The effect of visceral fat on the hemodilution effect of serum carcinoembryonic antigen in Korean population
Authors:
Youn-Joon Jung aff001; Seung-Su Han aff001
Authors place of work:
Department of Obstetrics and Gynecology, Chung-Ang University College of Medicine, Seoul, Korea
aff001
Published in the journal:
PLoS ONE 14(12)
Category:
Research Article
doi:
https://doi.org/10.1371/journal.pone.0225649
Summary
Objective
To investigate the relationship between visceral fat and the hemodilution effect of carcinoembryonic antigen in both sexes.
Methods
A total of 15,340 females and 20,024 males who visited the health promotion center at Chung-Ang University Hospital from 2011 to 2014 were retrospectively collected. Correlation analysis and chi-square test for linear by linear association were used to determine the correlation between carcinoembryonic antigen concentration, carcinoembryonic antigen mass and visceral fat. Multivariable linear regression analysis was used to calculate the mean of carcinoembryonic antigen concentration and the mean of carcinoembryonic antigen mass, reflecting age, aspartate aminotransferase, alanine aminotransferase, creatinine, body fat percentage, body mass index, lean body mass and waist circumference as confounding variables.
Results
Higher body mass index was related with lower carcinoembryonic antigen concentration in men (r = -0.019, P = 0.019), but higher carcinoembryonic antigen concentration in women (r = 0.084, P<0.001). Average of waist circumference for male is greater than that of female (P<0.01). Average of body fat percentage for male is lesser than that of female (P<0.01). Male lean body mass mean is larger than that of women (P<0.01). Increased waist circumference was significantly associated with higher carcinoembryonic antigen mass in both female and male (P<0.001 for trend). Postmenopausal women might be more likely to have increased carcinoembryonic antigen mass and carcinoembryonic antigen concentration (P<0.001 for trend).
Conclusions
This study suggests that visceral fat may increase total amount of CEA in the body. Visceral fat should be taken into account when evaluating serum CEA levels in both sexes.
Keywords:
body mass index – Fats – obesity – Creatinine – Plasma volume – Adipose tissue – Aminotransferases – Hemodilution
Introduction
Cancer is the second leading cause of death globally and accounted for 8.8 million death in 2015 according to the World Health Organization [1]. However, early diagnosis of cancer can improve the survival rate. Because tumor markers are important in early diagnosis of cancer, precise measurement and criteria of tumor marker are needed.
Obesity has been identified as a risk factor for several cancers. Previous studies have shown the correlation between cancer and obesity [2–4]. In addition, increased visceral fat in obesity is related to metabolic syndrome, and metabolic syndrome is also a risk factor for cancer [5]. Therefore, early diagnosis through screening test is even more important for obese people, and accurate tumor marker standards are emphasized. However, obese people may be difficult to diagnose early due to the hemodilution effect, which refers to diluted tumor marker concentrations as a result of increased plasma volume secondary to obesity [6–8].
In our previous study, CA 125 and CA 19–9 followed the hemodilution effect, but Carcinoembryonic antigen (CEA) and α-fetoprotein (AFP) showed positive correlations with body mass index (BMI) in women [9]. CEA has been shown to increase not only in cancer but also in the metabolic syndrome, which is closely associated with obesity [10, 11]. In addition, CEA concentration increases with increasing visceral fat in women [12]. These findings suggest that visceral fat which is a common risk factor for cancer and metabolic syndrome that may be associated with elevated CEA. This association will affect cancer screening using CEA in obese people. Therefore, we investigated the relationship between serum CEA concentration and visceral fat in Korean women and men.
