Severity of scleroderma lung disease is related to alveolar concentration of nitric oxide

K. P. Tiev, J. Cabane, F. Aubourg, A. Kettaneh, M. Ziani, L. Mouthon, S. Duong-Quy, I. Fajac, L. Guillevin, A. T. Dinh-Xuan
European Respiratory Journal 2007 30: 26-30; DOI: 10.1183/09031936.00129806

Abstract

The alveolar concentration of exhaled nitric oxide (CA,NO) is increased in patients with systemic sclerosis (SSc), but whether this increase is related to the severity of interstitial lung disease (ILD) in SSc has not yet been investigated.

In total, 58 SSc patients prospectively underwent pulmonary function tests (PFTs), echocardiogram and fibrosis scoring on pulmonary computed tomography (CT). Patients were divided into two groups according to the presence (or not) of ILD. Measurements of CA,NO were assessed in all SSc patients and compared with those obtained in 19 healthy volunteers. Relationships were sought between CA,NO PFTs and CT scan fibrosis scores.

Overall, CA,NO was significantly increased in SSc patients (median (range) 6.2 (3.8–9.9) ppb) as compared with controls (2.0 (1.2–3.0) ppb). Among SSc patients, CA,NO was significantly higher in patients with ILD compared with patients without ILD (n = 33, 7.5 (5.2–11.9) ppb versus n = 25, 4.9 (3.1–7.0) ppb, respectively). CA,NO was inversely related to total lung capacity (r =  −0.34) and the diffusing capacity of the lung for carbon monoxide (r =  −0.37) and was directly related to CT scan fibrosis scores (r = 0.36).

An increased alveolar concentration of exhaled nitric oxide could, at least in part, either reflect or contribute to the severity of lung disease and could be used to noninvasively assess the extent of interstitial lung disease in systemic sclerosis.

Systemic sclerosis (SSc) is a multi-system disorder of unknown aetiology. It is characterised by fibrosis of the skin and organs including the lungs, heart, gastrointestinal tract and kidneys 1. Interstitial lung disease (ILD) occurs in 35–40% of patients with SSc. Multiple factors such as oxidative stress and chronic inflammation may be responsible for lung injury leading to pulmonary fibrosis, resulting in restrictive lung function and reduced gas lung transfer. The extent of ILD can be evaluated by pulmonary computed tomography (CT), which shows ground-glass attenuation or a reticular fibrosis aspect that are related to the presence of unknown interstitial pneumonia or nonspecific interstitial pneumonia in pathological pulmonary biopsy specimens 2, 3. These CT scan signs, particularly ground-glass attenuation, could reflect the area of the active pulmonary lesion in SSc 4. The pathogenetic aspects of scleroderma lung disease remains unclear and the reversibility of ILD with treatment is uncommon in SSc. Currently, assessment of lung involvement or prognosis in SSc is often difficult and unreliable, with direct evidence of alveolitis or detailed histological diagnosis only provided by invasive means, such as bronchoscopy and bronchoalveolar lavage (BAL) cell count 5 or transbronchial biopsy, which are difficult to perform on a regular basis. Hence, there is a need to develop noninvasive tools with which to assess severity of lung impairment in SSc.

Partitioning of nitric oxide (NO) in the exhaled air 6, 7, into alveolar concentration of exhaled NO (CA,NO) and conducting airway flux (J’aw,NO), can differentiate the anatomic origin of the inflammation, i.e. distinguishing alveoli from inflammatory airways disorders, thus providing a useful tool with which to evaluate the local NO production in respiratory disease. CA,NO is increased in patients with SSc and ILD 8. However, it has not yet been investigated as to whether this increase actually reflects the importance of functional lung impairment and the extent of morphological lung involvement in SSc. Therefore, the aim of the current study was to investigate the relationship between exhaled NO (eNO) levels, detailed lung function testing and high resolution CT fibrosis-scoring in SSc patients. The current authors hypothesised that the degree of lung involvement as assessed by eNO could reflect the extent of ILD in SSc.

