Obesity, obstructive sleep apnoea
and metabolic syndrome
The fatal association!!
Ravindran
Chetambath
Abstract:
Obesity
is the most common health risk for individuals of all age groups across the
globe. Obstructive sleep apnoea (OSA) is now recognized as a major health
problem in developed countries. Prevalence of OSA is undoubtedly rising given
the epidemic of obesity. Recent data also suggest that OSA is associated with
the metabolic syndrome. Pathophysiological
triggers of intermittent hypoxia and sleep fragmentation in OSA is responsible
for cardiometabolic dysfunction. The potential mechanisms of OSA-obesity-metabolic
syndrome interaction involve sympathetic activation, oxidative stress,
inflammation and neurohumoral changes. In spite of support for an independent
role of OSA in the contribution towards metabolic dysfunction, obesity plays a
determinant role in initiating both these conditions.
Keywords:
obesity, cardiometabolic dysfunction, metabolic syndrome.
Introduction:
The
obesity epidemic and its impact on the prevalence of both metabolic syndrome
and OSA are well recognized. OSA is widely prevalent in patients with obesity,
diabetes, and hypertension. Clustering of cardiovascular risk factors (metabolic
syndrome or Syndrome X) was recognized as early as 1920s and is currently
thought to be linked to obesity and OSA. Given the obesity epidemic at hand, the
prevalence of both metabolic syndrome and OSA are rising. In patients with
established coronary artery disease, treatment of OSA may confer long term
cardiovascular benefits. Our understanding of the relative importance and
interactions of these cardiovascular disease mechanisms and risk factors in
patients with OSA may have direct implications for the development of targeted
preventive and therapeutic strategies1. The results of various
studies have undisputedly shown that appropriate treatment of OSA with
Continuous Positive Airway Pressure (CPAP) therapy significantly reduces blood
pressure2 and other cardiovascular complications like CAD,
arrhythmias and stroke. Treatment of OSA also improves the altered metabolic
physiology in patients with syndrome X. Further a new syndrome, syndrome-Z was recognized
to highlight the dreadful combination of syndrome-X and OSA as a risk factor
for coronary artery disease (CAD).
Obesity
Obesity
is a complex disease involving an excessive amount of body fat. Obesity is a
risk factor for diabetes, hypertension, obstructive sleep apnoea and
cardiovascular events3 and increases mortality, especially in
middle-aged adults. In adults obesity is diagnosed when the body mass index (BMI)
is 30 Kg/M2 or more. Obesity rates are also increasing in children4.
Since obese children tend to become obese adults, the cardio-metabolic disease
associated with obesity could begin in childhood5.
Individuals
with high body mass index (BMI) are classified as overweight when BMI is
between 25-29.9, class-1 obesity when BMI is between 30-34.9, class-II Obesity
when BMI is between 35-40 and class-III obesity when BMI is more than 40.
Obesity
is characterized by the expansion of white adipose tissue, as a result of
increased size (hypertrophy), and, additionally, by an increased number of
adipocytes (hyperplasia). Adipose tissue is a central player in metabolic
regulation through the production and release of multiple adipokines6.
Moreover, adipocytes and inflammatory cells, such as macrophages, show a high degree
of interaction in obesity7.
The
localization of excess white adipose tissue in the body carries relevant
metabolic consequences. Increased visceral fat mass is associated with more
severe health effects compared to peripheral obesity, which is characterized by
predominant accumulation of subcutaneous fat. The expansion of visceral fat
increases the risk of developing insulin resistance (IR), type-II diabetes,
atherosclerosis, OSA, steatohepatitis, and cardio- and cerebrovascular disease.
Changes in body weight are known to affect OSA severity. Most adult patients
with OSA have central obesity and increased visceral fat8, the
latter being associated with neck adiposity, increased upper airway fat and
metabolic abnormalities9.
The
adverse consequences of obesity may be attributed in part to comorbidities, but
results from several observational studies detailed by the Expert Panel on the
Identification, Evaluation, and Treatment of Overweight Adults, show that
obesity on its own is associated with increased cardiovascular morbidity and
mortality and greater all-cause mortality10. For a person with a BMI
of 25-28.9 kg/m2, the relative risk for coronary heart disease is
1.72. The risk progressively increases with an increasing BMI; with BMIs
greater than 33 kg/m2, the relative risk is 3.44. Similar trends
have been demonstrated in the relationship between obesity and stroke or
chronic heart failure. For persons with severe obesity (BMI
≥40), life expectancy is reduced by as much as 20 years in men and by about 5
years in women.
