past, present & future · n engl j med 1971; 284:1333-1340 june 17, 1971 . ... death during...
TRANSCRIPT
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The Preterm Lung: Past, Present & Future
Richard J. Martin, M.D. Drusinsky-Fanaroff Chair in Neonatology
Rainbow Babies & Children’s Hospital
Professor, Pediatrics
Case Western Reserve University
Cleveland, Ohio
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Before 1974
After 1974
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Advice for an Entry Level Neonatologist in the 1970s
“A solution for prematurity is at hand”. Implication: this is a risky career move
“All the respiratory problems have been solved”. Implication: avoid respiratory research
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The Preterm Lung
Historical successes
Antenatal steroids
Postnatal surfactant
Ventilatory support
Ongoing strategic challenges
Spectrum of neonatal lung disease
Novel therapeutic approaches
Longer term respiratory outcome
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NIH Consensus Statement Volume 12, Number 2
February 20-March 2 1994
Effect of Corticosteroids
for Fetal Maturation on
Perinatal Outcomes
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Antenatal Steroids: Unresolved
Lower and upper limits of gestational age for administration not uniformly accepted
Likely benefit at 24 weeks
Benefit at 34 weeks under study
No consensus on repetitive doses
A second course after 14 days may offer benefit
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Relative Contributions to Neonatal Respiratory Distress
24 27 30 33 36 39
Gestational Age (weeks)
Ra
tes
of
Res
pir
ato
ry D
istr
ess
100%
Inefficient fluid absorption
Surfactant deficiency
Helve, Neonatology 2009
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Cord Plasma Cortisol, ng/mL
Airw
ay E
pith
elia
l
EN
aC
mR
NA
am
ol/fm
ol C
K18
Janer, Pediatrics 2011
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Respiratory Distress after Elective Repeat Cesarean Section
0
1
2
3
4
5
37 38 39 40
RDS TTN
Per
cen
t [%
]
Gestation [weeks]
Tita, A. et al, N Engl J Med 2009
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Births Induced at 36-38 Weeks with No Apparent Medical Indication for Early
Delivery (by month) 2006-2012
Pe
rc
en
t w
ith
N
o M
ed
ica
l In
dic
ati
on
2006 to 2012
0
2
4
6
8
10
12
14
16
Source: Ohio Department of Health, Vital Statistics
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Surface Properties in Relation to Atelectasis
and Hyaline Membrane Disease
Mary Ellen Avery, M.D., and Jere Mead, M.D., Boston
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Whitsett and Weaver, N Engl J Med, 2002
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Timing of Surfactant Administration
100
80
60
40
20
0
Inborn Outborn
Med
ian
Tim
e o
f F
irst
Do
se (
Min
)
1998 1999 2000
Horbar, Pediatrics 2004
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Prophylactic vs Selective Surfactant
“When all studies were evaluated together, the benefits of prophylactic surfactant could no longer be demonstrated.”
Cochrane Update 2012
“The day for routine aggressive prophylactic surfactant to all infants at risk of RDS has passed.”
Roger F. Soll
Neonatology 2012
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Surfactant Therapy: Unresolved
Role of dosage versus preparation in subtle differences in benefit
Optimal preparation for selective indications
Animal based vs. synthetic
Role in immune protection (SP-A and SP-D)
Potential role for later dosing to prevent BPD
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Surfactant Therapy: Unresolved
Possible non-invasive administration
Laryngeal mask, aerosol, intratracheal catheter
Assessment of need via gastric aspirate
Microbubble test, lamellar body count
Surfactant as a vehicle for other drugs, e.g., steroids
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Frequency Spectrum for Assisted Ventilation
Carlo and Martin, 1986
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Treatment of the Idiopathic Respiratory-Distress Syndrome with Continuous Positive Airway Pressure
George A. Gregory, M.D., Joseph A. Kitterman, M.D., Roderic H. Phibbs,
M.D., William H. Tooley, M.D., and William K. Hamilton, M.D.
N Engl J Med 1971; 284:1333-1340 June 17, 1971
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CPAP-Based Strategy for Neonatal Respiratory Distress
Should CPAP/PEEP begin in the delivery room?