METHODS

Subjects

Between November 2004 and December 2005, 58 patients (52 females, six males, median age (1st–3rd quartile) 53.5 (45–60) yrs) who met the American College of Rheumatology criteria for SSc 9, were included in the prospective study conducted in two academic SSc referral centres in France (Hôpital Saint-Antoine and Hôpital Cochin, both Paris). Clinical data, including a modified Rodnan skin score, were collected from all SSc patients (table 1). Patients were divided into two groups according to the presence (or not) of ILD documented by pulmonary CT. In total, 33 SSc patients (55.8 (47.3–60.8) yrs) had ILD and 25 patients (52.4 (44.7–59.0) yrs) had no ILD (table 2). Patients with a recent respiratory tract infection (<3 months) and patients receiving immunosuppressive treatment (cyclophosphamide, mycophenolate mofetil), corticosteroids >10 mg·day−1 or bosentan, were excluded from the present study. Among the 58 enrolled patients with SSc, 11 received low dose corticosteroids (5–10 mg·day−1), and 10 were current smokers. None of the SSc patients had a history of atopy or took NO donors. Measurement of the diffusing capacity of the lung for carbon monoxide (DL,CO) could not be performed in two SSc patients. eNO was measured in all SSc patients and in 19 healthy nonsmoking controls (nine females, 10 males, aged 42.7 (28.1–50.4) yrs). This study was approved by the local ethics committee and all subjects provided informed consent.

View this table:
Table 1—

Alveolar concentration of exhaled nitric oxide(CA,NO) and conducting airway flux of nitric oxide (Jaw,NO) from systemic sclerosis patients (SSc) and healthy volunteers

View this table:
Table 2—

Exhaled nitric oxide(NO) levels from systemic sclerosis (SSc) patients with and without interstitial lung disease (ILD)

Pulmonary CT scanning

All patients underwent a high-resolution CT (HRCT) scan of the lungs in the week prior the measurement of eNO. ILD was considered present if the HRCT scan of the chest demonstrated compatible changes in reticular or air-space opacities. The extent of the individual CT scan patterns was estimated in each lobe with five levels of scoring for ground glass and fibrosis 10 as follows: 0) no abnormality; 1) <5% of the lobe; 2) 6–25% of the lobe; 3) 26–50% of the lobe; 4) 51–75% of the lobe; and 5) 76–100% of the lobe. Ground-glass attenuation was defined as a hazy increase of lung parenchymal attenuation and fibrosis score included lobular septal thickening and subpleural honeycomb change.

Echocardiogram

All patients underwent an echocardiogram (Vivid® 7; G.E Medical Systems, Horten, Norway) in the week prior to measurement of eNO. Pulmonary hypertension was defined by a right ventricular systolic pressure of >40 mmHg on echocardiogram.

Lung function measurement

Pulmonary function tests (PFT; forced vital capacity, forced expiratory volume in one second), DL,CO (MasterScreen® Body; VIASYS Healthcare GmbH, Hoechberg, Germany) and blood gas measurement were performed. PFT parameters were expressed as percentage of predicted normal values 11.

Fractional exhaled NO measurement

NO was measured using a chemiluminescent NO analyser (EndoNO 8000®; SERES, Aix-en-Provence, France), according to a validated method for the online measurement of the exhaled NO fraction (FeNO) in adults 12. After full inspiration on room air with ambient NO levels <20 parts·billion−1 (ppb), the subject exhaled against a positive pressure that was constantly kept between 5–20 cmH2O to generate exhalation flow rates (EFR) of 50, 100, 150 and 200 mL·s−1. For each EFR, the elimination rate of NO (ERNO) was calculated as ERNO =  EFR×FeNO 6, 7. FeNO is inversely related to EFR, whereas ERNO varies directly as a function of EFR. At a flow rate >50 mL·s−1, the latter relationship is linear and can be expressed as ERNO = EFR×FeNO = CA,NO×EFR+Jaw,NO 6, 7. For each patient and control, the R2 values of the relationship between FeNO and EFR were calculated.

