Title: The Physiology of Respiration
1The Physiology of Respiration
2Introduction
- prime function of the respiratory system is to
facilitate transport of oxygen (O2) from the
atmosphere into blood - and the transport of carbon dioxide (CO2) from
the blood into the atmosphere.
3Why do we need to breathe?
- Breathing gets O2 into the body so that cells can
make energy - Cells use energy to contract muscles and power
thousands of biochemical reactions taking place
in cells every second - Without O2 cells cant make energy - without
energy cells die
4- Inside cells, most energy is made by the
mitochondria - In the form of a small packet of energy called
ATP (adenosine triphosphate) - During energy production, glucose and lipids are
broken down and their energy used to produce ATP - O2 is consumed and CO2 is formed as a waste gas.
5Figure 01. Oxygen (O2) from the air in the lungs
diffuses into the blood. It is transported in the
blood to the cells. Oxygen diffuses from the
blood into the cells. Carbon dioxide (CO2) from
the cells diffuses into the blood, It is
transported in the blood to the lungs. In the
lungs carbon dioxide diffuses into the air and is
breathed out
6The anatomy of the Respiratory System
- The structure of the respiratory system allows
transfer of air between the outside of the body
and the respiratory membranes in the lungs - Site
of gas exchange
7pharynx
epiglottis
larynx
oesophagus
cartilage ring
trachea
rib
intercostal muscles
bronchus
bronchiole
heart
parietal pleura
visceral pleura
left lung
diaphragm
8- A series of tubes Trachea, Bronchi, to the
smallest bronchioles, transfer air from outside
to the alveoli - where gas exchange takes place
- millions of alveoli in each lung
- each surrounded by a network of capillaries
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10Respiratory Zone
- Gas exchange site
- Smallest (terminal) bronchioles and alveoli
- Walls of alveoli single layer
- Type I cells (simple squamous)
- Type II cells
- Cuboidal
- Secrete surfactant
- Alveolar macrophages (dust cells)
11The Pleura and Pleural Fluid
- The Pleural membranes
- Parietal pleura lines thoracic wall and
diaphragm - Visceral pleura covers external lung surface
- Pleural Fluid
- Fills pleural cavity
- Lubricates
- Surface tension of pleural fluid prevents
separation of pleura - Prevents collapse
12Airflow
- Airflow rate is dependant upon
- Airway Resistance
- Magnitude of frictional interactions between
flowing gas molecules - Length of airway
- Radius of conducting airways
- Main determinant of resistance
- Pressure gradient
- Movement from high to low (i.e. diffusion)
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14Airway resistance
- In a healthy respiratory system airway resistance
is low so main determinant of airflow rate is
pressure gradient - Changes in airway size are achieved by ANS
depending upon the bodys needs - Parasympathetic
- Occurs in quiet relaxed situations (rest
digest) - Promotes bronchoconstriction
- Sympathetic
- Occurs during exercise / active situations (fight
or flight) - Promotes bronchodilation
15Inspiration
- Can be quiet or forced
- Contraction of diaphragm and external intercostal
muscles increase volume of thoracic cavity - As thoracic cavity increases, lungs are stretched
- pleura - Intrapulmonary volume increases
- Results in a drop in intrapulmonary pressure
- Air will rush in until pressure is equal on both
sides
16Inspiration
- Deep (Forced) inspiration
- Occurs during
- Vigorous exercise
- COPD
- Capacity of lungs increased
- Involves other neck and chest muscles
- Sternocleidomastoid muscles
- Scalenes
- Pectoralis minor
17Expiration
- Passive process
- diaphragm and external intercostal muscles relax
- decreases volume of thoracic cavity
- As thoracic cavity decreases, lungs recoil
- Intrapulmonary volume decreases
- Results in an increase in intrapulmonary pressure
- Causes gases to flow out of lungs
18Forced expiration
- Active process (requires energy)
- Produced by contraction of abdominal wall muscles
(most influential) and internal intercostal
muscles - Contractions
- Increase intra-abdominal pressure by forcing
abdominal organs against diaphragm - Depresses rib cage
19Ventilation
- Thus
- Air enters and leaves lungs by changes in
pressure gradients. - pressure changes brought about by Volume changes
- Volume changes brought about by actions of
respiratory muscles
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21Factors affecting pulmonary ventilation
- Airway resistance
- Elasticity
- Elastic recoil
- Connective tissue contains large amounts of
elastin fibres - Compliance
- Distensibility of lungs
- Compliant lung easily stretched, little pressure
required to inflate lungs
22Surface tension
- Alveolar surface tension displayed by thin
liquid film that lines each alveolus - At an air-water interface, water molecules are
more strongly attracted to each other than to air
molecules - This produces a force known as surface tension
- Consequently an alveolus would
- Resist being stretched
- Tend to reduce in size
- Tend to recoil after being stretched.
