Skip to main content

Main menu

  • Home
  • Content
    • First Release
    • Current
    • Archives
    • Collections
    • Audiovisual Rheum
    • COVID-19 and Rheumatology
  • Resources
    • Guide for Authors
    • Submit Manuscript
    • Payment
    • Reviewers
    • Advertisers
    • Classified Ads
    • Reprints and Translations
    • Permissions
    • Meetings
    • FAQ
    • Policies
  • Subscribers
    • Subscription Information
    • Purchase Subscription
    • Your Account
    • Terms and Conditions
  • About Us
    • About Us
    • Editorial Board
    • Letter from the Editor
    • Duncan A. Gordon Award
    • Privacy/GDPR Policy
    • Accessibility
  • Contact Us
  • JRheum Supplements
  • Services

User menu

  • My Cart
  • Log In
  • Log Out

Search

  • Advanced search
The Journal of Rheumatology
  • JRheum Supplements
  • Services
  • My Cart
  • Log In
  • Log Out
The Journal of Rheumatology

Advanced Search

  • Home
  • Content
    • First Release
    • Current
    • Archives
    • Collections
    • Audiovisual Rheum
    • COVID-19 and Rheumatology
  • Resources
    • Guide for Authors
    • Submit Manuscript
    • Payment
    • Reviewers
    • Advertisers
    • Classified Ads
    • Reprints and Translations
    • Permissions
    • Meetings
    • FAQ
    • Policies
  • Subscribers
    • Subscription Information
    • Purchase Subscription
    • Your Account
    • Terms and Conditions
  • About Us
    • About Us
    • Editorial Board
    • Letter from the Editor
    • Duncan A. Gordon Award
    • Privacy/GDPR Policy
    • Accessibility
  • Contact Us
  • Follow jrheum on Twitter
  • Visit jrheum on Facebook
  • Follow jrheum on LinkedIn
  • Follow jrheum on YouTube
  • Follow jrheum on Instagram
  • Follow jrheum on RSS
Research ArticlePsoriatic Arthritis

Comparison of Composite Indices Tailored for Psoriatic Arthritis Treated with csDMARD and bDMARD: A Cross-sectional Analysis of a Longitudinal Cohort

Ennio Lubrano, Antonia De Socio and Fabio Massimo Perrotta
The Journal of Rheumatology August 2017, 44 (8) 1159-1164; DOI: https://doi.org/10.3899/jrheum.170112
Ennio Lubrano
From the Dipartimento di Medicina e Scienze della Salute Vincenzo Tiberio, Università degli Studi del Molise, Campobasso, Italy.
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site
  • For correspondence: enniolubrano@hotmail.com
Antonia De Socio
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site
Fabio Massimo Perrotta
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site
  • Article
  • Figures & Data
  • Info & Metrics
  • References
  • PDF
  • eLetters
PreviousNext
Loading

Abstract

Objective. In a complex disease such as psoriatic arthritis (PsA), several methods are available to define remission or low disease activity (LDA), including the assessment of different clinical features. The aim of this study was to compare the composite indices tailored for PsA in patients treated with conventional synthetic disease-modifying antirheumatic drugs (csDMARD) and biological DMARD (bDMARD).

Methods. Patients with PsA classified with the ClASsification criteria for Psoriatic ARthritis criteria and with > 6 months followup treated with first csDMARD and bDMARD were consecutively enrolled. To assess disease activity, composite indices tailored for PsA were used, such as the Disease Activity Index for Psoriatic Arthritis (DAPSA), clinical DAPSA (cDAPSA), Psoriatic Arthritis Disease Activity Score (PASDAS), minimal disease activity (MDA) 5/7, and MDA 7/7. DAPSA and cDAPSA score ≤ 4, MDA 7/7, and PASDAS ≤ 1.9 identified remission. MDA 5/7, DAPSA score ≤ 14, cDAPSA score ≤ 13, and PASDAS < 3.2 identified the MDA and LDA criteria.

