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Cardiovascular Risk, Diabetes
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Obstructive Sleep Apnoea and Vascular Disease in Patients with Type 2 Diabetes

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Published Online: Nov 2nd 2015 European Endocrinology, 2015;11(2):81–9 DOI: http://doi.org/10.17925/EE.2015.11.02.81
Authors: Abd A Tahrani
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Abstract
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Abstract:
Overview

Obstructive sleep apnoea (OSA) is common and is associated with many vascular risk factors, such as hypertension, insulin resistance, albuminuria, dyslipidaemia, increased inflammation and endothelial dysfunction. Epidemiological studies have shown that OSA is associated with increased cardiovascular disease (CVD) and that continuous positive airway pressure (CPAP) might reduce CVD events in patients with OSA. In addition, OSA has also been shown to be associated with albuminuria, chronic kidney disease, a wide range of ocular diseases and peripheral neuropathy. Considering that CVD and microvascular complications are major contributors to the morbidity, mortality and the economic burden of diabetes and that OSA is common in patients with type 2 diabetes (T2D), it is important to understand the role of OSA in the development and/or progression of vascular disease in patients with T2D and to explore the impact of CPAP on diabetes-related vascular outcomes. The purpose of this article is to review the evidence for the relationship and impact of OSA on vascular disease and vascular risk factors particularly in patients with T2D.

Keywords

Type 2 diabetes, obstructive sleep apnoea, vascular disease, vascular risk

Article:

Diabetes-related macro- and microvascular complications contribute significantly to the increased morbidity, mortality, worsened quality of life and social and financial burden observed in patients with diabetes.1–5 Hence, reducing the development and/or the progression of these complications is one of the main aims of treatment in patients with diabetes.

Over the last 2 decades, strategies resulting in the improvements of glycaemic control, blood pressure (BP) and lipids and the use of renin angiotensin aldosterone inhibitors, resulted in reductions in cardiovascular disease (CVD) in patients with diabetes, but there was little impact on diabetic microvascular complications.6 Nonetheless, both CVD and microvascular complications remain common and a better understanding of the pathogenesis of these complications is needed in order to identify new treatment strategies.

Obstructive sleep apnoea (OSA) is common in patients with type 2 diabetes (T2D) (up to 86 % prevalence), which is not surprising considering that increasing age and obesity are common risk factors to both conditions.7,8 OSA is characterised by upper airway instability during sleep that results in recurrent upper airway obstruction resulting in either complete or partial cessation of airflow (i.e. apnoea and hypopnoea, respectively).9 The recurrent obstructions of the upper airway usually result in recurrent oxygen desaturations/re-saturations, cyclical changes in intrathoracic pressure (as the patient attempts to breath against a blocked airway) and recurrent micro arousals that cause sleep fragmentation and reduction in slow wave and rapid eye movement (REM) sleep and result in termination of the apnoea/ hypopnoea episodes.9

Several large epidemiological studies and randomised controlled trials (RCTs) have shown that OSA was associated with CVD and CVD risk factors in general populations, while the impact of OSA on vascular disease in patients with T2D has only gained attention in the last few years.7,10,11 In this article the evidence of the relationship and impact of OSA on vascular disease and CVD risk factors will be reviewed, particularly in patients with T2D.

Obstructive Sleep Apnoea and Vascular Risk Factors
Obstructive Sleep Apnoea and Hypertension

Several cross-sectional, prospective and interventional studies showed that OSA was associated with sustained hypertension, lack of the nocturnal dipping of BP and incident hypertension and that OSA treatment lowered BP. Most of these studies were not in patients with T2D, but the limited evidence available in patients with T2D seems to support the findings of studies from the general population.

In General Population Studies
In a cross-sectional analysis from the Sleep Heart Health Study, OSA was associated with hypertension in 6,132 middle-aged and older persons (aged ≥40 years) odds ratio (OR) (95 % confidence interval [CI]) for hypertension for the highest versus the lowest category of the apnoea–hypopnoea index (AHI) was 1.37 (1.03–1.83; p=0.005) after adjustment for body mass index (BMI), neck circumference, waist–hip ratio, alcohol and smoking.12 This association was present in men and women, older and younger, multiple ethnic groups and among normal weight and overweight patients.12< In the Wisconsin Sleep Cohort Study, OSA was associated with the presence of hypertension in 709 participants after 4 years of follow-up; relative to an AHI of 0 at baseline, the adjusted ORs for the presence of hypertension at follow-up were 1.42 (95 % CI 1.13–1.78), 2.03 (1.29–3.17) and 2.89 (1.46–5.64) for an AHI of 0.1 to 4.9, 5.0 to 14.9 and ≥15.0 respectively (p=0002 for the trend).13 OSA was also a predictor of incident systolic nocturnal non-dipping of BP (based on 24-hour ambulatory BP) over an average of 7.2 years follow-up in 328 adults from the Wisconsin Sleep Cohort Study (adjusted OR [95 % CI] for baseline AHI 5–14.9 and ≥15, versus AHI <5, were 3.1 [1.3–7.7] and 4.4 [1.2–16.3], respectively).14

