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Pulmonology 3
Sleep disorders
Attilio Boner
University of Verona, Italy
attilio.boner@univr.it
WHAT YOU SOULD HAVE READ BUT ………………… 2018
Sleep Physiology
 Telomeres are repetitive DNA sequences
(in humans, TTAGGGn) and associated
proteins that cap the end of chromosomes.
 With each cycle of chromosomal replication
and cellular division, the telomere becomes
shorter, except in specialized cells
expressing telomerase.
 This means that telomere length gradually
decreases with age in most cells.
 Difficult life experiences may be associated with an accelerated rate
of telomere attrition.
Sleep Duration and Telomere Length in Children
S James, J Pediatr. 2017;187:247-252
Sleep Duration and Telomere Length in Children
S James, J Pediatr. 2017;187:247-252
 Inadequate nightly sleep duration is linked to morbidities and mortality, as
well as a number of physiological sequelae, including inflammation,
oxidative stress, increased sympathetic tone, and neuroendocrine
dysregulation.
 Short sleep duration in childhood is associated with changes
in hypothalamic–pituitary–adrenocortical system activity,
autonomic nervous system activity, and metabolic regulation.
 This type of stress-altered hypothalamic–pituitary–adrenocortical activity
is known to correlate with telomere length.
Sleep Duration and Telomere Length in Children
S James, J Pediatr. 2017;187:247-252
Distribution of children's hours of sleep
at 9 years of age in the analytic sample
 Data for 1567 children
from a population-based
birth cohort of children
born between 1998 and
2000.
 Telomere length using
quantitative polymerase
chain reaction.
 Data for 1567 children
from a population-based
birth cohort of children
born between 1998 and
2000.
 Telomere length using
quantitative polymerase
chain reaction.
Sleep Duration and Telomere Length in Children
S James, J Pediatr. 2017;187:247-252
• Children with shorter sleep
durations have shorter telomeres
than children with longer sleep
durations.
• Each hour less of nightly sleep
duration is associated with having
telomeres that are 0.015 log-
kilobases per chromosome shorter
(P < 0.05).
 Data for 1567 children
from a population-based
birth cohort of children
born between 1998 and
2000.
 Telomere length using
quantitative polymerase
chain reaction.
Sleep Duration and Telomere Length in Children
S James, J Pediatr. 2017;187:247-252
• Children with shorter sleep
durations have shorter telomeres
than children with longer sleep
durations.
• Each hour less of nightly sleep
duration is associated with having
telomeres that are 0.015 log-
kilobases per chromosome shorter
(P < 0.05).
That suboptimal
sleep duration is a
risk for increased
physiological stress
and impaired health.
Sleep Duration and Telomere Length in Children
S James, J Pediatr. 2017;187:247-252
 The biological mechanism by which sleep duration becomes linked to
telomere length in children, may be:
• telomere erosion (eg, owing to oxidative stress)
• suppression of telomerase activity
• hypothalamic–pituitary–adrenal axis activation,
• inflammation,
• oxidation.
Sleep education
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
 Cross-sectional study with
bedroom electronic devices
(EDs) placement and
parental restriction
reported by parents.
 Relationship between
school readiness
and ED placement.
 556 young children
attending the 3° year
of kindergarten.
% parents placing at least one electronic
devices in their children’s bedroom
30%
30 –
25 –
20 –
15 –
10 –
05 –
00 –
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
 Cross-sectional study with
bedroom electronic devices
(EDs) placement and
parental restriction
reported by parents.
 Relationship between
school readiness
and ED placement.
 556 young children
attending the 3° year
of kindergarten.
% parents placing at least one electronic
devices in their children’s bedroom
30%
30 –
25 –
20 –
15 –
10 –
05 –
00 –
Placement of television in the bedroom
was associated with
lower overall school readiness
and
the placement of game console with
lower social competence
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
 Cross-sectional study with
bedroom electronic devices
(EDs) placement and
parental restriction
reported by parents.
 Relationship between
school readiness
and ED placement.
 556 young children
attending the 3° year
of kindergarten.
% parents placing at least one electronic
devices in their children’s bedroom
30%
30 –
25 –
20 –
15 –
10 –
05 –
00 –
Such harmful effect was more
prominent among lower
socioeconomic status families
School readiness
• School readiness is an indicator of whether a child possesses the
cognitive, social and emotional skills necessary for success in school
and has been shown to predict
long-term educational outcomes.
Forget-Dubois N,
Early Educ Dev 2007;18:405–26
Silburn SR,
Early Hum Dev 2007;83:S125
• School readiness was measured
using the Early Development
Instrument (EDI), a comprehensive
teacher-rated scale.
Janus M, Can J Behav Sci 2007;39:1–22
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
Effect of bedroom electronic device (ED) placement on school readiness moderated
by family socioeconomic status (SES)
P<0.05
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
Effect of bedroom ED placement on school readiness moderated by parental restriction
P<0.001
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
Effect of bedroom ED placement on school readiness moderated by parental restriction
P<0.001
Parental restriction reduces the harmful effects
of in-bedroom electronic devices
King-wa Fu, Arch Dis Child. 2017;102:1125-1131
ED placement in
children’s bedroom was
associated with lower
school readiness,
particularly among lower
SES families.
Parental restriction
might help
to alleviate the harm.
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Importance:
Although multiple cross-sectional and longitudinal
studies have established that sleep problems and
behavioral difficulties are associated in children,
the directionality of this association and whether
sleep problems are differentially associated with
different types of childhood behavioral difficulties
are unclear. Understanding these associations will
inform the focus and timing of interventions.
Objective:
To determine whether longitudinal and reciprocal associations exist between child
sleep problems and externalizing, internalizing, or both behavioral difficulties.
Prospective cohort study using
nationally representative data
from 5 waves
2004 (4983 children mean age of 4.7 ),
2006,
2008,
2010, and
2012)
kindergarten cohort
(4983 children aged
4-5 years in 2004)
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Sleep problems were defined using
parent-reported child sleep problem
severity and specific difficulties:
1. difficulty getting to sleep at night,
2. not happy sleeping alone,
3. waking during the night,
4. restless sleep
on 4 or more nights of the week.
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Child behavioral difficulties using the
parent-reported Strengths and
Difficulties Questionnaire for
1. externalizing difficulties
(conduct problems and
hyperactivity/inattention subscales)
and
2. internalizing difficulties
(emotional problems subscale).
Prospective cohort study using
nationally representative data
from 5 waves
2004 (4983 children mean age of 4.7 ),
2006,
2008,
2010, and
2012)
kindergarten cohort
(4983 children aged
4-5 years in 2004)
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Prospective cohort study using
nationally representative data
from 5 waves
2004 (4983 children mean age of 4.7 ),
2006,
2008,
2010, and
2012)
kindergarten cohort
(4983 children aged
4-5 years in 2004)
Significant bidirectional associations
were detected between sleep
problems and externalizing
difficulties during the elementary
school transition period,
with
greater sleep problems
associated with
later externalizing
behavior
and vice versa
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Prospective cohort study using
nationally representative data
from 5 waves
2004 (4983 children mean age of 4.7 ),
2006,
2008,
2010, and
2012)
kindergarten cohort
(4983 children aged
4-5 years in 2004)
Although sleep was a significant
driver of later internalizing
difficulties,
the reverse association
was not significant.
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Prospective cohort study using
nationally representative data
from 5 waves
2004 (4983 children mean age of 4.7 ),
2006,
2008,
2010, and
2012)
kindergarten cohort
(4983 children aged
4-5 years in 2004)
Conclusions and Relevance:
These results suggest that future
studies should investigate whether
implementing sleep problem
intervention decreases the
occurrence of both externalizing and
internalizing difficulties.
Interventions targeting
externalizing, but not internalizing,
difficulties may benefit childhood
sleep
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
Bidirectional Associations Between Child Sleep Problems
and Internalizing and Externalizing Difficulties
from Preschool to Early Adolescence.
Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
•Sleep-
Disordered
Breathing
General
considerations
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
The present statement was produced by a European Respiratory Society
Task Force to summarise the evidence and current practice on the diagnosis
and management of obstructive sleep disordered breathing (SDB) in children
aged 1-23 months.
A systematic literature search was completed and 159 articles were
summarised to answer clinically relevant questions.
SDB is suspected when symptoms or abnormalities related to upper airway
obstruction are identified.
Morbidity (pulmonary hypertension, growth delay, behavioural problems) and
coexisting conditions (feeding difficulties, recurrent otitis media) may be
present. SDB severity is measured objectively, preferably by
polysomnography, or alternatively polygraphy or nocturnal oximetry.