- Greater the surface tension the less compliant
the lungs
23Pulmonary surfactant
- If alveoli were lined with water alone lungs
would collapse and i.e. poor compliance - Type II alveolar cells secrete surfactant
- a phospholipoprotein which spreads between water
molecules thereby reducing surface tension.
24Causes of pulmonary surfactant deficiency
25Work of breathing
- Energy expenditure during breathing depends upon
- Rate and depth of ventilation
- Lung compliance
- Airway resistance
26External (Pulmonary) Respiration
- PO2 of alveolar air is 13.3kPa/105mmHg
- PO2 of deoxygenated blood entering pulmonary
capillaries is 5.3kPa/40mmHg. - Consequently oxygen diffuses from alveoli into
blood stream until equilibrium is reached at
13.3kPa - PCO2 of deoxygenated blood is 6.1kPa, PCO2 of
alveolar air is 5.3kPa. What will occur?
27Internal (Tissue) Respiration
- PO2 in tissue cells is 5.3kPa
- PO2 of oxygenated blood entering pulmonary
capillaries is 13.3kPa. - Consequently oxygen diffuses from blood stream
into cells until PO2 in blood declines to 5.3kPa - PCO2 of oxygenated blood is 5.3kPa, PCO2 in
tissue cells is 6.1kPa. What will occur?
28Principles of gaseous exchange
- Daltons Law states total pressure exerted by a
mixture of gases sum of pressures exerted by
each gas in mixture. - The pressure exerted by each gas (partial
pressure p) is directly proportional to its
percentage in the total gas mixture. - Related to blood gas partial pressures pCO2 and
pO2. Thus if concentration of oxygen in plasma
decreases, pO2 decreases
29- Boyles law states volume is inversely
proportional to pressure - relevant to
principles of ventilation. - When intra-pulmonary volume increases pressure
decreases
30- Henrys Law states when a mixture of gases is in
contact with a liquid, each gas will dissolve in
the liquid in proportion to its partial pressure - This relates to gaseous exchange at alveolar /
pulmonary capillary membrane.
31Respiratory Control Centres
- Inspiratory centre in medulla oblongata
- Expiratory centre in medulla oblongata
- Apneustic centre in pons
- Pneumotaxic centre in pons
32Control of Respiration
- The inspiratory centre in medulla sets breathing
rhythm - connected to diaphragm via phrenic nerves
(III,IV,V cervical nerves) and to intercostal
muscles via intercostal nerves (T1-12 thoracic
nerves). - Impulses stimulate contraction and inspiration
follows - When impulses cease, muscles relax and expiration
occurs - Cycle repeats approx. 12-15 times per minute
(autorhythmic neurones).
33Control of Respiration
- Expiration results from passive recoil of the
lungs ( muscles) - Neurones of expiratory centre (Ventral
Respiratory Group) are inactive during quiet
breathing but are activated during
forced/laboured breathing - Expiratory centre contains both inspiratory and
expiratory neurones and is activated during
forced breathing. - stimulates contraction of internal intercostals
and abdominal muscles. Furthermore VRG increases
inspiratory activity.
34Control centres in the pons
- Pons exerts fine tuning influences over the
medullary centres - Pneumotaxic centre
- Switch off inspiratory neurones, thus limiting
duration of inspiration - Apneustic centre
- prevents inspiratory neurones from being
switched off thus prolonging inspiration.
