PDF version

Faris Al Lami ¹ and Zainab Salim ²

انتشار وعوامل خطورة مرض الانسداد الرئوي المزمن في عينة من البالغين المدخنين في بغداد، العراق، 2014

فارس حسن اللامي، زينب سالم كاظم

الخلاصة: اجريت هذة الدراسة القطعية على عينة مناسبه من 325 من البالغين المدخنين لتقدير مدى انتشار مرض الانسداد الرئوي المزمن وبعض عوامل الخطورة الكامنة وراء انتشاره في بغداد, العراق 2014 . اضافة الى الخصائص الديموغرافية تم تقديم "استبانة وظائف الرئة" لتحديد الاعراض التنفسية وتم فحص وظائف الرئة لكل شخص يسجل 18 او اقل في هذا الاستبيان. اذا كانت نسبة FEV1\FVC أقل من 70% يعاد الفحص بعد استعمال الموسعات القصبية اذا كانت النسبة اقل من 70% مع تحسن اقل من 200 مل في ال FEV1 اعتبرهذا دليل على وجود مرض الانسداد الرئوي المزمن. كان معدل انتشار المرض 15.1%. 62.5% منهم من النوع المتوسط و 27.1% من النوع الشديد وان 12.6% فقط كان لديهم تشخيص سابق للمرض من قبل طبيب. اظهر تحليل الانحدار اللوجستي وجود علاقة معتدة بين المرض والتدخين اكثر من 40 باكيت ، وازدياد السن اكثر من 55 سنة. يوصى باجراء فحص وظائف الرئة لجميع البالغين المدخنين وتقديم المشورة لترك التدخين.

ABSTRACT This cross-sectional study was conducted to estimate the prevalence and identify determinants of chronic obstructive pulmonary disease (COPD) among a convenience sample of 325 adult smokers in Baghdad, Iraq, 2014. Beside demographic variables, participants had Lung Function Questionnaire to assess respiratory symptoms; individuals with a score of ≤18 had a spirometry examination. Those with FEV1/FVC ratio <70% had post bronchodilator spirometry; those with FEV1/FVC% of 40 (OR =5.37, 95% confidence interval = 1.70-16.91) were the significant independent determinants.  All adult smokers should have a spirometry testing and counseled to stop smoking.

Prévalence et déterminants de la bronchopneumopathie chronique obstructive dans un échantillon de fumeurs adultes à Bagdad (Iraq) en 2014

RÉSUMÉ La présente étude transversale a été conduite dans le but d’estimer la prévalence de la bronchopneumopathie chronique obstructive (BPCO) et d’identifier ses déterminants dans un échantillon de commodité de 325 fumeurs adultes à Bagdad (Iraq) en 2014. En plus des variables démographiques, les participants devaient remplir un questionnaire sur les fonctions pulmonaires afin d’évaluer les symptômes respiratoires. Les individus ayant obtenu un score inférieur ou égal à 18 devaient se soumettre à un test de spirométrie. Ceux qui présentaient un rapport VEMS/CVF (volume maximal expiré pendant la première seconde d'une expiration forcée/capacité vitale forcée) inférieur à 70 % avaient une spirométrie post-bronchodilatateur  ; ceux avec un rapport VEMS/CVF de moins de 70 % et une amélioration du VEMS inférieure à 200 ml étaient considérés comme des cas de BPCO. Les stades de la BPCO sont déterminés en fonction du degré de diminution du VEMS. La prévalence de la BPCO était de 15,1 % (intervalle de confiance à 95 % = 11,5-19,4 %), 62,5 % souffraient de BPCO modérée et 27,1 % d’une BPCO sévère. Un diagnostic médical avait été posé au préalable pour seulement  12,5  % des participants. Un âge supérieur à 55 ans (OR = 2,14, intervalle de confiance à 95 % =  1,04-4,39), et une consommation de paquets-année supérieure à 40 (OR = 5,37, intervalle de confiance à 95 %  = 1,70-16,91) était les déterminants indépendants significatifs. Tous les fumeurs adultes devraient bénéficier d’un test de spirométrie et de conseils pour arrêter de fumer.

¹Department of Community Medicine, College of Medicine, Baghdad University, Baghdad, Iraq (correspondence to: F. Al Lami: This e-mail address is being protected from spambots. You need JavaScript enabled to view it ). ²Ministry of Health, Baghdad, Iraq.

