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Infants with chronic neonatal lung disease: recommendations for the use of home oxygen therapy

Dominic A Fitzgerald, R John H Massie, Gillian M Nixon, Adam Jaffe, Andrew Wilson, Louis I Landau, Jacob Twiss, Greg Smith, Claire Wainwright and Margaret Harris
Med J Aust 2008; 189 (10): 578-582. || doi: 10.5694/j.1326-5377.2008.tb02186.x
Published online: 17 November 2008

This is a position statement developed by the working party (the authors, chaired by Dominic Fitzgerald) of the Australasian Paediatric Respiratory Group (APRG) within the Thoracic Society of Australia and New Zealand (TSANZ). We performed a MEDLINE search with the keywords bronchopulmonary dysplasia, chronic neonatal lung disease and home oxygen among articles dated from 1966 to July 2007. Sixty-two articles were identified, of which 23 publications of relevance were considered. Levels of evidence were derived and designated E1–E4 (according to the ratings of the National Health and Medical Research Council [NHMRC]1). The position statement was presented in a workshop at the annual meeting of the APRG. All co-authors provided additional comments from their respective centres. A revised manuscript was circulated to the entire group for final comment before further peer review and endorsement by the Clinical Care and Resources Subcommittee of the TSANZ. A summary of our recommendations is provided in the Box at the end of this article. This document is due for review in 2012.

The development of home oxygen programs for infants born prematurely who have chronic neonatal lung disease (CNLD) followed the successful introduction of such schemes for adults with chronic obstructive pulmonary disease.2,3 In adults, long-term home oxygen therapy is prescribed for the relief of breathlessness in the presence of hypoxia, defined by an arterial oxygen tension (Pao2) of less than 55 mmHg (7.3 kPa; an oxygen saturation [Spo2] level of ≤ 88%).4 In contrast, the assessment of home oxygen requirements for infants involves a combination of clinical assessment, oximetry and intermittent blood gas analyses5,6 (levels of evidence, E3, E41).

The first significant report on the utility of home oxygen therapy for children was published in 1976, and it reported on the use of home oxygen therapy in children with CNLD allowing earlier discharge from hospital5 (E3). Over the past 30 years, small-scale home oxygen programs were developed to shorten hospitalisation and reduce health care costs for young infants with CNLD6 (E3). However, there remains little objective evidence to guide the use of home oxygen therapy in infants with CNLD.

Features of chronic neonatal lung disease
Predominantly a consequence of preterm birth

Most infants with CNLD are born prematurely (< 28 weeks’ gestation) at extremely low birthweight (< 1000 g).7 CNLD results from a combination of arrested pulmonary development occurring as a consequence of antenatal factors, preterm delivery coupled with ventilator-induced barotrauma, volutrauma, oxygen toxicity and complications of persistent patent ductus arteriosus, lower respiratory tract infections and, possibly, undetermined genetic susceptibilities to chronic lung disease.7-10

Can CNLD occur in a full-term infant?

CNLD is a descriptive term rather than a histopathological dia-gnosis.7 Positive-pressure ventilation delivered at high pressure and a high concentration of inspired oxygen used in full-term infants may also result in CNLD.11,12 Conditions that may require home oxygen therapy in full-term infants include structural lung disease, meconium aspiration syndrome with pulmonary hypertension, or severe cyanotic congenital heart disease.6

Phenotype and pathophysiology of CNLD

The predominant clinical findings in infants with CNLD are tachypnoea, wheeze, cough, chest wall retractions, and paradoxical respirations7-9,13-19 that occur as a consequence of small airways disease (airflow obstruction, hyperplasia of bronchial epithelium, increased mucus production from glandular hyperplasia, decreased mucociliary clearance and bronchial hyper-reactivity).7-9,11,12 Additional complications may include parenchymal and interstitial lung damage, dynamic obstruction from degrees of bronchomalacia, and fixed obstruction from subglottic narrowing related to damage from endotracheal tube positioning and frequent suctioning.7,8 Other abnormalities include increased dead space ventilation, decreased lung compliance, maldistribution of ventilation and increased work of breathing, and ventilation–perfusion mismatching.7,8,14

Demographic characteristics of CNLD

CNLD is the commonest form of chronic lung disease in infancy, occurring in up to 20% of infants with respiratory distress syndrome12 and about 40%–50% of infants born at less than 28 weeks’ gestation.13 The risk of CNLD increases with decreasing gestational age and decreasing birthweight.8,11 CNLD has been reported in up to 85% of infants with birthweights of 501–750 g, up to 45% of infants with birthweights of 751–1000 g, but decreasing to 5% of infants with birthweights over 1500 g.5,8,11,12