Statistical analysis

All results are expressed as median (1st–3rd quartile). Comparisons between the two SSc groups (with and without ILD) and controls were performed by Kruskal–Wallis test. Comparisons between SSc patients with and without ILD, and those between patients with pulmonary hypertension and healthy controls were performed by Mann–Whitney U-test. Correlations between CA,NO and total lung capacity (TLC), ground-glass score, fibrosing score and systolic pulmonary arterial pressure (sPAP) were made by Spearman’s test. A p-value <0.05 was considered as statistically significant.

RESULTS

Demographic characteristics and PFT results are presented in table 1. The median CA,NO was significantly increased in the entire SSc group compared with healthy controls (n = 58, 6.2 (3.8–9.9) ppb versus n = 19, 2.0 (1.2–3.0) ppb, respectively; p<0.001; table 1, fig. 1). The median R2 values of the relationship between FeNO versus EFR were 0.95 for patients and 0.96 for controls. The median Jaw,NO of SSc patients was lower than that of healthy controls (n = 58, 6.3 (-9.8–31.3) nL·min−1 versus n = 19, 35.5 (25.8–54.9) nL·min−1, respectively; table 1). FeNO values measured in SSc patients did not significantly differ from those obtained from healthy controls (10.1 (5.9–17.8) versus 13.1 (11.6–19.6), respectively; table 1).

Fig. 1—
Fig. 1—

Alveolar concentration of nitric oxide (CA,NO) in healthy controls (n = 19) and systemic sclerosis (SSc) patients with (n = 33) or without (n = 25) interstitial lung disease (ILD). **: p<0.01; ***: p<0.001, comparisons between the three groups were made with the Kruskal–Wallis test. Horizontal lines represent median values.

Among the 58 patients with SSc, HRCT images revealed heterogeneous areas of both ground-glass and honeycombing in 33 patients, and were consistent with ILD associated with SSc. TLC was significantly reduced, consistent with restrictive lung disease, in the SSc patients with ILD compared with those without ILD (82 (68–95)% versus 105 (90–107)%, respectively; p<0.001). DL,CO/alveolar volume values were not different between the two groups of SSc patients (table 2). Reticular and ground-glass scores were significantly higher in SSc patients with ILD (7 (4–9) and 8 (6–12), respectively) compared with SSc patients without ILD (p<0.001). CA,NO was significantly higher in SSc patients with ILD compared with SSc patients without ILD (n = 33, 7.5 (5.2–11.9) ppb versus n = 25, 4.9 (3.1–7.0) ppb, respectively; p<0.01). Conversely, Jaw,NO was lower in SSc patients with ILD than in patients without ILD (table 2).

In patients with SSc, CA,NO was inversely related to TLC (r =  -0.34; p<0.01) and DL,CO (r =  -0.37, p<0.01). Furthermore, CA,NO was directly related to radiological indexes of lung fibrosis, i.e. ground-glass attenuation score (r = 0.36; p<0.01) and reticular score (r = 0.33; p<0.05).

No correlation was found between sPAP estimated by echocardiogram and CA,NO. Furthermore, the median level of CA,NO from SSc patients with pulmonary hypertension (sPAP≥40 mmHg) was comparable with that from SSc patients whose sPAP was <40 mmHg (n = 8, 6.9 (5.9–8.9) ppb versus n = 50, 6.0 (3.4–9.0) ppb, respectively). Note that CA,NO from SSc patients with pulmonary hypertension was significantly higher than that from healthy controls (n = 19; 2.0 (1.2–3.0) ppb; p<0.01). The use of low dose corticosteroid, <10 mg·day−1, did not significantly affect the CA,NO treated SSc patients as compared with untreated patients.

DISCUSSION

The present study demonstrates that CA,NO is significantly increased in SSc patients compared with healthy controls, a result consistent with previous findings using the two compartment model method; partitioning eNO into CA,NO and Jaw,NO 8. The observation that eNO is increased in SSc patients is also consistent with previous studies measuring mixed NO concentration in the exhaled air of scleroderma patients with, or without, ILD 13, 14. The current authors have also demonstrated that CA,NO is inversely related to lung volumes, and directly related to the extent of ILD, as assessed by the ground-glass score and the reticular score on pulmonary CT scans in patients with SSc. Moreover, the present authors have found that the levels of CA,NO are different among SSc patients, being significantly higher in patients with ILD compared with patients without ILD. The low r-values, however, suggest that increased CA,NO only accounts for part of the mechanisms causing lung impairment in SSc patients. The relative importance of NO with regards to other pathophysiological factors in individual patients, and how its concentration will vary during the time course of the disease are questions that still remain to be addressed.

