the association of serum long-chain omega-3 polyunsaturated fatty … · the association of serum...
TRANSCRIPT
THE ASSOCIATION OF SERUM LONG-CHAIN OMEGA-3 POLYUNSATURATED
FATTY ACIDS WITH SERUM RESISTIN
Behnam Tajik
Master’s Thesis
Public Health Nutrition
School of Medicine
Faculty of Health Sciences
University of Eastern Finland
1
UNIVERSITY OF EASTERN FINLAND, Faculty of Health Sciences
Public Health Nutrition
Tajik B.: THE ASSOCIATION OF SERUM LONG-CHAIN OMEGA-3 POLYUNSATURATED
FATTY ACIDS WITH SERUM RESISTIN
Master’s thesis, 52 pages
Instructors: Jyrki Virtanen, PhD. Tomi-Pekka Tuomainen, Professor
Keywords: Resistin, n-3 PUFA, Fish, Adipokines
THE ASSOCIATION OF SERUM LONG-CHAIN N-3 POLYUNSATURATED FATTY ACIDS
WITH SERUM RESISTIN
Resistin concentration and long chain omega-3 PUFA (n-3 PUFA) are both integrated with the risk
of cardiovascular disease (CVD) and diabetes. However, there is little prior information about the
association between the serum n-3 PUFA and serum resistin concentration in healthy population.
A total of 892 men free of CVD and type 2 diabetes from prospective, population-based Kuopio
Ischemic Heart Disease Risk Factor study (KIHD) at baseline in 1984–1989, were studied. Serum
esterified and non-esterified fatty acids were determined in one gas chromatographic run without
pre-separation. Serum long chain n-3 PUFA was set as an exposure. Dietary intake of nutrients was
assessed quantitatively with a 4-day food recording at the KIHD baseline examinations. Intake of
nutrients was calculated by use of Nutrica version 2.5 software. Serum resistin concentration was
measured using ELISA kit. The univariate associations between the serum n-3 PUFAs
concentration and demographic, lifestyle and clinical characteristics at baseline were assessed by
means and linear regression for continuous variables and chi2-test for categorical variables. We used
linear regression models to determine the association between serum n-3 PUFAs and serum resistin
level and analysis of covariates to estimate the average resistin level in quartiles of the serum long-
chain n-3 PUFA.
The mean age was 61.7 years (s.d. 6.4). The mean serum concentration as a percentage of all serum
fatty acids was 2.78 % for docosahexaenoic acid (DHA) (s.d. 0.90), which was highest serum
concentration among all long chain n-3 PUFAs, followed by eicosapentaenoic acid (EPA) and
docosapentaenoic acid (DPA) which were 1.66% (s.d. 0.92) and 0.78% (s.d. 0.16) respectively. The
mean concentration of serum resistin was 1.92 ng/ml (s.d. 0.67 ng/ml). Serum resistin was inversely
associated with total n-3 PUFA and with individual long chain n-3 PUFA, DPA and DHA after age,
gender and examination year adjustment. However, after further adjustments, only the association
between the serum DHA and serum resistin concentration remained significant. No significant
associations were observed between the EPA and serum resistin concentration in both models.
We observed that serum long chain n-3 PUFA and especially DHA, an objective biomarker of fish
or fish oil consumption, were inversely associated with serum resistin concentration. As resistin is
known as a potential marker for increased risk of obesity, inflammation, diabetes and heart diseases,
the beneficial effect of serum long chain n-3 PUFA on these diseases can be partially explained by
their impact on serum resistin concentration.
2
Abbreviations
ALA: alpha linolenic acid
AMI: acute myocardial infraction
BMI: body mass index
CAD: coronary artery disease
CRP: C - reactive protein
CHD: coronary heart disease
CVD: cardiovascular disease
DA: Dalton molecular scale
DHA: docosahexaenoic acid
DPA: docosapentaenoic acid
EPA: eicosapentaenoic acid
HC: hip circumference
HDL: high-density lipoprotein
HR: heart rate
KIHD: Kuopio Ischaemic Heart Disease Risk Factor study
IL-6: interleukin-6
LDL: low-density lipoprotein
MUFA: monounsaturated fatty acid
N-3 PUFA: long-chain n-3 polyunsaturated fatty acids
PCI: percutaneous coronary intervention
3
PBMC: peripheral blood mononuclear cells
PPARγ: peroxisome proliferator-activated receptor gamma
POS: polycystic ovary syndrome
RELM: resistin-like molecule
SAFA: saturated fatty acid
T2D: type 2 diabetes
TG: triglyceride
TNF: tumor necrosis factor
WC: waist circumference
WHR: waist to hip ratio
4
”Science is organized knowledge. Wisdom is organized life”
Immanuel Kant
To my family Mr. N. Tajik, Mrs. A. Cheraghi and Mr. B. Tajik
Thanks a million to my supervisors
Jyrki Virtanen, PhD. and Tomi-Pekka Tuomainen, Professor.
5
Contents
1 INTRODUCTION ....................................................................................................................... 7
2 LITERATURE REVIEW ............................................................................................................ 8
2.1 Resistin .................................................................................................................................. 8
2.2 Polyunsaturated fatty acids .................................................................................................... 9
2.2.1 N-3 PUFA recommendation .......................................................................................... 9
2.3 Possible association between the n-3 PUFAs and resistin level ......................................... 10
2.3.1 Heart diseases ............................................................................................................... 10
2.3.2 Insulin resistance and diabetes ..................................................................................... 11
2.3.3 Obesity ......................................................................................................................... 12
2.3.4 Inflammation ................................................................................................................ 13
2.4 Potential mechanism of the association between EPA and DHA and adipokines .............. 14
2.5 Previous studies ................................................................................................................... 15
2.6 Factors affecting resistin level ............................................................................................. 15
2.6.1 Age and gender ............................................................................................................ 16
2.6.2 Anthropometric measurement ...................................................................................... 16
2.6.3 Smoking and alcohol .................................................................................................... 16
2.6.4 Blood pressure.............................................................................................................. 17
2.6.5 Dietary factors .............................................................................................................. 17
2.6.6 Cholesterol ................................................................................................................... 18
2.6.7 Triglycerides ................................................................................................................ 18
2.6.8 Other factors ................................................................................................................. 18
2.7 Therapeutic consideration ................................................................................................... 19
3 AIM OF STUDY ....................................................................................................................... 20
4 MATERIALS AND METHODS ............................................................................................... 21
4.1 Study design and participants .............................................................................................. 21
6
4.2 Measurements ...................................................................................................................... 21
4.2.1 Assessment of dietary intake........................................................................................ 22
4.2.2 Measurement of PUFA ................................................................................................ 23
4.2.3 Serum resistin ............................................................................................................... 23
4.2.4 Statistical analysis ........................................................................................................ 23
5 RESULTS .................................................................................................................................. 25
5.1.1 Baseline characteristics ................................................................................................ 25
5.1.2 Serum long chain n-3 PUFA and serum resistin .......................................................... 25
6 DISCUSSION ............................................................................................................................ 31
6.1 Strengths and limitations of the study ................................................................................. 33
7 CONCLUSIONS ........................................................................................................................ 34
7
1 INTRODUCTION
One of the biggest challenges in the twenty-first century is the increasing burden of chronic diseases
like cardiovascular disease (CVD) and diabetes, which are responsible for the large portion of
mortality and disability in the whole world (World Health Organization). For this reason, ever
increasing importance of recognizing the factors which are associated with these chronic diseases
becomes undeniable. Diet and nutritional factors have significant role in prevention of CVD and
diabetes, and also take part in the CVD and diabetes treatments. Amid nutritional factors, long-
chain n-3 polyunsaturated fatty acids (n-3 PUFA) seem to ameliorate obesity and may play a crucial
role in the lower incidence of CVD (Mozaffarian& Wu 2011). Moreover, one of the recently
discovered factor, which has been associated with the risk of diabetes and CVD is resistin
(McTernan et al. 2002, Reilly et al. 2005, Burnett et al. 2006a). N-3 PUFA seems to alter resistin
concentration; however, the association between intake of n-3 PUFA and resistin concentration has
not been well evaluated.
There is little prior information about the association between the serum n-3 PUFA and serum resistin
concentration in healthy population. However, over the past years, relevant studies have been
conducted among animals and findings about the association between the n-3 PUFA and serum
resistin concentration are inconsistent (Haugen et al. 2005, Ye Wang 2014). In the population-based
studies, the association between the n-3 PUFA and resistin concentration/expression were carried
out among people with coronary heart disease (CHD) and acute myocardial infraction (AMI) and
results are highly contrasting (Mizia-Stec et al. 2011, Mostowik et al. 2013, Oner & Muderris
2013). Primary objective of the current study was to evaluate the association between the serum n.3
PUFA and serum resistin concentration in healthy population.
8
2 LITERATURE REVIEW
2.1 Resistin
Adipose tissue is an active metabolic and endocrine organ, which secretes numerous substances
including hormones, growth factors, cytokines, chemokines and adipokines (Morrison & Farmer
2000). Adipokines are bioactive substances, which include adiponectin, leptin, ghrelin and resistin
(Deng & Scherer 2010). Adipokines provide a link between the obesity and inflammation disorders
and they may influence on the weight regulation by affecting appetite, energy expenditure, and
glucose and lipid homeostasis (Mora & Pessin 2002), though the data are not consistent.
Adiponectin is a collagen-like protein that is mainly secreted by the adipocytes and it is known as
an anti-inflammatory and an insulin-sensitizer factor. Also it could suppress the risk of
atherosclerosis and liver diseases (Kadowaki et al. 2006) . Leptin is another adipokines, which is
secreted from the white adipocytes and it may affect the whole-body energy balance in rodents and
humans (Houseknecht et al. 1998).
Among adipokines, role of resistin in body was the interest in previous studies. Resistin is a
cysteine-rich adipose-derived peptide hormone and is a member of the resistin-like molecule
(RELM) family with 12.5k Dalton Molecular scale (DA) molecular weight (Steppan et al. 2001). It
includes mature sequence of 108 amino acid (Steppan et al. 2001). Resistin originally named for its
resistance to insulin (Steppan et al. 2001). In mice, resistin expression occurs predominantly in the
adipocytes (Steppan et al. 2001, Nogueiras et al. 2003, Milan et al. 2002). In contrast, it has been
suggested that significant level of resistin expression predominantly occurs in the macrophages
(mainly), peripheral blood mononuclear cells (PBMCs), bone marrow, spleen and mature
adipocytes (Patel et al. 2003, Janke et al. 2002, Fain et al. 2003, Degawa-Yamauchi et al. 2003).
Resistin is known as a pro-inflammatory cytokine that seems to be a link between the obesity and
type II diabetes (T2D) (Holcomb et al. 2000, Steppan et al. 2001). It has been reported that resistin
concentration is directly associated with the risk of breast cancer (Wei-kai et al. 2007, Hou et al.
2007), myocardial infarction (Weikert et al. 2008), colon cancer (Salageanu et al. 2010, Gonullu et
al. 2010, Nakajima et al. 2010), and rheumatoid arthritis (Senolt et al. 2007, Otero et al. 2006).
9
2.2 Polyunsaturated fatty acids
PUFA are fatty acids, which structurally have double bonds. PUFA are divided into two categories:
n-3 PUFA (omega-3) and n-6 PUFA (omega-6). N-3 PUFA are fatty acids, which have a double
bond at the carbon atom number 3, while in n-6 PUFA this double bond sits at carbon atom number
6 (Russo 2009, Ruxton et al. 2004).
Individual n-3 PUFAs are: 1- Alpha linolenic acid (ALA) (18:3n-3) is an essential fatty acid, which
cannot be synthesized in human body and is obtained from the plants sources such as canola, rapeseed
oils, linseed oils and nuts (Burdge & Calder 2005, Barceló-Coblijn & Murphy 2009). It has been
shown that ALA may improve insulin sensitivity by decreasing lipid accumulation in skeletal muscle
and liver (Muramatsu et al. 2010). Moreover, some studies reported that higher intake of ALA is
inversely associated with the risk of CVD (Mozaffarian 2005).
