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Significance of connective tissue disease features in idiopathic interstitial pneumonia

T.J. Corte, S.J. Copley, S.R. Desai, C.J. Zappala, D.M. Hansell, A.G. Nicholson, T.V. Colby, E. Renzoni, T.M. Maher, A.U. Wells
European Respiratory Journal 2012 39: 661-668; DOI: 10.1183/09031936.00174910
T.J. Corte
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S.J. Copley
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S.R. Desai
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C.J. Zappala
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D.M. Hansell
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A.G. Nicholson
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T.V. Colby
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E. Renzoni
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T.M. Maher
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A.U. Wells
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  • For correspondence: athol.wells@rbht.nhs.uk
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Abstract

In idiopathic interstitial pneumonia (IIP), the significance of connective tissue disease (CTD) features in the absence of a specific CTD diagnosis remains unclear. We studied the clinical and prognostic utility of a diagnosis of undifferentiated CTD (UCTD) in patients with biopsy-proven IIP.

IIP patients undergoing surgical lung biopsy (1979–2005) were studied (nonspecific interstitial pneumonia (NSIP), n=45; idiopathic pulmonary fibrosis, n=56). UCTD was considered present when serum autoantibodies were present and symptoms or signs suggested CTD. The relationship between UCTD and NSIP histology was evaluated. A clinical algorithm that best predicted NSIP histology was constructed using a priori variables. The prognostic utility of UCTD, and of this algorithm, was evaluated.

UCTD was present in 14 (31%) NSIP and seven (13%) IPF patients. UCTD was not associated with a survival benefit. The algorithm predictive of NSIP (OR 10.4, 95% CI 3.21–33.67; p<0.0001) consisted of the absence of typical high-resolution computed tomography (HRCT) features for IPF and 1) a compatible demographic profile (females aged <50 yrs) or 2) Raynaud’s phenomenon. In patients with an HRCT scan not typical for IPF, this algorithm predicted improved survival (hazard ratio 0.35, 95% CI 0.14–0.85; p=0.02) independent of IIP severity.

UCTD is associated with NSIP histology. However, the diagnostic and prognostic significance of UCTD in IIP patients remains unclear.

  • Connective tissue disease
  • idiopathic interstitial pneumonia
  • idiopathic pulmonary fibrosis
  • nonspecific interstitial pneumonia
  • prognosis
  • undifferentiated connective tissue disease

Nonspecific interstitial pneumonia (NSIP) is the most common histological finding when patients fulfilling American College of Rheumatology (ACR) criteria for specific connective tissue diseases (CTDs) undergo lung biopsy for investigation of fibrotic lung disease [1–3]. However, up to 25% of patients with features of CTD do not fulfil ACR criteria for specific CTD, and are considered to have undifferentiated CTD (UCTD) [4–8]. UCTD is usually considered present when patients have signs or symptoms suggestive of CTD and positive autoimmune serology for >12 months [4, 5, 7, 9–11]. A minority of patients with UCTD develop specific CTD over time [4–8, 12].

It is not uncommon for patients with idiopathic interstitial pneumonia (IIP) to have symptoms and serological findings consistent with UCTD [13–15]. A recent expert commentary has highlighted the fact that many IIP patients do not satisfy specific CTD diagnostic criteria, but clearly have significant end-organ disease [16]. The majority of patients with these autoimmune features have NSIP at surgical lung biopsy [17, 18]. Thus, it has been proposed that UCTD manifests in the lung as “idiopathic NSIP” [9]. The distinction of idiopathic NSIP from idiopathic pulmonary fibrosis (IPF) has important prognostic and treatment implications [19–21]. However, a confident diagnosis of NSIP requires surgical lung biopsy. In a recent study using a broad, and somewhat controversial, definition of UCTD, Kinder et al. [9] showed that UCTD is common in patients with IIP, especially in a small subset of 17 patients with biopsy-proven idiopathic NSIP [9, 16]. On this basis, those authors suggested that a diagnosis of UCTD may be able to distinguish patients with idiopathic NSIP before obtaining surgical lung biopsy [9].

