Leg Atherosclerosis in Japanese COPD Patients: Prevalence of Undiagnosed Peripheral Artery Disease and Association between Leg Atherosclerosis and Clinical Indices

doi:10.4236/ojrd.2013.31005

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Open Journal of Respiratory Diseases, 2013, 3, 25-30

http://dx.doi.org/10.4236/ojrd.2013.31005 Published Online February 2013 (http://www.scirp.org/journal/ojrd)

Leg Atherosclerosis in Japanese COPD Patients:

Prevalence of Undiagnosed Peripheral Artery Disease

and Association between Leg Atherosclerosis and

Clinical Indices

Hirofumi Matsuoka, Yusuke Matsumoto, Kengo Kimura, Midori Koyama,

Towa Uzu, Yasuko Koma, Kensuke Fukumitsu, Yoshitaka Kasai,

Nariyasu Nakashima, Daiki Masuya, Harukazu Yoshimatsu, Yujiro Suzuki

Department of Respiratory Medicine, Shinko Hospital, Kobe, Japan

Email: h-matsuoka@shinkohp.or.jp

Received September 25, 2012; revised October 28, 2012; accepted November 7, 2012

ABSTRACT

Introduction: Several studies have suggested that decreased FEV1 is associated with cardiovascular risk in COPD pa-

tients. Objective: To identify the prevalence of undiagnosed peripheral artery disease (PAD) and the relationship be-

tween leg atherosclerosis and clinical indices, which predict COPD mortality in Japanese COPD patients. Methods: We

performed a cross-sectional study in 51 COPD patients and 51 age-matched, healthy control smokers. We measured

ankle-brachial index (ABI) as a marker of atherosclerosis of the legs, pulmonary function, body mass index, modified

Medical Research Council (MMRC) dyspnea scale, and smoking pack-years. We also calculated the ADO index (Age,

Dyspnea, and Obstruction), an established predictor of mortality in COPD patients. Co-morbidities including diabetes

mellitus, hypertension, and hypercholesterolemia were identified from blood laboratory tests and medical records. Re-

sults: Five subjects (9.8%) had an ABI < 0.9. ABI was significantly lower in the COPD patients than in the healthy

control smokers (p < 0.05). The prevalence of PAD was marginally higher in COPD patients than in control smokers (p

= 0.09), with the prevalence of ABI < 1.0 being significantly higher in COPD patients than in control smokers (p =

0.04). In the COPD patients, ABI showed significant correlations with age (p = 0.006), FEV1 (p = 0.004), smoking

pack-years (p = 0.047), MMRC dyspnea scale (p = 0.0005), SaO2 (p = 0.001), and ADO index (p < 0.001). Multiple

linear regression modeling showed the factors associated independently with ABI were age, FEV1, smoking pack-years,

MMRC dyspnea scale, and SaO2. Conclusion: The risk of leg atherosclerosis in Japanese COPD patients is higher than

in smokers without COPD. Leg atherosclerosis in COPD patients is associated with clinical indices that predict COPD

mortality.

Keywords: COPD; Peripheral Artery Disease; Leg Atherosclerosis; Ankle-Brachial Index

1. Introduction

Tobacco smoking is the most important risk factor for

both the development and progression of COPD. Chronic

obstructive pulmonary disease (COPD) is the fourth lead-

ing cause of death worldwide [1]. Recently, COPD has

been recognized as a systemic disease [2,3], and in par-

ticular, is associated with a markedly increased risk of

cardiovascular disease [4], which accounts for approxi-

mately 25% to 40% of mortality in COPD patients [5,6].

OPD is characterized by chronic airflow limitation re-

sulting from an excessive inflammatory response of the

lungs to cigarette smoking [7], an established risk factor

for cardiovascular disease. However, recent studies have

also shown that COPD is associated with cardiovascular

risk independent of classical risk factors [8-10]. Further-

more, several studies have demonstrated that atheroscle-

rosis is associated with FEV1 [11-14]. These findings in-

dicate that the severity of COPD is associated with athe-

rosclerosis.