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
Children with apparent upper airway obstruction during wakefulness, those
with abnormal sleep study in combination with SDB symptoms (e.g. snoring)
and/or conditions predisposing to SDB (e.g. mandibular hypoplasia) as well as
children with SDB and complex conditions (e.g. Down syndrome, Prader-Willi
syndrome) will benefit from treatment.
Adenotonsillectomy and continuous positive airway pressure are the most
frequently used treatment measures along with interventions targeting
specific conditions (e.g. supraglottoplasty for laryngomalacia or
nasopharyngeal airway for mandibular hypoplasia).
Hence, obstructive SDB in children aged 1-23 months is a multifactorial
disorder that requires objective assessment and treatment of all underlying
abnormalities that contribute to upper airway obstruction during sleep.
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
•American Thoracic Society. Standards and indications for cardiopulmonary sleep studies in
children. Am J Respir Crit Care Med 1996; 153: 866–878.
•Dayyat E, Kheirandish-Gozal L, Gozal D. Childhood obstructive sleep apnea: one or two
distinct disease entities? Sleep Med Clin 2007; 2: 433–444.
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
A stepwise approach to the management of obstructive sleep disordered breathing
in 1- to 23-month-old children
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
A stepwise approach to the management of obstructive sleep disordered breathing
in 1- to 23-month-old children
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
A stepwise approach to the management of obstructive sleep disordered breathing
in 1- to 23-month-old children
ERS statement on obstructive sleep disordered breathing
in 1- to 23-month-old children.
Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
FIGURE 1 A stepwise approach to the management of obstructive sleep disordered breathing
in 1- to 23-month-old children reflecting the Task Force members’ current practice.
This scheme is not intended as a recommendation for clinicians.
OSAS: obstructive sleep apnoea syndrome;
ALTE: apparent life-threatening event;
GOR: gastro-oesophageal reflux;
ENT: ear, nose and throat;
PSG: polysomnography;
AHI: apnoea–hypopnoea index;
UAO: upper airway obstruction;
CPAP: continuous positive airway pressure;
NPPV: non-invasive positive pressure ventilation;
nCPAP: nasal CPAP.
Allergic sensitization and objective measures of sleep
in urban school-aged children with asthma
CA Esteban, Ann Allergy Asthma Immunol 2017;119:238-245
Background
• Allergic sensitization is associated with increased child asthma morbidity
and decreased pulmonary function.
• Nocturnal symptoms and/or awakenings typically are measured
by self-report from diary data, whereas objective assessments
of sleep in child asthma studies are lacking.
Objective
• To investigate the association between increased allergic sensitization
(number of positive allergy test results measured by SPTs or sIgE)
and sleep outcomes (sleep efficiency, sleep duration,
and mean number of awakenings measured by actigraphy)
in urban schoolchildren with persistent asthma.
 196 children with
persistent asthma
(7–9 years old).
 Sleep outcomes were
measured with a wrist
Actiwatch during a
1-month period in the
fall and winter seasons.
Allergic sensitization and objective measures of sleep
in urban school-aged children with asthma
CA Esteban, Ann Allergy Asthma Immunol 2017;119:238-245
• Children with more positive test
results experienced:
• less efficient sleep.
• more night awakenings. P=0.05.
Allergic sensitization and objective measures of sleep
in urban school-aged children with asthma
CA Esteban, Ann Allergy Asthma Immunol 2017;119:238-245
Number of positive allergy test results and variability in sleep efficiency
by variability in FEV1 (median split).
For children above the median FEV1 value of variability, more allergy tests were associated with more variability in sleep efficiency
(b = .38, P = .00, R2 adjusted = 0.13). In contrast, for children below the median (less variability in FEV1),
there was no significant association between number of positive allergy test results and variability in sleep
 42 obese adolescents with the
obstructive sleep apnoea
syndrome (OSAS) and
37 weight-matched controls.
 Upper airway MRI,
measurements of upper airway
critical closing pressure (Pcrit),
genioglossal electromyography
and ventilatory response to
CO2 during wakefulness and
sleep.
• Adenotonsillar volume (ATV),
• nasopharyngeal airway volume
(NPAV),
• activated and hypotonic upper
airway critical closing pressure
(Pcrit),
• genioglossal electromyography
• ventilatory response to CO2
during sleep
were all associated
with OSAS risk.
The obstructive sleep apnoea syndrome in adolescents
Marcus CL, Thorax 2017;72:720–728
 42 obese adolescents with the
obstructive sleep apnoea
syndrome (OSAS) and
37 weight-matched controls.
 Upper airway MRI,
measurements of upper airway
critical closing pressure (Pcrit),
genioglossal electromyography
and ventilatory response to
CO2 during wakefulness and
sleep.
• Adenotonsillar volume (ATV),
• nasopharyngeal airway volume
(NPAV),
• activated and hypotonic upper
airway critical closing pressure
(Pcrit),
• genioglossal electromyography
• ventilatory response to CO2
during sleep
were all associated
with OSAS risk.
The obstructive sleep apnoea syndrome in adolescents
Marcus CL, Thorax 2017;72:720–728
OSAS in adolescents
is mediated by a
combination of anatomic
(ATV, NPAV) and
neuromotor factors
(activated Pcrit).
The obstructive sleep apnoea syndrome in adolescents
Marcus CL, Thorax 2017;72:720–728
3D plots of the predicted probability (Pr) of
obstructive sleep apnoea syndrome (OSAS)
High predicted probabilities of OSAS are
shown in red, probabilities around 0.5 in grey
and low predicted probabilities in blue
Nasopharyngeal airway volume (NPAV)
 42 obese adolescents with the
obstructive sleep apnoea
syndrome (OSAS) and
37 weight-matched controls.
 Upper airway MRI,
measurements of upper airway
critical closing pressure (Pcrit),
genioglossal electromyography
and ventilatory response to
CO2 during wakefulness and
sleep.
The obstructive sleep apnoea syndrome in adolescents
Marcus CL, Thorax 2017;72:720–728
3D plots of the predicted probability (Pr) of
obstructive sleep apnoea syndrome (OSAS)
High predicted probabilities of OSAS are
shown in red, probabilities around 0.5 in grey
and low predicted probabilities in blue
Activated critical closing pressure (Pcrit)
 42 obese adolescents with the
obstructive sleep apnoea
syndrome (OSAS) and
37 weight-matched controls.
 Upper airway MRI,
measurements of upper airway
critical closing pressure (Pcrit),
genioglossal electromyography
and ventilatory response to
CO2 during wakefulness and
sleep.
The obstructive sleep apnoea syndrome in adolescents
Marcus CL, Thorax 2017;72:720–728
High predicted probabilities of OSAS are
shown in red, probabilities around 0.5 in grey
and low predicted probabilities in blue
Nasopharyngeal airway volume (NPAV)
3D plots of the predicted probability (Pr) of
obstructive sleep apnoea syndrome (OSAS)
 42 obese adolescents with the
obstructive sleep apnoea
syndrome (OSAS) and
37 weight-matched controls.
 Upper airway MRI,
measurements of upper airway
critical closing pressure (Pcrit),
genioglossal electromyography
and ventilatory response to
CO2 during wakefulness and
sleep.
•Sleep-
Disordered
Breathing
Diagnosis
questionnaires
•Sleep-
Disordered
Breathing
Diagnosis
polisonnigraphy
Nocturnal Oximetry-based Evaluation of Habitually
Snoring Children.
Hornero R, Am J Respir Crit Care Med. 2017;196(12):1591-1598.
RATIONALE:
The vast majority of children around the world undergoing
adenotonsillectomy for obstructive sleep apnea-hypopnea syndrome
(OSA) are not objectively diagnosed by nocturnal polysomnography
because of access availability and cost issues.
Automated analysis of nocturnal oximetry (nSpO2), which is readily and
globally available, could potentially provide a reliable and convenient
diagnostic approach for pediatric OSA.
Nocturnal Oximetry-based Evaluation of Habitually
Snoring Children.
Hornero R, Am J Respir Crit Care Med. 2017;196(12):1591-1598.
Deidentified nocturnal
oximetry (nSpO2 ) recordings
from a total of 4,191 children
originating from 13 pediatric
sleep laboratories
prospectively evaluated after
developing and validating an
automated neural network
algorithm using an initial set
of single-channel nSpO2
recordings from 589 patients
referred for suspected OSA.
The automatically estimated
apnea-hypopnea index (AHI)
showed high agreement with
AHI from conventional
polysomnography
(intraclass correlation coefficient, 0.785)
when tested in 3,602 additional
subjects.
Nocturnal Oximetry-based Evaluation of Habitually
Snoring Children.
Hornero R, Am J Respir Crit Care Med. 2017;196(12):1591-1598.
