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OXYGEN THERAPY

   Dr. Vinod K. Ravaliya
     Resident –I year
          KMPIP
Oxygen is in the air we breathe and is
necessary to live. The three basic nutrients without
which planet earth could not exist as a home for
living things are OXYGEN, LIGHT and WATER.
 Oxygen may be classified as an element, a gas,
  and a drug.

                    Definition
 Oxygen therapy is the administration of oxygen at
  concentrations greater than that in room air to treat or
  prevent hypoxemia (not enough oxygen in the blood)
Purpose
 The body is constantly taking in O2   & releasing CO2.
  If this process is inadequate, oxygen levels in the
  blood decrease, and the patient may need
  supplemental oxygen. Oxygen therapy is a key
  treatment in respiratory care.
 The purpose is to increase oxygen saturation in
  tissues where the saturation levels are too low due to
  illness or injury.
Oxyhemoglobin Dissociation Curve
 Definition : A relationship between the amount of
  oxygen dissolved in the blood and the amount
  attached to the hemoglobin. This is called the
  normal Oxyhemoglobin dissociation curve.
 Oxygen can be measured in two forms:
      - partial atmospheric pressure of oxygen
             (PaO2)
      - oxygen saturation (SaO2)
      - calculated estimate of oxygen saturation
             (SpO2): an indirect SaO2
Normal Oxyhemoglobin Dissociation Curve




97% saturation = 97 PaO2 (normal)
90% saturation = 60 PaO2 (danger)
80% saturation = 45 PaO2 (severe hypoxia)
Reference       Arterial blood   Venous blood
ranges

pH              7.35 – 7.45      7.35 – 7.43
pCO2            35 – 45 mmHg     38 – 50 mmHg
pO2             80 – 100 mmHg    30 – 50 mmHg
HCO3-           22 - 26 mM       23 – 27mM


O2 saturation   95 – 100 %       60 – 85 %
SHIFT TO LEFT
                            • Increase in pH
                            • Decrease in CO2
                            • Decrease in 2.3-DPG
                            • Decrease in temperature




SHIFT TO RIGHT
• Decrease in pH
• Increase in CO2
• Increase in 2,3-DPG
• Increase in temperature
Markers of O2 monitoring
PiO2 = (760 – 47) x 0.21 = 150 mmHg
FiO2 = 0.21
PAO2 = 100 mmHg
PaO2 = 90 mmHg
SaO2 = O2 saturation derived from
        arterialized cap. Blood.
SpO2 = O2 saturation by pulse. ox
Oxygen Flux and Requirements
     The supply of oxygen is dependent upon the
 hemoglobin (Hb), O2 saturation % (SaO2) and cardiac
 output (Q).
     "Oxygen flux" denotes the total amount of oxygen
 delivered to the body per minute and is given by the
 equation:
Oxygen flux = 1.34 x Hb in g/dL x (SaO2/100) x (Q in
 mL/min)/100 = 1000 mL/min
Assessment of need
 Need is determined by measurement of inadequate
  oxygen tensions and/or saturations, by invasive or
  noninvasive methods, and/or the presence of
  clinical indicators as previously described.
              • Arterial blood gases
              • Pulse oximetry
              • Clinical presentation
How to assess oxygenation ?
 Arterial blood gases
 Pulse oximetry



                  Errors in pulse oximetry
   Artificial fingernails •Nail Polish
   Dark pigmentation         •Pulsatile venous system
   Electrical                •Radiated light
   Intravenous dyes          •Edema
   Movement
Indications of O2 therapy
1. Documented hypoxemia
   In adults, children, and infants older than 28 days,
       arterial oxygen tension (PaO2) of < 60 mmHg
       or arterial oxygen saturation (SaO2) of < 90%
       in subjects breathing room air or with PaO2
       and/or SaO2 below desirable range for specific
       clinical situation
   In neonates, PaO2 < 50 mmHg and/or SaO2 <
       88% or capillary oxygen tension (PcO2) < 40
       mmHg
2.      An acute care situation in which hypoxemia is
               suspected
               Substantiation of hypoxemia is required
      within an appropriate period of time following
      initiation of therapy
3.      Severe trauma
4.      Acute myocardial infarction
5.      Short-term therapy (e.g., post-anesthesia
   recovery)
6.      Increased metabolic demands, i.e. burns,
   multiple injuries, and severe infections.
 Goal directed approach
    - post operative (thoracic/abdominal
    surgery)
    - post extubation
    - conscious state/coughing
    - redistribution of fluid
    - positioning
Three clinical goals of O2 therapy

