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COPD
Chronic obstructive pulmonary disease (COPD), also known as
chronic obstructive airway disease (COAD), is a group of diseases characterized by limitation of
airflow in the airway that is not fully reversible. COPD is the umbrella term for chronic
bronchitis,
emphysema and a range of other disorders. It is most often due to tobacco smoking
but can be due to other airborne irritants such as coal dust, asbestos or solvents, as well as preserved meats containing nitrites.
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Signs and Symptoms
The main symptoms of COPD include dyspnea (shortness of breath) lasting for months or perhaps years, possibly accompanied by wheezing, and a persistent cough with sputum
production. It is possible the sputum may contain blood (hemoptysis), usually due to damage of the blood vessels of the airways. Severe COPD could lead to cyanosis (bluish
decolorization usually in the lips and fingers) caused by a lack of oxygen in the blood. In extreme cases it could lead to cor pulmonale due the extra work required by the heart to get
blood to flow through the lungs.
COPD is particularly characterised by a ratio of forced expiratory volume over 1 second (FEV1) to forced vital capacity (FVC) being < 0.7 and the FEV1 < 70% of the predicted value.
Other signs include a rapid breathing rate (tachypnea) and a wheezing sound heard through a stethoscope.
Emphysema may be detected by the sounds produced on palpation.
Causes
Cigarette Smoking
A primary factor of COPD is chronic tobacco smoking. In the United States, around 90% of cases of COPD are due to smoking. However, not all smokers will develop COPD but
continuous smokers have at least a 25% risk.
Occupational Pollutants
Some occupational pollutants, such as cadmium and silica, have shown to be a contributing risk factor for COPD. The people at highest risk for these pollutants include coal
workers, construction workers, metal workers and cotton workers, amongst others. However, in most cases these pollutants are combined with cigarette smoking further
increasing the chance of developing COPD. These occupations are commonly associated with other respiratory diseases, particularly pneumoconiosis (black lung disease).
Air Pollution
Urban air pollution may be a contributing factor for COPD as it is thought to impair the development of the lung function. In developing countries indoor air pollution, usually due to
biomass fuel, has been linked to COPD, especially in women.
Genetics
Rarely, there may be a deficiency in an enzyme known as alpha 1-antitrypsin deficiency which can cause COPD.
Other Risk Factors
Increasing age, male gender, and general impaired lung function are also related to the development of COPD.
Pathophysiology
Chronic Bronchitis
Chronic
bronchitis is defined in clinical terms as a cough with sputum production on most days for 3 months of a year, for 2 consecutive years.
Chronic
bronchitis is hallmarked by hyperplasia (increased number) and hypertrophy (increased size) of the goblet cells (mucous gland) of the airway, resulting in an increase in
secretion of mucus which contributes to the airway obstruction. Microscopically there is infiltration of the airway walls with inflammatory cells, particularly neutrophils. Inflammation
is followed by scarring and remodelling that thickens the walls resulting in narrowing of the small airway. Further progression leads to metaplasia (abnormal change in the tissue)
and fibrosis (further thickening and scarring) of the lower airway. The consequence of these changes is a limitation of airflow.
Emphysema
Emphysema is defined histologically as the enlargement of the air spaces distal to the terminal bronchioles, with destruction of their walls.
The enlarged air sacs (alveoli) of the lungs reduces the surface area available for the movement of gases during respiration. This ultimately leads to dyspnea in severe cases.
The exact mechanism for the development of
Emphysema is not understood, although it is known to be linked with smoking and age.
Diagnosis
The diagnosis of COPD is usually suggested by symptoms; it is a clinical diagnosis and no single test is definitive. A comprehensive history from the patient is very important with
regard to smoking and occupation. Physical examination with a plethysmograph can reveal the true extent of COPD.
