The Risk of Metabolic Syndrome According to the White Blood Cell Count in Apparently Healthy Korean Adults

Chan-Hee Jung; Won-Young Lee; Bo-Yeon Kim; Se Eun Park; Eun-Jung Rhee; Cheol-Young Park; Ki-Won Oh; Ji-Oh Mok; Chul-Hee Kim; Sung-Woo Park; Sun-Woo Kim; Sung-Koo Kang

doi:10.3349/ymj.2013.54.3.615

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Jung, Lee, Kim, Park, Rhee, Park, Oh, Mok, Kim, Park, Kim, and Kang: The Risk of Metabolic Syndrome According to the White Blood Cell Count in Apparently Healthy Korean Adults

Original Article

Endocrinology & Metabolism

Yonsei Medical Journal

Yonsei Medical Journal 2013; 54(3): 615-620.

Published online: 19 March 2013

DOI: https://doi.org/10.3349/ymj.2013.54.3.615

The Risk of Metabolic Syndrome According to the White Blood Cell Count in Apparently Healthy Korean Adults

Chan-Hee Jung¹

, Won-Young Lee², Bo-Yeon Kim¹, Se Eun Park², Eun-Jung Rhee², Cheol-Young Park², Ki-Won Oh², Ji-Oh Mok¹, Chul-Hee Kim¹, Sung-Woo Park², Sun-Woo Kim², Sung-Koo Kang¹

¹Division of Endocrinology and Metabolism, Department of Internal Medicine, Soonchunhyang University School of Medicine, Bucheon, Korea.

²Division of Endocrinology and Metabolism, Department of Internal Medicine, Kangbuk Samsung Hospital, Sungkyunkwan University School of Medicine, Seoul, Korea.

Corresponding author: Dr. Won-Young Lee, Division of Endocrinology and Metabolism, Department of Internal Medicine, Kangbuk Samsung Hospital, Sungkyunkwan University School of Medicine, 29 Saemunan-ro, Jongno-gu, Seoul 110-746, Korea. Tel: 82-2-2001-1543, Fax: 82-2-2001-1588, drlwy@hanmail.net

Received 30 May 2012 Revised 17 August 2012 Accepted 20 August 2012

(open-access):

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

Purpose

Considerable amount of interest has been focused on the positive relationship between inflammation and the metabolic syndrome (MS). However, few studies have been performed to evaluate the relationship between baseline white blood cell (WBC) count and future risk for developing MS. Therefore, we investigated whether the baseline plasma levels of WBC count could be associated with future risk for MS in apparently healthy Korean.

Materials and Methods

A total of 1135 subjects (781 men and 354 women with a mean age of 49 years), who underwent health examinations at Kangbuk Samsung Hospital in both 2002 and 2005 were enrolled. The presence of MS was defined using the modified criteria of the National Cholesterol Education Program Adult Treatment Panel III using BMI instead of waist circumference.

Results

The baseline levels of WBC count were significantly higher among incident MS cases than among subjects without MS. The relative risks of incident MS were 1.4, 3.2 and 2.7 for WBC quartiles 2, 3, and 4, respectively, when compared with the first quartile (p-value for trend <0.001). These positive associations persisted after adjustment for baseline body mass index, blood pressure, fasting glucose, high density lipoprotein-cholesterol, triglyceride and homeostatic model assessment-insulin resistance; adjusted relative risk of incident MS for the 2nd, 3rd and 4th quartile groups vs. the lowest quartile were 1.2, 2.4 and 1.7, respectively (p-value for trend =0.011).

Conclusion

This retrospective cohort study suggests that an elevated WBC count could be associated with incident MS, suggesting that baseline inflammation mirrored by WBC level can impact future MS development.