Impact of Obstructive Sleep Apnoea Treatment
The causality between OSA and hypertension was further confirmed in interventional and RCTs. A recent meta-analysis of RCTs showed that continuous positive airway pressure (CPAP) lowered BP in hypertensive patients with OSA, particularly in relation to diastolic BP, nocturnal systolic BP and in patients receiving anti-hypertensives.15 In a RCT of hypertensive patients with OSA in which patients were randomised to oral appliances with or without mandibular advancement, there was a trend for lowering BP in the active versus control groups, particularly in those with BP >135/85 mmHg and AHI >15.16 CPAP also might have had a BP-lowering effect even in those with resistant hypertension.15 In a small RCT of moderate to severe OSA patients with resistant hypertension, in which patients were randomised to medical therapy versus CPAP + medical therapy, 6 months of CPAP was associated with greater reductions in systolic and diastolic BP (systolic +3.1±3.3 versus −6.5±3.3; diastolic +2.1±2.7 versus –4.5±1.9 mm Hg; p<0.05 for both comparisons).17 This effect was mainly for diurnal rather than nocturnal BP.17 Another open-label RCT in which patients with moderate to severe OSA and resistant hypertension were randomised to CPAP or no CPAP in addition to usual medical therapy, showed that 12 weeks of CPAP resulted in a greater reduction compared with the control group in terms of the average 24-hour BP (3.1 mm Hg [95 % CI 0.6 to 5.6]; p=0.02) and diastolic BP (3.2 mm Hg [95 % CI 1.0 to 5.4]; p=0.005), but not systolic BP.18 In addition, CPAP resulted in a greater proportion of patients having nocturnal BP dipping compared with the control group (35.9 % versus 21.6 %, adjusted OR 2.4 [95 % CI, 1.2 to 5.1]; p=0.02).18There was a significant modest positive correlation between hours of CPAP use and the decrease in 24-hour mean BP, diastolic BP and systolic BP (correlation coefficients were 0.25–0.30).18 However, not all studies showed similar results; in recent RCTs 3–6 months of CPAP had no impact on BP in patients with moderate to severe OSA and resistant hypertension.19,20Furthermore, in an 8-week RCT with a crossover design, both CPAP and valsartan resulted in a significant reduction in mean 24-hour BP but valsartan was superior to CPAP (−7.0 mm Hg, 95 % CI −10.9 to −3.1 mm Hg; p<0.001).21

The impact of CPAP on incident hypertension was assessed in one RCT, in which 723 patients with AHI ≥20 and ESS ≤10 were randomised to CPAP versus no CPAP. After 4 years, CPAP treatment had not had any impact on the incidence of hypertension and CVD (combined) in the intention-to-treat analysis (OR 0.83, 95 % CI 0.63–1.1; p=0.20), but sub-group analysis showed that adherence to CPAP treatment (≥4 hours/night) lowered the incidence of the combined outcome (OR 0.72, 95 % CI 0.52–0.98; p=0.04).22 There was no significant impact of CPAP when incident hypertension and incident CVD were analysed separately but this might be related to sample size.

In Patients with Type 2 Diabetes
Unlike the extensive evidence for the relationship between OSA and hypertension in the general population, data in patients with T2D are rather limited, despite the high prevalence of OSA in patients with T2D and the importance of maintaining good BP targets to reduce diabetesrelated vascular complications. In a large cross-sectional study that included 12,765 patients with hypertension (2,954 with T2D), patients with T2D and either awake BP ≥135/85 mm Hg or asleep BP ≥120/70 mm Hg, had a higher prevalence of OSA than those with T2D, but lower BP and patients with T2D had a higher prevalence of non-dipping of nocturnal BP than those without T2D;23 these findings suggest that OSA might contribute to the non-dipping of nocturnal BP in patients with T2D.

Impact of Continuous Positive Airway Pressure
In a retrospective cohort database study of 221 patients with newly diagnosed OSA, CPAP was associated with a mean change of –7.44 (95 % CI –10.41 to –4.47) and –3.14 (–4.99 to –1.29) at 3–6 months and –6.81 mmHg (–9.94 to –3.67 mmHg) and –3.69 mmHg (–5.53 to –1.85 mmHg) at 9–12 months in systolic and diastolic BP, respectively.24 Greater adherence was associated with greater reductions in diastolic BP, but the association was modest (R2=0.04; p=0.04).24 Another randomised parallel group intervention trial, in which patients with T2D and OSA were randomised to early (<1 week) or late (1–2 months) CPAP for 3 months, showed that CPAP resulted in reductions in systolic and diastolic BP (149±23/80±12 to 140±18/73±13 mm Hg; p=0.005 and 0.007 for systolic and diastolic BP, respectively).25 Clearly, much more evidence is needed before proving causality between OSA and hypertension in patients with T2D. There is a need for randomised placebo and active controlled trials assessing the impact of OSA and CPAP on hypertension in patients with T2D, particularly in those
with resistant hypertension.