Peripheral arterial disease (PAD) is a manifestation of

systemic atherosclerosis, and is a common disorder asso-

ciated with a very high risk of myocardial infarction, is-

chemic stroke, and death [15]. The prognosis of patients

with lower extremity PAD is characterized by an increa-

sed risk for cardiovascular ischemic events due to con-

comitant coronary artery disease and cerebrovascular

disease [16,17]. There is evidence that these cardiovas-

cular ischemic events are more frequent than ischemic

limb events in cohorts of patients with lower extremity

H. MATSUOKA ET AL.

PAD [18]. Lower extremity PAD should therefore be con-

sidered as a sign of potentially diffuse and significant ar-

terial disease [15].

Several studies have reported that the rate of cardio-

vascular death in the smoking population in Japan is

lower than in other developed countries [19,20]. How-

ever, there are no data comparing the prevalence of PAD

in COPD patients and healthy smokers in the Japanese

population, and only limited data on the relationship be-

tween leg atherosclerosis and clinical indices in COPD

patients.

2. Method

2.1. Subjects Studied

Subjects with COPD with a smoking history and age-

matched control smokers were recruited from an outpa-

tient clinic at Shinko Hospital. The control smokers with-

out COPD were recruited from individuals treated at our

hospital for chronic bronchitis without lung function ab-

normalities, or for health status check-ups. Control smok-

ers were ex-smokers or current smokers without lung func-

tion abnormalities. An age-matched (within 1 year) con-

trol smoker was selected randomly for each subject with

COPD. Subjects with a history of respiratory infection

within the previous 4 weeks, asthma, or active malignan-

cy were not included in the study. Cardiovascular comor-

bidity was recorded carefully. Patients already diagnosed

with PAD were excluded from the study.

Body mass index (BMI) was calculated as weight (in

kilograms) divided by height squared (in meters). Hyper-

tension was defined as either a systolic blood pressure ≧

140 mmHg, diastolic blood pressure ≧ 90 mmHg, or

self-reported use of antihypertensive medication. Diabe-

tes mellitus was defined as either a fasting glucose level

≧ 126 mg/dl, a non-fasting glucose level ≧ 200 mg/dl,

a self-reported physician diagnosis, or pharmacologic hy-

poglycemic treatment. Subjects with a low-density lipo-

protein (LDL)-cholesterol level ≧ 140 mg/dl or using li-

pid-lowering drugs were considered to have hypercholes-

terolemia. The subjects also completed a medical history

that included questions about their current smoking status

and history.

Spirometry was performed on all subjects using a com-

puted spirometer (CHESTAC-8800, CHEST M. I., Inc.,

Tokyo, Japan). The protocol for the lung function mea-

surements conformed to the recommendations of the Ame-

rican Thoracic Society [21]. This study was approved by

the Ethics Committee of Shinko Hospital, and informed

consent was obtained from all subjects prior to enroll-

ment.

2.2. Ankle-Brachial Index

The ABI is calculated as the ratio of ankle to arm systolic

blood pressure and is used commonly in clinical practice

to assess lower extremity PAD [15]. In all cases, the sub-

jects rested in the supine position for 5 min before meas-

urement of ABI. Using appropriately sized blood pres-

sure cuffs, systolic blood pressure was measured in both

brachial arteries and both leg arteries using an automated

device. All measurements were performed by staff in a

blinded manner. We used the measurement from the leg

with the lower ABI in the analyses.

2.3. Clinical Evaluation

Patients completed the modified Medical Research Coun-

cil dyspnea scale (MMRC) questionnaire [22]. The ADO

index is calculated using age, MMRC, and FEV1, and is a

better predictor of mortality from COPD than the tradi-

tional BODE index [23]. The ADO score ranges from 0

to 10 points, with higher scores indicating higher morta-

lity.

2.4. Statistical Analysis

JMP software (SAS Institute Inc., Cary, NC, USA) was

used for the analyses. The results are presented as mean

(SEM) or number (percentage). Differences between the

COPD patients and control smokers were compared us-

ing unpaired Student’s t-tests for continuous variables

and χ2-tests for categorical data. Spearman’s rank test

was used to examine correlations between the variables.

