2. Respiratory abnormalities during sleep Prof. Dr. J. Verbraecken
Dept of Pulmonary Medicine and Sleep Disorders Center
Antwerp University Hospital, Belgium
3. outlines Snoring
Obstructive sleep apnea (OSA)
Central sleep apnea (CSAS)
Cheyne-Stokes respiration (CSR)
UARS
Hypoventilation
Nocturnal dyspnea DD
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking,
…
4. Snoring Turbulence of inspired air
Vibrations of the mucosa
Mostly during inspiration
Partial occlusion/flow limitation of the pharynx during sleep
7. Anamnesis �Snoring Intermittent and discrete snoring only when lying in the supine position
Constant and loud snoring
Supine/all positions
Socially unacceptable snoring
sleeping with partner impossible, disturbing environment
Bothers relationship
Maximal limit for noise in the house at night: 45 decibel
8. Snoring according to body position
9. Snoring
11. outlines Snoring
Obstructive sleep apnea (OSA)
Central sleep apnea (CSAS)
Cheyne-Stokes respiration (CSR)
UARS
Hypoventilation
Nocturnal dyspnea DD
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking,
…
12. SLEEP APNEA�DEFINITIONS Apnea= interruption of flow at nose and mouth during at least 10 seconds.
Central apnea
Obstructive apnea
Mixed apnea
Hypopnea
15. OSAS: CURRENT DEFINITION Sleep apnea-syndrome: > 5 apneas-hypopneas/hour sleep
AND
Excessive daytime sleepiness unexplained by any other factors
OR
2 or more of the following symptoms:
choking or gasping during sleep
Awakening regularly during sleep
Unrefreshed in the morning
Fatigue
Disturbed concentration Obstructive sleep apnea syndrome (OSAS)
Central sleep apnea syndrome (CSAS)
16. Severity criteria
18. Repetitive Oxygen desaturations �
20. OSA and cardiovascular consequences: negative thoracic pressure (1) Obstructive apneas will lower intrathoracic pressures and therefore increase transmural systolic left ventricular pressure. This will increase left ventricular afterload and compromise left ventricular functionObstructive apneas will lower intrathoracic pressures and therefore increase transmural systolic left ventricular pressure. This will increase left ventricular afterload and compromise left ventricular function
22. OSA and cardiovascular consequences: arousal reaction (2) During the apnea the reflex from pulmonary stretch receptors, that normally suppresses SNA, is interrupted leading to an increase in SNA. Hypoxia and hypercapnia also increases SNA by stimulation of the peripheral chemoreceptors and by provoking arousals.
Increased sympathetic nervous system activity, a cardinal
feature of obstructive apnea, results from the interaction of
several excitatory mechanisms normally dormant during
sleep. During apnea, the reflex arising from pulmonary
stretch receptors that suppresses central sympathetic discharge
during normal breathing ceases, disinhibiting central
sympathetic outflow. The ensuing hypoxia and hypercapnia
further augment sympathetic activity by stimulating peripheral
and central chemoreceptors.39,40
Although arousal from sleep at the
termination of obstructive apnea facilitates the resumption
airflow by stimulating pharyngeal dilator muscles,37,42 the
resulting excitatory input from cortical centers will cause a
further burst of sympathetic outflow accompanied by a loss of
vagal tone.11,43
During the apnea the reflex from pulmonary stretch receptors, that normally suppresses SNA, is interrupted leading to an increase in SNA. Hypoxia and hypercapnia also increases SNA by stimulation of the peripheral chemoreceptors and by provoking arousals.
Increased sympathetic nervous system activity, a cardinal
feature of obstructive apnea, results from the interaction of
several excitatory mechanisms normally dormant during
sleep. During apnea, the reflex arising from pulmonary
stretch receptors that suppresses central sympathetic discharge
during normal breathing ceases, disinhibiting central
sympathetic outflow. The ensuing hypoxia and hypercapnia
further augment sympathetic activity by stimulating peripheral
and central chemoreceptors.39,40
Although arousal from sleep at the
termination of obstructive apnea facilitates the resumption
airflow by stimulating pharyngeal dilator muscles,37,42 the
resulting excitatory input from cortical centers will cause a
further burst of sympathetic outflow accompanied by a loss of
vagal tone.11,43
23. OSA and cardiovascular consequences: myocardial ischemia (3) During the apnea the reflex from pulmonary stretch receptors, that normally suppresses SNA, is interrupted leading to an increase in SNA. Hypoxia and hypercapnia also increases SNA by stimulation of the peripheral chemoreceptors and by provoking arousals.
