Hypoxia (medical)

Hypoxia
Other names: Anoxia, hypoxiation, oxygen desaturation, lack of oxygen, low blood oxygen, oxygen starvation
Cyanosis of the hand in an elderly person with low oxygen saturation
SpecialtyPulmonology, toxicology
SymptomsShortness of breath, confusion, headache, bluish skin[1]
TypesHypoxemia, ischemia[1][2]
CausesHypoxemia: Pneumonia, asthma, COPD, pulmonary edema, foreign body aspiration, opioid overdose, pulmonary embolism, congenital heart defects, high altitude, carbon monoxide toxicity, interstitial lung disease[1]
Ischemia: Arterial blood clot, vasospasm, peripheral artery disease[2]
Other: Anemia, cardiogenic shock, cyanide poisoning[1]
Diagnostic methodPulse oximetry[1]
TreatmentAirway management, oxygen therapy, improving lung function[1]
FrequencyCommon[1]

Hypoxia is a condition in which body tissues are deprived of adequate oxygen.[3] When onset is sudden, symptom may include shortness of breath and fast heart rate.[1] When moderate in severity, confusion and headache may occur, while in severe disease the skin may become bluish and the person may become unresponsive.[1] When more gradual in onset, the initial symptom is often shortness of breath with exercise.[1]

There are two main causes of hypoxia: low oxygen content in the blood (hypoxemia) and insufficient blood flow to tissue (ischemia).[1] Hypoxemia can occurs due to pneumonia, asthma, COPD, pulmonary edema, foreign body aspiration, opioid overdose, pulmonary embolism, congenital heart defects, high altitude, carbon monoxide toxicity, and interstitial lung disease.[1] Ischemia can occur due to an arterial blood clot, vasospasm, or peripheral artery disease.[2] Hypoxia may also occur due to anemia, cardiogenic shock, and cyanide poisoning.[1] Diagnosis is most commonly by pulse oximetry finding saturations of less than 90 to 95%.[1][4]

Management may involve airway management, increasing the amount of oxygen being breathed, and improving the uptake of oxygen by the lungs.[1] This may be achieved with measures that vary from the use of nasal cannula to endotracheal intubation.[1] Hypoxia is common.[1]

Signs and symptoms

Generalized

The symptoms of generalized hypoxia depend on its severity and acceleration of onset.

In the case of altitude sickness, where hypoxia develops gradually, the symptoms include fatigue, numbness / tingling of extremities, nausea, and cerebral anoxia.[5] These symptoms are often difficult to identify, but early detection of symptoms can be critical.[6]

In severe hypoxia, or hypoxia of very rapid onset, ataxia, confusion, disorientation, hallucinations, behavioral change, severe headaches, reduced level of consciousness, papilloedema, breathlessness,[5] pallor,[7] tachycardia, and pulmonary hypertension eventually leading to the late signs cyanosis, slow heart rate, cor pulmonale, and low blood pressure followed by heart failure eventually leading to shock and death.[8][9]

Because hemoglobin is a darker red when it is not bound to oxygen (deoxyhemoglobin), as opposed to the rich red color that it has when bound to oxygen (oxyhemoglobin), when seen through the skin it has an increased tendency to reflect blue light back to the eye.[10] In cases where the oxygen is displaced by another molecule, such as carbon monoxide, the skin may appear 'cherry red' instead of cyanotic.[11] Hypoxia can cause premature birth, and injure the liver, among other deleterious effects.

Localized

If tissue is not being perfused properly, it may feel cold and appear pale; if severe, hypoxia can result in cyanosis, a blue discoloration of the skin. If hypoxia is very severe, a tissue may eventually become gangrenous. Extreme pain may also be felt at or around the site.

Tissue hypoxia from low oxygen delivery may be due to low haemoglobin concentration (anaemic hypoxia), low cardiac output (stagnant hypoxia) or low haemoglobin saturation (hypoxic hypoxia).[12] The consequence of oxygen deprivation in tissues is a switch to anaerobic metabolism at the cellular level. As such, reduced systemic blood flow may result in increased serum lactate.[13] Serum lactate levels have been correlated with illness severity and mortality in critically ill adults and in ventilated neonates with respiratory distress.[13]

Cause

Oxygen passively diffuses in the lung alveoli according to a pressure gradient. Oxygen diffuses from the breathed air, mixed with water vapour, to arterial blood, where its partial pressure is around 100 mmHg (13.3 kPa).[14] In the blood, oxygen is bound to hemoglobin, a protein in red blood cells. The binding capacity of hemoglobin is influenced by the partial pressure of oxygen in the environment, as described in the oxygen–hemoglobin dissociation curve. A smaller amount of oxygen is transported in solution in the blood.