    1. Treat hypoxemia

    2. Decrease work of breathing (WOB)

    3. Decrease myocardial Work
FACTORS THAT DETERMINE WHICH SYSTEM
                    TO USE
1. Patient comfort / acceptance by the Pt
2. The level of FiO2 that is needed
3. The requirement that the FiO2 be controlled
   within a certain range
4. The level of humidification and /or
   nebulization
5. Minimal resistance to breathing
6. Efficient & economical use of oxygen
O2 delivery methods

 Low flow oxygen delivery system
     ( variable performance )

 High flow oxygen delivery system
     ( fixed performance )
Low flow O2 delivery system
Fio2 depends on O2 flow, patient factors and
device factors
     Nasal cannula
     Simple face mask
     Partial rebreathing mask
     Non - rebreathing mask
Nasal cannula
 Simple plastic tubing + prongs
 Flow from 1-6 LPM of O2
 Fio2   ranges from 24-44% of O2
                  1 - 24%
                  2 - 28%
                  3 - 32%
                  4 - 36%
                  5 - 40%
                  6 - 44%
 Correct placement
 No nasal obstruction


  Advantages                    Disadvantages
 Inexpensive                   Pressure sores
 well tolerated, comfortable   Crusting of secr.
 easy to eat, drink            Drying of mucosa
 used in pt with COPD          Epistaxis
 used with humidity
Low flow O2 delivery system
Fio2 depends on O2 flow, patient factors and
device factors
     Nasal cannula
     Simple face mask
     Partial rebreathing mask
     Non - rebreathing mask
Simple face mask
     The placing of mask over the patient’s face
increases the size of the oxygen reservoir beyond the
limits of the anatomic reservoir ;therefore a higher
FiO2 can be delivered.

       The oxygen flow
must be run at a sufficient
rate, usually 5 lpm or
more to prevent
rebreathing of exhaled
gases.
 Advantages: simple, lightweight, FiO2 upto 0.60,
  can be used with humidity




 Disadvantages: need to remove when speak, eat,
  drink, vomiting, expectoration of secretions, drying /
  irritation of eyes, uncomfortable when facial burns /
  trauma application problem when RT in situ
Low flow O2 delivery system
Fio2 depends on O2 flow, patient factors and
device factors
     Nasal cannula
     Simple face mask
     Partial rebreathing mask
     Non - rebreathing mask
Partial rebreathing bag
 Advantages: FiO2 delivered >0.60 is delivered
  in mod. to severe hypoxia, exhaled oxygen
  from anatomic dead space is conserved.

 Disadvantages: insufficient flow rate may lead to
  rebreathing of CO2,claustrophobia;drying and
  irritation of eyes
Low flow O2 delivery system
Fio2 depends on O2 flow, patient factors and
device factors
     Nasal cannula
     Simple face mask
     Partial rebreathing mask
     Non - rebreathing mask
 Non-rebreathing bag
High flow O2 delivery system
     Venturi mask
     Face tent
     Aerosol mask
     Tracheostomy collar
     T-piece
VENTURI VALVE
Venturi valve
Color         FiO2        O2 Flow

Blue          24%        2 L/min
White         28%        4 L/min
Orange        31%        6 L/min
Yellow        35%        8 L/min
 Red          40%        10 L/min
Green         60%        15 L/min
Venturi mask
Face tent   Tracheostomy collar
Pediatric oxygen delivery system

 Oxygen hood
Oxygen hood
Oxygen tent
Long-term oxygen therapy
   Long-term oxygen therapy (LTOT) improves survival,
    exercise, sleep and cognitive performance.
   Reversal of hypoxemia supersedes concerns about
    carbon dioxide (CO2) retention.
   Arterial blood gas (ABG) is the preferred measure and
    includes acid-base information.
   Oxygen sources include gas, liquid and concentrator.
   Oxygen delivery methods include nasal continuous flow,
    pulse demand, reservoir cannulae and transtracheal
    catheter.
 Physiological indications for oxygen include an
  arterial oxygen tension (Pa,O2) <7.3 kPa (55 mmHg).
  The therapeutic goal is to maintain Sa,O2 >90%
  during rest, sleep and exertion.
 Active patients require portable oxygen.