Results. One hundred nine patients with PsA were enrolled: 79 patients were receiving stable treatment with bDMARD and 30 with csDMARD. Overall, 28 (25.6%), 23 (21.1%), 19 (17.4%), and 13 patients (11.9%) were in cDAPSA remission, DAPSA remission, MDA 7/7, and PASDAS ≤ 1.9, respectively. Moreover, 54 (49.5%), 80 (73.3%), 79 (72.3%), and 38 patients (34.8%) were in MDA 5/7, DAPSA LDA, cDAPSA LDA, and PASDAS LDA. Patients treated with bDMARD had significantly lower median DAPSA, cDAPSA, and PASDAS score than patients treated with csDMARD.

Conclusion. Patients with PsA receiving bDMARD are more likely to achieve a status of MDA and remission when compared with csDMARD. PASDAS ≤ 1.9 and MDA 7/7 seem to be stringent remission criteria.

Key Indexing Terms:
  • PSORIATIC ARTHRITIS
  • REMISSION
  • COMPOSITE INDICES
  • BIOLOGIC THERAPY
  • DMARD

Psoriatic arthritis (PsA) is a multifaceted chronic inflammatory disease characterized by association of psoriasis and arthritis1. The peripheral joint involvement of PsA seems to be progressive in the majority of patients, and the presence of enthesitis, dactylitis, axial disease, cutaneous involvement, and extraarticular manifestations reinforces the need for optimal management and treatment strategies1,2. Moreover, patients with PsA have functional impairment, reduced quality of life, and a significant increase in mortality compared with the general population3. In the context of the disease, there are still different unmet needs that should be addressed, mainly on treatment strategies to achieve the best possible disease control such as disease remission or low disease activity (LDA)4. Tumor necrosis factor-α (TNF-α) blockers showed to be effective in clinical trials and in real-life experiences, with the possibility to induce a state of remission or LDA5,6,7,8,9. More recently, new treatment strategies with biologic disease-modifying antirheumatic drugs (bDMARD) and targeted synthetic DMARD, such as the inhibitors of interleukin (IL)-12/23, IL-17A, and phosphodiesterase 4, have shown to be effective in clinical trials10,11,12. However, the latest Group for Research and Assessment of Psoriasis and Psoriatic Arthritis (GRAPPA)13 and European League Against Rheumatism14 recommendations still proposed conventional synthetic DMARD (csDMARD) such as methotrexate (MTX), sulfasalazine (SSZ), and leflunomide as a first step in treatment of peripheral joint involvement in PsA, although there are limited data on the possibility of inducing remission with these drugs15. The same concept of disease remission is still debated, and at present, there are different composite indices to assess remission16. Recently, the concept of minimal disease activity (MDA) has been introduced and validated for PsA. Concerning the latter point, Coates, et al developed a composite outcome measure as a target of treatment for patients with PsA that encompasses most of the disease domains17. Patients are considered in MDA when they satisfy 5/7 of the following criteria: tender joint count ≤ 1, swollen joint count ≤ 1, psoriasis activity and severity index ≤ 1 or body surface area (BSA) ≤ 3, patient pain visual analog scale (VAS) score of ≤ 15, patient’s global disease activity VAS score of ≤ 20, Health Assessment Questionnaire (HAQ) score ≤ 0.5, and tender entheseal points ≤ 1. These criteria were validated using interventional trial data17,18. The importance of disease control with the lowest grade of disease activity is justified because achieving sustained MDA (defined as MDA for over 12 mos at consecutive clinic visits) reduced radiographic joint damage progression over a 3-year period18. In a more recent study, the same authors proposed a more stringent definition of remission in which all 7/7 criteria had to be satisfied19. The GRAPPA Composite Exercise project recently developed the Psoriatic Arthritis Disease Activity Score (PASDAS), and different thresholds to identify disease activity were provided20,21, while Schoels, et al proposed the remission criteria for the Disease Activity Index for Psoriatic Arthritis (DAPSA)22, which can be calculated with or without C-reactive protein [CRP; clinical DAPSA (cDAPSA)]. There are a limited number of reports that assessed the MDA and the remission rate in patients with PsA treated with csDMARD and bDMARD in a real-life setting using specific measures tailored for PsA15,23. The aim of our study was to evaluate the remission or MDA in a group of patients with PsA consecutively seen in an outpatient clinic and regardless of the treatment strategy by using the composite indices validated and tailored for PsA.