Keywords: White blood cell count, metabolic syndrome, inflammation

INTRODUCTION

Recent epidemiologic studies increased our understanding on the role of inflammation played in atherosclerosis and cardiovascular disease (CVD)1-4 and considerable amount of interest has also been focused on the positive relationship between inflammation and metabolic syndrome (MS).5,6 Inflammation is known to be associated with the pathogenesis of MS itself as well as coronary heart disease,7,8 and proinflammatory cytokines play important roles in the relation between MS and CVD. Recent studies have also demonstrated that high serum C-reactive protein concentrations are associated with MS.9,10

White blood cell (WBC) count is an objective marker of acute infection, tissue damage, and other inflammatory conditions. An increase in the WBC count is closely related with advanced atherosclerosis and the incidence and mortality rate of CVD.11 In cross-sectional studies, WBC counts are correlated with isolated variables of MS and clearly increased with numbers of MS.5,6,12,13 In addition, Oda and Kawai14 reported that the prevalence of MS and diabetes increases through the quartiles of WBC in Japanese men and women. Although several epidemiological studies have already noted a relationship between WBC counts and MS, most of these studies are cross-sectional studies. Few studies have been performed to evaluate the relationship between baseline WBC count and future risk for developing MS.15,16

Therefore, we investigated whether the baseline plasma levels of the WBC count could impact the future risk for MS in apparently healthy Korean adults.

MATERIALS AND METHODS

Subjects

We conducted a retrospective study of 1476 participants who underwent annual health examinations at Kangbuk Samsung Hospital in both 2002 and 2005. The subjects were inhabitants of either Seoul (capital of South Korea) or Gyeonggi province (satellite town). We excluded those subjects who already met the MS criteria at baseline (n=217) and those subjects with other missing data for components of metabolic syndrome. The subjects whose WBC counts beyond 10400/µL were also excluded from the study. The subjects with documented acute infection and malignancy were also excluded. Finally, we analyzed 1135 subjects (781 males, 354 females). Informed consent requirement for this study was exempted by the institutional review board because researchers accessed only the database for analysis, and personal information was not accessed. This study was approved by the institutional review board at Kangbuk Samsung Hospital.

Measurements

The participants underwent routine physical examinations that included the measurement of height, weight, blood pressure, and overnight fasting blood sampling. The standing height was measured without shoes to the nearest 0.1 cm. Weight was determined without shoes on a light cloth. Blood pressure was measured by using a standard mercury sphygmomanometer after being seated for at least 5 min. Blood was sampled after 12 hours of fasting, and the venous blood glucose, insulin, total cholesterol (TC), triglyceride (TG) and high- and low-density lipoprotein cholesterol (HDL-C and LDL-C, respectively) were measured. Plasma glucose was measured in duplicate by the hexokinase method using an autoanalyzer (Hitachi, Tokyo, Japan), which had an interassay coefficient of variation of 1.6%. An enzymatic calorimetric test was used to measure the TC and TG levels. The selective inhibition method was used to measure the level of HDL-C and a homogeneous enzymatic calorimetric test was used to measure the level of LDL-C. The fasting serum insulin level was measured by immunoradiometric assay (RIABEAD II, Abbott, Tokyo, Japan) having an intra-assay coefficient of variance of 1.2% to 1.9% and an inter-assay coefficient of variance of 1.4% to 3.3%. Insulin resistance status was calculated by using the homeostatic model assessment-insulin resistance (HOMA-IR). HOMA-IR=[fasting insulin (µIU/mL)×fasting blood glucose (mmol/L)]/22.5. The total WBC count and differential count were assessed by an autoanalyzer (ADVIA 129, Bayer, Germany). The presence of MS was defined by using a modified version of the ATP III criteria.17 Briefly, four of the five MS components were defined using the following ATP III categorizations: 1) high blood pressure (BP), ≥130/85 mm Hg or patients using anti-hypertensive agents; 2) Hypertriglyceridemia, ≥150 mg/dL (1.693 mmol/L); 3) Low HDL-C, <40 mg/dL (1.034 mmol/L) in men and <50 mg/dL (1.293 mmol/L) in women; 4) High fasting glucose, ≥100 mg/dL (5.6 mmol/L). The fifth component was defined based on body mass index (BMI) because waist circumference was not available in all subjects. Central obesity was diagnosed at a BMI (≥25 kg/m²). The subjects with three or more of the following criteria were defined as having MS. The smoking status of subjects was classified as non-smoker or smoker (former or current).

Statistical analysis

Statistical analyses were performed by SPSS version 11.0. All values were presented as mean±SD. Comparisons of WBC counts according to two groups who have MS or not were performed by independent sample t-test. The chi-square test was used for categorical variables. WBC counts were divided into quartiles and logistic regression analysis was used to evaluate the risk for each category of WBC count for the association with MS. For each risk, a 95% confidence interval was determined. Also, quartile-specific risk estimates were obtained through logistic regression after adjusting for age, gender, smoking, BMI, HOMA-IR and other components of MS. Differences in the prevalence of MS according to the quartiles of WBC count were determined by chi-square test. p values of <0.05 were considered statistically significant.