The severity of COPD can be classified as follows using spirometry (see above):
| Severity | Post-bronchodilator FEV1/FVC | FEV1 % predicted |
| At risk | >0.7 | ≥80 |
| Mild COPD | ≤0.7 | ≥80 |
| Moderate COPD | ≤0.7 | 50-80 |
| Severe COPD | ≤0.7 | 30-50 |
| Very Severe COPD | ≤0.7 | <30 or 30-50 with Chronic Respiratory Failure symptoms |
Management
Although COPD is not curable, it can be controlled in a variety of ways.
Smoking Cessation
Smoking cessation is one of the most important factors in slowing down the progression of COPD. Even at a late stage of the disease it can reduce the rate of deterioration and
prolong the time taken for disability and death.
Occupational Change
Workers may be able to transfer to a significantly less contaminated area of the company depending on circumstances. Often however, workers may need complete occupational
change.
Pharmacotherapy
Bronchodilators
There are several types of bronchodilators used clinically with varying efficacy: β2 agonists, M3 antimuscarinics, leukotriene antagonists, cromones and xanthines. These drugs relax
the smooth muscles of the airway allowing for improved airflow. The change in FEV1 may not be substantial, but changes in the vital capacity are significant. Many patients feel less
breathless after taking bronchodilators.
β2 Agonists
There are several highly specific β2 agonists available. Salbutamol (Ventolin) is the most widely used short acting β2 agonist to provide rapid relief and should be prescribed as a
front line therapy for all classes of patients. Other β2 agonists are Bambuterol, Clenbuterol, Fenoterol, and Formoterol. Longer acting β2 agonists such as Salmeterol act too slowly
to be used as relief for dypsnea so these drugs should be used as a secondary therapy. An increased risk is associated with long acting β2 agonists due to decreased sensitivity to
inflammation so generally the use of a concomitant corticosteroid is indicated.
M3 Muscarinic Antagonists (Anticholinergics)
Derived from the deadly agaric Amanita muscaria, specific antimuscarinics were found to provide effective relief to COPD. Inhaled antimuscarinics have the advantage of avoiding
endocrine and exocrine M3 receptors. The quaternary M3 muscarinic antagonist Ipratropium is widely prescribed with the β2 agonist salbutamol. Ipratropium is offered combined
with salbutamol (Combivent) and with fenoterol (Duovent). Tiotropium provides improved specificity for M3 muscarinic receptors.
Cromones
Cromones are mast cell stabilizers that are thought to act on a chloride channel found on mast cells that help reduce the production of histamine and other inflammatory factors.
Chromones are also thought to act on IgE-regulated calcium channels on mast cells. Cromoglicate and Nedocromil, which has a longer half-life, are two chromones available.
Leukotriene Antagonists
More recently leukotriene antagonists block the signalling molecules used by the immune system. Montelukast, Pranlukast, Zafirlukast are some of the leukotrienes antagonists.
Xanthines
Theophylline is the prototype of the xanthine class of drug. Teas are natural sources of methylxanthines, xanthines and caffeine while chocolate is a source of theobromine. Caffeine
is approximately 16% metabolized into theophylline. Nebulized theophylline is used in the EMR for treatment of dyspnea (Difficulty in breathing). Patients need continual monitoring
as theophylline has a narrow therapeutic range. More aggressive EMR interventions include IV H1 antihistamines and IV dexamethasone.
Corticosteroids
Inhaled corticosteriods (specifically glucocorticoids) act in the inflammatory cascade and may improve airway function considerably, however the long term value has not been
proven. Corticosteroids are often combined with bronchodilators in a single inhaler. Some of the more common inhaled steroids in use are beclomethasone, mometasone, and
fluticasone.
Salmeterol and fluticasone are combined (Advair), however the reduction in death from all causes among patients with COPD in the combination therapy group did not reach the
predetermined level of statistical significance.