Methods
Patients and clinical variables
This retrospective study was approved by the Institutional Review Board of the Chung-Ang university hospital (approval No. 2016–1639). The electronic medical records of 15,340 women and 20,024 men who visited the Health Promotion Center at Chung-Ang University Hospital for routine examination from 2011 to 2014 were reviewed for the retrospective analysis. Patients underwent screening for tumor markers involving CEA. Serum creatinine, serum alanine aminotransferase (ALT) and serum aspartate aminotransferase (AST) were measured to monitor the renal and liver function, which may affect the metabolism of tumor markers. The records of 14,374 women and 16,953 men were obtained after excluding those with abnormal data (CEA greater than 5.0 ng/ml) to minimize the effects of unknown cancers and benign conditions that affect tumor marker levels, such as pro-inflammatory conditions. CEA concentrations were measured as ng/ml. The weight and height of patients were measured directly. BMI was calculated by dividing weight in kg by the square of the height in meters, and patients were stratified by the WHO recommendations for Asian populations for international comparison. Patients were categorized according to BMI less than 18.5, 18.5 to less than 23, 23 to less than 27.5 and 27.5 or greater. According to metabolic syndrome diagnostic criteria of the National Cholesterol Education Program (NCEP) Adult Treatment Panel III (ATP III), waist circumference (WC) was divided into two groups based on 80cm for females and 90cm for males. Women over 50 years old were classified as menopausal [13–15]. Estimated body surface area (BSA) was calculated as (bodyweight)0.425 × (height)0.72 × 0.007184 [16]. Estimated plasma volume (in liters) was calculated from BSA×1.670 [17]. Estimated Lean body mass (LBM) was calculated as (0.29569 × weight) + (0.41813 × height)– 43.2933 for women, and (0.32810 × weight) + (0.33929 × height)– 29.5336 for men [18]. Tumor marker mass (in micro-grams) was defined as the total amount of tumor marker proteins in circulation at the time of the examination and was calculated as serum tumor marker concentration times total circulating plasma volume.
Statistical analysis
Pearson correlation analysis was used to examine the association between BMI and tumor marker concentration. Serum CEA concentrations not exhibiting a normal distribution were analyzed with continuous terms after logarithmic transformation and were back-transformed to ease interpretation. Multivariable linear regression analysis was used to calculate the mean of CEA concentration and the mean of CEA mass, considering age, AST, ALT, creatinine, body fat percentage, BMI, LBM and WC as confounding variables. Trends in serum tumor marker concentrations and tumor marker masses were tested for across BMI categories across BMI categories, waist circumference categories and menopausal grouping by chi-square test for linear by linear association. SPSS 19.0 was used for statistical analysis and associations with P<0.05 were considered statistically significant.
Results
Table 1 lists the demographic and physical characteristics, plasma volume, serum CEA concentration, CEA mass, AST, ALT, and creatinine. Male subjects had a higher age, BMI, WC, LBM, CEA, AST, ALT, and creatinine level, but lower body fat percentage (P<0.01).
Table 2 shows the distribution of subjects according to BMI classification and waist circumference in females and males, and the distribution of subjects according to menopause in females. As a percentage, the proportion of obesity in male subjects was significantly higher than that in female subjects. The proportion of WC exceeding the criteria in female subjects (35.82%) was significantly higher than that in male subjects (33.19%). A total of 26.97% of female were post-menopausal.
Higher BMI was related with higher CEA concentration in women (r = 0.084, P<0.001) but lower CEA concentration in men (r = -0.019, P = 0.013) (Fig 1).
Plasma volume was significantly increased with higher BMI in both sexes (P for trend <0.01). After controlling for age, waist circumference, BMI, AST, ALT and creatinine, the relations between serum CEA concentration, CEA mass and BMI, waist circumference, menopause were analyzed (Tables 3–5). Table 3 shows that higher CEA concentration (P for trend <0.01) and CEA mass (P for trend <0.01) were associated with higher BMI in females. Increased BMI seems to decrease CEA concentration in males, but this is not statistically significant (P = 0.074). In Table 4, greater CEA concentration (P for trend <0.01) and CEA mass (P for trend <0.01) were significantly associated with higher waist circumference in females. Greater CEA mass (P for trend <0.01) was related to higher waist circumference, but CEA concentration (P = 0.595) did not change according to WC categories in males. Table 5 suggests that greater CEA concentration (P for trend <0.01) and CEA mass (P for trend <0.01) were significantly related to menopause in women.
Discussion
Our cross-sectional study demonstrated that as visceral fat increases, serum CEA mass increases in Korean females and males. This study has once again showed that the hemodilution effect of CEA with increasing BMI occurs in only men but not in women [9].