2- Eicosapentaenoic acid (EPA) (20:5n-3) and decosahexaenoic acid (DHA) (22:6n-3) are derived
mainly from seafood such as anchovy, bluefish, herring, mackerel, mullet, sardines, salmon,
sturgeon, tuna and other marine food sources and fish oils (Saldeen & Saldeen 2006). Little part of
plasma ALA is destined for the synthesis of EPA and DHA in healthy individuals due to various
factors (0.2% and 8% - 0% to 4% respectively). For example, it has been indicated that higher
intake of ALA leads to increased conversion of ALA to EPA, and EPA to DHA (Burdge & Calder
2005, Barceló-Coblijn & Murphy 2009). Moreover, this conversion is higher in women as
compared to men. Since this conversion cannot meet the EPA demand, the majority of DHA and
EPA are obtained from diet (Burdge & Calder 2005, Barceló-Coblijn & Murphy 2009).
3- Docosapentaenoic acid (DPA) is an EPA metabolite. Since fish contains limited amount of DPA
(Kaur et al. 2011) and the correlation between the fish consumption and circulating DPA is weaker
than DHA and EPA (von Schacky & Weber 1985, Arterburn et al. 2006), the major source of DPA
is based on internal metabolism rather than directly from diet.
2.2.1 N-3 PUFA recommendation
According to the European Food Safety Authority dietary recommendations, 250-500mg/day EPA
and DHA may decrease the risk of CVD in healthy adult population (Djuricic et al. 2014).
Moreover, International Society for the Study of Fatty Acids and Lipids recommend at least 500
mg/day (EPA+DHA) for primary prevention of CHD (Cunnane et al. 2004) . American Heart
Association (AHA) recommended intake of 1 g EPA+DHA per day from fish oil as a secondary
10
prevention for people with CHD background (American Heart Association Nutrition Committee et
al. 2006).
2.3 Possible association between the n-3 PUFAs and resistin level
Resistin concentration and n-3 PUFA are both integrated with the health issues such as heart
disease, insulin resistance and diabetes, obesity and inflammation, which suggest that there may be
an association between them.
2.3.1 Heart diseases
It has been reported that resistin can play a pathogenic role in development of atherosclerosis and
coronary artery diseases (CAD) (Jamaluddin et al. 2012, Lee & Kim 2012, Lim et al. 2008, Burnett
et al. 2006, Tuttolomondo et al. 2010). Resistin concentration can be a risk marker for ischemic
heart disease in the generally healthy population (Cabrera de León et al. 2014) since resistin
concentration is directly associated with the coronary calcium score, which is one of the marker of
atherosclerosis (Reilly et al. 2005). Resistin concentration is also directly associated with the
incidence of atherosclerosis because of its role in inflammation process (Ding et al. 2011). It has
been shown that resistin concentration was significantly higher in 220 patients coronary acute
syndrome as compared to healthy participants (Wang et al. 2009). This finding was in agreement
among patients with CAD (Ohmori et al. 2005).
However, some studies did not found any association between resistin concentration and risk of
CVD. A study conducted among 547 consecutive patients (age 63 ± 10 years) undergoing coronary
angiography reported that there is no associations between resistin concentration with the presence
of coronary stenoses and also with incidence of future vascular events (Hoefle et al. 2007). This
finding was supported with another study among 1162 subjects with and without angiographic
coronary artery disease (Pilz et al. 2007).
The association between higher resistin concentration and CVD may be partially explained by the
association between resistin concentration and endothelial function. Endothelial function is strongly
correlated with the endothelial nitric oxide synthase system in human coronary artery endothelial
cells (Murohara et al. 1998, Palmer et al. 1987, Zeng & Quon 1996, Moore et al. 2011). It has been
shown that resistin concentration is inversely associated with the expression of endothelial nitric
oxide synthase (Chen et al. 2010, Chen et al. 2002, Verma et al. 2003, Kawanami et al. 2004).
11
It has been indicated that n-3 PUFA play an important role in the lower incidence of CVD by its
impacts on cardiovascular risk factors (Mozaffarian & Wu 2011). N-3 PUFA consumption may lead
to reduction in plasma triglyceride (TG) (Harris & Bulchandani 2006), decreased resting heart rate
(HR) and HR respond to exercise (Mozaffarian & Wu 2011, Peoples et al. 2008), lower systolic and
diastolic blood pressure (Geleijnse et al. 2002) and improvement in cardiac filling and myocardial
efficiency (Pepe & McLennan 2002). Moreover, it has been pointed out that n-3 PUFA may have an
anti-thrombotic effects (Wang et al. 2004).
According to the recent prospective, population-based Kuopio Ischemic Heart Disease Risk Factor
study (KIHD), among 1981 men aged 42–60 years and free of CVD, dietary n-3 PUFA intake was
associated with the lower risk of fatal, but not with non-fatal CHD (Virtanen et al. 2012). Some
factors may have effects on the association between the fish intake and risk of CHD. For example, it
has been suggested that inverse association between fish intake and risk of CHD was stronger in
women than men (Järvinen et al. 2006). Mercury content, which is known as an environmental
contaminant, is another factor, which can attenuate the association between fish intake and risk of
CHD (Rissanen et al. 2000, Virtanen et al. 2005).
2.3.2 Insulin resistance and diabetes
Insulin resistance is a condition, which the body cells do not respond properly to the insulin. In this
condition, the insulin that is produced in the body is more than normal and it cannot function
sufficiently in skeletal muscle, liver and adipocytes (Caro 1991, Shulman 2000). It has been
suggested that insulin resistance is linked to the obesity and it often leads to T2D and CVD (Bo et
al. 2005, Balkau & Eschwege 1999).
Resistin was postulated to contribute to insulin resistance (Holcomb et al. 2000, Steppan et al. 2001,
Bo et al. 2005). The majority of animal studies showed that resistin can attenuate insulin action in
hepatic and skeletal muscle and it may have impact on the glucose metabolism (Rajala et al. 2002,
Rangwala et al. 2004, Muse et al. 2004, Banerjee et al. 2004, Fan et al. 2007), hepatocytes activity,
homeostasis of fatty acids and lipoprotein metabolism in skeletal muscle (Borst et al. 2005, Sato et
al. 2005).
Resistin can be a potential risk factor in central obesity, which may lead to T2D (McTernan et al.
2002). It has been shown that resistin concentration was directly associated with the insulin
resistance in population-based studies (Silha et al. 2003). In addition, the level of resistin increased
in diabetic participants as compared to non-diabetic participants (McTernan et al. 2002) . According
12
to (Gharibeh et al. 2010) findings among 125 participants suffering from T2D, serum resistin
concentration in obese diabetic participants was higher than non-diabetics. Resistin mRNA
expression seems to be higher in diabetic women as compared to the non-diabetic women (Tsiotra
et al. 2008). It has been also indicated that resistin concentration is higher in patients with
gestational diabetes that pregnant women with normal glucose tolerance (Kuzmicki et al. 2009).
In contrast, some studies did not show any association between the serum resistin concentration and
risk of T2D (Pfutzner et al. 2003, Stejskal et al. 2003, Lee et al. 2003, Levy et al. 2002). Regarding
to the cross-sectional study in 123 middle-aged and 120 healthy young subjects, resistin
concentration was not correlated with BMI, WHR, fat mass and insulin resistance. Also resistin
concentrations were non different in diabetics and non-diabetics (Lee et al. 2003). Moreover, it has
been demonstrated that resistin gene expression is not associated with insulin resistance
determinants in human abdominal adipocyte (Janke et al. 2002).
The evidences regarding to an association between the n-3 PUFA and diabetes remained unclear. It
has been suggested that n-3 PUFA is associated with the risk of diabetes since it may have
association with diabetes risk factors such as hypertension, inflammation and dyslipidemia and the
translocation of glucose transporters. Recently in KIHD, serum n-3 PUFA was inversely associated
with the risk of T2D among 2212 middle-aged and older men (Virtanen et al. 2014).
However, in two meta analyses among 40184 individuals and 25670 cases of incident diabetes, and
among 527441 participants and 24082 diabetes cases, they could not find a statistically significant
association between EPA and DHA intake with risk of diabetes (Wu et al. 2012, Wallin et al. 2012).
According to another meta-analysis, which was conducted among 24509 T2D patients and 545275
participants, n-3 PUFA was inversely associated with the risk T2D among Asians population. In
contrast, a direct association has been found between the n-3 PUFA consumption and risk of T2
diabetes among western study population (Zheng et al. 2012).
2.3.3 Obesity
Resistin and n-3 PUFA seem to be associated with the risk of obesity, as a chronic low-grade
inflammation. A study among 27 men and women with body mass index (BMI) 21.7 ± 0.4 kg/m2,
and 50 obese with BMI 49.8 ± 1.5 kg/m2 showed that obese subjects had higher resistin
concentration as compared to lean subjects (Degawa-Yamauchi et al. 2003). A number of animal
studies have shown that higher intake of n-3 PUFA can protect against the development of obesity
by the reduction of body fat accumulation (Buckley & Howe 2009). It has been pointed out that n-3
13
PUFA may be a protective factor for obesity by its impact on determinants of obesity. For example,
plasma concentration of n-3 PUFA was inversely associated with BMI, waist circumference (WC)
and hip circumference (HC) (Micallef et al. 2009).
The correlation between resistin concentration and obesity was not supported by all studies. For
example, Regarding to the cross-sectional study in 123 middle-aged women and 120 healthy young
subjects, resistin concentration was not correlated with BMI, WHR, fat mass and insulin resistance.
Also resistin concentrations were non different in diabetics and not diabetics (Lee et al. 2003). This
finding was supported by another study among 177 non-diabetic subjects (75 male, 102 female; age
32-75 years). In this study, resistin was only associated with body fat, whereas no associations have
been found between resistin concentration and BMI and waist circumference (Utzschneider et al.
2005)
2.3.4 Inflammation
Inflammation has been known as a risk factor for the beginning and progression of chronic diseases
(Hansson et al. 2006). Resistin concentration and intake of n-3 PUFA are two factors that may be
involved in the inflammation process. Resistin is known as a pro-inflammatory cytokine and
structurally is similar to proteins, which are directly related to inflammation process (Holcomb et al.
2000, Steppan et al. 2001). Substantial evidence from epidemiological studies indicates that serum
resistin concentration is directly associated with the some inflammatory markers, such as tumor
necrosis factor (TNF), interleukin-6 (IL-6) and C-reactive protein (CRP) (Bo et al. 2005, Al-Daghri
et al. 2005, Shetty et al. 2004, Stejskal et al. 2003).
It has been shown that serum resistin concentration was directly related to CRP concentration among
77 diabetics or participants who were at high risk to develop diabetes (Shetty et al. 2004). This
association remained significant after sex and BMI adjustment. Direct association between resistin
concentration and CRP has been supported in another prospective study among 213 obese participants
(mean age 45.1 + 16.7 years, and mean BMI 35.6 + 5.7) (De Luis et al. 2009). Serum resistin level
was directly correlated with CRP among 300 obese and non-obese men (Bo et al. 2005). It has been
reported that resistin concentration enhances the synthesis and secretion of TNF as a pro-
inflammatory cytokines (Bokarewa et al. 2005, Silswal et al. 2005).
Findings about the association between the n-3 PUFA and inflammation markers are inconsistent.
In the KIHD, there was an inverse association between the serum n-3 PUFA and serum CRP
concentration among 1395 middle-aged and older men (Reinders et al. 2012). Regarding to the
14
some observational studies findings, higher fish consumption was associated with lower CRP
concentration (He et al. 2009, Kalogeropoulos et al. 2010, Kalupahana et al. 2011).
In contrast, another study could not find any association between habitual dietary intake of n-3
PUFA and CRP concentration among 859 healthy men and women (Pischon et al. 2003).
Furthermore, finding from a placebo-controlled randomized trial showed that fish oil
supplementation could not alter CRP concentration among healthy population with mild
hypertriglyceridemia (Skulas-Ray et al. 2011).