Multivariate linear regression was performed using each

parameter as a dependent variable in order to determine

the independent predictors of ABI. Due to the strong as-

sociation between age and SaO2, these variables were in-

cluded in separate models as candidate variables. P-va-

lues < 0.05 were considered statistically significant.

3. Results

3.1. Subject Characteristics

The characteristics of the subjects are shown in Table 1.

The mean age of the COPD subjects was 72.4 years. The

prevalence of ABI < 0.9 was marginally higher in the

COPD group than in the control group (9.8% vs 2.0%, p

= 0.092). The prevalence of ABI < 1.0 was significantly

higher in the COPD group than in the control group

(19.6% vs 5.9%, p = 0.037). FEV1, BMI, and ABI were

significantly lower in the COPD subjects compared to

the control smokers (all p < 0.05). Age, gender, smoking

status and pack-year histories, and prevalence of comor-

bidities were similar between the two groups.

The association of ABI with cardiovascular risk factors

and clinical indices

In the COPD patients, ABI correlated significantly

with age (r = −0.37, p = 0.006), FEV1 (r = 0.28, p =

0.004), smoking pack-years (r = −0.28, p = 0.047),

H. MATSUOKA ET AL. 27

Table 1. Characteristics of the subjects.

Control smoker

(n = 51) COPD (n = 51)P-value

Age (yr) 72.1 (7.4) 72.4 (6.8) 0.76

Male gender, n (%) 45 (88.2) 44 (84.6) 0.56

Current smokers, n (%) 15 (30.0) 8 (15.7) 0.084

Pack-years 55.9 (31.6) 60.0(34.5) 0.66

FEV1 (%) 95.4 (19.1) 47.2 (20.4) <0.001

BMI (kg/m2) 23.8 (3.4) 21.8 (3.5) 0.0042

ABI 1.13 (0.1) 1.07 (0.1) 0.0054

ABI < 0.9

ABI < 1.1

1 (2.0)

3 (5.9)

5 (9.8)

10 (19.6)

0.092

0.037

Comorbidity, n (%)

Hypertension 14 (27.5) 19 (37.3) 0.29

Diabetes mellitus 8 (15.7) 4 (7.8) 0.22

Hypercholesterolemia 13 (25.5) 7 (13.7) 0.075

Ischemic heart disease 7 (13.7) 3 (5.9) 0.19

Values are expressed as mean (SD) unless stated otherwise.

MMRC dyspnea scale (r = −0.47, p = 0.0005), resting

SaO2 (r = 0.45, p = 0.001) (Table 2), and ADO index (r =

−0.51, p < 0.001) (Figure 1). There were no associations

between ABI and BMI, smoking status, prevalence of

comorbidities, or history of ischemic heart disease (Table

3).

Multiple linear regression modeling, after adjustment

for age, FEV1, smoking pack-years, and MMRC dyspnea

scale, showed that age (p = 0.0046), FEV1 (p = 0.027),

smoking pack-years (p = 0.0018), and MMRC dyspnea

scale (p = 0.023) were independent factors associated

significantly with ABI (Table 4 (a)). Adjustment for SaO2,

FEV1, smoking pack-years, and MMRC dyspnea scale,

showed that SaO2 (p = 0.037), smoking pack-years (p =

0.037), and MMRC dyspnea scale (p = 0.013) were sig-

nificant independent determinants of ABI (Table 4 (b)).

4. Discussion

In this study we showed that the prevalence of undiag-

nosed PAD was approximately 10% in Japanese COPD

patients, a rate marginally higher than that of age-ma-

tched healthy control smokers. ABI in COPD patients

was lower than in healthy smokers. Age, MMRC, FEV1,

smoking pack-years, and SaO2 were associated with ABI

in COPD patients. There was also a negative correlation

between ABI and the ADO index, which predicts COPD

mortality. To our knowledge, this is the first report on the

prevalence of undiagnosed PAD in Japanese COPD pa-

tients and also the relationship between ABI and clinical-

Table 2. Association between continuous variables and ABI

analyzed by spearman’s rank test.

r p

Age −0.37 0.006

FEV1 0.28 0.004

BMI 0.079 0.58

Pack-years −0.28 0.047

MMRC −0.47 0.0005

SaO2 0.45 0.001

Table 3. Mean difference in ABI between the dichotomous

groups.