TNF Antagonists
Tumor necrosis factor antagonists (TNF) are the most recent class of medications designed to deal with refractory cases. Tumor necrosis factor-alpha is a cachexin or cachectin
and is considered a so-called biological drug. They are considerered immunosopressive with attendant risks. These rather expensive drugs include infliximab, adalimumab and
etanercept.
Vaccination
Patients with COPD should be routinely vaccinated against
influenza, pneumococcus and other diseases to prevent illness and the possibility of death.
Pulmonary Rehabilitation
Pulmonary rehabilitation is a program of disease management, counseling and exercise coordinated to benefit the individual. Pulmonary rehabilitation has been shown to relieve
difficulties breathing and fatigue. It has also been shown to improve the sense of control a patient has over their disease as well as their emotions.
Diet
A recent French study conducted over 12 years with almost 43,000 men concluded that eating a Mediterranean diet "halves the risk of serious lung disease like
Emphysema and
bronchitis".
Prognosis
A good prognosis of COPD relies on an early diagnosis and prompt treatment. Most patients will have improvement in lung function once treatment is started, however eventually
signs and symptoms will worsen as COPD progresses. The median survival is about 10 years if two-thirds of expected lung function was lost by diagnosis.
Bronchitis
Acute
bronchitis usually resolves in 7-10 days with no underlying lung disease. Chronic
bronchitis however is dependent on early recognition and smoking cessation which improves
the outcome significantly.
Emphysema
The outcome is better for patients with less damage to the lung who stop smoking immediately. Still, patients with extensive lung damage may live for many years so predicting
prognosis is difficult. Death may occur from respiratory failure, pneumonia, or other complications.
Asbestosis
The outcome is clouded by the many complications associated with asbestosis. Malignant mesothelioma is refractory to management affording patients with 6-12 months of life
expectancy upon clinical presentation.
Pneumoconiosis
The outcome is good for patients with minimal damage to the lung. However, patients with extensive lung damage may live for many years so predicting prognosis is difficult. Death
may occur from respiratory failure, pneumonia, cor pulmonale or other complications.
Pulmonary Neoplasms
The stage of the tumor(s) has a major impact on neoplasm prognosis. Staging is the process of determining tumor size, growth rate, potential metastasis, lymph node involvement,
treatment options and prognosis. Two-year prognosis for limited small cell pulmonary neoplasms is twenty percent and for extensive disease five percent. The average life
expectancy for someone with recurrent small cell pulmonary neoplasms is two to three months.
The 5-year overall survival rate for pulmonary neoplasms is 14%.
Epidemiology
According to the World Health Organization (WHO), 80 million people suffer from moderate to severe COPD and 3 million died due to it in 2005. The WHO predicts that by 2030, it will
be the 4th largest cause of mortality worldwide.
Since COPD is not diagnosed until it becomes clinically apparent, prevalence and mortality data greatly underestimate the socioeconomic burden of COPD. In the UK, COPD
accounts for about 7% of all days of sickness related absence from work.
Smoking rates in the industrialized world have continued to fall, causing rates of
Emphysema and pulmonary neoplasms to slowly decline.
While the cause of
ulcerative colitis is unknown, several, possibly interrelated, causes have been suggested.