The inverse correlation between CA,NO and DL,CO may reflect greater oxidative stress and/or more severe inflammation causing an increase in the alveolar production of NO that results in impaired pulmonary gas transfer. Conversely, reduced gas diffusion (as reflected by low DL,CO) may in turn account for the accumulation of NO, hence its high concentration in the alveolar compartment. However, DL,CO/alveolar volume values did not significantly differ between patients with versus those without ILD. It is unlikely that diffusion abnormalities could account for increased CA,NO.

No relationship was found between CA,NO and sPAP. The current results are consistent with those from a previous study showing increased eNO in a limited number of SSc patients with pulmonary arterial hypertension 8. In contrast, by measuring FeNO in mixed expired air, Kharitonov et al. 15 found decreased eNO in SSc patients with pulmonary hypertension. It is, however, difficult to compare these results with data from the present study due to different methodological approaches used to measure eNO.

Many factors might account for increased pulmonary vascular tone, including overproduction of vasoconstrictors and growth factors 16, inflammatory cytokines 17 or reduced synthesis of pulmonary vasodilators 17, 18. The current results are consistent with the hypothesis suggesting that pulmonary hypertension in SSc is due, at least in part, to inflammatory processes, rather than reduced endothelial NO synthase activity, as seen in idiopathic pulmonary hypertension 19.

Pulmonary inflammation and lung damage leading to subsequent fibrosis can be assessed by measuring eNO. The present study has shown that CA,NO correlates positively with ground-glass attenuation score and with reticular score, further supporting the association between the severity of ILD and an increased alveolar production of NO.

Together with the increase in CA,NO, the current authors have found that Jaw,NO values are significantly lower in SSc patients compared with those from control subjects. Such a difference has not previously been described. The present authors hypothesise that the low J′aw,NO could reflect reduced NO production in the airways of SSc patients as a result of the inhibitory effects that a high alveolar NO concentration might exert on bronchial epithelial NO synthase activity 20. Alternatively, as CA,NO and Jaw,NO are derived from the slope and intercept of the linear relationship between EFR and ERNO 6, 7, it is conceivable that the higher the slope, the lower the intercept, based on the two-compartment model of pulmonary NO exchange dynamics 6, 7.

The limitation of the present results relates to the fact that alveolitis was not evidenced by another method, such as bronchoscopy and bronchoalveolar cell count. Such investigations are invasive. Moreover, they could yield false-negative results, for example with BAL cell counts, particularly when alveolitis involves the lower lung lobe 21.

CONCLUSION

The current authors conclude that alveolar nitric oxide production is significantly increased in patients with systemic sclerosis, probably as a result of a lung fibrosis development. The authors submit that the alveolar concentration of nitric oxide could be used as a surrogate marker for scleroderma lung disease. Furthermore, an increased alveolar concentration of nitric oxide may reflect the extent of lung restriction. The present data highlight the potential interest of this noninvasive method in the diagnosis and the monitoring of interstitial lung disease in patients with systemic sclerosis.

Acknowledgments

The authors would like to thank the technical and nursing staff of the Service de Physiologie-Explorations Fonctionelles (Cochin Hospital, Paris, France) for their technical help.

  • Received October 4, 2006.
  • Accepted March 25, 2007.

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Severity of scleroderma lung disease is related to alveolar concentration of nitric oxide
K. P. Tiev, J. Cabane, F. Aubourg, A. Kettaneh, M. Ziani, L. Mouthon, S. Duong-Quy, I. Fajac, L. Guillevin, A. T. Dinh-Xuan
European Respiratory Journal Jul 2007, 30 (1) 26-30; DOI: 10.1183/09031936.00129806
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