Current smoking 0.053 0.18

Hypertension 0.0077 0.30

Hyperlipidemia 0.046 0.79

Diabetes mellitus 0.0027 0.96

Ischemic heart disease 0.074 0.25

Table 4. Multiple linear regression of ABI. (a) Adjusted for

age, FEV1, pack-years, and MMRC; (b) Adjusted for SaO2,

FEV1, pack-years, and MMRC.

(a)

OR 95% CI p

Age 0.999 0.991 - 0.998 0.0046

FEV1 1.001 1.000 - 1.003 0.027

Pack-years 0.998 0.998 - 0.999 0.0018

MMRC 0.977 0.958 - 0.996 0.023

(b)

OR 95% CI p

SaO2 1.016 1.001 - 1.031 0.037

FEV1 1.000 0.999 - 1.072 0.34

Pack-years 0.999 0.998 - 0.999 0.037

MMRC 0.973 0.953 - 0.993 0.013

indices associated with COPD mortality.

Approximately 10% of COPD patients in this study

had an ABI < 0.9. There are only limited published data

on the prevalence of lower extremity PAD in COPD pa-

tients. A high prevalence of lower extremity PAD in

COPD patients was reported in a study from France, that

showed 123 of 151 (81.4%) of patients with moderate-

to-severe COPD had pathological ABI values (ABI < 0.9)

[24]. On the basis of the findings of the present study it

appears that the prevalence of lower extremity PAD in

COPD patients in Japan may be lower than that in pa-

tients in Europe. One reason for this result may be that

we excluded subjects who had already been diagnosed

with PAD. Another reason may be that the prevalence of

H. MATSUOKA ET AL.

Figure 1. Association between ABI and ADO index. ABI

showed a significant and negative correlation with ADO in-

dex (r = −0.51, p = 0.0001).

PAD is low in both COPD patients and the general popu-

lation in Japan compared with other developed countries.

Several studies have also reported that the rate of car-

diovascular death in the smoking population and PAD

patients is lower in Japan than in other developed coun-

tries [19,20,25,26]. However, in this study, the preva-

lence of PAD in COPD patients tended to be high, with

the proportion of subjects with an ABI < 1.1 being sig-

nificantly greater than in control subjects. Fowkes et al.

demonstrated that subjects with an ABI 0.91 to 1.10 had

higher mortality and cardiovascular event rates than those

with a normal ABI [27]. Therefore, as in other countries,

attention should be paid to the risk of cardiovascular dis-

eases in Japanese COPD patients.

Recent studies have demonstrated that atherosclerosis

is associated with FEV1 [11-14]. In the Atherosclerosis

Risk in Communities (ARIC) Study, decreased FEV1 was

associated with decreased ABI in smoking subjects even

after adjustment for cardiovascular risk factors [12]. Iwa-

moto et al. [14], measured the carotid intima-media thick-

ness and focal atheromatous plaque as indicators of sub-

clinical atherosclerosis in patients with airflow limitation

and control smokers. They showed that mean carotid in-

tima-media thickness was greater in patients with an air-

flow limitation than in the controls. Furthermore, their

data showed significant associations between thickened

intima-media thickness and decreased FEV1. Although

the mechanism for these associations was unclear, it is

possible hypoxia occurring in the later stages of COPD

may have induced an abnormal inflammatory response,

reflected by increased CRP [28] and oxidative stress [29].

In our study, resting SaO2 showed a significant and posi-

tive correlation with ABI, and was an independent deter-

minant of ABI. This finding indicates that hypoxia may

contribute to atherosclerosis in COPD patients. Further

studies are required to conclusively determine the mecha-

nisms of these interactions.

We also showed that MMRC was associated with ABI.