In peripheral tissues, oxygen again diffuses down a pressure gradient into cells and their mitochondria, where it is used to produce energy in conjunction with the breakdown of glucose, fats, and some amino acids.[15]

Hypoxia can result from a failure at any stage in the delivery of oxygen to cells. This can include decreased partial pressures of oxygen, problems with diffusion of oxygen in the lungs, insufficient available hemoglobin, problems with blood flow to the end tissue, and problems with breathing rhythm.

Experimentally, oxygen diffusion becomes rate limiting (and lethal) when arterial oxygen partial pressure falls to 60 mmHg (5.3 kPa) or below.

Almost all the oxygen in the blood is bound to hemoglobin, so interfering with this carrier molecule limits oxygen delivery to the periphery. Hemoglobin increases the oxygen-carrying capacity of blood by about 40-fold,[16] with the ability of hemoglobin to carry oxygen influenced by the partial pressure of oxygen in the environment, a relationship described in the oxygen–hemoglobin dissociation curve. When the ability of hemoglobin to carry oxygen is interfered with, a hypoxic state can result.[17]:997–99

Ischemia

Ischemia, meaning insufficient blood flow to a tissue, can also result in hypoxia. This is called 'ischemic hypoxia'. This can include an embolic event, a heart attack that decreases overall blood flow, or trauma to a tissue that results in damage. An example of insufficient blood flow causing local hypoxia is gangrene that occurs in diabetes.[18]

Diseases such as peripheral vascular disease can also result in local hypoxia. For this reason, symptoms are worse when a limb is used. Pain may also be felt as a result of increased hydrogen ions leading to a decrease in blood pH (acidity) created as a result of anaerobic metabolism.

Hypoxemic hypoxia

This refers specifically to hypoxic states where the arterial content of oxygen is insufficient.[19] This can be caused by alterations in respiratory drive, such as in respiratory alkalosis, physiological or pathological shunting of blood, diseases interfering in lung function resulting in a ventilation-perfusion mismatch, such as a pulmonary embolus, or alterations in the partial pressure of oxygen in the environment or lung alveoli, such as may occur at altitude or when diving.

Carbon monoxide poisoning

Carbon monoxide competes with oxygen for binding sites on hemoglobin molecules. As carbon monoxide binds with hemoglobin hundreds of times tighter than oxygen, it can prevent the carriage of oxygen.[20] Carbon monoxide poisoning can occur acutely, as with smoke intoxication, or over a period of time, as with cigarette smoking. Due to physiological processes, carbon monoxide is maintained at a resting level of 4–6 ppm. This is increased in urban areas (7–13 ppm) and in smokers (20–40 ppm).[21] A carbon monoxide level of 40 ppm is equivalent to a reduction in hemoglobin levels of 10 g/L.[21] The formula can be used to calculate the amount of carbon monoxide-bound hemoglobin. For example, at carbon monoxide level of 5 ppm, , or a loss of half a percent of their blood's hemoglobin.[21]

CO has a second toxic effect, namely removing the allosteric shift of the oxygen dissociation curve and shifting the foot of the curve to the left. In so doing, the hemoglobin is less likely to release its oxygens at the peripheral tissues.[16] Certain abnormal hemoglobin variants also have higher than normal affinity for oxygen, and so are also poor at delivering oxygen to the periphery.

Altitude

Atmospheric pressure reduces with altitude and with it, the amount of oxygen.[22] The reduction in the partial pressure of inspired oxygen at higher altitudes lowers the oxygen saturation of the blood, ultimately leading to hypoxia.[22] The clinical features of altitude sickness include: sleep problems, dizziness, headache and oedema.[22]

Hypoxic breathing gases

The breathing gas in underwater diving may contain an insufficient partial pressure of oxygen, particularly in malfunction of rebreathers. Such situations may lead to unconsciousness without symptoms since carbon dioxide levels are normal and the human body senses pure hypoxia poorly. Hypoxic breathing gases can be defined as mixtures with a lower oxygen fraction than air, though gases containing sufficient oxygen to reliably maintain consciousness at normal sea level atmospheric pressure may be described as normoxic even when slightly hypoxic. Hypoxic mixtures in this context are those which will not reliably maintain consciousness at sea level pressure. Gases with as little as 2% oxygen by volume in a helium diluent are used for deep diving operations. The ambient pressure at 190 msw is sufficient to provide a partial pressure of about 0.4 bar, which is suitable for saturation diving. As the divers are decompressed, the breathing gas must be oxygenated to maintain a breathable atmosphere.[23]