Received: 19/04/15; accepted: 10/05/16

---

Introduction

Chronic obstructive pulmonary disease (COPD) is an important and growing cause of morbidity and mortality worldwide (1–3). The WHO Global Burden of Disease Project estimated that COPD was the fifth leading cause of death worldwide in 2001 and will be the third leading cause by 2020 (1). It is a preventable and treatable disease characterized by airflow limitation that is not fully reversible (3).

In the early stages, COPD can be symptomless; later long episodes of coughing, often with sputum production, develops. In the later stages, when a large portion of the lung capacity may already have been lost, symptoms of dyspnoea on exertion will develop. Usually COPD is diagnosed in the later stages, and this diagnostic delay may either be due to the patient’s gradual adaptation to a decreasing lung function or because doctors are unaware of, or not responding to, the symptoms (4).

The major risk factor for COPD is cigarette smoking (5), other irritants such as domestic fuel, air pollution and chemical fumes or dust from the environment or workplace can also contribute. Older age and male sex are also associated with COPD (6). Spirometry is needed to make a confident diagnosis of irreversible airway obstruction: (post-bronchodilator FEV1/FVC < 0.7 according to GOLD guidelines (3).

Although around 90% of deaths due to COPD occur in low- or middle-income countries, very few data on the prevalence of this illness are available in these countries (7). In one large study done in the Middle East and North Africa, which included a large sample of individuals aged > 40 years in 10 countries, the overall prevalence of COPD was 3.6% (8). Prevalence increases considerably with age and intensity of smoking, and can vary from 25% in a general smoking population to approximately 50% in an elderly smoking population (9–11).

The objective of the current study was to estimate the prevalence of COPD among a sample of adult smokers in Baghdad and to identify certain determinants underlying its development.

Methods

Sample

A cross-sectional study was conducted in 3 primary health care centres in Baghdad, Iraq, during the period 1 May–30 October 2014. There are 118 PHCCs in Al Karekh Directorate of Health (western Baghdad) and 116 in Al Rusafa (eastern Baghdad). After discussion with the officials at the 2 directorates of health, we made a convenience selection of 3 centres where we had determined that the catchment populations included different socioeconomic classes.

The sample size was calculated using the formula n = z2pq/d2

n = (1.96)2 × 0.15 × 0.85/(0.04)2

n = 318

We selected 325 individuals to be included in our study. We invited all current or former cigarette smokers aged ≥ 35 years attending these 3 primary health care centres for any reason other than respiratory problems and who fulfilled the inclusion criteria to participate in the study until we achieved the required sample size. There were no refusals to participate. Pregnant women and those with contraindications to bronchodilators were excluded.

Previously, a pilot study was done on 10 smokers aged ≥ 35 years in one of the selected primary health care centres to assess the validity of the questionnaire and the time needed to complete the questionnaires and having the spirometry test. No changes were made to the questionnaire and the time allocated to complete the tests was adequate.

Data collection

Two questionnaires were used and completed by the investigator through direct interviews with the study participants. The first included questions on sociodemographic data: age, sex, residence, occupation, education, and income. Smoking history was documented as current or former smoker besides the number of cigarettes smoked per day and years of smoking. Pack years smoking was calculated by multiplying number of cigarette smoked per day by years of smoking divided by 20 (no. of cigarettes per pack) (2). This was categorized into 3 groups: 1–20, 21–40 and > 40.

History of comorbid chronic diseases, including hypertension, diabetes and liver or renal diseases, and any previous diagnosis of chronic bronchitis, emphysema or COPD was recorded.

The second questionnaire was the Lung Function Questionnaire, which comprises 5 questions scored on a 5-point Likert scale (very often = every day, often = most days of the week, sometimes = 1–2 times per week, rarely = < 1 time per week, never = 0 times per week), with lower scores indicating increased risk of airflow obstruction (12). The questionnaire was administered via face-to-face interview by one of the researchers (ZS). The first 3 questions asked about how often the patients experienced coughing up mucus, wheezing and shortness of breath during physical activity. A total score of ≤ 18 suggests an increased risk of airway obstruction (12): all individuals with a score of ≤ 18 on the questionnaire were given a pulmonary function test using the spirometer.