MATERIALS AND METHODS

Patient selection

In our cross-sectional analysis of a longitudinal cohort, patients were enrolled at the Rheumatology Unit, Department of Medicine and Health Science, University of Molise, Campobasso, Italy. During the period January 1, 2016, to December 31, 2016, all patients with PsA who were receiving at least a 6-month followup treatment were considered potentially eligible for our study. Inclusion criteria were PsA classified with the ClASsification criteria for Psoriatic ARthritis criteria24, age > 18 years, at least 6 months of followup at the study visit, and stable treatment with a first csDMARD or bDMARD for at least 6 months. To assess MDA and remission, composite indices tailored for PsA [DAPSA, cDAPSA, PASDAS, MDA (5/7), and MDA (7/7)] were used. The subject’s written consent was obtained according to the Declaration of Helsinki and the study was approved by our institution. Ethics approval was not required for this study, in accordance with the policy of our institution.

Data collection

Patient data collection included a medical history, physical examination, current use of medications, and laboratory assessment. Demographics and disease characteristics including age, sex, disease duration, and pattern of articular manifestation were taken into account. The clinical assessment documented the number of tender joints (of the 68 assessed joints) and swollen joints (total of 66 joints), enthesitis, and dactylitis. Enthesitis was measured using the Leeds Enthesitis Index (LEI)25, and dactylitis as present/absent. Skin assessment included the Psoriasis Area Severity Index (PASI) score and the BSA26. The HAQ27 and the Medical Outcomes Study Short Form-3628 were used to assess function and quality of life. Patient’s global assessment (PtGA) and pain assessment on visual analog scale (VAS) were performed by all patients29. Physician’s global evaluation of disease on VAS was also recorded. Erythrocyte sedimentation rate and CRP were also collected.

Minimal disease activity and remission criteria

MDA was defined according to Coates, et al17. MDA 7/7 was satisfied when all 7 criteria were met19. DAPSA score was identified according to Nell-Duxneuner, et al and was calculated by adding the number of tender and swollen joints, VAS pain, PtGA, and CRP (mg/dl)30. The cDAPSA was calculated without the contribution of CRP22. PASDAS was calculated according to Helliwell, et al20. DAPSA and cDAPSA score ≤ 4, MDA 7/7, and PASDAS ≤ 1.9 identified remission, while MDA 5/7 was the minimal disease activity criterion, and PASDAS < 3.2, DAPSA ≤ 14, and cDAPSA ≤ 13 identified a condition of LDA19,21,22.

Statistical analysis

Categorical variables were analyzed by chi-square test with Yates correction or Fisher’s exact test. The significance of the differences was determined using the Mann–Whitney U test for unpaired samples. Correlations among the different variables were assessed using Spearman test for nonparametric variables. Concordance was assessed using Cohen κ and was considered as follows: < 0.20 = poor, 0.21–0.40 = fair, 0.41–0.60 = moderate, 0.61–0.80 = good, and 0.81–1.00 = very good. Sensitivity, specificity, and likelihood ratios were evaluated to assess the accuracy of the different criteria. P values < 0.05 were considered significant. Results were expressed as median (interquartile range).

RESULTS

In the study period, 109 patients with PsA satisfied the inclusion criteria and were enrolled. Of these, 79 patients were in stable treatment with bDMARD (32 with etanercept, 24 with adalimumab, 18 with golimumab, and 5 with ustekinumab) and 30 with csDMARD (28 with MTX and 2 with SSZ, monotherapy). Of the 79 patients receiving bDMARD treatment, 14 were in combination therapy with MTX. Overall, median followup of our patients was 1.6 years. Overall, 28 (25.6%), 23 (21.1%), 19 (17.4%), and 13 patients (11.9%) with PsA were in cDAPSA remission, DAPSA remission, MDA 7/7, and PASDAS ≤ 1.9, respectively. On the other hand, 54 (49.5%), 80 (73.3%), 79 (72.3%), and 38 patients (34.8%) were in MDA 5/7, DAPSA LDA, cDAPSA LDA, and PASDAS LDA (Figure 1). As expected, patients receiving bDMARD had significantly lower median DAPSA, cDAPSA, and PASDAS scores than patients treated with csDMARD monotherapy (Table 1). Interestingly, the PASI score and enthesitis score (assessed by LEI) were also significantly lower in patients treated with bDMARD. A significant (p < 0.001) rate of patients receiving bDMARD treatment achieved a status of remission (cDAPSA score ≤ 4, DAPSA score ≤ 4), DAPSA LDA, MDA 5/7, and PASDAS LDA compared to csDMARD treatment. Although a higher rate of patients with PsA receiving bDMARD reached MDA 7/7 and PASDAS ≤ 1.9 compared to csDMARD, the differences were not significant (Table 2). Overall, the concordance between the indices ranged from poor to good. In particular, the highest agreement was found between MDA 7/7 and DAPSA and cDAPSA remission (κ= 0.63 and 0.65, respectively) while poor agreement (κ< 0.2) was found between DAPSA LDA and MDA 7/7 and PASDAS ≤ 1.9.