Many
clinical and biochemical factors associated with increased cardiovascular risk
(i.e. dyslipidaemia, arterial hypertension, hyperglycaemia, hyperuricaemia and
microalbuminuria) are often present in visceral (or central) obesity. The term
“adiposopathy” has been proposed to indicate the strong link between visceral
fat and obesity-associated metabolic abnormalities11.
Treatment
of obesity starts with comprehensive lifestyle management which includes diet,
physical activity and behavior modification. In addition, several surgical
options are also available for morbid obesity.
Obstructive Sleep Apnoea
The
spectrum of breathing disorder ranges from intermittent, partial obstruction of
the airway without sleep disturbance (snoring) to frequent arousals associated
with hypoxemia leading to sleep fragmentation and daytime sleepiness. There
will be recurrent episodes of cessation of respiration (apneas), decrements in
airflow (hypopneas), or respiratory event related arousals (RERAS). This
spectrum ranges from snoring, upper airway resistance syndrome (UARS), sleep
hypopnea syndrome, to obstructive sleep apnea syndrome (OSAS) of which OSAS is
the most severe form having considerable impact on the individual’s health.
Obstructive
sleep apnea affects approximately 10% of middle aged men and 5% of women and is
therefore a common condition. The prevalence of clinically significant
obstructive sleep apnea (OSA) in middle-aged adults is estimated to be 2–5% in
males and 2% in females. However 82% of men and 93% of women suffering from
moderate to severe sleep apnea have not been clinically detected or treated. There
are many serious consequences for undiagnosed and untreated OSA. The quality of
life of these patients is seriously impaired mainly due to their excessive
daytime sleepiness. These patients also suffer from psychological impairment
such as cognitive dysfunction, decreased vigilance, disturbed concentration and
memory, increased mental stress, fatigue, general mood disorders, and male
sexual dysfunction12. There is an estimated three- to seven fold
greater prevalence of motor vehicle accidents involving drivers with OSA13.
Most of these accidents are attributed to poor vigilance and falling asleep
while driving.
The
cardiovascular consequences of untreated OSA are coronary artery disease,
congestive heart failure, myocardial infarction, stroke, systemic hypertension,
and pulmonary hypertension14. The association between hypertension
and OSA is well established. It is shown that hypertension associated with
untreated OSA is often refractory and that a high prevalence of OSA has been
observed in men with therapy-resistant hypertension15. Patients with OSA have many features in
common with those with syndrome X, including systemic hypertension which is
commonly reported. Obstructive sleep apnea (OSA) has been linked to increased
cardiovascular morbidity and mortality16 and
can be considered an independent risk factor for CAD. Pathophysiologic
mechanisms that are present in patients with OSA, including sympathetic
activation, endothelial dysfunction, oxidative stress, systemic inflammation, hypercoagulability,
hyperleptinemia, and insulin resistance, may influence the development and
progression of cardiac and vascular pathology. These mechanisms are found to be
common for both metabolic syndrome and OSA.
Metabolic Syndrome (Syndrome-X)
Metabolic
Syndrome” or “Syndrome X” constitutes one of the most important risk factors
for CAD. The diagnosis of metabolic syndrome is made when an individual has
three of the following five characteristics: increased waist circumference,
high blood pressure, elevated fasting glucose, elevated triglycerides, and
decreased high-density lipoprotein (HDL) cholesterol. The criteria proposed by
the Third Report of the National Cholesterol Education Program (NCEP) Expert
Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in
Adults (Adult Treatment Panel III) are the most current and widely used.
According to the ATP III criteria, the metabolic syndrome is identified by the
presence of three or more of these components:
•
Central obesity as measured by waist circumference: In men greater than 40
inches and in women greater than 35 inches
•
Fasting blood triglycerides greater than or equal to 150 mg/dL
•
Blood HDL cholesterol: In men less than 40 mg/dL and in women less than 50
mg/dL
•
Blood pressure greater than or equal to 130/85 mmHg
•
Fasting blood glucose greater than or equal to 110 mg/dL
Other
important features of the metabolic syndrome include microalbuminuria,
hypercoagulability, increased inflammation, endothelial dysfunction, poor
cardiorespiratory function and sympathetic activation. Cardiovascular metabolic
syndrome X is becoming very common in India.