The anti-inflammatory properties of n-3 PUFAs can be partially explained by their impact on the
secretion of proinflammatory mediators (Calder 2006, Tai & Ding 2010), inflammatory
eicosanoids, cytokines, and reactive oxygen species and the expression of adhesion molecules
(Calder 2006, Tai & Ding 2010) and reduction of macrophage migration into adipose tissue (He et
al. 2009, Kalogeropoulos et al. 2010, Kalupahana et al. 2011). For example, it has been reported
that intake of n-3 PUFA, particularly EPA and DHA, are inversely associated with the production
of some pro-inflammatory cytokines like TNF and IL-6 in the monocytes and endothelial cells
(Babcock et al. 2002, Khalfoun et al. 1997, Lo et al. 1999, Novak et al. 2003).
2.4 Potential mechanism of the association between EPA and DHA and adipokines
The pathophysiological mechanisms of serum n-3 PUFAs and adipokines concentration have not
been fully explored. However, it seems that the secretion and expression of adipokines may be
influenced by intake of n-3 PUFA, particularly EPA and DHA. This role can be partially explained
by the relationship between EPA, DHA and peroxisome proliferator-activated receptor gamma
(PPARγ). PPARγ is a group of the nuclear receptors, which are mainly expressed in adipose tissue,
colon and macrophages and can regulate fatty acid storage, regulation of cellular differentiation and
energy metabolism (Fajas et al. 1997, Houseknecht et al. 1998).
Resistin gene expression is affected by the expression of PPARγ (Way et al. 2001, Steppan et al.
2001, Patel et al. 2003). It has been suggested that the activation of PPARγ in fat can be affected by
EPA and DHA (Han et al. 2014) and this association can have indirect impact on the secretion of
the adipokines (Neschen et al. 2006). However, more evaluations are needed to confirm this
possible mechanism.
Moreover, it has been reported the resistin expression is strongly directly associated with production
of some proinflammatory cytokines such as tumor necrosis factor, interleukin-1, and interleukin-6
15
in peripheral blood mononuclear cells (PBMCs) (Anderson et al. 2007, Bokarewa et al. 2005).
Since, N-3 PUFA may reduce production of these cytokines (Calder 2006), n-3 PUFA may play an
indirect role in the secretion and expression of resistin.
Noteworthy that higher resistin expression in macrophages can decrease production of adenosine
monophosphate-activated protein kinase and it leads to reduction in fatty acid uptake and
metabolism in skeletal muscle, which can be another reason for the inverse association between the
resistin concentration and serum n-3 PUFA concentration (Palanivel & Sweeney 2005).
2.5 Previous studies
There are few studies that evaluated the association between the n-3 PUFA and resistin
concentration and expression. It has been suggested that plasma EPA and arachidonic acid may lead
to a small reduction in the expression of resistin mRNA in murine adipocytes (Haugen et al. 2005).
Moreover, in non-alcoholic steatohepatitis rats, resistin concentration was decreased by 8 weeks
high-fat diet with n-3 PUFA (Ye Wang 2014).
In population-based studies, a randomized control trial among 38 patients with acute myocardial
infraction (AMI) indicated that n-3 PUFA therapy slightly increased serum resistin concentration in
the first month after AMI (Mizia-Stec et al. 2011). In contrast, regarding to the two randomized –
placebo control trials among participants with stable coronary artery disease (CAD) undertaking
elective percutaneous coronary intervention (PCI) and women with polycystic ovary syndrome
(POS), n-3 PUFA treatments did not alter resistin concentration (Mostowik et al. 2013, Oner &
Muderris 2013).
2.6 Factors affecting resistin level
For evaluating the association between the serum resistin concentration and serum n-3 PUFA, it is
necessary to take into account the impact on dietary and non-dietary factors on the resistin
concentration. For example, it has been suggested metabolic syndrome determinants are associated
with resistin concentration (Norata et al. 2007). Metabolic syndrome is cluster of metabolic
disorders, which is linked to increasing incidence of heart diseases, insulin resistance and diabetes.
BMI, age, gender, blood pressure, concentrations of triglyceride, low-density lipoprotein cholesterol
(LDL) and high-density lipoprotein cholesterol (HDL), CRP concentration, use of tobacco,
hormonal changes and glucose level are known as the metabolic syndrome determinants. (Mottillo
et al. 2010, Timar et al. 2000).
16
2.6.1 Age and gender
The role of age on resistin level is still unclear. However, some studies found that resistin
concentration is directly associated with the age. Regarding to case-control study among 140 type II
diabetic patients and 125 control subjects, plasma resistin concentration was higher among the older
diabetic participants. Also resistin concentration was higher in diabetic women was higher
compared to diabetic men (Gharibeh et al. 2010). This finding was supported by another study,
which was conducted among healthy population (Silha et al. 2003). In contrast, another study
showed that age and gender did not have effect on resistin among healthy population (Vilarrasa et
al. 2005). This finding was in agreement with another study among 120 healthy Greek students
(Yannakoulia et al. 2003).
2.6.2 Anthropometric measurement
It has been pointed out that resistin concentration was directly associated with the BMI among in
healthy men aged 15 to 70 (Vilarrasa et al. 2005). Another study among 114 healthy Greek students
showed that serum resistin concentration was inversely associated with waist to hip ratio (WHR),
while, a direct association was observed between the resistin concentration and body fat mass
(Yannakoulia et al. 2003). Resistin content was slightly higher in men with normal BMI as
compared to overweight and obese men (Bo et al. 2005). Moreover, resistin level was directly
correlated with BMI only among normal BMI participants. It has been indicated that serum resistin
level was directly associated with WC in diabetic participants (Gharibeh et al. 2010). It has been
reported that resistin concentration was not associated with BMI among 17 participants with mean
BMI 23 and non-diabetic obese participants with mean BMI 33 (Silha et al. 2003). Another cross-
sectional study also could not find any association between the BMI and expression of resistin
(Savage et al. 2001).
2.6.3 Smoking and alcohol
Smoking is known as a risk factor for several health problems and it is known as an important risk
factor of CVD. Few studies have investigated the impact of smoking and alcohol on the resistin
concentration. It has been pointed out that smokers had higher plasma resistin level compared to
non-smokers (Vilarrasa et al. 2005). In addition, it has been demonstrated that serum resistin
concentration was inversely associated with moderate alcohol consumption among women
(Fargnoli et al. 2008).
17
2.6.4 Blood pressure
Association between resistin concentration and blood pressure is still matter of debate. It has been
demonstrated that resistin concentration was directly associated with the systolic blood pressure in
healthy population (Norata et al. 2007). According to a prospective cohort study, which was
conducted in 213 non-diabetic obese male and female subjects, serum resistin concentration was
inversely associated with the systolic and diastolic blood pressure (De Luis et al. 2009). Another
study among 300 healthy participants found a direct association between serum resistin
concentration and diastolic blood pressure, but after age and BMI adjustment, this association did
not remain (Bo et al. 2005).
2.6.5 Dietary factors
It seems that dietary factors may have impacts on the resistin concentration. For example, it has
been indicated that people with high score Alternate Healthy Eating Index (AHEI) may have lower
concentration of resistin (Fargnoli et al. 2008). AHEI is the way that reflects a healthier dietary
pattern. It has some parameters including intake of fruit and vegetables intake, the ratio of white
meat to red meat, trans fat, the ratio of polyunsaturated fat to saturated fat (P:S), intake of cereal
fiber, nuts and soy, alcohol consumption, use of multivitamin . Each of them has the scores that
show the quality of individual dietary pattern (Fargnoli et al. 2008). It has been reported that some
parameters like fiber intkae, use of multivitamin and P: S were associated with the reduction of the
resistin concentration. (Fargnoli et al. 2008). In addition, a low- caloric diet based on the increase
consumption of high fiber foods, vegetables and seasonal fruits combined by 60 min per day
walking led to decrease in the resistin concentration in 20 obese women (BMI > 30kg/m2) (Fethi et
al. 2013).
It has been shown that resistin concentration is directly related to the intake of saturated fatty acids
(Cabrera de León et al. 2014). In contrast, an inverse association has been observed between the
intake of monounsaturated fatty acids (MUFA) and serum resistin concentration in generally
healthy population. Another study by Greco et al. (2014) showed that Mediterranean, hypocaloric
diet including carbohydrates (55% of total calories), proteins (20% of total calories), and mostly
mono- and polyunsaturated fats (25% of total calories)and 25-30 g/day fiber, did not change serum
resistin level among obese adults with mean BMI was 37 kg/m2 (Cabrera de León et al. 2014).
Another study, which was conducted among 114 healthy Greek students showed that total energy
intake or macronutrient intake did not significantly alter resistin concentration after gender and
18
body fat adjustments (Yannakoulia et al. 2003). Another study among healthy and normal-weight
women (age 22 ± 3 years) could not find any changes in resistin concentration after 4-weeks
reduced-calorie diet. However, adiponectin and leptin levels were reduced by this diet (Wolfe et al.
2004). Noteworthy that some observational studies indicated that fasting leads to reduction in
resistin mRNA expression. However, after feeding, resistin mRNA expression gets back to normal
level (Kim et al. 2001; Rajala et al. 2002).
2.6.6 Cholesterol
Resistin mRNA expression has an inverse correlation with plasma cholesterol level (Jové et al.
2003). In addition, it has been shown that serum resistin concentration was inversely associated
with HDL-cholesterol in 77 diabetics or participants who were high risk of diabetes (Shetty et al.
2004). This association was supported by another study in healthy population (Norata et al. 2007).
Also it has been demonstrated that there was an inverse association between resistin level and HDL
in non- diabetic obese people (De Luis et al. 2009). It has been reported that resistin level was
inversely correlated with ApoAI level and directly associated with ApoAI/ApoB in women (Norata
et al. 2007).
2.6.7 Triglycerides
It has been shown that there is a highly direct association between resistin concentration and
triglyceride level (Norata et al. 2007). Regarding to a study by (Haugen et al. 2005), which was
conducted among 54 adolescents, serum resistin concentration was directly correlated with the
triglyceride concentration after six-month lifestyle intervention. Moreover, a direct association has
been observed between the resistin concentration and triglyceride level among non-diabetic obese
subjects (De Luis et al. 2009). Another study, which was conducted among 300 adult men,
indicated that plasma resistin level was directly associated with triglyceride level among normal
BMI participants, However, this association was strongly dependent to the glucose level (Bo et al.
2005).
2.6.8 Other factors
There are other factors, which affect resistin level but number of studies showing association
between these factors and resistin level is limited. For example, it has been reported that resistin and
leptin concentrations are related to each other (Silha et al. 2003) . Moreover, serum resistin
19
concentration is strongly associated with plasma urea, insulin and creatinine in diabetic people
(Gharibeh et al. 2010).
2.7 Therapeutic consideration
Since higher resistin concentration is associated with the risk of chronic diseases including CVD
and T2D, several therapeutic approaches have been investigated the possibility of decreasing
resistin concentration and resistin gene expression. Use of statins drugs including atorvastatin and
simvastatin was one of the most effective approaches. It has been found that resistin concentration
and resistin mRNA expression may be reduced among patients with T2D after atorvastatin
treatment (Ichida et al. 2006). It has been also found that atorvastatin treatment was inversely
associated with the resistin expression by the impact of this treatment on the TNF-α (Shyu et al.
2009).
Higher folic acid intake (folic acid-fortified foods or folic acid supplementation) is another
treatments, which seems to be effective in lowering resistin concentration and expression. It has
been reported that daily high-dose folic acid consumption (71µ per kg body weight) decreased
resistin concentration in obese diabetic mice (Seto et al. 2010).
In addition to these treatments, the beneficial impact of oleic acid, mainly from olive oil has been
investigated and it seems that higher consumption of oleic acid may reduce the resistin gene
expression in the isolated adipocytes (L6 muscle cells) and enhance the impact of glucose-lowering
therapies and rosiglitazone, which seems to be inversely associated with lower risk of
hyperresistinemia (Rea & Donnelly 2006). However, the evaluation of the effect of high-dose oleic
acid consumption on the resistin concentration among humans are still ongoing and future studies
are needed to confirm this beneficial treatment.
20
3 AIM OF STUDY
Tackling chronic diseases like CVD and T2D is integrated with recognition are factors, which are
associated with the risk of these chronic diseases. Intake of n-3 PUFAs, as an important dietary
component and serum resistin concentration are two factors, which seem to be associated with the
risk and incidence of chronic diseases. However, there is no information about possible association
between them in generally healthy population.
