Research ArticleArticle
Open Access

An Open-label, Phase II Study of the Safety and Tolerability of Pirfenidone in Patients with Scleroderma-associated Interstitial Lung Disease: the LOTUSS Trial

Dinesh Khanna, Carlo Albera, Aryeh Fischer, Nader Khalidi, Ganesh Raghu, Lorinda Chung, Dan Chen, Elena Schiopu, Margit Tagliaferri, James R. Seibold and Eduard Gorina
The Journal of Rheumatology September 2016, 43 (9) 1672-1679; DOI: https://doi.org/10.3899/jrheum.151322

Abstract

Objective. Systemic sclerosis-associated interstitial lung disease (SSc-ILD) shares a number of clinical features and pathogenic mechanisms with idiopathic pulmonary fibrosis (IPF). This study was designed to evaluate the tolerability of the IPF treatment pirfenidone in SSc-ILD. The known gastrointestinal, skin, and liver adverse events (AE) of pirfenidone are of importance given the involvement of these organs in SSc.

Methods. All patients received pirfenidone and were randomized 1:1 to either a 2- or 4-week titration starting at 801 mg/day and finishing at a maintenance dose of 2403 mg/day. Patients received pirfenidone for 16 weeks in total. Assessments included treatment-emergent AE (TEAE) and exploratory disease outcomes.

Results. Sixty-three patients were randomized; 96.8% experienced a TEAE and more patients reported TEAE during the titration versus the maintenance period. The most commonly reported TEAE were consistent with those observed for pirfenidone in IPF (nausea, headache, fatigue) and were similar regardless of titration schedule. More patients discontinued treatment because of TEAE in the 2- versus 4-week titration group (5 vs 1, respectively); all discontinuation events occurred > 3 weeks after reaching the full dose of pirfenidone. Mycophenolate mofetil (MMF), taken by 63.5% of patients in addition to pirfenidone, did not appear to affect tolerability. Exploratory disease outcomes remained largely unchanged.

Conclusion. Pirfenidone showed an acceptable tolerability profile in SSc-ILD, although a longer titration may be associated with better tolerability. Tolerability was not affected by concomitant MMF. The present findings support further investigation of pirfenidone in future clinical trials in patients with SSc-ILD. Trial registration: ClinicalTrials.gov; www.clinicaltrials.gov NCT01933334.

Key Indexing Terms:

Interstitial lung disease (ILD) is a frequent complication of systemic sclerosis (SSc), a rare heterogeneous systemic autoimmune disease, characterized by excessive collagen production and tissue fibrosis of the skin and internal organs1,2. Up to 90% of patients with SSc show evidence of ILD on high-resolution computed tomography (HRCT) and 40%–75% show impairment in pulmonary function tests2. Further, ILD and pulmonary arterial hypertension (PAH) are the 2 main causes of death in SSc2,3. SSc-ILD is characterized by interstitial and alveolar inflammation and fibrosis, typically manifesting on radiographic imaging and histology as a nonspecific interstitial pneumonia pattern4,5,6.

To date, there are no approved treatments for SSc-ILD. Treatment with cyclophosphamide (CYC) has been recommended7; however, improvements in lung function are generally modest8,9 and concerns exist regarding its safety profile2,7,10. Mycophenolate mofetil (MMF) is frequently used with the intention to stabilize lung function in SSc-ILD2,10,11, particularly in patients who cannot tolerate CYC. A study comparing MMF and CYC in patients with SSc is currently under way, with interim results showing a similar but minimal improvement for both treatments of about 4%–4.5% in percent-predicted forced vital capacity (FVC) at 24 months (Scleroderma Lung Study II, NCT00883129)2,10,12.

Pirfenidone is an antifibrotic agent13 with antiinflammatory properties, including inhibition of proinflammatory cytokines14 and inhibition of inflammatory cell proliferation15. Pirfenidone was approved by European and US regulatory agencies in 2011 and 2014, respectively, for the treatment of patients with idiopathic pulmonary fibrosis (IPF)16,17,18,19, a chronic, progressive, and almost invariably fatal disease20. Unlike SSc-ILD, however, IPF is limited to the lungs and is defined by a pattern of usual interstitial pneumonia5. Despite differences in their clinical presentation5, IPF and SSc-ILD share some overlapping pathogenic mechanisms, including injury to structural cells, fibroblast activation, myofibroblast accumulation, expression of fibrogenic cytokines and growth factors, and progressive ILD2,5,21.