Coughlin
and colleagues17 performed a
cross-sectional study of 61 otherwise healthy subjects with OSA and 29 subjects
without OSA. To mitigate confounding due to obesity, they also matched 34 of
the OSA patients by body-mass index (BMI) to the 29 controls. Their results
suggest that the prevalence of metabolic syndrome is about 40% greater in
patients with OSA. Also, proper management of syndrome X reduces the apnea
hypopnea index in patients with co-existent OSA thus underlying the importance
of simultaneous management of both the conditions
Syndrome-Z
It
has even been suggested that the metabolic syndrome (Syndrome X) may co-exist
with OSA (Syndrome Z)18. Syndrome Z was introduced in medical
practice by Ian Wilcox in 199618. Wilcox attached the respiratory
partner for CAD risk, OSA, to syndrome X (Table-1). The importance lies in the
fact that the medical fraternity is now challenging CAD by risk factor
modification, but one of the major culprits, OSA, remains largely unnoticed and
under treated.
|
Components of syndrome Z
|
|
1
2
3
4
5
6
|
Hypertension
Glucose
intolerance
Low
serum high-density lipoprotein (HDL)-cholesterol
Elevated
serum triglyceride
Abdominal
obesity
OSA
|
Table-1: Components of syndrome Z
Interaction
It
is conceivable that OSA and obesity may interact and potentiate their
detrimental consequences. OSA-associated metabolic abnormalities have been
reproduced in animal models exposed to a pattern of intermittent hypoxia
similar to that found in humans with sleep disordered breathing19.
However, hypoxia of adipocytes could play an important role in the metabolic
disturbances associated with obesity20. In addition, OSA and obesity
share common mechanisms. Nocturnal ischemia in these patients is probably a
result of simultaneous oxygen desaturation, increased sympathetic activity,
tachycardia and increased systemic vascular resistance, a prothrombotic state,
and any underlying subclinical coronary artery disease. Experimental studies
support the theory that there might be a cause-and-effect relationship between
OSA and atherosclerosis. OSA and metabolic syndrome share the common
pathophysiologic mechanism increasing CAD risk.
Human
obesity is usually associated with high plasma leptin and attenuated leptin
signalling (leptin resistance)21. Leptin might be involved in the
pathogenesis of hypoventilation disorders and its transcription is activated by
exposure to continuous severe hypoxia in vitro22. In recent years,
the role of leptin in immune function and inflammation has been increasingly
studied, and some data indicate that leptin could contribute to the
pathogenesis of atherosclerotic lesions by promoting inflammation23.
Adiponectin exerts an insulin-sensitizing action, and its levels are decreased
in obesity24. Adiponectin has anti-atherogenic and anti-inflammatory
properties, and its circulating levels are lower than normal in patients with
type-II diabetes, metabolic syndrome (MetS), hypertension and coronary artery
disease25. The protective role of adiponectin and its modulation by
hypoxia suggest that it may be a useful marker of metabolic dysfunction in
obesity and OSA.
Although
inflammation contributes to the development of IR and MetS26, the
sequence of events leading to the inflammatory response in the adipose tissue
is incompletely defined. An increased adipocyte size may be an important
signal, through dys-regulation of insulin signaling at the level of insulin
receptor substrates (IRS). Phosphorylation of IRS-1, an early event in insulin signaling,
is decreased in large adipocytes27.
Independent
association between OSA and metabolic syndrome were assessed in two
case-controlled studies on Caucasian men and reported a 6-9 fold cardiovascular
risk in these subjects28. In a community-based study among Chinese
subjects29, a positive correlation was demonstrated between AHI and
the number of metabolic components. There are other studies also demonstrating
association between sleep-disordered breathing and metabolic factors within the
metabolic syndrome, independent of obesity.
OSA and Obesity
Obesity
is considered as an important risk factor for the development of OSA30.
It also plays an important role in the pathogenesis of the metabolic syndrome31.
Positive correlations between the severity of OSA and the degree of obesity in
various ethnic populations have been established through epidemiologic studies32.
Waist-to-hip ratio, waist circumference, and neck circumference are found to be
better predictors of OSA severity than BMI33. How adiposity and its
distribution predispose to development of OSA is not clearly described. Greater
mechanical load imposed by central obesity on the upper and lower-respiratory
tracts and obesity-related inflammation may predispose to pharyngeal collapse30.
On the other hand OSA itself may modulate the secretion of hormones and other
biological mediators which in turn lead to obesity.