Obstructive Sleep Apnoea and Insulin Resistance
Insulin resistance (IR) is an important risk factor for the development of vascular dysfunction and CVD.26–29 IR is also associated with many cardiovascular risk factors such as the metabolic syndrome, hypertension, dyslipidaemia, hypercoagulability and sympathetic activation.28,30–32

In General Population Studies
Several cross-sectional studies showed an association between OSA and IR but some studies did not show such an association.7,10,11 Obesity is obviously a major confounder but the association between OSA and IR was also found in lean individuals, suggesting that the relationship is independent of obesity.33,34 One study examined the effect of OSA on IR longitudinally; over
11-year follow-up OSA, AHI, oxygen desaturation index (ODI) and minimal oxygen saturations overnight were independently associated with IR after adjustment for age, baseline BMI, hypertension, BMI change over followup and CPAP treatment.35 CPAP was shown to lower IR (improve insulin sensitivity) in several studies and meta-analysis,36–38 particularly when CPAP usage was >4 hours per night.39

In Patients with Type 2 Diabetes
Data about the impact of OSA on IR in patients with T2D are limited. Two cross-sectional studies from the same group showed that OSA was associated with IR (based on the homeostatic model assessment [HOMA]) in patients with T2D.40,41 A meta-analysis42 of two non-randomised trials43,44 showed that CPAP treatment improved insulin sensitivity in patients with T2D suggesting possible causality. Further studies and clinical trials are needed to assess the impact of OSA on IR in patients with T2D, particularly in those with severe IR considering that the pharmacological options to treat severe IR in T2D are limited.

Obstructive Sleep Apnoea and Lipids
In General Population Studies
Many cross-sectional studies examined the relationship between OSA and hyperlipidaemia. The results are conflicting mainly due to differences in the population examined (particularly the choice of the control group, the sample size and the possible confounding effects of CPAP).45,46 A recent meta-analysis of 64 studies showed that OSA was associated with higher total cholesterol, higher low-density lipoprotein (LDL), higher triglycerides and lower high-density lipoprotein (HDL).45 AHI correlated positively with triglyceride levels and negatively with HDL levels but not with total cholesterol or LDL.45 The association between OSA/AHI and triglyceride levels was also evident in non-obese patients34 suggesting that relationship is independent of obesity and possibly more related to IR. However, despite these findings, a good evidence of causality between OSA and hyperlipidaemia is lacking, although mechanistically it is plausible that chronic intermittent hypoxia might lead to hyperlipidaemia via the generation of stearoyl-coenzyme A desaturase-1 and oxidative stress, peroxidation of lipids and sympathetic activation.46

Impact of Continuous Positive Airway Pressure
The CPAP impact on dyslipidaemia was assessed in several meta-analyses. In a meta-analysis that included 29 clinical trials, the majority of which were uncontrolled and not RCTs with a study duration of 3–6 months (range 2 days to 8 months), CPAP reduced total cholesterol and LDL and increased HDL and had no effect on triglycerides.47 Another meta-analysis that included only RCTs (n=6) showed slightly different results in that CPAP had no effect on LDL, HDL or triglycerides but CPAP did lower total cholesterol levels particularly in patients who were younger, more obese and who used CPAP for a longer period.48 Hence, the impact of CPAP on lipids remains unclear. It needs to be noted that the impact of CPAP might be less relevant than that of lipid-lowering treatments currently available.

In Patients with Type 2 Diabetes
In patients with T2D, the impact of CPAP is limited to one RCT in which patients were randomised to early versus late CPAP treatment; the combined analysis of both arms showed that 3 months of CPAP had no effect on the lipids.25 However, the levels of total cholesterol, LDL, HDL and triglycerides were largely within recommended targets for patients with T2D at baseline and approximately 80 % of the study participants were on lipid-lowering treatment.25 Clearly there is need for RCTs and appropriately designed longitudinal studies to understand the impact of OSA on dyslipidaemia in diabetes.

Obstructive Sleep Apnoea, Inflammation and Endothelial Dysfunction
As OSA is associated with increased oxidative stress and activation of the sympathetic nervous system and free fatty acid release, hence, it is plausible that OSA is associated with increased systematic inflammation.49
Chronic intermittent hypoxia, a feature of OSA, was associated with increased nuclear factor κB (NF-κB) and hypoxia-inducible factor-1 (HIF-1) in vivo and in vitro; both of which can result in systematic inflammation.50,51 OSA has been shown to be associated with increased systematic cytokines such as interleukin (IL)-6, IL-8, tumour necrosis factor alpha (TNF-α), c-reactive protein (CRP), granulocyte chemotactic protein-2 (GCP-2) and monocyte chemotactic protein-1 (MCP-1) independent of obesity.52-61 However, not all studies showed a relationship between OSA and inflammation62,63 with obesity being the main confounder.64 Whether CPAP reduces systematic inflammation and cytokines is unclear as some studies showed that CPAP reduced systematic inflammation while others did not.49, 65, 66