Based upon these a priori observations, we first aimed to determine the relationship between the diagnosis of UCTD and NSIP histology in a large cohort of patients with biopsy-proven idiopathic NSIP and IPF. Secondly, we aimed to explore the clinical utility of a diagnosis of UCTD, with regard to the identification of NSIP at surgical lung biopsy and in the prognostic evaluation of IIP patients.

METHODS

Study subjects

Subjects were identified from a hospital database (n=232) who met the histological criteria at surgical biopsy and the clinical criteria for idiopathic interstitial pneumonia: IPF (n=138) or idiopathic fibrotic NSIP (n=94) between January 1, 1978 and June 30, 2005. 152 patients were identified (IPF, n=91; NSIP, n=61) whose clinical notes were available (not destroyed). 20 patients had incomplete clinical and laboratory data, and were excluded from the analysis. We studied the 101 patients (IPF, n=56; NSIP, n=45) with concurrent high-resolution computed tomography (HRCT).

Data were collected retrospectively from medical records. IPF patients met American Thoracic Society (ATS)/European Respiratory Society (ERS) diagnostic criteria [22]. Clinical criteria for NSIP comprised: 1) bilateral, predominantly basal or widespread crackles; 2) radiographic evidence of predominantly basal, bilateral lung infiltrates with ground-glass or reticular opacities on HRCT; 3) a restrictive functional defect or isolated reduction in diffusing capacity; 4) absence of features suggestive of hypersensitivity pneumonia or organising pneumonia; and 5) no other known cause of pulmonary fibrosis or associated disease. Clinical diagnosis was confirmed by multidisciplinary consensus. No patients met ACR criteria for a specific CTD. The treatment regimen included: 1) combination immunosuppressive treatment including low-dose prednisolone (10 mg); or 2) high-dose prednisolone, reducing to a maintenance dose (mean 10 mg).

It is our routine practice to question patients for symptoms of CTD, including: Raynaud’s phenomenon, arthralgia, myalgia, morning stiffness, Sicca symptoms, gastro-oesophageal reflux or dysphagia, and skin changes. Other symptoms were noted to be present if documented as such in the medical records and assumed absent if not recorded.

Patients were followed up until death, to lung transplantation or to June 1, 2008, with follow-up complete in 93 out of 101 cases. Vital status was determined at June 1, 2008 from hospital databases and confirmed with local physicians. 52 (51%) deaths occurred during follow-up (median 44 months, range 2–258months). No patients underwent lung transplantation during the follow-up period. Local ethical committee approval was in place for retrospective studies.

Investigations

Histopathology

All lung biopsy specimens were independently reviewed by two histopathologists blinded to the clinical data (κ=0.53), with diagnostic divergences resolved by consensus. Histopathological diagnosis was made according to the ATS/ERS international consensus classification of IIPs [23, 24].

HRCT

All patients underwent concurrent HRCT. HRCT was reviewed by two specialist respiratory radiologists. HRCT diagnosis was considered “typical of IPF”, “indeterminate” or “compatible with NSIP”. Consensus scores were generated for the extent of disease, and the proportions of ground-glass opacity, fine reticular changes, and micro- and macrocystic changes at each of five levels, and the total extent of each feature was calculated.

Pulmonary function testing

Pulmonary function testing was performed in all patients (Jaeger Masterscreen 240; Cardinal Health UK Ltd, Basingstoke, UK) and predicted values were calculated according to ATS/ERS guidelines [25–28]. Lung volumes, spirometric volumes and diffusing capacity of the lung for carbon monoxide were measured. The composite physiologic index (CPI) was calculated as previously described [29].