Figure 1.
  • Download figure
  • Open in new tab
  • Download powerpoint
Figure 1.

Overall rate (%) of PASDAS ≤ 1.9, PASDAS LDA, MDA 5/7, MDA 7/7, DAPSA remission, and DAPSA LDA in patients with psoriatic arthritis with > 6 months of followup treatment with bDMARD and csDMARD, according to the different definitions. PASDAS: Psoriatic Arthritis Disease Activity Score; LDA: low disease activity; MDA: minimal disease activity, DAPSA: Disease Activity Index for Psoriatic Arthritis; DMARD: disease-modifying antirheumatic drug; bDMARD: biological DMARD; csDMARD: conventional synthetic DMARD.

View this table:
  • View inline
  • View popup
Table 1.

Demographic and clinical disease activity characteristics in patients treated with bDMARD and csDMARD. Values are median (interquartile range) unless otherwise specified.

View this table:
  • View inline
  • View popup
Table 2.

Percentage of PASDAS ≤ 1.9, PASDAS LDA, MDA 5/7, MDA 7/7, DAPSA ≤ 4, or DAPSA LDA in patients treated with bDMARD and csDMARD therapy. Values are n (%).

Accuracy of the criteria

Table 3 shows the sensitivity, specificity, and likelihood ratio of the different scores compared to physician’s definition of remission (physician VAS < 10 mm). The composite indices with the most stringent criteria provide the high specificity for remission, although they lack sensitivity. Table 4 shows which disease domains were not satisfied by the different composite indices. In our analysis, a percentage of patients with PsA ranging from 18.5 to 33.7 that satisfied the different criteria had a PASI score > 1.

View this table:
  • View inline
  • View popup
Table 3.

Sensitivity and specificity of the different indices regarding physician VAS < 10 mm.

View this table:
  • View inline
  • View popup
Table 4.

No. and rate of patients with PsA who achieved PASDAS ≤ 1.9, PASDAS LDA, MDA 5/7, MDA 7/7, DAPSA ≤ 4, or DAPSA LDA with residual disease activity/functional impairment in the single domains. Values are n (%).

DISCUSSION

Remission or LDA status is the goal of therapy in chronic inflammatory arthritis. In patients with axial spondyloarthritis treated with anti-TNF-α, remission could be achieved in 53.2% of the patients with the nonradiographic form and in 50.9% of the patients with ankylosing spondylitis in a setting of clinical practice31,32. In PsA, several tools could be used to assess disease activity and remission/LDA state16. Further, despite the wide use of bDMARD and their proven efficacy on all PsA manifestations, several patients in clinical practice still continue treatment with csDMARD for different reasons (good response to csDMARD, costs, contraindication/intolerance, or fear of biologic treatment). The need to achieve remission remains unmet in this group of patients. On the other hand, in recent years, the development of composite indices tailored for the assessment of PsA posed the question of which is the better tool to identify a state of real remission. Until a few years ago, the Disease Activity Score in 28 joints (DAS28) was still used to assess disease activity state and remission. In a previous study, we demonstrated that using this tool showed that about 69% of patients with PsA treated with anti-TNF achieved a DAS28 ≤ 2.6 after 12 months of therapy8. However, DAS28 is a measure tailored mainly for small joint involvement of the hands, while PsA is a real heterogeneous disease and this composite measure does not fully evaluate the multiple clinical domains of psoriatic disease (e.g., enthesitis, dactylitis, and axial and skin involvement).

