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Medicina (Buenos Aires)

Print version ISSN 0025-7680

Medicina (B. Aires) vol.74 no.2 Ciudad Autónoma de Buenos Aires Apr. 2014

 

ARTÍCULO ESPECIAL

Rheumatoid arthritis associated interstitial lung disease: a review

 

Deborah Assayag, Joyce S. Lee, Talmadge E. King, Jr.

Division of Pulmonary, Critical Care, Allergy and Sleep Medicine; Department of Medicine, University of California San Francisco (UCSF), San Francisco, CA, USA

Postal address: Dr. Deborah Assayag, University of California San Francisco (UCSF), 505 Parnassus Avenue, Room M1093, San Francisco, CA, 94143-0111.
Phone: 001 415-502-2361 e-mail: Deborah.Assayag@ucsf.edu

 


Abstract
Rheumatoid arthritis is a common inflammatory disease affecting about 1% of the population. Interstitial lung disease is a serious and frequent complication of rheumatoid arthritis. Rheumatoid arthritis associated interstitial lung disease (RA-ILD) is characterized by several histopathologic subtypes. This article reviews the proposed pathogenesis and risk factors for RA-ILD. We also outline the important steps involved in the work-up of RA-ILD and review the evidence for treatment and prognosis.

Key words: Rheumatoid arthritis; Interstitial lung disease; Pathogenesis; Risk factors

Resumen
La artritis reumatoide asociada a la enfermedad intersticial pulmonar: una revisión. La artritis reumatoide es una enfermedad inflamatoria común, que afecta cerca del 1% de la población. La enfermedad pulmonar intersticial es una complicación frecuente y seria de la artritis reumatoide y esta asociación está caracterizada por diferentes subtipos histológicos. Este artículo analiza la patogénesis y los factores de riesgo de esta asociación. Además señala los esfuerzos realizados y las evidencias para el diagnóstico y tratamiento.

Palabras clave: Artritis reumatoide; Enfermedad intersticial pulmonar; Patogénesis; Factores de riesgo


 

Rheumatoid arthritis (RA) is a common systemic inflammatory disorder of unknown etiology. It is characterized by symmetric arthritis and synovial inflammation leading to progressive joint erosion and eventually, deformity1.The world-wide prevalence of RA ranges from 0.5% to 1%, while the incidence is estimated to be 30 cases per 100,000 people per year, and varies based on gender, population and ethnicity2, 3.In the United States, there is some evidence that the incidence and the prevalence of RA has been increasing over the past 20 years4.
Women are more commonly affected than men. This gender imbalance has been observed across different ethnic populations, as well as in familial studies5. There are important clinical differences between men and women with RA. Men have later RA disease onset. They are more likely to have positive anti-cyclic citrullinated peptide (CCP) antibodies, and higher titers. Men are more likely to have a history of smoking and a higher prevalence of extra-articular manifestations6. One explanation for this difference between men and women is genetic variability causing increased susceptibility to autoimmunity6. In addition, there may be hormonal factors contributing to this increased susceptibility. Early menarche and irregular menses are associated with increased risk of RA, while breast feeding seems to be protective against the development of RA7. Men with RA have been shown to have lower levels of bio-available testosterone, with low levels of luteinizing hormone. This suggests that low testosterone levels may play a role in the pathogenesis of RA8.
The etiology of RA is unknown. Known genetic susceptibility are thought to predispose to RA, which can be triggered by environmental exposures such as smoking and air pollutants9.Different genetic loci have been found to be significantly associated with presence of RA in genome wide association studies and replications cohorts10,11. Presence of HLA-DR alleles within the major histo-compatibility complex are strongly associated with RA and can account for about one third of the genetic susceptibility to the disease12.
The disease burden of RA is significant. Patients with RA have lower wages, more missed workdays, lower employment rates and higher limitations at work and home compared to healthy adults. Even after adjusting for age, sex, gender, income and education, people with RA were 53% less likely to be employed compared to those without RA13.
The disease burden is even greater in patients who develop extra-articular manifestations of RA, which affects
approximately 40% of patients14. Pulmonary involvement is a common extra-articular feature of RA. The chest manifestations are varied and include pleuritis and pleural effusions, airways disease such as bronchiolitis obliterans, rheumatoid nodules and interstitial lung diseases (ILD)15.
Interstitial lung diseases are a group of diseases characterized by fibrosis and inflammation of the pulmonary interstitium. Interstitial lung disease can be secondary to RA, but can also be caused by the medications used to treat RA. Several anti-inflammatory and biologic drugs have been associated with the development of ILD16. The focus of this review will be RA associated ILD (RA-ILD), including the epidemiology and pathogenesis, work-up and treatment, and prognosis of RA-ILD.