Spirometry

Spirometry was performed according to the recommendations of the American Thoracic Society (13). We used the Discovery 2 portable spirometer (Futuremed). Every patient who had FEV1/FVC < 70% then underwent post-bronchodilator spirometry, using 2 puffs 1 minute apart of inhaled Ventolin, and after 30 minutes spirometry was repeated; FEV1/FVC % < 7 0% and < 200 mL improvement of FEV1 is considered irreversible obstruction (COPD). Staging of COPD was then done according to the GOLD classification (3): mild FEV1/FVC < 0.7 FEV1 ≥ 80% of predicted, moderate FEV1 < 0.7 FEV1 ≥ 50–< 80% of predicted, severe FEV1\FVC < 0.7 FEV1 ≥30–

Statistical analysis

We used SPSS, version 20, for data entry and analysis. The chi-squared test of independence was used to test the association between variables. Logistic regression analysis was applied with the presence of COPD as the outcome variable and the demographic and smoking characteristics as independent variables. Odds ratio (OR) and its 95% confidence interval (CI) were calculated; P-value < 0.05 was considered statistically significant.

Ethical approval

Ethical approval was obtained from the health research committee in the Iraqi Ministry of Health and the Iraqi Board of Medical Specializations. All participants were informed about the study and verbal approval was obtained before enrolment.

Results

From the total sample of 325 smokers and ex-smokers of both sexes, 273 (84%) were males. The mean age was 51.1 [standard deviation (SD) 10.8] years. All were urban residents. Further demographic characteristics are detailed in Table 1.

Chronic disease was present in 46.5% of the participants, hypertension in 37.8%, diabetes in 18.8% and ischaemic heart diseases in 6.5%. The study sample included current smokers (85.8%) and ex-smokers (14.2%). Mean pack years smoking was 40.7 (SD 30.2).

We found that 282 (86.8%) participants scored ≤ 18 on the Lung Function Questionnaire, i.e. were at risk of COPD (Figure 1). All were given the pulmonary function (spirometry) test; this was obstructive in 59 (20.9%) participants. Those who showed an obstructive pattern had post-bronchodilator spirometry and in 48 (81.3%) the obstruction was irreversible, i.e. COPD. The remaining 11 (18.7%) showed reversible obstruction (asthma) (Figure 1) .

The prevalence of COPD among the study sample was 15.1% (95% CI: 11.5–19.4%): 10.4% had mild (stage I), 62.5% had moderate (stage II) and 27.1% had severe (stage III) COPD. Of the 48 participants identified as having COPD, only 7 (14.6%) had been previously diagnosed with chronic bronchitis by a physician, and only 1 (2.1%) with COPD, i.e. 40 (83.3%) of the patients with COPD had not been previously diagnosed.

All 216 (66.5%) participants with scores ≤ 18 but who had a normal result for spirometry are considered at risk of developing COPD according to the GOLD classification (3). The mean score was 13.9 (SD 3.6); all participants diagnosed with COPD in our study scored between 7 and 15.

The prevalence of COPD is significantly higher with older age (P < 0.01); the highest prevalence was reported in the age group ≥ 65 years (31.2%) (Table 1). There was almost equal distribution between males (15.0%) and females (15.7) (P = 0.897). (Table 1). Education level was not a statistically significant factor for COPD in our participants (P = 0.134).

The prevalence of COPD was greater among unemployed participants (44.2%). Only 5.3% of government employees had COPD (P 2 (19.5%) (P = 0.041).

Similarly, COPD prevalence was greater among those who had other chronic diseases (20.7%) than those without (10.4%) (P = 0.011) (Table 2).

Prevalence of COPD was significantly higher with increasing pack years smoking. The prevalence was 21.4% among those with > 40 pack years followed by 19.4% among those with 21–40 pack years and only 3.9% among those with ≤ 20 pack years (P = 0.001) (Table 2) .

Logistic regression was used to identify the independent, unconfounded, risk factors of COPD (as the outcome variable). Two explanatory variables had a statistically significant association with COPD risk: pack years smoking, highest pack year (> 40) (OR =5.37; 95% CI: 1.70–16.91, P = 0.004) and pack year 21–40 (OR = 5.15; 95% CI: 1.62–16.29, P = 0.005), and older age (≥ 55 years) (OR =2.14, 95% CI: 1.04–4.39, P = 0.038) (Table 3).