It
is proved through longitudinal cohort study that a 10% weight loss was associated
with a 26% decrease in AHI34. It is also proved that weight loss
could result in complete resolution of OSA in the mild-to-moderate AHI range35.
Weight reduction is best achieved by reducing energy intake through dietary
modifications and enhancing energy expenditure through physical activity.
Bariatric surgery has been used and shown to improve the metabolic profile as
well as sleep-disordered breathing in morbid obese individuals.
OSA and Insulin Resistance
Insulin
resistance and glucose intolerance are two essential components of metabolic
syndrome. There are evidences of positive and independent association between
OSA and insulin resistance or glucose intolerance36. Subjects with
OSA may have multiple factors leading to insulin resistance and glucose
intolerance. Central obesity itself leads to insulin resistance through
increased lipolysis and fatty acid availability37. Insulin
resistance was observed not only in obese, but also in the non-obese patients
suffering from OSA38.
In
the Wisconsin Sleep Cohort study conducted on 1300 subjects, an independent
relationship between OSA and diabetes was not established even after 4-year
follow-up, despite a higher prevalence of diabetes in OSA subjects39.
Intravenous glucose-tolerance test did not show impaired insulin sensitivity or
impaired insulin secretion in diabetic with OSA.
OSA and Dyslipidemia
Obesity
is associated with increased plasma lipids, and adipose tissue distribution40.
The American Sleep Heart Health Study reported that HDL-cholesterol levels were
inversely related to AHI levels, independent of obesity. Similarly
triglycerides levels were positively correlated with AHI in younger men and
women, but not in elderly41. Many patients attending the sleep
clinic show a higher prevalence of dyslipidemia compared with those without
OSA, after adjustment for BMI. Significant association between high AHI and
presence of CAD and dyslipidemia was shown by case-controlled studies. Even though
few observational studies reported that treatment with nasal CPAP improved
lipid parameters; it was not validated through randomized, controlled studies.
It is proved that low-density lipoprotein is more injurious to endothelial
cells and underlying smooth muscle cells, and is thus more atherogenic.
Pathogenesis of cardio-metabolic dysfunction
in OSA
Intermittent
hypoxemia with re-oxygenation and sleep fragmentation, may lead to multiple
events altering cellular metabolism.
Obstructive sleep apnea is considered to be a chronic stress state with
activation of neuro-humoral pathways that participate in metabolic regulation.
Obese subjects have increased sympathetic activity, and in subjects with OSA
there is further elevation of sympathetic activity more than what is attributed
to obesity42. Surges of sympathetic over activity, causes transient
increases in systemic blood pressure. Sympatho-adrenal activation persists in
the day, as evidenced by sympathetic nerve activity and catecholamine output43.
This sympathetic activation may modulate many other mechanisms or mediators,
including the angiotensin-renin system, insulin and adiponectin, which may all
contribute to cardio-metabolic dysfunction in OSA43. Sympathetic
over activity in OSA, is an important factor in the pathogenesis of
hypertension44. At the same time its role in glucose and lipid
metabolism is less clear. Changes in the duration or quality of sleep may
affect neuroendocrine and metabolic function45. OSA subjects have
been reported to have altered pattern of cortisol secretion46.
Obstructive sleep apnea may also modulate hormones that regulate energy
metabolism. These patients have lower leptin levels, in proportion to weight
gain47.
The
recurrent intermittent hypoxia with reoxygenation, may result in generation of
oxidative stress, which itself lead to cardio-metabolic dysfunction48.
Obesity and the metabolic syndrome have been associated with this enhanced
oxidative stress48. It is proved in animal models that intermittent
hypoxia induces various metabolic alterations, such as insulin resistance and dyslipidemia49.
These patients have increased levels of various oxidative stress markers, such
as nitric oxide, 8-isoprostane, reactive oxygen species, and lipid
peroxidation.
It
is believed that inflammation plays a pivotal role in the pathogenesis of endothelial
dysfunction, insulin resistance and lipid peroxidation. Inflammation is a key
component in OSA. Inflammation in OSA, independent of obesity, is evidenced by
activation of neutrophils, lymphocytes, monocytes, and platelets; activation of
NF-κB and increased circulating levels of pro-inflammatory cytokines50.
Expression of adipocytokines in obesity state is associated with inflammation.
In obesity, inflammation occurs in adipose tissue and has an impact on glucose,
lipid and energy metabolism. It is possible that OSA-induced intermittent
hypoxia may interact with adiposity to promote metabolic dysfunction.