Pirfenidone is generally well tolerated in patients with IPF, and compared with placebo, pirfenidone significantly reduces disease progression (as measured by change in percent-predicted FVC) and increases progression-free survival17,18,22. Pirfenidone also significantly reduces the risk of mortality in patients with IPF compared with placebo and can benefit patient outcomes including the 6-min walking distance and dyspnea17,23. However, pirfenidone is known to be associated with adverse events (AE) of the liver, gastrointestinal (GI) system, and skin17,18, which may overlap with the organ systems frequently affected in patients with SSc1,24,25. Therefore, in the setting of SSc-ILD, it is important to investigate the tolerability of pirfenidone before assessing its efficacy.

The LOTUSS study (An Open Label, RandOmized, Phase 2 STUdy of the Safety and Tolerability of Pirfenidone when Administered to Patients with Systemic Sclerosis-Related Interstitial Lung Disease) was designed to assess the safety and tolerability of pirfenidone in patients with SSc-ILD at the same therapeutic dose used in IPF, and using 2 dose-titration schedules, with or without stable background SSc-ILD therapy.

MATERIALS AND METHODS

Design and patients

The LOTUSS study (NCT01933334) was an international, multicenter, randomized, open-label, phase II study (Figure 1). Eligible patients were men or women aged 18–75 years with a confirmed diagnosis of SSc based on the preliminary criteria of the American College of Rheumatology for the classification of SSc26 and an HRCT scan with evidence of ILD within 2 years of the study start. Eligibility criteria included SSc disease duration of < 7 years from first non-Raynaud symptoms; percent-predicted FVC of ≥ 50%; DLCO of ≥ 40% (adjusted for hemoglobin); absence of clinically significant PAH, right atrial or ventricular enlargement or left ventricular dysfunction; absence of underlying liver disease; and absence of moderate to severe gastroesophageal reflux [as assessed by the University of California Los Angeles Scleroderma Clinical Trial Consortium Gastrointestinal Tract (UCLA SCTC GIT) 2.0 questionnaire reflux subscale score > 1.0]27. Concomitant background SSc-ILD medication of oral CYC (≤ 2 mg/kg/day) or MMF (≤ 1.5 g twice daily) was permitted if patients had received a stable dose for ≥ 3 months prior to study start. Full inclusion and exclusion criteria are provided in the Supplementary Material 1 (available online at jrheum.org).

Figure 1.
Figure 1.

LOTUSS study design. Analysis periods were defined as follows: titration period, weeks 1–6; maintenance period, weeks 7–16. LOTUSS: An Open Label, RandOmized, Phase 2 STUdy of the Safety and Tolerability of Pirfenidone when Administered to Patients with Systemic Sclerosis-Related Interstitial Lung Disease; TID: 3× daily; EOT: end of treatment.

We conducted our study in accordance with the International Conference on Harmonisation guidelines, consistent with the Declaration of Helsinki, and applicable laws and regulations of the countries in which the research was conducted. Local institutional review boards and independent ethics committees approved the protocol (Supplementary Table 1, available online at jrheum.org). All patients provided written informed consent.

Randomization

Patients received pirfenidone (267 mg oral capsules with food) at a starting dose of 801 mg/day (1 capsule, 3× daily) titrated to a maintenance dose of 2403 mg/day (3 capsules, 3× daily). Patients were randomized 1:1 to a 2-week titration group (as standard for patients with IPF) or a 4-week titration group (Figure 1). Randomization occurred through a blocked scheme prospectively prepared by the study sponsor and was stratified by background SSc-ILD treatment.

Assessments

Safety assessments were treatment-emergent AE (TEAE) and treatment-emergent serious AE (TE SAE), and their relationship to pirfenidone. AE were collected from study start until 28 days after the last dose or the posttreatment visit, whichever occurred later. Changes in clinical laboratory variables or electrocardiogram results were recorded. The frequency of GI symptoms and their effect on patient quality of life were assessed using the UCLA SCTC GIT 2.0 questionnaire27.

Exploratory disease outcomes included relevant lung function assessments [percent-predicted FVC, DLCO (adjusted for hemoglobin)], patient-reported outcomes [Mahler baseline and Transition Dyspnea Indices (TDI), Health Assessment Questionnaire-Disability Index (HAQ-DI), patient’s global assessment of disease activity (PtGA)], and the modified Rodnan skin score (mRSS).