Rheumatoid arthritis associated interstitial lung disease

Epidemiology

The prevalence of RA-ILD has been reported to be between 4 and 50%17-21. The variability in the reported prevalence can be attributed to the method of detection used in each study. Studies in which a higher proportion of subjects are found to have ILD are those in which the lung involvement is identified on computed tomography (CT) scan. Computed tomography scanning has been shown to be highly sensitive for detecting ILD and can identify patients with asymptomatic and subclinical disease. One study identified 33% of subjects with early RA to have abnormal CT scans, but only 6% had an abnormal chest radiograph22. A significant number of those subjects have mild abnormalities that are subclinical. While some of these patients have progression of RA-ILD, others have disease that never becomes clinically significant22, 23.
The 30-year cumulative incidence of developing clinically significant RA-ILD in cohorts of RA subjects is between 6 and 8%14, 24.One study looking at the prevalence of ILD in U.S. decedents with RA found a prevalence of RA-ILD of 6.6% at the time of death25. Results of this study also suggested that the age-adjusted mortality rates from RA-ILD have been increasing over the past 25 years in women, despite decreasing mortality rates from RA alone. Patients with RA-ILD have a median survival after ILD diagnosis of 2.6 years, which translates to a threefold higher risk for death than for RA patients without ILD24.

Etiology and pathogenesis

The etiology of RA-ILD is unknown. It is likely that most patients have some underlying genetic predisposition to fibrosis that is triggered by some form of injury to the lung. Some of the genetic polymorphisms that have been studied in RA have been studied in patients with RA-ILD. Specifically, certain polymorphisms of the human leukocyte antigen (HLA)-DRB shared epitope have been associated with increased risk of ILD (e.g. HLA-DRB1*1502), while others appear to be protective against the development of ILD (e.g. HLA-DRB1*04, DQB1*04 and DRB1*16)26.One study investigated the association between the MUC5B polymorphism, a polymorphism associated with idiopathic pulmonary fibrosis (IPF), and the presence of RA-ILD, but found no significant association27.
A new mouse model for RA has been developed with a single abnormality in the skg gene. These SKG mice develop a spontaneous autoimmune CD4+T cell mediated illness that resembles RA joint disease andits extra-articular manifestations28. They develop cellular and fibrotic interstitial pneumonia when subjected to cigarette smoke and bleomycin, while normal mice do not29. This suggests that both genetic predisposition and lung injury with inflammation are required for the development of ILD in RA.