Inert gas asphyxiation may be deliberate with use of a suicide bag. Accidental death has occurred in cases where concentrations of nitrogen in controlled atmospheres, or methane in mines, has not been detected or appreciated.[24]

Other

Hemoglobin's function can also be lost by chemically oxidizing its iron atom to its ferric form. This form of inactive hemoglobin is called methemoglobin and can be made by ingesting sodium nitrite[25] as well as certain drugs and other chemicals.[26]

Anemia

Hemoglobin plays a substantial role in carrying oxygen throughout the body,[16] and when it is deficient, anemia can result, causing 'anaemic hypoxia' if tissue perfusion is decreased. Iron deficiency is the most common cause of anemia. As iron is used in the synthesis of hemoglobin, less hemoglobin will be synthesised when there is less iron, due to insufficient intake, or poor absorption.[17]:997–99

Anemia is typically a chronic process that is compensated over time by increased levels of red blood cells via upregulated erythropoetin. A chronic hypoxic state can result from a poorly compensated anaemia.[17]:997–99

Histotoxic hypoxia

Cyanide poisoning

Histotoxic hypoxia results when the quantity of oxygen reaching the cells is normal, but the cells are unable to use the oxygen effectively as a result of disabled oxidative phosphorylation enzymes. This may occur in cyanide poisoning.[27]

Pathophysiology

Acute

If oxygen delivery to cells is insufficient for the demand (hypoxia), electrons will be shifted to pyruvic acid in the process of lactic acid fermentation. This temporary measure (anaerobic metabolism) allows small amounts of energy to be released. Lactic acid build up (in tissues and blood) is a sign of inadequate mitochondrial oxygenation, which may be due to hypoxemia, poor blood flow (e.g., shock) or a combination of both.[28] If severe or prolonged it could lead to cell death. [29]

In humans, hypoxia is detected by the peripheral chemoreceptors in the carotid body and aortic body, with the carotid body chemoreceptors being the major mediators of reflex responses to hypoxia.[30] This response does not control ventilation rate at normal pO
2
, but below normal the activity of neurons innervating these receptors increases dramatically, so much so to override the signals from central chemoreceptors in the hypothalamus, increasing pO
2
despite a falling pCO
2

In most tissues of the body, the response to hypoxia is vasodilation. By widening the blood vessels, the tissue allows greater perfusion.

By contrast, in the lungs, the response to hypoxia is vasoconstriction. This is known as hypoxic pulmonary vasoconstriction, or "HPV".[31]

Chronic

When the pulmonary capillary pressure remains elevated chronically (for at least 2 weeks), the lungs become even more resistant to pulmonary edema because the lymph vessels expand greatly, increasing their capability of carrying fluid away from the interstitial spaces perhaps as much as 10-fold. Therefore, in patients with chronic mitral stenosis, pulmonary capillary pressures of 40 to 45 mm Hg have been measured without the development of lethal pulmonary edema.[Guytun and Hall physiology]

Hypoxia exists when there is a reduced amount of oxygen in the tissues of the body. Hypoxemia refers to a reduction in PO2 below the normal range, regardless of whether gas exchange is impaired in the lung, CaO2 is adequate, or tissue hypoxia exists. There are several potential physiologic mechanisms for hypoxemia, but in patients with COPD the predominant one is V/Q mismatching, with or without alveolar hypoventilation, as indicated by PaCO2. Hypoxemia caused by V/Q mismatching as seen in COPD is relatively easy to correct, so that only comparatively small amounts of supplemental oxygen (less than 3 L/min for the majority of patients) are required for LTOT. Although hypoxemia normally stimulates ventilation and produces dyspnea, these phenomena and the other symptoms and signs of hypoxia are sufficiently variable in patients with COPD as to be of limited value in patient assessment. Chronic alveolar hypoxia is the main factor leading to development of cor pulmonale—right ventricular hypertrophy with or without overt right ventricular failure—in people with COPD. Pulmonary hypertension negatively affects survival in COPD, to an extent that parallels the degree to which resting mean pulmonary artery pressure is elevated. Although the severity of airflow obstruction as measured by FEV1 is the best correlate with overall prognosis in patients with COPD, chronic hypoxemia increases mortality and morbidity for any severity of disease. Large-scale studies of LTOT in patients with COPD have demonstrated a dose–response relationship between daily hours of oxygen use and survival. There is reason to believe that continuous, 24-hours-per-day oxygen use in appropriately selected patients would produce a survival benefit even greater than that shown in the NOTT and MRC studies.[32]