The severity of dyspnea has been shown to be a better

predictor of mortality in COPD than airway obstruction

[20]. COPD patients with the most severe dyspnea were

shown to be more likely to die than those with only mild

dyspnea [20]. A low ABI is a predictor of systemic athe-

rosclerosis and risk of cardiovascular events [27]. Eng-

strom et al. reported that reduced FEV1 was associated

with an increased incidence of hospitalizations due to

heart failure [30]. Therefore, not only poor lung function,

but also impaired cardiac function may contribute to dys-

pnea in patients with a low ABI.

In this study, the presence of cardiac risk factors (hy-

pertension, diabetes mellitus, and hypercholesterolemia)

was not associated with ABI. One reason for this result

may be that the prevalence of these diseases was low in

COPD subjects in this study.

In the present study the ADO index correlated better

with ABI than either age, FEV1, or MMRC. The ADO in-

dex is a multidimensional index developed by Puhan et

al. [23] that incorporates age, dyspnea, and airflow ob-

struction. The index predicts 3-year mortality from COPD

more accurately than the BODE index, which is currently

used to estimate a patient’s risk of death from COPD.

There is evidence that both these multidimensional indi-

ces predict survival better than FEV1 alone [31]. Several

studies have shown that airflow limitation is an inde-

pendent risk factor for cardiovascular disease. However,

there is no established threshold for the relationship be-

tween cardiovascular risk and FEV1. In this study all

patients with an ABI < 0.9 had an ADO index score of 5

points or greater. This result suggests that the ADO index

has the ability to predict cardiovascular risk in COPD

patients. A study in a large number of subjects is required

to determine the cut-off point of the ADO index for

screening cardiovascular disease in COPD patients.

Coronary and cerebrovascular diseases frequently co-

exist in PAD patients [15]. There is an approximately 2-

to 4-fold excess of cardiovascular disease in patients with

lower extremity PAD [16,17]. The prognosis of patients

with lower extremity PAD is characterized by an in-

creased risk for cardiovascular ischemic events due to

concomitant coronary artery disease and cerebrovascular

disease [16,17]. These cardiovascular ischemic events are

more frequent than ischemic limb events in any cohort of

patients with lower extremity PAD [18]. Lower extremity

arterial disease should therefore also be viewed as a sign

of potentially diffuse and significant arterial disease [15].

Measurement of ABI may be useful for identifying pa-

tients at high risk who may benefit from aggressive the-

rapeutic intervention [32-35]. The guidelines of the Ame-

H. MATSUOKA ET AL. 29

rican College of Cardiology (ACC) and American Heart

Association (AHA) for the management of patients with

PAD recommends that ABI should be considered as a

routine test for all patients who are 49 years of age and

younger with a history of diabetes and 1 other risk factor,

those 50 to 69 years of age with a history of smoking or

diabetes, and those aged 70 years or older [15]. In accor-

dance with these guidelines the majority of COPD pa-

tients should have ABI measured.

There were some limitations in this study. The number

of subjects was small and therefore a study on a larger

number of subjects is needed to conclusively establish

the prevalence of PAD in COPD subjects. Although some

studies have reported an association between atheroscle-

rosis and nocturnal hypoxia [36], the current study did not

evaluate this relationship.

5. Conclusion

In this study we showed that the rate of atherosclerosis in

COPD patients in Japan was lower than in similar pa-

tients in other developed countries. However, we showed

the rate of atherosclerosis in COPD patients was higher

than in healthy smokers, with this finding being consis-

tent to data of other countries. Leg atherosclerosis was

also shown to be associated with clinical indices related

to COPD mortality. It is therefore important that more

attention is paid to leg atherosclerosis in Japanese COPD

patients.

6. Acknowledgements

We thank Masahiro Motoki, Takanori Matsutani, Taka-

hiko Ando, Kaori Tai, Megumi Sakano, Nanae Kiyokawa,

and Kanako Ichimaru of the clinical laboratory of Shinko

Hospital for carrying out the pulmonary function tests

and measuring ABI.