RESULTS

Clinical characteristics

Comparisons of the baseline characteristics of the subjects who were subsequently developed MS and did not develop MS are shown in Table 1. The mean age of the subjects were 49 years. Subjects who were subsequently diagnosed with MS in 2005 had a higher baseline BMI, systolic BP, diastolic BP, triglyceride, T-cholesterol, fasting glucose, fasting insulin and HOMA-IR. The subjects who did not develop MS in 2005 had a higher baseline HDL-C. The mean baseline levels of the WBC were significantly higher for the MS group (p<0.001). The overall present incident MS in 2005 was 8.9%.

Clinical characteristics according to the quartiles of WBC count

We classified subjects according to the quartiles of WBC count and their clinical characteristics were compared (Table 2). BMI, triglyceride, LDL-C, total cholesterol, fasting glucose, fasting insulin and HOMA-IR increased significantly from the 1st quartile to the 4th quartile of WBC count. HDL-C decreased significantly from the 1st quartile to the 4th quartile of WBC count.

Risk of developing MS according to the quartiles of baseline WBC levels

The relative risks for MS according to the quartile groups of WBC count are shown in Table 3. In unadjusted models, the relative risks of incident MS in 2005 were 1.4, 3.2 and 2.7 for the WBC quartiles 2, 3, 4 when compared with first quartile (p-value for trend <0.001). After further adjustment for HOMA-IR as index of insulin resistance, the relative risks of incident MS in 2005 were 1.1, 2.5 and 2.1 for the WBC quartiles 2, 3 and 4, respectively, when compared with the first quartile (p-value for trend=0.011). Additional multivariable adjustments for components of MS i.e., baseline BMI, BP, fasting glucose, HDL-C and triglycerides, attenuated these associations, but these positive associations persisted (Table 3).

DISCUSSION

This retrospective cohort study indicates that an elevated level of WBC is associated with later risk of developing MS in apparently healthy Koreans. Several cross-sectional studies have reported the association between WBC and MS.12-14,18-20 Wang, et al.5 reported that subjects in the highest quartile of WBC counts demonstrated a threefold increase, in the odds ratio for MS compared to subjects in the lowest quartile of WBC counts. Also, in the study of Lao, et al.,19 the risk of MS increased significantly with higher total WBC, and vascular risk factors were positively associated with WBC in older Chinese, and Lohsoonthorn, et al.13 showed that, the risk of MS increased across the successive quartiles of the WBC counts among Thai women. Finally, Kim, et al.20 reported that the OR for MS was 2.64 in the highest quartile of total WBC count versus the lowest quartiles of commensurate total WBC count in a Korean population. However, all of these studies are cross-sectional studies. Only few studies have been performed to evaluate the association between baseline WBC counts and future development of MS. Odagiri, et al.15 investigated the 7-year incidence of MS in relation to quartiles of WBC in healthy workers, and found that the incidence of MS was 1.2 to 1.6 times higher in the higher quartile of the WBC compared with the lowest quartile.

Although the mechanisms involved in the linking of WBC counts with MS remain unclear, there are several postulations. Some authors proposed that insulin resistance or hyperinsulinemia, an essential component of MS, probably results from the chronic activation of the immune system and inflammation.21 Proinflammatory cytokines such as tumor necrosis factor-alpha (TNF-α) and interleukin-6 (IL-6), in addition to being produced by activated macrophages, were shown to be appreciably synthesized in adipose tissue,22,23 and TNF-α and IL-6 secreted from adipose tissue were shown to impair the action of insulin on adipocytes and muscle cells by paracrine/autocrine manner.23,24 Because WBC counts are increased by cytokines and are closely associated with both insulin resistance and hyperinsulinemia, their association could result in a subclinical inflammatory reaction and the expression of an insulin-resistant state.25 In the present study, we also showed that fasting insulin and HOMA-IR increased according to the increasing of WBC quartiles, in agreement with the findings that WBC count is associated with insulin resistance and insulin concentration.26 Nevertheless, the risks for MS, as calculated according to baseline WBC levels' quartile distribution in the present study, persisted after adjustment for HOMA-IR. Future large scale study is needed to clarify underlying pathophysiological role of WBC played in the genesis of MS.