In our present study of 109 patients with PsA, 28 (25.6%), 23 (21.1%), 19 (17.4%), and 13 patients (11.9%) with PsA were in cDAPSA remission, DAPSA remission, MDA 7/7, and PASDAS ≤ 1.9, respectively, while 54 (49.5%), 80 (73.3%), 79 (72.3%), and 38 patients (34.8%) were in MDA 5/7, DAPSA LDA, cDAPSA LDA, and PASDAS LDA. Further, MDA or remission was achieved at a higher rate in patients receiving bDMARD compared with csDMARD. While the rate of MDA or DAPSA remission in patients receiving bDMARD is very similar to that in other studies8,33, the rate of MDA/remission in patients receiving csDMARD was quite low. In fact, in the Tight Control Of inflammation in early Psoriatic Arthritis study, 22.4% of 188 patients with PsA treated with MTX achieved MDA after 12 months34, and in a recent study of 167 patients with PsA treated with MTX, 29 (17.4%) achieved MDA35. In our study, the rate of patients with > 6 months of followup in MDA status was similar (16.6%), underlining the difficulty of using csDMARD to induce a state of complete control of the disease activity, even when assessed with less stringent criteria. Moreover, our study shows that MDA 7/7 criteria and PASDAS ≤ 1.9 are the most stringent criteria to assess a status of remission. These 2 composite indices consist of all clinical manifestations of the disease (in the PASDAS, even the assessment of objective inflammation such as CRP) and probably represent the most complete criteria, even if MDA is, overall, easier to perform during clinical evaluation.

The data obtained seem to show that MDA is a reliable instrument to assess a low disease status in patients with PsA during chronic treatment, as well as PASDAS LDA. On the other hand, MDA 7/7 and PASDAS ≤ 1.9 seem to be reliable in assessing a condition of disease remission and this, in turn in our study, was more evident in those patients receiving bDMARD therapy. The analysis of sensitivity and specificity provide further useful information; regarding physician’s definition of remission, the composites indices with the most stringent criteria provide high specificity for remission, although they lack sensitivity. Although MDA 5/7 and DAPSA remission could not assess important domains, they provide good sensitivity and specificity. On this point, our results showed that a relatively high percentage of patients with PsA (ranging from 18.5 to 33.7) who satisfied the different criteria had a PASI score > 1, while a relatively low percentage of patients showed a residual disease activity in other domains such as enthesitis or had functional impairment (defined as both LEI > 1 and HAQ > 0.5; Table 4). Finally, DAPSA and cDAPSA LDA are good instruments to assess a low disease status, but their potential weakness is that they are instruments to evaluate only peripheral arthritis, with a risk of underestimating disease activity in important domains such as skin and enthesitis. In fact, a relatively high number of patients in DAPSA LDA still present active tender joints, enthesitis, or skin disease. Our present study could be of some interest because there are few reports on the rate of different ways to assess remission in PsA in real life.

Patients with PsA receiving bDMARD are more likely to achieve a status of MDA and remission compared to csDMARD. PASDAS ≤ 1.9 and MDA 7/7 seem to be stringent criteria.

  • Accepted for publication April 26, 2017.