Laboratory testing

All patients had autoimmune serology, C-reactive protein (CRP) and erythrocyte sedimentation rate (ESR) measurements performed. Antinuclear antibody (ANA) testing was performed using indirect immunofluorescence, and considered positive when ≥3+. Extractable nuclear antigen (ENA) and double-stranded DNA analyses were performed using automated ELISA. Specific antibody characterisation was performed in most patients when ENA testing was positive, including anti-Ro (SS-A), anti-La (SS-B), anti-Scl-70, anti-centromere, anti-ribonucleoprotein (RNP) and Jo-1 antibodies. Rheumatoid factor (RF) was analysed using partial agglutination and considered positive when greater than 1/160.

Diagnosis of UCTD

Patients were considered to have a diagnosis of UCTD (table 1) if they had one of the specific autoantibodies (SS-A, SS-B, anti-Scl-70, anti-centromere, anti-RNP or Jo-1), or a positive ENA or ANA titre, as well as symptoms or signs of CTD (including Raynaud’s phenomenon, Sicca symptoms, arthralgia, morning stiffness or proximal muscle weakness) [10]. We also considered whether patients met the broader UCTD definition proposed by Kinder et al. [9] (table 1).

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Table 1– Diagnostic criteria for undifferentiated connective tissue disease (UCTD)

Statistical analysis

All analyses were performed using STATA statistical software (version 10.0; StataCorp, College Station, TX, USA). Data are presented as mean±sd or median (range). Group comparisons were made using unpaired t-tests, Wilcoxon’s rank-sum test or the Chi-squared test. The sensitivity and specificity of a diagnosis of UCTD for NSIP histology was determined.

Outcome was evaluated for mortality, from the time of surgical lung biopsy, using Cox regression, with satisfaction of the assumptions of proportional hazards analysis, for a priori covariates: 1) diagnosis of UCTD, as well as satisfying the broader definition of UCTD of Kinder et al. [9]; 2) demographic variables (age, female sex and females aged <50 yrs, as the mean age of females was 50 yrs); 3) UCTD features (Raynaud’s phenomenon, positive autoimmune serology, and one or more of Raynaud’s or positive serology); 4) functional severity (CPI); 5) HRCT typical of IPF; and 6) histological diagnosis of IPF.

Multivariate survival analysis was performed for UCTD diagnosis, adjusting for functional severity (CPI) and histological diagnosis.

We set out to construct a clinical algorithm predictive of a histological diagnosis of NSIP using step-wise multiple logistic regression analysis. A priori covariates included absence of HRCT typical of IPF, a compatible demographic profile (females aged <50 yrs) and UCTD features (Raynaud’s phenomenon and positive autoimmune serology). The sensitivity and specificity of this algorithm for NSIP histology was determined. The prognostic value of this algorithm was determined using multivariate Cox survival analysis.

RESULTS

Patient characteristics

The mean age of the cohort was 54 yrs and 38 (38%) out of 101 were female. As shown in table 2, patients with NSIP were younger (p=0.003) and more likely to be female (p<0.0001). Pulmonary function tests did not differ between IPF and NSIP. The most common systemic symptom was gastro-oesophageal reflux (39%), followed by arthralgia (24%), Sicca symptoms (19%), Raynaud’s phenomenon (13%) and lethargy (13%). Raynaud’s phenomenon (p<0.0001) was more common in NSIP but no other systemic symptom was associated with histological subtype. NSIP patients were more likely to present with wheeze (p<0.0001).

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Table 2– Demographic and clinical characteristics of patients with biopsy-proven nonspecific interstitial pneumonia (NSIP) compared with patients with idiopathic pulmonary fibrosis (IPF)

The most common laboratory findings were elevation of CRP (39%), elevated ESR (19%), positive ANA (15%), positive ENA (19%) and positive RF (9%) (table 3). Patients with NSIP were more likely to have any positive autoimmune serology (p=0.007) than IPF patients.