REFERENCES

[1] C. J. Murray and A. D. Lopez, “Global Mortality, Dis-

ability, and the Contribution of Risk Factors: Global Bur-

den of Disease Study,” Lancet, Vol. 349, No. 9063, 1997,

pp. 1436-1442. doi:10.1016/S0140-6736(96)07495-8

[2] L. M. Fabbri, F. Luppi, B. Beghe, et al., “Complex Chro-

nic Comorbidities of COPD,” European Respiratory Jour-

nal, Vol. 31, No. 1, 2008, pp. 204-212.

doi:10.1183/09031936.00114307

[3] J. D. Maclay, D. A. McAllister and W. Macnee, “Cardio-

vascular Risk in Chronic Obstructive Pulmonary Disea-

se,” Respirology, Vol. 12, No. 5, 2007, pp. 634-641.

doi:10.1111/j.1440-1843.2007.01136.x

[4] D. D. Sin and S. F. Man, “Chronic Obstructive Pulmona-

ry Disease as a Risk Factor for Cardiovascular Morbidity

and Mortality,” Proceedings of the American Thoracic

Society, Vol. 2, No. 1, 2005, pp. 8-11.

doi:10.1513/pats.200404-032MS

[5] P. M. Calverley, J. A. Anderson, B. Celli, et al., “Salme-

terol and Fluticasone Propionate and Survival in Chronic

Obstructive Pulmonary Disease,” The New England Jour-

nal of Medicine, Vol. 356, No. 8, 2007, pp. 775-789.

doi:10.1056/NEJMoa063070

[6] R. A. Pauwels, C. G. Lofdahl, L. A. Laitinen, et al., “Long-

Term Treatment with Inhaled Budesonide in Persons with

Mild Chronic Obstructive Pulmonary Disease Who Con-

tinue Smoking,” The New England Journal of Medicine,

Vol. 340, No. 25, 1999, pp. 1948-1953.

doi:10.1056/NEJM199906243402503

[7] W. MacNee, “Pathogenesis of Chronic Obstructive Pul-

monary Disease,” Proceedings of the American Thoracic

Society, Vol. 2, No. 4, 2005, pp. 258-266.

doi:10.1513/pats.200504-045SR

[8] H. J. Schunemann, J. Dorn, B. J. Grant, et al., “Pulmo-

nary Function Is a Long-Term Predictor of Mortality in

the General Population: 29-Year Follow-Up of the Buf-

falo Health Study,” Chest, Vol. 118, No. 3, 2000, pp.

656-664. doi:10.1378/chest.118.3.656

[9] D. D. Sin, L. Wu and S. F. Man, “The Relationship Be-

tween Reduced Lung Function and Cardiovascular Mor-

tality: A Population-Based Study and a Systematic Re-

view of the Literature,” Chest, Vol. 127, No. 6, 2005, pp.

1952-1959. doi:10.1378/chest.127.6.1952

[10] S. M. Curkendall, C. DeLuise, J. K. Jones, et al., “Car-

diovascular Disease in Patients with Chronic Obstructive

Pulmonary Disease, Saskatchewan Canada Cardiovascu-

lar Disease in COPD Patients,” Annals of Epidemiology,

Vol. 16, No. 1, 2006, pp. 63-70.

doi:10.1016/j.annepidem.2005.04.008

[11] M. Zureik, A. Benetos, C. Neukirch, et al., “Reduced Pul-

monary Function Is Associated with Central Arterial Stiff-

ness in Men,” American Journal of Respiratory and Criti-

cal Care Medicine, Vol. 164, No. 12, 2001, pp. 2181-2185.

[12] E. B. Schroeder, V. L. Welch, G. W. Evans, et al., “Im-

paired Lung Function and Subclinical Atherosclerosis.

The ARIC Study,” Atherosclerosis, Vol. 180, No. 2, 2005,

pp. 367-373. doi:10.1016/j.atherosclerosis.2004.12.012

[13] D. A. McAllister, J. D. Maclay, N. L. Mills, et al., “Arte-

rial Stiffness Is Independently Associated with Emphy-

sema Severity in Patients with Chronic Obstructive Pul-

monary Disease,” American Journal of Respiratory and

Critical Care Medicine, Vol. 176, No. 12, 2007, pp.