Statistical analyses

The study was designed to enroll about 50 patients (25 per titration group) to provide a ≥ 95% probability of observing a common AE with a true event rate of ≥ 6%. Analyses were summarized descriptively by titration group for all patients, for the entire treatment period, during the titration period (weeks 1–6) and during the maintenance period (weeks 7–16). Study endpoints were also summarized by subgroups, defined by background SSc-ILD treatment and type of cutaneous SSc. Fisher’s exact test was used to provide p values for safety outcomes with numeric differences for descriptive purposes.

RESULTS

Patients

Overall, 63 patients were recruited at 18 sites across 3 countries (Canada, Italy, and the United States) and were randomized to the 2-week or 4-week pirfenidone titration groups (Figure 2). An additional 26 patients did not satisfy the eligibility criteria and were not randomized. The first patient was enrolled on October 31, 2013, and the last patient completed the study on September 16, 2014. All randomized patients received ≥ 1 dose of study medication.

Figure 2.
Figure 2.

Summary of patient disposition. a Following initiation of study medication, 3 patients were discovered to not meet all eligibility criteria [DLCO < 40% (n = 2) and systemic sclerosis disease duration > 7 yrs (n = 1)], but were permitted to continue. b All TEAE leading to discontinuation started > 3 weeks after completion of the 2- or 4-week titration. TEAE: treatment-emergent adverse event; UCLA SCTC GIT: University of California Los Angeles Scleroderma Clinical Trial Consortium Gastrointestinal Tract.

Baseline demographics and clinical characteristics were comparable in the 2 titration groups with the exception that more patients in the 2-week titration group had limited SSc and that the 4-week titration group had slightly better lung function (Table 1). Background SSc-ILD medication was used by 63.5% of patients, all of whom were receiving MMF (Table 1). No patients were receiving CYC. Prednisone was used by 17.5% of patients.

View this table:
Table 1.

Summary of baseline demographic characteristics. Values are n (%) unless otherwise specified.

Most patients (88.9%) completed our study; 7 patients (11.1%) withdrew early, 6 (9.5%) because of AE (5 in the 2-week group and 1 in the 4-week group; Figure 2). All patients reached the target dose of pirfenidone 2403 mg/day, except 1 patient in the 2-week group owing to a site dosing error.

Overall, 57.1% of patients had a dose adjustment; in both titration groups, the majority of dose adjustments occurred during the maintenance versus titration period (dose reductions: 48.4% vs 12.7%, respectively; dose interruptions: 22.6% vs 6.3%, respectively). Patients in the 2-week titration group had more dose adjustments overall compared with the 4-week group; the difference between the 2 titration groups was most striking during the titration period (dose reductions: 21.9% vs 3.2%, difference 18.7%, p = 0.0534; dose interruptions: 12.5% vs 0%, difference 12.5%, p = 0.1132, for the 2- vs 4-week group, respectively).

Safety

Overall, 96.8% of patients experienced at least 1 TEAE (Table 2A). The most commonly reported TEAE were nausea, headache, and fatigue. The frequency and type of TEAE were similar for both the 2- and 4-week titration groups (Table 2A).

View this table:
Table 2A.

Summary of TEAE. Values are n (%).

A greater proportion of patients experienced TEAE during the titration versus the maintenance period (92.1% vs 79.0%). Of the TEAE reported by > 10% of patients during the entire treatment period (Table 2B), nausea (44.4% vs 8.1%), gastroesophageal reflux disease (19.0% vs 4.8%), fatigue (31.7% vs 9.7%), and headache (30.2% vs 19.4%) were reported in more patients during the titration versus the maintenance period. Rash was reported in more patients during the maintenance period (17.7% vs 4.8% during the titration period).

View this table:
Table 2B.

TEAE reported in ≥ 10% of patients from both treatment groups overall. Values are n (%).

The majority of TEAE were mild or moderate in intensity28. Sixteen severe TEAE were reported by 12 patients, 9 (28.1%) and 3 (9.7%) of whom were in the 2- and 4-week titration groups, respectively (difference 18.4%, p = 0.1069; Table 2A). Overall, most severe TEAE were reported after the completion of the titration periods (13/16 TEAE) and when the patients had been receiving the full dose of pirfenidone for > 2 weeks (11/16 TEAE). Severe TEAE reported by > 1 patient were fatigue (4.8%), diarrhea (3.2%), and nausea (3.2%; Table 2B).