Deidentified nocturnal
oximetry (nSpO2 ) recordings
from a total of 4,191 children
originating from 13 pediatric
sleep laboratories
prospectively evaluated after
developing and validating an
automated neural network
algorithm using an initial set
of single-channel nSpO2
recordings from 589 patients
referred for suspected OSA.
the widely used AHI cutoff points
of 1, 5, and 10 events/h revealed
an incremental diagnostic ability
(75.2, 81.7, and 90.2% accuracy;
0.788, 0.854, and 0.913 area under
the receiver operating
characteristic curve,
respectively).
Machines Learning to Detect Obstructive Sleep Apnea
in Children. Are We There Yet? Editorial
Combs D, Am J Respir Crit Care Med. 2017;196(12):1506-1507.
•In this issue of the Journal, Hornero and colleagues (pp. 1591–1598) take a
new approach to nocturnal pulse oximetry screening tool.
•Specifically, they used an innovative approach of machine learning to
generate a neural network algorithm to detect OSA from overnight pulse
oximetry tracings.
•Most prior attempts involved manual interpretation
of nocturnal pulse oximetry as a screening tool
for OSA.
•Such a machine learning approach enabled the
authors to evaluate thousands of potential
algorithms to optimize a screening algorithm.
•On the basis of their results, the authors suggest a diagnostic protocol
for applying this tool in clinical practice.
•Children with an estimated AHI lower than 1 based on overnight pulse
oximetry are unlikely to have moderate or severe sleep apnea and may
not require polysomnography.
•Children with a machine-estimated AHI of 5 or more per hour are likely to
have at least mild OSA by polysomnography (AHI >1), and could be referred
to treatment directly without undergoing polysomnography.
•Children with a machine-estimated AHI of 1–5 per hour would be considered
indeterminate and can be referred for polysomnography.
•Based on the author’s findings, approximately 1 in 20 children would be
incorrectly diagnosed with OSA and potentially treated unnecessarily.
Machines Learning to Detect Obstructive Sleep Apnea
in Children. Are We There Yet? Editorial
Combs D, Am J Respir Crit Care Med. 2017;196(12):1506-1507.
•Sleep-
Disordered
Breathing
Etiology
Comorbidities
And
Risk factors
Asthma outcomes improve with continuous positive
airway pressure for obstructive sleep apnea
J Serrano-Pariente, Allergy 2017;72:802-812
• The mean ± SD score of
the ACQ decreased from
1.39 ± 0.91 at baseline to
1.0 ± 0.78 at 6 months
(P = 0.003).
 Continuous positive airway
pressure (CPAP).
 Asthma outcomes after
6 months of CPAP in
99 adult asthma patients
(mean age 57 years)
with OSAS.
 Asthma Control
Questionnaire (ACQ).
Asthma outcomes improve with continuous positive
airway pressure for obstructive sleep apnea
J Serrano-Pariente, Allergy 2017;72:802-812
• The mean ± SD score of
the ACQ decreased from
1.39 ± 0.91 at baseline to
1.0 ± 0.78 at 6 months
(P = 0.003).
 Continuous positive airway
pressure (CPAP).
 Asthma outcomes after
6 months of CPAP in
99 adult asthma patients
(mean age 57 years)
with OSAS.
 Asthma Control
Questionnaire (ACQ).
Asthma outcomes improve with continuous positive
airway pressure for obstructive sleep apnea
J Serrano-Pariente, Allergy 2017;72:802-812
• The mean ± SD score of
the ACQ decreased from
1.39 ± 0.91 at baseline to
1.0 ± 0.78 at 6 months
(P = 0.003).
 Continuous positive airway
pressure (CPAP).
 Asthma outcomes after
6 months of CPAP in
99 adult asthma patients
(mean age 57 years)
with OSAS.
 Asthma Control
Questionnaire (ACQ).
Asthma control
(both actual and future risk),
quality of life, and lung
function improved after
starting continuous
positive airway pressure
in asthmatics with
moderate to severe
obstructive sleep
apnea syndrome.
Asthma outcomes improve with continuous positive
airway pressure for obstructive sleep apnea
J Serrano-Pariente, Allergy 2017;72:802-812
Pre
41.4%
17.2%
Post
50 –
40 –
30 –
20 –
10 –
00 –
CPAP
% patients with
uncontrolled asthma
% patients with asthma
attacks in the 6 months
Pre
35.4%
17.2%
Post
50 –
40 –
30 –
20 –
10 –
00 –
CPAP
P=0.006
P=0.015
Asthma outcomes improve with continuous positive
airway pressure for obstructive sleep apnea
J Serrano-Pariente, Allergy 2017;72:802-812
Number of patients with well-controlled asthma (ACQ score ≤ 0.75)
and not well-controlled asthma (ACQ score ≥ 1.5) after starting
continuous positive airway pressure
 Continuous positive airway
pressure (CPAP).
 Asthma outcomes after
6 months of CPAP in
99 adult asthma patients
(mean age 57 years)
with OSAS.
 Asthma Control
Questionnaire (ACQ).
Asthma outcomes improve with continuous positive
airway pressure for obstructive sleep apnea
J Serrano-Pariente, Allergy 2017;72:802-812
 The mechanisms by which treatment with CPAP may improve symptoms and
asthma control are multiple.
 OSAS is associated with a systemic and local inflammation of the airways, as well
as pulmonary vascular changes and release of endothelial factors (such as vascular
endothelial growth factor) with proinflammatory effects.
 The use of CPAP reduces inflammation and its mediators.
 Improvement of gastroesophageal reflux may also be accompanied by a reduction
in nocturnal asthma symptoms.
 Additionally, reduction in bronchial hyperresponsiveness produced by CPAP can be
also associated with a clinical improvement of asthma.
•Sleep-
Disordered
Breathing
Red-Ox
Epigenetic
inflammation
•Sleep-
Disordered
Breathing
Consequences
in children
•Sleep-
Disordered
Breathing
Consequences
in adults
•Sleep-
Disordered
Breathing
Treatment
adenotonsillectomy
• Although adenotonsillectomy is the first line
treatment for children with obstructive sleep apnea
syndrome (0SAS), improvement in objectively
documented outcomes is often inadequate and a substantial number
of children have residual disease, as most of them have additional
risk factors for OSAS and comorbidities.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Non-syndromic uncomplicated children
Syndromic children and children with complex
medical conditions
OSA with an AHI > 5 episodes/h Major craniofacial abnormalities
Children with cardiovascular morbidity (e.g.,
elevated blood pressure
Neurological disorders including neuromuscular
disorders and neurodisability
Children with neurological morbidity (e.g.,
excessive daytime sleepiness, hyperactivity,
inattention, academic difficulties)
Achondroplasia
Enuresis Down syndrome
Somatic growth delay or failure to thrive Prader–Willi syndrome
Obesity Mucopolysaccharidoses
Asthma
Priority Indication for adenotonsillectomy
Which Examinations Should/Could Be Performed In Children With Residual
Disease To Guide Further Treatment?
• Many children with OSAS have multiple sites of upper airway (UA)
obstruction during sleep and this may contribute to persistent OSAS
following AT.
• Possible sites of persistent UA obstruction are the region of the soft
palate, tongue base with lingual tonsillar hypertrophy, the supraglottis,
inferior turbinates, and the adenoid region with regrowth of adenoids.
• The diagnostic work-up to identify the levels of persistent UA obstruction
starts with a detailed history and flexible nasopharyngoscopy up to the
level of the larynx in the awake patient.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Which Examinations Should/Could Be Performed In Children With Residual
Disease To Guide Further Treatment?
• Sleep cine-magnetic resonance imaging (MRI) and drug induced sedation
endoscopy (DISE) were the most commonly used tools for dynamic
evaluation of the pediatric UA.
• Children with persistent OSAS had a higher percentage of lingual tonsillar
hypertrophy compared to controls (33% vs. 0%), and lingual tonsillar
hypertrophy occurred predominantly in children with Down syndrome.
• DISE might be particularly useful for the evaluation
of lingual tonsillar hypertrophy
and late-onset laryngomalacia.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Site-specific Treatment: Orthodontic Treatment
• An orthodontic treatment is indicated in children with OSAS and
craniofacial alterations such as retrusive chin, steep mandibular plane,
vertical direction of growth and a Class II malocclusion
• Oral appliances may improve UA patency during sleep by enlarging the UA,
decreasing UA collapsibility and improving UA muscle tone.
• Rapid maxillary expansion (RME) and mandibular advancement by an oral
jaw-positioning device are the available orthodontic treatment options in
the pediatric population.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Site-specific Treatment: Upper Airway Surgery
• Late-onset laryngomalacia is typically characterized by inspiratory
prolapse of prominent mucosal folds on the accessory cartilages
above the arytenoids resulting in supraglottic obstruction and has
a prevalence of 3.9% among older children with OSAS.
