Etiology

Pulmonary edema is defined as an excess of fluid in the extravascular compartment of the lung and is classified into four categories based on pathophysiology: hydrostatic edema, permeability edema with diffuse alveolar damage, permeability edema without diffuse alveolar damage, and mixed edema resulting from hydrostatic and permeability edema. Permeability pulmonary edema is almost always a manifestation of capillary endothelial injury or alveolar epithelial damage with resultant loss of fluid and protein into the airspaces or interstitium. Less commonly, permeability edema may occur in the absence of diffuse alveolar damage, such as in patients with the hantavirus pulmonary syndrome or after interleukin therapy. Patients who have permeability edema were originally classified clinically into two groups: those with acute lung injury and those with acute respiratory distress syndrome (ARDS). However, this definition, which was recommended by the American-European Consensus Conference in 1994, was refined in 2011, with the new outline being referred to as the Berlin definition . That updated definition removes the term acute lung injury and includes four clinical criteria for a diagnosis of ARDS. Those criteria focus on (1) timing (acute onset within 1 week of clinical insult or onset of respiratory symptoms), (2) chest imaging (bilateral opacities representing an airspace process on chest radiography or computed tomography [CT]), (3) origin of edema (respiratory failure not fully explained by cardiac failure or fluid overload), (4) oxygenation (now based on PaO ₂ /FiO ₂ [partial pressure of oxygen in arterial blood/forced inspiratory oxygen] ratio while on 5 cm of continuous positive airway pressure [CPAP]). The three categories of oxygenation are mild (PaO ₂ /FiO ₂ of 201–300), moderate (PaO ₂ /FiO ₂ of 101–200), and severe (PaO ₂ /FiO ₂ of ≤100).

The majority of patients who are at increased risk for the development of ARDS can be classified into two categories: pulmonary (or direct injury) and extrapulmonary (or indirect injury). The main causes of direct lung injury are pneumonia and aspiration; the main causes of indirect lung injury are sepsis, major trauma, and multiple transfusions. A large cohort study reported that the most common risk factor is severe sepsis with a suspected pulmonary source, followed by severe sepsis with a suspected extrapulmonary source. In some series, sepsis (pulmonary or extrapulmonary), pneumonia, aspiration of gastric contents, and major trauma account for more than 85% of causes of ARDS. Other more rare causes include burns, drug overdose, near drowning, postperfusion injury after cardiopulmonary bypass, pancreatitis, fat embolism, and high-altitude pulmonary edema.

Prevalence and Epidemiology

An accurate estimate of the incidence of ARDS has been hampered by the lack of a uniform definition and the heterogeneity of the causes and clinical manifestations. An early estimate by the National Institutes of Health (NIH) suggested that the annual incidence in the United States was 75 per 100,000 population, and a more recent study from 2005 demonstrated an incidence of 86 per 100,000. It is currently estimated that there are approximately 190,000 case annually in the United States, resulting in 75,000 deaths.

Clinical Presentation

Patients with permeability edema typically present with acute onset of shortness of breath (generally <72 hours after initial onset or inciting event), bilateral parenchymal opacities on imaging, and refractory hypoxemia and no significant evidence of left-sided heart failure.

ARDS is often associated with other organ failure. Patients who die early (within the first 72 hours of ARDS onset [26%–44%]) usually die of the presenting injury or illness that resulted in ARDS. Patients whose deaths occur late (>72 hours after ARDS onset [56%–74%]) most often die of complications (i.e., new organ failures) that arose during the course of ARDS. Although the mortality rate for patients with ARDS has declined from 50% to 70% in the 1980s to 35% to 46% in 2014, the distribution of causes of death has not changed. Sepsis with multiorgan failure is the most common cause of death (30%–50%), whereas respiratory failure results in a smaller percentage of deaths (13%–19%). The increased survival during the past 2 decades is due largely to advances in supportive care, such as dialysis, and a decrease in extrapulmonary organ failure. Nevertheless, survival for those patients who have sepsis syndrome has not changed appreciably.