Intervention
Nowadays,
the focus is on primary prevention of coronary artery disease (CAD), which
means risk factor modification. Early recognition of risk factors and primary
prevention have significantly decreased the morbidity and mortality associated
with CAD. The risk assessment and preventive therapy is a combined decision taken
by the patient and their physician. Modifiable risk factors for coronary artery
disease include:
·
Type 2 diabetes mellitus
·
Hypertension
·
Smoking
·
Dyslipidemia
·
Obesity
·
Metabolic syndrome
Lifestyle
modification with diet, exercise, and smoking cessation is crucial to reduce
cardiovascular risk factors. Further control of hypertension, diabetes, and
hyperlipidemia is essential to reduce the risk of CAD. Replacing saturated fats
with dietary mono-saturated and polyunsaturated fats are found to be beneficial
to reduce cardiovascular risks. Besides, dietary sodium reduction is found to
have reduced blood pressure and decreased risk for cardiovascular events.
Physical
activity is also equally beneficial for CAD risk reduction. Moderate activities
like brisk walking, cycling, active yoga, and swimming or vigorous activities like
jogging/running, biking playing tennis, etc. may help in reducing the risks. Weight
loss has consistently shown to improve the cardiovascular risk profile. Strong
recommendations include high levels of physical activities, low-calorie diet,
and if possible, weight-loss maintenance programs.
Control
of hypertension by pharmacological management along with non-pharmacological
measures is recommended to reduce cardiovascular morbidity. Weight
loss also has a positive impact on lowering blood pressure.
Diabetes
mellitus is another important cardiovascular disease risk. Dietary
modifications using a heart-healthy diet and physical activities are
encouraged. Additionally, weight loss is recommended if the individual is
overweight or obese. Metformin can also be considered as first-line therapy for
type 2 DM to improve the glycemic index and reduce cardiovascular risk.
Most
of the above measures have a positive impact on obesity and OSA. These measures
also help to control the two important health risk of metabolic syndrome such
as diabetes and hypertension. OSA symptoms are well controlled on weight
reduction and many of the pathophysiological changes associated with OSA can be
controlled with weight reduction and CPAP therapy.
Conclusion
Obesity
is a primary determinant of OSA and metabolic syndrome. OSA can modify the
components of metabolic syndrome and vice versa. Early diagnosis and treatment
of OSA is the cornerstone in the management of metabolic syndrome and hence
CAD. The important measures include weight reduction, regular exercises,
control of hypertension and diabetes, along with treatment of OSA. Thus
clinicians should keep high index of suspicion for obesity, OSA and MetS while
dealing patients with cardiovascular morbidity.
References
1.
Harilakshmanan P, Arun P, Sethu Babu,
Ravindran C. Syndrome Z- A case report. Pulmon 2006;8:3: 91-94
2.
DS Hui, KW To, FW Ko, JP Fok, MC Chan,
JC Ngai, AH Tung, CW Ho, MW Tong, C-C Szeto, CM Yu. Nasal CPAP reduces systemic
blood pressure in patients with OSA and mild sleepiness. Thorax 2006;
61:1083-1090
3.
Jensen MK, Chiuve SE, Rimm EB, et al.
Obesity, behavioral lifestyle factors, and risk of acute coronary events.
Circulation 2008; 117: 3062–3069. Google Scholar
4.
Jackson-Leach R, Lobstein T. Estimated burden
of paediatric obesity and co-morbidities in Europe. Part 1. The increase in the
prevalence of child obesity in Europe is itself increasing. Int J Pediatr Obes
2006; 1: 26–32.CrossRefPubMedGoogle Scholar
5.
Cali AM, Caprio S. Obesity in children
and adolescents. J Clin Endocrinol Metab 2008; 93: Suppl. 1,
s31–s36.CrossRefPubMedGoogle Scholar
6.
Trayhurn P, Wood S. Adipokines:
inflammation and the pleiotropic role of white adipose tissue. Br J Nutr 2004;
92: 347–355.CrossRefPubMedWeb of ScienceGoogle Scholar
7.
Hotamisligil GS. Inflammation and
metabolic disorders. Nature 2006; 444: 860–867.CrossRefPubMed Google Scholar
8.
Grunstein RR, Wilcox I, Yang TS, et al.