Adhesion molecules (selectins and integrins) play an important role in inflammation and in the interaction between the endothelium, platelets and white cells.64 Polymorphnuclear cells, monocytes and T lymphocytes from patients with OSA had increased adhesion molecules, increased avidity to endothelial cells and increased prolonged lifespan of active polymorphmuclear cells compared with controls.67–74 In addition, endothelial cells from patients with OSA showed increased expression of adhesion molecules (intercellular adhesion molecule 1 [ICAM-1], vascular cell adhesion molecules (VCAM) and E-selectin and P-selectin) compared with controls, which might be reversible with CPAP treatment.60,61,75–77
Several studies showed that OSA was associated with endothelial dysfunction. OSA patients had reduced circulating and endothelial levels of nitric oxide, which can improve after CPAP,78–80 partly because of reduction in nitric oxide production secondary to the inhibition of nitric oxide synthase.81 Patients with OSA exhibited impaired endothelial-dependent and independent vasodilatation82 independent of hypertension,83 obesity84 and cardiovascular risk factors.85 In patients with T2D, OSA and hypoxaemia, measures were associated with increased nitrosative stress and oxidative stress despite adjustment for many confounders.64, 86 In addition, OSA and lower nadir nocturnal oxygen saturations were also associated with reduction in nitric oxideinduced vasodilation compared with those with T2D but without OSA, despite adjustment for many confounders.86

Obstructive Sleep Apnoea and Cardiovascular Disease
In General Population Studies

Several cross-sectional and case-controlled studies showed an association between OSA and CVD.87,88 In patients with stable coronary artery disease (CAD), OSA patients had a larger atherosclerotic plaque volume (based on intravascular ultrasound) compared with patients without OSA; the AHI correlated positively with the plaque volume measured by ultrasound (r=0.6; p=0.01)89 or computed tomography (CT) angiogram (r=0.4; p=0.02).90 Patients with OSA were also more likely to develop acute myocardial infarction between 12 am and 6 am compared with matched controls without OSA (32 % versus 7 %; p=0.01)91 supporting the role of nocturnal events in OSA in the development of myocardial infarction.

Longitudinal Studies and the Impact of Continuous Positive Airway Pressure
Several prospective observational studies have also shown that OSA predicts the development of incident CVD and that CPAP might reduce CVD incidence in patients with OSA.92–97 In a study of 182 consecutive middle-aged men who were free of CVD at baseline and were followed up for 7 years, OSA was an independent predictor of incident CVD (adjusted OR 4.9, 95 % CI 1.8–13.6).92 CPAP treatment was associated with a reduction in CVD incidence (56.8 % versus 6.7 % for incompletely treated versus efficiently treated with CPAP, respectively; p<0.001).92 In another study of men with OSA, patients with untreated severe OSA had a higher incidence of fatal and non-fatal CVD compared with untreated patients with mild to moderate OSA, simple snorers, patients treated with CPAP and healthy participants after a mean follow-up of 10.1 years.93 Untreated severe OSA significantly increased the risk of fatal (adjusted OR 2.87, 95 % CI 1.17–7.51) and non-fatal (adjusted OR 3.17, 95 % CI 1.12–7.51) CVD compared with healthy participants.93 In another study in which 1,022 patients were followed up for a median of 3.4 years, OSA increased the risk of stroke or death (hazard ratio [HR] 1.97, 95 % CI 1.12–3.48; p=0.01).94 In a longitudinal study of 1,189 patients from the general population; AHI ≥20 was associated with an increased risk of suffering a first-ever stroke over the next 4 years in the unadjusted analysis (OR 4.31, 95 % CI 1.31–14.15; p=0.02), but this association became non-significant after adjustment for age, sex and BMI (OR 3.08, 95 % CI 0.74–12.81; p=0.12).98
Not all studies showed that CPAP was associated with a reduction in CVD incidence: in a large cohort of US veterans (over 3 million, 97 % men, average age 60.5 years) and after a median follow-up of 7.7 years, untreated and treated OSA were associated with incident CAD (HR 3.54, 95 % CI 3.40 to 3.6 and 3.06, 95 % CI 2.62 to 3.56) and incident stroke (HR 3.48, 95 % CI 3.28 to 3.64 and HR 3.50, 95 % CI 2.92 to 4.19) for untreated and treated OSA, respectively.96 Finally, a recent study suggested that the impact of OSA on incident CVD might be modulated by age and gender: in a cohort of 1,927 men and 2,495 women who were free of CAD and heart failure at baseline and were followed-up for a median of 8.7 years OSA was an independent predictor of incident CAD only in men younger than 70 years of age (adjusted HR 1.10, 95 % CI 1.00–1.21 per 10 unit increase in the AHI).97 OSA also predicted incident heart failure in men only (adjusted HR 1.13; 95 % CI 1.02–1.26 per 10 unit increase in AHI).97 In another prospective study of 5,422 participants without a history of stroke at baseline, after a median of 8.7 years men in the highest AHI quartile (>19) had an adjusted HR of 2.86 (95 % CI 1.1–7.4). In men with AHI 5–25, each one unit increase in AHI was associated with increased stroke risk by 6 % (95 % CI 2–10 %):no such associations were found in women.99 However, in another prospective study in which the primary outcome was to examine the impact of OSA on a composite endpoint of stroke and CAD in women (n=967), after a median follow-up of 6.8 years, the untreated OSA group had greater risk of incident stroke and CAD combined compared with the control group (adjusted HR 2.76, 95 % CI 1.35–5.62) and 0.91 (95 % CI 0.43–1.95) for the CPAP-treated group.100 Most of the impact of untreated OSA was due to increased incident stroke (adjusted HR 6.44; 95 % CI 1.46–28.3) rather than incident CAD (adjusted HR 1.77, 95 % CI 0.76–4.09).100

