SciELO - Scientific Electronic Library Online

 
vol.25 número4Clozapina e Crises Epilépticas: Três Casos Clínicos e Revisão da LiteraturaA evolução do consumo do tabaco na áfrica subsariana índice de autoresíndice de assuntosPesquisa de artigos
Home Pagelista alfabética de periódicos  

Serviços Personalizados

Journal

Artigo

Indicadores

Links relacionados

  • Não possue artigos similaresSimilares em SciELO

Compartilhar


Arquivos de Medicina

versão On-line ISSN 2183-2447

Arq Med vol.25 no.4 Porto ago. 2011

 

ARTIGO DE REVISÃO

Clinical Epidemiology of Chronic Obstructive Pulmonary Disease

Epidemiologia clínica da doença pulmonar obstrutiva crónica

Joana Mascarenhas1,2,3, Paulo Bettencourt3,4, Ana Azevedo1,2,4,5

 

1 Departamento de Epidemiologia Clínica, Medicina Preditiva e Saúde Pública, Faculdade de Medicina da Universidade do Porto, Porto

2 Instituto de Saúde Pública da Universidade do Porto (ISPUP), Porto

3 Serviço de Medicina Interna, Hospital de São João, Porto

4 Unidade de Investigação e Desenvolvimento Cardiovascular do Porto, Porto

5 Centro de Investigação Clínica, Hospital de São João, Porto

 

Correspondência

 

ABSTRACT

Chronic obstructive pulmonary disease (COPD) is responsible for early morbidity and high mortality and significant costs to health systems. Smoking remains the main risk factor for COPD but additional factors, such as indoor and outdoor air pollution, occupational exposure and genetic susceptibility are increasingly recognized. The burden of COPD has been difficult to estimate owing to the multiple definitions applied, with variations between estimates of prevalence exceeding 15%. Definitions based on objective spirometric measurements have yielded higher prevalence estimates than patients’ self-report of a clinical diagnosis of COPD. Th e Global Initiative for Chronic Obstructive Lung Disease (GOLD) proposed a physiologic definition of COPD characterized by airflow limitation that is not fully reversible (post-bronchodilator FEV1/FVC < 0.70). Many authors have argued against this fixed ratio definition and advocate the use of a “lower limit of normal” criterion to define COPD in order to avoid overdiagnosis of the disease in the elderly. Despite controversies, the definition proposed by GOLD is unambiguous, easily remembered by clinicians, reproducible in different settings and suitable for cross-sites comparisons. Recently, two multinational studies adopted the GOLD definition to provide standardized population-based estimates of the prevalence of COPD in adults aged 40 years or over throughout the world. These estimates varied between 11.4 and 26.1% in the international BOLD study and between 2.6% and 7.1% in the five Latin American cities of the PLATINO study. Although debate on COPD definition is ongoing, the burden of the disease is high and growing. The major challenge in coming years will be to stop the smoking epidemic, particularly in developing countries, and to increase physician knowledge of the disease favouring an early diagnosis.

Palavras-chave: chronic obstructive pulmonary disease, spirometry, prevalence, burden

 

RESUMO

A nível mundial, a morbilidade e mortalidade atribuíveis à doença pulmonar obstrutiva crónica (DPOC) têm vindo a aumentar e, actualmente, esta doença assume-se como uma importante ameaça económica e social. O tabagismo é o factor de risco quantitativamente mais importante e a poluição interior e exterior, a exposição ocupacional e a susceptibilidade genética têm sido reconhecidos como factores de risco adicionais. A prevalência de DPOC a nível populacional tem sido difícil de estimar devido à utilização de múltiplas definições. A variação das estimativas de prevalência é superior a 15% e as definições baseadas na espirometria apontam para valores mais elevados do que a auto-declaração do diagnóstico prévio de doença. A Global Initiative for Chronic Obstructive Lung Disease (GOLD) propôs uma definição fisiológica da doença caracterizada por uma obstrução aérea não completamente reversível (FEV1/ FVC<70%, após broncodilatador). Criticando esta definição assente numa razão fixa, muitos autores advogam a utilização do critério baseado no “limite inferior do normal” para definir DPOC, na tentativa de diminuir o sobre diagnóstico nos idosos. Apesar da controvérsia, a definição proposta pelo GOLD é clara, fácil de memorizar, reprodutível em diferentes contextos e adequada para fazer comparações entre regiões. Esta definição foi recentemente adoptada por dois estudos multinacionais com o objectivo de obter estimativas padronizadas de base populacional em adultos com idade igual ou superior a 40 anos. As estimativas variaram entre 11,4 e 26,1% no estudo BOLD e entre 2,6 e 7,1% nas 5 cidades latino-americanas do estudo PLATINO. Independentemente do debate acerca da definição de DPOC, é indiscutível que a carga atribuível à doença é elevada e tem vindo a aumentar. No futuro, o principal desafio é combater a epidemia tabágica, em particular nos países em desenvolvimento, e promover o diagnóstico mais precoce por parte dos clínicos.