Increased sympathetic nervous system activity, a cardinal
feature of obstructive apnea, results from the interaction of
several excitatory mechanisms normally dormant during
sleep. During apnea, the reflex arising from pulmonary
stretch receptors that suppresses central sympathetic discharge
during normal breathing ceases, disinhibiting central
sympathetic outflow. The ensuing hypoxia and hypercapnia
further augment sympathetic activity by stimulating peripheral
and central chemoreceptors.39,40
Although arousal from sleep at the
termination of obstructive apnea facilitates the resumption
airflow by stimulating pharyngeal dilator muscles,37,42 the
resulting excitatory input from cortical centers will cause a
further burst of sympathetic outflow accompanied by a loss of
vagal tone.11,43
During the apnea the reflex from pulmonary stretch receptors, that normally suppresses SNA, is interrupted leading to an increase in SNA. Hypoxia and hypercapnia also increases SNA by stimulation of the peripheral chemoreceptors and by provoking arousals.
Increased sympathetic nervous system activity, a cardinal
feature of obstructive apnea, results from the interaction of
several excitatory mechanisms normally dormant during
sleep. During apnea, the reflex arising from pulmonary
stretch receptors that suppresses central sympathetic discharge
during normal breathing ceases, disinhibiting central
sympathetic outflow. The ensuing hypoxia and hypercapnia
further augment sympathetic activity by stimulating peripheral
and central chemoreceptors.39,40
Although arousal from sleep at the
termination of obstructive apnea facilitates the resumption
airflow by stimulating pharyngeal dilator muscles,37,42 the
resulting excitatory input from cortical centers will cause a
further burst of sympathetic outflow accompanied by a loss of
vagal tone.11,43
24. OSA: inhibition lung stretch receptors (4) During the apnea the reflex from pulmonary stretch receptors, that normally suppresses SNA, is interrupted leading to an increase in SNA. Hypoxia and hypercapnia also increases SNA by stimulation of the peripheral chemoreceptors and by provoking arousals.
Increased sympathetic nervous system activity, a cardinal
feature of obstructive apnea, results from the interaction of
several excitatory mechanisms normally dormant during
sleep. During apnea, the reflex arising from pulmonary
stretch receptors that suppresses central sympathetic discharge
during normal breathing ceases, disinhibiting central
sympathetic outflow. The ensuing hypoxia and hypercapnia
further augment sympathetic activity by stimulating peripheral
and central chemoreceptors.39,40
Although arousal from sleep at the
termination of obstructive apnea facilitates the resumption
airflow by stimulating pharyngeal dilator muscles,37,42 the
resulting excitatory input from cortical centers will cause a
further burst of sympathetic outflow accompanied by a loss of
vagal tone.11,43
During the apnea the reflex from pulmonary stretch receptors, that normally suppresses SNA, is interrupted leading to an increase in SNA. Hypoxia and hypercapnia also increases SNA by stimulation of the peripheral chemoreceptors and by provoking arousals.
Increased sympathetic nervous system activity, a cardinal
feature of obstructive apnea, results from the interaction of
several excitatory mechanisms normally dormant during
sleep. During apnea, the reflex arising from pulmonary
stretch receptors that suppresses central sympathetic discharge
during normal breathing ceases, disinhibiting central
sympathetic outflow. The ensuing hypoxia and hypercapnia
further augment sympathetic activity by stimulating peripheral
and central chemoreceptors.39,40
Although arousal from sleep at the
termination of obstructive apnea facilitates the resumption
airflow by stimulating pharyngeal dilator muscles,37,42 the
resulting excitatory input from cortical centers will cause a
further burst of sympathetic outflow accompanied by a loss of
vagal tone.11,43
25. Severe (O)SAS
26. Extremely severe OSAS
27. Hypoxia/reoxygenation �Alterations in energy (ATP) metabolism and oxidative stress� In response to hypoxia the aerobic production of ATP is impaired and degradation products as ADP, AMP, hypoxanthine and uric acid accumulate, indicating energy crisis. As a consequence, glycolysis is upregulated.
Concomitantly, due to hypoxia, circulating xanthine oxidase and endothelial xanthine oxidase are activated by action of proteases (xanthine dehydrogenase is converted to xanthine oxidase).
During the period of reoxygenation, the newly activated xanthine oxidases utilize the hypoxanthine and molecular oxygen to produce free radicals and oxidants as superoxide.
ROS production is amplified, namely due to the potent oxidant OH-.