Clinical Presentation

Patients with permeability edema typically present with acute onset of shortness of breath (generally <72 hours after initial onset or inciting event), bilateral parenchymal opacities on imaging, and refractory hypoxemia and no significant evidence of left-sided heart failure.

ARDS is often associated with other organ failure. Patients who die early (within the first 72 hours of ARDS onset [26%–44%]) usually die of the presenting injury or illness that resulted in ARDS. Patients whose deaths occur late (>72 hours after ARDS onset [56%–74%]) most often die of complications (i.e., new organ failures) that arose during the course of ARDS. Although the mortality rate for patients with ARDS has declined from 50% to 70% in the 1980s to 35% to 46% in 2014, the distribution of causes of death has not changed. Sepsis with multiorgan failure is the most common cause of death (30%–50%), whereas respiratory failure results in a smaller percentage of deaths (13%–19%). The increased survival during the past 2 decades is due largely to advances in supportive care, such as dialysis, and a decrease in extrapulmonary organ failure. Nevertheless, survival for those patients who have sepsis syndrome has not changed appreciably.

Pathophysiology

The histologic features of ARDS are characterized by diffuse alveolar damage and represent a time-dependent, stereotypic response to acute lung injury. The changes can be viewed as evolving from epithelial and endothelial necrosis to alveolar collapse and eventually to fibroblast proliferation and fibrosis. Permeability edema is prominent in the early stages and heralds the onset of rapidly progressive fibroblast proliferation, which predominates in the late phase of disease. The microscopic appearance varies according to both the time interval between injury and biopsy and the extent and localization of the injury. Diffuse alveolar damage has traditionally been divided into three sequential and overlapping phases: the acute exudative phase of edema and hemorrhage, the subacute proliferative phase of organization and repair, and the fibrotic phase of collagen deposition and end-stage fibrosis. The last two phases are designated the fibroproliferative phase. It is of clinical importance that the histologic features of diffuse alveolar damage correlate with the duration of injury more than with its initiating cause.

The acute exudative phase predominates within the first 7 days of injury and is characterized by edema, intraalveolar hemorrhage, and hyaline membrane formation ( Fig. 55.1 ). The histologic changes in the early exudative phase consist of capillary congestion, alveolar edema, and intraalveolar hemorrhage. Hyaline membranes, the histologic hallmark of this stage of the lesion, develop later and are most numerous 3 to 7 days after injury. Fibrin thrombi may be seen in the alveolar capillaries and pulmonary arterioles.

Acute exudative phase of diffuse alveolar damage caused by sepsis. (A) Pathologic specimen shows characteristic intraalveolar hyaline membranes (arrows) and exudates. (B) Chest radiograph shows extensive bilateral ground-glass opacities and consolidation. (C) High-resolution CT scan at the level of the right upper lobe shows patchy ground-glass opacities demarcated by secondary lobules and associated with dependent consolidation.

In the subacute proliferative phase of diffuse alveolar damage, fibroblast proliferation, mainly within the interstitium but also within airspaces, becomes prominent ( Fig. 55.2 ). The proliferation of alveolar type 2 pneumocytes, which is seen as early as 3 days after injury and is a reparative phenomenon, occurs in the early proliferative phase and persists throughout this phase. Within the interstitium, fibroblasts and myofibroblasts proliferate and subsequently migrate into fibrinous intraalveolar exudate and convert the exudate to cellular granulation tissue. With the proliferation of fibroblasts (subacute proliferative phase), there is remodeling of the parenchyma, resulting in dilatation of the bronchi (traction bronchiectasis) and bronchioles (traction bronchiolectasis). Subsequently, typically 2 weeks or more after the injury, there is progressive fibrosis with collagen deposition (chronic fibrotic phase; Fig. 55.3 ). Microcystic airspaces 1 mm or larger in diameter (microscopic honeycombing) and traction bronchiectasis and bronchiolectasis are most pronounced in the late fibrotic phase. Cyst-like spaces in end-stage ARDS may also result from chronic interstitial emphysema.