REFERENCES

  1. 1.↵
    1. Gladman DD,
    2. Antoni C,
    3. Mease P,
    4. Clegg DO,
    5. Nash P
    . Psoriatic arthritis: epidemiology, clinical features, course, and outcome. Ann Rheum Dis 2005;64 Suppl 2:ii14–7.
    OpenUrlAbstract/FREE Full Text
  2. 2.↵
    1. McHugh NJ,
    2. Balachrishnan C,
    3. Jones SM
    . Progression of peripheral joint disease in psoriatic arthritis: a 5-yr prospective study. Rheumatology 2003;42:778–83.
    OpenUrlCrossRefPubMed
  3. 3.↵
    1. Gladman DD
    . Disability and quality of life considerations. Psoriatic arthritis. In: Gordon GB, Ruderman E, eds. Psoriasis and psoriatic arthritis: an integral approach. Heidelberg: Springer-Verlag; 2005:118–237.
  4. 4.↵
    1. Helliwell P,
    2. Coates L,
    3. Chandran V,
    4. Gladman D,
    5. de Wit M,
    6. FitzGerald O,
    7. et al.
    Qualifying unmet needs and improving standards of care in psoriatic arthritis. Arthritis Care Res 2014;66:1759–66.
    OpenUrlCrossRef
  5. 5.↵
    1. Perrotta FM,
    2. Lubrano E
    . Subcutaneous anti-TNF alfa induced sustained minimal disease activity and remission in psoriatic arthritis patients: a retrospective study. Postgrad Med 2016;128:693–6.
    OpenUrl
  6. 6.↵
    1. Ash Z,
    2. Gaujoux-Viala C,
    3. Gossec L,
    4. Hensor EM,
    5. FitzGerald O,
    6. Winthrop K,
    7. et al.
    A systematic literature review of drug therapies for the treatment of psoriatic arthritis: current evidence and meta-analysis informing the EULAR recommendations for the management of psoriatic arthritis. Ann Rheum Dis 2012;71:319–26.
    OpenUrlAbstract/FREE Full Text
  7. 7.↵
    1. Glintborg B,
    2. Østergaard M,
    3. Dreyer L,
    4. Krogh NS,
    5. Tarp U,
    6. Hansen MS,
    7. et al.
    Treatment response, drug survival, and predictors thereof in 764 patients with psoriatic arthritis treated with anti-tumor necrosis factor α therapy: results from the nationwide Danish DANBIO registry. Arthritis Rheum 2011;63:382–90.
    OpenUrlCrossRefPubMed
  8. 8.↵
    1. Perrotta FM,
    2. Marchesoni A,
    3. Lubrano E
    . Minimal disease activity and remission in psoriatic arthritis patients treated with anti-TNF-α drugs. J Rheumatol 2016;43:350–5.
    OpenUrlAbstract/FREE Full Text
  9. 9.↵
    1. Lubrano E,
    2. Parsons WJ,
    3. Perrotta FM
    . Assessment of response to treatment, remission, and minimal disease activity in axial psoriatic arthritis treated with tumor necrosis factor inhibitors. J Rheumatol 2016;43:918–23.
    OpenUrlAbstract/FREE Full Text
  10. 10.↵
    1. Lubrano E,
    2. Perrotta FM
    . Secukinumab for ankylosing spondylitis and psoriatic arthritis. Ther Clin Risk Manag 2016;12:1587–92.
    OpenUrl
  11. 11.↵
    1. Perrotta FM,
    2. Lubrano E
    . New approved drugs for psoriatic arthritis. Reumatismo 2016;68:57–64.
    OpenUrl
  12. 12.↵
    1. Lubrano E,
    2. Perrotta FM
    . Beyond TNF inhibitors: new pathways and emerging treatments for psoriatic arthritis. Drugs 2016;76:663–73.
    OpenUrl
  13. 13.↵
    1. Coates LC,
    2. Kavanaugh A,
    3. Mease PJ,
    4. Soriano ER,
    5. Laura Acosta-Felquer M,
    6. Armstrong AW,
    7. et al.
    Group for Research and Assessment of Psoriasis and Psoriatic Arthritis 2015 Treatment Recommendations for Psoriatic Arthritis. Arthritis Rheumatol 2016;68:1060–71.
    OpenUrl
  14. 14.↵
    1. Gossec L,
    2. Smolen JS,
    3. Ramiro S,
    4. de Wit M,
    5. Cutolo M,
    6. Dougados M,
    7. et al.
    European League Against Rheumatism (EULAR) recommendations for the management of psoriatic arthritis with pharmacological therapies: 2015 update. Ann Rheum Dis 2016;75:499–510.
    OpenUrlAbstract/FREE Full Text
  15. 15.↵
    1. Lubrano E,
    2. Soriano E,
    3. FitzGerald O
    . Can traditional disease-modifying anti-rheumatic drugs be withdrawn or tapered in psoriatic arthritis? Clin Exp Rheumatol 2013;31 Suppl 78:S54–8
    OpenUrlPubMed
  16. 16.↵
    1. Lubrano E,
    2. Perrotta FM,
    3. Kavanaugh A
    . An overview of low disease activity and remission in psoriatic arthritis. Clin Exp Rheumatol 2015;33 Suppl 93:51–4.
    OpenUrl
  17. 17.↵
    1. Coates LC,
    2. Fransen J,
    3. Helliwell PS
    . Defining minimal disease activity in psoriatic arthritis: a proposed objective target for treatment. Ann Rheum Dis 2010;69:48–53.
    OpenUrlAbstract/FREE Full Text
  18. 18.↵
    1. Coates L,
    2. Helliwell P
    . Validation of minimal disease activity criteria for psoriatic arthritis using interventional trial data. Arthritis Car Res 2010;62;965–9.
    OpenUrl
  19. 19.↵
    1. Coates LC,
    2. Helliwell PS