The primary objective of the present study was to find out the association between n-3 PUFA and
serum resistin concentration among middle-aged and older participants from KIHD cohort.
21
4 MATERIALS AND METHODS
4.1 Study design and participants
The participants of this study were drawn from people who participated in Kuopio Ischemic Heart
Disease Risk Factor Study (KIHD). The primary goal of KIHD study was to investigate risk factors
for CVD, atherosclerosis, and other health related issues among randomly selected men living in
Eastern Finland (Salonen 1988). The baseline examination was accomplished between March 1984
and December 1989, consisted of 3235 men who were 42, 48, 54, or 60 years old. Out of total
population, 2682 men (82.9% eligible) was taken into the study population. 4-Year follow-up
examinations were carried out between March 1991 and December 1993 and 1038 men (88%
eligible) were participated. Next round was an 11- year follow-up examinations (1998-2001), which
included 854 men from second cohort and 920 new women (1774 Participants). This stage was
followed by 20- year follow-up examinations, which were conducted between 2005 and 2008
among 1860 participants (1230 men and 630 women, 80.1%). The KIHD protocol was approved by
the Research Ethics Committees of the University of Kuopio. All the subjects signed a written
informed consent.
For the current analysis between serum long chain n-3 and serum resistin in healthy population, we
used the data from the 11-year examination round. We excluded from the analysis subjects with
CVD and T2D. These exclusion left 892 subjects (467 females and 425 males).
4.2 Measurements
Subjects gave blood specimens between 8:00 and 10:00 AM on Tuesday, Wednesday, or Thursday
after having abstained from ingesting alcohol for 3 days, smoking for 12 hours, and eating for 12
hours. After the subject had rested in the supine position for 30 minutes, blood was drawn with
Terumo Venoject VT-100PZ vacuum (Terumo Corp., Tokyo). No tourniquet was used (Salonen et
al. 1992).
The number of cigarettes, cigars, and of tobacco currently smoked daily, the duration of regular
smoking in years, history of myocardial infarction, angina pectoris and other ischemic heart disease,
the presence of hypertension, and current antihypertensive medication were recorded using a self-
administered questionnaire, which was checked by an interviewer. Reinter views to obtain medical
history were conducted by a physician. The family history of CHD was defined as positive if the
biological father, mother, sister, or brother of the subject had CHD history. The history of
22
hypertension in siblings was defined as positive if any sisters or brothers were reported to ever have
had hypertension (Salonen et al. 1992).
A subject was defined as a smoker if he had ever smoked on a regular basis and had smoked
cigarettes cigars, or a pipe within the past 30 days. The lifelong exposure to smoking (cigarette
pack-years) was estimated as the product of years smoked and the number of tobacco products
smoked daily at the time of examination. Years smoked were defined as the sum of years of
smoking regardless of when smoking had started, whether the subject had stopped smoking, or
whether it had occurred continuously or during several periods. The consumption of alcohol in the
previous 12 months was assessed with the Nordic Alcohol Consumption Inventory, which contains
15 items (Salonen et al. 1992).
Resting blood pressure was measured between 8:00 and 10:00AM on the examination day by one
nurse with a random-zero mercury sphygmomanometer. The measuring protocol included, after a
supine rest of minutes, three measurements in supine, one in standing, and two in sitting position
with 5-minutes intervals. The mean of all six systolic pressure values was used in the present
analyses as the systolic blood pressure and the mean of all six diastolic measurements as diastolic
blood pressure (Salonen et al. 1992).
Both at baseline and at the 11-years examinations, plasma glucose was measured by using a glucose
dehydrogenase method after precipitation of proteins by trichloroacetic acid. The serum samples for
insulin determination were stored frozen at –80C. Serum insulin was determined with a Novo
Biolabs radioimmunoassay kit (Novo Nordisk). Serum CRP was measured with an immunometric
assay (Immulite High Sensitivity CRP Assay; Diagnostic Products Corporation).
4.2.1 Assessment of dietary intake
The consumption of foods at baseline was assessed with a guided food record of 4 consecutive
days, one of which was a weekend day, by household measures. A picture book of common foods
and dishes was used to help in the estimation of portion sizes and contained 126 of the most
common foods and drinks consumed in Finland during the 1980s. For each food item, the
participant could choose from 3 to 5 commonly used portion sizes or describe the portion size in
relation to those shown in the book. To further improve accuracy, instructions were given and
completed food records were checked by a nutritionist together with the participant. Nutrient
intakes were estimated by using NUTRICA 2.5 software (Social Insurance Institution). The
23
software’s databank is mainly based on Finnish values of nutrient composition of foods.
(Voutilainen et al. 2001).
4.2.2 Measurement of PUFA
Serum esterified and non-esterified fatty acids were determined in one gas chromatographic run
without pre-separation (Laaksonen et al. 2002). Serum fatty acids were extracted with chloroform-
methanol. Chloroform phase was evaporated and treated with sodium methoxide, which methylated
esterified fatty acids. Quantification was performed with the reference standard purchased from Nu-
check Prep Inc. (MN, USA). Each analyte had individual reference standard and recovery of
analytes was confirmed with an internal standard eicosan (arachidonic acid C20H40O2). Fatty acids
were chromatographed in an NB-351 capacity column (HNU-Nordion, Helsinki, Finland) by a
Hewlett-Packard 5890 series II gas chromatograph (Hewlett-Packard Company, Avondale, PA,
USA) with a flame ionization detector. The coefficient of variation of major esterified fatty acids
and non-esterified fatty acids for repeated measurements were ~5% and ~ 15% respectively. The
esterified fatty acids concentration were adjusted for serum low-density lipoprotein cholesterol,
high-density lipoprotein cholesterol and triglyceride concentration an account of the fact that
relative degree of saturation of fatty acids varies amid esterified fatty acids type (i.e., cholesterol
esters, phospholipid and triglycerides). No adjustment was performed for non-esterified fatty acids.
For the serum total long-chain omega-3 PUFA, we used the sum of eicosapentaenoic acid (EPA,
20:5n-3), docosapentaenoic acids (DPA, 22:5n-3) and docosahexaenoic acid (DHA, 22:5n-3).
4.2.3 Serum resistin
Serum resistin levels were measured using enzyme-linked immunosorbent assay (ELISA) with a
commercial kit (Phoenix Pharmaceuticals Inc., USA). The lower detection limit of the assay was
0.0625 ng/ml. Intra- assay coefficients of variation for the assay was 3%, while inter-assay was
10%.
4.2.4 Statistical analysis
All statistical analysis was applied using SPSS software version 21 for windows (SPSS Inc.,
Chicago, IL, USA). The univariate associations between the serum EPA+DPA+DHA concentration
and demographic, lifestyle and clinical characteristics at baseline were assessed by means and linear
regression for continuous variables and chi2-test for categorical variables. We used linear regression
models to determine the association between serum n-3 PUFAs and serum resistin level and
24
analysis of covariates to estimate the average resistin level in quartiles of the serum long-chain n-3
PUFA. Correlations were assessed by the Spearman’s correlation coefficients.
Two models were adjusted for possible confounders which were associated with resistin level in
previous studies or association with exposures or outcomes in the present analysis. The model 1
was adjusted for age, gender and examination year. Model 2 was a multivariate-adjusted model
including model 1 variables and leisure time physical activity (kcal/day), BMI (kg/m2), alcohol
intake(g/week), smoking (cig packs/day), serum TG (mmol/l), systolic and diastolic blood pressure
(mm Hg), serum LDL(mmol/l), serum HDL(mmol/l), serum CRP (mg/l), SAFA (energy %) and
MUFA (energy%). Tests for linear trend for each model were conducted by using median values for
each category of variable. All P-values were two-tailed (α = 0.05). Cohort mean was used to replace
missing values in covariates (<0.5%).
25
5 RESULTS
5.1.1 Baseline characteristics
Baseline characteristic of participants are presented in Table 1. The mean age was 61.7 years (s.d.
6.4). The mean serum concentration as a percentage of all serum fatty acids was 2.78 % for DHA
(s.d. 0.90), which was highest serum concentration among all long chain n-3 PUFAs, followed by
EPA and DPA that were 1.66% (s.d. 0.92) and 0.78% (s.d. 0.16) respectively. The mean fish intake
was 80.6 g/d (s.d. 123.71) at the baseline. Subjects with higher concentration of total long chain n-3
PUFA (Q4) were more likely to have higher education, income and leisure time physical activity,
serum HDL-c, protein and vegetables intake, and more likely to be current smokers as compared to
subjects with lower serum total long chain n-3 concentration. Furthermore, they had lower waist to
hip ratio, serum triglyceride and total cholesterol, and intake of carbohydrates and saturated fatty
acids (Table 1). Based on the gender, men had higher concentration of TG, LDL, higher intake of
fish and total energy and lower LDL concentration as compared to the women (Table 2).
5.1.2 Serum long chain n-3 PUFA and serum resistin
The mean concentration of serum resistin was 1.92 ng/ml (s.d. 0.67 ng/ml). Results of the Model 1
adjusted for age, gender and examination year showed that serum total long chain n-3 PUFA
(EPA+DPA+DHA) was inversely associated with serum resistin (Table 3). Among individual fatty
acids, serum DHA had strongest inverse association with serum resistin level (Table 3).
Furthermore, in the multivariate-adjusted model, the association between serum DHA and serum
total long chain n-3 PUFA and serum resistin remained statistically significant, while and serum
DPA and EPA were not associated with serum resistin anymore (Table 3). We could not find any
differences between genders (P for interaction: 0.99)
26
Table 1. Baseline characteristics according to serum total n-3 PUFAs
Serum total n-3 PUFA quartile (median)
Variables Q1 (3.47) Q2 (4.40) Q3 (5.44) Q4 (7.23) P
Number of subjects 223 223 223 223
Age (y) 61.35(6.52) 61.89(6.65) 61.48(6.35) 61.96(6.26) 0.696
BMI (kg/m2) 27.2 (4.25) 27.3 (4.01) 27.1 (3.85) 26.8 (4.08) 0.461
Smoking (%) 25.3% 10.5% 13.4% 7.8% <0.001
Serum EPA (%) 0.88 (0.23) 1.26 (0.23) 1.66 (0.31) 2.82 (1.01) <0.001
Serum DPA (%) 0.64 (0.13) 0.75 (0.13) 0.81 (0.13) 0.90 (0.15) <0.001
Serum DHA (%) 1.83 (0.37) 2.39 (0.30) 2.95 (0.35) 3.95 (0.67) <0.001
Serum ALA (%) 0.98 (0.30) 0.96 (0.30) 0.92 (0.26) 0.91 (0.25) 0.039
Serum CRP (mg/l) 2.87 (3.93) 2.33 (3.42) 2.68 (5.11) 2.40 (4.17) 0.492
Physical activity
(kcal/d) 170.92 (202.37) 190.14 (202.16) 196.56 (266.70) 199.38 (171.87) 0.501
Waist to hip ratio 0.91 (0.08) 0.90 (0.08) 0.90 (0.09) 0.88 (0.09) 0.005
Mean SBP (mm Hg) 137 (18) 137 (18) 135 (18) 134 (15) 0.156
Mean DBP (mm
Hg) 82 (9) 82 (9) 82 (9) 81 (8) 0.607
Education (years) 9.0 (2.91) 9.5 (3.38) 10.1 (3.61) 10.7 (3.79) <0.001
Income (euro) 12,923 (6,821) 14,088 (9,256) 14,809 (10,830) 15,351(9,848) 0.001
Blood Glucose
(mmol/l) 4.80 (0.44) 4.84 (0.43) 4.78 (0.46) 4.74 (0.41) 0.110
Insulin (mU/l) 7.35 (4.00) 7.83 (4.60) 7.20 (4.50) 7.72 (20.82) 0.920
Serum TG (mmol/l) 1.38 (0.79) 1.21 (0.58) 1.13 (0.53) 1.00 (0.46) <0.001
Serum LDL
(mmol/l) 3.61 (0.89) 3.73 (0.91) 3.68 (0.92) 3.67 (0.94) 0.599
Serum HDL
(mmol/l) 1.19 (0.29) 1.27 (0.29) 1.30 (0.31) 1.40 (0.33) <0.001
Serum LDL
(mmol/l) 3.61 (0.89) 3.73 (0.91) 3.68 (0.92) 3.67 (0.94) 0.599
27
Dietary factors
Total energy
(Kcal/d) 1891 (569) 1834 (558) 1814 (580) 1785 (501) 0.239
Fat (% E) 34.82 (6.22) 34.39 (5.85) 34.01 (6.32) 32.90 (5.93) 0.008
SAFA (% E) 15.17 (3.43) 14.69 (3.33) 14.31 (3.36) 13.55 (3.23) <0.001
MUFA (% E) 10.52 (2.61) 10.52 (2.21) 10.52 (2.59) 10.19 (2.43) 0.393
PUFA (% E) 4.72 (1.49) 4.89 (1.35) 4.89 (1.38) 4.97 (1.32) 0.324
Trans fatty acids (%
E) 0.60 (0.18) 0.59 (0.19) 0.57 (0.17) 0.53 (0.18) <0.001
Carbohydrate (% E) 44.97 (7.10) 47.69 (6.33) 46.41 (6.82) 47.09 (7.01) 0.086
Protein (% E) 16.35 (2.88) 16.77 (2.69) 18.14 (3.23) 18.19 (2.95) <0.001
Alcohol (% E) 2.53 (4.41) 2.28 (3.60) 3.23 (4.45) 3.19 (4.33) 0.061
Abbreviation: EPA, eicosapentaenoic acid; DPA, docosapentaenoic acid; DHA, docosahexanoic acid;
ALA, alpha-linolenic acid
SBP, systolic blood pressure; DBP, diastolic blood pressure; TG, triglyceride; HDL, high density
lipoprotein; Values are means (s.d.) or percentages. Mean and linear regression for continuous
variables, chi2 –test for categorical variables.
