描述与早产相关的肺疾病的气道阻塞、突触障碍和 PRISm 表型。
Characterising airway obstructive, dysanaptic and PRISm phenotypes of prematurity-associated lung disease.
机构信息
Department of Child Health, Cardiff University School of Medicine, Cardiff, UK.
MRC Integrative Epidemiology Unit, Population Health Sciences, Bristol Medical School, University of Bristol, Bristol, UK.
出版信息
Thorax. 2023 Sep;78(9):895-903. doi: 10.1136/thorax-2022-219301. Epub 2023 Feb 1.
INTRODUCTION
Although obstructive airway disease has been shown to be associated with prematurity, other spirometry phenotypes are less well described.
OBJECTIVES
We characterised abnormal spirometry phenotypes in preterm-born children, including prematurity-associated obstructive lung disease (POLD, forced expiratory volume in 1 s (FEV)<lower limit of normal (LLN), FEV/forced vital capacity (FVC)<LLN), prematurity-associated preserved ratio of impaired spirometry (pPRISm, FEV<LLN, FEV/FVC≥LLN) and prematurity-associated dysanapsis (pDysanapsis, FEV≥LLN, FEV/FVC<LLN), and associated them with early life factors, bronchodilator responsiveness and fractional exhaled nitric oxide (FE).
METHODS
768 children, aged 7-12 years, underwent FE measurements and spirometry before and after salbutamol. Groups were compared using parametric tests; multinomial regression was used.
RESULTS
22.6% of 544 preterm-born (mean gestation: 31 weeks) and 9.2% of 195 term-born children, with satisfactory data available, were classified into one of four abnormal spirometry groups. Each phenotype was generally more prevalent in preterm-born children than in the term-born children. For the preterm group, POLD-reversible (4.4%) was associated with increased FE, bronchopulmonary dysplasia (BPD) and intrauterine growth restriction. POLD-fixed group (3.3%) did not have increased FE but was associated with BPD. 41% of the pDysanapsis group (5.9%) had bronchodilator response, 31% had increased FE and was associated with postnatal weight gain. In the pPRISm group (9%), 13% responded to bronchodilators, FE was not increased and was non-significantly associated with body mass index (p=0.064).
CONCLUSIONS
Further to airway obstruction, we describe airway dysanapsis and pPRISm spirometry phenotypes in survivors of prematurity, both of which have poor outlook in other disease groups. By identifying specific phenotypes, targeted therapy can be developed to improve long-term outcomes.
简介
尽管阻塞性气道疾病与早产有关,但其他肺量计表型的描述较少。
目的
我们描述了早产儿的异常肺量计表型,包括与早产相关的阻塞性肺疾病(POLD,1 秒用力呼气量(FEV)<正常下限(LLN),FEV/用力肺活量(FVC)<LLN)、与早产相关的受损肺量计比保留率(pPRISm,FEV<LLN,FEV/FVC≥LLN)和与早产相关的呼吸功能不全(pDysanapsis,FEV≥LLN,FEV/FVC<LLN),并将其与早期生活因素、支气管扩张剂反应性和呼出气一氧化氮分数(FE)相关联。
方法
768 名 7-12 岁的儿童在沙丁胺醇治疗前后进行了呼出气一氧化氮(FE)和肺量计检测。采用参数检验比较各组;采用多项回归分析。
结果
在 544 名早产儿(平均胎龄 31 周)和 195 名足月出生的儿童中,22.6%和 9.2%的儿童有可接受的数据,他们被分为四种异常肺量计表型之一。每个表型在早产儿中的发生率普遍高于足月出生的儿童。对于早产儿组,POLD-可逆组(4.4%)与 FE 增加、支气管肺发育不良(BPD)和宫内生长受限有关。POLD-固定组(3.3%)FE 不增加,但与 BPD 有关。41%的 pDysanapsis 组(5.9%)有支气管扩张剂反应,31%有 FE 增加,与出生后体重增加有关。在 pPRISm 组(9%)中,13%的儿童对支气管扩张剂有反应,FE 没有增加,与体重指数(p=0.064)无显著相关性。
结论
除了气道阻塞外,我们还描述了早产儿幸存者的气道功能不全和 pPRISm 肺量计表型,这两种表型在其他疾病组的预后较差。通过识别特定的表型,可以开发针对性的治疗方法,以改善长期预后。
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