Three patients reported 4 TE SAE; all events were new in onset and occurred in the 2-week titration group during the maintenance period. TE SAE were bronchitis (not related to study medication, per site investigator), intestinal obstruction (possibly related to study medication), and PAH (associated with SSc and diagnosed by right heart catheterization) alongside worsening ILD (neither of which were related to the study medication). The patient with PAH/ILD also discontinued the study because of PAH. A further 5 patients discontinued the study (Table 2A): 3 because of skin-related TEAE (2 in the 2-week group and 1 in the 4-week group); 1 patient owing to drug hypersensitivity to pirfenidone (with vomiting, 2-week group); and 1 patient after an exacerbation of existing fibromyalgia (2-week group). All TEAE leading to discontinuation occurred > 3 weeks after reaching the full dose of pirfenidone. No life-threatening TEAE or deaths occurred.

The incidence of TEAE was generally comparable in the predefined subgroups. However, the incidence of infections was higher in the no-MMF versus MMF subgroup (n = 13, 56.5% vs n = 10, 25.0%, respectively, difference 31.5%, p = 0.0161). A greater proportion of patients reported severe TEAE in the no-MMF versus MMF subgroup (n = 8, 34.8% vs n = 4, 10.0%, respectively, difference 24.8%, p = 0.0223) and in the diffuse versus limited cutaneous SSc subgroup (n = 8, 25.8% vs n = 4, 12.5%, respectively, difference 13.3%, p = 0.2132). Similarly, more patients discontinued treatment because of a TEAE in the no-MMF versus MMF subgroup (n = 4, 17.4% vs n = 2, 5.0%, respectively, difference 12.4%, p = 0.1794), as did patients with diffuse versus limited cutaneous SSc (n = 5, 16.1% vs n = 1, 3.1%, respectively, difference 13.0%, p = 0.1042).

Results for the patient assessment of GI symptoms using the UCLA SCTC GIT 2.0 questionnaire at Day 1 and Week 16 showed that mean total GIT scores and subscale scores remained stable throughout the study with no notable differences between the 2- and 4-week titration groups (Supplementary Table 2, available online at jrheum.org). Liver function tests showed that bilirubin values did not exceed the upper limit of normal (ULN) and aminotransferase levels remained below 3× the ULN. Minor elevations in liver function tests were sporadic and not considered clinically relevant. There were no abnormalities identified in other clinical laboratory data.

Exploratory disease outcomes

Percent-predicted FVC and DLCO values were basically unchanged throughout our study, and no clinically relevant differences were observed in lung function variables between the 2- and 4-week groups or in any of the subgroup analyses (Table 3). Mean change from baseline in percent-predicted FVC was 0.6% and −0.3% in the MMF and no-MMF subgroups at Week 16, respectively; mean change from baseline in percent-predicted DLCO was 3.2% and −0.2% in the MMF and no-MMF subgroups at Week 16, respectively (Table 3).

View this table:
Table 3.

Summary of exploratory disease outcomes.

Relative to baseline at Week 16, dyspnea remained unchanged with a mean score of 1.0 on the Mahler TDI scale in all patients. Mean change from baseline in Mahler overall TDI score was greater in the 4- versus 2-week titration group (Table 3) and dyspnea was slightly more pronounced at baseline and more improved at Week 16 in the MMF versus no-MMF subgroup (Table 3).

Skin thickening, as measured by mean mRSS total score, remained unchanged from baseline to Week 16 (Table 3) and no clinically relevant differences were seen at Week 16 in the 2- versus 4-week titration groups or in the subgroup analyses. HAQ-DI score showed little change from baseline to Week 16, with results similar across the 2- and 4-week titration groups. Mean PtGA scores showed a slight worsening of disease status at study end, and a larger increase in mean PtGA score was seen at Week 16 in the 2- versus 4-week titration group (Table 3), although the data were highly variable. Similarly, a larger increase in PtGA score was seen in the no-MMF versus MMF subgroup.

DISCUSSION

Our present findings suggest that pirfenidone has an acceptable tolerability profile in patients with SSc-ILD. The TEAE reported during our study were consistent with those observed in 3 randomized, placebo-controlled phase III trials of pirfenidone in IPF (n = 1247)17,18 and a longterm safety assessment of pirfenidone in IPF (n = 789)29. Common side effects included headache and fatigue, which were reported by 44.4% and 36.5% of patients, respectively. The high proportion of these events may warrant further investigation into their effect on the tolerability of pirfenidone in SSc-ILD. However, these events were all mild or moderate in severity and none were classified as serious or led to treatment discontinuation.