Key-words: doença pulmonar obstrutiva crónica, espirometria, prevalência

 

Introdução

Chronic obstructive pulmonary disease (COPD) is a major health problem throughout the world1, assuming epidemic proportions. It has been increasingly recognized as an important cause of premature death and disability, resulting in a tremendous economic and social burden2,3. In 2004, COPD was the fourth leading cause of death worldwide, accounting for 3.02 million deaths, 3.5% of the total in high-and low-income countries and 7.4% in middle-income countries4. During the same period, 1.9% of disability-adjusted life years (DALYs) were attributable to this condition5. Although a substantial proportion of COPD cases can be attributable to other exposures6, cigarette smoking is by far the most important causally-related risk factor for the disease in the western world and it is becoming a growing and widespread habit in developing countries7-9. Based on current trends10 and taking into account the expected aging of the world’s population11,12, the anticipated increases in smoking rate13 and the decline in competing causes of death, COPD is projected to be the third leading cause of death and to rank fifth in the global burden of disease in 20205,14 .

Currently, direct and indirect costs of COPD treatment and disability represent a major global threat to health care systems and economies15-17 . This scenario emphasizes that the implementation of preventive measures is an urgent public health priority, particularly in developing countries where an epidemiologic and demographic transition is ongoing very fast18. Reflecting the preventable and treatable nature of COPD, multiple guidelines on prevention and management of the disease have been published, aiming at improving awareness of disease and its risk factors, disseminating available treatment options for patients with established disease and encouraging continuous research in this area1,19,20. Despite these efforts, COPD is under diagnosed and under treated and estimates suggest that about one fifth of “healthy” adult smokers aged over 40 years actually have unrecognized disease21 .

Definition and classification of copd

COPD is a relatively new term for an old disease presenting with different phenotypes7,22. The definition of COPD recently proposed by the Global Initiative for Chronic Obstructive Lung Disease (GOLD)1 emerged from the need to unify several imprecise definitions that have proliferated over the years, based on different criteria. Historically, COPD has been defined clinically as chronic bronchitis and pathologically as emphysema7.More recently, a physiological definition based on spirometry has become consensual and is being increasingly used in epidemiological studies to objectively assess airflow limitation. The working definition established by GOLD and subsequently adopted by other international scientific societies20 states that COPD is “a preventable and treatable disease state with some significant extrapulmonary effects” and “its pulmonary component is characterized by airflow limitation that is not fully reversible.”1. Spirometry is considered the gold-standard for accurate and reproducible measurement of lung function and post-bronchodilator testing is essential to identify not fully reversible air flow obstruction and to classify disease severity1. According to currently adopted criteria, airflow limitation is defined as a post-bronchodilator forced expiratory volume in one second to forced vital capacity (FEV1/FVC) ratio lower than 70% and classification of COPD severity is based on the thresholds presented in Table 1. This “fixed” ratio criterion used to define obstruction is a generalized standard that has the advantage of allowing comparisons across different populations. Notwithstanding, considering the linear decline of FEV1/FVC ratio that normally occurs with age23,24, there is some concern that its use may led to overdiagnosis of COPD in healthy elderly individuals25-27. Conversely, young subjects with lung functional impairment could be under diagnosed28,29. Moreover, the specific spirometric cut-points applied to categorize stages of disease are used for simplicity and have not been clinically validated3, undoubtedly promoting some degree of misclassification.

 

 

To overcome these shortcomings and minimize misclassification of older and younger subjects, some experts have proposed the adoption of a “lower limit of normal” criterion (the bottom 5% of the normal distribution of FEV1/FVC in a healthy reference population) to define COPD30. This definition is currently considered in some guidelines32 but debate continues about whether this approach misclassifies as “normal” patients who are at increased risk for death and COPD-related hospitalization and who might benefit from treatment23. This risk is much higher among patients classified in GOLD stage II or above. Thus, besides being a practical threshold to identify clinically relevant disease, a FEV1 lower than 80% of predicted seems to convey some prognostic information23. The need of post-bronchodilator spirometry data to identify airflow limitation is another controversial issue related to disease classification. Strictly, GOLD criteria require the use of post-bronchodilator lung volumes because there is evidence that 20-30% of a population labeled as “obstructed” pre-bronchodilator will meet criteria of reversibility33,34. However, pre-bronchodilator spirometry is valuable in predicting mortality and morbidity outcomes in epidemiological studies34,35.The usefulness of looking at reversibility in epidemiological studies is still questioned by some authors arguing that there are no data supporting the superiority of post-bronchodilator lung function over pre-bronchodilator lung function inpredicting mortality and other adverse out comes15 .

Alternative classification schemes of COPD were suggested based on the acknowledgment of in-between phenotypes and manifestations of the disease, including increased airways reactivity, abnormal repair process, genetic factors, systemic involvement, distinctive response to infections and co-existence of co-morbid conditions15. This heterogeneity has motivated the emergence of multiple theories regarding the possible genesis of the disease and ultimately may provide opportunities for targeted interventions in selected patients7.