    . Defining low disease activity states in psoriatic arthritis using novel composite disease instruments. J Rheumatol 2016;43:371–5.
    OpenUrlAbstract/FREE Full Text
  20. 20.↵
    1. Helliwell PS,
    2. FitzGerald O,
    3. Fransen J,
    4. Gladman DD,
    5. Kreuger GG,
    6. Callis-Duffin K,
    7. et al.
    The development of candidate composite disease activity and responder indices for psoriatic arthritis (GRACE project). Ann Rheum Dis 2013;72:986–91.
    OpenUrlAbstract/FREE Full Text
  21. 21.↵
    1. Helliwell PS,
    2. FitzGerald O,
    3. Fransen J
    . Composite disease activity and responder indices for psoriatic arthritis: a report from the GRAPPA 2013 meeting on development of cutoffs for both disease activity states and response. J Rheumatol 2014;41:1212–7.
    OpenUrlAbstract/FREE Full Text
  22. 22.↵
    1. Schoels MM,
    2. Aletaha D,
    3. Alasti F,
    4. Smolen JS
    . Disease activity in psoriatic arthritis (PsA): defining remission and treatment success using the DAPSA score. Ann Rheum Dis 2016;75:811–8.
    OpenUrlAbstract/FREE Full Text
  23. 23.↵
    1. Soriano ER
    . The actual role of therapy with traditional disease-modifying antirheumatic drugs in psoriatic arthritis. J Rheumatol 2012;89:67–70.
    OpenUrl
  24. 24.↵
    1. Taylor W,
    2. Gladman D,
    3. Helliwell P,
    4. Marchesoni A,
    5. Mease P,
    6. Mielants H;
    7. CASPAR Study Group
    . Classification criteria for psoriatic arthritis: development of new criteria from a large international study. Arthritis Rheum 2006;54:2665–73.
    OpenUrlCrossRefPubMed
  25. 25.↵
    1. Healy PJ,
    2. Helliwell PS
    . Measuring clinical enthesitis in psoriatic arthritis: assessment of existing measures and development of an instrument specific to psoriatic arthritis. Arthritis Rheum 2008;59:686–91.
    OpenUrlCrossRefPubMed
  26. 26.↵
    1. Chandran V,
    2. Gottlieb A,
    3. Cook RJ,
    4. Duffin KC,
    5. Garg A,
    6. Helliwell P,
    7. et al.
    International multicenter psoriasis and psoriatic arthritis reliability trial for the assessment of skin, joints, nails, and dactylitis. Arthritis Rheum 2009;61:1235–42.
    OpenUrlCrossRefPubMed
  27. 27.↵
    1. Ranza R,
    2. Marchesoni A,
    3. Calori G,
    4. Bianchi G,
    5. Braga M,
    6. Canazza S,
    7. et al.
    The Italian version of the Functional Disability Index of the Health Assessment Questionnaire. A reliable instrument for multicenter studies on rheumatoid arthritis. Clin Exp Rheumatol 1993;11:123–8.
    OpenUrlPubMed
  28. 28.↵
    1. Ware JE Jr,
    2. Sherbourne CD
    . The MOS 36-item short-form health survey (SF-36). I. Conceptual framework and item selection. Med Care 1992;30:473–83.
    OpenUrlCrossRefPubMed
  29. 29.↵
    1. Cauli A,
    2. Gladman DD,
    3. Mathieu A,
    4. Olivieri I,
    5. Porru G,
    6. Tak PP,
    7. et al;
    8. GRAPPA 3PPsA Study Group
    . Patient global assessment in psoriatic arthritis: a multicenter GRAPPA and OMERACT study. J Rheumatol 2011;38:898–903.
    OpenUrlAbstract/FREE Full Text
  30. 30.↵
    1. Nell-Duxneuner VP,
    2. Stamm TA,
    3. Machold KP,
    4. Pflugbeil S,
    5. Aletaha D,
    6. Smolen JS
    . Evaluation of the appropriateness of composite disease activity measures for assessment of psoriatic arthritis. Ann Rheum Dis 2010;69:546–9.
    OpenUrlAbstract/FREE Full Text
  31. 31.↵
    1. Lubrano E,
    2. Perrotta FM,
    3. Marchesoni A,
    4. D’Angelo S,
    5. Ramonda R,
    6. Addimanda O,
    7. et al.
    Remission in nonradiographic axial spondyloarthritis treated with anti-tumor necrosis factor-α drugs: an Italian multicenter study. J Rheumatol 2015;42:258–63.
    OpenUrlAbstract/FREE Full Text
  32. 32.↵
    1. Spadaro A,
    2. Lubrano E,
    3. Marchesoni A,
    4. D’Angelo S,
    5. Ramonda R,
    6. Addimanda O,
    7. et al.
    Remission in ankylosing spondylitis treated with anti-TNF-α drugs: a national multicentre study. Rheumatology 2013;52:1914–9.
    OpenUrlCrossRefPubMed
  33. 33.↵
    1. Haddad A,
    2. Thavaneswaran A,
    3. Ruiz-Arruza I,
    4. Pellett F,
    5. Chandran V,
    6. Cook RJ,
    7. et al.
    Minimal disease activity and anti-tumor necrosis factor therapy in psoriatic arthritis. Arthritis Care Res 2015;67:842–7.
    OpenUrlCrossRef
  34. 34.↵
    1. Coates LC,
    2. Helliwell PS
    . Methotrexate efficacy in the tight control in psoriatic arthritis study. J Rheumatol 2016;43:356–61.
    OpenUrlAbstract/FREE Full Text
  35. 35.↵
    1. Sheane BJ,
    2. Thavaneswaran A,
    3. Gladman DD,
    4. Chandran V
    . Attainment of minimal disease activity using methotrexate in psoriatic arthritis. J Rheumatol 2016;43:1718–23.
    OpenUrlAbstract/FREE Full Text
PreviousNext
Back to top