Are all CPAP strategies and delivery systems equivalent?
What pH, PCO2, FiO2 constitutes CPAP failure?
Is the incidence of BPD reduced?
Role of other non-invasive techniques
Bi-level CPAP, nasal IMV, high flow nasal cannula [HFNC]
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CPAP or Intubation?
“Good” Infants
Marginal Infants
“Bad” Infants
Success on CPAP Require Intubation
Early Extubation
Jobe A., Personal Conversation
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The Preterm Lung
Historical successes
Antenatal steroids
Postnatal surfactant
Ventilatory support
Ongoing strategic challenges
Spectrum of neonatal lung disease
Novel therapeutic approaches
Longer term respiratory outcome
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Patterns of Progression to BPD
Laughon, Pediatrics 2009
50
40
30
21
FIO
2 (
%)
0 1 2 3 4 5 6 7 14
Postnatal Day
CLD = 67%
CLD = 51%
CLD = 17%
(n = 76)
(n = 484)
(n = 249)
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Inspired O2 Baro/
volutrauma
Low Gestation
Sepsis/
inflammation
BPD/CLD
Low Birthweight
Nutritional
Deficit
Genetic Susceptibility
PDA
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The BPD Challenge
Incidence in ELBW infants approaches 50%
No clear definition
Animal models remain a challenge
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Interventions for BPD
Early Treatment Late Treatment
• Infants more vulnerable
• Intervention may be
unnecessary
• Benefit likely maximized
• Infants less vulnerable
• Intervention selective
• Benefit probably decreased
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Risk of Bronchopulmonary Dysplasia
“The only treatments that have reduced the incidence of BPD in randomized trials without serious adverse events in premature infants are caffeine and vitamin A”.
Laughon: JAMA Pediatr 2014
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Effect of Vitamin A Shortage on Death or BPD
Tolia VN: JAMA Pediatr 2014
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Vitamin A & Chronic Lung Disease in Infants: What Happened When There Wasn’t Any?
[500-1000 gm infants who survived 28 days]
Vitamin A
[n=74]
No Vitamin A
[n=140]
p value
BPD @ 36 wk 37.8 58.6 0.004
Mortality 1.3 5.7 0.13
O2 @ 28 days 67.5 75.7 0.26
Paluso AM et al: PAS 2015
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Novel Strategies for BPD
Control of inflammation
Inositol
Elastase inhibition
Antioxidants
Stem cell therapy
Enhancement of NO bioactivity
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Postnatal Steroids: Unresolved
To Whom?
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Postnatal Steroids: Unresolved
May be indicated in a subpopulation with significant ventilator dependence if BPD risk exceeds about 50%
Aim for as short a course and as low a dose as possible
Do not assume there is a safe window for treatment
Clarification of mechanism in order to identify more specific anti-inflammatory approaches
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Ureaplasma has been associated with BPD, however, further studies should be done to confirm a possible benefit of azithromycin in the neonatal population.
Neonatology 2014
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Novel Strategies for BPD
Control of inflammation
Inositol
Elastase inhibition
Antioxidants
Stem cell therapy
Enhancement of NO bioactivity
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Inositol Supplementation in Premature Infants with RDS
Hallman M: N Engl J Med 1992
Death during first 28 days
Survival up to 28 days
with BPD
without BPD
26
26
55
13
20
81
0.012
.022
0.005
Placebo [n=107]
Inositol [n=114] P value
No. of infants
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Novel Strategies for BPD
Control of inflammation
Inositol
Elastase inhibition
Antioxidants
Stem cell therapy
Enhancement of NO bioactivity
![Page 42: Past, Present & Future · N Engl J Med 1971; 284:1333-1340 June 17, 1971 . ... Death during first 28 days Survival up to 28 days with BPD without BPD 26 26 55 13 20 81 0.012 .022](https://reader033.vdocuments.us/reader033/viewer/2022050117/5f4dc5a530e40c60d30ad6a8/html5/thumbnails/42.jpg)
Novel Strategies for BPD
Control of inflammation
Inositol
Elastase inhibition
Antioxidants
Stem cell therapy
Enhancement of NO bioactivity
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Recombinant Human CuZn Superoxide Dismutase and 1 year Pulmonary Outcome
Davis, JM, Pediatrics 2003
Placebo
R-hCuZnSOD
* **
Entire Group <27 Weeks Gestation
Asthma Medications
Per
cen
t of
Infa
nts
50
45
40
35
30
25
20
15
10
5
0
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0
0,5
1
1,5
2
2,5
0 1 2 3 4 5 6 7 8
0
20
40
60
80
100
120
140
160
0 1 2 3 4 5 6 7 8
A
B Days before birth since last dose of antenatal corticosteroid administration.