Several independent studies that demonstrate increased accumulation of ATP degradation products in OSA patients are consistent with this mechanism:
- Findley: increase in plasma adenosine levels in OSA (3 fold increase).In response to hypoxia the aerobic production of ATP is impaired and degradation products as ADP, AMP, hypoxanthine and uric acid accumulate, indicating energy crisis. As a consequence, glycolysis is upregulated.
Concomitantly, due to hypoxia, circulating xanthine oxidase and endothelial xanthine oxidase are activated by action of proteases (xanthine dehydrogenase is converted to xanthine oxidase).
During the period of reoxygenation, the newly activated xanthine oxidases utilize the hypoxanthine and molecular oxygen to produce free radicals and oxidants as superoxide.
ROS production is amplified, namely due to the potent oxidant OH-.
Several independent studies that demonstrate increased accumulation of ATP degradation products in OSA patients are consistent with this mechanism:
- Findley: increase in plasma adenosine levels in OSA (3 fold increase).
28. As you know three models have been proposed to explain the pathophysiology of UAC:
As you know different mechanisms are possible to explain the pathophysiology of UAC and each mechanism has its place, but no one is able to fully explain UAC. Therefore it is important to keep in mind a potential influence of all these mechanisms.
The mechanisms leading to upper airway collapse can be put in 3 different models:
1) The oldest model explains UAC by the occurrence of an anatomic abnormality which causes structural narrowing,
(but there are more than enough arguments against an important role for this model: Cephalometric variables and BMI only explain 33% of the variance of AHI and the UAC can occur at different sites.)
2) In the balance of forces theory UAC occurs due to an imbalance between activation of diaphragm and upper airway muscle activity
Impaired reflex activation of upper airway dilator muscle activity
3) In the third model the upper airway is considered as a rigid tube with a flexible segment which behaves like a Starling resistor.
When we want to evaluate the upper airway, we have to keep in mind a potential influence of all these measurements.
As you know three models have been proposed to explain the pathophysiology of UAC:
As you know different mechanisms are possible to explain the pathophysiology of UAC and each mechanism has its place, but no one is able to fully explain UAC. Therefore it is important to keep in mind a potential influence of all these mechanisms.
The mechanisms leading to upper airway collapse can be put in 3 different models:
1) The oldest model explains UAC by the occurrence of an anatomic abnormality which causes structural narrowing,
(but there are more than enough arguments against an important role for this model: Cephalometric variables and BMI only explain 33% of the variance of AHI and the UAC can occur at different sites.)
2) In the balance of forces theory UAC occurs due to an imbalance between activation of diaphragm and upper airway muscle activity
Impaired reflex activation of upper airway dilator muscle activity
3) In the third model the upper airway is considered as a rigid tube with a flexible segment which behaves like a Starling resistor.
When we want to evaluate the upper airway, we have to keep in mind a potential influence of all these measurements.
29. outlines Snoring
Obstructive sleep apnea (OSA)
Central sleep apnea (CSAS)
Cheyne-Stokes respiration (CSR)
UARS
Hypoventilation
Nocturnal dyspnea DD
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking,
…
30. Spectrum of sleep-disordered breathing
31. Pathogenesis of SDB �Mechanisms of unstable breathing ? drive occurs as part of the breathing instability that can be caused by several mechanisms:
? ‘wakefulness drive’, breathing becomes dependent of feedback control mechanisms
Depressed central drive & defective effector organs (respiratory muscles/thoracic wall)
… So inspiratory drive is linked by this mechanism to upper airway collapse
Drive may decrease due to lower central drive or defective effector organs
So inspiratory drive is linked by this mechanism to upper airway collapse
Drive may decrease due to lower central drive or defective effector organs
32. Mechanisms of unstable breathing ? drive occurs as part of the breathing instability that can be caused by several mechanisms:
…
? O2 (HVR) and CO2 drive (HCVR)
Unmasking of CO2 threshold
Stage effects and arousals
Upper airway reflexes So inspiratory drive is linked by this mechanism to upper airway collapse
Drive may decrease due to lower central drive or defective effector organs
So inspiratory drive is linked by this mechanism to upper airway collapse
Drive may decrease due to lower central drive or defective effector organs