Risk factors

Risk factors have been identified in the development of RA-ILD. Some risk factors are patient-specific while others are related to the RA itself. ILD has been shown to be more common in males compared to females in some studies21, 30,but not in others31, 32.Older age is also associated with increased risk of ILD in RA. One study found that for each 10-year increase in age, the likelihood of having ILD increased by 64%32. In another study, age above 65 years increased the risk of ILD more than four-fold31.
Smoking is a risk factor for the development of RA33.Risk of developing RA increases with increasing numbers of pack-years smoked9. It is also an important modifiable risk factor for the development of ILD in this population. Cigarette smoking was found to be associated with presence of radiographic interstitial abnormalities as well as with reduced pulmonary function, both diffusion capacity for carbon monoxide (DLCO) and forced vital capacity (FVC)34.
There is also data to suggest that the severity of RA may be related to the development of ILD. Presence of erosive joint disease, high levels of erythrocyte sedimentation rate (ESR) and presence of rheumatoid nodules are risks factors for the development of ILD24, 32.In one study, high titers of rheumatoid factor (>100 IU/mL) significantly increased the risk of RA-ILD, while there was a trend towards high levels of anti-CCP antibodies and RA-ILD31. A recent preliminary study showed that higher levels of a variety of specific anti-citrullinated peptide antibodies and an expandedrepertoire of these antibodies were present in patients with RA-ILD withlung function abnormalities35.This suggested a link between autoimmunity against citrullinated proteins and RA-ILD.

Diagnosis

Usually, RA-ILD is diagnosed in patients with RA presenting with symptoms suggestive of lung disease, such as dyspnea (on exertion or at rest) or cough. They are often found to have pulmonary function impairment or abnormal chest imaging. Rarely, RA-ILD will be diagnosed on surgical lung biopsy.
Other causes of lung disease in RA should be excluded. The differential diagnosis for lung disease includes drug toxicity and infection. Drugs that have been associated with ILD in RA include disease-modifying agents such as methotrexate, leflunomide, gold, and cyclophosphamide, as well as biologics, includinganti-TNF-alpha agents.[36, 37]Infection, especially atypical infections (e.g., Mycobacterium species, Pneumocystis jirovecii), should also be ruled out38.

Subtypes of RA-ILD

Several histopathologic subtypes of ILD can be observed in patients with RA. The most common subtypes are the usual interstitial pneumonia pattern (UIP) and the non-specific interstitial pneumonia pattern (NSIP)39,40. Other patterns of ILD seen in RA include organizing pneumonia (OP), lymphocytic interstitial pneumonia (LIP), desquamative interstitial pneumonia (DIP), and diffuse alveolar damage (DAD).
There is increasing data to suggest that RA-ILD patients with a UIP pattern may have a distinct clinical phenotype and natural history compared to the other histopathologic phenotypes observed in RA-ILD, primarily those with NSIP (Table 1). RA-ILD patients with the UIP pattern tend to be older, more likely to be male, and have a more significant smoking history21,30,39-42. In contrast, those without the UIP pattern tend to be younger, more likely to be women, and have a less significant smoking history. What is most compelling is the observed survival difference between RA-ILD patients with and without a UIP pattern. Patients with RA-ILD and a UIP pattern appear to have a worse survival compared to those without a UIP pattern41,43. In addition, the RA-ILD patients with UIP pattern have a similar clinical phenotype and natural history seen in patients with IPF, a disease characterized by idiopathic UIP pattern.

TABLE 1.- Differences between UIP and non-UIP in RA-ILD

Abbreviations: UIP, usual interstitial pneumonia; CCP, cyclic citrullinated peptide; PFT, pulmonary function tests.

Work-up of RA-ILD

The steps involved in the work-up of patients with RA-ILD are summarized in Table 2.

TABLE 2.- Work-up for rheumatoid-arthritis related interstitial lung disease

Abbreviations: RA-ILD, rheumatoid arthritis associated interstitial lung disease; FVC, forced vital capacity; DLCO, diffusion capacity for carbon monoxide; HRCT, high resolution computed tomography of the chest; UIP, usual interstitial pneumonia; CCP, cyclic citrullinated peptides.