Although controversies in COPD definition, classification, staging and screening persist, it is generally agreed that, at the population level, good quality spirometry should be widely available and extensively performed to permit an accurate estimate of the disease burden36.This will affect resource allocation and planning of cost-effective strategies and interventions aiming at preventing the disease and modifying its natural course. Arguments apart, given the un availability of a definitive gold standard, it seems advisable to use the COPD definition proposed by GOLD since it is unambiguous, easy to re-member, reproducible in different settings and may serve as a guide to clinicians and as a standardized criterion valuable for population comparisons.

 

Prevalence of COPD

COPD is frequently unrecognized and a large proportion of available prevalence data probably underestimates the true burden of the disease3,37. In many instances, the disease becomes clinically apparent only when moderately advanced airflow obstruction is established, delaying the definite diagnosis36. Until recently, the interpretation of data regarding COPD burden has been impaired by the use of different methodologies to estimate its prevalence across different populations. Discrepancies interminology, definition and diagnostic criteria, methods of identifying cases, disease coding and analytical approaches have led to conflicting prevalence estimates, with variations exceeding 15%37. In addition, high-quality prevalence data were largely unavailable for regions outside Europe and North America38 .

The overlap between reported respiratory symptoms, diagnosed disease and impaired lung function is variable. Symptom-based diagnosis provided the highest estimates of COPD prevalence37. For example, in 1979, the Mini-Finland Health Survey reported a symptom-based COPD prevalence of 22.1% in men and 7.2% in women, whilst airflow obstruction was present in 11.0% of men and 5.2% of women39 . The inclusion of patients with chronic bronchitis but without spirometric obstruction accounted for the disagreement between estimates. Studies reporting prevalence data relying on a previous physician-diagnosed COPD provide the lowest estimates of the disease prevalence. In a semi-rural general practice in England, the overall prevalence of undiagnosed COPD was 6.2%, with 2.69 “true cases” of COPD beingdetectedforeachdiagnosedcase40. In theThird National Health and Nutrition Examination Survey (NHANES III), 24 million US adults had evidence of airflow obstruction, although, in the National Health Interview Survey, only about 10 million self-reported physician-diagnosed disease2. Recent epidemiological studies have adopted the criterion of airflow obstruction to provide accurate estimates of COPD prevalence. In NHANES III, the prevalence of pre-bronchodilator GOLD Stage I or higher among adults aged older than 17 years was 13.9%41 . A population survey conducted in Spain, using post-bronchodilator spirometric data, confirmed the diagnosis of COPD in 9.1% of the population aged between 40 and 69 years42. The European Community Respiratory Health Survey, conducted between 1991 and 1993, reported a prevalence of 3.6% for stage I or higher COPD among young adults aged 20 to 44 years43. It is noticeable that, even in these studies reporting objective lung function data, the measured prevalence was highly variable. Despite having used spirometry to quantify airflow obstruction, these estimates are undoubtedly influenced by the specific lung function parameters adopted to define COPD and bydistinct population demography,and comparisons should be made carefully.

Considering all the available data, definitions based on objective measurement of lung function tend to produce higher prevalence estimates than patients’ self-report of a clinical diagnosis of COPD38. In a recently published meta-analysis, providing the first quantitative summary of COPD prevalence, whereas spirometric criteria yielded prevalence estimates of about9-10%, a previous physician diagnosis of the disease was reported by less than 6% of subjects38. These numbers clearly reflect the low level of awareness of COPD, resulting in substantial under diagnosis and underreporting of the disease. The mentioned metaanalysis observed that the pooled prevalence estimates were significantly higher in strata containing smokers, males and persons aged over 40 years. However, the authors concluded that this significant heterogeneity was incompletely explained by sub group analysis38 .

Additional sources of variation may affect estimates of COPD prevalence, namely sampling methods, response rates, spirometry quality control and use of pre-or post-bronchodilator lung volumes to assess obstruction.

To overcome these limitations, two multinational population-based investigations, the BOLD project44 and the PLATINO study45, were conducted to provide more accurate and standardized estimates of country-specific COPD prevalence, appropriate for making cross-sites comparisons. Both surveys, adopting systematic quality control of spirometric data, observed a higher than previously reported prevalence of the disease in people aged 40 years and older. The overall prevalence of stage II or higher COPD reported by the BOLD initiative was 10.1% (standard error: 4.8%). In addition, a large amount of variability was observed across sites, with estimates of GOLD stage I or higher ranging between 11.4 and 26.1%. Similar data were reported in the PLATINO study, estimates of stage II or higher COPD varying between 2.6% in Mexico City and 7.1% in Montevideo. These studies showed that COPD is a greater health epidemic than has been previously realized and that differences in prevalence of COPD across sites cannot be fully explained by different patterns of exposure to known risk factors, including ageand smoking.

 

Risk factors for COPD

Current knowledge concerning risk factors for COPD comes mainly from cross-sectional epidemiological studies1. A complex interaction between genetic factors and environmental exposures has been implicated in the development of the disease and several risk factors have been identified but a causal link is not established for all.