The known adverse effects of pirfenidone on the GI system, skin, and liver17,18 were of interest in SSc-ILD because these organ systems are also affected in patients with SSc1,24,25. Although GI AE were common, this was not unexpected because of the high frequency of such events observed in clinical trials of pirfenidone in patients with IPF, although patients with moderate to severe gastroesophageal reflux disease (UCLA GIT reflux subscale score > 1.0) were excluded from our study. Patient assessment of GI side effects using the UCLA SCTC GIT 2.0 score suggested the GI effects were stable between baseline and Week 16. This tool has previously been shown to be sensitive to changes in GI symptoms in SSc2,30,31. However, because the UCLA SCTC GIT questionnaire only identified AE occurring within 7 days prior to its use at the baseline and final visits, it is possible that the symptoms reported as AE during our study may have resolved in the intervening weeks. More AE may have been identified if the questionnaire had been administered more frequently.

The frequency and type of TEAE reported during the standard 2-week and the longer 4-week titration schedule reflect the favorable tolerability profile of pirfenidone in SSc-ILD. Over the course of our study, severe TEAE, TE SAE, and TEAE leading to discontinuation were more common in patients who had undertaken the 2- rather than the 4-week titration. This was also the case for dose modifications; however, it should be noted that dose adjustments were made at the discretion of the investigator for safety or tolerability reasons; more specific information was not recorded. Overall, these findings suggest that the titration schedule may affect pirfenidone tolerability and it is possible that patients who are susceptible to the AE commonly associated with pirfenidone may benefit from a longer titration period. Indeed, future studies investigating pirfenidone in SSc-ILD should use a 4-week titration schedule.

MMF is increasingly used in SSc-ILD and it is important that any new SSc-ILD therapy can be tolerated in conjunction with this medication. In our study, MMF was received by 63.5% of patients in addition to pirfenidone, with similar tolerability to pirfenidone alone; this is notable given the known GI toxicity of both treatments17,18,32. Further, patients who took pirfenidone and MMF, compared with pirfenidone alone, appeared to experience fewer severe TEAE and discontinuations and had a greater improvement in dyspnea scores (although this may be due to the small size of each subgroup or imbalances in patient characteristics or background disease at baseline). The reason for the lower rate of infections reported in patients receiving MMF versus no MMF remains unclear; however, it is reassuring that MMF did not increase the rate of infections in patients with SSc-ILD. Further research is required to support this finding and provide a rationale.

Given the overlapping pathogenic mechanisms between SSc-ILD and IPF2,5,21, it may be possible that pirfenidone would slow the deterioration of lung function in patients with SSc-ILD17,18. Although stable results were reported in the exploratory disease outcomes, our study was not designed with sufficient duration to assess efficacy and the study population was not enriched for more advanced disease (which may explain why no patients received concomitant CYC). Future trials should consider enrichment of study populations to include patients with progressive disease to reduce the number of patients needed to detect a treatment effect33,34. A further limitation to be considered when reviewing the results from efficacy analyses is that ours was a small-scale exploratory study without a comparator group, and the dosing of MMF was also not uniform.

In our study, pirfenidone showed an acceptable tolerability profile in patients with SSc-ILD. While co-administration of MMF did not appear to affect overall tolerability, a longer dose titration may have a favorable effect on tolerability. Although these results have few immediate clinical implications, the findings from the LOTUSS study are encouraging and permit further investigation of the efficacy and longterm safety of pirfenidone in future clinical trials in patients with SSc-ILD.

ONLINE SUPPLEMENT

Supplementary data for this article are available online at jrheum.org.

Acknowledgment

The authors thank all the patients who consented to participate in our exploratory study. The authors thank Dr. Renato Carignola, Clinical Rheumatologist, at the Scleroderma Unit, University of Turin, for his helpful contributions to the Multidisciplinary Interstitial Lung Disease Group discussions. The authors acknowledge David Kardatzke and Chin-Yu Lin of Roche-Genentech, and Hong Tang, formerly of InterMune, for their work on the statistical analyses for the LOTUSS study. Medical writing support was provided by Lauren Donaldson, on behalf of Complete Medical Communications Ltd., funded by F. Hoffmann-La Roche Ltd.

