Lung Function Tests in Neonates and Infants with Chronic Lung Disease of Infancy: Functional Residual Capacity

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Summary. Rationale: With increasing use of infant pulmonary function tests (IPFTs) in both clinical and research studies, appropriate interpretation of results is essential. Objectives: To investigate the potential bias associated with ''normalising'' IPF by expressing results as a ratio of body size and to develop reference ranges for tidal breathing parameters, passive respiratory mechanics (compliance [C rs ] and resistance [R rs ]) and plethysmographic functional residual capacity (FRC p ) for white infants during the first 2 years of life. Methods: IPFTs were measured using the Jaeger BabyBody system and standardized protocols. Reference equations, adjusted for body size, age, and sex where appropriate, were created using multilevel modeling. Results: The ratio of lung function to body length changes markedly with growth, thereby precluding its use for any outcome. While the ratio of tidal volume and C rs to body weight remained relatively constant with growth, this was not the case for FRC p . Even in healthy infants, a strong inverse relationship was observed between lung function/body weight and weight z-score which could distort interpretation of results in growth-restricted infants with lung disease, such as cystic fibrosis. Reference equations were derived from 153 healthy white infants on 232 test occasions (median age 35.5 weeks [range: 2.6-104.7]). Crown-heel length was the strongest predictor of IPF. Conclusions: When reporting IPF, use of size-corrected ratios should be discouraged, with interpretation instead based on appropriate reference equations. The current equations are applicable to white infants and young children up to 2 years of age, studied using the same commercially available equipment. The extent to which these equations are applicable to infants and young children of other ethnic backgrounds or who are tested with different equipment needs to be established.

Section: Passive Respiratory Mechanicsmentioning

confidence: 92%

New reference equations to improve interpretation of infant lung function

Nguyen¹,

Hoo²,

Lum³

et al. 2012

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“…[8][9][10][11]13,14 Problems in study design, including failure to recruit sufficient subjects or appropriate controls, ambiguity regarding the definition of CLDI, 3,[19][20][21] or true clinical status at time of testing, 22 use of inappropriate equipment or methods with respect to underlying pathophysiology and lack of data on repeatability with which to interpret what constitutes a clinically significant change, 14,15 have all contributed to contradictory results and difficulties in drawing firm conclusions from many of the published studies in this field. If we are to avoid such problems in the future, there is an urgent need for collaboration between clinicians and physiologists to facilitate optimal use of the exciting technological developments.…”

Section: Limitations Of Published Studiesmentioning

confidence: 99%

“…The importance of assessing lung volume in this challenging population has long been recognized, with firm evidence that acute neonatal lung disease is characterized by severely reduced functional residual capacity (FRC). 10 While FRC may remain reduced in established CLDI, more commonly it becomes normalized or even elevated due to hyperinflation, with or without gas trapping, secondary to airway obstruction. Unfortunately, interpretation of these findings and their use in guiding clinical management is still limited by difficulties in 'normalizing data' according to body size and maturation.…”

Section: Introductionmentioning

confidence: 99%

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Lung function in infants and young children with chronic lung disease of infancy: The next steps?

Stocks

Coates

Bush

2006

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Summary. Over the past year, a series of papers have reviewed the literature concerning assessment and interpretation of lung function in infants and young children with chronic lung disease of infancy. This manuscript, which represents the final paper in that series, summarizes the findings to date and highlights key areas for future research. Despite the huge literature in this field, interpretation of results and their use in guiding clinical management are still limited by difficulties in 'normalizing data' according to body size and maturation and selection of appropriate control groups. Furthermore, sensitive tests that more closely reflect the underlying pathophysiology of 'new' bronchopulmonary dysplasia, together with simple and reliable methods of assessing lung maturity at birth and true oxygen requirements at specified time points are urgently required. Research in this field is also challenged by the need to separate the independent effects of genetic predisposition, gene-environment interactions, preterm delivery, neonatal respiratory disorders and various treatment strategies on the growing lung. The extent to which disruption of lung growth following premature exposure to the extra-uterine environment leads to an earlier or more aggravated decline in respiratory function in later adult life remains to be elucidated. Whatever its origin, given the increasing survival of smaller and more immature infants, the long term sequelae of neonatal lung disease, are likely to continue to change, requiring ongoing, carefully designed longitudinal studies. Future research strategies need to encompass a multicenter, multidisciplinary, collaborative approach with closer links between clinicians and basic scientists, to ensure that the most relevant research questions are addressed using appropriate methodology and that findings are implemented into clinical practice in a more timely fashion. Pediatr Pulmonol.

“…11 Such a technique, although demonstrating infants with respiratory distress syndrome have low lung volumes and their response to such treatment strategies as addition of positive end expiratory pressure, 12 may under-record lung volumes if there is an elevated respiratory resistance, as suboptimal gas diffusion occurs in lung units with long time constants. Assessment of lung area by calculation of chest radiograph (CXR) thoracic areas avoids such a problem.…”

Section: Introductionmentioning

confidence: 99%

Chest radiograph thoracic areas and lung volumes in infants developing bronchopulmonary dysplasia

May

Prendergast

Salman

et al. 2008

Summary. Objectives: To determine whether chest radiograph (CXR) thoracic areas and lung volumes differed between infants who did and did not develop BPD and according to the severity of BPD developed. Working Hypothesis: Infants developing BPD, particularly if moderate or severe, would have low CXR thoracic areas and lung volumes in the perinatal period. Study Design: Prospective study. Patient-Subject Selection: 53 infants with a median gestational age of 28 (range 24-32) weeks. Methodology: CXR thoracic areas were calculated using a Picture Archiving and Communicating System (PACS) and lung volume assessed by measurement of functional residual capacity (FRC) in the first 72 hr after birth. BPD was diagnosed if the infants were oxygen dependent beyond 28 days, mild BPD in infants no longer oxygen dependent at 36 weeks postmenstrual age (PMA) and moderate/severe BPD in infants who required supplementary oxygen with or without respiratory support at 36 weeks PMA. Results: Thirty two infants developed BPD, 21 had moderate/severe BPD. The median CXR thoracic areas were higher (P < 0.0001) and FRCs were lower (P < 0.0001) in the BPD compared to no BPD infants. The median CXR thoracic areas of the moderate/severe group (P < 0.001) and the mild group (P < 0.05) were greater than that of the no BPD group and the median FRC of the moderate/severe BPD group was lower than the no BPD group (<0.001) and the mild BPD group (P < 0.05). Conclusion: These results highlight that in the perinatal period infants developing BPD, particularly if moderate/severe, have low functional lung volumes and may have gas trapping, which likely reflects ventilation inhomogeneity.