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Respiratory System
Acute respiratory distress syndrome (ARDS) is an acute and persistent lung disease
characterized by an arterial hypoxemia (PaO2/FiO2<200 mmHg), resistant to oxygen
therapy and bilateral infiltrates on chest X ray’ (Lucangelo et al). Brunner and
Suddarth defined ARDS is a clinical syndrome characterized by a sudden and
progressive pulmonary edema, increasing bilateral infiltrates on chest x-ray,
hypoxemia refractory to oxygen supplementation, and reduced lung compliance.
These signs occur in the absence of left-sided heart failure. Patients with ARDS
usually require mechanical ventilation with a higher-than normal airway pressure.
In general, ARDS has two different pathogeneses: a direct ‘pulmonary’ insult to the
lung cell or an indirect ‘‘extrapulmonary’ insult resulting in a systemic inflammatory
response. ARDS is a progressive disease, with different stages, different mediators,
and both inflammatory and anti-inflammatory activity (cellular and humoural). At the
beginning of the inflammatory response, changes occur in the alveolar capillary
barrier, including the formation of a protein-rich fluid, alteration of surfactant and
migration into the lung of neutrophils, lymphocytes and macrophages. Plasma factors,
such as complement, and mediators generated by the cells, such as cytokines, oxidants
and leucotrienes, are secreted inappropriately and at high levels. Resolution of the
disease starts with a decrease in the levels of inflammatory mediators, the migration
of fibroblasts into the lung, collagen deposition and the re-absorption of oedema fluid.
In the acute phase of ARDS, damage to the alveolar capillary barrier, including an
increase in its permeability, causes the accumulation of a protein-rich fluid. The
degree of injury to the epithelium and endothelium influences both the severity of
lung injury and the clinical outcome. The protein-rich fluid may gradually become
organised, producing the characteristic hyaline membrane that further destroys the
alveolar structure.
In the early phases of ARDS, there is an intense alveolar inflammatory process that is
characterized by the local accumulation and activation of neutrophils and
macrophages. These cells, in turn, release oxidants and inflammatory mediators. The
lung per se has a large reservoir of alveolar and interstitial macrophages, both of
which come from blood monocytes. Alveolar macrophages release oxygen
metabolites, cytokines, hormones, proteases and anti-proteases, all of which are
fundamental for normal lung homeostasis and have the ability to eliminate
microorganisms. According to an animal model of lung injury, there is an initial
accumulation of neutrophils and then macrophages, which is followed by resolution
of the inflammatory process. During phagocytosis, macrophages produce oxygen
radicals and proteases, which eliminate most particulate matter and microorganism
from the distal airways, thus keeping the alveoli ‘clean’. Similar to macrophages,
neutrophils secrete several enzymes, such as hydrolases, myeloperoxidate, lysozyme
and neutral proteases, which can cause further damage to the injured lung. In the
presence of lung injury there is also breakdown of alveolar cells, with the subsequent
release of nuclear debris and membrane damage and thus activation of the
complement pathway.
Trauma is the most common cause of ARDS, possibly because trauma-related factors,
such as fat emboli, sepsis, shock, pulmonary contusions, and multiple transfusions,
increase the likelihood of microemboli developing.
The primary focus in the management of ARDS includes identification and treatment
of the underlying condition. Aggressive, supportive care must be provided to
compensate for the severe respiratory dysfunction. This supportive therapy almost
always includes intubation and mechanical ventilation. In addition, circulatory
support, adequate fluid volume, and nutritional support are important. Supplemental
oxygen is used as the patient begins the initial spiral of hypoxemia. As the hypoxemia
progresses, intubation and mechanical ventilation are instituted. The concentration of
oxygen and ventilator settings and modes are determined by the patient’s status. This
is monitored by arterial blood gas analysis, pulse oximetry, and bedside pulmonary
function testing.