Smoking is recognized as the most important modifiable risk-factor causally related to development and progression of COPD3. Comparatively to nonsmokers, smokers have an accelerated annual decline of lung function and a higher COPD mortality rate. Cumulative lifetime smoking exposure increases the risk for disease1.

Nevertheless, not all smokers develop COPD, suggesting that genetic factors may influence subjects’ individual susceptibility to disease. Smoking cessation is the single most effective intervention in COPD management because it can prevent the development of airflow obstruction or cause a marked reduction in the decline of FEV146 and can have a substantial impact on mortality47. The finding that cessation rates are far from ideal, under 30% in the best programs48 , suggests the urgent need for better tailored treatments.

There is consistent epidemiological evidence that non-smokers may develop COPD, suggesting that additional risk factors are implicated in the pathogenesis of the disease.

Age has long been recognized as a risk factor for COPD1,49. Across populations, the prevalence, morbidity and mortality of disease are consistently higher among the elderly15,38,41,50. Recently, the BOLD study reported an overall pooled adjusted odds ratio of 1.94 for stage II or higher COPD per 10-year age increment, confirming the role of age as a powerful contributing factor for COPD prevalence and possibly to disease severity44. In some BOLD and PLATINO countries, COPD prevalence exceeded 20% in individuals aged over 60 years44,45. The changing age structure of the world’s population, with more people living longer due to enhanced interventions for acute cardiovascular disease and infections and, consequently, being at risk for chronic medical co-morbidities, has been claimed as one of the principal reasons for the worldwide increase in COPD prevalence10. Also, the effects of increasing age appear to act synergistically with those of tobacco smoking50, further contributing to an increased prevalence of the disease among elderly smokers. Occupational exposure to several dusts, chemicals, vapours and fumes are an underappreciated riskfactorforCOPD51. Ananalys is of the NHANES III survey, estimated that 19.2% of COPD cases in the USA were attributable to work exposures, the proportion being higher(31.1%)in never-smokers52 . These exposures are, in general, more important as a risk factor in low-and middle-income countries due to less stringent protective laws15 .

The role of indoor air pollution caused by exposure to biomass fuel in poorly ventilated dwellings is perfectly established as a risk factor for the development of COPD53, being one the most important determinants of the disease, especially among women in developing countries54.Conversely,although outdoor air pollution is associated with increased morbidity and mortality of COPD patients55,56, its role as a risk factor for the development of the disease remains controversial57,58, but seems to be small when compared to cigarette smoking.

Evidence that genetic factors are involved in the pathogenesis of COPD arose from the observation of an increased risk of developing the disease among individuals with severe deficiency of alpha-1-antitryps in 59. COPD is a polygenic disease and several other genetic factors are sought to contribute to the individual susceptibility for its occurrence60 .

Controversy regarding gender differences in susceptibility to airflow obstruction and COPD exists61,62 and this issue has been the topic of a great deal of research. Trends in COPD prevalence demonstrate that, in developed countries, the disease is becoming equally frequent in men and women2, probably reflecting changing patterns of smoking habits63. Besides, women seem to be more predisposed to earlyonset and to non-smoking-related COPD64 .

Additional potential risk factors, like lung growth, oxidative stress, respiratory infections, socioeconomic status, nutrition and asthma, although being associated with COPD, are less clearly causally related to its development1.

At present, a comprehensive knowledge of COPD is impaired by the complexity underlying its network of causation. Further investigation that includes pre- and perinatal periods to provide a better understanding of the interactions between risk factors for disease is required. Notwithstanding, the identification of recognized modifiable risk factors is an important step toward the development of preventive strategies to reduce or minimize the burden of COPD, both at population and individual level.

 

Natural history and prognosis

The natural history of COPD highlights that it is largely preventable and treatable, clearly illustrating that averting exposure to noxious agents would halt or at least slow lung function decline46. This is particularly relevant given the fact that the most important risk factor for disease is largely modifiable. In addition, recent studies suggest that interventions other than smoking cessation may alter the natural history of COPD65 .

Despite this scenario, COPD mortality rates continue to increase. According to current estimates of the World Health Organization (WHO), COPD is the fourth leading cause of death worldwide, accounting for 3.02 million deaths, corresponding to more than 5% of the total4. Considering that disease-specific mortality rates are probably being underestimated due to under diagnosis and underreporting, a higher proportion of COPD patients is dying because of the disease. In addition, COPD is frequently listed as a contributory cause of death rather than being labeled as the primary cause of death, further biasing mortality data. Moreover, the information provided by trends in COPD mortality rates over time is greatly affected by terminology and awareness1.

In COPD patients, the relation between changing smoking patterns and disease outcomes is complex. In the US, despite the decline of smoking prevalence observed in men since the mid sixties, COPD mortality has been increasing2. Conversely, in developing countries that are at relatively early stages of the smoking epidemic, an increase in smoking-related COPD can be anticipated. Since COPD mortality tracks several decades behind smoking trends, an increase in mortality will probably be noticed in coming years. Contrasting with these estimates, the mortality from COPD is already decreasing in many European countries66. Particularly striking are the mortality trends observed in women. In Canada the death rate from COPD accelerated in the nineties and is expected to soon overtake the rate among men67. In US, a steep rise in COPD deaths among women has been observed since the seventies and, for the first time, in 2000, the number of women dying from COPD surpassed the number of men dying from COPD (59936 vs. 59118)2.