1208-1214. doi:10.1164/rccm.200707-1080OC

[14] H. Iwamoto, A. Yokoyama, Y. Kitahara, et al., “Airflow

Limitation in Smokers Is Associated with Subclinical

Atherosclerosis,” American Journal of Respiratory and

Critical Care Medicine, Vol. 179, No. 1, 2009, pp. 35-40.

doi:10.1164/rccm.200804-560OC

[15] A. T. Hirsch, Z. J. Haskal, N. R. Hertzer, et al., “ACC/

AHA 2005 Practice Guidelines for the Management of

Patients with Peripheral Arterial Disease (Lower Extremi-

ty, Renal, Mesenteric, and Abdominal Aortic): A Col-

laborative Report from the American Association for Va-

scular Surgery/Society for Vascular Surgery, Society for

Cardiovascular Angiography and Interventions, Society

for Vascular Medicine and Biology, Society of Interven-

H. MATSUOKA ET AL.

tional Radiology, and the ACC/AHA Task Force on Prac-

tice Guidelines (Writing Committee to Develop,” Circu-

lation, Vol. 113, No. 11, 2006, pp. e463-e654.

[16] M. H. Criqui, J. O. Denenberg, R. D. Langer, et al., “The

Epidemiology of Peripheral Arterial Disease: Importance

of Identifying the Population at Risk,” Vascular Medicine,

Vol. 2, No. 3, 1997, pp. 221-226.

[17] J. Ness, W. S. Aronow, “Prevalence of Coexistence of

Coronary Artery Disease, Ischemic Stroke, and Peripheral

Arterial Disease in Older Persons, Mean Age 80 Years, in

an Academic Hospital-Based Geriatrics Practice,” Jour-

nal of the American Geriatrics Society, Vol. 47, No. 10,

1999, pp. 1255-1256.

[18] J. I. Weitz, J. Byrne, G. P. Clagett, et al., “Diagnosis and

Treatment of Chronic Arterial Insufficiency of the Lower

Extremities: A Critical Review,” Circulation, Vol. 94, No.

11, 1996, pp. 3026-3049. doi:10.1161/01.CIR.94.11.3026

[19] D. R. Jacobs Jr., H. Adachi, I. Mulder, et al., “Cigarette

Smoking and Mortality Risk: Twenty-Five-Year Follow-

Up of the Seven Countries Study,” The Archives of In-

ternal Medicine, Vol. 159, No. 7, 1999, pp. 733-740.

doi:10.1001/archinte.159.7.733

[20] K. Nishimura, T. Izumi, M. Tsukino, et al., “Dyspnea Is a

Better Predictor of 5-Year Survival than Airway Obstruc-

tion in Patients with COPD,” Chest, Vol. 121, No. 5, 2002,

pp. 1434-1440. doi:10.1378/chest.121.5.1434

[21] American Thoracic Society, “Standardization of Spi-

rometry,” American Journal of Respiratory and Critical

Care Medicine, Vol. 152, No. 3, 1995, pp. 1107-1136.

[22] D. A. Mahler, C. K. Wells, Evaluation of Clinical Meth-

ods for Rating Dyspnea,” Chest, Vol. 93, No. 3, 1988, pp.

580-586. doi:10.1378/chest.93.3.580

[23] M. A. Puhan, J. Garcia-Aymerich, M. Frey, et al., “Ex-

pansion of the Prognostic Assessment of Patients with Chro-

nic Obstructive Pulmonary Disease: The Updated BODE

Index and the ADO Index,” Lancet, Vol. 374, No. 9691,

2009, pp. 704-711. doi:10.1016/S0140-6736(09)61301-5

[24] O. Castagna, A. Boussuges, E. Nussbaum, et al., “Pe-

ripheral Arterial Disease: An Underestimated Aetiology

of Exercise Intolerance in Chronic Obstructive Pulmonary

Disease Patients,” European Journal of Cardiovascular

Prevention & Rehabilitation, Vol. 15, No. 3, 2008, pp.

270-277. doi:10.1097/HJR.0b013e3282f009a9

[25] T. Fujiwara, S. Saitoh, et al., “Prevalence of Asymptoma-

tic Arteriosclerosis Obliterans and Its Relationship with

Risk Factors in Inhabitants of Rural Communities in Ja-

pan: Tanno-Sobetsu study,” Atheroscle rosis, Vol. 177, No.