Treatment

To counter the effects of high-altitude diseases, the body must return arterial pO
2
toward normal. Acclimatization, the means by which the body adapts to higher altitudes, only partially restores pO
2
to standard levels. Hyperventilation, the body's most common response to high-altitude conditions, increases alveolar pO
2
by raising the depth and rate of breathing. However, while pO
2
does improve with hyperventilation, it does not return to normal. Studies of miners and astronomers working at 3000 meters and above show improved alveolar pO
2
with full acclimatization, yet the pO
2
level remains equal to or even below the threshold for continuous oxygen therapy for patients with chronic obstructive pulmonary disease (COPD).[33] In addition, there are complications involved with acclimatization. Polycythemia, in which the body increases the number of red blood cells in circulation, thickens the blood, raising the danger that the heart can't pump it.

In high-altitude conditions, only oxygen enrichment can counteract the effects of hypoxia. By increasing the concentration of oxygen in the air, the effects of lower barometric pressure are countered and the level of arterial pO
2
is restored toward normal capacity. A small amount of supplemental oxygen reduces the equivalent altitude in climate-controlled rooms. At 4000 m, raising the oxygen concentration level by 5 percent via an oxygen concentrator and an existing ventilation system provides an altitude equivalent of 3000 m, which is much more tolerable for the increasing number of low-landers who work in high altitude.[34] In a study of astronomers working in Chile at 5050 m, oxygen concentrators increased the level of oxygen concentration by almost 30 percent (that is, from 21 percent to 27 percent). This resulted in increased worker productivity, less fatigue, and improved sleep.[33]

Oxygen concentrators are uniquely suited for this purpose. They require little maintenance and electricity, provide a constant source of oxygen, and eliminate the expensive, and often dangerous, task of transporting oxygen cylinders to remote areas. Offices and housing already have climate-controlled rooms, in which temperature and humidity are kept at a constant level.

A prescription renewal for home oxygen following hospitalization requires an assessment of the patient for ongoing hypoxemia.[35]

Research

The 2019 Nobel Prize in Physiology or Medicine was awarded to William G. Kaelin Jr., Peter J. Ratcliffe, and Gregg L. Semenza for their discovery of cellular mechanisms to sense and adapt to different oxygen concentrations, establishing a basis for how oxygen levels affect physiological function.[36][37]

See also

  • Asphyxia  Condition of severely deficient supply of oxygen to the body caused by abnormal breathing
  • Cerebral hypoxia  Oxygen shortage of the brain or cerebral anoxia, a reduced supply of oxygen to the brain
  • Erotic asphyxiation  Intentional restriction of oxygen to the brain for sexual arousal or autoerotic hypoxia, intentional restriction of oxygen to the brain for sexual arousal
  • Fink effect, or diffusion hypoxia, a factor that influences the partial pressure of oxygen within the pulmonary alveolus
  • G-LOC cerebral hypoxia induced by excessive g-forces
  • Histotoxic hypoxia, the inability of cells to take up or utilize oxygen from the bloodstream
  • Hyperoxia  Exposure of tissues to abnormally high concentrations of oxygen.
  • Hypoventilation training  Physical training method in which reduced breathing frequency are interspersed with periods with normal breathing
  • Hypoxemia  Abnormally low level of oxygen in the blood or hypoxemic hypoxia, a deficiency of oxygen in arterial blood
  • Hypoxia in fish  Response of fish to environmental hypoxia, responses of fish to hypoxia
  • Hypoxia-inducible factors
  • Hypoxic hypoxia, a result of insufficient oxygen available to the lungs
  • Hypoxic ventilatory response
  • Hypoxicator a device intended for hypoxia acclimatisation in a controlled manner
  • Intermittent hypoxic training
  • Intrauterine hypoxia, when a fetus is deprived of an adequate supply of oxygen
  • Latent hypoxia  Tissue oxygen concentration which is sufficient to support consciousness at depth, but not at surface pressure or deep water blackout, loss of consciousness on ascending from a deep freedive
  • Pseudohypoxia, increased cytosolic ratio of free NADH to NAD+ in cells
  • Rhinomanometry
  • Sleep apnea  Disorder involving pauses in breathing during sleep
  • Time of useful consciousness
  • Tumor hypoxia, the situation where tumor cells have been deprived of oxygen