• Potential surgical interventions for upper airway obstruction
in children with residual OSAS include:
(i) adenoidectomy for those with regrowth of adenoids;
(ii) lingual tonsillectomy;
(iii) supraglottoplasty; and
(iv) partial midline glossectomy and tongue suspension with or without
lingual tonsillectomy.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Treatment That Alters Underlying Conditions Contributing To Osas:
Weight Loss
• There is consensus that weight loss therapy should be initiated in every
child with OSAS because of its beneficial effects on other obesity-
related complications.
Medical Treatment
• Intranasal budesonide and montelukast.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Treatment That Alters Underlying Conditions Contributing To Osas:
Myofunctional Therapy
• Mouth breathing is associated with malposition of the tongue, hypotonic
lips, and incorrect swallowing pattern and may predispose subjects to
persistent or recurrent OSAS following adenotonsillectomy.
• Myofunctional therapy consist of oropharyngeal exercises, that is,
repetitive isotonic and isometric exercises of tongue, soft palate and
lateral pharyngeal walls, increasing muscle tone throughout the upper
respiratory tract and helping to obtain correct nasal breathing habits,
speech, swallowing and chewing.
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
 Endoscopic view of lingual tonsillar
hypertrophy in a child residual OSA
following prior AT.
 Note: A complete obstruction the
UA at the level of the tongue with
the epiglottis pushed backwards
against the pharyngeal wall.
Lingual tonsillar hypertrophy
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
• Endoscopic view of supraglottic
obstruction in a child with OSA
cause by late-onset laryngomalacia.
• Note: A complete obstruction of
the glottis inlet by inspiratory
collaps of redundant
supra-arythenoidal mucosa.
Late-onset laryngomalacia
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Proposed algorithm for the management of persistent OSAS post-AT (part1)
Adenotonsillectomy to treat obstructive sleep apnea:
Is it enough?
A Boudewyns, Pediatr Pulmonol 2017;52:699-709
Proposed algorithm for the management of persistent OSAS post-AT (part2)
Adenotonsillotomy Versus Adenotonsillectomy
in Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
• An important risk factor for OSA in children
is adenotonsillar hypertrophy.
• Adenotonsillectomy (ATE) is considered first-line
treatment and is one of the most common surgical
procedures throughout the world.
• ATE is an effective treatment of pediatric OSA but has the
disadvantages of risk of postoperative hemorrhage and pain.
• In recent decades, partial tonsillectomy, or adenotonsillotomy
(ATT), with subtotal removal of the tonsils, has gained
popularity because it is associated with less postoperative
hemorrhage and pain.
Adenotonsillotomy Versus Adenotonsillectomy in
Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
 79 children, aged 2
to 6 years, with OSA
(Apnea-Hypopnea
Index [AHI] 5-30).
 Randomized to
adenotonsillotomy
(ATT) (n = 40)
or adenotonsillectomy
(ATE) (n = 39).
 Polysomnography
and questionnaire
at baseline and
1 year postsurgery.
12.7
BEFORE
Apnea-Hypopnea Index (median)
20 –
15 –
10 –
05 -
00
15.8
2.0
4.0
BEFOREAFTER AFTER
ATE ATT
Adenotonsillotomy Versus Adenotonsillectomy in
Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
 79 children, aged 2
to 6 years, with OSA
(Apnea-Hypopnea
Index [AHI] 5-30).
 Randomized to
adenotonsillotomy
(ATT) (n = 40)
or adenotonsillectomy
(ATE) (n = 39).
 Polysomnography
and questionnaire
at baseline and
1 year postsurgery.
12.7
BEFORE
Apnea-Hypopnea Index (median)
20 –
15 –
10 –
05 -
00
15.8
2.0
4.0
BEFOREAFTER AFTER
ATE ATT
For both groups,
significant
improvements of PSG
and OSA-18
questionnaire outcomes
were observed,
with no significant
differences
between groups.
Adenotonsillotomy Versus Adenotonsillectomy in
Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
 79 children, aged 2
to 6 years, with OSA
(Apnea-Hypopnea
Index [AHI] 5-30).
 Randomized to
adenotonsillotomy
(ATT) (n = 40)
or adenotonsillectomy
(ATE) (n = 39).
 Polysomnography
and questionnaire
at baseline and
1 year postsurgery.
12.7
BEFORE
Apnea-Hypopnea Index (median)
20 –
15 –
10 –
05 -
00
15.8
2.0
4.0
BEFOREAFTER AFTER
ATE ATT
5 children (13%) in the
ATT group needed
repeated surgery for
tonsil regrowth
and recurrence of OSA.
Adenotonsillotomy Versus Adenotonsillectomy in
Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
 79 children, aged 2
to 6 years, with OSA
(Apnea-Hypopnea
Index [AHI] 5-30).
 Randomized to
adenotonsillotomy
(ATT) (n = 40)
or adenotonsillectomy
(ATE) (n = 39).
 Polysomnography
and questionnaire
at baseline and
1 year postsurgery.
12.7
BEFORE
Apnea-Hypopnea Index (median)
20 –
15 –
10 –
05 -
00
15.8
2.0
4.0
BEFOREAFTER AFTER
ATE ATT
• The results suggest that
ATT is noninferior to
ATE in treating pediatric
OSA regarding PSG
outcomes after 1 year.
• However, after ATT,
there is a nonnegligible
risk of recurrence of
OSA.
Boxplots and lines showing the AHI 1 (before surgical intervention)
and AHI 2 (after surgical intervention)
Adenotonsillotomy Versus Adenotonsillectomy
in Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
Adenotonsillotomy Versus Adenotonsillectomy
in Pediatric Obstructive Sleep Apnea: An RCT
Borgström A, Pediatrics 2017;139:e20163314
Tonsil regrowth and recurrence of OSA are known
disadvantages after ATT, and 13% of the children
in the ATT group underwent repeated tonsil surgery
within the follow-up period.
A recent Swedish study based on >28 000 children reported a 7 times
higher risk of reoperation after TT than after TE, with the difference most
markedly among the youngest children.
In our study, the children undergoing reoperation were also among the
youngest (median age 32 months).
Predicting the effect of treatment in paediatric OSA
by clinical examination and functional respiratory imaging
M Slaats, Pediatr Pulmonol 2017;52:799-805
 91 normal weight children
diagnosed with OSA by
polysomnography (PSG)
 Thorough evaluation and
an ultra-low dose computed
tomography scan
of the upper airway (UA).
 A 3-D reconstruction
of functional respiratory
imaging (FRI).
 A second PSG 3-12 months
after surgery (A&T).
• Children with more severe
OSA had a smaller volume
of the overlap region
between the adenoids and
tonsils
*
*
% children with persistent
OSA (oAHI >2/h)
3-12 months after
surgery (A&T).
32%
40 –
30 –
20 –
10 –
00
Predicting the effect of treatment in paediatric OSA
by clinical examination and functional respiratory imaging
M Slaats, Pediatr Pulmonol 2017;52:799-805
 91 normal weight children
diagnosed with OSA by
polysomnography (PSG)
 Thorough evaluation and
an ultra-low dose computed
tomography scan
of the upper airway (UA).
 A 3-D reconstruction
of functional respiratory
imaging (FRI).
 A second PSG 3-12 months
after surgery (A&T).
% children with persistent
OSA (oAHI >2/h)
3-12 months after
surgery (A&T).
32%
40 –
30 –
20 –
10 –
00
Predicting the effect of treatment in paediatric OSA
by clinical examination and functional respiratory imaging
M Slaats, Pediatr Pulmonol 2017;52:799-805
 91 normal weight children
diagnosed with OSA by
polysomnography (PSG)
 Thorough evaluation and
an ultra-low dose computed
tomography scan
of the upper airway (UA).
 A 3-D reconstruction
of functional respiratory
imaging (FRI).
 A second PSG 3-12 months
after surgery (A&T).
A higher tonsil score
predicted successful
treatment.
% children with persistent
OSA (oAHI >2/h)
3-12 months after
surgery (A&T).
32%
40 –
30 –
20 –
10 –
00
Predicting the effect of treatment in paediatric OSA
by clinical examination and functional respiratory imaging
M Slaats, Pediatr Pulmonol 2017;52:799-805
 91 normal weight children
diagnosed with OSA by
polysomnography (PSG)
 Thorough evaluation and
an ultra-low dose computed
tomography scan
of the upper airway (UA).
 A 3-D reconstruction
of functional respiratory
imaging (FRI).
 A second PSG 3-12 months
after surgery (A&T).
A less constricted
airway, as
characterized by both
FRI and a lower tonsil
score, was associated
with a less favorable
response to (adeno)
tonsillectomy.