Footnotes

  • Dr. Seibold and Dr. Gorina are joint senior authors.

  • Full Release Article. For details see Reprints/Permissions at jrheum.org.

  • Supported by InterMune Inc., which became a wholly owned subsidiary of F. Hoffmann-La Roche Ltd. in 2014. C.A. has received consulting fees from InterMune. E.S. has received a grant from InterMune to conduct this study. D.C., M.T., and E.G. were employees of InterMune at the time this study was conducted. J.R.S. has received consulting fees from InterMune.

  • Accepted for publication May 27, 2016.

Free online via JRheum Full Release option

REFERENCES

  1. 1.
    1. van den Hoogen F,
    2. Khanna D,
    3. Fransen J,
    4. Johnson SR,
    5. Baron M,
    6. Tyndall A,
    7. et al.
    2013 classification criteria for systemic sclerosis: an American College of Rheumatology/European League against Rheumatism collaborative initiative. Arthritis Rheum 2013;65:273747.
    OpenUrlCrossRefPubMed
  2. 2.
    1. Solomon JJ,
    2. Olson AL,
    3. Fischer A,
    4. Bull T,
    5. Brown KK,
    6. Raghu G
    . Scleroderma lung disease. Eur Respir Rev 2013;22:619.
    OpenUrlFREE Full Text
  3. 3.
    1. Steen VD,
    2. Medsger TA
    . Changes in causes of death in systemic sclerosis, 1972–2002. Ann Rheum Dis 2007;66:9404.
    OpenUrlAbstract/FREE Full Text
  4. 4.
    1. Khanna D,
    2. Seibold JR,
    3. Wells A,
    4. Distler O,
    5. Allanore Y,
    6. Denton C,
    7. et al.
    Systemic sclerosis-associated interstitial lung disease: lessons from clinical trials, outcome measures, and future study design. Curr Rheumatol Rev 2010;6:13844.
    OpenUrlCrossRefPubMed
  5. 5.
    1. Herzog EL,
    2. Mathur A,
    3. Tager AM,
    4. Feghali-Bostwick C,
    5. Schneider F,
    6. Varga J
    . Review: interstitial lung disease associated with systemic sclerosis and idiopathic pulmonary fibrosis: how similar and distinct? Arthritis Rheumatol 2014;66:196778.
    OpenUrlCrossRefPubMed
  6. 6.
    1. Bouros D,
    2. Wells AU,
    3. Nicholson AG,
    4. Colby TV,
    5. Polychronopoulos V,
    6. Pantelidis P,
    7. et al.
    Histopathologic subsets of fibrosing alveolitis in patients with systemic sclerosis and their relationship to outcome. Am J Respir Crit Care Med 2002;165:15816.
    OpenUrlCrossRefPubMed
  7. 7.
    1. Kowal-Bielecka O,
    2. Landewé R,
    3. Avouac J,
    4. Chwiesko S,
    5. Miniati I,
    6. Czirjak L,
    7. et al;
    8. EUSTAR Co-Authors
    . EULAR recommendations for the treatment of systemic sclerosis: a report from the EULAR Scleroderma Trials and Research group (EUSTAR). Ann Rheum Dis 2009;68:6208.
    OpenUrlAbstract/FREE Full Text
  8. 8.
    1. Bussone G,
    2. Mouthon L
    . Interstitial lung disease in systemic sclerosis. Autoimmun Rev 2011;10:24855.
    OpenUrlCrossRefPubMed
  9. 9.
    1. Tashkin DP,
    2. Elashoff R,
    3. Clements PJ,
    4. Goldin J,
    5. Roth MD,
    6. Furst DE,
    7. et al;
    8. Scleroderma Lung Study Research Group
    . Cyclophosphamide versus placebo in scleroderma lung disease. N Engl J Med 2006;354:265566.
    OpenUrlCrossRefPubMed
  10. 10.
    1. Cappelli S,
    2. Guiducci S,
    3. Bellando Randone S,
    4. Matucci Cerinic M
    . Immunosuppression for interstitial lung disease in systemic sclerosis. Eur Respir Rev 2013;22:23643.
    OpenUrlAbstract/FREE Full Text
  11. 11.
    1. Schoenfeld SR,
    2. Castelino FV
    . Interstitial lung disease in scleroderma. Rheum Dis Clin North Am 2015;41:23748.