There is a lack of RCTs assessing the impact of CPAP on CVD incidence in patients with OSA. In one RCT, in which 723 patients with AHI ≥20 and Epworth Sleepiness Scale (ESS) ≤10 were randomised to CPAP versus no CPAP; after 4 years CPAP treatment had no impact on the incidence of hypertension and CVD (combined) in the intention-to-treat analysis (OR 0.83, 95 % CI 0.63–1.1; p=0.20), but subgroup analysis showed that adherence to CPAP treatment (≥4 hours/night) lowered the incidence of the combined outcome (OR 0.72, 95 % CI 0.52–0.98; p=0.04).22 There was no significant impact of CPAP on incident CVD when analysed separately from hypertension, but this might be related to sample size. Hence, there is a need for RCTs of adequate study duration and sample size to assess the impact of OSA on CVD.

In Patients with Type 2 Diabetes
The evidence for the relationship between OSA and CVD in T2D is limited. In the Look AHEAD study, AHI was associated with self-reported history of stroke (adjusted OR 2.57, 95 % CI 1.03–6.42), but not with CAD in a cross-sectional analysis.101 A more recent study provided more convincing evidence of an association between OSA and CVD in T2D; in this study 132 consecutive asymptomatic patients with T2D and normal exercise echocardiography for ≤8 years were followed for a median of 4.9 years and found that OSA was associated with incident CAD (adjusted HR 2.2, 95 % CI 1.2–3.9, p=0.01) and heart failure (adjusted HR 3.5, 95 % CI 1.4–9.0; p<0.01).102 Whether CPAP treatment reduces CVD progression or incidence in patients with T2D is unknown.

Obstructive Sleep Apnoea and Microvascular Disease
There are many plausible reasons to postulate that OSA might result in microvascular disease. We have reviewed these potential mechanisms previously in this journal8 but, in summary, OSA and intermittent hypoxaemia can result in increased oxidative and nitrosative stress, Poly (ADP-ribose) polymerase (PARP) activation, increased advanced glycation end-products (AGE), protein kinase C (PKC) activation and inflammation in patients with and without diabetes – all of which can result in endothelial dysfunction and microvascular disease.7,11

Obstructive Sleep Apnoea and Nephropathy/ Chronic Kidney Disease
In General Population Studies

OSA has been shown to be prevalent in patients with end stage renal disease (30–80 %);103–105 but the direction of this relationship and causality is not clear.106 Several studies examined the association between OSA and albuminuria/renal function; however, the vast majority of these studies were cross-sectional making it difficult to infer causality.

Obstructive Sleep Apnoea and Albuminuria

In a cross-sectional study of 121 patients with newly diagnosed, untreated hypertension, patients with moderate to severe OSA had higher urinary albumin excretion compared with patients without OSA (14.5±6.9 versus 10.0±8.0 mg/24 hours; p=0.014) and the AHI was associated with urinary albumin excretion after adjustment for BP and components of the metabolic syndrome.107 Similar results were found in another crosssectional study of 40 patients with newly diagnosed OSA without diabetes or hypertension that found that the AHI was independently associated with increased urinary albumin creatinine ratio (ACR) after adjustment for gender, age, BMI, hyperlipidaemia, HOMA-IR, blood creatinine, albumin and estimated glomerular filtration rate (eGFR).108 In a cross-sectional study of 507 older community-dwelling men (age 76.0 ± 5.3 years), patients with severe OSA had greater urinary ACR compared with those without OSA (age- and race-adjusted mean ACR 9.35 versus 6.72 mg/g; p=0.007) but this difference became non-significant after adjustment for BMI, hypertension and diabetes.109 However, % time of oxygen saturation <90 % remained significantly associated with urinary ACR after adjustment for age, race, BMI, hypertension and diabetes (10.35 mg/g for ≥10 % time oxygen saturation <90 versus 7.45 mg/g for <1 % time oxygen saturation <90; p=0.046).109 In another study of 496 adults, AHI was an independent predictor of urinary ACR after adjustment for age, ethnicity, BMI, smoking, eGFR, diabetes and hypertension.110 In order to address the matter of hypertension as a possible confounder, a cross-sectional study of 62 untreated hypertensive patients with OSA and 70 hypertensive patients without OSA, who were matched for age, sex, smoking status, BMI and 24-hour pulse pressure, showed albuminuria to be greater by 57 % in patients with OSA versus those without and urinary ACR correlated with AHI and other markers of OSA severity.111 This relation remained significant following adjustment for confounders.111 However, other studies showed no relation between albuminuria or proteinuria and OSA.112–114