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Table 3– Laboratory data for patients with biopsy-proven nonspecific interstitial pneumonia (NSIP) compared to patients with idiopathic pulmonary fibrosis (IPF)

UCTD was present in 21 (21%) out of 101 patients and was more frequent in NSIP (14 out of 45, 31%) than in IPF (seven out of 56, 13%) (p=0.02). The diagnosis of UCTD was associated with a three-fold increase in the likelihood of NSIP (OR 3.16, 95% CI 1.14–8.70; p=0.03), and had a sensitivity of 31% and a specificity of 88% for NSIP histology (table 4).

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Table 4– Sensitivity and specificity of undifferentiated connective tissue disease (UCTD) diagnostic criteria for nonspecific interstitial pneumonia (NSIP) histology

We also considered the prevalence of the broader definition of UCTD of Kinder et al. [9], and found that these criteria were satisfied in a higher proportion of patients overall (52 out of 101, 52%) and were also more frequent in NSIP (32 out of 45, 71%) than IPF (20 out of 56, 36%). There was a similar association between this broader definition of UCTD and NSIP (OR 4.43, 95% CI 1.90–10.32; p=0.001), with a sensitivity of 71% and a specificity of 64% for NSIP histology.

Survival analysis

As shown in table 5, the diagnosis of UCTD was not associated with improved survival (hazard ratio (HR) 1.07, 95% CI 0.54–2.10; p=0.85) (fig. 1). This was also true for the broader definition of UCTD of Kinder et al. [9]. No single CTD symptom, sign or laboratory test predicted survival. Functional impairment (CPI) (HR 1.04, 95% CI 1.02–1.06; p<0.0001) and usual interstitial pneumonia (UIP) histology (HR 3.71, 95% CI 2.00–6.89; p<0.0001) were associated with increased mortality, whereas female sex was associated with lower mortality (HR 0.48, 95% CI 0.25–0.90; p=0.02) and age was not predictive of survival.

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Table 5– Univariate survival analysis
Figure 1–
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Figure 1–

Kaplan–Meier survival curve for patients with and without a diagnosis of undifferentiated connective tissue disease (UCTD).

HRCT appearance

As shown in table 6, IPF on surgical biopsy was associated with increased fine reticular (p=0.0004), microcystic (p=0.0001) and macrocystic (p=0.03) changes on HRCT, whereas NSIP histology was linked to increased ground-glass changes (p=0.0008). By contrast, HRCT findings did not differ between patients with and without UCTD, either in the whole cohort or within histological subgroups.

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Table 6– Radiological features according to biopsy diagnosis and the presence of undifferentiated connective tissue disease (UCTD)

A clinical algorithm predictive of a histological diagnosis of NSIP

Patients with HRCT appearances typical of IPF (n=23, 23%) had a low likelihood of NSIP (OR 0.19, 95% CI 0.06–0.61; p=0.005).

When HRCT appearance was not typical of IPF, the histological diagnosis was UIP in 37 (47%) out of 78 and NSIP in 41 (53%) out of 78 patients. In patients with HRCT not typical of IPF, NSIP was associated with female sex (OR 4.4, 95% CI 1.66–11.64; p=0.003) and younger age (OR 0.94, 95% CI 0.89–0.99; p=0.02). Females aged <50 yrs (n=16, 21%) were likely to have NSIP (OR 5.26, 95% CI 1.36–20.32; p=0.02). However, specific clinical or laboratory features of UCTD were not associated with NSIP within this demographic group, which was excluded from subsequent analysis. In the remaining 62 patients, the presence of Raynaud’s phenomenon (OR 10.67, 95% CI 1.22–93.08; p=0.03) was more strongly associated than positive autoimmune serology (OR 2.89, 95% CI 0.95–8.85; p=0.06) or one of the above (OR 3.75, 95% CI 1.27–11.11; p=0.02) with NSIP.