Estimated extent of CNLD in Australasia

Supplemental oxygen is used in neonatal intensive care units for over 95% of infants born before 28 weeks’ gestation in Australia and New Zealand.13 Supplemental oxygen is required by about 75% at 28 days of life and 50% at 36 weeks’ postmenstrual age. The median (interquartile range) duration of supplemental oxygen therapy in infants born before 28 weeks’ gestation is 53 days (12–95 days).13 The survival rate to discharge from hospital for infants born at 27 weeks’ gestation or later is at least 90%.13 In Australasia, 214 babies were discharged on home oxygen therapy in 2004, which represented 6.1% of survivors born at less than 32 weeks’ gestation (Robert Halliday, Neonatologist, The Children’s Hospital at Westmead, Sydney, personal communication). The proportion of preterm infants being discharged on home oxygen therapy varies widely between neonatal units, and is largely dependent on target oxygenation strategies.7,10,16,17

Determining adequate oxygenation

Intermittent oximetry is unreliable and should not be used as the basis for determining adequate oxygenation. Continuous oximetry provides better screening information.7 More information can be determined from polysomnography, which may provide an objective physiological measure of the impact of different oxygen levels on the carbon dioxide profile and sleep quality.7,18,19

Just as the oxygenation threshold for providing home oxygen therapy varies, so do the indications for home oxygen therapy. However, these commonly include lung disease, pulmonary hypertension and retinopathy of prematurity (ROP).7,8,20,21 It is unclear whether recommendations based on evidence acquired from the Benefits of Oxygen Saturation Targeting (BOOST) trial in preterm infants16 should be extrapolated to a full-term-equivalent age and beyond. In particular, the available data are limited to assessment of growth and development at 12-months corrected age rather than to cognitive outcome at school age.7,15

Thus, despite the existence of home oxygen programs in Australia, New Zealand and overseas, there has been limited consensus on:

Drawing on the limited evidence available, together with the combined views of paediatric respiratory physicians experienced in the care of infants with CNLD, we suggest a practical approach to the provision of home oxygen therapy for infants with CNLD (E4).

Indications for supplemental oxygen therapy
Rationale for the prolonged use of supplemental oxygen in infants with CNLD

The goal of home oxygen therapy is to prevent the effects of chronic hypoxaemia, which include pulmonary vasoconstriction leading to pulmonary hypertension, bronchial constriction leading to airway obstruction, and changes in growth of pulmonary and ocular vasculature.7,8,12 Improved oxygenation may result in improved lung growth and repair.7,17 In addition, there is observational evidence to support improved nutrition and somatic growth occurring in response to improved oxygenation.7,17,22 However, the long-term implications for cognitive development of mild hypoxaemia, either persistent or intermittent, have not been adequately studied.

Assessment of gas exchange in infants usually includes a combination of oximetry, transcutaneous carbon dioxide monitoring and venous or capillary blood gas analyses (E4). Arterial blood gas analyses are rarely used after the initial weeks in neonatal intensive care units because of the risks of trauma to the smaller vessels, embolic phenomena and arterial occlusion.

As a safety measure, some physicians will conduct an air challenge for infants immediately before discharge with supplemental oxygen (E4). The purpose of this is to see the nadir of Spo2 reached in room air should oxygen become disconnected.7 Protocols for these air challenges23 vary both in the duration of the challenge and the acceptable nadir of Spo2. Most units would recommend that a minimum Spo2 of greater than 80% be maintained in air for 30 minutes before discharge as a safety check (E4). Once discharged, the tools used to assess readiness for withdrawal of supplemental oxygen include clinical assessment (respiratory rate and growth) combined with continuous overnight oximetry (or polysomnography where available)17,18 (E4).

Target oxygen saturation levels
Evidence for higher and lower target Spo2 levels in CNLD

There are only two randomised controlled trials of supplemental oxygen for infants with CNLD to guide clinicians in setting target Spo2 levels.16,21 The BOOST trial randomly allocated infants born at less than 30 weeks’ gestation with CNLD to target Spo2 levels from 32 weeks’ postmenstrual age — either 91%–94% or 95%–98%.16 Higher target Spo2 levels (95%–98%) increased the median length of oxygen therapy (72 v 56 days; P < 0.0001), the rate of diagnosis of CNLD (64% v 46%; P = 0.0006), and the frequency of home oxygen therapy (30% v 17%; P = 0.004). Higher oxygenation did not afford any benefits in terms of growth or neurodevelopmental measures up to a corrected age of 12 months.16 However, there was no assessment of pulmonary hypertension nor of the relative proportions of adult versus fetal haemoglobin values and the relationship to oxygen-carrying capacity and the oxygenation profiles of the infants.