Snoring and sleep apnoea in men: association with central obesity and
hypertension. Int J Obes Relat Metab Disord 1993; 17: 533–540.PubMedGoogle
Scholar
9.
Katsuki A, Sumida Y, Urakawa H, et al.
Increased visceral fat and serum levels of triglyceride are associated with
insulin resistance in Japanese metabolically obese, normal weight subjects with
normal glucose tolerance. Diabetes Care 2003; 26: 2341–2344. Google Scholar
10.
Allison DB, Fontaine KR, Manson JE,
Stevens J, VanItallie TB. Annual deaths attributable to obesity in the United
States. JAMA. 1999 Oct 27. 282(16):1530-8. [Medline].
11.
Bays HE, Gonzales-Campoy JM, Bray GA, et
al. Pathogenic potential of adipose tissue and metabolic consequences of
adipocyte hypertrophy and increased visceral adiposity. Expert Rev Cardiovasc
Ther 2008; 6: 343–368.CrossRefPubMedGoogle Scholar
12.
Martin SE, Engleman HM, Deary IJ, Douglas
NJ. The effect of sleep fragmentation on daytime function. Am J Respir Crit
Care Med 1996; 153:1328–32.
13.
Young T, Blustein J, Finn L, Palta M.
Sleep-disordered breathing and motor vehicle accidents in a population-based
sample of employed adults. Sleep 1997; 20:608–613.
14.
Leung RS, Bradley DT. Sleep apnea and
cardiovascular disease. Am J Respir Crit Care Med 2001; 164:2147–2165.
15.
Lavie P, Hoffstein V. Sleep apnea
syndrome: a possible contributing factor to resistant hypertension. Sleep 2001;
24(6):721–725.
16.
Apoor
S. Gami, Virend K. Somers. Obstructive sleep apnea, metabolic syndrome and
cardiovascular outcomes. European Heart Journal 2004; 25:709–711.
17.
Coughlin
S. Mawdsley, L., Mugarza, JA et al. Obstructive sleep apnoea is independently
associated with an increased prevalence of metabolic syndrome. Eur Heart J
2004; 25:735–41.
18.
Wilcox
I, McNamara SG, Collins FL et al. “Syndrome Z”: the interaction of sleep
apnoea, vascular risk factors and heart disease. Thorax 1998; 53(Suppl
3):25–28.
19.
Bonsignore MR, Eckel J. Metabolic
aspects of obstructive sleep apnoea syndrome. Eur Respir Rev 2009; 18: 113–124.
Google Scholar
20.
Yin J, Gao Z, He Q, et al. Role of
hypoxia in obesity-induced disorders of glucose and lipid metabolism in adipose
tissue. Am J Physiol Endocrinol Metab 2009; 296: E333–E342. Google Scholar
21.
Myers MGJ, Leibel RL, Seeley RJ, et al.
Obesity and leptin resistance: distinguishing cause from effect. Trends
Endocrinol Met 2010; 21: 643–651.CrossRefPubMedGoogle Scholar
22.
Ambrosini G, Nath AK, Sierra-Honigmann
MR, et al. Transcriptional activation of the human leptin gene in response to
hypoxia. J Biol Chem 2002; 277: 34601–34609. Google Scholar
23.
Koh KK, Park SM, Quon MJ. Leptin and
cardiovascular disease: response to therapeutic interventions. Circulation
2008; 117: 3238–3249. Google Scholar
24.
Nawrocki AR, Rajala MW, Tomas E, et al.
Mice lacking adiponectin show decreased hepatic insulin sensitivity and reduced
responsiveness to peroxisome proliferator-activated receptor gamma agonists. J
Biol Chem 2006; 281: 2654–2660. Google Scholar
25.
Han SH, Sakuma I, Shin EK, et al.
Antiatherosclerotic and anti-insulin resistance effects of adiponectin: basic
and clinical studies. Prog Cardiovasc Dis 2009; 52:
126–140.CrossRefPubMedGoogle Scholar
26.
Shoelson SE, Lee J, Goldfine AB.
Inflammation and insulin resistance. J Clin Invest 2006; 116:
1793–1801.CrossRefPubMedGoogle Scholar
27.
Varlamov O, Somwar R, Cornea A, et al.
Single-cell analysis of insulin-regulated fatty acid uptake in adipocytes. Am J
Physiol Endocrinol Metab 2010; 299: E486–E496. Google Scholar
28.
