Dr. Hassan Ghobadi Assistant Professor of Internal MedicineArdabil University of Medical Sciences
In the name of GOD
COPD
COPDCOPD is present only if chronic airflow obstruction occurs.
Emphysema , An anatomically defined condition characterized by
destruction and enlargement of the lung alveoli. Chronic bronchitis, A clinically defined condition with chronic cough and
phlegm.
Small airways disease, a condition in which small bronchioles are narrowed.
COPD COPD is the fourth leading cause of death
COPD will rise from the fourth to the third most common cause of death worldwide by 2020.
COPD is characterized by airflow limitation that is not fully reversible.
The airflow limitation is usually progressive and associated with an abnormal inflammatory response.
Risk Factors
Cigarette Smoking (90%) Second-Hand, Smoking Exposure ( SHS ) Airway Hyper Responsiveness (AHR) Respiratory Infections Occupational Exposures Air Pollution Genetic Considerations Alpha 1 Antitrypsin Deficiency (1–2%)
Natural History
The effects of cigarette smoking on pulmonary function appear to depend on the intensity of smoking exposure.
The timing of smoking exposure.
The risk of mortality from COPD is closely associated with
reduced levels of FEV1.
Smoking cessation at an earlier age providing a more beneficial effect.
Genetic factors
Pathophysiology
Persistent reduction in forced expiratory flow rates.
Increases in the residual volume and the residual volume/total lung capacity ratio.
Nonuniform distribution of ventilation, and ventilation-perfusion mismatching.
Pathophysiology
Airflow Obstruction Hyperinflation (air trapping ) Gas Exchange
The PaO2 usually remains near normal until the FEV1 is decreased to ~50% of predicted,
An elevation of PaCO2 is not expected until the FEV1 is <25% of predicted.
Pathology
Cigarette smoke exposure may affect the large airways, small airways ( 2 mm diameter), and alveolar space.
Changes in large airways cause cough and sputum, while changes in small airways and alveoli are responsible for physiologic alterations.
Pathology
Pathology (Large
Airway) Mucous gland enlargement and goblet cell
hyperplasia (not related to airflow limitation ).
Bronchi also undergo squamous metaplasia, which not only predisposes to carcinogenesis but also disrupts mucociliary clearance.
smooth-muscle hypertrophy and bronchial hyperreactivity.
Pathology (Small Airway)
The major site of increased resistance is in airways less than 2 mm diameter.
Infiltrating mononuclear inflammatory cells.
Smooth-muscle hypertrophy may also be present.
loss of elastic recoil and increased resistance to airflow in small airways.
Pathology (Parenchyma)
Emphysema is characterized by destruction of gas-exchanging airspaces.
Bronchoalveolar lavage fluid contains roughly five times as many macrophages as lavage from nonsmokers.
In smokers' lavage fluid, macrophages comprise >95% of the total cell count.
T lymphocytes, particularly CD8+ cells, are also increased in the alveolar space of smokers.
Pathology (Parenchyma)
Emphysema is classified into distinct pathologic types: Centriacinar, and Panacinar.
1- Centriacinar emphysema, the type most frequently associated with cigarette smoking, is characterized by enlarged airspaces found (initially) in association with respiratory bronchioles.
Centriacinar emphysema is most prominent in the upper lobes and superior segments of lower lobes and is often quite focal.
2- Panacinar emphysema refers to abnormally large airspaces evenly distributed within and across acinar units.
Panacinar emphysema is usually observed in patients with 1AT deficiency, which has a predilection for the lower lobes.
Pathogenesis (1) Chronic exposure to cigarette smoke may lead to
inflammatory cell recruitment within the terminal airspaces of the lung.
(2) These inflammatory cells release elastolytic
proteinases which damage the extracellular matrix of the lung.
(3) Loss of matrix-cell attachment leads to apoptosis of structural cells of the lung.
(4) Ineffective repair of elastin and perhaps other extracellular matrix components result in airspace enlargement that defines pulmonary emphysema.
LUNG INFLAMMATIONLUNG INFLAMMATION
COPD PATHOLOGYCOPD PATHOLOGY
OxidativeOxidativestressstress ProteinasesProteinases
Repair Repair mechanismsmechanisms
Anti-proteinasesAnti-proteinasesAnti-oxidantsAnti-oxidants
Host factorsAmplifying mechanisms
Cigarette smokeCigarette smokeBiomass particlesBiomass particles
ParticulatesParticulates
Pathogenesis of COPD
YYYYYY
Mast cellMast cell
CD4+ cellCD4+ cell(Th2)(Th2)
EosinophilEosinophil
AllergensAllergens
Ep cellsEp cells
ASTHMAASTHMA
BronchoconstrictionBronchoconstrictionAHRAHR
Alv macrophageAlv macrophage Ep cellsEp cells
CD8+ cellCD8+ cell(Th1)(Th1)
NeutrophilNeutrophil
Cigarette smokeCigarette smoke
Small airway narrowingSmall airway narrowingAlveolar destructionAlveolar destruction
COPDCOPD
Reversible IrreversibleAirflow LimitationAirflow Limitation
Pathogenesis
The Elastase, Antielastase Hypothesis
This hypothesis was based on the clinical observation that patients with genetic deficiency in Alpha 1 AT .
Inflammation and Extra cellular Matrix Proteolysis Exposure to oxidants from cigarette smoke.
Cell Death Inflammatory cell proteinases degrade lung extracellular matrix , with
subsequent loss of cell anchoring leading to apoptosis.
Ineffective Repair Following injury, the ability of lung to repair damaged alveoli appears limited.