 If oxygen was prescribed during an exacerbation,
  recheck ABGs after 30–90 days.
 Withdrawal of oxygen because of improved Pa,O2 in
  patients with a documented need for oxygen may be
  detrimental.
 Patient education improves compliance
In-patient oxygen therapy-COPD
   The goal is to prevent tissue hypoxia by maintaining
    arterial oxygen saturation (Sa,O2) at >90%.

   Main delivery devices include nasal cannula and Venturi
    mask.

   Alternative delivery devices include non-rebreathing
    mask, reservoir cannula, nasal cannula or transtracheal
    catheter.

   Arterial blood gases should be monitored for arterial
    oxygen tension (Pa,O2), arterial carbon dioxide tension
    (Pa,CO2) and pH.
 Arterial oxygen saturation as measured by pulse
  oximetry (Sp,O2) should be monitored for trending
  and adjusting oxygen settings.
 Prevention of tissue hypoxia supercedes CO2
  retention concerns.
 If CO2 retention occurs, monitor for acidaemia.

 If acidaemia occurs, consider mechanical
  ventilation.
Monitoring oxygen therapy
     Oxygen therapy should be given continuously and
should not be stopped abruptly until the patient has
recovered, since sudden discontinuation can wash-out
small body stores of oxygen resulting in fall of alveolar
oxygen tension. The dose of oxygen should be calculated
carefully. Partial pressure of oxygen can be measured in
the arterial blood. Complete saturation of hemoglobin in
arterial blood should not be attempted. Arterial PO2 of 60
mmHg can provide 90% saturation of arterial blood, but if
acidosis is present, PaO2 more than 80 mmHg is required.
In a patient with respiratory failure, anaemia should be
corrected for proper oxygen transport to the tissue.
A small increment in arterial oxygen tension results
in a significant rise in the saturation of hemoglobin.
Under normal situations, no additional benefit is
secured by raising PaO2 level to greater than 60 to 80
mmHg. An increase of 1% oxygen concentration
elevates oxygen tension by 7 mmHg. It is necessary to
maintain normal hemoglobin level in the presence of
respiratory disease as proper oxygen transport to the
tissues is to be maintained. Measurement of arterial
blood gases repeatedly is difficult so a simple and non-
invasive technique like pulse oximeter may be used to
assess oxygen therapy.
When to stop oxygen therapy
    Weaning should be considered when the patient
becomes comfortable, his underlying disease is
stabilized, BP, pulse rate, respiratory rate, skin
color, and oxymetry are within normal range.
    Weaning can be gradually attempted by
discontinuing oxygen or lowering its concentration
for a fixed period for e.g., 30 min. and reevaluating
the clinical parameters and SpO2 periodically.
    Patients with chronic respiratory disease may
require oxygen at lower concentrations for
prolonged periods.
Impact on the patient
 Fear death is likely to occur sooner
 Become less active
 Experience a sense of loss of freedom
 May become more socially isolated
Hazards & complications of oxygen
            therapy
      Oxygen-induced hypoventilation
      Oxygen toxicity/O2 narcosis
      Absorption atelectasis
      Retinopathy
      Drying of mucous membranes
      Infection
      Fire hazards
Oxygen is one of the most important drugs you
will ever use, but it is poorly prescribed by medical
staff. In 2000, a Nicola Cooper and colleague did
survey of treatment with oxygen. The first looked at
prescriptions of oxygen in postoperative patients in a
large district hospital. They found that there were
many ways used to prescribe oxygen and that the
prescriptions were rarely followed.
Oxygen dissociation curve
Shift to the left in O2 curve
                                             { O2 affinity }

    1. Causes: pH,         CO2, 2-3 DPG,     Temp.

    2. Results: O2 sat. for any pao2 but resulting
       in less gradient to move O2 to tissue. (Carries more
       O2 but more difficult to release it at tissue level)

    3.    Examples: stored blood loses 2-3 dpg a shift to
         the left results from this. Hyperventilation,
          Hypothermia.
Shift to the right in O2 curve

                                        { O2 affinity }
      1. Causes:     pH , CO2 , 2-3 DPG,       Temp.

