High-altitude pulmonary oedema (HAPE) is a potentially fatal altitude illness affecting individuals within 2–4 days of rapid ascent to altitudes above 3,000 m. Although a minority of high-altitude travellers develop HAPE 1, there is some suggestion that many develop subclinical fluid accumulation without overt alveolar flooding 2. The inciting mechanism of the injury to the lung in HAPE still generates some controversy. However, there is an ever-growing body of evidence that mechanical injury to the pulmonary capillaries induced by high transmural pressures starts a cascade of events that ultimately results in the development of HAPE. This injury, termed “stress failure” described by West et al. 3, refers to mechanically induced breaks in the blood-gas barrier, and these have been suggested to be important the pathophysiology of a number of human diseases 4.
In animals, when pulmonary capillaries are subjected to increased transmural pressure, ultrastructural changes consisting of discrete areas of damage to the blood–gas barrier, with rupture of the capillary endothelium, extracellular matrix and the alveolar epithelium, interspersed with large areas of structurally intact blood–gas barrier are observed 5. Accompanying this is increased permeability of the lung to protein and red blood cells, as measured by increased concentrations in bronchoalveolar lavage fluid 6. Leukotriene (LT)B4 concentration is also increased in bronchoalveolar lavage fluid 6, perhaps representing cellular activation by exposed basement membrane. Similar findings are observed in some humans following maximal exercise in normoxia 7 where bronchoalveolar lavage fluid contains increased concentrations of red cells, protein and LTB4 thought to result from high pulmonary capillary pressures. In both of these instances, the blood–gas barrier retains sieving function for large molecular weight proteins 6. However, in established HAPE, permeability to macromolecules is increased 8, and an inflammatory response of the lung to hypoxia has been suggested as an alternate mechanism 9. In addition, some authors have suggested that HAPE results from altered sodium and water handling by the susceptible lung 10.
Stress failure has been suggested to be important in the development of HAPE largely because of the relationship between high pulmonary vascular pressures and the development of HAPE. A previous history of HAPE is the single greatest predictor of the development of HAPE in future exposures and HAPE-susceptible individuals generally have augmented hypoxic pulmonary vasoconstriction and increased pulmonary vascular pressures when exposed to hypoxia 11–15 and exercise 16. In addition, drugs such as sidenafil, nifedipine, tadaphil and dexamethasone reduce pulmonary vascular pressures and reduce the severity of HAPE 17, 18 or prevent the development when administered prophylactically 19. Since the primary site of hypoxic pulmonary vasoconstriction is thought to be pre-capillary, hypoxic pulmonary vasoconstriction is hypothesised to be uneven 20, 21, subjecting capillaries in nonconstricted lung regions to higher pressures and structural injury. This uneven perfusion is supported by studies in animals 22 as well as imaging studies in HAPE-susceptible humans 23, 24. Also, in support of the initial leak in HAPE as non-inflammatory and related to increased hydrostatic pressure are studies in HAPE-susceptible subjects and control subjects with a history of repeated exposure to high altitude without symptoms 25. At 4,559 m, HAPE-susceptible subjects had greater pulmonary capillary pressures than controls and this was greater in individuals who were clinically ill with HAPE. Bronchoalveolar lavage fluid obtained shortly after ascent showed increased red blood cell and protein concentrations in HAPE-susceptible subjects compared to control subjects, with a greater increase in those HAPE-susceptible subjects that were clinically ill with HAPE. However, there were no elevations in inflammatory mediators or cells in any of these subjects indicating that the development of the leak precedes the development of inflammation in these subjects. All of this evidence, however convincing, is not direct proof of the presence of capillary stress failure in HAPE.