Based on these findings, the optimal algorithm identifying a high likelihood of NSIP consisted of the absence of HRCT features typical of IPF and the presence of either: 1) a compatible demographic profile (females aged <50 yrs); or 2) Raynaud’s phenomenon (fig. 2). These criteria, which were satisfied in 24 (24%) out of 101 patients, were strongly associated with NSIP (OR 10.40, 95% CI 3.21–33.67; p<0.0001), with a low sensitivity (20 out of 44, 44%) but a very high specificity (55 out of 56, 93%) (table 4).

Figure 2–
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Figure 2–

Flow diagram for the clinical algorithm predictive of a histological diagnosis of nonspecific interstitial pneumonia (NSIP). HRCT: high-resolution computed tomography; IPF: idiopathic pulmonary fibrosis.

In order to evaluate the prognostic value of this algorithm, outcome was first evaluated against HRCT. Patients with appearances typical of IPF had a higher mortality (HR 2.82, 95% CI 1.54–5.15; p=0.001), after adjustment for CPI levels, which were independently positively associated with mortality. In the remaining patients, with HRCT appearances not typical of IPF, mortality was lower in patients satisfying algorithm inclusion criteria (females aged <50 yrs or the presence of Raynaud’s phenomenon) (HR 0.35, 95% CI 0.14–0.85; p=0.02) (table 7) following adjustment for disease severity (CPI). Similarly, mortality was lower if a diagnosis of UCTD was substituted for the presence of Raynaud’s phenomenon (HR 0.38, 95% CI 0.16–0.91; p=0.03). However, the histological diagnosis of IPF remained the strongest prognostic marker in this patient group (HR 4.18, 95% CI 1.93–9.00; p<0.0001).

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Table 7– Multivariate survival analysis if high-resolution computed tomography was not typical of idiopathic pulmonary fibrosis#

DISCUSSION

We report that CTD features are not uncommon in so-called IIP, with 21% of NSIP and 13% of IPF patients fulfilling Mosca's diagnostic criteria for UCTD [10]. When the less specific diagnostic criteria for UCTD of Kinder et al. [9] were applied, 71% of NSIP and 36% of IPF patients were found to have UCTD. It is not certain whether the classification of patients with CTD features who do not fulfil specific CTD criteria as having a diagnosis of UCTD has either clinical or prognostic significance.

Although we showed an association between UCTD and NSIP, this link was not as strong as in previous observations [9]. The diagnosis of UCTD provided no additional prognostic information over the histological IIP diagnosis. We constructed a clinical algorithm, which was specific for NSIP histology. In the absence of histological information or HRCT findings typical of IPF, patients fulfilling this clinical algorithm or the diagnostic criteria for UCTD had improved survival, following adjustment for CPI. Thus, the diagnosis of UCTD may have prognostic value in IIP patients not undergoing diagnostic surgical biopsy, particularly when HRCT features are not typical of IPF.

We were unable to reproduce earlier findings that suggested that UCTD might almost invariably be associated with idiopathic NSIP. Although UCTD, as defined by Kinder et al. [9], was present in ∼70% of NSIP patients, the highly nonspecific nature of the Kinder et al. [9] criteria was underlined by their satisfaction in a third of patients with IPF. Indeed, in the current study, 52% of patients fulfilled the broader definition of UCTD of Kinder et al. [9], which was only moderately specific (64%) but relatively sensitive (71%) for NSIP, compared with 21% of patients who satisfied more standard UCTD criteria, which were relatively specific (88%) but not sensitive (31%) for NSIP histology. Although UCTD diagnostic criteria specific for NSIP histology are empirically desirable, particularly when surgical biopsy is not possible, standard diagnostic criteria were not sensitive for NSIP. In contrast, the less specific criteria of Kinder et al. [9] were more sensitive for NSIP histology, potentially resulting in misclassification of IPF patients as NSIP. However, the clinical or prognostic impact of such misclassification is not certain. The validity of the diagnostic criteria of Kinder et al. [9] has been questioned by rheumatologists and our findings cast further doubt on their value [16]. Above all, the suggestion that these criteria might be used as a substitute for a diagnostic biopsy in distinguishing between IPF and NSIP [9] cannot be countenanced, judging from findings in the present study, and nor did the use of the criteria of Kinder et al. [9] add value to prognostic evaluation, once the histological pattern had been taken into account. In summary, our findings do not support the future use of the criteria of Kinder et al. [9] for the identification of UCTD in clinical practice.

