Introduction

Excess body mass, overweight affecting about 34% and obesity affecting 25-31% of population in the developed countries, increases the risk for type 2 diabetes mellitus (DM), cardiovascular disease (CVD), non-alcoholic fatty liver disease, different endocrine disorders, some forms of cancer, osteoarthropathies, and for sleep apnea [1]. Studies concerning the most common form of sleep apnea, obstructive sleep apnea (OSA), documented that 60-70% of patients are obese, hypertensive, have dyslipidemia, and 16% are diagnosed with DM [2]. Cytokines and insulin resistance are proposed to be mediators of excessive daytime sleepiness and pathogenetic factors for sleep apnea in obese patients, promoting cardiovascular disease [3]. Adipocytokines are released from the adipose tissue, including adipocytes and immune cells infiltrating fat, and affect vascular function, and immune regulation [4]. Biomarkers of adipose tissue may tell about glucose and lipid metabolism and pro-inflammatory properties; and consequently about the propensity for CVD [5].

Leptin, adipose-derived hormone, is a biomarker for body fat taking part in regulation of energy balance, including appetite and metabolism. Adipocytes are the major source of circulating leptin, but it can also be produced by skeletal muscles, fundic glands of stomach, bone marrow, ovaries, pituitary and liver [6]. The hypothalamus is the primary target for this adipocytokine, but leptin receptors are expressed also on polymorphonuclear leukocytes, monocytes, macrophages and lymphocytes. Leptin could modulate the immune response to atherosclerosis [7]. Failure of leptin production results from genetic abnormality. Regulatory defect concerns inadequately low leptin expression/secretion for a given fat mass and adipose tissue may expand in such subjects until the expected adipocytokine level is reached. Leptin resistance is associated with relative or absolute insensitivity to leptin [8]. Beside genetics, different metabolic factors are considered contributory to adipocytokine production and sensitivity [9]. Among the adipose tissue-derived signals (i.e., adiponectin, angiotensin, estradiol, IL-6, leptin, PAI-1, and TNF-α), resistin and its pathophysiological role in obesity and DM are a matter of controversy. Resistin has to do with endocrine pathways involved in insulin resistance [10], and consequently could be increased in obesity [11]. It also is linked to the inflammatory response and increases the expression of the interleukins IL-1, IL-6, and IL-12 and of TNF-α [12]. Resistin is not expressed in human primary adipocytes but is present in immune cells found in white adipose tissue in obesity; adipocytes may be target cells for resistin [1315]. There are studies showing a decreased serum concentration of resistin with increasing adiposity [16], which questions the possible role of this hormone in linking obesity to DM [17].

In the present study, we investigated the serum adipocytokines in overweight and obese subjects, with and without OSA.

Materials and methods

Subjects and Settings

The study was performed in accordance with the Declaration of Helsinki for Human Research, approved by the Bioethics Committee of the University of Medical Sciences in Poznan, Poland. All subjects participating in the study gave informed consent to the study procedure. Central obese non-smoking Caucasian males (at least 94 cm of waist circumference due to International Diabetes Federation 2005 criteria), aged 30-63, residents of Wielkopolska District in Poland, were enrolled into the study. Males with no acute disease or severe chronic disorder were screened by Epworth Sleepiness Scale. OSA suspected persons were evaluated in the Sleep Laboratory of the Department of Respiratory of Medicine of the University of Medical Sciences in Poznan, Poland. All studied persons were qualified for oral glucose tolerance test (OGTT) due to WHO recommendations. Newly diagnosed DM subjects were excluded from the study. Due to known gender differences, only male subjects were included. BMI, blood pressure, and metabolic factors were analyzed regarding the influence of OSA on the adipocytokine concentrations in the blood. Subjects were stratified into groups, 18 persons each, according to the BMI: overweight (Over) 25.0-29 and obese (Obese) 30.0-34.9 kg/m2. Apnea/hypopnea index (AHI ≥ 5) was used to diagnose OSA-positive (OSA-Pos) and OSA-negative (OSA-Neg) (AHI < 5). Accordingly, there were 4 groups: Over-OSA-Pos and Over-OSA-Neg, and Obese-OSA-Pos and Obese-OSA-Neg.

Measurements

Complete physical examination, systolic (SBP) and diastolic blood pressure (DBP) were taken. OSA-suspected persons underwent full-night polysomnography, using EMBLA S4000 system (Remlogic; EMBLA Co., Denver, Colorado). Airflow was monitored by a nasal flow cannula. Abdominal and thoracic movements were assessed by respiratory inductive plethysmography. Night recordings of arterial oxygen saturation were obtained by finger pulsoximetry. Snoring sounds, heart rate, and sleep position also were recorded. Apnea was defined as a cessation of airflow lasting more than 10 s, and hypopnea was defined as a discrete reduction (two thirds) of airflow and/or abdominal ribcage movements lasting more than 10 s and associated with a decrease of more than 4% in oxygen saturation.