The causes of death in COPD patients vary depending on the population studied68. Patients with mild or moderate disease usually die from cancer and from cardiovascular causes47. A different mortality profile emerges in patients with more severe disease, with respiratory disease being the leading cause of mortality65. Disease severity is usually determined based on pulmonary volumes, even though a weak correlation between airflow limitation and severity of symptoms has been demonstrated69. According to the ARIC study, lung function impairment is a strong predictor of mortality, with progressive airflow obstruction adversely affecting the prognosis of COPD patients70 . However, reducing COPD to a physiologically defined disease, although being a pragmatic approach, probably does not capture the complexity and multidimensional nature of the disease. Additional predictors of survival and quality of life have been recognized and incorporated into a composite score (BODE index) able to predict subsequent mortality more accurately than any component separately71 . This grading system uses body-mass index, airflow obstruction, dyspnoea and exercise capacity that are important components of the disease process. Emerging research suggests a potential role for several biomarkers in outcome predictions, but none of them is currently used72 .

Co-morbidities are frequently encountered in COPD patients and, in their presence, COPD can be under appreciated as a contributor to mortality. Cardiovascular disease, depression, muscle wasting, osteopenia and chronic infections often coexist with COPD, contributing to a high disease burden and to an adverse prognosis73 .

The natural history of disease illustrates that, unless interventions aiming at stopping exposures are implemented, the disease will likely progress to death3.

 

Copd in Portugal

In Portugal, the burden of COPD is high. Based on the available evidence collected up to 2008, the World Health Organization estimated an age-standardized death rate for COPD of 12.5 per 100,000 in 2004, corresponding to 2700 deaths74. The Pneumobil-2 project, conducted between May 2007 and May 2008, found a prevalence of pre-bronchodilator bronchial obstruction of 30% in men and 25% in women, among 5324 smoke-exposed individuals aged 40 years or older75. However, reliable data regarding the true burden of COPD are lacking because population-based studies reporting the prevalence of the disease using objective measurements of lung functionare not available.

Previous studies have placed Portugal at an early stage (transition between stage 2 and 3) of the smoking epidemic, the prevalence being higher in men and in more educated women76. This scenario is clearly in contrast with the decline in smoking habits among men observed in most European countries63. Considering the current worldwide estimates of COPD burden44 and the accepted role of smoking as one of the most important causally related risk factors for the disease, it is urgent to objectively quantify COPD prevalence at a national level. Accurate estimates of the magnitude of the problem are needed to guide future planning in the definition of cost-effective preventive measures directed at discontinuing smoking epidemics. Inaddition, given the high rate of under diagnosis observed in other European countries, it seems advisable to increase physician awareness for COPD and its risk factors, promoting its timely diagnosis.

 

Conclusion

Chronic obstructive pulmonary disease is a major and escalating cause of morbidity and death throughout the world, representing a substantial economic and social threat. Smoking is quantitatively the most important risk factor, highlighting that the disease is largely preventable. Less well-recognized risk factors should also be addressed because, in a large proportion of cases, they significantly contribute to the development of the disease. From a public heath perspective, the burden of the disease has been underestimated due to both the unavailability of a consensual “gold-standard” definition and under recognition of the disease by physicians. Symptoms are nonspecific, develop late in the course of the disease and can be attributable to concurrent co-morbidities. Accurate estimates of the prevalence of the disease are needed, supporting the widespread use of good quality spirometry for diagnosis. Based on current knowledge, the prevalence of COPD is high and continues to rise in parallel with smoking epidemic. Efforts to reduce its overall burden should include preventive measures like smoking cessation and strategies aiming at stopping disease progression to modify its ominous prognosis.

 

References

1. Rodriguez-Roisin R, Anzueto A, Bourbeau J, et al. Global Initiative for Chronic Obstructive Lung Disease. Global Strategy for the Diagnosis, Management and Prevention of Chronic Obstructive Pulmonary Disease. Updated 2009. (http://www.goldcopd.com/Guidelineitem.asp?l1=2&l2=1&intId=2003, Date last updated: 2009. Date last accessed: October 2010).         [ Links ]

2. Mannino DM, Homa DM, Akinbami LJ, Ford ES, Redd SC. Chronic obstructive pulmonary disease surveillance - United States, 1971-2000. MMWR Surveill Summ 2002;51:1-16.         [ Links ]

3. Pauwels RA, Rabe KF. Burden and clinical features of chronic obstructive pulmonary disease (COPD). Lancet 2004;364:613-20.         [ Links ]

4. Organization, World Health. Geneva, Switzerland 2002. Available at http://www.who.int/mediacentre/factsheets/fs310_2008.pdf.         [ Links ]

5. Lopez AD, Shibuya K, Rao C, et al. Chronic obstructive pulmonary disease: current burden and future projections. Eur Respir J 2006;27:397-412.         [ Links ]