    OpenUrlCrossRefPubMed
  12. 12.
    1. Clements PJ,
    2. Tashkin D,
    3. Roth M,
    4. Khanna D,
    5. Furst DE,
    6. Tseng CH,
    7. et al.
    The Scleroderma Lung Study II (SLS II) shows that both oral cyclophosphamide (CYC) and mycophenolate mofitil (MMF) are efficacious in treating progressive interstitial lung disease (ILD) in patients with systemic sclerosis (SSc) [abstract]. Arthritis Rheumatol 2015;67 Suppl 10:14012.
    OpenUrl
  13. 13.
    1. Schaefer CJ,
    2. Ruhrmund DW,
    3. Pan L,
    4. Seiwert SD,
    5. Kossen K
    . Antifibrotic activities of pirfenidone in animal models. Eur Respir Rev 2011;20:8597.
    OpenUrlAbstract/FREE Full Text
  14. 14.
    1. Nakazato H,
    2. Oku H,
    3. Yamane S,
    4. Tsuruta Y,
    5. Suzuki R
    . A novel antifibrotic agent pirfenidone suppresses tumor necrosis factor-alpha at the translational level. Eur J Pharmacol 2002;446:17785.
    OpenUrlCrossRefPubMed
  15. 15.
    1. Iyer SN,
    2. Hyde DM,
    3. Giri SN
    . Anti-inflammatory effect of pirfenidone in the bleomycin-hamster model of lung inflammation. Inflammation 2000;24:47791.
    OpenUrlCrossRefPubMed
  16. 16.
    1. European Medicines Agency
    . Esbriet: pirfenidone. [Internet. Accessed May 30, 2016.] Available from: www.ema.europa.eu/ema/index.jsp?curl=pages/medicines/human/medicines/002154/human_med_001417.jsp&mid=WC0b01ac058001d124
  17. 17.
    1. King TE Jr.,
    2. Bradford WZ,
    3. Castro-Bernardini S,
    4. Fagan EA,
    5. Glaspole I,
    6. Glassberg MK,
    7. et al.
    A phase 3 trial of pirfenidone in patients with idiopathic pulmonary fibrosis. N Engl J Med 2014;370:208392.
    OpenUrlCrossRefPubMed
  18. 18.
    1. Noble PW,
    2. Albera C,
    3. Bradford WZ,
    4. Costabel U,
    5. Glassberg MK,
    6. Kardatzke D,
    7. et al;
    8. CAPACITY Study Group
    . Pirfenidone in patients with idiopathic pulmonary fibrosis (CAPACITY): two randomised trials. Lancet 2011;377:17609.
    OpenUrlCrossRefPubMed
  19. 19.
    1. Genentech
    . Esbriet prescribing information. [Internet. Accessed May 30, 2016.] Available from: www.gene.com/download/pdf/esbriet_prescribing.pdf
  20. 20.
    1. Raghu G,
    2. Collard HR,
    3. Egan JJ,
    4. Martinez FJ,
    5. Behr J,
    6. Brown KK,
    7. et al;
    8. ATS/ERS/JRS/ALAT Committee on Idiopathic Pulmonary Fibrosis
    . An official ATS/ERS/JRS/ALAT statement: idiopathic pulmonary fibrosis: evidence-based guidelines for diagnosis and management. Am J Respir Crit Care Med 2011;183:788824.
    OpenUrlCrossRefPubMed
  21. 21.
    1. King TE Jr.,
    2. Pardo A,
    3. Selman M
    . Idiopathic pulmonary fibrosis. Lancet 2011;378:194961.
    OpenUrlCrossRefPubMed
  22. 22.
    1. Albera C,
    2. Bradford WZ,
    3. Costabel U,
    4. Fagan EA,
    5. Glaspole I,
    6. Glassberg MK,
    7. et al.
    Pirfenidone is efficacious in patients with idiopathic pulmonary fibrosis (IPF) and mild restrictive disease [abstract]. Am J Respir Crit Care Med 2015;191:A1018.
    OpenUrl
  23. 23.
    1. Noble PW,
    2. Albera C,
    3. Bradford WZ,
    4. Costabel U,
    5. du Bois RM,
    6. Fagan EA,
    7. et al.
    Pirfenidone for idiopathic pulmonary fibrosis: analysis of pooled data from three multinational phase 3 trials. Eur Respir J 2016;47:24353.
    OpenUrlAbstract/FREE Full Text
  24. 24.
    1. Rigamonti C,
    2. Bogdanos DP,
    3. Mytilinaiou MG,