Clinical symptoms and signs: Clinical symptoms suggesting RA-ILD are non-specific. Dyspnea, usually on exertion, is the most frequently reported symptom. Because of physical limitations from articular disease, exertional dyspnea may not be apparent in the early stages of the disease. Cough, sputum production, wheezing and chest pain can also be reported44, 45.A subset of patients can have subclinical disease, which is apparent on CT scan, but patients are clinically asymptomatic46.Patients who have abnormal pulmonary function tests are more likely to report respiratory symptoms45.
Pulmonary function tests: About one third of all RA patients will have pulmonary function abnormalities45.Pulmonary function tests (PFTs) in RA can be used as screening tools for early RA-ILD and a method to assess for disease progression. Patients most commonly have a restrictive pattern on their PFTs, like in other ILDs. A mean FVC between 60 and 70% of predicted has been reported in cohort studies of RA-ILD, with a reduced DLCOof40 to 60% of predicted values40, 41.

Computed tomography imaging: High resolution CT scan is essential in evaluating RA-ILD.Figure 1 illustrates different radiographic abnormalities observed. Most studies assessing CT abnormalities in RA-ILD did not differentiate between the different subtypes of ILD. The main abnormalities observedare reticulations and ground glass opacities21, 44, 47.When severe and extensive, interstitial fibrosis leads to parenchymal architectural distortion, traction bronchiectasis, and honeycombing48. Nodules that are centrilobular or perilymphatic can also be seen in RA-ILD, either alone, or with reticulations47.


Fig. 1.- CT abnormalities in patients with RA-ILD.Figure illustrates different patterns and abnormalities that can be seen on chest computed tomography: a. Bilateral, basilar predominant ground glass opacities and consolidation; b. Ground glass opacities with reticulations; c. Bilateral reticulations and traction bronchiectasis; d. Honeycombing with reticulations, consistent with the usual interstitial pneumonia pattern

The UIP pattern in RA-ILD shares the same definition as in the idiopathic interstitial pneumonias (IIPs). It is characterized by presence of subpleural, basilar predominant reticulations, traction bronchiectasis, and honeycombing with absence of nodules, ground glass opacities or consolidation49.Similar to the IIP literature, the radiologic pattern ofa definite UIP pattern on CT scan has been shown to be highly specific and moderately sensitivefor the UIP pattern on histopathology in patients with RA-ILD50 (Fig. 1).
Bronchoscopy and bronchoalveolar lavage:There is little role for bronchoscopy and bronchoalveolar lavage
(BAL) in the diagnostic algorithm of RA-ILD. One study found increased cellularity in BAL compared to normal controls, but not when compared with RA patients without ILD51. In another study, BAL showed an increase in neutrophil percentage, but this correlated poorly with extent of disease on CT scan42.BAL can be useful in patients who develop acute or subacute respiratory worsening in the context of RA-ILD in order to rule out opportunistic infection.
Surgical lung biopsy:Surgical lung biopsy as a diagnostic tool is generally not performed in the context of connective tissue diseases (CTD), unless the diagnosis of CTD is unclear or not established. In contrast to the IIPs, where histopathologic subtype is critical to the management of the ILD, ascertaining histopathologic subtype in CTD-ILD, including RA-ILD, is not done. This is primarily because management and treatment of RA-ILD is irrespective of histopathologic phenotype at this time.
Biomarkers: At this time, no biomarker has been shown to be sensitive or specific to RA-ILD disease activity or disease progression. KL-6 (Krebs von den Lungen-6)is a glycoprotein expressed by type-II pneumocytes and epithelial cells. It is a serum indicator for pulmonary fibrosis that has been evaluated in RA-ILD. It was shown to be correlated with reticular opacities and honeycombing on CT scan52. However, KL-6 has poor sensitivity in RA-ILD53.
Protein citrullination is thought to be associated with extra-articular manifestations of RA, including RA-ILD54.Serum citrullinated proteins Hsp90 isoforms a and β were found to be highly specific for RA-ILD in a cohort of RA patients, but poorly sensitive55. This suggests that they may be biomarkers for RA-ILD, although correlation with disease activity and severity has not yet been established.