COPD (Clinical Presentation ) The three most common symptoms:
Cough, sputum production, and exertional dyspnea
Physical Findings
Nicotine staining of fingernails, prolonged expiratory phase, signs of hyperinflation, use of accessory muscles of respiration, tripod position, cyanosis, pink puffers, blue bloaters, weight loss, bitemporal wasting,
Hoover's sign (the result of alteration of the vector of diaphragmatic contraction on the rib cage as a result of chronic hyperinflation ).
Clubbing of the digits is not a sign of COPD
COPD (Laboratory Findings ) The hallmark of COPD is airflow obstruction reduction in
FEV1 and FEV1/FVC .
With worsening disease severity, lung volumes may increase, resulting in an increase in total lung capacity, functional residual capacity, and residual volume.
In patients with emphysema, the diffusing capacity may be reduced, reflecting the parenchymal destruction characteristic of the disease.
The degree of airflow obstruction is an important prognostic factor in COPD and is the basis for the GOLD disease
classification
COPD (PFT) Stage I: Mild FEV1/FVC < 0.70
FEV1 > 80% predicted
Stage II: Moderate FEV1/FVC < 0.70 50% < FEV1 < 80% predicted
Stage III: Severe FEV1/FVC < 0.70 30% < FEV1 < 50% predicted
Stage IV: Very Severe FEV1/FVC < 0.70
FEV1 < 30% predicted or FEV1 < 50% predicted plus
chronic respiratory failure
COPD (Imaging Findings )
Radiographic studies may assist in the classification of the type of COPD.
Obvious bullae, paucity of parenchymal markings, or hyperlucency suggest the presence of emphysema.
Increased lung volumes and flattening of the diaphragm suggest hyperinflation.
Computed tomography (CT) scan is the current
definitive test for establishing the presence of emphysema.
Imaging Findings
SYMPTOMScoughcoughsputumsputum
shortness of breathshortness of breath
EXPOSURE TO RISKFACTORS
tobaccotobaccooccupationoccupation
indoor/outdoor pollutionindoor/outdoor pollution
SPIROMETRYSPIROMETRY
Diagnosis of COPDDiagnosis of COPD
COPD ( Treatment )
Emphysema is incurable, but it can be treatedCOPD is a preventable and treatable disease
Smoking cessation,
Oxygen therapy in hypoxemic patients, Lung volume reduction surgery in selected
patients with emphysema,
Pharmacotherapy,
Treatment (Pharmacotherapy)
Anticholinergic Agents
Does not appear to influence the rate of decline of lung function,
It improves symptoms and produces acute improvement in FEV1.
Beta Agonists These provide symptomatic benefit. The main side effects are
tremor and tachycardia.
The addition of a beta 2 agonist to inhaled anticholinergic therapy has been demonstrated to provide incremental benefit.
Using a long-acting beta 2 agonist without concomitant inhaled corticosteroids have an increased risk of deaths from respiratory causes.
Treatment (Pharmacotherapy) Inhaled GlucocorticoidsInhaled glucocorticoids reduce exacerbation frequency by ~25%.
A more recent meta-analysis suggests that they may also reduce mortality by ~25%.
A trial of inhaled glucocorticoids should be considered in patients with frequent exacerbations, defined as two or more per year, and in patients who demonstrate a significant amount of acute reversibility in response to inhaled bronchodilators.
Oral GlucocorticoidsThe chronic use of oral glucocorticoids for treatment of COPD is
not recommended .
The chronic use of oral glucocorticoids is associated with significant side effects.
Treatment (Pharmacotherapy)Theophylline
1- Theophylline produces modest improvements in expiratory flow rates and vital capacity .
2- Theophylline improve arterial oxygen and carbon dioxide levels in patients with moderate to severe COPD.
3- Nausea is a common side effect; tachycardia and tremor have also been reported.
4- Theophylline has an anti inflammatory effects.
Treatment (Pharmacotherapy)Oxygen1- Oxygen therapy decrease mortality in patients with COPD.
2- Oxygen therapy have a significant impact on mortality.
3- For patients with resting hypoxemia resting O2 sat. <88%
4- For patients with resting hypoxemia resting O2 sat. <90% with signs of pulmonary hypertension Right heart failure COPD with erythrocytosis.
5- Supplemental O2 is commonly prescribed for patients with exertional hypoxemia or nocturnal hypoxemia.
Exacerbations of COPD
Bacterial infections play a role in many, but by no means all, episodes.
Viral respiratory infections are present in approximately one-third of COPD exacerbations.
In a significant minority of instances (20–35%), no specific precipitant can be identified.
chronic suppressive or "rotating" antibiotics are not beneficial in patients with COPD.
Exacerbations of COPD (2)
Chronic oral glucocorticoids are not recommended for this purpose.
Inhaled glucocorticoids did reduce the frequency of
exacerbations by 25–30% .
The use of inhaled glucocorticoids should be considered in patients with frequent exacerbations .
In COPD exacerbation most frequent CXR findings being pneumonia and congestive heart failure.
Acute Exacerbations
1- BronchodilatorsInhaled beta 2 agonist, often with anticholinergic agent, methylxanthines.
2- AntibioticsThe choice of antibiotic should be based on local patterns of antibiotic
susceptibility of the common pathogens as well as the patient's clinical condition.
3- GlucocorticoidsThe use of glucocorticoids has been demonstrated to reduce the length
of stay, hasten recovery, and reduce the chance of subsequent exacerbation or relapse for a period of up to 6 months.
The GOLD guidelines recommend 30–40 mg of oral prednisolone or its equivalent for a period of 10–14 days.
Acute Exacerbations
4- Oxygen
Supplemental O2 should be supplied to keep arterial saturations 90%.
5- Mechanical Ventilatory Support