Progressive damage on high resolution computed tomography despite stable lung function in cystic fibrosis

Study population

Since 1996, Sophia Children's Hospital (Rotterdam, The Netherlands), a tertiary academic hospital has monitored CF patients using annual PFT and biennial HRCT scans. All children with CF who had two HRCT scans (HRCT₁ and HRCT₂) in combination with two routine PFT (PFT₁ and PFT₂) were selected for this follow-up study (n=48). CF was diagnosed by a positive sweat test and/or genotyping for known CF mutations and/or an abnormal potential difference measured across the nasal mucosa. The ethical review board of the hospital approved the study.

Lung structure

All HRCT scans were acquired using a GE Prospeed SXscanner (General Electric Medical Systems, Milwaukee, WI, USA). During the scanning procedure, children were notsedated, they were scanned in the supine position, and instructed to take a deep breath and hold it for ≥5 s. A complete HRCT series contained ∼25 1‐mm thick slices at 10‐mm intervals from lung apex to lung base. Scanning parameters were 120 kV, 160 mA (<9 yrs of age 120 mA), 1‐s scanning time and a field of view of 350 mm (<9 yrs of age 250 mm). Scans were reconstructed with a detail reconstruction algorithm (General Electric Medical Systems) and printed using window width −600 Hounsfield units (HU) and window level 1,500 HU. All HRCT scans were scored in random order by an experienced single observer blinded as to the date of the scan, patient identification and the PFT. Five different HRCT‐scoring systems were used: Castile et al. 2, Brody et al. 3, Helbich et al. 4, Santamaria et al. 5, and Bhalla et al. 6. In a previous study, in which the observer of this study participated, these five scoring systems were shown to be reliable between and within observers 7. All slices were used to score the lung lobes and the lingula 2, 3 or the bronchopulmonary segments of the lung 4–6. The systems score bronchiectasis, bronchial wall thickening, mucous plugging, atelectasis, bulla, cysts, consolidation, acinar nodules, septal thickening and/or air trapping in a semiquantitative fashion. A score of zero means “no abnormalities” in each system. Maximal scores are 92, 100, 27, 29 and 25 for Castile, Brody, Helbich, Santamaria and Bhalla scores, respectively.

Lung function

All PFT were done within 1 month of the HRCT scanning using a Jäger diagnostic system (MasterLab, Jäger, Germany). Most scans were performed on the same day (71 of 96 scans) as the PFT. All HRCT scans were done as part of a routine check-up and thus patients were scanned in a relatively stable condition and not during an exacerbation. PFT results were expressed as percentage of predicted values: forced expiratory volume in one second (FEV₁) 8, forced vital capacity (FVC) 8, forced expiratory flow between 25% and 75% of expiratory vital capacity (FEF_25–75%) 9, airway resistance (R_aw) 10, residual volume (RV) 10, total lung capacity (TLC) and RV/TLC 10. The ratio FEV₁/FVC and the ratio RV/TLC were expressed as a percentage (FEV₁/FVC % and RV/TLC %). Twelve patients were younger than patients studied by Wang et al. 9 in the development of the prediction equation for FEF_25–75%. Body plethysmography (TLC, RV and R_aw) was performed in 33 of the 48 children. Normal lung function was defined as a FEV₁ of >85% predicted.

Lung structure and lung function over time

Data obtained at the first evaluation are reported as HRCT₁ and PFT₁, and data obtained at the second evaluation are reported as HRCT₂ and PFT₂. ΔHRCT is the annual change for a scoring system ((HRCT₂‐HRCT₁)/time interval). To compare the annual changes of the five HRCT‐scoring systems, ΔHRCT was also expressed as a percentage of the maximal obtainable HRCT score for that system. ΔPFT is the annual change expressed as % pred for a lung function parameter ((PFT₂‐PFT₁)/time interval). A positive value for ΔHRCT indicates an increase of structural abnormalities and for ΔPFT an improvement in lung function. ΔHRCT and ΔPFT were evaluated for the whole group and separately for children younger than and older than 10 yrs of age. ΔHRCT and ΔPFT were also evaluated as a function of age and baseline disease severity (HRCT₁ and FEV₁ % pred).