6. Eisner MD, Anthonisen N, Coultas D, et al. An official Americam Thoracic Society public policy statement: Novel risk factors and the global burden of chronic obstructive pulmonary disease. Am J Respir Crit Care Med 2010;182:693-718.         [ Links ]

7. Mannino DM. COPD: epidemiology, prevalence, morbidity and mortality, and disease heterogeneity. Chest 2002;121:121S-6S.         [ Links ]

8. Rennard SI, Vestbo J. COPD: the dangerous underestimate of 15%. Lancet 2006;367:1216-9.         [ Links ]

9. Lundback B, Lindberg A, Lindstrom M, et al. Not 15 but 50% of smokers develop COPD? Report from the Obstructive Lung Disease in Northen Sweden Studies. Respir Med 2003;97:115-22.         [ Links ]

10. Jemal A, Ward E, Hao Y, Thun M. Trends in the leading causes of death in the United States, 1970-2002. JAMA 2005;294:1255-9.         [ Links ]

11. Active ageing: a policy framework. Organization, World Health. 2002. Avaliable at http://whqlibdoc.who.int/hq/2002/WHO_NMH_NPH_02.8.pdf.         [ Links ]

12. Worl Population Ageing 2009. Affairs., Population Division of United Nations Department of Econocmic and Social. Available at http://www.un.org/esa/population/publications/WPA2009/WPA2009-report.pdf        [ Links ]

13. WHO report on the global tobacco epidemic. Organization., World Health. 2008. Available at http://whqlibdoc.who.int/publications/2008/9789241596282_eng.pdf.         [ Links ]

14. Murray CJL, Lopez AD. Alternative projections of mortality and disability by cause 1990-2020: Global Burden of Disease Study. Lancet 1997;349:1498-504.         [ Links ]

15. Mannino DM, Buist AS. Global burden of COPD: risk factors, prevalence, and future trends. Lancet 2007;370:765-73.         [ Links ]

16. Mannino MD, Braman S. The epidemiology and economics of chronic obstructive pulmonary disease. Proc Am Thorac Soc 2007;4:502-6.         [ Links ]

17. Jansson SA, Andersson F, Borg S, Ericsson A, Jonsson E, Lundback B. Costs of COPD in Sweden according to disease severity. Chest 2002;122:1994-2002.         [ Links ]

18. Menezes AM, Perez-Padilla R, Hallal PC, et al. Worldwide burden of COPD in high- and low-income countries. Part II. Burden of chronic obstructive lung disease in Latin America: the PLATINO study. Int J Tuberc Lung Dis 2008;12:709-12.         [ Links ]

19. Pearson MG, Alderslade R, Allen SC, et al, on behalf of the COPD guidelines group of the Standards of Care Committee of the British Thoracic Society. BTS Guidelines for the management of chronic obstructive pulmonary disease. Thorax 1997;52:S1-28.         [ Links ]

20. Celi BR, MacNee W. Standards for the diagnosis and treatment of patients with COPD: a summary of the ATS/ERS position paper. Eur Respir J 2004;23:932-46.         [ Links ]

21. Tinkelman DG, Price DB, Nordyke RJ, Halbert RJ. COPD screening efforts in primary care: what is the yield? Prim Care Respir J 2007;16:41-8.         [ Links ]

22. Cazzola M, Donner CF, Hanania NA. One hundred years of chronic obstructive pulmonary disease (COPD). Respir Med 2007;101:1049-65.         [ Links ]

23. Mannino DM, Buist AS, Vollmer WM. Chronic obstructive pulmonary disease in the older adult: what defines abnormal lung function? Thorax 2007;62:237-41.         [ Links ]

24. Hansen JE, Sun X-G, Wasserman K. Discriminating measures and normal values for expiratory obstruction. Chest 2006;129:369-77.         [ Links ]

25. Medbo A, Melbye H. Lung function testing in the elderly – Can we still use FEV1/FVC as a criterion of COPD? Respir Med 2007;101:1097-105.         [ Links ]

26. Hardie JA, Buist AS, Vollmer WM, Ellingsen I, Bakke PS, Morkve O. Risk of over-diagnosis of COPD in asymptomatic elderly never-smokers. Eur Respir J 2002;20:1117-22.         [ Links ]

27. Hansen JE, Sun X-G, Wasserman K. Spirometric criteria for airway obstruction: Use percentage of FEV1/FVC ratio below the fifth percentile, not < 70%. Chest 2007;131:349-55.         [ Links ]

28. Cerveri I, Corsico AG, Accordini S, et al. Underestimation of airflow obstruction among young adults using FEV1/FVC <70% as a fixed cut-off: a longitudinal evaluation of clinical and functional outcomes. Thorax 2008;63:1040-5.         [ Links ]

29. Hnizdo E, Glindmeyer HW, Petsonk EL, Enright P, Buist AS. Case definitions of chronic obstructive pulmonary disease. COPD 2006;3:95-100.         [ Links ]

30. Celli BR, Halbert RJ, Isonaka A, Schau B. Population impact of different definitions of airway obstruction. Eur Respir J 2003;22:268-73.         [ Links ]