Because our study population included subjects who frequently received health check-up, several characteristics of the present study population may be different from other populations that do not receive available medical services. We think that most of the study subjects are in economic stability. Therefore, the generalizability of our study may be limited. In the present study, the prevalence of MS in 2005 was 8.9%, which is seemingly low compared with those values reported in other ethnic groups. There is a possibility that the participant bias might have affected these results.

Studies regarding inflammation and CVD have been confounded by the fact that cigarette smoking increases numerous inflammatory markers, including leukocyte counts.27,28 However, in several large-scale studies, there is positive correlation of total WBC count with CVD that is independent of smoking.6,29 Also, we found that increased WBC level was significantly associated with later risk of developing MS, even after adjusting for smoking.

The present study has some limitations. First, the subjects were urban habitants (either Seoul or Gyeonggi province). The participants were the employees of the company, whose annual health check-up was carried out in the health promotion center or their family members and most of the subjects were likely members of upper-middle economic class. Although it could be regarded as the strength of this study, the participants of this study were a group of relatively homogeneous characters:, a follow-up cohort of annual health check-up program in a single health promotion center in Korea, and not the representative of the ethnic group. Therefore, the generalizability of our study may be limited. This could have biased the baseline characteristics of the study cohort and future development of MS.

Second, the serum high-sensitivity C-reactive protein (hsCRP), a marker of chronic low-grade inflammation, is known to be a sensitive predictor of CVD and is related to components of MS. Comparison of WBC counts and hsCRP levels is needed for more definitive conclusion on the usefulness of WBC as an independent predictor of incident MS, since our study did not include hsCRP levels. The strengths of our study would be higher if we performed this analysis.

Third, we used BMI instead of waist circumference as criteria of central obesity. This might underestimate the effect of obesity on MS. Various diagnostic criteria of MS have been proposed by different organizations over the past decade.30 The main difference concerns the measure for central obesity. Indeed, there was no agreement on the definition of abdominal obesity between the International Diabetes Federation (IDF) and the American Heart Association/National Heart, Lung, and Blood Institute.31 Alberti, et al.31 indicated that waist circumference differs in different populations and may require modification for different ethnic group. The IDF values are closer to a BMI of 25≥ kg/m² in males. Recent studies have used BMI successfully to classify those with MS, lending support to the validity of our measure.32,33 In particular, Shiwaku, et al.34 stated that the definition of BMI 25≥ kg/m² as obesity is suitable for the determination of the MS among Korean and Japanese.

Fourth, we didn't exclude patients who were positive for hepatitis B virus surface antigen and/or hepatitis C virus antibody and with helicobacter pylori infection, which are prevalent in Korea.

Fifth, our study lacked information on drug use, which could affect serum WBC counts including antidiabetic, antihypertensive, or statin medication. The strengths of our study would be higher if we excluded these confounding factors.

In conclusion, in the present study, increased WBC level was associated with later risk of developing MS in apparently healthy adults. Further large-scale prospective studies are warranted to clearly reveal the underlying pathophysiological role of WBC for MS and to establish better clinical utility to predict the development of MS.

Figures and Tables

Table 1

Basal Characteristics of the Subjects

BMI, body mass index; BP, blood pressure; HDL-C, high density lipoprotein cholesterol; LDL-C, low-density lipoprotein cholesterol; FBG, fasting blood glucose; WBC, white blood cell; HOMA-IR, homeostatic model assessment-insulin resistance; MS, metabolic syndrome.

As triglyceride, insulin and HOMA-IR were not normally distributed, they were expressed by median levels (percentile 25 and 75).

Table 2

Basal Characteristics of the Subjects According to Quartiles of the WBC Counts

As triglyceride, insulin and HOMA-IR were not normally distributed, they were expressed by median levels (percentile 25 and 75).

Table 3

Prevalence and Odds Ratio for the Risk of the Metabolic Syndrome According to Baseline Quartiles of WBC Counts

BMI, body mass index; BP, blood pressure; HDL-C, high density lipoprotein cholesterol; FBG, fasting blood glucose; HOMA-IR, homeostatic model assessment-insulin resistance, TG, triglyceride; MS, metabolic syndrome; WBC, white blood cell.

Data are expressed as odds ratio (95% confidence interval).