Many previous papers have reported the hemodilution effect of tumor markers in men and women from many countries [6–8]. However, our previous study did not show the hemodilution effect of CEA in females [9]. We thought that this phenomenon was caused by visceral fat. As visceral fat measured on abdominal computed tomography (CT) increases, the serum concentration of CEA increases in women [12]. Thus, we wanted to identify the relationship between CEA concentration, CEA mass, and abdominal circumference, which represents visceral fat [19].
CEA is used to monitor disease recurrence and therapeutic efficacy in colorectal cancer and gynecologic cancer such as endometrial cancer, ovarian cancer, cervical cancer, and vulvar cancer [20–26]. However, serum CEA concentration is also mildly elevated in several nonmalignant conditions, including metabolic disturbances such as carotid atherosclerosis and metabolic syndrome, which make it difficult to monitor cancer patients [10, 11]. Thus, it is important to precisely identify the factors that affect serum CEA concentration.
From our results, as WC increases, serum CEA mass increases in both genders. It is not yet clear how visceral fat affects serum CEA mass. But, previous paper suggests that the inflammatory conditions created by increased visceral fat indirectly or directly promotes CEA production [12]. They noted that increased visceral fat resulted in increased secretion of cytokines and adipokines leading to chronic low-grade inflammatory status. Since serum CEA levels are related with a variety of chronic inflammatory disease [27, 28], increased inflammatory cytokines and adipokines due to visceral obesity may stimulate the cellular expression of CEA. Also, It has been reported that CEA can be secreted from non-CEA producing cells under certain conditions [29, 30]. For these reasons, they speculated that the altered environment due to visceral obesity would increase serum CEA levels. Basic experimental studies are needed to elucidate the precise mechanistic association between CEA and visceral obesity.
In our results, the LBM of males is significantly larger than that of females, and the body fat percentage of females is higher than that of males. It can be inferred that the proportion of bones and muscles in men is higher than in women. Bone density is 1.85g/cm3, fat density is 0.9g/cm3, and muscle density is 1.0597g/cm3 [31–33]. Fat is less dense than muscle and bone. Because plasma volume is determined by BSA, which is positively correlated with body weight, the amount of plasma that is increased by bones or muscles may be larger than that increased by fat. Taken together, it is also assumed that men with the same BMI have higher plasma volume than women. Also, Zhu et al. reported that the visceral fat (represented by trunk-to-limb fat mass ratio) of females is greater than that of males with a similar BMI range [34]. With similar BMI, increase of CEA mass due to visceral fat is thought to be greater in women than in men. Therefore, the hemodilution effect of CEA does not appear in females because the increased plasma volume according to BMI in females is smaller than that of males. The increased CEA mass due to visceral fat in females is higher than that of males with a similar BMI.
We also compared the CEA concentration and CEA mass of women before and after menopause. Increased visceral fat in women after menopause has already been proven several times [35, 36]. Based on this fact, we found that postmenopausal women had greater CEA concentration and CEA mass than premenopausal women. This is a reaffirmation of the effect of visceral fat on serum CEA.
This study had several limitations. First, we could not exclude the effect of confounding factors that affect the CEA levels such as smoking, hormonal levels, and past medical history. To minimize the effect of confounding factors, subjects with high serum CEA concentrations above the normal range were excluded. We also could not exclude the potential effect of racial difference. Further studies are needed to clarify the effect of visceral fat on CEA in well-organized cohort.
In conclusion, our study showed that visceral fat has an effect on increasing serum CEA mass in Korean women and men. These findings suggest that the effect of visceral fat could be considered in cancer screening using serum CEA concentration. The effect of visceral fat might also be considered when using serum CEA concentration to monitor cancer patients. This conclusion requires confirmation through large-scale studies with biochemical support.
Supporting information
S1 Fig [tif]
Receiver operating characteristics (ROC) curve for ability of the serum CEA concentration and CEA mass to identify abdominal obesity.
S1 Table [docx]
Linear regression analysis of serum CEA concentration in female and male subjects.
S2 Table [docx]
Linear regression analysis of serum CEA mass in female and male subjects.
Zdroje
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