SOD ACTIVITY
CAT ACTIVITY
male female
IU/g
Hg
b
IU/g
Hg
b
Antioxidant Enzyme Activity in Preterm Infant (<28 wk gestation) Cord Blood: Influence of Gender
□ Female ▲Male
Vento 2009
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Novel Strategies for BPD
Control of inflammation
Inositol
Elastase inhibition
Antioxidants
Stem cell therapy
Enhancement of NO bioactivity
![Page 46: Past, Present & Future · N Engl J Med 1971; 284:1333-1340 June 17, 1971 . ... Death during first 28 days Survival up to 28 days with BPD without BPD 26 26 55 13 20 81 0.012 .022](https://reader033.vdocuments.us/reader033/viewer/2022050117/5f4dc5a530e40c60d30ad6a8/html5/thumbnails/46.jpg)
Airway Delivery of BM-derived MSC Prevents Alveolar Injury in O2-induced BPD in Newborn Rats
0
10
20
30
40
50
60
Normoxia Hyperoxia Hyperoxia +
BM-MSC
Mean
Lin
ear
Inte
rcep
t (μ
m)
n=6/group
*p<0.05
* *
van Haaften: Am J Respir Crit Care Med 2009
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Challenges of Mesenchymal Stem Cell Therapy
Source and route of administration
Preventive vs therapeutic approach
Role of cell engraftment vs exposure to stem cell conditioned medium
Optimization of cell type targeted
Donor cells both produce growth factors (e.g., VEGF) and induce production by recipient cells
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Novel Strategies for BPD
Control of inflammation
Inositol
Elastase inhibition
Antioxidants
Stem cell therapy
Enhancement of NO bioactivity
![Page 49: Past, Present & Future · N Engl J Med 1971; 284:1333-1340 June 17, 1971 . ... Death during first 28 days Survival up to 28 days with BPD without BPD 26 26 55 13 20 81 0.012 .022](https://reader033.vdocuments.us/reader033/viewer/2022050117/5f4dc5a530e40c60d30ad6a8/html5/thumbnails/49.jpg)
Proposed Effects of Nitric Oxide on the Development of the Respiratory System
Martin, N Engl J Med 2005
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NIH Consensus Development Conference: Inhaled Nitric Oxide for Premature Infants
“Available evidence does not support use of iNO in routine care of premature infants who require respiratory support”.
“Future research should seek to understand the gap between benefits on lung development and function suggested by basic research and animal studies, and the results of clinical trials to date”.
Pediatrics 2011
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Collagen synthesis
Smooth muscle relaxation
Urea
L-citrulline
GTP sGC
cGMP
GDP
H2O
Cell proliferation
Arginase
NOS
NOS and Arginase Compete for the Substrate L-Arginine
L-ornithine
L-Arginine NO
Proline Polyamine
+
PDE5
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Collagen synthesis Smooth muscle
relaxation
Urea
L-citrulline
GTP sGC
cGMP
GDP
H2O
Cell proliferation
Arginase
NOS
NOS and Arginase Compete for the Substrate L-Arginine: Effect of Hyperoxia
L-ornithine
L-Arginine NO
Proline Polyamine
+
PDE5
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Potential Alternate Approaches to Enhance Endogenous NO Bioactivity
Arginine supplementation
Arginase inhibition
Phosphodiesterase inhibition
e.g., Sildenafil
Complementary antioxidant
Ethyl nitrite inhalation as a source of nitrosothiols
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The Preterm Lung
Historical successes
Antenatal steroids
Postnatal surfactant
Ventilatory support
Ongoing strategic challenges
Spectrum of neonatal lung disease
Novel therapeutic approaches
Longer term respiratory outcome
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“Most adolescents and young adults who had bronchopulmonary dysplasia in infancy have some degree of pulmonary dysfunction, consisting of airway obstruction, airway hyperreactivity, and hyperinflation. The clinical consequences of this dysfunction are not known.”
