history questionnaires. Fasting blood measurementsof glucose, insulin, and a lipid panel were performed. Umbilicus-levelwaist circumference was measured using a standard tape measurewith 4 oz tension. Resting seated blood pressure was measuredthree times using a Dinamap model Pro 100 automated oscillometricsphygmomanometer (Critikon, Tampa, FL). The average of the lasttwo measurements was used in analysis. The metabolic syndromeis the presence of three or more of the components (10,11):1) waist $≥$ 102 (men) or $≥$ 88 cm (women), 2) triglycerides $≥$ 150 mg/dl,3) HDL cholesterol $≤$ 40 (men) or $≤$ 50 mg/dl (women), 4) blood pressure $≥$ 130/85 mmHg or on antihypertensive treatment, and 5) fastingplasma glucose $≥$ 100 mg/dl or on anti-hyperglycemic treatment.

HOMA was calculated as fasting plasma insulin (µU/ml)x glucose (mmol/l)/22.5 (9). The maximum intimal-medial thickness(IMT) was measured at 12 bilateral locations for the internalcarotid arteries (IIMT) and four locations for the common carotidarteries (CIMT) using B-mode ultrasound and averaged.

Statistical analysis
Analyses were stratified by sex, because the criteria for themetabolic syndrome are sex specific.

Construct 1.
Association of each component with HOMA was tested using nonparametricrank-sum tests. Sensitivity analyses excluded individuals takingantidiabetic medications. The association of HOMA with the numberof co-prevalent components was tested using the Kusick nonparametrictrend test. Receiver-operating characteristic analysis for themetabolic components count used the upper quartile of HOMA todefine insulin resistance (13).

Construct 2.
The prevalence of each metabolic component was calculated bythe number of other co-prevalent components. Trends in prevalenceswere tested by the Kruskal and Goodman ${gamma}$ statistic. Expectedco-prevalences of 0, 1, ... 5 components were calculated basedon the marginal prevalences of each metabolic component (seethe online appendix at http://dx.doi.org/10.2337/dc07-0147)and compared against the observed distribution using ${chi}$ ² statistics.

For constructs 1 and 2, stratified analyses were done to confirmif the qualitative conclusions differed by race/ethnicity.

Construct 3.
CIMT and IIMT were analyzed on the log scale. Coefficients formultiple linear regression were adjusted for age and race/ethnicity.In model series 1, the population was restricted to those whohad no prevalent components, exactly one component, or threeor more components. (Those who had exactly two components neitherhave the defined metabolic syndrome nor reflect the individualcomponent contributions.) Regression models specified separatecoefficients for the five isolated components and a coefficientfor the metabolic syndrome cluster, compared with the referentgroup that has no prevalent component. The difference betweenthe linear combination of the five component coefficients andthe cluster coefficient was tested for statistical significance.In model series 2, individuals with all five metabolic syndromecomponents co-prevalent were included with those with exactlyone, or none, of the components prevalent. In confirmatory modelseries 3, all components (irrespective of being isolated) wereincluded, and the metabolic syndrome cluster variable was alsoincluded as a single interaction variable. However, this modelseries does not account for all possible two-component clusters,and hence the coefficients of the individual components cannotbe interpreted as unambiguously as in model series 1 and 2.Racial/ethnic heterogeneity of supra-additivity was tested usingomnibus F tests of the race-metabolic syndrome interaction variablesin models including a race/ethnicity-specific coefficient foreach isolated component and the metabolic syndrome cluster.

In separate models adjusted for age and racial/ethnic group,an interaction coefficient was estimated to test whether thepresence of each of 26 possible co-prevalent component combinationswas associated with IMT above and beyond the sum of the componentcoefficients.

RESULTS—

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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS--
RESULTS--
CONCLUSIONS--
APPENDIX
References

The proportions of MESA participants with the individual componentsof the metabolic syndrome were as follows: large waist circumference(38% men, 69% women), high triglycerides (32% men, 29% women),low HDL cholesterol (40% men, 49% women), high blood pressure(59% men, 59% women), and high fasting plasma glucose (49% men,36% women), with 40% of men and 46% of women having three ormore components.

Insulin resistance as an underlying "common denominator"
For each metabolic syndrome component, median HOMA was higherif the component was present (all differences P < 0.001,supplementary Table 1 in the online appendix). Table 1 showsthat an increasing number of co-prevalent components was associatedwith higher HOMA levels in men and women (all trends, P <0.001). This was true in race/ethnicity-stratified analysis(all groups, P < 0.001) (supplementary Table 2 in the onlineappendix).

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Table 1— Association of HOMA with the number of metabolic syndrome components in MESA (2000–2002)

For the number of co-prevalent components as the diagnosticfor insulin resistance, the area under the receiver-operatingcharacteristic curve was 0.80 (95% CI 0.78–0.81) for menand 0.80 (0.79–0.82) for women. The metabolic syndrome(three or more components) results in sensitivity and specificitylevels of 74 and 29% in men and 82 and 34% in women, respectively.A moderate to good diagnostic efficiency was present in menand women of all four race/ethnicities (area under the receiver-operatingcharacteristic curve range 0.74–0.86 for different groups)(detailed in supplementary Table 3 in the online appendix).