The only advantage for the infants who received higher target levels of oxygenation in the BOOST trial was in those with significant ROP, who required less ablative retinal surgery.16 This may have occurred because the higher target oxygen zone minimised the frequency and extent of swings in oxygenation, which has been shown in an animal model to contribute to ROP.20 This finding that a higher Spo2 was protective was consistent with the other trial of supplemental oxygen for premature infants, the Supplemental Therapeutic Oxygen for Prethreshold Retinopathy of Prematurity (STOP-ROP) trial.21 In this study, the effect of an Spo2 range of 89%–94% was compared with a range of 96%–99% in preterm infants with prethreshold ROP for a minimum of 2 weeks to see whether this influenced the progress of retinopathy. It did not, with the exception of a post-hoc analysis that suggested some benefit of higher Spo2 for infants without plus disease (tortuous and dilated vessels in at least two quadrants of the posterior pole), with a 30% lower rate of progression. However, it was noted that the respiratory morbidity (rates of pneumonia or exacerbations of CNLD) of the infants in the higher target Spo2 range was 50% higher (13.2% v 8.5%). In addition, infants in the higher target Spo2 range at 50 weeks’ postmenstrual age (approximately 8 months corrected age) were more likely to remain hospitalised (12.7% v 6.8%), on supplemental oxygen (46.8% v 37.0%) and on diuretics (35.8% v 24.4%).21 Infants in the STOP-ROP trial who were in the higher Spo2 range had a greater incidence of chest infections,21 raising the possibility that even low-flow nasally delivered oxygen may be toxic to respiratory epithelium.

Based on this information, our recommendation is to target a minimum mean Spo2 level of 93%–95% in infants with CNLD, as measured by continuous overnight oximetry. Despite this minimum target Spo2, some infants may have persistent tachypnoea, increased work of breathing, frequent oxygen desaturations during sleep, pulmonary hypertension and poor growth, which may require a higher target Spo2 level5-7,17-19,23 (E3,E4).

Duration of supplemental oxygen therapy

As infants are more vulnerable to hypoxaemia when feeding, sleeping and bathing,7,8,15-17 most clinicians would continue supplemental oxygen 24 hours a day until the infant is ready for weaning from the oxygen therapy (E4). However, if the infant is older (ie, closer to a corrected age of 12 months) and ambulant, restricting nasal catheter oxygen to sleep times may be practical6 (E4). This is not a common issue as most infants with CNLD in Australia and New Zealand are weaned from supplemental oxygen by a corrected age of 6 months.

Logistics and ongoing care
Delivery of supplemental oxygen

It is uncommon in most parts of Australasia for infants to be discharged from hospital until they have an oxygen requirement of 0.5 litres per minute or less.15 Supplemental oxygen is delivered by means of a nasal cannula for those receiving oxygen, usually at flow rates of 0.5 litres per minute or less, but this can be increased to 2 litres per minute if needed during a chest infection (E4). At oxygen flows of 0.5 litres per minute or less, humidification is rarely required. However, delivery of oxygen by nasal cannula may lead to nasal inflammation and trauma, especially in the presence of an intercurrent viral upper respiratory tract infection.7,12,14

A fixed oxygen concentrator may be viewed as a reliable and cheaper alternative for delivering oxygen in the child’s bedroom (E4). However, they are noisy, and the direct cost to the family for the electricity required should be considered. Portable oxygen cylinders are also needed to allow outings from the house8,14,15 and in case of power failures (for which priority reconnection to houses with CNLD infants can be arranged with local power authorities). Access to portable generators may be a consideration for CNLD infants living in regional areas. State-funded programs generally meet the cost of supplemental oxygen therapy in Australia and New Zealand. Most programs require a small financial contribution by families for consumables such as nasal catheters and disposable tubing. There is no funding for home oximeters.

Team approach to the care of infants in a home oxygen program

Many infants with CNLD who are discharged on home oxygen therapy will have other complications of their preterm birth and will need ongoing supervision by a well resourced multidisciplinary team.15 However, the availability of multidisciplinary teams to support home oxygen programs for infants with CNLD in Australasia varies considerably, primarily due to funding constraints.