Coughlin
SR, Mawdsley L, Mugarza JA, et al. Obstructive sleep apnea is independently
associated with an increased prevalence of metabolic syndrome. Eur Heart J
2004; 25:735–41.
29.
Lam JCM, Lam B, Lam CL, et al.
Obstructive sleep apnea and the metabolic syndrome in community-based Chinese
subjects in Hong Kong. Resp Med 2006; 100(6):980–87
30.
Schwartz AR, Patil SP, Laffan AM,
Polotsky VY, Schneider H, Smith PL. Obesity and obstructive sleep apnea:
pathogenic mechanism and therapeutic approaches. Proc Am Thorac Soc 2008; 5(2):185–92.
31.
Alberti KG, Zimmet P, Shaw J. The
metabolic syndrome: a new worldwide definition. Lancet 2005; 366:1059–1062.
32.
Punjabi NM. The epidemiology of adult
obstructive sleep apnea. Proc Am Thorac Soc 2008; 5:136–43.
33.
de Sousa AGP, Cercato C, Mancini MC,
Halpern A. Obesity and obstructive sleep apnea. Obes Rev 2008; 9:340–54.
34.
Peppard PE, Young T, Palta M, Dempsey J,
Skareyd J. Longitudinal study of moderate weight change and sleep-disordered
breathing. JAMA 2000; 284:3015–21.
35.
Lam B, Sam K, Mok WY, et al. Randomised
study of three non-surgical treatments in mild to moderate obstructive sleep
apnoea. Thorax 2007; 62(4):354–59.
36.
Börntorp P. Metabolic implications of
body fat distribution. Diabetes Care 1991; 14:1132–43.
37.
Tasali E, Ip MS. Obstructive sleep apnea
and metabolic syndrome: alterations in glucose metabolism and inflammation.
Proc Am Thorac Soc 2008; 5(2):207–17.
38.
Ip MS, Lam B, Ng MMT, Lam WK, Tsang KWT,
Lam KSL. Obstructive sleep apnea is independently associated with insulin
resistance. Am J Respir Crit Care Med 2002; 165:670–76.
39.
Reichmuth KJ, Austin D, Skatrud JB,
Young T. Association of sleep apnea and Type II diabetes: a population-based
study. Am J Respir Crit Care Med 2005; 172:1590–95.
40.
Anderson AJ, Sobocinski KA, Freedman DS,
et al. Body fat distribution, plasma lipids and lipoproteins. Arteriosclerosis
1998; 8:88–94.
41.
Newman AB, Nieto FJ. Relationship of
sleep-disordered breathing to cardiovascular risk factors. The Sleep Heart Health Study. Am J Epidemiol
2001; 154:50–59.
42.
Somers VK, Dyken ME, Clary MP, et al.
Sympathetic neural mechanisms in OSA. J Clin Invest 1995; 96:1897–1904.
43.
Wolk R, Shamsuzzaman, Somers VK.
Obesity, sleep apnea and hypertension. Hypertension 2003; 42:1067–74.
44.
Pratt-Ubunama MN, Nichizaka MK,
Boedefeld RL, et al. Plasma aldosterone is related to severity of obstructive
sleep apnea subjects with resistant hypertension. Chest 2007; 131:453–59.
45.
Yaggi HK, Araujo AB, McKinlay JB. Sleep
duration as a risk factor for the development of Type 2 diabetes. Diabetes Care
2006; 29:657–61.
46.
Ip MS, Mokhlesi B. Sleep and glucose
intolerance/diabetes mellitus. Sleep Med Clin 2007; 2:19–29.
47.
Taheri S, Lin L, Austin D, Young T,
Mignot E. Short sleep duration is associated with reduced leptin, elevated
ghrelin, and increased body mass index. PLoS Med 2004; 1(3):e62.
48.
Trayhurn P, Wang B, Wood IS. Hypoxia in
adipose tissue: Bases for the dysregulation of tissue function in obesity? Br J
Nutr 2008; 100:227–35.
49.
Li J, Savransky V, Nanayakkara A, Smith
PL, O'Donnell CP, Polotsky VY. Hyperlipidemia and lipid peroxidation are
dependent on the severity of chronic intermittent hypoxia. J Appl Physiol 2007;
102:557–63.
50.
Lam DCL, Xu A, Lam KSL, et al. Serum
adipocyte-fatty acid binding protein (A-FABP) level is elevated in severe
obstructive sleep apnea (OSA) and correlates with insulin resistance. Eur
Respir J 2009; 33:346–51.