Predicting the effect of treatment in paediatric OSA
by clinical examination and functional respiratory imaging
M Slaats, Pediatr Pulmonol 2017;52:799-805
3-D reconstruction of the UA Computerized 3-D model of the UA
Nostril to anterior end of
inferior turbinate (zone1),
anterior end of inferior
turbinate to choanae (zone2),
choanae to tip of uvula (zone3),
uvula to epiglottis (zone4), and
epiglottis to the first thoracic
vertebra (zone5)
Predicting the effect of treatment in paediatric OSA
by clinical examination and functional respiratory imaging
M Slaats, Pediatr Pulmonol 2017;52:799-805
3-D reconstruction of the UA Computerized 3-D model of the UA
Zone1: Nostril to anterior end
of inferior turbinate;
Zone2: anterior end of inferior
turbinate to choanae;
Zone3: choanae to tip of uvula;
Zone4 : uvula to epiglottis;
Zone5 : epiglottis to the first
thoracic vertebra .
•Sleep-
Disordered
Breathing
Treatment
Oropharyngeal
Exercises
CPAP
Ortodonzia
Oral-palatal
surgery
INSOMNIA

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What pulmonology 3 sonno

  • 1. Pulmonology 3 Sleep disorders Attilio Boner University of Verona, Italy attilio.boner@univr.it WHAT YOU SOULD HAVE READ BUT ………………… 2018
  • 3.  Telomeres are repetitive DNA sequences (in humans, TTAGGGn) and associated proteins that cap the end of chromosomes.  With each cycle of chromosomal replication and cellular division, the telomere becomes shorter, except in specialized cells expressing telomerase.  This means that telomere length gradually decreases with age in most cells.  Difficult life experiences may be associated with an accelerated rate of telomere attrition. Sleep Duration and Telomere Length in Children S James, J Pediatr. 2017;187:247-252
  • 4. Sleep Duration and Telomere Length in Children S James, J Pediatr. 2017;187:247-252  Inadequate nightly sleep duration is linked to morbidities and mortality, as well as a number of physiological sequelae, including inflammation, oxidative stress, increased sympathetic tone, and neuroendocrine dysregulation.  Short sleep duration in childhood is associated with changes in hypothalamic–pituitary–adrenocortical system activity, autonomic nervous system activity, and metabolic regulation.  This type of stress-altered hypothalamic–pituitary–adrenocortical activity is known to correlate with telomere length.
  • 5. Sleep Duration and Telomere Length in Children S James, J Pediatr. 2017;187:247-252 Distribution of children's hours of sleep at 9 years of age in the analytic sample  Data for 1567 children from a population-based birth cohort of children born between 1998 and 2000.  Telomere length using quantitative polymerase chain reaction.
  • 6.  Data for 1567 children from a population-based birth cohort of children born between 1998 and 2000.  Telomere length using quantitative polymerase chain reaction. Sleep Duration and Telomere Length in Children S James, J Pediatr. 2017;187:247-252 • Children with shorter sleep durations have shorter telomeres than children with longer sleep durations. • Each hour less of nightly sleep duration is associated with having telomeres that are 0.015 log- kilobases per chromosome shorter (P < 0.05).
  • 7.  Data for 1567 children from a population-based birth cohort of children born between 1998 and 2000.  Telomere length using quantitative polymerase chain reaction. Sleep Duration and Telomere Length in Children S James, J Pediatr. 2017;187:247-252 • Children with shorter sleep durations have shorter telomeres than children with longer sleep durations. • Each hour less of nightly sleep duration is associated with having telomeres that are 0.015 log- kilobases per chromosome shorter (P < 0.05). That suboptimal sleep duration is a risk for increased physiological stress and impaired health.
  • 8. Sleep Duration and Telomere Length in Children S James, J Pediatr. 2017;187:247-252  The biological mechanism by which sleep duration becomes linked to telomere length in children, may be: • telomere erosion (eg, owing to oxidative stress) • suppression of telomerase activity • hypothalamic–pituitary–adrenal axis activation, • inflammation, • oxidation.
  • 10. Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131  Cross-sectional study with bedroom electronic devices (EDs) placement and parental restriction reported by parents.  Relationship between school readiness and ED placement.  556 young children attending the 3° year of kindergarten. % parents placing at least one electronic devices in their children’s bedroom 30% 30 – 25 – 20 – 15 – 10 – 05 – 00 –
  • 11. Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131  Cross-sectional study with bedroom electronic devices (EDs) placement and parental restriction reported by parents.  Relationship between school readiness and ED placement.  556 young children attending the 3° year of kindergarten. % parents placing at least one electronic devices in their children’s bedroom 30% 30 – 25 – 20 – 15 – 10 – 05 – 00 – Placement of television in the bedroom was associated with lower overall school readiness and the placement of game console with lower social competence
  • 12. Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131  Cross-sectional study with bedroom electronic devices (EDs) placement and parental restriction reported by parents.  Relationship between school readiness and ED placement.  556 young children attending the 3° year of kindergarten. % parents placing at least one electronic devices in their children’s bedroom 30% 30 – 25 – 20 – 15 – 10 – 05 – 00 – Such harmful effect was more prominent among lower socioeconomic status families
  • 13. School readiness • School readiness is an indicator of whether a child possesses the cognitive, social and emotional skills necessary for success in school and has been shown to predict long-term educational outcomes. Forget-Dubois N, Early Educ Dev 2007;18:405–26 Silburn SR, Early Hum Dev 2007;83:S125 • School readiness was measured using the Early Development Instrument (EDI), a comprehensive teacher-rated scale. Janus M, Can J Behav Sci 2007;39:1–22 Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131
  • 14. Effect of bedroom electronic device (ED) placement on school readiness moderated by family socioeconomic status (SES) P<0.05 Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131
  • 15. Effect of bedroom ED placement on school readiness moderated by parental restriction P<0.001 Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131
  • 16. Effect of bedroom ED placement on school readiness moderated by parental restriction P<0.001 Parental restriction reduces the harmful effects of in-bedroom electronic devices King-wa Fu, Arch Dis Child. 2017;102:1125-1131 ED placement in children’s bedroom was associated with lower school readiness, particularly among lower SES families. Parental restriction might help to alleviate the harm.
  • 17. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363. Importance: Although multiple cross-sectional and longitudinal studies have established that sleep problems and behavioral difficulties are associated in children, the directionality of this association and whether sleep problems are differentially associated with different types of childhood behavioral difficulties are unclear. Understanding these associations will inform the focus and timing of interventions. Objective: To determine whether longitudinal and reciprocal associations exist between child sleep problems and externalizing, internalizing, or both behavioral difficulties.
  • 18. Prospective cohort study using nationally representative data from 5 waves 2004 (4983 children mean age of 4.7 ), 2006, 2008, 2010, and 2012) kindergarten cohort (4983 children aged 4-5 years in 2004) Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363. Sleep problems were defined using parent-reported child sleep problem severity and specific difficulties: 1. difficulty getting to sleep at night, 2. not happy sleeping alone, 3. waking during the night, 4. restless sleep on 4 or more nights of the week.
  • 19. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363. Child behavioral difficulties using the parent-reported Strengths and Difficulties Questionnaire for 1. externalizing difficulties (conduct problems and hyperactivity/inattention subscales) and 2. internalizing difficulties (emotional problems subscale). Prospective cohort study using nationally representative data from 5 waves 2004 (4983 children mean age of 4.7 ), 2006, 2008, 2010, and 2012) kindergarten cohort (4983 children aged 4-5 years in 2004)
  • 20. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363. Prospective cohort study using nationally representative data from 5 waves 2004 (4983 children mean age of 4.7 ), 2006, 2008, 2010, and 2012) kindergarten cohort (4983 children aged 4-5 years in 2004) Significant bidirectional associations were detected between sleep problems and externalizing difficulties during the elementary school transition period, with greater sleep problems associated with later externalizing behavior and vice versa
  • 21. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363. Prospective cohort study using nationally representative data from 5 waves 2004 (4983 children mean age of 4.7 ), 2006, 2008, 2010, and 2012) kindergarten cohort (4983 children aged 4-5 years in 2004) Although sleep was a significant driver of later internalizing difficulties, the reverse association was not significant.
  • 22. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363. Prospective cohort study using nationally representative data from 5 waves 2004 (4983 children mean age of 4.7 ), 2006, 2008, 2010, and 2012) kindergarten cohort (4983 children aged 4-5 years in 2004) Conclusions and Relevance: These results suggest that future studies should investigate whether implementing sleep problem intervention decreases the occurrence of both externalizing and internalizing difficulties. Interventions targeting externalizing, but not internalizing, difficulties may benefit childhood sleep
  • 23. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
  • 24. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
  • 25. Bidirectional Associations Between Child Sleep Problems and Internalizing and Externalizing Difficulties from Preschool to Early Adolescence. Quach JL, JAMA Pediatr. 2018 Feb 5;172(2):e174363.