Treatment

The management of RA-ILDin patients with subclinical disease remains unclear. It is not known whether treatment will alter the course of the disease in these patients.The mainstay of treatment in RA-ILD is immunosuppression. First line therapy is prednisone at high doses, for prolonged duration. Observational studies suggest that there may be benefit in using other forms of immunosuppression, such as steroid sparing agents, in the treatment of RA-ILD.In a cohort of 40 patients with RA-ILD, the addition of disease-modifying anti-rheumatic drugs (DMARDS) to tapering doses of prednisone was associated with improvement in baseline FVC. The DMARDS used by treating physicians in this study included methotrexate, leflunomide and azathioprine56.There was no difference in pulmonary function improvement between the different agents used. In a subgroup analysis, patients with a lower fibrosis score on CT were the ones who had a response to treatment. In this study, patients with RA-UIP had a higher mean fibrosis score. In another cohort of patients, thepresence of ILD was associated with an increasedodds of developing leflunomide induced pneumonitis and ILD (OR 8.2)57.
Anti-TNF alpha agents have been used in RA for several years to treat articular disease. There were reports of increased risk of developing ILD in RA patients using these biologic agents58. However, several studies have since demonstrated that these agents do not cause increased risk of developing RA-ILD36, 59.
No study thus far has looked at response to treatment according to histopathologicsubtype of RA-ILD. Lung transplant in end stage RA-ILD is being performed in some centers, but no long-term data has been published.

Prognosis

Patients with RA-ILD have an increased mortality compared to patients with RA but no evidence of ILD60.Median survival ranges between 3 and 8 years from time of diagnosis of RA-ILD40, 41, 43.Older age, male sex and greater impairment in pulmonary function at diagnosis have been associated with worse prognosis32, 37, 41. In one study, greater RA disease severity was associated with an increased hazard of death in RA-ILD37.Presence of rheumatoid factor and high LDH have also been shown to confer a poorer prognosis61.
Patients with RA-ILD may experience bouts of acute exacerbations (AE) similar to those reported in other patients with ILD, especially those with RA-ILD and a UIP pattern (RA-UIP)62, 63.The etiology of AE in RA-ILD is unknown. These events are associated with older age at ILD diagnosis, a UIP pattern on HRCT and methotrexate usage. Acute exacerbations are also associated witha worse prognosis in RA-ILD63.
As previously mentioned, the underlying histopathologic and/or radiologic phenotype may inform prognosis in RA-ILD. In general, the extent of honeycombing and severity of traction bronchiectasis appear to be independently associated with increasing mortality in fibrotic ILD associated with CTD, especially in patients with RA-ILD64.Furthermore, studieshave demonstrated that RA-ILD patients with a UIP pattern have a worse prognosis compared to those without UIP41, 43, 63. In one of those studies, the survival in patients with RA-UIP was similar to patients with IPF41.However, another study demonstrated that when IPF and RA-UIP patients are matched for age, sex, smoking and baseline lung function, RA-UIP patients havea longersurvival timecompared to IPFpatients (median survival, 53 vs. 41 months in RA-UIP vs IPF,respectively, p = 0.015)62.Another study showed no difference in survival between the UIP and NSIP forms of RA-ILD, but this may be due to limited sample size. Regardless, survival in patients with fibrotic ILD wasreduced compared to non-fibrotic RA-ILD in this study40.
ILD is a frequent complication of RA and is associated with increased morbidity and mortality. There are distinct histopathologicsubtypes of RA-ILD, which appear to have different clinical phenotypes and natural histories.At this time, it remains unclear if there is benefit to classifying patients by their histopathologic subtype. However, if the pathobiology of UIP in RA-ILD is more similar to that of IPF than in non-UIP forms of RA-ILD, it may be that we are harming a subset of RA-ILD patients with our generalized approach to treatment of RA-ILD65. Further research investigating the differences between those with and without UIP pattern in RA-ILD are needed as it may shift our current paradigm of RA-ILD management and treatment to be more in line with what has been established in the idiopathic interstitial pneumonias.

Conflict of interest: The authors report no conflict of interest related to this manuscript

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Recibido: 24-II-2014
Aceptado: 12-III-2014

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