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GOOD MORNING

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Title: GOOD MORNING


1
GOOD MORNING
www.anaesthesia.co.in anaesthesia.co.in_at_gmail.c
om
2
Oxygen Therapy O2 Delivery Systems
  • Piyush / Dr.Chitra

3
Oxygen
  • Colorless,odorless
  • Scheele prepared before Priestley but could not
    recognise it.
  • By Priestley in 1774
  • MW-32
  • Noninflammable but strongly helps combustion

4
Oxygen cascade
  • During transit from the ambient air to the
    cellular structures the po2 oxygen drops from
    152mm Hg to a few mmHg in the mitochondria this
    gradient drop is described as oxygen cascade

5
O2 Cascade
Air
mitochondria
6
O2 Cascade
159mm Hg (20.95 of 760)
Atm. Air (dry)
Humidification 6 Vol (47mm Hg)
Lower Resp. Tract (moist 37oc)
149mm Hg 20.95 of 713 (760-47)
7
O2 Cascade
Lower Resp. Tract (moist 37oc)
149mm Hg (20.95 of 713)
O2 consumption
Alv. ventilation
101mm Hg
Alveolar air
PA O2 FI O2 (Pb 47) PaCo2 x F
8
O2 Cascade
101mm Hg
Alveolar air
Venous admixture
Arterial blood
97mm Hg
Pa O2 100 0.3 x age (years) mm Hg A a
4 25 mmHg
9
Venous admixture(physiological shunt)
O2 Cascade
Low VA/Q
Normal True shunt (normal anatomical shunt)
Pulmonary (Bronchial veins)
Extra Pulm. (Thebesian veins)
Normal upto 5 of cardiac output
10
O2 Cascade
Pa O2 97mm Hg (Sat. gt 95 )
Arterial blood
Utilization by tissue
Mixed Venous blood
Cell Mitochondria PO2 7 37 mmHg
PV O2 40mm Hg Sat. 75
Pasteur point The critical level for aerobic
metab. to continue (PO2 1-2 mmHg in
mitochondria, 22mmHg in capillary)
11
Blood Oxygen Content and Dissociation Curve
  • ODC relates the saturation of the hemoglobin to
    the PO2.
  • It is a sigmoid in shape .

12
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13
  • Arterial oxygen content O2.CONTHbX1.34XSaO2
    PaO2 X.0034
  • 15 x 1.34 x 0.98
  • 20 ml 100 ml-1 of blood (ignoring that
    dissolved in plasma)
  • or 200 ml l-1

14
Dissolved O2 in plasma
  • Breathing Air (PaO2 100mm Hg)
  • 0.3ml / 100ml of blood
  • Breathing 100 O2 (PaO2 600mm Hg)
  • 1.8ml / 100ml of blood
  • Breathing 100 O2 at 3 Atm. Pressure
  • 5.4ml / 100ml of blood

15
Oxygen delivery/Flux
  • It is amount of oxygen carried by arterial blood
    per minute.
  • Overall oxygen delivery arterial oxygen content
    x cardiac output
  • Oxygen delivery 5 x 200
  • 1000 ml min-1

16
Oxygen Therapy
  • Indications

17
Criteria for Ordering Oxygen Therapy
  • PaO2 at or below 55 mm Hg
  • Saturation O2 lt 88 resting
  • PO2 lt55 mm Hg or lt 88 for 5 min. (sleep)
  • A drop in PO2 10 mm Hg or 5 in O2 sat. during
    sleep
  • Symptoms or signs of heart failure (cor
    pulmonale), pulmonary hypertension,
    erythrocytosis, P pulmonale on EKG
  • PO2 lt55 mm Hg or lt 88 during exercise

18
Oxygen Therapy
Indications
FIO2 - FIO2 during anaes. - Rebreathing
Barometric Pressure - High altitude
PIO2
  • O2 Consumption
  • convulsions
  • thyrotoxicosis
  • -shivering
  • -pyrexia
  • (7 / o C)
  • Alveolar Ventilation
  • resp. depression
  • Resp. muscle paresis
  • resp.effort (trauma)
  • airway obstruction

PAO2
19
Oxygen Therapy
Indications
  • Low VA/Q
  • Abn. Pulmonary shunt
  • - pneumonia
  • lobar atelectasis
  • ARDS
  • Normal Anat. shunt
  • Abn.extra Pulm. Shunt
  • cong. heart disease
  • (R L )

PaO2
Perfusion local - PVD, thrombosis gen
shock, Hypovol.,
card. Failure cardiac arrest
  • Hb concentration
  • Anaemia
  • CO poisoning