33. Central sleep apnea occurs in 2 categories Normocapnia or hypocapnia: normal CO2 drive
Idiopathic or Cheyne-Stokes breathing
PB at high altitude
Acromegaly
Intracranial hypertension
Congestive heart failure
Chronic renal failure
Use of opioids
Hypercapnia: reduced CO2 drive Sleep hypoventilation syndrome
Idiopathic or secondary alveolar hypoventilation
Neuromuscular disorders
Brainstem dysfunction
Musculoskeletal disorders
35. CSR-CSA
37. Clinical picture Normocapnic central sleep apnea
symptoms similar to OSA
frequent nocturnal awakenings and insomnia Hypercapnic central sleep apnea
polycythemia, cor pulmonale, peripheral edema, muscle weakness, morning headache, snoring, equal M/F ratio
38. Hypoxia and hypercapnia related with the apnea can lead to arousal, stimulation of CR and thus increased SNA. The increased SNA can give a higher heart rate and rise in blood pressureHypoxia and hypercapnia related with the apnea can lead to arousal, stimulation of CR and thus increased SNA. The increased SNA can give a higher heart rate and rise in blood pressure
39. Hypoxia and hypercapnia related with the apnea can lead to arousal, stimulation of CR and thus increased SNA. The increased SNA can give a higher heart rate and rise in blood pressureHypoxia and hypercapnia related with the apnea can lead to arousal, stimulation of CR and thus increased SNA. The increased SNA can give a higher heart rate and rise in blood pressure
40. Cheyne-Stokes breathing
41. CSR �Cycle length and circulation time
42. Central Sleep Apnea
43. CSR and deterioration of heart function Changes in cycle length and apnea length
45. outlines Snoring
Obstructive sleep apnea (OSA)
Central sleep apnea (CSAS)
Cheyne-Stokes respiration (CSR)
UARS
Hypoventilation
Nocturnal dyspnea DD
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking,
…
46. A – Excessive Daytime Sleepiness
or B – At least two of the following items
Nocturnal gasping or breathing arrests
Frequent awakenings
Non restorative sleep
Chronic fatigue
Loss of concentration
and C - > 5 obstructive events / hour (A, H, RERA’s) As you know, SDB is characterized by the presence of: ….. The minimal criteria to define OSAS are based on the Chicago criteria.
There are however patients who demonstrate an AHI<5 and have the same complaints. In these patients UARS can be considerd.
As you know, SDB is characterized by the presence of: ….. The minimal criteria to define OSAS are based on the Chicago criteria.
There are however patients who demonstrate an AHI<5 and have the same complaints. In these patients UARS can be considerd.
47. UARS� A disease which is characterized by chronic sleepiness and daytime somnolence in the absence of frank apneas/hypopneas.
EDS unexplained by another cause and associated with more than 50% of respiratory events that are non apneic and non hypopneic
? more subtle changes in breathing pattern
50. A – Pattern of progressively negative oesophageal pressure terminated by a sudden return to normal, associated with a micro-arousal
and
B – Duration of >10 seconds
Requires the use of an oesophageal catheter
Alternatives : nasal canula (IFL detection) and PTT In the new definitions of UARS RERA’s are implemented, which are characterized by …In the new definitions of UARS RERA’s are implemented, which are characterized by …
51. UARS: most typical features
53. �Flow limitation Flattening index: mean of flow-limitation of the 5 previous breaths:
0.30: patent airway
0.20-0.30: normal breath
0.10-0.15: flow limitation
0.05-0.10: severe flow limitation
0.00: closed airway
55. outlines Snoring
Obstructive sleep apnea (OSA)
Central sleep apnea (CSAS)
Cheyne-Stokes respiration (CSR)
UARS
Hypoventilation
Nocturnal dyspnea DD
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking,
…
56. HYPOVENTILATION
57. HYPOVENTILATION �
58. HYPOVENTILATION �MANY DEFINITIONS Nocturnal oxygen desaturation:
SaO2 ? 4% 10%
Nocturnal hypoxemia:
(ICSD-2)
- SaO2 <90% >30% TIB
- SaO2 <90% > 5 min ; nadir <85% AASM Task Force:
One or more of the following: cor pulmonale, PHT, EDS, polycythemia, PaCO2>45 mmHg
Overnight monitoring: one or both of the following
An increase in PaCO2 during sleep >10 mmHg from awake supine values
Oxygen desaturation during sleep not explained by apnea or hypopnea events.
60. �Hypoventilation�(Chronic) Respiratory Failure COPD
Restrictive disorders:
Musculoskeletal Disorders
Neuromuscular disorders
Obesity
Central Alveolar Hypoventilation Syndrome
62. Changes in FRC during sleep in normals (? V/Q mismatch)
63. Ventilatory changes during sleep in COPD�Chadwick (MD thesis)1989
64. Ventilatory patterns in chronic lung disease COPD and asthma:
significant ?TV during sleep
with little change in breath frequency
Overall, MV falls during sleep. Interstitial lung disease:
Significant ? freq
?TV
MV is not significantly lower during sleep.