References

  1. 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 Bhutta, BS; Alghoula, F; Berim, I (January 2020). "Anoxia". PMID 29493941. {{cite journal}}: Cite journal requires |journal= (help)
  2. 1 2 3 "Ischemia and Hypoxia". www.cvphysiology.com. Archived from the original on 27 November 2020. Retrieved 22 February 2021.
  3. "Definition of HYPOXIC". www.merriam-webster.com. Archived from the original on 9 July 2021. Retrieved 22 February 2021.
  4. "Oxygen Desaturation - Critical Care Medicine". Merck Manuals Professional Edition. Archived from the original on 22 January 2021. Retrieved 22 February 2021.
  5. 1 2 Robinson, Grace; Strading, John; West, Sophie (2009). Oxford Handbook of Respiratory Medicine. Oxford University Press. p. 880. ISBN 978-0199545162.
  6. Bergqvist, Pia (15 April 2015). "Preventing Hypoxia: What To Do Now". Flying. Archived from the original on 21 September 2017. Retrieved 22 April 2015.
  7. Illingworth, Robin; Graham, Colin; Hogg, Kerstin (2012). Oxford Handbook of Emergency Medicine. Oxford University Press. p. 768. ISBN 978-0199589562.
  8. Hillman, Ken; Bishop, Gillian (2004). Clinical Intensive Care and Acute Medicine. Cambridge University Press. p. 685. ISBN 978-1139449366.
  9. Longmore, J.; Longmore, Murray; Wilkinson, Ian; Rajagopalan, Supraj (2006). Mini Oxford Handbook of Clinical Medicine. Oxford University Press. p. 874. ISBN 978-0198570714.
  10. Ahrens, Thomas; Rutherford Basham, Kimberley (1993). Essentials of Oxygenation: Implication for Clinical Practice. Jones & Bartlett Learning. p. 194. ISBN 978-0867203325.
  11. Ramrakha, Punit; Moore, Kevin (2004). Oxford Handbook of Acute Medicine. Oxford University Press. p. 990. ISBN 978-0198520726.
  12. Lacroix, Jacques; Tucci, Marisa; Tinmouth, Alan; Gauvin, France; Karam, Oliver (2011). Pediatric Critical Care. Elsevier. pp. 1162–76. doi:10.1016/b978-0-323-07307-3.10082-5. ISBN 978-0323073073.
  13. 1 2 Kluckow, Martin; Seri, Istvan (2012). Hemodynamics and Cardiology: Neonatology Questions and Controversies. Elsevier. pp. 237–67. doi:10.1016/b978-1-4377-2763-0.00012-3. ISBN 978-1437727630.
  14. Kenneth Baillie; Alistair Simpson. "Altitude oxygen calculator". Apex (Altitude Physiology Expeditions). Archived from the original on 2017-06-11. Retrieved 2006-08-10. – Online interactive oxygen delivery calculator.
  15. Jae-Hwan, Lee; Eun-Kyeong, Shin; Dongoh, Lee; Eui-Bae, Jeung (April 2015). "SAT-532: Expression of Beta-Oxidation Related Genes Under Hypoxic Condition Induced Preeclamptic Model in Vitro and in Vivo". Endocrine Reviews. 36 (2). doi:10.1210/endo-meetings.2015.
  16. 1 2 3 Martin, Lawrence (1999). All you really need to know to interpret arterial blood gases (2nd ed.). Philadelphia: Lippincott Williams & Wilkins. ISBN 978-0-683-30604-0.
  17. 1 2 3 Nicki R. Colledge; Brian R. Walker; Stuart H. Ralston, eds. (2010). Davidson's principles and practice of medicine. illustrated by Robert Britton (21st ed.). Edinburgh: Churchill Livingstone/Elsevier. ISBN 978-0-7020-3085-7.
  18. Marvin E. Levin; Lawrence W. O'Neal; John H. Bowker (1993). The Diabetic foot. Mosby Year Book. ISBN 978-0-8016-6878-4. Archived from the original on 2020-05-08. Retrieved 2019-03-20.
  19. West, John B. (2008). Respiratory Physiology: The Essentials (8th ed.). La Jolla: Wolters Kluwer Lippincott Williams & Wilkins. pp. 88–89.
  20. Douglas CG, Haldane JS, Haldane JB (Jun 12, 1912). "The laws of combination of hemoglobin with carbon monoxide and oxygen". The Journal of Physiology. 44 (4): 275–304. doi:10.1113/jphysiol.1912.sp001517. PMC 1512793. PMID 16993128.