(adapted from Wikipedia, the free encyclopedia http://en.wikipedia.org/wiki/Chronic_obstructive_pulmonary_disease)
Improving Outcomes for COPD Patients with Mild-to-Moderate Anxiety and Depression: A Systematic Review of Cognitive Behavioural Therapy
Authors: Coventry PA, Gellatly JL
Purpose
Anxiety and
depression are highly prevalent in patients with chronic obstructive pulmonary disease (COPD) and are associated with lower levels of self-efficacy, impaired
health status, poorer treatment outcomes and reduced survival following emergency admission. Cognitive behavioural therapy (CBT) may be effective for treating
anxiety and
depression in COPD patients but evidence for this is uncertain.MethodsA systematic review of controlled trials that evaluated the effectiveness of CBT for treating mild-to-moderate
anxiety or depression in adults with clinically stable COPD. Ovid electronic bibliographic databases were searched from inception to May 2006; all content held by the Cochrane
Library Issue 3, 2006 was also searched.ResultsOne small randomized controlled trial (RCT) of moderate quality showed that CBT, when given with exercise training and education,
was associated with large and significant treatment effects for both
anxiety (-1.39 (95% CIs -2.19, -0.59)) and depression (-0.86 (95% CIs -1.61, -0.11)). Additionally, a larger RCT of
higher quality demonstrated that CBT, when given with exercise and education, was associated with large and significant treatment effects for depression (-0.76
(95% CIs -1.34, -0.17)), but not for
anxiety. No other included study reported significant reductions in either
anxiety or
depression in COPD patients given CBT.ConclusionThere is
only limited evidence that CBT, when used with exercise and education, can contribute to significant reductions in
anxiety and depression in COPD patients. There is scope for a
well-powered RCT to evaluate the effectiveness and acceptability of CBT among this patient population
Journal: Br J Health Psychol. 2007 Apr 18
Adapted from PubMed; click here to access full journal article.
Emerging Trends in the Therapy of COPD: Novel Anti-Inflammatory Agents in Clinical Development
Authors: Fitzgerald MF, Fox JC
8/9 Spire Green Centre, Flex Meadow, Harlow, CM19 5TR, UK.
During the past ten years, the pharmaceutical industry has focussed on treating chronic obstructive pulmonary disease (COPD) as distinct to
asthma, and no novel anti-inflammatory
agents have been launched as therapies for this disease. As our understanding of the pathology of COPD has increased it has been established that the progressive pulmonary
inflammation that is associated with COPD relates to disease severity. Thus, it is anticipated that drugs that reduce pulmonary inflammation will provide effective, disease-modifying
therapies. Here, we consider the potential of anti-inflammatory drugs that are currently in clinical development for COPD and discuss how these might reduce pulmonary
inflammation in this disease.
Journal: Drug Discov Today. 2007 Jun;12(11-12):479-86. Epub 2007 May 7.
Adapted from PubMed; click here to access full journal article.
Nasal and Sinus Inflammation in Chronic Obstructive Pulmonary Disease
Authors: Kim JS, Rubin BK
Department of Otolaryngology, Kyungpook National University. Daegu. Korea.
Epidemiologic studies suggest that as many as 75% of patients with COPD have concomitant nasal symptoms and more than 1/3 of patients with sinusitis also have lower airway
symptoms of
asthma or COPD. Because the inflammatory response of the upper and lower airways are similar, and both sites have a similar exposure to allergens and irritants, it
is not surprising that rhinitis or sinusitis would coexist with COPD. Possible mechanisms of combined upper and lower airway dysfunction include the so-called nasal-bronchial
reflex, inflammation caused by smoking, mouth breathing caused by nasal obstruction, and pulmonary aspiration of nasal contents. Patients with chronic sinusitis commonly have
nonspecific bronchial hyperresponsiveness, suggesting a neural reflex. Postnasal drainage of nasal inflammatory mediators during sleep also may increase lower airway
responsiveness. Therapy of nasal and sinus disease is associated with improved pulmonary function in patients with COPD.
Journal: COPD. 2007 Apr-Jun;4(2):163-6
Adapted from PubMed; click here to access full journal article.
Impact of Regular Inhaled Corticosteroid Use on Chronic Obstructive Pulmonary Disease Outcomes
Authors: Vollmer WM, Peters D, Crane B, Kelleher C, Buist AS.