31. Hankinson JL, Odencrantz JR, Fedan KB. Spirometric reference values from a sample of the general U.S. population. Am J Crit Care Med 1999;159:179-87.         [ Links ]

32. Peces-Barba G, Barberà JA, Agustí A, et al. [Diagnosis and management of chronic obstructive pulmonary disease: joint guidelines of the Spanish Society of Pulmonology and Thoracic Surgery (SEPAR) and the Latin American Thoracic Society (ALAT)]. Arch Bronconeumol 2008;44:271-81.         [ Links ]

33. Johannessen A, Omenaas ER, Bakke PS, Gulsvik A. Implications of reversibility testing on prevalence and risk factors for chronic obstructive pulmonary disease: a community study. Thorax 2005;60:842-7.         [ Links ]

34. Probst-Hensch NM, Curjuric I, Pierre-Olivier B, et al. Longitudinal change of prebronchodilator spirometric obstruction and health outcomes: results from the SAPALDIA cohort. Thorax 2010;65:150-6.         [ Links ]

35. Mannino DM, Davis KJ. Lung function decline and outcomes in an elderly population. Thorax 2006;61:472-7.         [ Links ]

36. Soriano JB, Zielinski J, Price D. Screening for and early detection of chronic obstructive pulmonary disease. Lancet 2009; 74:721-32.         [ Links ]

37. Halbert RJ, Isonaka S, George D, Iqbal A. Interpreting COPD prevalence estimates: what is the true burden of disease? Chest 2003;123:1684-92.         [ Links ]

38. Halbert RJ, Natoli JL, Gano A, Badamgarav E, Buist AS, Mannino DM. Global burden of COPD: systematic review and meta-analysis. Eur Respir J 2006;28:523-32.         [ Links ]

39. Von Hertzen L, Reunanen A, Impivaara O, Mälkiä E, Aromaa A. Airway obstruction in relation to symptoms in chronic respiratory disease: a nationally representative population study. Respir Med 2000;94:356-63.         [ Links ]

40. Dickison JA, Meacker M, Searle M, Ratcliffe G. Screening older patients for obstructive airways disease in a semi-rural practice. Thorax 1999;54:501-5.         [ Links ]

41. Mannino DM, Gagnon RC, Petty TL, Lydick E. Obstructive lung disease and low lung function in adults in the United States: data from the National Health and Nutrition Examination Survey, 1988-1994. Arch Intern Med 2000;160:1683-9.         [ Links ]

42. Pena VS, Miravitlles M, Gabriel R, et al. Geographic variations in prevalence and underdiagnosis of COPD: results of the IBERPOC multicentre epidemiological study. Chest 2000;118:981-9.         [ Links ]

43. De Marco R, Accordini S, Cerveri I, et al, on behalf of the European Community Health Survey Study Group. An international survey of chronic obstructive pulmonary disease in young adults according to GOLD stages. Thorax 2004;59:120-5.         [ Links ]

44. Buist AS, McBurnie MA, Vollmer WM, et al. International variation in the prevalence of COPD (The BOLD Study): a population-based prevalence study. Lancet 2007;370:741-50.         [ Links ]

45. Menezes AMB, Perez-Padilla R, Jardim JRB, et al, on behalf of the PLATINO Team. Chronic obstructive pulmonary disease in five Latin American cities (the PLATINO study): a prevalence study. Lancet 2005;366:1875-81.         [ Links ]

46. Anthonisen NR, Connett JE, Murray RP. Smoking and lung function of Lung Health Study after 11 years. Am J Respir Crit Care Med 2002;166:675-9.         [ Links ]

47. Anthonisen NR, Skeans MA, Wise RA, et al. The effects of smoking cessation intervention on 14.5 year mortality: a randomized clinical trial. Ann Intern Med 2005;142:233-9.         [ Links ]

48. Chandler MA, Rennard SI. Smoking cessation. Chest 2010;137:428-35.         [ Links ]

49. Feenstra TL, van Genugten MLL, Hoogenveen RT, Wouters EF, Rutten- van Molken MPMH. The impact of aging and smoking on the future burden of chronic obstructive pulmonary disease: a model analysis in the Netherlands. Am J Respir Crit Care Med 2001;164:590-6.         [ Links ]

50. Lindberg A, Jonsson AC, Ronmark E, Lundgren R, Larsson LG, Lundbäck Prevalence of obstructive pulmonary disease according to BTS, ERS, GOLD, and ATS criteria in relation to doctor diagnosis, symptoms, age, gender, and smoking habits. B. Respiration 2005;72:471-9.         [ Links ]

51. Trupin L, Earnest G, San Pedro M, et al. The occupational burden of chronic obstructive pulmonary disease. Eur Respir J 2003;22:462-9.         [ Links ]

52. Hnizdo E, Sullivan PA, Bang KM, Wagner G. Association between chronic obstructive pulmonary disease and employment by industry and occupation in the US population: a study of data from the Third National Health and Nutrition Examination Survey. Am J Epidmiol 2002;156:738-46.         [ Links ]