Cell PO2
Hypoxia
20
  • Hypoxia lack of adequate oxygen in the blood
  • 4 types of hypoxia
  • Hypoxic Hypoxia
  • lack of O2 in air
  • Anemic Hypoxia
  • decreased hemoglobin (Hgb) level in blood
  • Ischemic (Stagnant) Hypoxia
  • decreased blood flow (heart)
  • Dysoxic (Tissue) Hypoxia
  • Cells unable to use O2 in blood
  • Cyanide poisoning

21
Benefit of O2 therapy in Hypoxia
  • Hypoxic hypoxia (gas phase)
  • Anaemic hypoxia (fluid phase const.)
  • Stagnant hypoxia (fluid phase flow)
  • Histotoxic hypoxia (tissue phase) -

22
Dark side of oxygen therapy
23
Oxygen induced Free Radical Cell Injury
  • It can occur due to overzealous use of oxygen
    which produces reactive oxygen species (ROS) as a
    metabolite.
  • Major ROS are
  • Superoxide (O2.-)
  • Hydrogen peroxide (H2O2)
  • Hydroxyl radical (HO.)

24
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25
Free Radical Mediation of Cell Injury
  • Free Radical Injury Mechanisms
  • Lipid peroxidation of membranes
  • double bonds in polyunsaturated lipids
  • Lesions in DNA
  • reactions with thymine with single-strand breaks
  • Cross-linking of proteins
  • Leading to denaturation

26
Cellular defenses against ROS(Antioxidants)
  • Enzymatic
  • SOD, catalase, GPX
  • Non-enzymatic
  • Vitamins A, C, E
  • Glutathione
  • selenium
  • Ceruloplsmin and transferrin

27
  • OXYGEN
    THERAPY
    APPARATUS AND DEVICES

28
Oxygen sources and delivery
  • There are three typical sources of oxygen used
    therapeutically
  • Liquid oxygen is contained in thermally
    insulating tanks. The liquid has to boil changing
    into a gas for breathing. Large tanks are used by
    hospitals. Small tanks can be used domestically.
    Liquid oxygen tanks are refilled by liquid oxygen
    suppliers.
  • Cylinders contain compressed gaseous oxygen.
    Small cylinders are used for first aid and for
    home oxygen patients when mobility is required.
    Cylinders are refilled by a gas supplier.

29
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30
  • Oxygen concentrators are electrically powered
    devices which remove nitrogen from air.
  • They are most commonly used in a domestic
    situation, because they do not need refilling.
  • FIO2 is never 100
  • The higher the liter flow setting the lower the
    FIO2

31
O2 Delivery systems
  • Ambient pressure
  • Variable performance devices
  • Fixed performance devices
  • Positive pressure ventilation
  • Non invasive (BIPAP, CPAP)
  • Invasive
  • ECMO

32
O2 Delivery systems
  • Ambient pressure
  • Variable performance devices (Pt. dependent) low
    flow
  • No capacity system no rebreathing
  • nasal catheter / cannulae
  • Capacity system chance of rebreathing
  • Small (mass shell only)
  • Large (with reservoir bag)
  • Fixed performance devices (Pt. independent) high
    flow
  • HAFOE (ventimask)
  • Anaesthesia circuits

33
Nasal Catheter
  • simplest, most common appliance
  • Approximate FiO2s
  • 1 L/m O2 20 4
  • assume patient is breathing normally
  • Liter flow not to exceed 6 L/m
  • not well tolerated by patients
  • FiO2 doesnt increase over 6 L/m

34
Nasal Catheter
  • Merits
  • Easy to fix
  • Keeps hands free
  • Not much interference with further airway care
  • Small but definite rise in FiO2 (dose not
    critical)
  • Demerits
  • Mucosal irritation (uncomfortable)
  • Gastric dilatation (especially with high flows)

35
Simple face mask
  • Extension of anatomic reservoir to provide
    higher FiO2s
  • Flow 6-10 L/m
  • Ensure flush of CO2
  • FiO2 35-60
  • Dependent on
  • oxygen flow
  • mask seal to face
  • ventilatory pattern
  • exhale air through side holes

36
Face Masks
  • Merits
  • Higher Oxygen Conc.
  • Demerits
  • Proper fitting is required
  • Rebreathing (if O2 flow is inadequate)
  • Interfere with further airway care
  • Uncomfortable (sweating, spitting)

37
Partial Rebreather
  • Uses bag as additional reservoir
  • Exhaled air mixed with 100 O2 in bag
  • 1st 1/3 of exhaled air is anatomic dead
    space gas with very little CO2
  • Bag fills, directs remaining 2/3 of exhaled air
    out the vent holes

38
Non-Rebreather
  • No exhaled gas is rebreathed
  • Flap covers vent hole
  • One-way valve between bag and mask
  • Can achieve 90 FiO2
  • Flow adjusted same as partial RB

39
Venturi mask
  • The venturi mask, also known as an
    air-entrainment mask, is a medical device to
    deliver a known oxygen concentration to patients
    on controlled oxygen therapy.
  • The mechanism of action depends on the venturi
    effect.

