Hypoxia Clinical Trial
Official title:
High Altitude Medical Research Expedition Himlung 2013 - an Observational Cohort Study of Human Adaption to Hypobaric Hypoxia
The aim of the project "High Altitude Medical Research Expedition Himlung 2013"
(HiReach2013) is to comprehensively investigate the cerebral, cardiovascular and pulmonary
adaptation and the reactions of the human immune system during an ascent to extreme
altitudes of over 7000 m. A total of 44 healthy and trained volunteers will be included in
the study after written informed consent has been obtained.Baseline sea level clinical
examination will be performed in Bern, Switzerland (BE1) at 550 m 8 to 4 weeks before
departure. High altitude research facilities will be available at the altitudes of 5000m,
6100m and 6900m. Post-expedition examination will be performed within 2 to 6 weeks after the
end of the expedition in Bern. In the context of 3 sub-projects specific measurements and
examinations are performed.
These include: cMRI before and after the climb and neurovascular doppler examination during
the climb; blood sampling for coagulation studies, cardiac and thoracic ultrasound, stress
tests for assessment of cardiovascular performance.
Background
Altitude related medical problems are gaining more importance and attention as an ever
increasing number of people travel to higher altitudes for work or pleasure. Resort towns in
Europe and the Western United States at elevations in the 2000 m to 3000 m range attract
millions of visitors annually. Many more visit cities in South America and Asia situated
above 3000 m. In addition, tens of thousands of travelers, trekkers, and skiers worldwide
ascend to elevations in the range of 3000 to 5500 m. An ever-increasing number of
recreational climbers attempt ascents of summits of very high (3500 m to 5500 m) or extreme
(>5500 m) altitudes. The Nepalese Ministry of Tourism and Civil Aviation and the Nepal
Mountaineering Association reported having issued permits to 6032 climbers for peaks higher
than 6000 m in the year 2010 alone. When considering that the number of people residing at
high altitude is bound to increase, it is of importance to further deepen our understanding
of the physiologic changes and dangers associated with exposure to high altitude. Oxygen
homeostasis is essential for survival of healthy humans at high altitudes. Various
physiological changes involving different organ systems occur during exposition and
acclimatization to hypobaric hypoxia in the context of a high altitude sojourn. These
include marked adaptations of pulmonary and systemic vascular function, changes in cerebral
perfusion and metabolism, physiologic and metabolic adaptations of the immune system and
innate defense mechanisms against infection. These changes are a consequence of tissue
hypoxia per se or can be mediated by hypoxia induced activation of sympathoadrenal pathways.
An example of important research activities in recent years is the discovery of
hypoxia-inducible factor 1 alpha (HIF1α) and its role in oxygen homoeostasis by regulation
of multiple gene loci. Additionally, as a result of hypoxia induced increase in
oxidative/reductive stress, enhanced generation of reactive oxygen (ROS) and nitrogen
species (RNS), altered activity of antioxidant systems, and related oxidative damage to
lipids, proteins, and DNA can occur as well as injury at the cellular, sub-cellular and
molecular levels. These short-lived intermediates include among others superoxide anion
(O2), hydrogen peroxide (H2O2), and hypochloride (HOCI. In addition, hydroxyl radicals (OH),
hydroxide ions (OH) and superoxide radicals (O2-) are highly reactive members of the ROS
family that accumulate under certain physiological and pathophysiological conditions. As a
consequence, prolonged hypobaric hypoxia leads to systemic oxidative stress similar to
severe inflammation.
Tissue hypoxia and increased oxidative stress as well as adaptive or reactive changes in
sympathoadrenal and neuroendocrine processes also occur in various disease states. Hypoxia
per se plays an important role in the pathogenesis of major causes of mortality, including
cancer, cerebral and myocardial ischemia, and chronic heart and lung disease. Global
hypoxemia is a common problem in critically ill patients: In patients with pulmonary failure
profound hypoxia can occur due to ventilation/perfusion mismatch or impaired diffusion
capacity across the alveolo-capillary membrane despite best medical support including
mechanical ventilation. Oxygen delivery to tissues might also be impaired due to low cardiac
output or reduced oxygen carrying capacity in anemia. Microcirculatory dysfunction -
occurring in the context of severe sepsis - can lead to local hypoxia on a cellular level
even in patients with normal or increased arterial oxygen content and oxygen delivery.
In critically ill patients cellular hypoxia induces oxidative stress which can deplete
cellular antioxidative capacities and lead to impaired ability to use available oxygen.
Depleted levels of reduced glutathione, an important intra-mitochondrial antioxidant, in
combination with increased generation of ROS and RNS seem to inhibit oxidative
phosphorylation and ATP generation. There is increasing interest in ROS-intermediates and
their role in the progression and modulation of vascular dysfunction and remodelling seen in
different chronic disease entities, such as diabetes mellitus, chronic heart failure or
chronic obstructive pulmonary disease (COPD) and development of pulmonary hypertension
(PHT). The mechanisms of ROS-generation are not fully understood. ROS are produced in
leukocytes, but the generation of ROS might also occur through disruption of the electron
transport chain in mitochondria. The resulting mitochondrial dysfunction has been described
as an additional factor causing pulmonary vasoconstriction and remodelling in PHT. In
hypoxic patients with respiratory failure an increase of pulmonary vascular pressure
frequently occurs (WHO Class III - pulmonary hypertension) which may worsen hypoxemia by
impairing lung perfusion. If this increase is caused by a direct vasoconstrictive effect of
hypoxia on the pulmonary endothelial cells or by an increase in ROS is still not fully
understood.
Generally, the mechanisms leading to adaptation to prolonged hypoxic conditions in healthy
humans and in critically ill patients are not well understood. In the context of critical
illness these mechanisms are difficult to explore due to the heterogeneity of patients and
precipitating illnesses. Furthermore, effects of hypoxia and concurring disease related
processes are difficult or impossible to distinguish. Animal models of critical illness
might have substantial limitations and often do not represent the human patient. It has been
suggested that the physiological and pathophysiological responses to hypobaric hypoxia may
be similar to responses seen in critical illness. In the context of a high altitude
expedition human subjects can safely be submitted to prolonged hypoxia and oxidative stress
and the resulting cerebral, cardiovascular and pulmonary adaptation and changes in
mitochondrial function, inflammatory cascade, and coagulatory activity can be explored in a
controlled fashion. The study of human responses to hypoxia occurring in a hypobaric
environment in healthy volunteers ascending to high altitudes may therefore serve as a model
of isolated hypoxia and might help to improve our understanding of the effects in critically
ill patients.
Objective
The aim of the project "High Altitude Medical Research Expedition Himlung 2013"
(HiReach2013) is to comprehensively investigate the cerebral, cardiovascular and pulmonary
adaptation and the reactions of the human coagulation system during an ascent to extreme
altitudes of over 7000 m.
Methods
Cardiopulmonary exercise testing will be done using a testing system on a bicycle using a
roller trainer for standardization and regulation of the work load. Static and dynamic lung
volumes will be assessed at each study site. The measurements will include the assessment
DLCO using a commercially available spirometer. Transthoracic Doppler echocardiography will
be performed for assessment of systolic/diastolic cardiac function and pulmonary artery
pressures. Lung ultrasound will be applied in each subject at each study site to quantify
extravascular lung water by ultrasound lung comets. Microparticle measurements will be
performed using an Annexin V based ELISA. Cerebral blood flow velocity will be measured from
a middle cerebral artery using transcranial Doppler. Structural cerebral changes and
cerebral volume will be assessed with MRI of the brain. At each study site extensive
coagulation studies will be performed.
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