Fasting glucose (G 0), glucose at 120 min (G 120) of the OGTT, total cholesterol (T-C), HDL cholesterol (HDL-C), triglycerides (TG), uric acid (UA) concentrations, and plasma glucose at G 120 were determined using enzymatic methods (BioMérieux, Marcyl'Etoile, France) and UV-160A Shimadzu spectrophotometer (Shimadzu, Kyoto, Japan). LDL cholesterol (LDL-C) was calculated from Friedewald's formula. Fasting serum insulin (Ins 0) was measured by ELISA method (BioSource, Nivelles, Belgium) on microplate reader Sunrise™ (Tecan Group, Männedorf, Switzerland). Insulin resistance (IR) was calculated as Ins/G0 ratio. Homeostasis model assessment of insulin resistance (HOMA-IR), defined as Ins 0xG 0/22.5, was established.

Serum samples were stored at -80°C until leptin and resistin were measured using ELISA (R&D Systems, Minneapolis, Minnesota) on a microplate reader Sunrise™ (Tecan Group, Männedorf, Switzerland). The minimum detectable levels of leptin and resistin were 0.0078 ng/ml and 0.026 ng/ml, respectively. The intraassay coefficients of variation (CV) for leptin (2.5-3.0%) and resistin (5.1-5.3%) and the inter-assay CV for leptin (4.7-5.4%) and resistin (6.5-7.0%) were calculated.

Statistical Analysis

All results are shown as means ± SD and medians. The normality of value distributions was checked by Shapiro-Wilk's test. Significant differences between studied groups were calculated by nonparametric Man Whitney-U test and correlations were described by Spearman's coefficient (R), while P < 0.05. Data were analyzed with Statistica version 6.0 packet.

Results

Clinical and laboratory data of the studied groups are shown in Table 1. The Over-OSA-Pos and Over-OSANeg as well as Obese-OSA-Pos and Obese-OSA-Neg groups did not differ regarding the age, BMI, SBP and DBP, glycemia during OGTT, insulinemia, and plasma lipid and uric acid concentrations.

Table 1 Clinical and biochemical characteristics of the studied groups.

A decreased level of resistin was found in both Over-OSA-Pos and Obese-OSA-Pos subjects compared with the respective Neg groups (Figure 1). No differences in the leptin concentration were observed in both BMI categories.

Figure 1
figure 1

Comparison of serum resistin concentration between the studied groups; *P = 0.037, **P = 0.045.

A positive correlation between leptin and BMI was found in both overweight groups of subjects, Over-OSA-Pos and Over-OSA-Neg (r = 0.60 and r = 0.44, respectively; P < 0.05), and a negative correlation between the levels of resistin and G 0 in both obese groups of subjects, Obese-OSA-Pos and Obese-OSA-Neg (r = -0. 63 and r = -0.54, respectively; P < 0.05).

Discussion

There is an explosion in research and clinical interest in bidirectional association between sleep apnea and metabolic abnormalities. Sleep fragmentation and intermittent hypoxemia are proposed to implicate sleep apnea as an independent risk factor for metabolic abnormalities [18]. Shortened sleep duration was demonstrated to provoke insulin resistance and glucose intolerance [19].

The coexistence of obesity and OSA is well known. Adiposity-related signals such as insulin and leptin circulate in proportion to body fat composition and should control satiety balance [20]. Resistin, adiposity related but immune cell-derived hormone is considered as one possible proinflammatory factor that may link obesity-related metabolic disturbances to CVD.

Previous studies show that increased serum leptin levels in OSA subjects correlate with BMI, insulin resistance, and high incidents of CVD [21, 22]. A Japanese study found elevated leptin concentrations with increasing severity of OSA, while the subjects with severe OSA presented higher BMI and insulin resistance than those with moderate OSA [23]. These authors did not find any differences in the leptin level between moderate OSA and control subjects. The findings suggest that the degree of obesity may be a more important factor for elevated leptin level in OSA patients than the severity of disease.

The present study adds to the controversy surrounding the level of leptin in subjects with increased body mass, OSA subjects in particular, supporting the role of adiposity-derived proinflammatory state, rather than obesity per se, in the pathogenesis of CVD. That is why recently we refer to discuss 'metabolically healthy but obese' individuals in the context of cardiovascular risk factors [24]. It is also suggested that leptin receptor gene polymorphism could be associated with the prevalence of OSA, and might determine obesity and lipid disturbances in homozygotic Arg/Arg genotype carries [25].

The present study on overweight and obese subjects shows no differences in their carbohydrate and lipid metabolic parameters as well as insulin resistance. Both OSA positive and negative subjects had similar leptin concentrations and, rather surprisingly, decreased serum resistin levels in both overweight and obese OSA positive subjects negatively correlated with the fasting glucose level. Positive correlations between resistin, insulin resistance, and carbohydrate disturbances have recently been reported and explained mainly by engaged proinflammatory state [10]. Controversies concerning resistin can be found in other reports on the subject. Resistin levels do not change during effective CPAP therapy, whereas insulin sensitivity index improves in the OSA patients which also closely relates with the inflammatory parameters [26]. In that study, resisitin concentration increased in OSA patients who lost weight and decreased in those who gained weight [26]. Elevated serum levels of resistin and IL-6 have been found in OSA male subjects compared with those without OSA [27], which suggests a relationship between and IL-6 changes. Since the latter is a marker of inflammatory state, inflammation-associated serum resistin changes in OSA patients are suggested. In the study in question [27], leptin level did not change in OSA subjects, which is in accord with the present results.

We conclude that serum resistin is decreased in obstructive sleep apnea subjects of excess body mass, whereas serum leptin level is unaffected.

Conflicts of interest

The authors declare that they have no competing interests.