      2. Results: O2 sat for any PaO2 but resulting
          in more gradient to move o2 into the tissues.

      3. Examples: hypoventilation, fever, metabolic
                   acidosis.
Transtracheal oxygen

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Oxygen therapy by Dr.Vinod Ravaliya

  • 1. OXYGEN THERAPY Dr. Vinod K. Ravaliya Resident –I year KMPIP
  • 2. Oxygen is in the air we breathe and is necessary to live. The three basic nutrients without which planet earth could not exist as a home for living things are OXYGEN, LIGHT and WATER.
  • 3.  Oxygen may be classified as an element, a gas, and a drug. Definition  Oxygen therapy is the administration of oxygen at concentrations greater than that in room air to treat or prevent hypoxemia (not enough oxygen in the blood)
  • 4. Purpose  The body is constantly taking in O2 & releasing CO2. If this process is inadequate, oxygen levels in the blood decrease, and the patient may need supplemental oxygen. Oxygen therapy is a key treatment in respiratory care.  The purpose is to increase oxygen saturation in tissues where the saturation levels are too low due to illness or injury.
  • 5. Oxyhemoglobin Dissociation Curve  Definition : A relationship between the amount of oxygen dissolved in the blood and the amount attached to the hemoglobin. This is called the normal Oxyhemoglobin dissociation curve.  Oxygen can be measured in two forms: - partial atmospheric pressure of oxygen (PaO2) - oxygen saturation (SaO2) - calculated estimate of oxygen saturation (SpO2): an indirect SaO2
  • 6. Normal Oxyhemoglobin Dissociation Curve 97% saturation = 97 PaO2 (normal) 90% saturation = 60 PaO2 (danger) 80% saturation = 45 PaO2 (severe hypoxia)
  • 7. Reference Arterial blood Venous blood ranges pH 7.35 – 7.45 7.35 – 7.43 pCO2 35 – 45 mmHg 38 – 50 mmHg pO2 80 – 100 mmHg 30 – 50 mmHg HCO3- 22 - 26 mM 23 – 27mM O2 saturation 95 – 100 % 60 – 85 %
  • 8. SHIFT TO LEFT • Increase in pH • Decrease in CO2 • Decrease in 2.3-DPG • Decrease in temperature SHIFT TO RIGHT • Decrease in pH • Increase in CO2 • Increase in 2,3-DPG • Increase in temperature
  • 9. Markers of O2 monitoring PiO2 = (760 – 47) x 0.21 = 150 mmHg FiO2 = 0.21 PAO2 = 100 mmHg PaO2 = 90 mmHg SaO2 = O2 saturation derived from arterialized cap. Blood. SpO2 = O2 saturation by pulse. ox
  • 10. Oxygen Flux and Requirements The supply of oxygen is dependent upon the hemoglobin (Hb), O2 saturation % (SaO2) and cardiac output (Q). "Oxygen flux" denotes the total amount of oxygen delivered to the body per minute and is given by the equation: Oxygen flux = 1.34 x Hb in g/dL x (SaO2/100) x (Q in mL/min)/100 = 1000 mL/min
  • 11. Assessment of need  Need is determined by measurement of inadequate oxygen tensions and/or saturations, by invasive or noninvasive methods, and/or the presence of clinical indicators as previously described. • Arterial blood gases • Pulse oximetry • Clinical presentation
  • 12. How to assess oxygenation ?  Arterial blood gases  Pulse oximetry Errors in pulse oximetry  Artificial fingernails •Nail Polish  Dark pigmentation •Pulsatile venous system  Electrical •Radiated light  Intravenous dyes •Edema  Movement
  • 13. Indications of O2 therapy 1. Documented hypoxemia In adults, children, and infants older than 28 days, arterial oxygen tension (PaO2) of < 60 mmHg or arterial oxygen saturation (SaO2) of < 90% in subjects breathing room air or with PaO2 and/or SaO2 below desirable range for specific clinical situation In neonates, PaO2 < 50 mmHg and/or SaO2 < 88% or capillary oxygen tension (PcO2) < 40 mmHg
  • 14. 2. An acute care situation in which hypoxemia is suspected Substantiation of hypoxemia is required within an appropriate period of time following initiation of therapy 3. Severe trauma 4. Acute myocardial infarction 5. Short-term therapy (e.g., post-anesthesia recovery) 6. Increased metabolic demands, i.e. burns, multiple injuries, and severe infections.
