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成骨不全成年患者的肺功能:一项队列研究。

Lung function in adult patients with osteogenesis imperfecta: a cohort study.

作者信息

Lenoir Alexandra, Aubry-Rozier Bérengère, Bregou Aline, Gonzalez Rodriguez Elena, Paquier Célia, Tanniger Joëlle, Faouzi Mohamed, Lazor Romain

机构信息

Department of Medicine V, LMU University Hospital, LMU, Munich, Germany.

Department of Genetic Medicine, Lausanne University Hospital and University of Lausanne, Lausanne, Switzerland.

出版信息

Orphanet J Rare Dis. 2024 Dec 4;19(1):455. doi: 10.1186/s13023-024-03452-y.

Abstract

BACKGROUND

Osteogenesis imperfecta (OI) is a rare hereditary bone disease resulting from a defect in collagen synthesis or processing, leading to bone fragility, frequent fractures and skeletal deformities. OI is associated with increased respiratory morbidity and mortality, but the mechanisms of lung involvement are poorly understood, and there are no data on the natural history of lung function. We studied lung function over time in a cohort of adult OI patients at one center.

METHODS

We used data from OI patients aged 15 and above followed up at the Lausanne university hospital between 2012 and 2023 with available pre-bronchodilator spirometry. Associations between spirometric measurements at first visit and clinical characteristics were studied through linear regression. Changes of spirometric variables over time were analysed through mixed linear regression. Models were adjusted for age, sex, height and OI type (Sillence classification).

RESULTS

Among 46 subjects, 24% had impaired spirometry at baseline, with similar distribution between restrictive (8.7%), obstructive (8.7%) and mixed (6.5%) ventilatory patterns. At first visit, higher age was associated with lower FEV (β = -0.019 l, p = 0.014) and lower FEV/FVC (β = -0.175%, p = 0.012). A history of asthma was associated with higher FEV (β = 0.636 l, p = 0.028) and FVC (β = 0.834 l, p = 0.010). At first visit, FEV (β = -0.750 l, p = 0.006) and FVC (β = -0.859 l, p = 0.004) was lower in individuals with OI Sillence types 3, 4 or 5 compared to type 1. Over a mean follow-up of 3.4 years, smokers had a greater decline of FEV/FVC compared to non-smokers (β = -6.592%, p = 0.007). Individuals with a mutation in the gene COL1A2 had 740 ml lower FVC compared to those with a mutation in COL1A1 (p = 0.037). After adjustment for sex, age, height and OI type, FEV increased by 26 ml (95% CI 8; 45) or 1.28%pred (0.51; 2.05) and FVC increased by 25 ml (95% CI 8; 43) or 0.93%pred (0.31; 1.55) per year of follow-up.

CONCLUSIONS

An increase of FEV and FVC over time was observed in OI patients after adjustment for other variables, suggesting that the defective collagen synthesis may impact the pulmonary interstitium and lead to increased lung compliance and hyperinflation, in contrast to skeletal deformities, which reduce the thoracic volume. Lung function changes in OI thus result from the interplay of several mechanisms.

摘要

背景

成骨不全症(OI)是一种罕见的遗传性骨病,由胶原蛋白合成或加工缺陷引起,导致骨脆性增加、频繁骨折和骨骼畸形。OI与呼吸疾病的发病率和死亡率增加有关,但肺部受累的机制尚不清楚,且尚无关于肺功能自然史的数据。我们在一个中心对一组成年OI患者的肺功能进行了长期研究。

方法

我们使用了2012年至2023年在洛桑大学医院随访的15岁及以上OI患者的数据,这些患者有支气管扩张剂使用前的肺功能测定数据。通过线性回归研究首次就诊时肺功能测定指标与临床特征之间的关联。通过混合线性回归分析肺功能变量随时间的变化。模型根据年龄、性别、身高和OI类型(Sillence分类)进行了调整。

结果

在46名受试者中,24%在基线时肺功能测定受损,限制性(8.7%)、阻塞性(8.7%)和混合性(6.5%)通气模式的分布相似。首次就诊时,年龄较大与较低的第一秒用力呼气容积(FEV)(β = -0.019升,p = 0.014)和较低的FEV/用力肺活量(FVC)(β = -0.175%,p = 0.012)相关。哮喘病史与较高的FEV(β = 0.636升,p = 0.028)和FVC(β = 0.834升,p = 0.010)相关。首次就诊时,与1型相比,3、4或5型OI患者的FEV(β = -0.750升,p = 0.006)和FVC(β = -0.859升,p = 0.004)较低。在平均3.4年的随访中,吸烟者的FEV/FVC下降幅度大于非吸烟者(β = -6.592%,p = 0.007)。与COL1A1基因突变者相比,COL1A2基因突变者的FVC低740毫升(p = 0.037)。在调整性别、年龄、身高和OI类型后,随访每年FEV增加26毫升(95%置信区间8;45)或预测值的1.28%(0.51;2.05),FVC增加25毫升(95%置信区间8;43)或预测值的0.93%(0.31;1.55)。

结论

在调整其他变量后,观察到OI患者的FEV和FVC随时间增加,这表明有缺陷的胶原蛋白合成可能影响肺间质,导致肺顺应性增加和肺过度充气,这与减少胸廓容积的骨骼畸形相反。因此,OI患者的肺功能变化是多种机制相互作用的结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d703/11616175/ad8a260f8df6/13023_2024_3452_Fig1_HTML.jpg

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