53. Kurmi OP, Semple S, Simkhada P, Smith WC, Ayres JC. COPD and chronic bronchitis risk of indoor air pollution from solid fuel: a systematic review and meta-analysis. Thorax 2010;65:221-8.         [ Links ]

54. Ezzati M. Indoor air pollution and health in developing countries. Lancet 2005;366:104-6.         [ Links ]

55. Ko FWS, Hui DSC. Outdoor air pollution: impact on chronic obstructive pulmonary disease patients. Curr Opin Pulm Med 2009;15:150-7.         [ Links ]

56. Liu Y, Lee K, Perez-Padilla R, Hudson NL, Mannino DM. Outdoor and indoor air pollution and COPD-related diseases in high and low-income countries. Int J Tuberc Lung Dis 2008;12:115-27.         [ Links ]

57. Downs SH, Schindler C, Liu LJ, et al. Reduced exposure to PM10 and attenuated age-related decline in lung function. N Engl J Med 2007;357:2338-47.         [ Links ]

58. Schikowski T, Sugiri D, Ranft U, et al. Long-term air pollution exposure and living close to busy roads are associated with COPD in women. Respir Res 2005;6:152.         [ Links ]

59. Stoller JK, Aboussouan LS.a1-antitrypsin deficiency. Lancet 2005;365:2225-36.         [ Links ]

60. Sandford AJ, Silverman EK. Chronic obstructive pulmonary disease. Susceptibility factors for COPD the genotype-environment interaction. Thorax 2002;57:736-41.         [ Links ]

61. de Torres JP, Campo A, Casanova C, Aguirre-Jaime A, Zulueta J. Gender and chronic obstructive pulmonary disease in high-risk smokers. Respiration 2006;73:306-10.         [ Links ]

62. Silverman EK, Weiss ST, Drazen JM, et al. Gender-Related differences in severe, early-onset chronic obstructive pulmonary disease. Am J Respir Crit Care Med 2000;162:2152-8.         [ Links ]

63. Cavelaars AEJM, Kunst AE, Geurts JJM, et al. Educational differences in smoking: international comparison. BMJ 2000;320:1102-7.         [ Links ]

64. Varkey AB. Chronic obstructive pulmonary disease in women: exploring gender differences. Curr Opin Pulm Med 2004;10:98-103.         [ Links ]

65. Calverley PM, Anderson JA, Celli B, et al. TORCH investigators. Salmeterol and fluticasone propionate and survival in chronic obstructive pulmonary disease. N Engl J Med 2007;356:775-89.         [ Links ]

66. Chapman KR, Mannino DM, Soriano JB, et al. Epidemiology and costs of chronic obstructive pulmonary disease. Eur Respir J 2006;27:397-412.         [ Links ]

67. Chapman KR. Chronic obstructive pulmonary disease: are women more susceptible than men? Clin Chest Med 2004;25:331-41.         [ Links ]

68. Celli BR. Predictors of mortality on COPD. Respir Med 2010;104:773-339.         [ Links ]

69. Ries AL. Impact of chronic obstructive pulmonary disease on quality of life: The role of dyspnoea. Am J Med 2006;119:12-20.         [ Links ]

70. Mannino DM, Doherty DE, Buist AS. Global Initiative on Obstructive Lung Disease (GOLD) classification of lung disease and mortality: findings from the Atherosclerosis Risk in Communities (ARIC) study. Respir Med 2006;100:115-22.         [ Links ]

71. Celli BR, Cote CG, Marin JM, et al. The body-mass index, airflow obstruction, dyspnea, and exercise capacity index in chronic obstructive pulmonary disease. N Engl J Med 2004; 350:1005-12.         [ Links ]

72. Barnes PJ, Chowdhury B, Kharitonov SA, et al. Pulmonary biomarkers in chronic obstructive pulmonary disease. Am J Respir Crit Care Med 2006;174:6-14.         [ Links ]

73. Sinn DD, Anthonisen NR, Soriano JB, Agusti AG. Mortality in COPD: role of comorbidities. Eur Respir J 2006;28:1245-57.         [ Links ]

74. http://www.who.int/healthinfo/statistics/bodgbddeathdalycountryestimates2004.xls. Organization, World Health. Accessed October 2010.         [ Links ]

75. Reis Ferreira JM, Matos MJ, Rodrigues F, et al. Prevalence of bronchial obstruction in a tobacco smoke exposed population – the PNEUMOBIL project. Rev Port Pneumol 2009; 15:803-46.         [ Links ]

76. Santos AC, Barros H. Smoking patterns in a community sample of Portuguese adults, 1999-2000. Prev Med 2004;38:114-1.         [ Links ]

 

Correspondencia:

Joana Mascarenhas

Departamento de Epidemiologia Clínica, Medicina Preditiva e Saúde Pública Faculdade de Medicina da Universidade do Porto, Alameda Prof. Hernâni Monteiro 4300-319 Porto. Email: joanamaspinto@gmail.com

Creative Commons License Todo o conteúdo deste periódico, exceto onde está identificado, está licenciado sob uma Licença Creative Commons