Clustering of metabolic syndrome components
In both men and women, there is a graded relationship betweenthe prevalence of any given component and the number of othercomponents (for all components, P < 0.001) (supplementaryFig. 1 in the online appendix).

The observed distribution of co-prevalence of components wassignificantly different from the co-prevalence expectation giventhe prevalence of each of the individual components (Fig. 1,P < 0.001 for men and women). Specifically, nonprevalenceof any component, and co-prevalence of four and five componentswere observed more frequently than expected (i.e., tails ofthe distribution were heavier), suggesting that clustering isnot a chance event. Similarly, significantly heavier-taileddistributions were observed for men and women in analyses stratifiedby race/ethnicity (all groups, P < 0.001). In all men, thelargest contributors to ${chi}$ ² were 1) no components; 2) all components;3) obesity, high triglycerides, low HDL cholesterol, and highblood pressure, without high glucose (all more frequent thanexpected); and 4) isolated high blood pressure and low HDL cholesterol.Isolated high blood pressure and high triglycerides were lessfrequently observed than expected. The highest deviating clustersin all women include those listed above in 1) through 4), asin men, with the cluster of isolated obesity and high triglyceridesless frequently observed than expected.

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Figure 1— Expected co-prevalence of metabolic syndrome components based on the prevalence of individual components, compared with the observed co-prevalences in MESA (2000–2002).

The additive association of metabolic syndrome components with subclinical atherosclerosis
Figure 2 shows that the association of CIMT or IIMT with theco-prevalence of three or more components (model series 1),or all five components (model series 2), is no greater thanthe added isolated component associations (i.e., no supra-additiveinteraction) either in men or women. Note that the small nonsignificant(P = 0.66) negative association of CIMT with isolated glycemiaamong women is conditioned on the absence of all other components.There are no significant racial/ethnic differences in the lackof supra-additive interaction of the metabolic syndrome clusterabove the five isolated components. The lack of supra-additiveassociation of the metabolic syndrome with IMT variables wasconfirmed in models estimating the marginal rather than isolatedcomponent effects (model series 3).

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Figure 2— Percentage greater common and internal carotid artery IMT in subjects with metabolic syndrome components (individual or co-prevalent) compared with age- and race-adjusted subjects with no metabolic syndrome components in MESA (2000–2002). Glu, high fasting plasma glucose; HBP, high blood pressure; HDL, low HDL cholesterol level; Ob, abdominal obesity; TG, high triglyceride level. The cut points for these components are detailed in the text. Left arrow within stacked bars represents a negative association. All associations of single components are conditional to the absence of all other components. Under this condition, note that the direction of the isolated Glu association with common carotid IMT is nonsignificantly negative in women, and the association of isolated TG with common carotid IMT is zero in men.

Using the Bonferroni criterion level ( ${alpha}$ = 0.05/26 = 0.0019),no positive additive interaction was found for any of the combinationsof two or more metabolic components in relation to either CIMTor IIMT.

CONCLUSIONS—

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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS--
RESULTS--
CONCLUSIONS--
APPENDIX
References

We showed that the metabolic syndrome qualified as a "syndrome"under some, but not all constructs hypothesized in the presentstudy.

Construct 1 postulated a common denominator for the componentsof the syndrome. We confirmed the graded association of HOMAwith the number of components. If direct measurement of insulinresistance is not feasible, the metabolic syndrome as definedmay be used as a clinical diagnosis of insulin resistance.

The assumption of the primacy of insulin resistance is controversial,since abdominal obesity has been suggested as an essential etiologicalbasis for the metabolic syndrome (14). Nevertheless, the metabolicsyndrome could be used as a marker of insulin resistance. Iftreatment of insulin resistance per se may not affect the syndromecomponents, the practical significance of this finding is notclear.

Construct 2 postulated that clustering was not by chance andthus was hypothesis generating. We presented a metric and directlytested for the hypothesis of clustering that allowed for additivecomponent count, because components of syndromes are used additivelyby clinicians (15,16). We showed that the components were correlated,such that component counts of four or five, and correspondingly,zero components, occurred more frequently than chance expectation.Data reduction techniques such as factor analysis generate newlinear combinations of components (reviewed by Lawlor et al.[6]) and do not test the syndrome construct hypothesis. Thoughfactor analysis may be useful for generating latent phenotypes(6,17), this was outside the scope of our analyses.

Practically, the detection of any one component should alertthe clinician to seek other abnormalities. Clustering generatesthe hypothesis of a common source for the abnormalities. Thissource may be biochemical, such as insulin resistance, but ouranalyses do not exclude the possibility that other sources areresponsible for the clustering, such as psychosocial causes.