40
  • The Venturi effect is the fluid pressure that
    results when an incompressible fluid flows
    through a constricted section of pipe.
  • The Venturi effect may be derived from a
    Bernoulli's principle.
  • The fluid velocity must increase through the
    constriction while its pressure must decrease due
    to conservation of energy the gain in kinetic
    energy is supplied by a drop in pressure or a
    pressure gradient force.

41
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42
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43
  • The color of the device reflects the delivered
    oxygen concentrationfor
  • blue 24
  • white 28
  • orange 31
  • yellow 35
  • red 40
  • green 60.

44
  • Entrainment ratio
  • Entrained flow/driving flow
  • As 9 to 1 ratio indicates that there are
    9lit/min being entrained by a driving gas of 1
    lit/min.

45
HIGH FLOW DEVICE (venturi principle)
  • FiO2 O2 flow l/m
  • 24 4
  • 28 6
  • 31 8
  • 35 10
  • 40 12
  • 50 15
  • O2air Totalflowl/m
  • 125 105
  • 110 68
  • 17.0 63
  • 14.6 56
  • 13.2 50
  • 11.67 32

46
Paediatric oxygen therapy
47
Incubator
  • Small infants not on ventilator
  • Works on venturi principle
  • Complete air change 10 times / hour
  • Control of humidity temperature
  • O2 conc. falls rapidly when access ports are open

48
Oxygen hood
  • Used for infants.
  • Made up of transparent plexiglass box.
  • Placed over infant head and neck to ensure
    adequate FiO2.
  • Oxygen flow should be three times of the minute
    ventilation to prevent CO2 accumulation.

49
O2 tents
  • For children not tolerating mask / catheter
  • Large capacity system
  • Upto 50 O2 concentration
  • Flush tent with high flow of oxygen and maintain
    _at_8-10 lit/min.
  • Large tent cap. and leak port limited CO2 build
    up.
  • Disadvantage
  • Limited access
  • Risk of fire
  • Conflict in O2 therapy / nursing care

50
Bag Valve Mask assembly(Ambu Resuscitator)
  • Delivers O2 during BOTH spont. artf. Vent
  • O2 concentration
  • 30 50 (without reservoir)
  • 80 100 (with reservoir)
  • To deliver 100 O2
  • Reservoir as large as bag vol
  • O2 flow rate gt minute volume (10 l/m)
  • Drawback keeps rescuers hands engaged

51
HELIOX
  • Helium 79 with 21 oxygen
  • Low density helium decreases turbulence at narrow
    airway and also reduces pressure drop
  • turbulent flow depends proportionally to pressure
    drop, density ,velocity
  • Useful in croup, tracheal stenosis, laryngeal,
    tracheal tumors (large airway obstruction)

52
Extra-corporeal membrane oxygenation
  • ECMO which is Extra-corporeal membrane
    oxygenation, is a temporary life support system
    used for patients who have failed traditional
    mechanical ventilation.

53
  • Used in severe lung injury where high PEEP or
    PIP causes further lung damage eg pneumonia
    ,ARDS
  • 2 techniques veno-venous
  • blood (central venous circ oxygenator
    right atrium) lung not bypassed, ventilated
    to maintain ABG.
  • veno-arterial central venous circ
    oxygenator systemic circulation
  • lung completely rested,or static inflation

54
INTRAVASCULAR OXYGENATION
  • IVOX long bundle of hollow microporous
    polypropylene fibres with double lumen gas tube
    for passing oxygen.
  • Placed in IVC thru femoral vein
  • Gas exchange depends on pr. Gradient
  • 40 70 ml/min O2 and CO2
  • In ARDS, helps to reduce the intensity of lung
    ventilation.
  • DISADV blood loss, thrombotic event, infection,
    dec. venous return, vasc. injury

55
Hyperbaric oxygen
  • Is a treatment in which a patient breathes 100
    oxygen intermittently while pressure of the
    treatment chamber increased to a point higher
    than sea level pressure
  • HBO was proved to cause hyperoxygenation of
    normal tissue and of tissue with poor blood
    perfusion by increasing the dissolved fraction of
    oxygen in plasma

56
  • At sea level the plasma oxygen concentration is 3
    ml/l.
  • At a pressure of 3 atmospheres dissolved oxygen
    approaches 54 ml/l of plasma, which is almost
    sufficient to supply the resting total oxygen
    requirement of many tissues without a
    contribution from oxygen bound to haemoglobin.