Obstructive Sleep Apnoea and Renal Function
Similar to albuminuria, the relationship between OSA and renal function was mainly assessed in cross-sectional studies and the results are conflicting. In a cross-sectional study of selective 91 morbidly obese adults (BMI 48.3±8.9 kg/m2) before bariatric surgery, serum creatinine was significantly higher in the OSA group (0.8±0.2 mg/dl in no OSA, 0.9±0.2 mg/dl in OSA; p=0.01)112 and AHI remained independently associated with serum creatinine after adjustment.112 In a study of 505 men with OSA (defined as respiratory disturbance index [RDI] ≥15 events/hour), serum cystatin-C correlated with RDI, but this relation was lost after adjustment for possible confounders.115 Based on the Mayo clinic formula (and not Modification of Diet in Renal Disease [MDRD]), men with renal impairment had 2.1-fold greater odds of OSA even after adjustments for confounders.115 In a similar study by the same group, lower eGFR (based on MDRD) was not associated with higher RDI.116 In an interesting crosssectional study that included 100 patients who already have CKD (eGFR 28.5 ml/minute/1.73 m2) and who were not obese (23.1 kg/m2), a 10 ml/ minute/1.73 m2 decrease in eGFR was associated with 42 % increased odds of OSA after adjustment for age, BMI and diabetes mellitus and eGFR was inversely correlated with AHI after adjustment for covariates.117

In a prospective study of 858 patients with an average follow-up of 2.1 years, patients with nocturnal hypoxia (defined as oxygen saturation <90 % for ≥12 % of the nocturnal monitoring time) had a significant increase in the adjusted risk of accelerated kidney function loss (defined as decline in eGFR ≥4 ml/minute/1.73 m2 per year) compared with controls without hypoxia after adjustment for RDI, age, BMI, diabetes, heart failure and the use of angiotensin-converting-enzyme (ACE) inhibitors or angiotensin receptor blockers (OR 2.89, 95 % CI 1.25–6.67).118 In this study, OSA was associated with accelerated kidney function loss in the univariate analysis, which became non-significant after adjustment for confounders.118 In a large prospective study of a nationally representative cohort of over 3 million (n=3,079,514) US veterans (93 % male) with baseline eGFR ≥60 ml/ minute/1.73 m2, the risk of incident chronic kidney disease (CKD) (defined as eGFR <60 ml/min/1.73 m2) was greater in untreated (adjusted HR 2.27, 95 % CI 2.19–2.36) and treated (adjusted HR 2.79, 95 % CI 2.48 to 3.13) patients with OSA.96

Impact of Continuous Positive Airway Pressure
The impact of CPAP on albuminuria is unclear. In an uncontrolled study of 18 patients (four women), the use of CPAP for 1 month resulted in lowering of urinary albumin excretion and urinary ACR by more than 50 %.119 In a small pilot, RCT patients with moderate to severe OSA (n=13) were randomised to CPAP for 4 weeks versus no treatment; CPAP resulted in important reductions in urinary albumin compared with no treatment, although this was not statistically significant, most likely due to the small sample size.120 Longitudinal and interventional studies assessing the impact of OSA and CPAP on albuminuria are needed.

An uncontrolled clinical trial of 39 patients with newly diagnosed severe OSA on CPAP for 3 months did not result in any changes in serum creatinine or eGFR, but cystatin C (a biomarker of early CKD) declined significantly (0.
87±0.18 versus 0.77±0.21; p<0.001);121 the lack of impact on eGFR may not be surprising considering the short duration of treatment. In another uncontrolled study of 38 patients with OSA, 3 months of CPAP resulted in a decrease in the serum creatinine levels (0.87±0.09 to 0.82±0.01 mg/dl; p=0.013) and increased eGFR (72.9±12.0 to 79.3±17.9 ml/minute/1.73 m2; p=0.014).122

Although the results from these studies are conflicting, the majority showed an association between OSA or one of its parameters and renal function, decline in renal function and/or CKD but the impact of CPAP is unclear and well-designed RCTs are required.

In Patients with Type 2 Diabetes

Several studies examined the association between OSA and diabetic nephropathy (DN)/CKD, all except one study were cross-sectional. OSA was found to be associated with DN (defined as albuminuria and/or reduced eGFR) in patients with T2D after adjustment for a wide range of potential confounders (adjusted OR 2.64, 95 % CI 1.13–6.16; p=0.02).123 In this study, patients with OSA had significantly more albuminuria, higher creatinine, lower eGFR and a greater proportion of patients with eGFR <60 ml/minute/1.73 m2 compared with patients without OSA.123 Lower nadir nocturnal oxygen saturation was also associated with DR after adjustment for potential confounders (OR 0.96, 95 % CI 0.93–1.00; p=0.05).123 After a 2.5-year follow-up, the eGFR decline was greater in patients with OSA compared with those without OSA (median −1.4 %[interquartile range (IQR) −7.7 to 5.2] versus −5.3 % [−16.5 to 2.7] versus −8.7 % [−16.1 to 2.0]; p=0.003, for no OSA versus mild versus moderate to severe OSA) and OSA was an independent predictor of study end eGFR (B=−4.2; p=0.03) and eGFR decline.123 Baseline AHI was also an independent predictor of study end eGFR after adjustment (B= −4.6, p=0.02).123 The progression to albuminuria was numerically but not statistically greater in patients with OSA compared those without OSA (22.6 % versus 13.3 %; p=0.23).123