  • 27. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. The present statement was produced by a European Respiratory Society Task Force to summarise the evidence and current practice on the diagnosis and management of obstructive sleep disordered breathing (SDB) in children aged 1-23 months. A systematic literature search was completed and 159 articles were summarised to answer clinically relevant questions. SDB is suspected when symptoms or abnormalities related to upper airway obstruction are identified. Morbidity (pulmonary hypertension, growth delay, behavioural problems) and coexisting conditions (feeding difficulties, recurrent otitis media) may be present. SDB severity is measured objectively, preferably by polysomnography, or alternatively polygraphy or nocturnal oximetry.
  • 28. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. Children with apparent upper airway obstruction during wakefulness, those with abnormal sleep study in combination with SDB symptoms (e.g. snoring) and/or conditions predisposing to SDB (e.g. mandibular hypoplasia) as well as children with SDB and complex conditions (e.g. Down syndrome, Prader-Willi syndrome) will benefit from treatment. Adenotonsillectomy and continuous positive airway pressure are the most frequently used treatment measures along with interventions targeting specific conditions (e.g. supraglottoplasty for laryngomalacia or nasopharyngeal airway for mandibular hypoplasia). Hence, obstructive SDB in children aged 1-23 months is a multifactorial disorder that requires objective assessment and treatment of all underlying abnormalities that contribute to upper airway obstruction during sleep.
  • 29. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. •American Thoracic Society. Standards and indications for cardiopulmonary sleep studies in children. Am J Respir Crit Care Med 1996; 153: 866–878. •Dayyat E, Kheirandish-Gozal L, Gozal D. Childhood obstructive sleep apnea: one or two distinct disease entities? Sleep Med Clin 2007; 2: 433–444.
  • 30. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985.
  • 31. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. A stepwise approach to the management of obstructive sleep disordered breathing in 1- to 23-month-old children
  • 32. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. A stepwise approach to the management of obstructive sleep disordered breathing in 1- to 23-month-old children
  • 33. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. A stepwise approach to the management of obstructive sleep disordered breathing in 1- to 23-month-old children
  • 34. ERS statement on obstructive sleep disordered breathing in 1- to 23-month-old children. Kaditis AG, Eur Respir J. 2017 Dec 7;50(6). pii: 1700985. FIGURE 1 A stepwise approach to the management of obstructive sleep disordered breathing in 1- to 23-month-old children reflecting the Task Force members’ current practice. This scheme is not intended as a recommendation for clinicians. OSAS: obstructive sleep apnoea syndrome; ALTE: apparent life-threatening event; GOR: gastro-oesophageal reflux; ENT: ear, nose and throat; PSG: polysomnography; AHI: apnoea–hypopnoea index; UAO: upper airway obstruction; CPAP: continuous positive airway pressure; NPPV: non-invasive positive pressure ventilation; nCPAP: nasal CPAP.
  • 35. Allergic sensitization and objective measures of sleep in urban school-aged children with asthma CA Esteban, Ann Allergy Asthma Immunol 2017;119:238-245 Background • Allergic sensitization is associated with increased child asthma morbidity and decreased pulmonary function. • Nocturnal symptoms and/or awakenings typically are measured by self-report from diary data, whereas objective assessments of sleep in child asthma studies are lacking. Objective • To investigate the association between increased allergic sensitization (number of positive allergy test results measured by SPTs or sIgE) and sleep outcomes (sleep efficiency, sleep duration, and mean number of awakenings measured by actigraphy) in urban schoolchildren with persistent asthma.
  • 36.  196 children with persistent asthma (7–9 years old).  Sleep outcomes were measured with a wrist Actiwatch during a 1-month period in the fall and winter seasons. Allergic sensitization and objective measures of sleep in urban school-aged children with asthma CA Esteban, Ann Allergy Asthma Immunol 2017;119:238-245 • Children with more positive test results experienced: • less efficient sleep. • more night awakenings. P=0.05.
  • 37. Allergic sensitization and objective measures of sleep in urban school-aged children with asthma CA Esteban, Ann Allergy Asthma Immunol 2017;119:238-245 Number of positive allergy test results and variability in sleep efficiency by variability in FEV1 (median split). For children above the median FEV1 value of variability, more allergy tests were associated with more variability in sleep efficiency (b = .38, P = .00, R2 adjusted = 0.13). In contrast, for children below the median (less variability in FEV1), there was no significant association between number of positive allergy test results and variability in sleep
  • 38.  42 obese adolescents with the obstructive sleep apnoea syndrome (OSAS) and 37 weight-matched controls.  Upper airway MRI, measurements of upper airway critical closing pressure (Pcrit), genioglossal electromyography and ventilatory response to CO2 during wakefulness and sleep. • Adenotonsillar volume (ATV), • nasopharyngeal airway volume (NPAV), • activated and hypotonic upper airway critical closing pressure (Pcrit), • genioglossal electromyography • ventilatory response to CO2 during sleep were all associated with OSAS risk. The obstructive sleep apnoea syndrome in adolescents Marcus CL, Thorax 2017;72:720–728
  • 39.  42 obese adolescents with the obstructive sleep apnoea syndrome (OSAS) and 37 weight-matched controls.  Upper airway MRI, measurements of upper airway critical closing pressure (Pcrit), genioglossal electromyography and ventilatory response to CO2 during wakefulness and sleep. • Adenotonsillar volume (ATV), • nasopharyngeal airway volume (NPAV), • activated and hypotonic upper airway critical closing pressure (Pcrit), • genioglossal electromyography • ventilatory response to CO2 during sleep were all associated with OSAS risk. The obstructive sleep apnoea syndrome in adolescents Marcus CL, Thorax 2017;72:720–728 OSAS in adolescents is mediated by a combination of anatomic (ATV, NPAV) and neuromotor factors (activated Pcrit).
  • 40. The obstructive sleep apnoea syndrome in adolescents Marcus CL, Thorax 2017;72:720–728 3D plots of the predicted probability (Pr) of obstructive sleep apnoea syndrome (OSAS) High predicted probabilities of OSAS are shown in red, probabilities around 0.5 in grey and low predicted probabilities in blue Nasopharyngeal airway volume (NPAV)  42 obese adolescents with the obstructive sleep apnoea syndrome (OSAS) and 37 weight-matched controls.  Upper airway MRI, measurements of upper airway critical closing pressure (Pcrit), genioglossal electromyography and ventilatory response to CO2 during wakefulness and sleep.
  • 41. The obstructive sleep apnoea syndrome in adolescents Marcus CL, Thorax 2017;72:720–728 3D plots of the predicted probability (Pr) of obstructive sleep apnoea syndrome (OSAS) High predicted probabilities of OSAS are shown in red, probabilities around 0.5 in grey and low predicted probabilities in blue Activated critical closing pressure (Pcrit)  42 obese adolescents with the obstructive sleep apnoea syndrome (OSAS) and 37 weight-matched controls.  Upper airway MRI, measurements of upper airway critical closing pressure (Pcrit), genioglossal electromyography and ventilatory response to CO2 during wakefulness and sleep.
  • 42. The obstructive sleep apnoea syndrome in adolescents Marcus CL, Thorax 2017;72:720–728 High predicted probabilities of OSAS are shown in red, probabilities around 0.5 in grey and low predicted probabilities in blue Nasopharyngeal airway volume (NPAV) 3D plots of the predicted probability (Pr) of obstructive sleep apnoea syndrome (OSAS)  42 obese adolescents with the obstructive sleep apnoea syndrome (OSAS) and 37 weight-matched controls.  Upper airway MRI, measurements of upper airway critical closing pressure (Pcrit), genioglossal electromyography and ventilatory response to CO2 during wakefulness and sleep.
  • 45. Nocturnal Oximetry-based Evaluation of Habitually Snoring Children. Hornero R, Am J Respir Crit Care Med. 2017;196(12):1591-1598. RATIONALE: The vast majority of children around the world undergoing adenotonsillectomy for obstructive sleep apnea-hypopnea syndrome (OSA) are not objectively diagnosed by nocturnal polysomnography because of access availability and cost issues. Automated analysis of nocturnal oximetry (nSpO2), which is readily and globally available, could potentially provide a reliable and convenient diagnostic approach for pediatric OSA.
  • 46. Nocturnal Oximetry-based Evaluation of Habitually Snoring Children. Hornero R, Am J Respir Crit Care Med. 2017;196(12):1591-1598. Deidentified nocturnal oximetry (nSpO2 ) recordings from a total of 4,191 children originating from 13 pediatric sleep laboratories prospectively evaluated after developing and validating an automated neural network algorithm using an initial set of single-channel nSpO2 recordings from 589 patients referred for suspected OSA. The automatically estimated apnea-hypopnea index (AHI) showed high agreement with AHI from conventional polysomnography (intraclass correlation coefficient, 0.785) when tested in 3,602 additional subjects.