1, 2004, pp. 83-88.

[26] H. Ohnishi, Y. Sawayama, et al., “Risk Factors for and

the Prevalence of Peripheral Arterial Disease and Its Re-

lationship to Carotid Atherosclerosis: The Kyushu and Oki-

nawa Population Study (KOPS),” Journal of Atheroscle-

rosis and Thrombosis, Vol. 30, Vol. 17, 2010, pp. 751-758.

[27] F. G. Fowkes, G. D. Murray, I. Butcher, et al., “Ankle

Brachial Index Combined with Framingham Risk Score

to Predict Cardiovascular Events and Mortality: A Meta-

Analysis,” Journal of the American Medical Association,

Vol. 300, No. 2, 2008, pp. 197-208.

doi:10.1001/jama.300.2.197

[28] G. Hartmann, M. Tschop, R. Fischer, et al., “High Alti-

tude Increases Circulating Interleukin-6, Interleukin-1 Re-

ceptor Antagonist and C-Reactive Protein,” Cytoki ne, Vol.

12, No. 3, 2000, pp. 246-252. doi:10.1006/cyto.1999.0533

[29] V. Savransky, A. Nanayakkara, J. Li, et al., “Chronic

Intermittent Hypoxia Induces Atherosclerosis,” American

Journal of Respiratory and Critical Care Medicine, Vol.

175, No. 12, 2007, pp. 1290-1297.

doi:10.1164/rccm.200612-1771OC

[30] G. Engstrom, O. Melander, B. Hedblad, ‘Population-Ba-

sed Study of Lung Function and Incidence of Heart Fai-

lure Hospitalisations,” Thorax, Vol. 65, No. 7, 2010, pp.

633-638. doi:10.1136/thx.2010.135392

[31] B. R. Celli, C. G. Cote, J. M. Marin, et al., “The Body-

Mass Index, Airflow Obstruction, Dyspnea, and Exercise

Capacity Index in Chronic Obstructive Pulmonary Dis-

ease,” The New England Journal of Medicine, Vol. 350,

No. 10, 2004, pp. 1005-1012.

doi:10.1056/NEJMoa021322

[32] M. McKenna, S. Wolfson and L. Kuller, “The Ratio of

Ankle and Arm Arterial Pressure as an Independent Pre-

dictor of Mortality,” Atherosclero sis, Vol. 87, No. 2, 1991,

pp. 119-128. doi:10.1016/0021-9150(91)90014-T

[33] M. T. Vogt, M. McKenna, S. J. Anderson, et al., “The

Relationship between Ankle-Arm Index and Mortality in

Older Men and Women,” Journal of the American Geri-

atrics Society, Vol. 41, No. 5, 1993, pp. 523-530.

[34] G. C. Leng, F. G. Fowkes, A. J. Lee, et al., “Use of Ankle

Brachial Pressure Index to Predict Cardiovascular Events

and Death: A Cohort Study,” British Medical Journal,

Vol. 313, No. 7070, 1996, pp. 1440-1444.

doi:10.1136/bmj.313.7070.1440

[35] H. E. Resnick, R. S. Lindsay, M. M. McDermott, et al.,

“Relationship of High and Low Ankle Brachial Index to

All-Cause and Cardiovascular Disease Mortality: The

Strong Heart Study,” Circulation, Vol. 109, No. 6, 2004,

pp. 733-739. doi:10.1161/01.CIR.0000112642.63927.54

[36] R. Schulz, Seeger, et al., “Changes in Extracranial Arte-

ries in Obstructive Sleep Apnoea,” European Respiratory

Journal, Vol. 25, No. 1, 2005, pp. 69-74.

Abbreviations

COPD: Chronic Obstructive Pulmonary Disease

FEV1: Forced Expiratory Volume in one second

PAD: Peripheral Artery Disease

BI: Ankle-Brachial Index

BMI: Body Mass Index

MMRC: Modified Medical Research Council

SaO2: Arterial Oxygen Saturation

Ease of Use (Heading 2)