Statistical analysis

For the purpose of this article, the term sensitivity is not used in the statistical sense but rather as a measure of the techniques' ability to track pulmonary disease progression in CF. It was assumed that, on average, CF lung disease would be progressive over 2 yrs and that the method that detected the largest change was most “sensitive”. The relationships between HRCT₁ and PFT₁, HRCT₂ and PFT₂, between ΔHRCT and ΔPFT and between ΔHRCT, ΔPFT, HRCT₁, PFT₁ and age were evaluated using the Spearman correlation coefficient. t‐tests (unpaired) were performed for ΔHRCT and ΔPFT to determine whether HRCT and/or PFT changed significantly in the whole group and for children below andabove 10 yrs of age. Wilcoxon-signed ranks tests were used to determine which of the HRCT abnormalities changed significantly. Statistical significance was set at a p‐value of <0.05. Data are presented as mean±sd and range.

Study population

Characteristics of the 48 children (28 male) are shown in table 1⇓. At HRCT₁, 15 children had normal lung function (31%). HRCT scores were 13.7±8.7, 8.1±6.8, 6.1±2.9, 6.4±3.2 and 6.1±2.9 for Castile, Brody, Helbich, Santamaria and Bhalla, respectively.

Lung structure and lung function over time

All HRCT scores worsened significantly. The mean changes for the whole group expressed as a percentage of the maximal scores were 2.6, 2.2, 3.3, 3.1 and 3.5% per year for Castile, Brody, Helbich, Santamaria, and Bhalla, respectively. Spirometric parameters (ΔFEV₁, ΔFVC, ΔFEF_25–75% and ΔFEV₁/FVC) did not change significantly. RV % pred, RV/TLC % and RV/TLC % pred decreased by 8.9% (p=0.004), 2.4% (p=0.0005) and 0.66% (p<0.0001) per year, respectively. R_aw and TLC did not change significantly. The subgroup analysis of children below and above 10 yrs of age showed the same results, with the exception that RV % pred remained unchanged in the children >10 yrs of age. ΔHRCT and ΔPFT did not differ as a function of baseline disease severity or age, with the exception of significant relationships between age and ΔRV % pred (R=0.53, p=0.001) and between age and ΔRV/TLC % (R=0.46, p=0.008).

Of the HRCT scan parameters only mucous plugging (p=0.001) and the severity (p=0.005), extent (p<0.0001) and peripheral extension (p=0.02) of bronchiectasis worsened significantly. Of the 48 patients, the severity of bronchiectasis increased in 15, the score for the extent of bronchiectasis increased in 19 and the score for the peripheral extension of bronchiectasis increased in eight. In only three patients there was a reduction of the severity of bronchiectasis (in all three cases, the airway lumen diameter changed from ∼2–3‐times vessel diameter to ∼1–2‐times vessel diameter). One patient showed a reduction in the peripheral extension score.

Correlation between lung structure and lung function

Cross-sectional data showed a significant correlation between HRCT₁ and first FEV₁ (R<−0.49, p<0.0001), and between HRCT₂ and second FEV₁ (R<−0.58, p<0.0001). Longitudinal data showed significant but weak correlation between ΔPFT and ΔHRCT: ΔFEV₁/FVC versus ΔSantamaria (R=−0.31, p=0.04), ΔR_aw versus ΔHelbich (R=0.37, p=0.04), ΔR_aw versus ΔSantamaria (R=0.38, p=0.03), ΔRV versus ΔBrody (R=0.35, p=0.04), ΔRV/TLC versus ΔBrody (R=0.38, p=0.03), and ΔRV/TLC versus ΔHelbich (R=0.41, p=0.02). The relationship between ΔFEV₁/FVC and ΔSantamaria is shown in figure 1⇓.

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Fig. 1.—

The weak correlation (R=−0.31, p=0.04) between changes in lung function (forced expiratory volume in one second (FEV₁)/forced vital capacity (FVC)) over a 1‐yr period and structural changes on high-resolution computed tomography (HRCT; Santamaria score) is shown. Patients with improved lung function have a change in FEV₁/FVC above 0, and patients with progressive structural lung damage have a Santamaria score above 0.