    4. Smyk DS,
    5. Rigopoulou EI,
    6. Burroughs AK
    . Primary biliary cirrhosis associated with systemic sclerosis: diagnostic and clinical challenges. Int J Rheumatol 2011;2011:976427.
    OpenUrlPubMed
  25. 25.
    1. Savarino E,
    2. Furnari M,
    3. de Bortoli N,
    4. Martinucci I,
    5. Bodini G,
    6. Ghio M,
    7. et al.
    Gastrointestinal involvement in systemic sclerosis. Presse Med 2014;43:e27991.
    OpenUrlCrossRefPubMed
  26. 26.
    Preliminary criteria for the classification of systemic sclerosis (scleroderma). Subcommittee for scleroderma criteria of the American Rheumatism Association Diagnostic and Therapeutic Criteria Committee. Arthritis Rheum 1980;23:58190.
    OpenUrlCrossRefPubMed
  27. 27.
    1. Khanna D,
    2. Hays RD,
    3. Maranian P,
    4. Seibold JR,
    5. Impens A,
    6. Mayes MD,
    7. et al.
    Reliability and validity of the University of California, Los Angeles Scleroderma Clinical Trial Consortium Gastrointestinal Tract Instrument. Arthritis Rheum 2009;61:125763.
    OpenUrlCrossRefPubMed
  28. 28.
    1. Cancer Therapy Evaluation Program
    . Common terminology criteria for adverse events, version 3.0 (CTCAE). [Internet. Accessed May 30, 2016.] Available from: ctep.cancer.gov/protocolDevelopment/electronic_applications/docs/ctcaev3.pdf
  29. 29.
    1. Valeyre D,
    2. Albera C,
    3. Bradford WZ,
    4. Costabel U,
    5. King TE Jr.,
    6. Leff JA,
    7. et al.
    Comprehensive assessment of the long-term safety of pirfenidone in patients with idiopathic pulmonary fibrosis. Respirology 2014;19:7407.
    OpenUrlCrossRefPubMed
  30. 30.
    1. Bae S,
    2. Allanore Y,
    3. Furst DE,
    4. Bodukam V,
    5. Coustet B,
    6. Morgaceva O,
    7. et al.
    Associations between a scleroderma-specific gastrointestinal instrument and objective tests of upper gastrointestinal involvements in systemic sclerosis. Clin Exp Rheumatol 2013;31 Suppl 76:5763.
    OpenUrl
  31. 31.
    1. Khanna D,
    2. Furst DE,
    3. Maranian P,
    4. Seibold JR,
    5. Impens A,
    6. Mayes MD,
    7. et al.
    Minimally important differences of the UCLA Scleroderma Clinical Trial Consortium Gastrointestinal Tract Instrument. J Rheumatol 2011;38:19204.
    OpenUrlAbstract/FREE Full Text
  32. 32.
    1. Behrend M
    . Adverse gastrointestinal effects of mycophenolate mofetil: aetiology, incidence and management. Drug Saf 2001;24:64563.
    OpenUrlCrossRefPubMed
  33. 33.
    1. Khanna D,
    2. Brown KK,
    3. Clements PJ,
    4. Elashoff R,
    5. Furst DE,
    6. Goldin J,
    7. et al.
    Systemic sclerosis-associated interstitial lung disease-proposed recommendations for future randomized clinical trials. Clin Exp Rheumatol 2010;28 Suppl 58:S5562.
    OpenUrlPubMed
  34. 34.
    1. Khanna D,
    2. Nagaraja V,
    3. Tseng CH,
    4. Abtin F,
    5. Suh R,
    6. Kim G,
    7. et al.
    Predictors of lung function decline in scleroderma-related interstitial lung disease based on high-resolution computed tomography: implications for cohort enrichment in systemic sclerosis-associated interstitial lung disease trials. Arthritis Res Ther 2015;17:372.
    OpenUrlCrossRefPubMed
View Abstract
Back to top

In this issue

Print
Download PDF
Article Alerts
Email Article
Citation Tools

 Request Permissions

Bookmark this article

Jump to section

Keywords

SYSTEMIC SCLEROSIS
SCLERODERMA
INTERSTITIAL LUNG DISEASES
PIRFENIDONE
SAFETY
TOLERABILITY

Keywords