Subacute proliferative phase of diffuse alveolar damage caused by viral pneumonia (3–7 days after the onset of lung injury). (A) Pathologic specimen shows diffuse fibroblastic proliferation (arrows) within the interstitium associated with organized hyaline membranes. (B) Chest radiograph demonstrates bilateral ground-glass opacities, consolidation, and low lung volumes. (C) High-resolution CT scan at the level of the right upper lobe bronchus shows extensive ground-glass opacities with associated reticulation and traction bronchiectasis (arrows).

Chronic fibrotic phase of diffuse alveolar damage from acute interstitial pneumonia (2 weeks after the onset of lung injury). (A) Pathologic specimen shows dilated alveolar spaces and architectural distortion caused by interstitial collagen deposition. (B) Chest radiograph shows low lung volumes with bilateral middle and lower lung zone–predominant ground-glass opacities and coarse reticulation. (C) High-resolution CT scan at the level of the right middle lobe shows extensive ground-glass opacities associated with reticulation (crazy paving pattern), traction bronchiectasis, and cystic changes (arrows).

Manifestations of the Disease

Radiography

In the initial phase of ARDS, the parenchymal abnormalities may be mild and the chest radiograph normal. In some cases the lung volumes may be decreased because of shallow breathing and tachypnea. Characteristic radiographic findings of the exudative phase of ARDS consist of extensive bilateral ground-glass opacities and consolidation ( Fig. 55.4 ; see also Fig. 55.1 ). Their distribution may be patchy or diffuse and symmetric or asymmetric, and they may involve all lung zones to a similar extent or mainly the upper or lower lung zones. The bronchi typically remain patent, resulting in air bronchograms (see Fig. 55.4 ). With progression to the fibroproliferative phase, a coarse reticular pattern is seen superimposed on the ground-glass opacities, and there is progressive volume loss (see Figs. 55.2 and 55.3 ). The radiographic findings are markedly influenced by the positive end-expiratory pressure ventilation that is routinely used in patients with extensive permeability edema.

Acute respiratory distress syndrome: radiographic findings. (A) Admission radiograph showing mild bronchial wall thickening and diffuse interstitial opacities. (B) Thirty-six hours later, both lungs show extensive consolidation with air bronchograms.

Computed Tomography

Similar to the radiograph, the CT findings may be normal in the early phase of ARDS, but an abnormality is usually detected within 12 hours. The CT findings have been shown to correlate well with the pathologic phases of diffuse alveolar damage. In the exudative and early proliferative phase of diffuse alveolar damage, CT typically shows extensive bilateral ground-glass opacities with or without associated consolidation ( Fig. 55.5 ; see also Fig. 55.1 ). Interlobular septal thickening is frequently superimposed on the ground-glass opacities, resulting in a pattern known as crazy paving ( Fig. 55.6 ). This interlobular septal thickening corresponds histologically to edematous thickening in the exudative phase and to alveolar collapse adjacent to interlobular septa and subsequent organization in the proliferative or fibrotic phase of diffuse alveolar damage. In the early stages the consolidation, when present, tends to have a patchy distribution. Later in the exudative phase, the consolidation becomes more homogeneous and gravity dependent (see Fig. 55.6 ). In the late proliferative and fibrotic phase, the CT findings also include traction bronchiectasis and bronchiolectasis associated with loss of lung volume (as demonstrated by displacement or distortion of interlobar fissures, bronchi, or vessels; see Figs. 55.2 and 55.3 ). In the fibrotic phase, coarse reticular opacities and small cystic spaces caused pathologically by marked restructuring of distal airspaces and interstitial dense fibrosis are also seen ( Fig. 55.7 ; see also Fig. 55.3 ). In some patients the distribution of residual fibrosis after resolution of the airspace disease will be anterior lung predominant ( Fig. 55.8 ).

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