  • 15.  Goal directed approach - post operative (thoracic/abdominal surgery) - post extubation - conscious state/coughing - redistribution of fluid - positioning
  • 16. Three clinical goals of O2 therapy 1. Treat hypoxemia 2. Decrease work of breathing (WOB) 3. Decrease myocardial Work
  • 17. FACTORS THAT DETERMINE WHICH SYSTEM TO USE 1. Patient comfort / acceptance by the Pt 2. The level of FiO2 that is needed 3. The requirement that the FiO2 be controlled within a certain range 4. The level of humidification and /or nebulization 5. Minimal resistance to breathing 6. Efficient & economical use of oxygen
  • 18. O2 delivery methods  Low flow oxygen delivery system ( variable performance )  High flow oxygen delivery system ( fixed performance )
  • 19. Low flow O2 delivery system Fio2 depends on O2 flow, patient factors and device factors  Nasal cannula  Simple face mask  Partial rebreathing mask  Non - rebreathing mask
  • 20. Nasal cannula  Simple plastic tubing + prongs  Flow from 1-6 LPM of O2  Fio2 ranges from 24-44% of O2 1 - 24% 2 - 28% 3 - 32% 4 - 36% 5 - 40% 6 - 44%
  • 21.  Correct placement  No nasal obstruction Advantages Disadvantages  Inexpensive Pressure sores  well tolerated, comfortable Crusting of secr.  easy to eat, drink Drying of mucosa  used in pt with COPD Epistaxis  used with humidity
  • 22. Low flow O2 delivery system Fio2 depends on O2 flow, patient factors and device factors  Nasal cannula  Simple face mask  Partial rebreathing mask  Non - rebreathing mask
  • 23. Simple face mask The placing of mask over the patient’s face increases the size of the oxygen reservoir beyond the limits of the anatomic reservoir ;therefore a higher FiO2 can be delivered. The oxygen flow must be run at a sufficient rate, usually 5 lpm or more to prevent rebreathing of exhaled gases.
  • 24.  Advantages: simple, lightweight, FiO2 upto 0.60, can be used with humidity  Disadvantages: need to remove when speak, eat, drink, vomiting, expectoration of secretions, drying / irritation of eyes, uncomfortable when facial burns / trauma application problem when RT in situ
  • 25. Low flow O2 delivery system Fio2 depends on O2 flow, patient factors and device factors  Nasal cannula  Simple face mask  Partial rebreathing mask  Non - rebreathing mask
  • 26. Partial rebreathing bag  Advantages: FiO2 delivered >0.60 is delivered in mod. to severe hypoxia, exhaled oxygen from anatomic dead space is conserved.  Disadvantages: insufficient flow rate may lead to rebreathing of CO2,claustrophobia;drying and irritation of eyes
  • 27. Low flow O2 delivery system Fio2 depends on O2 flow, patient factors and device factors  Nasal cannula  Simple face mask  Partial rebreathing mask  Non - rebreathing mask
  • 29. High flow O2 delivery system  Venturi mask  Face tent  Aerosol mask  Tracheostomy collar  T-piece
  • 31. Venturi valve Color FiO2 O2 Flow Blue 24% 2 L/min White 28% 4 L/min Orange 31% 6 L/min Yellow 35% 8 L/min Red 40% 10 L/min Green 60% 15 L/min
  • 33. Face tent Tracheostomy collar
  • 34. Pediatric oxygen delivery system  Oxygen hood
  • 38. Long-term oxygen therapy (LTOT) improves survival, exercise, sleep and cognitive performance.  Reversal of hypoxemia supersedes concerns about carbon dioxide (CO2) retention.  Arterial blood gas (ABG) is the preferred measure and includes acid-base information.  Oxygen sources include gas, liquid and concentrator.  Oxygen delivery methods include nasal continuous flow, pulse demand, reservoir cannulae and transtracheal catheter.
  • 39.  Physiological indications for oxygen include an arterial oxygen tension (Pa,O2) <7.3 kPa (55 mmHg). The therapeutic goal is to maintain Sa,O2 >90% during rest, sleep and exertion.  Active patients require portable oxygen.  If oxygen was prescribed during an exacerbation, recheck ABGs after 30–90 days.  Withdrawal of oxygen because of improved Pa,O2 in patients with a documented need for oxygen may be detrimental.  Patient education improves compliance