28
Table 2. Summary mean (SD) of the variables evaluated in this study and the results
according to the gender
Variables Total Women Men P
Number of subjects 892 467 425
Age (y) 61.67 (6.44) 61.84 (6.39) 61.48 (6.51) 0.501
BMI (kg/m2) 27.1 (4.05) 27.32 (4.65) 26.87 (3.25) <0.001
Physical activity (kcal/d) 189.16 (211.25) 191.88 (230.17) 186.18 (188.50) 0.533
Resistin (ng/ml) 1.92 (0.67) 1.96 (0.66) 1.88 (0.68) 0.868
Serum EPA (%) 1.66 (0.91) 1.71 (0.93) 1.59 (0.89) 0.230
Serum DPA (%) 0.78 (0.16) 0.77 (0.16) 0.78 (0.17) 0.126
Serum DHA (%) 2.78 (0.90) 2.87 (0.91) 2.67 (0.35) 0.218
EPA+ DHA + DPA (%) 5.21 (1.79) 5.36 (1.82) 5.05 (1.74) 0.267
Serum C-reactive protein (mg/l) 2.57 (4.20) 2.75 (4.55) 2.38 (3.77) 0.105
Mean systolic blood pressure (mm Hg) 135.9 (17.46) 136.9 (17.66) 134.9 (17.20) 0.489
Mean diastolic blood pressure (mm Hg) 82.0 (8.91) 81.5 (5.59) 82.5 (9.23) 0.167
Serum TG (mmol/l) 1.18 (0.61) 1.13 (0.53) 1.24 (0.69) 0.001
Serum HDL (mmol/l) 1.29 (0.31) 1.39 (0.31) 1.19 (0.31) 0.035
Serum LDL (mmol/l) 3.67 (0.91) 3.73 (0.89) 3.61 (0.94) 0.318
Total energy (kcal/d) 1831 (553.18) 1576 (424.75) 2111 (525.48) <0.001
Fat (energy %) 34.03 (6.11) 33.45 (5.93) 34.70 (6.25) 0.270
Carbohydrate (energy %) 47.29 (.83) 48.50 (6.50) 45.89 (6.95) 0.108
Protein (energy %) 17.36 (3.05) 17.49 (2.93) 17.22 (3.17) 0.270
SAFA (energy %) 14.42 (3.33) 14.21 (3.23) 14.66 (3.43) 0.742
MUFA (energy %) 10.44 (2.43) 10.17 (2.35) 10.73 (2.48) 0.789
PUFA (energy %) 4.87 (1.39) 4.80 (1.37) 4.95 (1.41) 0.343
Fish intake (g/d) 80.64 (123.71) 69.84 (113.82) 92.51 (129.29) 0.009
LDL, low density lipoprotein; SAFA, saturated fatty acids; MUFA, monounsaturated fatty acids,
PUFA, polyunsaturated fatty acids. Values are means (s.d.) or percentages.
29
Table 3. Concentration of serum resistin in serum n-3 polyunsaturated fatty acid quartiles
Serum total long chain n-3 polyunsaturated fatty acids quartile
r β P for
trend
Variables 1 (n =223) 2 (n =223) 3 (n =223) 4 (n =223)
EPA+DPA+DHA -0.12
Model 1 - 0.15 2.03 (1.94-2.11) 1.96 (1.88-2.05) 1.86 (1.78-1.95) 1.83 (1.74-1.92) 0.001
Model 2 - 0.12 1.99 (1.90-2.09) 1.97 (1.88- 2.05) 1.87 (1.78-1.96) 1.85 (1.76-1.95) 0.025
EPA -0.10
Model 1 - 0.13 1.99 (1.90-2.08) 1.97 (1.88-2.06) 1.85 (1.77-1.94) 1.87 (1.79-1.96) 0.039
Model 2 - 0.09 1.96 (1.86-2.05) 1.96 (1.87-2.05) 1.87 (1.78-1.96) 1.89 (1.80- 1.98) 0.243
DPA -0.09
Model 1 - 0.10 1.98 (1.88-2.06) 2.01 (1.92-2.10) 1.87 (1.79-1.96) 1.84 (1.75-1.92) 0.013
Model 2 - 0.07 1.94 (1.85-2.03) 2.00 (1.91-2.09) 1.89 (1.80-1.98) 1.85 (1.75-1.94) 0.097
DHA -0.14
30
Model 1 - 0.17 2.01 (1.92-2.10) 1.96 (1.87-2.04) 1.93 (1.85-2.02) 1.79 (1.70-1.88) <0.001
Model 2 - 0.14 1.98 (1.89-2.07) 1.96 (1.87-2.05) 1.94 (1.85- 2.03) 1.80 (1.7-1.90) 0.007
Abbreviation: EPA, eicosapentaenoic acid; DPA, docosapentaeboic acid; DHA, docosahexanoic acid;
Model 1 adjusted for age, gender and examination year.
Model 2 adjusted for Model 1 and physical activity, BMI, alcohol intake per week, smoking, serum TG, systolic and diastolic blood pressure,
serum LDL,
31
6 DISCUSSION
In this cross-sectional study in a healthy middle-aged population, we found that serum total long
chain n-3 PUFA (EPA+DHA+DPA), DHA and DPA concentration are inversely associated with
serum resistin concentration when adjusted for age, gender and year of examination. Only DHA
remained significantly associated with serum resistin level after additional adjustment for all
potential confounders. In contrast, serum concentration of EPA was not associated with serum
resistin concentration in our study. This suggests that fish or fish oil consumption may lead to lower
serum resistin concentration; notwithstanding, the role of potential confounders cannot be wholly
excluded.
Resistin is a cysteine-rich adipose-derived peptide hormone, which is originally named for its
resistance to insulin (Steppan et al. 2001). It has been suggested that significant level of resistin
expression predominantly occurs in macrophages, PBMCs, bone marrow, spleen and embedded in
in adipose tissue (Fain et al. 2003, Janke et al. 2002, Patel et al. 2003, Xu et al. 2006) and mature
adipocytes (Degawa-Yamauchi et al. 2003). Resistin is known as a pro-inflammatory cytokine that
seemed to be a link between obesity and T2D (Holcomb et al. 2000, Steppan et al. 2001). Also
resistin may increase the risk of arteriosclerosis by impairment of glucose and lipid metabolism
(Wang et al. 2009).
EPA and DHA are derived mainly from seafood and fish oils (Saldeen & Saldeen 2006). ALA can
be converted to EPA and DHA in human body in limited amounts. Since this conversion cannot
meet the EPA and DHA demand, the majority of DHA and EPA are obtained from the diet (Burdge
& Calder 2005, Barceló-Coblijn & Murphy 2009).
DPA is an EPA metabolite and majority of DPA circulating is from the endogenous metabolism
rather than directly from the diet (for example, fish contains limited amount of DPA) (Kaur et al.
2011). Moreover, the correlation between fish consumption and circulating DPA is much weaker
than the correlation between fish consumption and DHA and EPA (von Schacky & Weber 1985,
Arterburn et al. 2006). Hence, serum EPA and especially DHA are the better markers for evaluation
fish and fish oil consumption than DPA (Virtanen et al. 2009).
Resistin concentration and n-3 PUFA are both integrated with the health issues such as heart
disease, insulin resistance and diabetes, obesity and inflammation, which suggest that there may be
an association between them.
32
Although some animal and population-based studies experimental studies have evaluated the impact
of long chain n-3 PUFA on resistin concentration and resistin expression, to the best of our
knowledge, this is the first study evaluated association of serum n-3 PUFA concentration with
serum resistin concentration in a healthy population. It has been suggested that EPA may promote a
small reduction in expression of resistin mRNA in murine adipocytes (Haugen et al. 2005).
Moreover, in rat model of non-alcoholic steatohepatitis resistin level was decreased by 8 weeks
high fat diet with n-3 PUFA (Ye Wang 2014).
In population-based studies, in a randomized control trial among 38 patients with AMI and
successful coronary stent implantation, results indicated that n-3 PUFA therapy raised the resistin
concentration in the first month after AMI (Mizia-Stec et al. 2011). However, according to two
randomized placebo controlled trials among participants with stable coronary artery disease (CAD)
undertaking elective percutaneous coronary intervention (PCI) and women with polycystic ovary
syndrome, n-3 PUFA treatments did not alter resistin level (Mostowik et al. 2013, Oner & Muderris
2013).
The possible mechanism underlying the impact of serum n-3 PUFA on the serum resistin
concentration can be partially explained by the relationship of EPA, DHA and resistin expression
with PPARγ. PPARγ is a group of nuclear receptors mainly expressed in adipose tissue, colon and
macrophages and can regulate fatty acid storage, regulation of cellular differentiation and energy
metabolism (Fajas et al. 1997, Houseknecht et al. 1998).
It has been suggested that activation of PPARγ might be affected by serum EPA and DHA
concentration (Han et al. 2014) and PPARγ may influence the secretion of adipokines (Neschen et
al. 2006). It has been demonstrated that resistin gene expression was enhanced by overexpression of
PPARγ (Way et al. 2001, Steppan et al. 2001, Patel et al. 2003).
It has been reported that there was a strong direct association between the resistin expression and
some proinflammatory cytokines such as tumor necrosis factor, interleukin-1, and interleukin-6 in
PBMCs (Savage et al. 2001, Anderson et al. 2007, Bokarewa et al. 2005). According to review
study by (Calder 2006), higher n-3 PUFA intake could reduce production of these cytokines. So it
may be another potential mechanism underlying the association between the resistin level and n-3
PUFA.
33
Noteworthy that higher resistin expression in macrophages can decrease production of adenosine
monophosphate-activated protein kinase and it leads to reduction in fatty acid uptake and
metabolism in skeletal muscle, which can be another reason for the inverse association between the
resistin concentration and serum n-3 PUFA concentration (Palanivel & Sweeney 2005).
6.1 Strengths and limitations of the study
Use of serum long chain n-3 PUFA instead of dietary intake in our study increases accuracy of the
study owing to the fact that serum long chain n-3 PUFA is the better marker for evaluation fish and
fish oil consumption (Hodson et al. 2008). Wide examination of potential confounders and
evaluation of association between serum long-chain n-3 PUFA in healthy population for the first
time are the other strengths of our study. A limitation in our study was that our participants were
middle-age subject so we cannot refer our result to general population and it can be one of our
limitation.