For construct 3, "syndrome" implied that co-prevalence of componentswas associated with a supra-additive association with pathology,more than expected by summing individual component contributions.This understanding of the "syndrome" construct has been mentionedin a recent debate (1–3). This construct was also implicitin the demonstration by Golden et al. (18) that 18 of the 57six-component combinations were associated with supra-additivecarotid IMT. Surprisingly, this was not found in our analyses,which show no supra-additive association. However, our resultsmay not be directly comparable to those of Golden et al. (18),which used hyperinsulinemia ( $≥$ 110 pmol/l) and BMI $≥$ 25 kg/m² asmetabolic components, and more stringent criteria for hypertension( $≥$ 140 mmHg systolic), high triglycerides ( $≥$ 200 mg/dl), high glucose( $≥$ 110 mg/dl), and low HDL in women ( $≤$ 40 mg/dl) in a younger population(45–64 years). Carotid bulb IMT, needed to exactly replicatethe analyses of Golden et al. (18), was not measured in MESA.In analysis that used the metabolic criteria of Golden et al.(18) among individuals 45–64 years, our conclusion regardingconstruct 3 for common, internal, or mean IMT remained unchanged(results not shown). It is possible that there are differencesbetween the cohorts studied and that construct 3 may be validin some populations. Further, in our analysis, the associationof each component with IMT conditioned on the absence of allother components was somewhat weak, with a nonsignificant negativeassociation in one instance. The weak association of isolatedcomponents should result in an enhanced power to detect supra-additiveassociation of clustered components, yet no supra-additive associationwas seen in our analysis.

Interestingly, supra-additive association with a harmful outcomeis not expected in other clinically useful "syndromes." Forexample, the only prognosticator for acute rheumatic fever sequelaeis carditis (19) and not the other components of the Duckett-Jonescriteria (15); thus, there is no proven supra-additive riskfor component clustering. To examine supra-additive associationof clustering with upstream etiology, we can consider the exampleof the Down's syndrome using an eight-component syndrome definition(16). In a series of 19,000 live births, there was no incrementalassociation of trisomy 21 with the component counts beyond 5,suggesting a saturation of the association of cause at higherscores, which is statistically equivalent to a sub-additiveeffect of clustering.

However, should this construct come to be generally acceptedfor metabolic abnormalities, our results indicate that the metabolicsyndrome is not "syndromic" in terms of carotid IMT as pathology.The practical implication is that every metabolic componentshould be vigorously treated on its own, with no expectationof a putative supra-additive risk reduction for subclinicalcarotid atherosclerosis.

Our analysis has certain limitations. HOMA is not the gold standardfor the measurement of insulin resistance. However, the randomerror associated with the estimation of insulin resistance byHOMA would be more likely to dilute the findings resulting fromthe analysis of construct 1. We have used IMT, an intermediatecardiovascular outcome that is available in MESA. A valid outcomemeasure for construct 3 needs longitudinal follow-up for incidentdiabetes, myocardial infarction, or death. This limitation mustbe borne in mind while comparing the results of Golden et al.(18), which found construct 3 to be valid for a slightly differentmeasure of IMT in a different population using different metaboliccomponents.

In summary, while we could not observe a supra-additive interactionresulting from the simultaneous presence of metabolic syndromecomponents in terms of intimal-medial thickening of the carotidartery, co-prevalence of multiple components of the metabolicsyndrome was more frequent than expected by chance alone. Detectionof any of the components of the syndrome in a patient shouldraise the index of suspicion in the health care provider thatthe other components may also be present. This clustering isconsistent with the presence of a common underlying cause. Ifthe underlying cause is insulin resistance, our results suggestthat the metabolic syndrome provides a good proxy diagnosticfor insulin resistance, which is not assessed in routine clinicaltests. However, it remains to be determined if identificationof insulin resistance will result in a more effective therapeuticapproach than that aimed at the individual components of themetabolic syndrome.

APPENDIX

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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS--
RESULTS--
CONCLUSIONS--
APPENDIX
References

Calculation of expected component co-prevalences: Let p₁, p₂,... p₅ (q₁, q₂,... q₅) be the marginal prevalence (nonprevalence)of the five components of the metabolic syndrome.

The expected co-prevalences are given by the following:

Acknowledgments

This research was supported by contracts N01-HC-95159 throughN01-HC-95165 and N01-HC-95169 from the National Heart, Lung,and Blood Institute and M01-RR-02719 from the National Centerfor Research Resources.

The authors thank the other investigators, the staff, and theparticipants of MESA for their valuable contributions.

A full list of participating MESA investigators and institutionscan be found at http://www.mesa-nhlbi.org.

Footnotes

Published ahead of print at http://care.diabetesjournals.orgon 7 May 2007. DOI: 10.2337/dc07-0147.

Additional information for this article can be found in an onlineappendix at http://dx.doi.org/10.2337/dc07-0147.

A table elsewhere in this issue shows conventional and SystèmeInternational (SI) units and conversion factors for many substances.

The costs of publication of this article were defrayed in partby the payment of page charges. This article must thereforebe hereby marked "advertisement" in accordance with 18 U.S.CSection 1734 solely to indicate this fact.

Received for publication January 24, 2007. Accepted for publication May 1, 2007.

References

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APPENDIX
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