57
Approved Indications for HBO2
  • Enhancement of healing in selected problem wounds
  • Anaemia
  • Necrotizing soft tissue infections
  • Osteomyelitis (refractory)
  • Osteoradionecrosis (ORN),soft tissue
    radionecrosis,radiation tissue damage
  • Skin grafts and flaps failure
  • Thermal burns
  • Air or gas embolism
  • Carbon monoxide poisoning and smoke inhalation,
    carbon monoxide complicated with cyanide
    poisoning
  • Clostridial myonecrosis (gas gangrene)
  • Crush injuries, compartment syndrome and other
    acute traumatic ischemias
  • Decompressed sickness

58
Cellular and biochemical benefits of hyperbaric
oxygen
  • - Promotes angiogenesis, fibroblast
    activation and wound healing
  • - Kills certain anaerobes
  • - Prevents growth of species such as
    Pseudomonas
  • - Prevents production of clostridial alpha
    toxin
  • - Causes up regulation of growth factors,
    down regulation of inflammatory cytokines
  • - Restores neutrophil mediated bacterial
    killing in previously hypoxic tissues

59
Method of administration
  • Monoplace chamber (accomodates only a single
    person and pressurized to about 2-2.5 ATA with
    100 oxygen
  • Multiplace chamber (can accommodate several
    patients and/or health care peronnel, patients
    breath 100 oxygen through head tent, face mask
    or endotracheal tube.
  • In either case the arterial PO2 will approach
    1500 mm Hg (Normal 90-95 mm Hg).

60
Role in CO poisoning
  • CO is colorless odorless and tasteless.
  • Compete with oxygen for hemoglobin and form COHb.
  • Level of COHb does not correlate severity of
    poisoning.
  • Interfere with oxygen delivery and utilization by
    shifting ODC to left and inhibiting cytochrome
    oxidase respectively.

61
  • CO elimination is based on
  • FiO2
  • Individual metabolism
  • Duration of exposure
  • Minute ventilation

62
  • Half life of COHb
  • Breathing room air- 4-6 hrs
  • Normobaric 100 O2 40-80min
  • Hyperbaric O2 _at_ 2.8 ATA 15-30 min

63
HAZARDS OF OXYGEN THERAPY
  • Retinopathy of Prematurity (neonates)
  • PaO2 gt 80 100 torr
  • opaque, fibrotic tissue forms behind lens of
    eye
  • retina detachment
  • blindness

64
  • Oxygen-induced hypoventilation
  • seen in patients with chronic hypercapnia
  • knocks out hypoxic drive
  • Intermittent use may, in some patients, cause
    PaO2 to drop lt pre-Rx levels

65
  • Absorption Atelectasis
  • N2 comprises 78 of air,maintains alveolar
    stability
  • Poorly ventilated alveoli lose oxygen to blood
    faster than it can be replenished
  • Alveoli decrease in size collapse
  • True shunt hypoxemia increases

66
Complications of HBO2 Therapy
  • Confinement anxiety
  • Barotraumas
  • Increased gas density leading to turbulent flow
    and increased heat loss.
  • Oxygen toxicity
  • Reversible myopia
  • Decompression sickness
  • Fire hazards

67
Oxygen Toxicity
  • CNS -Oxygen toxicity seizures
  • Lung -Pulmonary Oxygen Toxicity
  • Eye -Refractory changes (transient)

68
CNS Oxygen Toxicity
  • Signs and Symptoms
  • Convulsion, nausea ,dizziness, hiccups, muscle
    twitching, vision and hearing abnormalities,
    difficulty breathing, unusual fatigue, anxiety
    and confusion,dizziness
  • Time/Dose
  • 2 ATA4 hrs
  • 3 ATA2 hrs
  • 4 ATA15 min
  • 5 ATA5 min

69
  • Visual Effects of Oxygen Toxicity
  • Refractive Index changes in patients greater than
    40 years old
  • following 2-3 weeks HBO treatment. Transient
    effect.
  • Cataracts may worsen.

70
Barotrauma
  • Middle Ear
  • Paranasal Sinus
  • Gastrointestinal Tract
  • Lungs
  • Pneumothorax

71
Take home message
  • O2 is a drug commonly prescribed by medical and
    paramedical staff.
  • It is life saving when correctly administered but
    it has known side effects.
  • It should be administered in proper dose for a
    clear indication by a proper delivery system for
    a duration of time required along with vigilant
    monitoring.

72
Thank you
www.anaesthesia.co.in anaesthesia.co.in_at_gmail.c
om
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