  • 47. Nocturnal Oximetry-based Evaluation of Habitually Snoring Children. Hornero R, Am J Respir Crit Care Med. 2017;196(12):1591-1598. Deidentified nocturnal oximetry (nSpO2 ) recordings from a total of 4,191 children originating from 13 pediatric sleep laboratories prospectively evaluated after developing and validating an automated neural network algorithm using an initial set of single-channel nSpO2 recordings from 589 patients referred for suspected OSA. the widely used AHI cutoff points of 1, 5, and 10 events/h revealed an incremental diagnostic ability (75.2, 81.7, and 90.2% accuracy; 0.788, 0.854, and 0.913 area under the receiver operating characteristic curve, respectively).
  • 48. Machines Learning to Detect Obstructive Sleep Apnea in Children. Are We There Yet? Editorial Combs D, Am J Respir Crit Care Med. 2017;196(12):1506-1507. •In this issue of the Journal, Hornero and colleagues (pp. 1591–1598) take a new approach to nocturnal pulse oximetry screening tool. •Specifically, they used an innovative approach of machine learning to generate a neural network algorithm to detect OSA from overnight pulse oximetry tracings. •Most prior attempts involved manual interpretation of nocturnal pulse oximetry as a screening tool for OSA. •Such a machine learning approach enabled the authors to evaluate thousands of potential algorithms to optimize a screening algorithm.
  • 49. •On the basis of their results, the authors suggest a diagnostic protocol for applying this tool in clinical practice. •Children with an estimated AHI lower than 1 based on overnight pulse oximetry are unlikely to have moderate or severe sleep apnea and may not require polysomnography. •Children with a machine-estimated AHI of 5 or more per hour are likely to have at least mild OSA by polysomnography (AHI >1), and could be referred to treatment directly without undergoing polysomnography. •Children with a machine-estimated AHI of 1–5 per hour would be considered indeterminate and can be referred for polysomnography. •Based on the author’s findings, approximately 1 in 20 children would be incorrectly diagnosed with OSA and potentially treated unnecessarily. Machines Learning to Detect Obstructive Sleep Apnea in Children. Are We There Yet? Editorial Combs D, Am J Respir Crit Care Med. 2017;196(12):1506-1507.
  • 51. Asthma outcomes improve with continuous positive airway pressure for obstructive sleep apnea J Serrano-Pariente, Allergy 2017;72:802-812 • The mean ± SD score of the ACQ decreased from 1.39 ± 0.91 at baseline to 1.0 ± 0.78 at 6 months (P = 0.003).  Continuous positive airway pressure (CPAP).  Asthma outcomes after 6 months of CPAP in 99 adult asthma patients (mean age 57 years) with OSAS.  Asthma Control Questionnaire (ACQ).
  • 52. Asthma outcomes improve with continuous positive airway pressure for obstructive sleep apnea J Serrano-Pariente, Allergy 2017;72:802-812 • The mean ± SD score of the ACQ decreased from 1.39 ± 0.91 at baseline to 1.0 ± 0.78 at 6 months (P = 0.003).  Continuous positive airway pressure (CPAP).  Asthma outcomes after 6 months of CPAP in 99 adult asthma patients (mean age 57 years) with OSAS.  Asthma Control Questionnaire (ACQ).
  • 53. Asthma outcomes improve with continuous positive airway pressure for obstructive sleep apnea J Serrano-Pariente, Allergy 2017;72:802-812 • The mean ± SD score of the ACQ decreased from 1.39 ± 0.91 at baseline to 1.0 ± 0.78 at 6 months (P = 0.003).  Continuous positive airway pressure (CPAP).  Asthma outcomes after 6 months of CPAP in 99 adult asthma patients (mean age 57 years) with OSAS.  Asthma Control Questionnaire (ACQ). Asthma control (both actual and future risk), quality of life, and lung function improved after starting continuous positive airway pressure in asthmatics with moderate to severe obstructive sleep apnea syndrome.
  • 54. Asthma outcomes improve with continuous positive airway pressure for obstructive sleep apnea J Serrano-Pariente, Allergy 2017;72:802-812 Pre 41.4% 17.2% Post 50 – 40 – 30 – 20 – 10 – 00 – CPAP % patients with uncontrolled asthma % patients with asthma attacks in the 6 months Pre 35.4% 17.2% Post 50 – 40 – 30 – 20 – 10 – 00 – CPAP P=0.006 P=0.015
  • 55. Asthma outcomes improve with continuous positive airway pressure for obstructive sleep apnea J Serrano-Pariente, Allergy 2017;72:802-812 Number of patients with well-controlled asthma (ACQ score ≤ 0.75) and not well-controlled asthma (ACQ score ≥ 1.5) after starting continuous positive airway pressure  Continuous positive airway pressure (CPAP).  Asthma outcomes after 6 months of CPAP in 99 adult asthma patients (mean age 57 years) with OSAS.  Asthma Control Questionnaire (ACQ).
  • 56. Asthma outcomes improve with continuous positive airway pressure for obstructive sleep apnea J Serrano-Pariente, Allergy 2017;72:802-812  The mechanisms by which treatment with CPAP may improve symptoms and asthma control are multiple.  OSAS is associated with a systemic and local inflammation of the airways, as well as pulmonary vascular changes and release of endothelial factors (such as vascular endothelial growth factor) with proinflammatory effects.  The use of CPAP reduces inflammation and its mediators.  Improvement of gastroesophageal reflux may also be accompanied by a reduction in nocturnal asthma symptoms.  Additionally, reduction in bronchial hyperresponsiveness produced by CPAP can be also associated with a clinical improvement of asthma.
  • 61. • Although adenotonsillectomy is the first line treatment for children with obstructive sleep apnea syndrome (0SAS), improvement in objectively documented outcomes is often inadequate and a substantial number of children have residual disease, as most of them have additional risk factors for OSAS and comorbidities. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 62. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709 Non-syndromic uncomplicated children Syndromic children and children with complex medical conditions OSA with an AHI > 5 episodes/h Major craniofacial abnormalities Children with cardiovascular morbidity (e.g., elevated blood pressure Neurological disorders including neuromuscular disorders and neurodisability Children with neurological morbidity (e.g., excessive daytime sleepiness, hyperactivity, inattention, academic difficulties) Achondroplasia Enuresis Down syndrome Somatic growth delay or failure to thrive Prader–Willi syndrome Obesity Mucopolysaccharidoses Asthma Priority Indication for adenotonsillectomy
  • 63. Which Examinations Should/Could Be Performed In Children With Residual Disease To Guide Further Treatment? • Many children with OSAS have multiple sites of upper airway (UA) obstruction during sleep and this may contribute to persistent OSAS following AT. • Possible sites of persistent UA obstruction are the region of the soft palate, tongue base with lingual tonsillar hypertrophy, the supraglottis, inferior turbinates, and the adenoid region with regrowth of adenoids. • The diagnostic work-up to identify the levels of persistent UA obstruction starts with a detailed history and flexible nasopharyngoscopy up to the level of the larynx in the awake patient. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 64. Which Examinations Should/Could Be Performed In Children With Residual Disease To Guide Further Treatment? • Sleep cine-magnetic resonance imaging (MRI) and drug induced sedation endoscopy (DISE) were the most commonly used tools for dynamic evaluation of the pediatric UA. • Children with persistent OSAS had a higher percentage of lingual tonsillar hypertrophy compared to controls (33% vs. 0%), and lingual tonsillar hypertrophy occurred predominantly in children with Down syndrome. • DISE might be particularly useful for the evaluation of lingual tonsillar hypertrophy and late-onset laryngomalacia. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 65. Site-specific Treatment: Orthodontic Treatment • An orthodontic treatment is indicated in children with OSAS and craniofacial alterations such as retrusive chin, steep mandibular plane, vertical direction of growth and a Class II malocclusion • Oral appliances may improve UA patency during sleep by enlarging the UA, decreasing UA collapsibility and improving UA muscle tone. • Rapid maxillary expansion (RME) and mandibular advancement by an oral jaw-positioning device are the available orthodontic treatment options in the pediatric population. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 66. Site-specific Treatment: Upper Airway Surgery • Late-onset laryngomalacia is typically characterized by inspiratory prolapse of prominent mucosal folds on the accessory cartilages above the arytenoids resulting in supraglottic obstruction and has a prevalence of 3.9% among older children with OSAS. • Potential surgical interventions for upper airway obstruction in children with residual OSAS include: (i) adenoidectomy for those with regrowth of adenoids; (ii) lingual tonsillectomy; (iii) supraglottoplasty; and (iv) partial midline glossectomy and tongue suspension with or without lingual tonsillectomy. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 67. Treatment That Alters Underlying Conditions Contributing To Osas: Weight Loss • There is consensus that weight loss therapy should be initiated in every child with OSAS because of its beneficial effects on other obesity- related complications. Medical Treatment • Intranasal budesonide and montelukast. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 68. Treatment That Alters Underlying Conditions Contributing To Osas: Myofunctional Therapy • Mouth breathing is associated with malposition of the tongue, hypotonic lips, and incorrect swallowing pattern and may predispose subjects to persistent or recurrent OSAS following adenotonsillectomy. • Myofunctional therapy consist of oropharyngeal exercises, that is, repetitive isotonic and isometric exercises of tongue, soft palate and lateral pharyngeal walls, increasing muscle tone throughout the upper respiratory tract and helping to obtain correct nasal breathing habits, speech, swallowing and chewing. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709
  • 69. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709  Endoscopic view of lingual tonsillar hypertrophy in a child residual OSA following prior AT.  Note: A complete obstruction the UA at the level of the tongue with the epiglottis pushed backwards against the pharyngeal wall. Lingual tonsillar hypertrophy
  • 70. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709 • Endoscopic view of supraglottic obstruction in a child with OSA cause by late-onset laryngomalacia. • Note: A complete obstruction of the glottis inlet by inspiratory collaps of redundant supra-arythenoidal mucosa. Late-onset laryngomalacia
  • 71. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709 Proposed algorithm for the management of persistent OSAS post-AT (part1)
  • 72. Adenotonsillectomy to treat obstructive sleep apnea: Is it enough? A Boudewyns, Pediatr Pulmonol 2017;52:699-709 Proposed algorithm for the management of persistent OSAS post-AT (part2)
  • 73. Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314 • An important risk factor for OSA in children is adenotonsillar hypertrophy. • Adenotonsillectomy (ATE) is considered first-line treatment and is one of the most common surgical procedures throughout the world. • ATE is an effective treatment of pediatric OSA but has the disadvantages of risk of postoperative hemorrhage and pain. • In recent decades, partial tonsillectomy, or adenotonsillotomy (ATT), with subtotal removal of the tonsils, has gained popularity because it is associated with less postoperative hemorrhage and pain.
