Undifferentiated connective tissue disease presenting with prevalent interstitial lung disease: Case report and review of literature

A 50-year-old non-smoking female textile worker after a flu-like episode started to suffer from dry cough and progressive dyspnoea. Chest radiography showed parenchymal pulmonary opacity in the lower posterior segment of the right haemithorax and bilateral interstitial thickening of the lower pulmonary segment. The patient was therefore treated with antibiotics and steroids but the clinical and radiological manifestations did not improve.

Computed tomography (CT) scan of the lungs three months later revealed a ground glass pattern in the apical segment of the upper and lower lobes. Lymphadenopathy in the paratracheal space was also observed (Figure 1). The laboratory results showed an increased level of inflammatory parameters (erythrocyte sedimentation rate: 78 mm; C-reactive protein: 5.7 mg/dl; Fibrinogen: 492 mg/dl), without any other positive tests (e.g. rheumatoid factor). The pulmonary function test showed a restrictive pattern (vital capacity: 1.59 L, 50% predicted; total lung capacity: 3.94 L, 75% predicted) with a reduction in the single breath diffusion capacity of carbon monoxide (TLCO/VA 0.84 mmol/min/kPa/l, 52% predicted). Arterial oxygen tension at rest was normal (pH: 7.44; pO₂: 92.4 mmHg; pCO₂: 38.8 mmHg). A six-minute walking test revealed oxygen desaturation (87%) with severe dyspnoea (BORG scale 5/10). Bronchoscopy with combined bronchoalveolar lavage and transbronchial biopsies were performed, but they provided no significant additional information.

Open lung biopsy was performed and based on a histological diagnosis of non specific interstitial pneumonia (NSIP) an accurate immunological follow-up was required.

The assay of a larger panel of autoantibodies showed only positivity of antinuclear antibodies (ANA), at titer 1/160. The other investigated antibodies (such as anti-ENA, anti-DNAds, anti-centromere, anti-cyclic citrullinated peptide and anti-tRNA synthetases) were all negative. Finally, a nailfold capillaroscopy (NFC) was recommended and showed the presence of minor capillary changes characteristic of a nonspecific pattern (Figure 2). Clear-cut signs of Raynaud's phenomenon (RP) were then reported during rheumatologic follow-up. After a multidisciplinary discussion (pneumologist, radiologist, pathologist and rheumatologist) a final diagnosis of NSIP associated with UCTD was made.

Therefore, the patient was discharged and started a treatment regimen of oral cyclophosphamide (100 mg/die) and prednisone (25 mg/die) for 12 months. The combination was then stopped and the patient was followed only with low dose of corticosteroids.

Up to now, over a follow-up period of three years, the clinical picture and the pulmonary function test remain stable and no definitive CTD has developed.

Low-magnification microscopy showed an uniform alveolar septa thickening by cellular infiltrate and fibrosis. At higher magnification, the alveolar septal interstitium was expanded by mild inflammation and collagen deposition with minimal honeycomb changes. No fibroblastic foci and active fibrosis were seen and patchy lymphoid aggregates were occasionally visible. The interstitial chronic inflammation consisted of lymphocytes and some plasma cells. Increased macrophagic infiltration was seen in some alveolar spaces. The appearance was consistent with the fibrosing variant of NSIP (Figure 3). Organising pleuritis with mesothelial hyperplasia was present. Medial vessel thickening was particularly seen in remodelled lung areas.