In this regard, a major problem facing clinicians is the lack of a standardised definition for UCTD, now appreciated to be a separate clinical entity [4, 5, 7, 10, 11]. Since LeRoy et al. [30] first proposed the concept of UCTD, there have been more than 10 published diagnostic criteria for UCTD [6, 7, 10, 31–39]. Most definitions are based upon some variation of signs and symptoms suggestive of CTD, positive autoimmune serology and disease duration >1 yr [4, 5, 7, 10, 11]. In some studies, broader definitions of UCTD have been used [9], but, as discussed above, there are major problems with this approach, as UCTD features are nonspecific, and symptoms such as weight loss and proximal muscle weakness are also common in advanced lung disease [40, 41]. In our study, 13% had unintentional weight loss and 4% had proximal muscle weakness.

A recent expert commentary on this issue highlights the dilemma of patients with so called IIP who have features suggestive of CTD. Many IIP patients do not fulfil CTD diagnostic criteria, but clearly have significant disease [16]. In that commentary, the authors suggested that these patients in whom there is “a rheumatologic flavor as supported by specific autoantibodies or histopathologic features”, but who do not meet criteria for a defined CTD, may be considered to have “lung-dominant CTD” [16]. In our study, we addressed this problem by studying the prevalence and utility of a diagnosis of UCTD in a cohort of patients considered to have IIP. We defined UCTD as the presence of autoantibodies and symptoms/signs suggestive of CTD. The major limitation of our retrospective study was the large time period over which the biopsies were performed. During this time period, laboratory tests were refined, moving to routine testing of specific autoantibodies when ENA tested positive. Despite this limitation, we found that the presence of UCTD was associated with NSIP histology, but portended no survival advantage over patients without UCTD.

In the current study, we show a three-fold increase in NSIP histology among patients with UCTD. This is consistent with several studies that show a clear link between NSIP histology and CTD [9, 42, 43]. Two recent studies have demonstrated that 10% and 52% of their patients who were considered to have idiopathic NSIP developed CTD during the follow-up period [43, 44]. In another study, a close association between NSIP histology and UCTD was demonstrated: NSIP was the histological diagnosis in 15 out of 17 patients with UCTD (OR 50; p=0.0001), leading the authors to surmise that the application of diagnostic criteria for UCTD may identify NSIP before obtaining surgical lung biopsy [9]. The necessity of surgical lung biopsy for the diagnosis of NSIP has been debated [45]. However, in our study, we found that having a diagnosis of UCTD was not sensitive (31%) but was relatively specific (88%) for NSIP histology. Our results do not support the use of more specific UCTD diagnostic criteria alone to identify patients with NSIP, but indicate that the diagnosis of NSIP continues to require surgical lung biopsy [46]. However, in the subset of patients in whom surgical biopsy is not practicable, the UCTD diagnostic criteria may be a useful predictor of NSIP histology. This needs to be confirmed in further prospective studies.

We developed a noninvasive algorithm for the presence of NSIP by testing a priori associations between NSIP and both demographic factors and the presence of UCTD [1–3, 17, 46–48]. The optimal algorithm consisted of the absence of HRCT features typical of IPF and the presence of either: 1) a compatible demographic profile (females aged <50 yrs); or 2) Raynaud’s phenomenon. 24 (24%) patients fulfilled the criteria for this algorithm, which was associated with a 10-fold increase in likelihood of NSIP. The striking demographic associations with NSIP observed in the present study mirror previous observations [17, 46–49], and lend further support for the inclusion of a typical demographic profile in diagnostic and prognostic algorithms. The age threshold of 50 yrs in females evaluated in our study was based upon the statement by an expert group that age <50 yrs is an atypical feature in IPF and the fact that 50 yrs was the mean age for females in this study [23].