  • 74. Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314  79 children, aged 2 to 6 years, with OSA (Apnea-Hypopnea Index [AHI] 5-30).  Randomized to adenotonsillotomy (ATT) (n = 40) or adenotonsillectomy (ATE) (n = 39).  Polysomnography and questionnaire at baseline and 1 year postsurgery. 12.7 BEFORE Apnea-Hypopnea Index (median) 20 – 15 – 10 – 05 - 00 15.8 2.0 4.0 BEFOREAFTER AFTER ATE ATT
  • 75. Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314  79 children, aged 2 to 6 years, with OSA (Apnea-Hypopnea Index [AHI] 5-30).  Randomized to adenotonsillotomy (ATT) (n = 40) or adenotonsillectomy (ATE) (n = 39).  Polysomnography and questionnaire at baseline and 1 year postsurgery. 12.7 BEFORE Apnea-Hypopnea Index (median) 20 – 15 – 10 – 05 - 00 15.8 2.0 4.0 BEFOREAFTER AFTER ATE ATT For both groups, significant improvements of PSG and OSA-18 questionnaire outcomes were observed, with no significant differences between groups.
  • 76. Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314  79 children, aged 2 to 6 years, with OSA (Apnea-Hypopnea Index [AHI] 5-30).  Randomized to adenotonsillotomy (ATT) (n = 40) or adenotonsillectomy (ATE) (n = 39).  Polysomnography and questionnaire at baseline and 1 year postsurgery. 12.7 BEFORE Apnea-Hypopnea Index (median) 20 – 15 – 10 – 05 - 00 15.8 2.0 4.0 BEFOREAFTER AFTER ATE ATT 5 children (13%) in the ATT group needed repeated surgery for tonsil regrowth and recurrence of OSA.
  • 77. Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314  79 children, aged 2 to 6 years, with OSA (Apnea-Hypopnea Index [AHI] 5-30).  Randomized to adenotonsillotomy (ATT) (n = 40) or adenotonsillectomy (ATE) (n = 39).  Polysomnography and questionnaire at baseline and 1 year postsurgery. 12.7 BEFORE Apnea-Hypopnea Index (median) 20 – 15 – 10 – 05 - 00 15.8 2.0 4.0 BEFOREAFTER AFTER ATE ATT • The results suggest that ATT is noninferior to ATE in treating pediatric OSA regarding PSG outcomes after 1 year. • However, after ATT, there is a nonnegligible risk of recurrence of OSA.
  • 78. Boxplots and lines showing the AHI 1 (before surgical intervention) and AHI 2 (after surgical intervention) Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314
  • 79. Adenotonsillotomy Versus Adenotonsillectomy in Pediatric Obstructive Sleep Apnea: An RCT Borgström A, Pediatrics 2017;139:e20163314 Tonsil regrowth and recurrence of OSA are known disadvantages after ATT, and 13% of the children in the ATT group underwent repeated tonsil surgery within the follow-up period. A recent Swedish study based on >28 000 children reported a 7 times higher risk of reoperation after TT than after TE, with the difference most markedly among the youngest children. In our study, the children undergoing reoperation were also among the youngest (median age 32 months).
  • 80. Predicting the effect of treatment in paediatric OSA by clinical examination and functional respiratory imaging M Slaats, Pediatr Pulmonol 2017;52:799-805  91 normal weight children diagnosed with OSA by polysomnography (PSG)  Thorough evaluation and an ultra-low dose computed tomography scan of the upper airway (UA).  A 3-D reconstruction of functional respiratory imaging (FRI).  A second PSG 3-12 months after surgery (A&T). • Children with more severe OSA had a smaller volume of the overlap region between the adenoids and tonsils * *
  • 81. % children with persistent OSA (oAHI >2/h) 3-12 months after surgery (A&T). 32% 40 – 30 – 20 – 10 – 00 Predicting the effect of treatment in paediatric OSA by clinical examination and functional respiratory imaging M Slaats, Pediatr Pulmonol 2017;52:799-805  91 normal weight children diagnosed with OSA by polysomnography (PSG)  Thorough evaluation and an ultra-low dose computed tomography scan of the upper airway (UA).  A 3-D reconstruction of functional respiratory imaging (FRI).  A second PSG 3-12 months after surgery (A&T).
  • 82. % children with persistent OSA (oAHI >2/h) 3-12 months after surgery (A&T). 32% 40 – 30 – 20 – 10 – 00 Predicting the effect of treatment in paediatric OSA by clinical examination and functional respiratory imaging M Slaats, Pediatr Pulmonol 2017;52:799-805  91 normal weight children diagnosed with OSA by polysomnography (PSG)  Thorough evaluation and an ultra-low dose computed tomography scan of the upper airway (UA).  A 3-D reconstruction of functional respiratory imaging (FRI).  A second PSG 3-12 months after surgery (A&T). A higher tonsil score predicted successful treatment.
  • 83. % children with persistent OSA (oAHI >2/h) 3-12 months after surgery (A&T). 32% 40 – 30 – 20 – 10 – 00 Predicting the effect of treatment in paediatric OSA by clinical examination and functional respiratory imaging M Slaats, Pediatr Pulmonol 2017;52:799-805  91 normal weight children diagnosed with OSA by polysomnography (PSG)  Thorough evaluation and an ultra-low dose computed tomography scan of the upper airway (UA).  A 3-D reconstruction of functional respiratory imaging (FRI).  A second PSG 3-12 months after surgery (A&T). A less constricted airway, as characterized by both FRI and a lower tonsil score, was associated with a less favorable response to (adeno) tonsillectomy.
  • 84. Predicting the effect of treatment in paediatric OSA by clinical examination and functional respiratory imaging M Slaats, Pediatr Pulmonol 2017;52:799-805 3-D reconstruction of the UA Computerized 3-D model of the UA Nostril to anterior end of inferior turbinate (zone1), anterior end of inferior turbinate to choanae (zone2), choanae to tip of uvula (zone3), uvula to epiglottis (zone4), and epiglottis to the first thoracic vertebra (zone5)
  • 85. Predicting the effect of treatment in paediatric OSA by clinical examination and functional respiratory imaging M Slaats, Pediatr Pulmonol 2017;52:799-805 3-D reconstruction of the UA Computerized 3-D model of the UA Zone1: Nostril to anterior end of inferior turbinate; Zone2: anterior end of inferior turbinate to choanae; Zone3: choanae to tip of uvula; Zone4 : uvula to epiglottis; Zone5 : epiglottis to the first thoracic vertebra .