  • 40. In-patient oxygen therapy-COPD  The goal is to prevent tissue hypoxia by maintaining arterial oxygen saturation (Sa,O2) at >90%.  Main delivery devices include nasal cannula and Venturi mask.  Alternative delivery devices include non-rebreathing mask, reservoir cannula, nasal cannula or transtracheal catheter.  Arterial blood gases should be monitored for arterial oxygen tension (Pa,O2), arterial carbon dioxide tension (Pa,CO2) and pH.
  • 41.  Arterial oxygen saturation as measured by pulse oximetry (Sp,O2) should be monitored for trending and adjusting oxygen settings.  Prevention of tissue hypoxia supercedes CO2 retention concerns.  If CO2 retention occurs, monitor for acidaemia.  If acidaemia occurs, consider mechanical ventilation.
  • 42. Monitoring oxygen therapy Oxygen therapy should be given continuously and should not be stopped abruptly until the patient has recovered, since sudden discontinuation can wash-out small body stores of oxygen resulting in fall of alveolar oxygen tension. The dose of oxygen should be calculated carefully. Partial pressure of oxygen can be measured in the arterial blood. Complete saturation of hemoglobin in arterial blood should not be attempted. Arterial PO2 of 60 mmHg can provide 90% saturation of arterial blood, but if acidosis is present, PaO2 more than 80 mmHg is required. In a patient with respiratory failure, anaemia should be corrected for proper oxygen transport to the tissue.
  • 43. A small increment in arterial oxygen tension results in a significant rise in the saturation of hemoglobin. Under normal situations, no additional benefit is secured by raising PaO2 level to greater than 60 to 80 mmHg. An increase of 1% oxygen concentration elevates oxygen tension by 7 mmHg. It is necessary to maintain normal hemoglobin level in the presence of respiratory disease as proper oxygen transport to the tissues is to be maintained. Measurement of arterial blood gases repeatedly is difficult so a simple and non- invasive technique like pulse oximeter may be used to assess oxygen therapy.
  • 44. When to stop oxygen therapy Weaning should be considered when the patient becomes comfortable, his underlying disease is stabilized, BP, pulse rate, respiratory rate, skin color, and oxymetry are within normal range. Weaning can be gradually attempted by discontinuing oxygen or lowering its concentration for a fixed period for e.g., 30 min. and reevaluating the clinical parameters and SpO2 periodically. Patients with chronic respiratory disease may require oxygen at lower concentrations for prolonged periods.
  • 45. Impact on the patient  Fear death is likely to occur sooner  Become less active  Experience a sense of loss of freedom  May become more socially isolated
  • 46. Hazards & complications of oxygen therapy  Oxygen-induced hypoventilation  Oxygen toxicity/O2 narcosis  Absorption atelectasis  Retinopathy  Drying of mucous membranes  Infection  Fire hazards
  • 47.
  • 48. Oxygen is one of the most important drugs you will ever use, but it is poorly prescribed by medical staff. In 2000, a Nicola Cooper and colleague did survey of treatment with oxygen. The first looked at prescriptions of oxygen in postoperative patients in a large district hospital. They found that there were many ways used to prescribe oxygen and that the prescriptions were rarely followed.
  • 49. Oxygen dissociation curve Shift to the left in O2 curve { O2 affinity } 1. Causes: pH, CO2, 2-3 DPG, Temp. 2. Results: O2 sat. for any pao2 but resulting in less gradient to move O2 to tissue. (Carries more O2 but more difficult to release it at tissue level) 3. Examples: stored blood loses 2-3 dpg a shift to the left results from this. Hyperventilation, Hypothermia.
  • 50. Shift to the right in O2 curve { O2 affinity } 1. Causes: pH , CO2 , 2-3 DPG, Temp. 2. Results: O2 sat for any PaO2 but resulting in more gradient to move o2 into the tissues. 3. Examples: hypoventilation, fever, metabolic acidosis.