The remaining variables (sex, marital status, education level, crowding index, body mass index, presence of chronic disease) had no statistically significant association with the outcome.

Discussion

The prevalence of COPD has been widely reported from several countries mainly the developed countries. There is a wide variation in the prevalence reported from different countries due to differences in methodology, diagnostic criteria and type and age of population included.

In the current study on adult smokers aged ≥ years, the risk of getting COPD was 86.8%, and the prevalence of COPD was 15.1%. This is similar to the prevalence reported in studies from Sweden (14%), Spain (15%), the United States of America (USA) (14.2%), Germany (13.2%) and Turkey (18.1%) (14–18). It is higher than the prevalence reported in the BREATHE study, which was conducted in Egypt (3.5%), Jordan (5.4%), Lebanon (5.3%), Syria (6.1%) and the United Arab Emirates (1.9%) (8). The difference in prevalence is because this large study included the general population, i.e. smokers and non-smokers, which accounts for the lower prevalence.

More than two-thirds of COPD cases in the current study were moderate stage; more than a quarter had severe and only 10% had the mild type. Similar findings were found in Lebanon with 58.3% of COPD patients having moderate disease, 20.3% severe disease and 17.6% mild disease (19).

In other countries, such as Sweden, the USA, Japan and Korea, most COPD cases were mild (stage I) followed by moderate and severe stages (14,16,20,21). This difference could be attributed to including the general population or the early detection of cases due to better health care in these developed countries. This is supported by the finding that more than 83% of the cases were diagnosed as having COPD for the first time during our study. This is supported by the findings of some other studies (19,22). There are 2 possible explanations for the low number of diagnoses of COPD. One is the reluctance of smokers to consult for symptoms they consider normal, such as cough or expectoration. Such patients usually seek medical help only when they experience dyspnoea and exacerbations at a relatively advanced stage of the disease. The second is the low use of pulmonary function tests by physicians.

Our study showed that older age and increased pack years smoking are the main factors associated with COPD development. Approximately 1 in 10 patients aged  30 develop COPD compared with 7.2% of those with pack years ≤ 30, This is comparable to the findings of other studies (19,22–24). Chronic inhaled cigarette smoke leads to chronic lung inflammatory response, which induces parenchymal tissue destruction and disrupts the normal repair mechanism leading to airway fibrosis and narrowing and a decrease in FEV1 (3).

As this was a cross sectional study any causal relationship cannot be inferred. Also we used a convenience sample (non-probability) which comprised attendees of primary health care centres. This could limit the generalizability of the study results.

Funding: None.

Competing interests: None declared.