The change in breathing pattern during sleep in ILD:
suggests that the rapid shallow breathing pattern that is characteristic of these patients may in part be a conscious behaviour.
65. HYPOVENTILATION IN SLEEP IN COPD MECHANISMS NON-REM
? ? ? Wakefulness drive
Position on O2-Hb-dissociation curve
Chemoreceptor responses ?
Respiratory muscle function ?
Hyperinflation
REM
Gamma paralysis intercostals and upper airways
Diaphragm in bad position on length tension curve
Chemoreceptor responses further ?
Arousability ?
68. outlines Snoring
Obstructive sleep apnea (OSA)
Central sleep apnea (CSAS)
Cheyne-Stokes respiration (CSR)
UARS
Hypoventilation
Nocturnal dyspnea DD
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking,
…
69. Nocturnal dyspnea attacks: �quit ? (Apnea)
COPD, asthma, pulmonary oedema
Sleep related laryngospasm
Sleep choking
Nocturnal stridor (inspiratory)
Mostly in MSA, NMD
70. In COPD: ? vagal activity
? levels of bronchoconstrictive cholinergic tone at night
NL: FEV1: -7% at 4 AM
COPD: FEV1: -27% at 4 AM
Postma. Clin Sci 1985;251.
71. � COPD and sleep apnea: �overlap syndrome
72. COPD and sleep apnea: �overlap syndrome OSAS occurs no more frequently in COPD than a similarly aged normal population.
Inadequate ventilatory drive in some patients with COPD may favour the development of OSA
Awake hypoxaemia, hypercapnia and pulmonary hypertension are more common than in either condition alone.
Patients develop more marked oxygen desaturation during apnoea because of the lower starting SaO2.
73. NOCTURNAL ASTHMA Clinical picture:
Asthma symptoms at night or early morning: wheezing/awakening
with decreases in PEFR
Is not a different condition,
but is severe asthma
Prevalence:
> 50% asthmatics sometimes
> 80% asthmatics if unstable
? normal circadian variation in airway calibre (max 4 PM, min 4 AM):
In asthmatics: 15-50% (morning dip)
Relevant dip > 20%
In normals: variability PEF 8%
Mechanisms:
Airway resistance progressively ? in asthmatics during sleep
Raw norm < 2x, NA 4x
Bellia V et al Chest 1988
Diurnal variation
in bronchomotor tone
Hetzel, Thorax 1980
in circulating hormones (cortisol, cholinergic tone, histamine, epinephrine…)
Related to PC20
74. Mechanisms of Nocturnal Asthma
76. Nocturnal asthma and OSAS: “overlap syndrome” ? Yigla et al. J Asthma 2003
22 consecutive patients with severe unstable asthma
14 on continuous oral CS (for a mean of 9?3 y)
8 on intermittent use of oral CS
Polysomnography regardless of sleep symptoms
All but one patient had OSA (mean AHI 18?3)
Prevalence OSA 95.5%
AHI significantly higher in the continuous CS group (21?3 vs. 11?2, p < 0.05].
The study group had above normal NC and BMI
77. NOCTURNAL DYSPNEA �Pulmonary oedema Usually associated with a history of heart disease, chest pain, cardiomegaly and typical radiographic features
78. NOCTURNAL DYSPNEA � Sleep related laryngospasm
Related to acid reflux in the distal part of the oesophagus
Reflex mechanism leading to spasm of the vocal cords
Occurs in the middle of the night
Severe dyspnea, suffocation, palpitations, anxiety; suffer agony
Duration: 30 to 60 seconds ?? quicker relief after apnea
R/ PPI Sleep choking
Related to stress
Always in the beginning of sleep (within a few minutes after falling asleep)
R/ relaxation, information, reassurance
DD apnea
79. Varia: Expiratory vocalization Sharp, intense noise during expiration
Episodic bradypneas CA
Prolonged expiration (narrowed glottis)
Mostly during REM (93% of all events)
No underlying NMD
80. Varia: Expiratory vocalization�Treatment disappointing BE= bradypneic episodesBE= bradypneic episodes
81. Conclusions Sleep disordered breathing has a broad spectrum from simple snoring over UARS and sleep apnea to hypoventilation syndrome.
Different clinical features in each entity
Nocturnal symptoms in asthma and COPD are characteristic for severe disease.
Coexistence of astma/COPD and sleep apnea.
Be aware of less common causes of nocturnal dyspnea.