In a carefully controlled study published in this issue, Bai et al. 26, working with a rat model, link for the first time direct histological evidence of pulmonary capillary stress failure and the development of a HAPE-like illness. Although it has been previously shown that rats, rapidly decompressed to extremely low barometric pressures, developed evidence of stress failure 27 the link to HAPE had not been fully established. The strength of the work of Bai et al. 26, is the comprehensive and well controlled nature of the study design: animals who were subjected to physiologically relevant levels of hypobaric hypoxia (420 mmHg, altitude ∼4,700 m) developed an increase in lung wet-to-dry ratio, and bronchoalveolar lavage fluid total protein, albumin and red blood cell concentrations, indicating that these animals had increased lung water and bronchoalveolar lavage findings similar to human HAPE. These changes were greater in animals that were subjected to very strenuous exercise while hypoxic and were not seen in normoxic resting or normoxic exercising control animals. Post mortem histological evaluation of the lung showed that both groups of hypoxic animals had an increase in the thickness of the alveolar septum on light microscopy compared with the normoxic animals. Haemorrhagic alveolar oedema was present in the hypoxic exercising animals but not the other three groups, although a small number of red blood cells were found in both the resting hypoxic and exercising normoxic groups. On electron microscopy, gross changes were observed in the blood–gas barrier of the hypoxic exercising animals consisting of regions of disruption of the alveolar epithelium and capillary endothelium as classically described by West. Importantly, changes of this magnitude were not observed in any of the other groups of animals. In addition, the number of breaks observed across the all of the animal groups showed highly significant relationships with the red cell, and protein concentrations as well as the wet-to-dry ratio of the lung and the alveolar arterial difference providing a link between the severity of the injury to the blood gas barrier and the clinical manifestations of illness.
Although stress failure is linked to the development of florid pulmonary oedema at altitude, there is good evidence that during intense sea level exercise both humans 7 and animals develop stress failure of pulmonary capillaries and in some species, such as horses, this is a regular occurrence 28. However alveolar flooding after sea level exercise has been rarely reported in humans and is limited to situations where the exercise task has been truly extraordinary 29 or during water immersion 30. Therefore, stress failure is not in itself enough to incite pulmonary oedema, leaving many questions about HAPE unanswered. So what are the next steps in the pathogenesis of HAPE after the initial damage to the blood–gas barrier? It has been shown that the breaks in the pulmonary blood–gas barrier close very quickly after the pressure is reduced and, given the rapid improvements with descent, oxygen and pulmonary vasodilators, an ongoing elevation of pulmonary vascular pressures is clearly important in HAPE. In addition, a brisk inflammatory response likely accentuates an underlying leak, but this has not been completely elucidated. What are the roles of previous viral infection and altered alveolar fluid clearance in the genesis of HAPE? There are many facets of this interesting problem yet to be elucidated. It should be noted that the exercising rat model may be helpful, but in general rats have proven to be quite resistant to the development of HAPE, requiring either very severe hypoxaemia, endotoxin priming or, as in the study of Bai et al. 26, extremely high levels of sustained exercise.
Why should we care about understanding the mechanism of HAPE, which affects so few individuals and is easily preventable simply by limiting altitude exposure or by prophylaxis with dexamethasone or pulmonary vasodilators? HAPE research may offer insights into several types of pulmonary oedema occurring at low elevations such as neurogenic pulmonary oedema and reperfusion pulmonary oedema. In addition, understanding the relationships between lung mechanical stress injury and oedema may, if not provide insights into the mechanism of acute lung injury and acute respiratory distress syndrome, at least allow better selection of therapeutic strategies that minimize the risk of additional lung injury 31.
In an era of reductionist science where organ-level physiology is commonly viewed as lacking in mechanistic insights, research investigating the mechanisms of HAPE has largely been conducted in whole animal models and humans. From the early work of West and co-workers, first comprehensively identifying the vulnerability of the lung to mechanical stress failure and predicting the importance of stress failure in a variety of human illness 4, 32–34, to later work in human volunteers providing the first evidence for stress failure in HAPE 25, the work of Bai et al. 26, and that of a great many other contributors, highlights the importance of applying the understanding of normal physiological responses in humans and whole animal models to the study of disease. To quote the French physiologist Claude Bernard, “Effects vary with the conditions which bring them to pass, but laws do not vary. Physiological and pathological states are ruled by the same forces; they differ only because of the special conditions under which the vital laws manifest themselves” 35.
Statement of interest
None declared.
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