Model 1: no adjustment. Model 2: adjusted for age, sex, smoking. Model 3: adjusted for age, sex, smoking, BMI. Model 4: adjusted for age, sex, smoking, BMI, HOMA-IR. Model 5: adjusted for age, sex, smoking, BMI, HOMA-IR, BP, TG, HDL-C, FBG.

Notes

The authors have no financial conflicts of interest.

References

1. Alexander RW. Inflammation and coronary artery disease. N Engl J Med. 1994. 331:468–469.

2. Koenig W. Predicting risk and treatment benefit in atherosclerosis: the role of C-reactive protein. Int J Cardiol. 2005. 98:199–206.

3. Pearson TA, Mensah GA, Alexander RW, Anderson JL, Cannon RO 3rd, Criqui M, et al. Markers of inflammation and cardiovascular disease: application to clinical and public health practice: a statement for healthcare professionals from the Centers for Disease Control and Prevention and the American Heart Association. Circulation. 2003. 107:499–511.

4. Danesh J, Collins R, Appleby P, Peto R. Association of fibrinogen, C-reactive protein, albumin, or leukocyte count with coronary heart disease: meta-analyses of prospective studies. JAMA. 1998. 279:1477–1482.

5. Wang YY, Lin SY, Liu PH, Cheung BM, Lai WA. Association between hematological parameters and metabolic syndrome components in a Chinese population. J Diabetes Complications. 2004. 18:322–327.

6. Yen ML, Yang CY, Yen BL, Ho YL, Cheng WC, Bai CH. Increased high sensitivity C-reactive protein and neutrophil count are related to increased standard cardiovascular risk factors in healthy Chinese men. Int J Cardiol. 2006. 110:191–198.

7. Festa A, D'Agostino R Jr, Howard G, Mykkänen L, Tracy RP, Haffner SM. Chronic subclinical inflammation as part of the insulin resistance syndrome: the Insulin Resistance Atherosclerosis Study (IRAS). Circulation. 2000. 102:42–47.

8. Aguilar-Salinas CA, Rojas R, Gómez-Pérez FJ, Mehta R, Franco A, Olaiz G, et al. The metabolic syndrome: a concept hard to define. Arch Med Res. 2005. 36:223–231.

9. Ridker PM, Buring JE, Cook NR, Rifai N. C-reactive protein, the metabolic syndrome, and risk of incident cardiovascular events: an 8-year follow-up of 14 719 initially healthy American women. Circulation. 2003. 107:391–397.

10. Han TS, Sattar N, Williams K, Gonzalez-Villalpando C, Lean ME, Haffner SM. Prospective study of C-reactive protein in relation to the development of diabetes and metabolic syndrome in the Mexico City Diabetes Study. Diabetes Care. 2002. 25:2016–2021.

11. Kannel WB, Anderson K, Wilson PW. White blood cell count and cardiovascular disease. Insights from the Framingham Study. JAMA. 1992. 267:1253–1256.

12. Nagasawa N, Tamakoshi K, Yatsuya H, Hori Y, Ishikawa M, Murata C, et al. Association of white blood cell count and clustered components of metabolic syndrome in Japanese men. Circ J. 2004. 68:892–897.

13. Lohsoonthorn V, Dhanamun B, Williams MA. Prevalence of metabolic syndrome and its relationship to white blood cell count in a population of Thai men and women receiving routine health examinations. Am J Hypertens. 2006. 19:339–345.

14. Oda E, Kawai R. The prevalence of metabolic syndrome and diabetes increases through the quartiles of white blood cell count in Japanese men and women. Intern Med. 2009. 48:1127–1134.

15. Odagiri K, Uehara A, Mizuta I, Yamamoto M, Kurata C. Longitudinal study on white blood cell count and the incidence of metabolic syndrome. Intern Med. 2011. 50:2491–2498.

16. Chen W, Srinivasan SR, Xu J, Berenson GS. Black-white divergence in the relation of white blood cell count to metabolic syndrome in preadolescents, adolescents, and young adults: the Bogalusa Heart Study. Diabetes Care. 2010. 33:2474–2476.

17. Grundy SM, Cleeman JI, Daniels SR, Donato KA, Eckel RH, Franklin BA, et al. Diagnosis and management of the metabolic syndrome: an American Heart Association/National Heart, Lung, and Blood Institute Scientific Statement. Circulation. 2005. 112:2735–2752.