35Pneumotaxic centre
-ve
Apneustic centre
ve
Respiratory centre
-ve
ve
LUNGS
Neuronal control of respiration
36Factors affecting rate and depth of respiration
- Hering Breuer reflex
- Stretch receptors in bronchi and bronchioles
- When stimulated, send impulses along vagus nerve
to inspiration (Pneumotaxic?) centre - Inspiration is inhibited and expiration occurs
- Prevents over inflation of lungs
37Factors affecting rate and depth of respiration
- Voluntary Control
- Control from cerebral cortex (breath-holding,
speech etc.) - Chemical regulation
- Central chemoreceptors in medulla sensitive to
changes in H conc or PCO2 in CSF - Peripheral chemoreceptors in aortic and carotid
bodies are sensitive to changes in H, PCO2 and
PO2
38ChemoreceptorsCO2 H2O ? H2CO3 ? H HCO3-
- H sensitive
- Central ( poor diffusion across BBB)
- Peripheral
- Carbon dioxide sensitive powerful respiratory
stimulant - Peripheral
- Weakly sensitive to arterial pCO2
- Central
- Very sensitive to H in CSF
- Oxygen sensitive
- Peripheral (carotid arteries and aortic arch)
- Stimulated when oxygen tension falls below 8kPa
/90 sat - Sensitive to pO2 implications?
39Gas transport
40Oxygen transport
- Total oxygen content includes
- Percentage dissolved 2
- Reflected by pO2
- Amount of O2 dissolved in plasma
0.23ml/litre/kPa - Carriage by haemoglobin 98
- Reflected by SaO2
- 1g of Hb can carry 1.34ml of oxygen if fully
saturated
41Haemoglobin (Hb)
- Protein part globulin is composed of 4
polypeptide chains - Each polypeptide chain has an iron containing
haem group - Oxygen binds to the haem group forming
oxyhaemoglobin - Each haemoglobin molecule can carry up to 4 units
of oxygen - Haemoglobin binding to oxygen is reversible
42Haemoglobin
Each subunit has an iron ion
43Haemoglobin
Oxygen binds to the iron ion
Insufficient iron in the diet means less oxygen
can bind and may result in anaemia
44Oxygen dissociation curve
- The degree to which oxygen binds with Hb depends
upon (PO2)(oxygen tension) see oxygen
dissociation curve - The affinity of Hb for O2 is not constant
- The first molecule of oxygen binds with Hb with
relative difficulty - The second and third molecules have a greater
affinity (as seen by the steepest part of the
sigmoid curve) - The fourth oxygen molecule binds with the
greatest difficulty
45Oxygen dissociation curve
- The sigmoid shape of the O2 curve is
physiologically significant - Oxygen diffuses into red blood cells at the
lungs, then diffuses out at the site of the
tissues - The speed of loading and unloading of oxygen is
dictated by partial pressure gradients
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47Partial pressure gradients oxygen binding
- Blood arriving in the lungs has a low PO2 of
5.3kPa and is exposed to alveolar PO2 of 13.3kPa - Oxygen diffuses down the gradient from alveoli
into plasma - This causes a rise in plasma PO2 enabling oxygen
to diffuse into the red blood cells - As PO2 increases from 5.3 to 8kPa in the red
blood cells, there is rapid loading so Hb
saturation reaches 90 ( steepest part of the
curve) - Thereafter O2 uptake declines until 97 is
attached at 13.3kPa O2 - This flat portion of the curve provides a safety
barrier as even if PO2 falls to 8kPa as might
occur in lung disease, 90 of Hb remains saturated
48Partial pressure gradients oxygen release
- As blood enters the tissues, still with a PO2 of
13.3kPa, it is exposed to PO2 of 5.3kPa so oxygen
is readily released - oxygen diffuses from the plasma into the tissues,
causing a drop in plasma PO2 and thus HbO2 to
dissociate - Plasma PO2 remains relatively high, facilitating
oxygen diffusion into the cells - If tissue activity increases, Plasma PO2 may fall
to 2kPa which allows Hb to release 80 of its
oxygen - Below PO2 of 1.3kPa myoglobin allows greater
oxygen extraction from the blood
49Factors affecting Hb affinity