  21. 1 2 3 Wald, NJ; Idle, M; Boreham, J; Bailey, A (May 1981). "Carbon monoxide in breath in relation to smoking and carboxyhaemoglobin levels". Thorax. 36 (5): 366–69. doi:10.1136/thx.36.5.366. PMC 471511. PMID 7314006.
  22. 1 2 3 Netzer, Nikolaus; Strohl, Kingman; Faulhaber, Martin; Gatterer, Hannes; Burtscher, Martin (1 July 2013). "Hypoxia‐Related Altitude Illnesses". Journal of Travel Medicine. 20 (4): 247–55. doi:10.1111/jtm.12017. PMID 23809076. Archived from the original on 19 July 2018. Retrieved 18 July 2018.
  23. Staff, US Navy (2006). "15". US Navy Diving Manual, 6th revision. United States: US Naval Sea Systems Command. Archived from the original on 2 May 2008. Retrieved 15 June 2008.
  24. Milroy, Christopher (Autumn 2018). "Deaths from Environmental Hypoxia and Raised Carbon Dioxide". Academic Forensic Pathology. 8 (1): 2–7. doi:10.23907/2018.001. PMC 6474450. PMID 31240022.
  25. Roueché, Berton (1953) Eleven blue men, and other narratives of medical detection. Boston: Little, Brown.
  26. "Methemoglobinemia and Medications A to Z". British Columbia Drug and Poison Information Centre. Archived from the original on 2020-01-31. Retrieved 2020-01-31.
  27. Pittman, RN (2011). "Regulation of Tissue Oxygenation". Morgan & Claypool Life Sciences. p. Chapter 7. Archived from the original on 2021-01-25. Retrieved 2017-08-31.
  28. Hobler, K.E.; L.C. Carey (1973). "Effect of acute progressive hypoxemia on cardiac output and plasma excess lactate". Ann Surg. 177 (2): 199–202. doi:10.1097/00000658-197302000-00013. PMC 1355564. PMID 4572785.
  29. Fulda, Simone; Gorman, Adrienne M.; Hori, Osamu; Samali, Afshin (2010). "Cellular Stress Responses: Cell Survival and Cell Death". International Journal of Cell Biology. 2010: 214074. doi:10.1155/2010/214074. ISSN 1687-8876. PMC 2825543. PMID 20182529.
  30. Arieff, Allen I. (2013). Hypoxia, Metabolic Acidosis, and the Circulation. Springer. pp. 4–5. ISBN 978-1461475422.
  31. Michiels, Carine (2004). "Physiological and Pathological Responses to Hypoxia". The American Journal of Pathology. 164 (6): 1875–82. doi:10.1016/S0002-9440(10)63747-9. PMC 1615763. PMID 15161623.
  32. Pierson, D. J. (2000). "Pathophysiology and clinical effects of chronic hypoxia". Respir Care. 45 (1): 39–51, discussion 51–53. PMID 10771781.
  33. 1 2 West, John B.; American College Of Physicians; American Physiological Society (2004). "The Physiologic Basis of High-Altitude Diseases". Annals of Internal Medicine. 141 (10): 789–800. doi:10.7326/0003-4819-141-10-200411160-00010. PMID 15545679.
  34. West, John B. (1995). "Oxygen Enrichment of Room Air to Relieve the Hypoxia of High Altitude". Respiration Physiology. 99 (2): 225–32. doi:10.1016/0034-5687(94)00094-G. PMID 7777705.
  35. American College of Chest Physicians; American Thoracic Society (September 2013), "Five Things Physicians and Patients Should Question", Choosing Wisely: an initiative of the ABIM Foundation, American College of Chest Physicians and American Thoracic Society, archived from the original on 3 November 2013, retrieved 6 January 2013
  36. "The Nobel Prize in Physiology or Medicine 2019". NobelPrize.org. Archived from the original on 2020-05-23. Retrieved 2019-10-28.
  37. "Hypoxia | GeneTex". www.genetex.com. Archived from the original on 2019-07-18. Retrieved 2019-10-28.
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