Fitness to fly

Air travel results in a mildly hypoxic environment where cabin pressure equivalent to 1500–2500 metres results in an equivalent fraction of inspired oxygen (Fio2) of about 15%–17% of that at sea level.25 This can be simulated in a respiratory laboratory with the infant and parent seated in a body plethysmograph, where inspired oxygen is diluted with nitrogen to give an Fio2 of about 15%, while oximetry is measured continuously over 20 minutes.25,26 Nasal prong oxygen can be titrated to achieve satisfactory Spo2 levels. If such a test is not readily accessible and the infant is flying for longer than an hour, supplemental oxygen could be increased by 0.25 litres per minute or provided at 0.25 litres per minute for the flight if the infant has ceased supplemental oxygen therapy in the past 3 months (E4).

Long-term outcomes of oxygen supplementation strategies applied in infancy

Infants with CNLD who require home oxygen therapy have been found to use more health care resources and have delayed developmental progress in the preschool years compared with infants with CNLD who did not require home oxygen therapy.29-31 An Australasian register of infants with CNLD is needed to document baseline practice and subsequently study proposed parameters for home oxygen therapy and outcome measures to school age. Ideally, this would incorporate the expertise of neonatologists, respiratory and general paediatricians, and allied health care professionals cooperating in designing appropriate randomised controlled trials of target Spo2 levels and weaning strategies to assess not only short-term measures like weight and length, but more important long-term outcomes like pulmonary hypertension, respiratory function, exercise capacity and neurocognitive function.32,33

  • Dominic A Fitzgerald1
  • R John H Massie2,3
  • Gillian M Nixon4,5
  • Adam Jaffe6,7
  • Andrew Wilson8,9
  • Louis I Landau8,9
  • Jacob Twiss10,11
  • Greg Smith12
  • Claire Wainwright13,14
  • Margaret Harris14,15

  • 1 Department of Respiratory Medicine, The Children’s Hospital at Westmead, Sydney, NSW.
  • 2 Royal Children’s Hospital, Melbourne, VIC.
  • 3 University of Melbourne, Melbourne, VIC.
  • 4 Monash Medical Centre, Melbourne, VIC.
  • 5 Monash Institute of Medical Research, Monash University, Melbourne, VIC.
  • 6 Sydney Children’s Hospital, Sydney, NSW.
  • 7 School of Women’s and Children’s Health, University of New South Wales, Sydney, NSW.
  • 8 Princess Margaret Hospital, Perth, WA.
  • 9 School of Paediatrics and Child Health, University of Western Australia, Perth, WA.
  • 10 Starship Children’s Health, Auckland, New Zealand.
  • 11 Department of Paediatrics, University of Auckland, Auckland, New Zealand.
  • 12 Women’s and Children’s Hospital, Adelaide, SA.
  • 13 Children’s Respiratory Centre, Royal Children’s Hospital, Brisbane, QLD.
  • 14 Department of Paediatrics and Child Health, University of Queensland, Brisbane, QLD.
  • 15 Mater Children’s Hospital, Brisbane, QLD.


Correspondence: dominif2@chw.edu.au

Acknowledgements: 

Members of the Australasian Paediatric Respiratory Group, all of whom contributed in presentations and in manuscript drafting and revisions, include — Alice Springs, Northern Territory: R Rosebury. Adelaide, South Australia: A J Martin, J D Kennedy, G Smith, R Staugas. Brisbane, Queensland: D M Cooper, C Daikin, L Gauld, M Harris, S Suresh, A Chang, N Dore, P Francis, A Isles, B Masters, C Wainwright. Canberra, Australian Capital Territory: T McDonald, L Teoh. Melbourne, Victoria: D Armstrong, N Freezer, R J H Massie, G Nixon, S Raganathan, C Robertson, P Robinson, S Sawyer, M Griffiths. Newcastle, New South Wales: T Gulliver, J Hilton, B Whitehead. Perth, Western Australia: B Clements, L Landau, P LeSouef, P D Sly, S M Stick, A Wilson. Sydney, NSW: H Allen, P Cooper, P Field, D A Fitzgerald, A Kemp, C Mellis, H Selvadurai, P Van Asperen, K Waters, Y Belessis, A Jaffe, M Haifer, J Morton, A Numa. Auckland, New Zealand: I Asher, C Byrnes, E Edwards, J Twiss. Christchurch, New Zealand: P Pattemore.

Competing interests:

None identified.

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