In the absence of histological information, HRCT findings typical of IPF are widely viewed as diagnostically conclusive. However, when HRCT features are not typical of IPF, both IPF and NSIP histology are frequent, as seen in the current study. In this subgroup, the presence of either a compatible demographic profile (females aged <50 yrs) or Raynaud’s phenomenon was highly specific for NSIP histology (93%) and was associated with improved survival, independent of the severity of the underlying fibrosis. We observed similar relationships with the substitution of a diagnosis of UCTD for the presence of Raynaud’s phenomenon in the above algorithm. Thus, in the absence of histological information and HRCT features typical of IPF, our results support the application of these clinical and demographic features for diagnostic and prognostic assessment of IIP patients. In further support of this conclusion, recent studies have suggested that a diagnosis of UCTD confers a minor prognostic advantage in IIP [50, 51].

Our study has several limitations. Unlike the study by Kinder et al. [9], in which a prospective, systematic collection of CTD features was performed, our study was retrospective, spanning two decades. The retrospective design limited our ability to collect comprehensive clinical and serological details. However, patients excluded because of incomplete data did not differ with regard to age, sex and pulmonary function. Although we routinely specifically question patients for the more common symptoms of CTD, other symptoms were considered present if documented and assumed absent if not recorded. To compensate for this potential bias, we first focused upon symptoms for which we had comprehensive data. Secondly, we recognise that in IIP patients undergoing surgical biopsy (a pre-requisite for a diagnosis of NSIP), IIP tends to be less advanced and the HRCT findings less diagnostically conclusive. Thus, the prognostic value of systemic findings in the proposed noninvasive algorithm needs to be further explored in IIP patients with more severe disease. Finally, we recognise the potential risk of “chance fitting” due to the number of variables assessed. This prompted us to examine a priori thresholds, including a single demographic threshold (females aged <50 yrs), and restricting UCTD data to components in which we have confidence (Raynaud’s phenomenon and positive autoimmune serology). However, despite testing a priori observations, our findings need further evaluation in a separate patient cohort.

Conclusion

In IIP, the significance of CTD features (in the absence of a specific CTD diagnosis) is not clear. Nonspecific CTD features may be the first, or primary, manifestation of an underlying and undeclared CTD. We demonstrate that it is not uncommon for patients with IIP to display CTD features in the absence of a specific CTD diagnosis, with 21% of IIP patients fulfilling accepted diagnostic criteria for UCTD. Less specific diagnostic criteria for UCTD that are associated with high prevalence of “UCTD” are not useful. We show that in IIP, the diagnosis of UCTD is associated with NSIP histology, but is neither sensitive nor specific for NSIP, nor associated with a survival advantage. However, the diagnosis of UCTD may have some diagnostic and prognostic significance in the subset of patients in which surgical biopsy is impracticable and HRCT findings are not diagnostic.

Footnotes

  • Statement of Interest

    None declared.

  • Received November 11, 2010.
  • Accepted July 21, 2011.
  • ©ERS 2012

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Significance of connective tissue disease features in idiopathic interstitial pneumonia
T.J. Corte, S.J. Copley, S.R. Desai, C.J. Zappala, D.M. Hansell, A.G. Nicholson, T.V. Colby, E. Renzoni, T.M. Maher, A.U. Wells
European Respiratory Journal Mar 2012, 39 (3) 661-668; DOI: 10.1183/09031936.00174910

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Significance of connective tissue disease features in idiopathic interstitial pneumonia
T.J. Corte, S.J. Copley, S.R. Desai, C.J. Zappala, D.M. Hansell, A.G. Nicholson, T.V. Colby, E. Renzoni, T.M. Maher, A.U. Wells
European Respiratory Journal Mar 2012, 39 (3) 661-668; DOI: 10.1183/09031936.00174910
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