In the same observational longitudinal study the use of CPAP was associated with a favourable impact on eGFR decline over the followup (median –1.4 % [IQR –7.7 % to 5.2 %] versus –5.3 % [–16.5 % to 2.7 %] versus – 7.7 % [–15.9 % to –1.8 %] versus –10.0 % [–17.2 % to 2.3 %]) for no OSA versus mild OSA versus moderate to severe OSA CPAP-compliant versus moderate to severe OSA non-compliant with CPAP respectively (p=0.01 for the trend).123
In a study of Japanese patients with T2D, an ODI≥5 was independently associated with microalbuminuria in women but not in men after adjustment for confounders.124 Another cross-sectional study showed no relationship between OSA and microalbuminuria in patients with T2D, but this study was of a small sample size (n=52).125 In another small study utilising data collected during routine clinical care from 90 patients with T2D and morbid obesity, the time spent with oxygen saturations <90 % and AHI correlated with AHI after adjustment for potential confounders.126

It is possible that OSA contributes to the development and/or progression of nephropathy and CKD in patients with T2D, but further well-designed longitudinal studies and interventional trials are needed.

Obstructive Sleep Apnoea and Retinopathy
In General Population Studies
There are no typical retinal changes that are associated with OSA in patients without T2D; however, several cross-sectional studies showed that OSA is associated with a variety of ocular lesions. In the Sleep Heart Health Study, 2,927 patients had retinal photographs taken.127 The overall prevalence of retinopathy was non-significantly higher in people with higher RDI values; an increase of RDI from 0 to 10 was associated with a predicted decrease in arteriole-to-venule ratio of 0.01.127 However, it must be noted that retinal images were obtained from one randomly selected eye after 5 minutes of dark adaptation without the use of dilators.127 OSA has been reported to be associated with other eye lesions such as central serous chorioretinopathy, retinal vein thrombosis, ocular hypertension and optic neuropathy.128–132

OSA was also associated with reduced retinal sensitivity, measured with standard automated perimetry compared with age-matched healthy controls.133 In another study of 124 patients, the AHI correlated negatively with the nasal retinal nerve fibre layer thickness (measured by optical coherence tomography) after adjustment.134

In Patients with Type 2 Diabetes
Similar to DN, several studies examined the relationship between OSA and DR but they were all cross-sectional, except for one longitudinal study. In Japanese patients undergoing vitreous surgery for advanced diabetic retinopathy (DR), lower oxygen saturations were associated with proliferative DR after adjustment for age, glycated haemoglobin (HbA1c) and hypertension.135 In a study from the UK, OSA was independently associated with DR and maculopathy after adjusting for age, BMI, diabetes duration and hypertension in men with T2D.136 Similarly, in another study from the UK, patients with OSA were three to four times more likely to have sight-threatening DR, pre-proliferative/proliferative DR or maculopathy, after adjustment for a wide range of confounders including gender and ethnicity.137

Longitudinally, patients with OSA were more likely to develop preproliferative/ proliferative DR (adjusted OR 6.6, 95 % CI 1.2–35.1;p=0.03); patients who were compliant with CPAP treatment had lower progression to pre-proliferative/proliferative DR compared with noncomplaint patients.137

Minimum nocturnal oxygen saturations were also associated with DR/ maculopathy independent of potential confounders in cross-sectional studies.138,139 An interesting study of patients receiving anti-VEGF treatment for diabetic and age-related macular oedema (n=103) showed patients with poor response to treatment had a significantly higher risk of OSA compared with age-matched controls.140 Whether OSA contributed to the lack of efficacy of anti-vascular endothelial growth factor (VEGF) treatment is unclear.

In a proof of concept uncontrolled, hypothesis-generating study, CPAP treatment for 6 months was associated with improvement in visual acuity without an impact on macular oedema/thickness, suggesting improved functionality, rather than actual change in the oedema.141

The studies are suggestive of an association between OSA and DR; however, whether this association is with the development or the progression of DR is unclear. It is plausible that OSA is mainly associated with the progression rather than the development of DR; studies from the general population showed that OSA did not result in retinal changes similar to those observed in diabetes. Hence, while the development of DR is primarily dependent on the presence of hyperglycaemia, the progression of DR might be associated with OSA. Further longitudinal studies and interventional trials are needed to assess the impact of OSA on DR.