34
7 CONCLUSIONS
To sum up, serum long chain n-3 PUFA and especially DHA, an objective biomarker of fish or fish
oil consumption, were inversely associated with serum resistin concentration. As resistin is known as
a potential marker for increased risk of obesity, inflammation, diabetes and heart diseases, the
beneficial effect of serum long chain n-3 PUFA on these diseases can be partially explained by their
impact on serum resistin concentration.
35
REFERENCES:
Al-Daghri N, Chetty R, McTernan PG, Al-Rubean K, Al-Attas O, Jones AF and Kumar S, Serum
resistin is associated with C-reactive protein & LDL cholesterol in type 2 diabetes and coronary
artery disease in a Saudi population. Cardiovasc.Diabetol. 2005; 4:10.
American Heart Association Nutrition Committee, Lichtenstein AH, Appel LJ, Brands M,
Carnethon M, Daniels S, Franch HA, Franklin B, Kris-Etherton P, Harris WS, Howard B, Karanja
N, Lefevre M, Rudel L, Sacks F, Van Horn L, Winston M and Wylie-Rosett J, Diet and lifestyle
recommendations revision 2006: a scientific statement from the American Heart Association
Nutrition Committee. Circulation 2006; 114:82-96.
Anderson PD, Mehta NN, Wolfe ML, Hinkle CC, Pruscino L, Comiskey LL, Tabita-Martinez J,
Sellers KF, Rickels MR and Ahima RS, Innate immunity modulates adipokines in humans. The
Journal of Clinical Endocrinology & Metabolism 2007; 92:2272-2279.
Arterburn LM, Hall EB and Oken H, Distribution, interconversion, and dose response of n-3 fatty
acids in humans. Am.J.Clin.Nutr. 2006; 83:1467S-1476S.
Babcock TA, Novak T, Ong E, Jho DH, Helton WS and Espat NJ, Modulation of
lipopolysaccharide-stimulated macrophage tumor necrosis factor-α production by ω-3 fatty acid is
associated with differential cyclooxygenase-2 protein expression and is independent of interleukin-
10. J.Surg.Res. 2002; 107:135-139.
Balkau B and Eschwege E, Insulin resistance: an independent risk factor for cardiovascular disease?
Diabetes, Obesity and Metabolism 1999; 1:23-31.
Banerjee RR, Rangwala SM, Shapiro JS, Rich AS, Rhoades B, Qi Y, Wang J, Rajala MW, Pocai A,
Scherer PE, Steppan CM, Ahima RS, Obici S, Rossetti L and Lazar MA, Regulation of fasted blood
glucose by resistin. Science 2004; 303:1195-1198.
36
Barceló-Coblijn G and Murphy EJ, Alpha-linolenic acid and its conversion to longer chain n− 3
fatty acids: Benefits for human health and a role in maintaining tissue n− 3 fatty acid levels.
Prog.Lipid Res. 2009; 48:355-374.
Bo S, Gambino R, Pagani A, Guidi S, Gentile L, Cassader M and Pagano G, Relationships between
human serum resistin, inflammatory markers and insulin resistance. Int.J.Obes. 2005; 29:1315-
1320.
Bokarewa M, Nagaev I, Dahlberg L, Smith U and Tarkowski A, Resistin, an adipokine with potent
proinflammatory properties. J.Immunol. 2005; 174:5789-5795.
Borst SE, Conover CF and Bagby GJ, Association of resistin with visceral fat and muscle insulin
resistance. Cytokine 2005; 32:39-44.
Buckley JD and Howe PRC, Anti‐ obesity effects of long‐ chain omega‐ 3 polyunsaturated fatty
acids. Obesity reviews 2009; 10:648-659.
Burdge GC and Calder PC, Conversion of alpha alpha alpha-linolenic acid to longer-chain
polyunsaturated fatty acids in human adults. Reproduction Nutrition Development 2005; 45:581-
597.
Burnett MS, Devaney JM, Adenika RJ, Lindsay R and Howard BV, Cross-sectional associations of
resistin, coronary heart disease, and insulin resistance. The Journal of Clinical Endocrinology &
Metabolism 2006; 91:64-68.
Cabrera de León A, Almeida González D, González Hernández A, Juan Alemán Sánchez J, Brito
Díaz B, Domínguez Coello S, Marcelino Rodríguez I, Gregorio Oliva García J, Aguirre Jaime A
and Rodríguez Pérez, María del Cristo, The association of resistin with coronary disease in the
general population. J.Atheroscler.Thromb. 2014; 21:273-281.
37
Calder PC, Polyunsaturated fatty acids and inflammation. Prostaglandins, Leukotrienes and
Essential Fatty Acids 2006; 75:197-202.
Caro JF, Insulin resistance in obese and non-obese Man. The Journal of Clinical Endocrinology &
Metabolism 1991; 73:691-695.
Chen C, Jiang J, Lu JM, Chai H, Wang X, Lin PH and Yao Q, Resistin decreases expression of
endothelial nitric oxide synthase through oxidative stress in human coronary artery endothelial
cells. Am.J.Physiol.Heart Circ.Physiol. 2010; 299:H193-201.
Chen J, Wang L, Boeg YS, Xia B and Wang J, Differential dimerization and association among
resistin family proteins with implications for functional specificity. J.Endocrinol. 2002; 175:499-
504.
Cunnane S, Drevon C, Harris W, Sinclair A and Spector A, Recommendations for intakes of
polyunsaturated fatty acids in healthy adults. ISSFAL Newsl 2004; 11:12-25.
De Luis D, Sagrado MG, Conde R, Aller R, Izaola O, Castrillon JP and Dueñas A, Relation of
resistin levels with cardiovascular risk factors and insulin resistance in non-diabetes obese patients.
Diabetes Res.Clin.Pract. 2009; 84:174-178.
Degawa-Yamauchi M, Bovenkerk JE, Juliar BE, Watson W, Kerr K, Jones R, Zhu Q and Considine
RV, Serum resistin (FIZZ3) protein is increased in obese humans. The Journal of Clinical
Endocrinology & Metabolism 2003; 88:5452-5455.
Deng Y and Scherer PE, Adipokines as novel biomarkers and regulators of the metabolic syndrome.
Ann.N.Y.Acad.Sci. 2010; 1212:E1-E19.
Ding Q, White SP, Ling C and Zhou W, Resistin and cardiovascular disease. Trends
Cardiovasc.Med. 2011; 21:20-27.
38
Djuricic ID, Mazic SD, Kotur-Stevuljevic JM, Djordjevic VR and Sobajic SS, Long-chain n-3
polyunsaturated fatty acid dietary recommendations are moderately efficient in optimizing their
status in healthy middle-aged subjects with low fish consumption: a cross-over study. Nutr.Res.
2014; 34:210-218.
Fain JN, Cheema PS, Bahouth SW and Hiler ML, Resistin release by human adipose tissue explants
in primary culture. Biochem.Biophys.Res.Commun. 2003; 300:674-678.
Fajas L, Auboeuf D, Raspé E, Schoonjans K, Lefebvre A, Saladin R, Najib J, Laville M, Fruchart J
and Deeb S, The organization, promoter analysis, and expression of the human PPARγ gene.
J.Biol.Chem. 1997; 272:18779-18789.
Fan H, Gu N, Liu F, Fei L, Pan X, Guo M, Chen R and Guo X, Prolonged exposure to resistin
inhibits glucose uptake in rat skeletal muscles. Acta Pharmacol.Sin. 2007; 28:410-416.
Fargnoli JL, Fung TT, Olenczuk DM, Chamberland JP, Hu FB and Mantzoros CS, Adherence to
healthy eating patterns is associated with higher circulating total and high-molecular-weight
adiponectin and lower resistin concentrations in women from the Nurses' Health Study.
Am.J.Clin.Nutr. 2008; 88:1213-1224.
Geleijnse JM, Giltay EJ, Grobbee DE, Donders AR and Kok FJ, Blood pressure response to fish oil
supplementation: metaregression analysis of randomized trials. J.Hypertens. 2002; 20:1493-1499.
Gharibeh M, Al Tawallbeh G, Abboud M, Radaideh A, Alhader A and Khabour O, Correlation of
plasma resistin with obesity and insulin resistance in type 2 diabetic patients. Diabetes Metab. 2010;
36:443-449.
Gonullu G, Kahraman H, Bedir A, Bektas A and Yücel I, Association between adiponectin, resistin,
insulin resistance, and colorectal tumors. Int.J.Colorectal Dis. 2010; 25:205-212.
39
Han W, Zhao H, Jiao B and Liu F, EPA and DHA increased PPARγ expression and deceased
integrin-linked kinase and integrin β1 expression in rat glomerular mesangial cells treated with
lipopolysaccharide. Bioscience trends 2014; 8:120-125.
Hansson GK, Robertson AL and Söderberg-Nauclér C, Inflammation and atherosclerosis.
Annu.Rev.Pathol.Mech.Dis. 2006; 1:297-329.
Harris WS and Bulchandani D, Why do omega-3 fatty acids lower serum triglycerides?
Curr.Opin.Lipidol. 2006; 17:387-393.
Haugen F, Zahid N, Dalen KT, Hollung K, Nebb HI and Drevon CA, Resistin expression in 3T3-L1
adipocytes is reduced by arachidonic acid. J.Lipid Res. 2005; 46:143-153.
He K, Liu K, Daviglus ML, Jenny NS, Mayer-Davis E, Jiang R, Steffen L, Siscovick D, Tsai M and
Herrington D, Associations of dietary long-chain n-3 polyunsaturated fatty acids and fish with
biomarkers of inflammation and endothelial activation (from the Multi-Ethnic Study of
Atherosclerosis [MESA]). Am.J.Cardiol. 2009; 103:1238-1243.
Hodson L, Skeaff CM and Fielding BA, Fatty acid composition of adipose tissue and blood in
humans and its use as a biomarker of dietary intake. Prog.Lipid Res. 2008; 47:348-380.
Hoefle G, Saely CH, Risch L, Koch L, Schmid F, Rein P, Aczél S, Berchtold S and Drexel H,
Relationship between the adipose-tissue hormone resistin and coronary artery disease. Clinica
Chimica Acta 2007; 386:1-6.
Holcomb IN, Kabakoff RC, Chan B, Baker TW, Gurney A, Henzel W, Nelson C, Lowman HB,
Wright BD, Skelton NJ, Frantz GD, Tumas DB, Peale FV,Jr, Shelton DL and Hebert CC, FIZZ1, a
novel cysteine-rich secreted protein associated with pulmonary inflammation, defines a new gene
family. EMBO J. 2000; 19:4046-4055.
40
Hou WK, Xu YX, Yu T, Zhang L, Zhang WW, Fu CL, Sun Y, Wu Q and Chen L, Adipocytokines
and breast cancer risk. Chin.Med.J.(Engl) 2007; 120:1592-1596.
Houseknecht KL, Baile CA, Matteri RL and Spurlock ME, The biology of leptin: a review.
J.Anim.Sci. 1998; 76:1405-1420.
Ichida Y, Hasegawa G, Fukui M, Obayashi H, Ohta M, Fujinami A, Ohta K, Nakano K, Yoshikawa
T and Nakamura N, Effect of atorvastatin on in vitro expression of resistin in adipocytes and
monocytes/macrophages and effect of atorvastatin treatment on serum resistin levels in patients
with type 2 diabetes. Pharmacology 2006; 76:34-39.
Jamaluddin MS, Weakley SM, Yao Q and Chen C, Resistin: functional roles and therapeutic
considerations for cardiovascular disease. Br.J.Pharmacol. 2012; 165:622-632.
Janke J, Engeli S, Gorzelniak K, Luft FC and Sharma AM, Resistin gene expression in human
adipocytes is not related to insulin resistance. Obes.Res. 2002; 10:1-5.
Järvinen R, Knekt P, Rissanen H and Reunanen A, Intake of fish and long-chain n− 3 fatty acids
and the risk of coronary heart mortality in men and women. Br.J.Nutr. 2006; 95:824-829.