Center for Health Research, Kaiser Permanente Northwest. Portland, OR
Inhaled corticosteroids are often used to manage chronic obstructive pulmonary disease, although the evidence regarding their long-term efficacy in preventing or reducing adverse
health outcomes is not definitive. This retrospective cohort study analyzed whether regular inhaled corticosteroid use is associated with reduced health care utilization and all-cause
mortality related to chronic obstructive pulmonary disease. Subjects were 2,902 health maintenance organization members aged 50 and over who met criteria for chronic obstructive
pulmonary disease. The study used a composite endpoint of time to (1) death or (2) hospitalization or emergency room care related to chronic obstructive pulmonary disease,
whichever occurred first, during a 4-year follow-up. Among the 42% of chronic obstructive pulmonary disease patients with an indication of co-morbid
asthma, inhaled corticosteroid
use was associated with significantly reduced risk for both all-cause mortality and the composite outcome. The reduction in risk was greatest in never- and ex-smokers. Among
chronic obstructive pulmonary disease patients with no indication of asthma, inhaled corticosteroid use was associated with reduced risk only in never smokers. These findings
generally persisted in separate analyses stratified by
asthma status and in sensitivity analyses using four alternative definitions of regular medication use, with comparable results
when regular medication use was treated as a fixed covariate defined at the start of follow-up. We conclude that use of inhaled corticosteroids was associated with reduced risk of
chronic obstructive pulmonary disease exacerbations and all-cause mortality. This benefit was most pronounced among never-smokers and in those with evidence of co-morbid
asthma.
Journal: COPD. 2007 Apr-Jun;4(2):135-42
Adapted from PubMed; click here to access full journal article.
Survival Among COPD Patients Using Fluticasone/Salmeterol in Combination Versus Other Inhaled Steroids and Bronchodilators Alone
Authors: Mapel DW, Nelson LS, Lydick E, Soriano J, Yood MU, Davis KJ.
Lovelace Clinic Foundation. Albuquerque, NM.
Recent retrospective studies have suggested that use of inhaled corticosteroids (ICS) may improve survival in chronic obstructive pulmonary disease (COPD), particularly when
combined with a long-acting beta-agonist (LABA). However, the study methodologies have been questioned, and no study has examined the survival effect of the newer combination
ICS/LABA inhalers. The goal of this project was to further examine the relationship between ICS treatment, with or without LABA, and survival in COPD. COPD patients were identified
from the administrative databases of four different integrated health care delivery systems. All patients who were diagnosed with COPD between September 1, 2000 and August 31,
2001 and who had at least 3 months treatment with either a combined fluticasone/salmeterol inhaler (FSI, N = 866), any ICS used with a LABA (ICS/LABA, N = 525), ICS alone (N =
742), LABA alone (N = 531), or a short-acting bronchodilator alone (SABD, N = 1832), were included. Analyses were conducted using three different analysis approaches that adjust
for various biases that may affect the results. In the basic Cox proportional hazards models, use of FSI, ICS/LABA, ICS alone, and LABA alone had significant survival benefits as
compared to SABD, after adjustment for differences in age, gender, comorbidities,
asthma status, and disease severity (HRs 0.61 [0.45-0.83], 0.59 [0.46-0.77], 0.76 [0.61-0.95],
0.75 [0.57-0.98], respectively). Propensity score matching to reduce the clinical differences between the treatment groups versus the SABD reference group found very similar results.
Nested case-control analyses, which are based on survival status instead of treatment, continued to show a significant survival benefit for FSI, ICS/LABA, and ICS alone. Treatment
with FSI or another ICS with or without LABA is associated with improved survival in COPD. The treatment benefit is reproducible and is robust to application of a number of different
analysis techniques designed to adjust for differences in confounding variables and for bias by indication.
Journal: COPD. 2007 Apr-Jun;4(2):127-34
Adapted from PubMed; click here to access full journal article.