18. Grau AJ, Buggle F, Becher H, Werle E, Hacke W. The association of leukocyte count, fibrinogen and C-reactive protein with vascular risk factors and ischemic vascular diseases. Thromb Res. 1996. 82:245–255.

19. Lao XQ, Neil Thomas G, Jiang C, Zhang W, Adab P, Lam TH, et al. White blood cell count and the metabolic syndrome in older Chinese: the Guangzhou Biobank Cohort Study. Atherosclerosis. 2008. 201:418–424.

20. Kim DJ, Noh JH, Lee BW, Choi YH, Chung JH, Min YK, et al. The associations of total and differential white blood cell counts with obesity, hypertension, dyslipidemia and glucose intolerance in a Korean population. J Korean Med Sci. 2008. 23:193–198.

21. Fernández-Real JM, Ricart W. Insulin resistance and inflammation in an evolutionary perspective: the contribution of cytokine genotype/phenotype to thriftiness. Diabetologia. 1999. 42:1367–1374.

22. Mohamed-Ali V, Goodrick S, Rawesh A, Katz DR, Miles JM, Yudkin JS, et al. Subcutaneous adipose tissue releases interleukin-6, but not tumor necrosis factor-alpha, in vivo. J Clin Endocrinol Metab. 1997. 82:4196–4200.

23. Hotamisligil GS, Shargill NS, Spiegelman BM. Adipose expression of tumor necrosis factor-alpha: direct role in obesity-linked insulin resistance. Science. 1993. 259:87–91.

24. Fernandez-Real JM, Vayreda M, Richart C, Gutierrez C, Broch M, Vendrell J, et al. Circulating interleukin 6 levels, blood pressure, and insulin sensitivity in apparently healthy men and women. J Clin Endocrinol Metab. 2001. 86:1154–1159.

25. Sims E. Humoral factors. 1993. Oxford: IRL Press;1–373.

26. Targher G, Seidell JC, Tonoli M, Muggeo M, De Sandre G, Cigolini M. The white blood cell count: its relationship to plasma insulin and other cardiovascular risk factors in healthy male individuals. J Intern Med. 1996. 239:435–441.

27. Kawada T. Smoking-induced leukocytosis can persist after cessation of smoking. Arch Med Res. 2004. 35:246–250.

28. Corre F, Lellouch J, Schwartz D. Smoking and leucocyte-counts. Results of an epidemiological survey. Lancet. 1971. 2:632–634.

29. Ford ES. Leukocyte count, erythrocyte sedimentation rate, and diabetes incidence in a national sample of US adults. Am J Epidemiol. 2002. 155:57–64.

30. Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults. Executive Summary of The Third Report of The National Cholesterol Education Program (NCEP) Expert Panel on Detection, Evaluation, And Treatment of High Blood Cholesterol In Adults (Adult Treatment Panel III). JAMA. 2001. 285:2486–2497.

31. Alberti KG, Eckel RH, Grundy SM, Zimmet PZ, Cleeman JI, Donato KA, et al. Harmonizing the metabolic syndrome: a joint interim statement of the International Diabetes Federation Task Force on Epidemiology and Prevention; National Heart, Lung, and Blood Institute; American Heart Association; World Heart Federation; International Atherosclerosis Society; and International Association for the Study of Obesity. Circulation. 2009. 120:1640–1645.

32. Malik S, Wong ND, Franklin SS, Kamath TV, L'Italien GJ, Pio JR, et al. Impact of the metabolic syndrome on mortality from coronary heart disease, cardiovascular disease, and all causes in United States adults. Circulation. 2004. 110:1245–1250.

33. Wong ND, Sciammarella MG, Polk D, Gallagher A, Miranda-Peats L, Whitcomb B, et al. The metabolic syndrome, diabetes, and subclinical atherosclerosis assessed by coronary calcium. J Am Coll Cardiol. 2003. 41:1547–1553.

34. Shiwaku K, Nogi A, Kitajima K, Anuurad E, Enkhmaa B, Yamasaki M, et al. Prevalence of the metabolic syndrome using the modified ATP III definitions for workers in Japan, Korea and Mongolia. J Occup Health. 2005. 47:126–135.

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ORCID iDs: Chan-Hee Jung
https://orcid.org/http://orcid.org/0000-0001-8988-0187
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