- Factors reducing affinity
- Reduction in pH
- Increase in pCO2
- Increase in temp
- Increase in 2,3-Diphosphoglycerate( produced
during anaerobic glycolosis) - Carbon monoxide (CO)
- Factors which increase affinity
- Increase in pH
- Reduction in pCO2
- Reduction in temp
- Reduction in 2,3-DPG
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51Hypoxia
- Hypoxia indicates the situation where tissues are
unable to undergo normal oxidative processes
because of a failure in the supply or utilisation
of oxygen. There are four categories of Hypoxia - Hypoxic hypoxia
- Anaemic hypoxia
- Stagnant (circulatory) hypoxia
- Histotoxic hypoxia
52Hypoxic hypoxia
- Inadequate PO2 in arterial blood (PaO2). May
results from - Inadequate PO2 in inspired air
- Major hypoventilation
- Inadequate alveolar capillary transfer
53Anaemic Hypoxia
- PaO2 normal but concentration of functional
haemoglobin is reduced. - Possible causes of anaemia
- Deficiencies of iron, vitamin B12, folate or
copper - Kidney disease affecting production of
erythropoietin - Excessive blood loss
- Hereditary spherocytosis (RBCs have short life
span) - Carbon monoxide poisoning
54Stagnant hypoxia
- Reduction in supply of oxygen to tissues produced
by a reduced blood flow i.e. circulatory failure
(e.g. angina, claudication etc.) - PaO2 (and PaCO2) may be normal but delivery is
not. Initially tissue oxygenation is maintained
by increasing the degree of oxygen extraction
from the blood, but as tissue perfusion worsens
this becomes insufficient and tissue hypoxia
occurs.
55Histotoxic hypoxia
- Occurs when respiring cells are prevented from
using oxygen disabled oxidative phosphorylation
enzymes - Causes include
- Cyanide poisoning
- Toxins produced by sepsis
- PaO2 is normal
56Management of hypoxia
- Aim maintain adequate perfusion pressure and
oxygen delivery to ensure regional delivery.
Reduce tissue oxygen demand by reducing metabolic
rate. Achieved by - Respiratory support
- Oxygen therapy
- Non invasive or mechanical ventilation
- Cardiovascular support
- Optimise preload
- Reduce afterload
- Increase contractility
- Increase HR
- Maintain Hb within normal levels if needed
57Transport of CO2
- Three methods of transport
- Dissolved in plasma (PCO2) approx 7
- Binds to haemoglobin to form carbaminohaemoglobin
approx 23 - Majority travels as bicarbonate ion HCO3- -
approx 70
58CO2 transport at cells
- CO2 leaves cell, diffuses through interstitial
fluid and enters capillary. Driven by pressure
gradient. - Most of the CO2 enters erythrocytes where the
following reaction occurs, catalysed by carbonic
anhydrase - CO2 H20 H2CO3 H HCO3-
- bicarbonate ions leave the RBC and travel to
lungs in the plasma. It often combines with Na
in the plasma to form sodium bicarbonate. In
exchange Cl- ions enter RBCs - Hydrogen ions bind to haemoglobin ( buffer /Bohr
shift) - Approx 23 of CO2 binds to amino group of Hb.
Binding is influenced by PCO2. High PCO2(i.e. in
tissue capillaries) promotes formation of
carbaminohaemoglobin.
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60CO2 transport in lungs
- When the RBCs arrive at the pulmonary capillaries
the chemical reaction is reversed. - The bicarbonate ions re-enter the cell, combine
with the hydrogen ions, forming carbonic acid
which then dissociates to carbon dioxide and
water. - The carbon dioxide diffuses across the capillary
wall, enters the alveolus and is exhaled.
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62References
- Treacher, D.F . and Leach,R.M. (1998) BMJ 317,
p1302-1306 - Leach,R.M. and Treacher,D.F. (1998) BMJ, 317,
1370-1373 - See Update in Anaesthesia articles on
- The physiology of oxygen delivery issue 10 (1999)
article 3, p1-3 - Oxygen Therapy issue 12 (2000) article 3 p1-3
- Oxygen Transport issue 12 (2000) article 11 p1-3
- http//www.lakesidepress.com/pulmonary/ABG/PO2.htm