References

1. Report on the global tobacco epidemic. Geneva: World Health Organization; 2011.
2. Lopez AD, Shibuya K, Rao C, Mathers CD, Hansell AL, Held LS, et al. Chronic obstructive pulmonary disease: current burden and future projections. Eur Respir J. 2006;27:397–412. PMID:16452599
3. (GOLD). Global strategy for the diagnosis, management and prevention of COPD – 2016. Global Initiative for Chronic Obstructive Lung Disease; 2016 (http://goldcopd.org/global-strategy-diagnosis-management-prevention-copd-2016/ http://www.goldcopd.org/, accessed 2 March 2017).
4. Van Schayck CP, Chavannes NH. Detection of asthma and chronic obstructive pulmonary disease in primary care. Eur Respir J. 2003;21(Suppl.39):16s–22s. PMID:12572697
5. Marsh S, Aldington S, Shirtcliffe P, Weatherall M and Beasley R. Smoking and COPD: what really are the risks? Eur Respir J. 2006;28:883–4. PMID:17012635
6. Boggia B, Farinaro E, Grieco L, Lucariello A, Carbone U. Burden of smoking and occupational exposure on etiology of chronic obstructive pulmonary disease in workers of southern Italy. J Occup Environ Med. 2008;50(3):366–70. PMID:18332787
7. Halpin DM, Miravitlles M. Chronic obstructive pulmonary disease: the disease and its burden to society. Proc Am Thorac Soc. 2006;3(7):619–23. PMID:16963544
8. Tageldin MA1, Nafti S, Khan JA, Nejjari C, Beji M, Mahboub B, et al. Distribution of COPD-related symptoms in the Middle East and North Africa: result of BREATHE study. Respir Med. 2012;106(Suppl.2):s25–32. PMID:23290701
9. Hasselgren M, Arne M, Lindahl A, Janson S, Lundback B. Estimated prevalences of respiratory symptoms, asthma and chronic obstructive pulmonary disease related to detection rate in primary health care. Scand J Prim Health Care. 2001;19(1):54–7. PMID:11303549
10. Lundback B, Lindberg A, Lindstrom M, Ronmark E, Jonsson AC, Jonsson E, et al. Not 15 but 50% of smokers develop COPD?—Report from the Obstructive Lung Disease in Northern Sweden studies. Respir Med 2003;97(2):115–22. PMID:12587960
11. Stratelis G, Jakobsson P, Molstad S, Zetterstrom O. Early detection of COPD in primary care: screening by invitation of smokers aged 40 to 55 years. Br J Gen Pract. 2004;54(500):201–6. PMID:15006126
12. Yawn BP, Mapel DW, Mannino DM, Martinez FJ, Donohue JF, Hanania NA, et al. Development of the Lung Function Questionnaire (LFQ) to identify airflow obstruction. Int J Chron Obstruct Pulmon Dis. 2010;5:1–10. PMID:20368906
13. Miller MR, Hankinson J, Brusasco V, Brugos F, Cassaburi R, Coates A, et al. ATS/ERS TASK FORCE. Standardization of lung function testing. Eur Respir J. 2005;26:319–38.
14. Lindberg A, Bjerg A, Ronmark E, Larsson LG, Lundback B. Prevalence and underdiagnosis of COPD by disease severity and the attributable fraction of smoking: report from the Obstructive Lung Disease in Northern Sweden Studies. Respir Med 2006, 100(2):264–72. PMID:15975774
15. Peña VS, Miravitles M, Gabriel R, Jimenez-Ruiz CA, Villasante C, Masa JF, et al. Geographic variations in prevalence and underdiagnosis of COPD. Chest. 2000;118(4):981–9. PMID:11035667
16. 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. PMID:12198919
17. Geldmacher H, Biller H, Herbst A, Urbanski K, Allison M, Buist AS, et al. [The prevalence of chronic obstructive pulmonary disease in Germany, result of BOLD study.] Dtsch Med Wochenschr. 2008 Dec;133(50):2609–14 [in German]. PMID 19052996.
18. Gunen H, Savas S, Agil H, Yetkin O, Gulbas G, Mutlu LC, et al. Prevalence of COPD, first epidemiological study of a large region in Turkey. Eur J Int Med. 2008;19(7):499–504. PMID:19013377
19. Salameh P, Waked M. Chronic obstructive pulmonary disease and risk factors in Middle East countries; facts from Lebanon. Beirut: Lebanese University; (www.ul.edu.lb/files/announcements/annonce_16_2149_2641.pdf, accessed 14 February 2017).
20. Fukuchi Y, Nishimura M, Ichinose M, Adachi M, Nagai A, Kuriyama T, et al. COPD in Japan: the Nippon COPD Epidemiology study. Respirology. 2004;9(4):458–65. PMID:15612956
21. Yoo KH, Kim YS, Sheen SS, Park JH, Hwang YI, Kim SH, et al. Prevalence of chronic obstructive pulmonary disease in Korea: the fourth Korean National Health and Nutrition Examination Survey, 2008. Respirology, 2011;16(4):659–65. PMID:21342331
22. Díaz J, de Castro Mesa C, Gontán García-Salamanca MJ, Lopez de Castro F. [Prevalence of chronic obstructive pulmonary disease and risk factors in smokers and ex-smokers.] Arch Bronconeumol. 2003;39(12):554–8 [in Spanish]. PMID:14636492
23. Mintz ML, Yawn BP, Mannino DM, Donohue JF, Hanania NA, Grellet CA, et al. Prevalence of airway obstruction assessed by lung function questionnaire. Mayo Clin Proc. 2011;86(5):375–81. PMID:21531880
24. Sandelowsky H, Ställberg B, Nager B and Hasselström J. The prevalence of undiagnosed chronic obstructive pulmonary disease in a primary care population with respiratory tract infections – a case finding study. BMC Fam Pract. 2011;12:122. PMID:22047519