Jové M, Planavila A, Cabrero À, Novell F, Ros E, Zambón D, Laguna JC and Carrera MV,
Reductions in plasma cholesterol levels after fenofibrate treatment are negatively correlated with
resistin expression in human adipose tissue. Metab.Clin.Exp. 2003; 52:351-355.
Kadowaki T, Yamauchi T, Kubota N, Hara K, Ueki K and Tobe K, Adiponectin and adiponectin
receptors in insulin resistance, diabetes, and the metabolic syndrome. J.Clin.Invest. 2006; 116:1784-
1792.
Kalogeropoulos N, Panagiotakos DB, Pitsavos C, Chrysohoou C, Rousinou G, Toutouza M and
Stefanadis C, Unsaturated fatty acids are inversely associated and n-6/n-3 ratios are positively
41
related to inflammation and coagulation markers in plasma of apparently healthy adults. Clinica
chimica acta 2010; 411:584-591.
Kalupahana NS, Claycombe KJ and Moustaid-Moussa N, (n-3) Fatty acids alleviate adipose tissue
inflammation and insulin resistance: mechanistic insights. Adv.Nutr. 2011; 2:304-316.
Kaur G, Cameron-Smith D, Garg M and Sinclair AJ, Docosapentaenoic acid (22: 5n-3): a review of
its biological effects. Prog.Lipid Res. 2011; 50:28-34.
Kawanami D, Maemura K, Takeda N, Harada T, Nojiri T, Imai Y, Manabe I, Utsunomiya K and
Nagai R, Direct reciprocal effects of resistin and adiponectin on vascular endothelial cells: a new
insight into adipocytokine–endothelial cell interactions. Biochem.Biophys.Res.Commun. 2004;
314:415-419.
Khalfoun B, Thibault F, Watier H, Bardos P and Lebranchu Y, Docosahexaenoic and
eicosapentaenoic acids inhibit in vitro human endothelial cell production of interleukin-6.
Adv.Exp.Med.Biol. 1997; 400B:589-597.
Kuzmicki M, Telejko B, Szamatowicz J, Zonenberg A, Nikolajuk A, Kretowski A and Gorska M,
High resistin and interleukin-6 levels are associated with gestational diabetes mellitus.
Gynecological endocrinology 2009; 25:258-263.
Laaksonen D, Lakka T, Lakka H, Nyyssönen K, Rissanen T, Niskanen L and Salonen J, Serum fatty
acid composition predicts development of impaired fasting glycaemia and diabetes in middle‐ aged
men. Diabetic Med. 2002; 19:456-464.
Lee JH, Chan JL, Yiannakouris N, Kontogianni M, Estrada E, Seip R, Orlova C and Mantzoros CS,
Circulating resistin levels are not associated with obesity or insulin resistance in humans and are not
regulated by fasting or leptin administration: cross-sectional and interventional studies in normal,
42
insulin-resistant, and diabetic subjects. The Journal of Clinical Endocrinology & Metabolism 2003;
88:4848-4856.
Lee SE and Kim H, Human resistin in cardiovascular disease. Journal of Smooth Muscle Research
2012; 48:27-35.
Levy JR, Davenport B, Clore JN and Stevens W, Lipid metabolism and resistin gene expression in
insulin-resistant Fischer 344 rats. Am.J.Physiol.Endocrinol.Metab. 2002; 282:E626-33.
Lim S, Koo BK, Cho SW, Kihara S, Funahashi T, Cho YM, Kim SY, Lee HK, Shimomura I and
Park KS, Association of adiponectin and resistin with cardiovascular events in Korean patients with
type 2 diabetes: the Korean atherosclerosis study (KAS): a 42-month prospective study.
Atherosclerosis 2008; 196:398-404.
Lo C, Chiu KC, Fu M, Lo R and Helton S, Fish oil decreases macrophage tumor necrosis factor
gene transcription by altering the NFκB activity. J.Surg.Res. 1999; 82:216-221.
McTernan CL, McTernan PG, Harte AL, Levick P, Barnett A and Kumar S, Resistin, central
obesity, and type 2 diabetes. The Lancet 2002; 359:46-47.
Micallef M, Munro I, Phang M and Garg M, Plasma n-3 polyunsaturated fatty acids are negatively
associated with obesity. Br.J.Nutr. 2009; 102:1370-1374.
Milan G, Granzotto M, Scarda A, Calcagno A, Pagano C, Federspil G and Vettor R, Resistin and
adiponectin expression in visceral fat of obese rats: effect of weight loss. Obes.Res. 2002; 10:1095-
1103.
Mizia-Stec K, Haberka M, Mizia M, Chmiel A, Gieszczyk K, Lasota B, Janowska J, Zahorska-
Markiewicz B and Gąsior Z, N-3 Polyunsaturated fatty acid therapy improves endothelial function
43
and affects adiponectin and resistin balance in the first month after myocardial infarction. Arch Med
Sci 2011; 7:788-795.
Moore C, Sanz-Rosa D and Emerson M, Distinct role and location of the endothelial isoform of
nitric oxide synthase in regulating platelet aggregation in males and females in vivo.
Eur.J.Pharmacol. 2011; 651:152-158.
Mora S and Pessin JE, An adipocentric view of signaling and intracellular trafficking.
Diabetes.Metab.Res. 2002; 18:345-356.
Morrison RF and Farmer SR, Hormonal signaling and transcriptional control of adipocyte
differentiation. J.Nutr. 2000; 130:3116S-3121S.
Mostowik M, Gajos G, Zalewski J, Nessler J and Undas A, Omega-3 polyunsaturated fatty acids
increase plasma adiponectin to leptin ratio in stable coronary artery disease. Cardiovascular Drugs
and Therapy 2013; 27:289-295.
Mottillo S, Filion KB, Genest J, Joseph L, Pilote L, Poirier P, Rinfret S, Schiffrin EL and Eisenberg
MJ, The metabolic syndrome and cardiovascular risk: a systematic review and meta-analysis.
J.Am.Coll.Cardiol. 2010; 56:1113-1132.
Mozaffarian D, Does alpha-linolenic acid intake reduce the risk of coronary heart disease? A review
of the evidence. Altern.Ther.Health Med. 2005; 11:24.
Mozaffarian D and Wu JH, Omega-3 fatty acids and cardiovascular disease: effects on risk factors,
molecular pathways, and clinical events. J.Am.Coll.Cardiol. 2011; 58:2047-2067.
Muramatsu T, Yatsuya H, Toyoshima H, Sasaki S, Li Y, Otsuka R, Wada K, Hotta Y, Mitsuhashi H
and Matsushita K, Higher dietary intake of alpha-linolenic acid is associated with lower insulin
resistance in middle-aged Japanese. Prev.Med. 2010; 50:272-276.
44
Murohara T, Asahara T, Silver M, Bauters C, Masuda H, Kalka C, Kearney M, Chen D, Symes JF,
Fishman MC, Huang PL and Isner JM, Nitric oxide synthase modulates angiogenesis in response to
tissue ischemia. J.Clin.Invest. 1998; 101:2567-2578.
Muse ED, Obici S, Bhanot S, Monia BP, McKay RA, Rajala MW, Scherer PE and Rossetti L, Role
of resistin in diet-induced hepatic insulin resistance. J.Clin.Invest. 2004; 114:232-239.
Nakajima TE, Yamada Y, Hamano T, Furuta K, Matsuda T, Fujita S, Kato K, Hamaguchi T and
Shimada Y, Adipocytokines as new promising markers of colorectal tumors: adiponectin for
colorectal adenoma, and resistin and visfatin for colorectal cancer. Cancer science 2010; 101:1286-
1291.
Neschen S, Morino K, Rossbacher JC, Pongratz RL, Cline GW, Sono S, Gillum M and Shulman
GI, Fish oil regulates adiponectin secretion by a peroxisome proliferator-activated receptor-gamma-
dependent mechanism in mice. Diabetes 2006; 55:924-928.
Nogueiras R, Gualillo O, Caminos JE, Garcı T, Casanueva FF and Diéguez C, Resistin is expressed
in different rat tissues and is regulated in a tissue-and gender-specific manner. FEBS Lett. 2003;
548:21-27.
Norata GD, Ongari M, Garlaschelli K, Raselli S, Grigore L and Catapano AL, Plasma resistin levels
correlate with determinants of the metabolic syndrome. Eur.J.Endocrinol. 2007; 156:279-284.
Novak TE, Babcock TA, Jho DH, Helton WS and Espat NJ, NF-kappa B inhibition by omega -3
fatty acids modulates LPS-stimulated macrophage TNF-alpha transcription. Am.J.Physiol.Lung
Cell.Mol.Physiol. 2003; 284:L84-9.
45
Ohmori R, Momiyama Y, Kato R, Taniguchi H, Ogura M, Ayaori M, Nakamura H and Ohsuzu F,
Associations between serum resistin levels and insulin resistance, inflammation, and coronary
artery disease. J.Am.Coll.Cardiol. 2005; 46:379-380.
Oner G and Muderris I, Efficacy of omega-3 in the treatment of polycystic ovary syndrome. Journal
of Obstetrics & Gynaecology 2013; 33:289-291.
Otero M, Lago R, Gomez R, Lago F, Dieguez C, Gomez-Reino JJ and Gualillo O, Changes in
plasma levels of fat-derived hormones adiponectin, leptin, resistin and visfatin in patients with
rheumatoid arthritis. Ann.Rheum.Dis. 2006; 65:1198-1201.
Palanivel R and Sweeney G, Regulation of fatty acid uptake and metabolism in L6 skeletal muscle
cells by resistin. FEBS Lett. 2005; 579:5049-5054.
Palmer RM, Ferrige A and Moncada S, Nitric oxide release accounts for the biological activity of
endothelium-derived relaxing factor. 1987; .
Patel L, Buckels AC, Kinghorn IJ, Murdock PR, Holbrook JD, Plumpton C, Macphee CH and
Smith SA, Resistin is expressed in human macrophages and directly regulated by PPARγ activators.
Biochem.Biophys.Res.Commun. 2003; 300:472-476.
Peoples GE, McLennan PL, Howe PR and Groeller H, Fish oil reduces heart rate and oxygen
consumption during exercise. J.Cardiovasc.Pharmacol. 2008; 52:540-547.
Pepe S and McLennan PL, Cardiac membrane fatty acid composition modulates myocardial oxygen
consumption and postischemic recovery of contractile function. Circulation 2002; 105:2303-2308.
Pfutzner A, Langenfeld M, Kunt T, Lobig M and Forst T, Evaluation of human resistin assays with
serum from patients with type 2 diabetes and different degrees of insulin resistance. Clin.Lab. 2003;
49:571-576.
46
Pilz S, Weihrauch G, Seelhorst U, Wellnitz B, Winkelmann BR, Boehm BO and März W,
Implications of resistin plasma levels in subjects undergoing coronary angiography.
Clin.Endocrinol.(Oxf) 2007; 66:380-386.
Pischon T, Hankinson SE, Hotamisligil GS, Rifai N, Willett WC and Rimm EB, Habitual dietary
intake of n-3 and n-6 fatty acids in relation to inflammatory markers among US men and women.
Circulation 2003; 108:155-160.
Rajala MW, Lin Y, Ranalletta M, Yang XM, Qian H, Gingerich R, Barzilai N and Scherer PE, Cell
type-specific expression and coregulation of murine resistin and resistin-like molecule-α in adipose
tissue. Molecular Endocrinology 2002; 16:1920-1930.
Rangwala SM, Rich AS, Rhoades B, Shapiro JS, Obici S, Rossetti L and Lazar MA, Abnormal
glucose homeostasis due to chronic hyperresistinemia. Diabetes 2004; 53:1937-1941.
Rea R and Donnelly R, Effects of metformin and oleic acid on adipocyte expression of resistin.
Diabetes, Obesity and Metabolism 2006; 8:105-109.
Reilly MP, Lehrke M, Wolfe ML, Rohatgi A, Lazar MA and Rader DJ, Resistin is an inflammatory
marker of atherosclerosis in humans. Circulation 2005; 111:932-939.
Reinders I, Virtanen J, Brouwer I and Tuomainen T, Association of serum n-3 polyunsaturated fatty
acids with C-reactive protein in men. Eur.J.Clin.Nutr. 2012; 66:736-741.