W. H. Northway Jr., et al. NEJM 1990
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“Although the aetiology and clinical course of BPD have changed during the past four decades, respiratory dysfunction continues to be observed. The largely obstructive nature of this dysfunction has long term implications for future lung health”.
UK EPICure Study data 2010
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160
140
120
100
80
60
40
20
0
FE
V1%
p<0.0001 p<0.0001
Airway Hyperresponsiveness in School Children Born Very Preterm
Pelkonen AS, Am J Resp Crit Care Med 1997
Non-BPD BPD Controls
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Asthma at School Age in ELBW Infants Born in the 1990’s
0
10
20
30
40
50
ELBW (n=219)
TERM CONTROLS (n=176)
OR 3.0, 95% CI 1.6-5.6, p=0.001
Ast
hm
a
Rate
* (
%)
Hack et al, JAMA 2005 * need for medication
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Incidence of Clinically Significant Airflow Reduction in Late Adolescence in VLBW (<1.5kg) Subjects
0
5
10
15
20
25
30
35
40
45
50
Per
cen
t w
ith
FE
V1 <
75%
Doyle, Pediatrics 2006
BPD No BPD
p=0.001
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Ventilation
(baro/volutrauma)
Oxygen
(oxidant/antioxidant balance)
Infection
(pre/postnatal)
Impaired Airway Structure and Function
Altered pulmonary
vasculature
Alveolar remodeling
Structural
Immaturity
Inflammatory
Response
Biochemical
Imbalance
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Biologic Contributors to Altered Airway Function in Former Preterm Infants
Lung parenchymal injury
Selective contribution from airway smooth
muscle
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Altered Neonatal Airway Function: Lung Parenchymal Injury
Colin, A. A. et al. Pediatrics 2010
Airway
Pleural
Space
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Effect of Neonatal Hyperoxia on Bronchiolar-Alveolar Attachments in 10 Month Old Mice
[65% oxygen from birth to DOL 7]
O’Reilly M: Neonatology 105:39, 2014
Control Hyperoxia
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Effect of 7-Day Oxygen Exposure in Mice on Lung Structure at 3 Weeks
Ctrl 40% O2 70% O2
Wang H: Am J Physiol: Lung Cell Mol Physiol, 2014
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Mild and Severe Hyperoxia Both Impair Subsequent Lung Structure in Mouse Pups
Wang H: Am J Physiol Lung Cell Mol Physiol 2014
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Mild Hyperoxia Markedly Increases Subsequent Airway Hyperreactivity in Mouse Pups
Wang H: Am J Physiol Lung Cell Mol Physiol 2014
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Mild Hyperoxia Markedly Increases Airway Smooth Muscle [ASM] in Mouse Pups
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Predisposition to Later “Wheezing Disorders”
Neonatal hyperoxia
Selective ASM proliferation
Alveolar simplification
Decreased bronchiolar-alveolar attachments
Airway hyperreactivity
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Predisposition to Later “Wheezing Disorders”
Neonatal hyperoxia
Selective ASM proliferation
Alveolar simplification
Decreased bronchiolar-alveolar attachments
Airway hyperreactivity
BPD non-BPD
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Recommendations: Clinical
Protect the immature airway against environmental hazards/infectious agents
Recognize risk of wheezing in the moderately low birth weight/late preterm infant
Recognize the increased risk of sleep disordered breathing in former preterm infants
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Speculation
Modest therapeutic interventions in the NICU, e.g., sustained low FiO2 and/or CPAP may predispose to selective airway smooth muscle proliferation and resultant symptomatology
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Obrigado