Obstructive Sleep Apnoea and Neuropathy
OSA and nocturnal hypoxia have been associated with the development of peripheral neuropathy in three small studies that included a small number of participants (n<40). In a case-control study, patients with severe OSA (AHI >30 events/hour) had worse parameters (amplitude and velocity) during nerve conduction studies compared with age-matched controls.142 In another study, the prevalence of possible polyneuropathy was much higher in OSA patients (AHI ≥10 events/hour) than that in age and BMI matched controls (71 % versus 33 %; p<0.05).143 In addition, the amplitudes of the sensory nerve action potentials were significantly smaller in the OSA group.143
One small uncontrolled study of CPAP for 6 months showed that OSA was associated with axonal dysfunction of the peripheral sensory nerves and that CPAP improved the amplitude of action potentials.144
A cross-sectional study found that patients with OSA and T2D were more likely to have DN (OR 2.82, 95 % CI 1.44–5.52) and foot insensitivity (OR 3.97, 95 % CI 1.80–8.74 ) compared with those with T2D but without OSA after adjustment for a large number of potential confounders.86

Obstructive Sleep Apnoea and Erectile Dysfunction

Erectile dysfunction has been recognised as a risk factor for CVD in patients with145 and without T2D.146 In addition, many CVD risk factors are known to cause erectile dysfunction.147 OSA and erectile dysfunction share many risk factors such as older age, obesity and T2D among others and hence it is not surprising that OSA is common in patients with erectile dysfunction and vice versa.147 Several population- and clinic-based studies showed that erectile dysfunction was associated with OSA and that erectile dysfunction severity was associated with the severity of OSA and the nocturnal hypoxaemia.147 Many of these studies used less than gold standard methods to assess erectile dysfunction including self-reported outcomes.147
However, the causality between OSA and erectile dysfunction cannot be proved due to the lack of longitudinal studies and the lack of convincing data from RCTs.147

Impact of Continuous Positive Airway Pressure
In one small RCT (n=27), 1 month of CPAP improved erectile function (assessed by the 5 item international index of erectile function) compared with the control group;148 but the control group in this study was no treatment rather than sham CPAP and hence it is difficult to draw conclusions as the study outcome was self-reported and the study was not blinded.147 Other uncontrolled and observational studies suggested beneficial effects of CPAP on erectile dysfunction. However, RCTs comparing the effect of CPAP to sildenafil showed that both improved erectile function but sildenafil was superior.147,149–151

There are no RCTs that assessed the impact of CPAP on erectile dysfunction in patients with T2D but one uncontrolled study showed that CPAP for 3 months had no effect on sexual function in 35 men with T2D.152

Obstructive Sleep Apnoea and Quality of
Life Several studies found a cross-sectional association between OSA, OSA severity and worse health-related quality of life (QOL).153 In the Wisconsin Sleep Cohort Study and the Sleep Heart Health Study, there was a linear association of OSA severity with decrements on the eight Short Form 36 (SF-36) scales.87 In another study, patients with OSA had significantly lower SF-36 scores compared with controls; nocturnal hypoxaemia and the ESS were independent factors for predicting the total score on the SF-36.154 In a recent study, undiagnosed OSA was associated with impairments in QOL independent of sleepiness and OSA-related comorbidities in men aged <69 years, but not in those ≥70 years old.155

In an uncontrolled clinical trial, OSA was associated with impaired QOL (based on SF-36) and 8 weeks of CPAP improved vitality, social functioning and mental health.156 The magnitude of improvement was related to the baseline QOL impairment rather than OSA severity.156 Another study found similar results in that 6 months of CPAP improved physical health, levels of independence and psychological health using the World Health Organization QOL questionnaire.157 However, a recent study found that the improvement in QOL following starting CPAP was similar in those who were compliant with treatment versus patients who were not treatment compliant.158

Summary and Conclusions
OSA is associated with several vascular risk factors including hypertension, albuminuria, IR, hyperlipidaemia, erectile dysfunction, increased inflammation and endothelial dysfunction. Large epidemiological studies have shown that OSA is associated with increased CVD and that CPAP might reduce CVD events, but evidence from RCTs is generally lacking. OSA has also been associated with chronic kidney disease and neuropathy. OSA is common in patients with T2D and, hence, understanding the impact of OSA on diabetes-related vascular complications is important considering the significant burden of these complications. In patients with T2D, a limited number of studies showed that OSA is associated with several vascular risk factors such as hypertension, IR and endothelial dysfunction. Emerging evidence also suggest that OSA is associated with CVD and diabetes-related microvascular complications including neuropathy, retinopathy and nephropathy in patients with T2D; however, the majority of these studies were cross-sectional and interventional studies are lacking. However, the limited number of prospective studies suggest a link between OSA and the development of CAD, heart failure and CKD and the progression of DR. Hence, clinicians should consider screening for OSA due to this high prevalence of diabetes and potential contribution to vascular disease, but there is a need to conduct larger longitudinal studies and adequately powered well-designed RCTs to further understand the role of OSA in the pathogenesis and treatment of CVD and diabetes-related microvascular complications.

Article Information:
Disclosure

Abd A Tahrani is a clinician scientist supported by the National Institute for Health Research (NIHR) in the UK. The views expressed in this publication are those of the author and not necessarily those of the National Health Service, the NIHR or the Department of Health. No funding was received for the publication of this article.

Correspondence

Abd A Tahrani, Department of Diabetes and Endocrinology, Birmingham Heartlands Hospital, Birmingham B9 5SS, UK. E: Abd.Tahrani@nhs.net

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This article is published under the Creative Commons Attribution Noncommercial License, which permits any non-commercial use, distribution, adaptation and reproduction provided the original author(s) and source are given appropriate credit.

Received

2015-07-01T00:00:00

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