Activity Monitoring and Energy Expenditure in COPD Patients: A Validation Study
Authors: Patel SA, Benzo RP, Slivka WA, Sciurba FC
Division of Pulmonary, Allergy, and Critical Care Medicine, University of Pittsburgh. Pittsburgh, PA
There is increasing interest in the objective measurement of physical activity in chronic obstructive pulmonary disease (COPD) patients due to the close relationship between
physical activity level, health, disability and mortality. We aimed to (a) determine the validity and reproducibility of an activity monitor that integrates accelerometry with multiple
physiologic sensors in the determination of energy expenditure in COPD subjects and (b) to document the independent contribution of the additional physiologic sensors to
accelerometry measures in improving true energy expenditure determination. Eight subjects (4 male, FEV(1) 56.4 +/- 14.1%, RV 145.0 +/- 75.7%) performed 2 separate 6-minute
walk and 2 incremental shuttle walk exercise tests. Energy expenditure was calculated during each exercise test using the physiologic activity monitor and compared to a validated
exhaled breath metabolic system. Test-retest reproducibility of physiologic activity monitor during the walking tests was comparable to an exhaled breath metabolic system.
Physiologic sensor data significantly improved the explained variance in energy expenditure determination (r(2) = 0.88) compared to accelerometry data alone (r(2) = 0.68). This
physiologic activity monitor provides a valid and reproducible estimate of energy expenditure during slow to moderate paced walking in a laboratory setting and represents an
objective method to assess activity in COPD subjects.
Journal: COPD. 2007 Apr-Jun;4(2):107-12
Adapted from PubMed; click here to access full journal article.
Potentially Avoidable Hospitalizations for COPD and Pneumonia: The Role of Physician and Practice Characteristics
Authors: O’malley AS, Pham HH, Schrag D, Wu B, Bach PB
From the *Center for Studying Health System Change, Washington, DC; †Epidemiology and Biostatistics, Memorial Sloan Kettering Cancer Center, New York, New York;
and ‡Social & Scientific Systems, Inc., Silver Spring, Maryland
BACKGROUND:: Hospitalizations for bacterial pneumonia and chronic obstructive pulmonary disease (COPD) occur frequently, but many are potentially avoidable. OBJECTIVE:: To
examine associations between elderly patients' usual physician and practice characteristics, and the risk of hospitalization for bacterial pneumonia and COPD. RESEARCH
DESIGN:: Time-to-event analysis of Medicare claims from 2000 (baseline year) through 2001-2002 (follow-up years) for beneficiaries whose usual physician participated in the
2000-2001 Community Tracking Study Physician Survey. SUBJECTS:: A total of 509,613 patients and 5764 physicians for pneumonia hospitalizations; subset of 91,318
beneficiaries with an antecedent diagnosis of COPD and 5074 physicians for COPD hospitalizations. MEASURES:: Hospitalizations for bacterial pneumonia or COPD occurring
in 2001-2002. RESULTS:: Beneficiaries whose usual physician had been in practice for >10 years (vs. </=10 years) were at lower risk for both pneumonia (AHR [adjusted
hazard ratio] 0.88, 95% CL [confidence limits] 0.82-0.94, and COPD hospitalization (AHR 0.87, 95% CL 0.80-0.96). Risk of hospitalization for COPD was lower among beneficiaries
whose usual physician reported that clinical practice guidelines had an important effect, compared with those reporting relatively little impact, on their clinical practice (AHR 0.88,
95% CL 0.80-0.96). Patients had higher risk of both types of hospitalizations if their physician's practice had >5% Medicaid revenue (vs. 0-5%, P < 0.0001), or reported more
(vs. less) difficulty securing ancillary services (P < 0.01 for bacterial pneumonia and P = 0.05 for COPD). Patient socioeconomic status, previous respiratory hospitalizations,
and comorbidities had the strongest associations with hospitalization. CONCLUSIONS:: Given that physicians who report limited access to ancillary services and high Medicaid
case volume have patients who experience higher rates of admission for COPD and pneumonia, additional resources and quality improvement interventions targeting these
providers should be priorities.
Journal: Med Care. 2007 Jun;45(6):562-570
Adapted from PubMed; click here to access full journal article.
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