Rissanen T, Voutilainen S, Nyyssonen K, Lakka TA and Salonen JT, Fish oil-derived fatty acids,
docosahexaenoic acid and docosapentaenoic acid, and the risk of acute coronary events: the Kuopio
ischaemic heart disease risk factor study. Circulation 2000; 102:2677-2679.
Russo GL, Dietary n− 6 and n− 3 polyunsaturated fatty acids: from biochemistry to clinical
implications in cardiovascular prevention. Biochem.Pharmacol. 2009; 77:937-946.
47
Ruxton C, Reed SC, Simpson M and Millington K, The health benefits of omega‐ 3
polyunsaturated fatty acids: a review of the evidence. Journal of Human Nutrition and Dietetics
2004; 17:449-459.
Salageanu A, Tucureanu C, Lerescu L, Caras I, Pitica R, Gangura G, Costea R and Neagu S, Serum
levels of adipokines resistin and leptin in patients with colon cancer. J.Med.Life. 2010; 3:416-420.
Saldeen P and Saldeen T, Omega-3 Fatty acids: structure, function, and relation to the metabolic
syndrome, infertility, and pregnancy. Metabolic syndrome and related disorders 2006; 4:138-148.
Salonen JT, Is there a continuing need for longitudinal epidemiologic research? The Kuopio
Ischaemic Heart Disease Risk Factor Study. Ann.Clin.Res. 1988; 20:46-50.
Salonen JT, Nyyssonen K, Korpela H, Tuomilehto J, Seppanen R and Salonen R, High stored iron
levels are associated with excess risk of myocardial infarction in eastern Finnish men. Circulation
1992; 86:803-811.
Sato N, Kobayashi K, Inoguchi T, Sonoda N, Imamura M, Sekiguchi N, Nakashima N and Nawata
H, Adenovirus-mediated high expression of resistin causes dyslipidemia in mice. Endocrinology
2005; 146:273-279.
Savage DB, Sewter CP, Klenk ES, Segal DG, Vidal-Puig A, Considine RV and O'Rahilly S,
Resistin / Fizz3 expression in relation to obesity and peroxisome proliferator-activated receptor-
gamma action in humans. Diabetes 2001; 50:2199-2202.
Senolt L, Housa D, Vernerova Z, Jirasek T, Svobodova R, Veigl D, Anderlova K, Muller-Ladner U,
Pavelka K and Haluzik M, Resistin in rheumatoid arthritis synovial tissue, synovial fluid and serum.
Ann.Rheum.Dis. 2007; 66:458-463.
48
Seto SW, Lam TY, Or PMY, Lee WYW, Au ALS, Poon CCW, Li RWS, Chan SW, Yeung JHK
and Leung GPH, Folic acid consumption reduces resistin level and restores blunted acetylcholine-
induced aortic relaxation in obese/diabetic mice. J.Nutr.Biochem. 2010; 21:872-880.
Shetty GK, Economides PA, Horton ES, Mantzoros CS and Veves A, Circulating adiponectin and
resistin levels in relation to metabolic factors, inflammatory markers, and vascular reactivity in
diabetic patients and subjects at risk for diabetes. Diabetes Care 2004; 27:2450-2457.
Shulman GI, Cellular mechanisms of insulin resistance. J.Clin.Invest. 2000; 106:171-176.
Shyu K, Chua S, Wang B and Kuan P, Mechanism of inhibitory effect of atorvastatin on resistin
expression induced by tumor necrosis factor-alpha in macrophages. J.Biomed.Sci. 2009; 16:50.
Silha JV, Krsek M, Skrha JV, Sucharda P, Nyomba BL and Murphy LJ, Plasma resistin,
adiponectin and leptin levels in lean and obese subjects: correlations with insulin resistance.
Eur.J.Endocrinol. 2003; 149:331-335.
Silswal N, Singh AK, Aruna B, Mukhopadhyay S, Ghosh S and Ehtesham NZ, Human resistin
stimulates the pro-inflammatory cytokines TNF-α and IL-12 in macrophages by NF-κB-dependent
pathway. Biochem.Biophys.Res.Commun. 2005; 334:1092-1101.
Skulas-Ray AC, Kris-Etherton PM, Harris WS, Vanden Heuvel JP, Wagner PR and West SG,
Dose-response effects of omega-3 fatty acids on triglycerides, inflammation, and endothelial
function in healthy persons with moderate hypertriglyceridemia. Am.J.Clin.Nutr. 2011; 93:243-252.
Stejskal D, Adamovská S, Bartek J, Juráková R and Prošková J, Resistin-concentrations in persons
with type 2 diabetes mellitus and in individuals with acute inflammatory disease. Biomedical Papers
2003; 147:63-69.
49
Steppan CM, Bailey ST, Bhat S, Brown EJ, Banerjee RR, Wright CM, Patel HR, Ahima RS and
Lazar MA, The hormone resistin links obesity to diabetes. Nature 2001; 409:307-312.
Steppan CM, Brown EJ, Wright CM, Bhat S, Banerjee RR, Dai CY, Enders GH, Silberg DG, Wen
X, Wu GD and Lazar MA, A family of tissue-specific resistin-like molecules.
Proc.Natl.Acad.Sci.U.S.A. 2001; 98:502-506.
Tai CC and Ding ST, N-3 polyunsaturated fatty acids regulate lipid metabolism through several
inflammation mediators: mechanisms and implications for obesity prevention. J.Nutr.Biochem.
2010; 21:357-363.
Timar O, Sestier F and Levy E, Metabolic syndrome X: a review. Can.J.Cardiol. 2000; 16:779-789.
Tsiotra PC, Tsigos C, Anastasiou E, Yfanti E, Boutati E, Souvatzoglou E, Kyrou I and Raptis SA,
Peripheral mononuclear cell resistin mRNA expression is increased in type 2 diabetic women.
Mediators Inflamm. 2008; 2008:892864.
Tuttolomondo A, La Placa S, Di Raimondo D, Bellia C, Caruso A, Lo Sasso B, Guercio G, Diana
G, Ciaccio M, Licata G and Pinto A, Adiponectin, resistin and IL-6 plasma levels in subjects with
diabetic foot and possible correlations with clinical variables and cardiovascular co-morbidity.
Cardiovasc.Diabetol. 2010; 9:50-2840-9-50.
Utzschneider K, Carr D, Tong J, Wallace T, Hull R, Zraika S, Xiao Q, Mistry J, Retzlaff B and
Knopp R, Resistin is not associated with insulin sensitivity or the metabolic syndrome in humans.
Diabetologia 2005; 48:2330-2333.
Verma S, Li SH, Wang CH, Fedak PW, Li RK, Weisel RD and Mickle DA, Resistin promotes
endothelial cell activation: further evidence of adipokine-endothelial interaction. Circulation 2003;
108:736-740.
50
Vilarrasa N, Vendrell J, Maravall J, Broch M, Estepa A, Megia A, Soler J, Simón I, Richart C and
Gómez JM, Distribution and determinants of adiponectin, resistin and ghrelin in a randomly
selected healthy population. Clin.Endocrinol.(Oxf) 2005; 63:329-335.
Virtanen JK, Laukkanen JA, Mursu J, Voutilainen S and Tuomainen T, Serum long-chain n-3
polyunsaturated fatty acids, mercury, and risk of sudden cardiac death in men: a prospective
population-based study. PloS one 2012; 7:e41046.
Virtanen JK, Mursu J, Voutilainen S, Uusitupa M and Tuomainen TP, Serum omega-3
polyunsaturated fatty acids and risk of incident type 2 diabetes in men: the Kuopio Ischemic Heart
Disease Risk Factor study. Diabetes Care 2014; 37:189-196.
Virtanen JK, Voutilainen S, Rissanen TH, Mursu J, Tuomainen TP, Korhonen MJ, Valkonen VP,
Seppanen K, Laukkanen JA and Salonen JT, Mercury, fish oils, and risk of acute coronary events
and cardiovascular disease, coronary heart disease, and all-cause mortality in men in eastern
Finland. Arterioscler.Thromb.Vasc.Biol. 2005; 25:228-233.
von Schacky C and Weber PC, Metabolism and effects on platelet function of the purified
eicosapentaenoic and docosahexaenoic acids in humans. J.Clin.Invest. 1985; 76:2446-2450.
Voutilainen S, Rissanen TH, Virtanen J, Lakka TA, Salonen JT and Kuopio Ischemic Heart Disease
Risk Factor Study, Low dietary folate intake is associated with an excess incidence of acute
coronary events: The Kuopio Ischemic Heart Disease Risk Factor Study. Circulation 2001;
103:2674-2680.
Wallin A, Di Giuseppe D, Orsini N, Patel PS, Forouhi NG and Wolk A, Fish consumption, dietary
long-chain n-3 fatty acids, and risk of type 2 diabetes: systematic review and meta-analysis of
prospective studies. Diabetes Care 2012; 35:918-929.
51
Wang H, Chen D, Cao J, He Z, Zhu B and Long M, High serum resistin level may be an indicator
of the severity of coronary disease in acute coronary syndrome. Chinese Medical Sciences Journal
2009; 24:161-166.
Wang C, Chung M, Lichtenstein A, Balk E, Kupelnick B, DeVine D, Lawrence A and Lau J,
Effects of omega-3 fatty acids on cardiovascular disease. Evid Rep.Technol.Assess.(Summ) 2004;
(94):1-8.
Way JM, Gorgun CZ, Tong Q, Uysal KT, Brown KK, Harrington WW, Oliver WR,Jr, Willson TM,
Kliewer SA and Hotamisligil GS, Adipose tissue resistin expression is severely suppressed in
obesity and stimulated by peroxisome proliferator-activated receptor gamma agonists. J.Biol.Chem.
2001; 276:25651-25653.
Wei-kai H, Yu-xin X, Ting Y, Li Z, Wen-wen Z, Chun-li F, Yu S, Qing W and Li C,
Adipocytokines and breast cancer risk. Chin.Med.J. 2007; 120:1592-1596.
Weikert C, Westphal S, Berger K, Dierkes J, Mohlig M, Spranger J, Rimm EB, Willich SN, Boeing
H and Pischon T, Plasma resistin levels and risk of myocardial infarction and ischemic stroke. The
Journal of Clinical Endocrinology & Metabolism 2008; 93:2647-2653.
World health organization , Chronic diseases and their common risk factors [Homepage of WHO],
[Online]. Available: www.who.int/respiratory/asthma/causes/en/index.html. [11.13, 2015].
Wu JH, Micha R, Imamura F, Pan A, Biggs ML, Ajaz O, Djousse L, B Hu F and Mozaffarian D,
Omega-3 fatty acids and incident type 2 diabetes: a systematic review and meta-analysis. Br.J.Nutr.
2012; 107:S214-S227.
Xu W, Yu L, Zhou W and Luo M, Resistin increases lipid accumulation and CD36 expression in
human macrophages. Biochem.Biophys.Res.Commun. 2006; 351:376-382.
52
Yannakoulia M, Yiannakouris N, Bluher S, Matalas A, Klimis-Zacas D and Mantzoros CS, Body
fat mass and macronutrient intake in relation to circulating soluble leptin receptor, free leptin index,
adiponectin, and resistin concentrations in healthy humans. The Journal of Clinical Endocrinology
& Metabolism 2003; 88:1730-1736.
Ye Wang M, Regulation of adipokines by polyunsaturated fatty acids in a rat model of non-
alcoholic steatohepatitis. Archives of Iranian medicine 2014; 17:563.
Ye Wang M, Regulation of adipokines by polyunsaturated fatty acids in a rat model of non-
alcoholic steatohepatitis. Archives of Iranian medicine 2014; 17:563.
Zeng G and Quon MJ, Insulin-stimulated production of nitric oxide is inhibited by wortmannin.
Direct measurement in vascular endothelial cells. J.Clin.Invest. 1996; 98:894-898.
Zheng J, Huang T, Yang J, Fu Y and Li D, Marine N-3 polyunsaturated fatty acids are inversely
associated with risk of type 2 diabetes in Asians: a systematic review and meta-analysis. 2012;
7:e44525.