In this issue

The Journal of Rheumatology
Vol. 44, Issue 8
1 Aug 2017
  • Table of Contents
  • Table of Contents (PDF)
  • Index by Author
  • Editorial Board (PDF)
Print
Download PDF
Article Alerts
Sign In to Email Alerts with your Email Address
Email Article

Thank you for your interest in spreading the word about The Journal of Rheumatology.

NOTE: We only request your email address so that the person you are recommending the page to knows that you wanted them to see it, and that it is not junk mail. We do not capture any email address.

Enter multiple addresses on separate lines or separate them with commas.
Comparison of Composite Indices Tailored for Psoriatic Arthritis Treated with csDMARD and bDMARD: A Cross-sectional Analysis of a Longitudinal Cohort
(Your Name) has forwarded a page to you from The Journal of Rheumatology
(Your Name) thought you would like to see this page from the The Journal of Rheumatology web site.
CAPTCHA
This question is for testing whether or not you are a human visitor and to prevent automated spam submissions.
Citation Tools
Comparison of Composite Indices Tailored for Psoriatic Arthritis Treated with csDMARD and bDMARD: A Cross-sectional Analysis of a Longitudinal Cohort
Ennio Lubrano, Antonia De Socio, Fabio Massimo Perrotta
The Journal of Rheumatology Aug 2017, 44 (8) 1159-1164; DOI: 10.3899/jrheum.170112

Citation Manager Formats

  • BibTeX
  • Bookends
  • EasyBib
  • EndNote (tagged)
  • EndNote 8 (xml)
  • Medlars
  • Mendeley
  • Papers
  • RefWorks Tagged
  • Ref Manager
  • RIS
  • Zotero

 Request Permissions

Share
Comparison of Composite Indices Tailored for Psoriatic Arthritis Treated with csDMARD and bDMARD: A Cross-sectional Analysis of a Longitudinal Cohort
Ennio Lubrano, Antonia De Socio, Fabio Massimo Perrotta
The Journal of Rheumatology Aug 2017, 44 (8) 1159-1164; DOI: 10.3899/jrheum.170112
Reddit logo Twitter logo Facebook logo Mendeley logo
  • Tweet Widget
  • Facebook Like
  • Google Plus One
Bookmark this article

Jump to section

  • Article
    • Abstract
    • MATERIALS AND METHODS
    • RESULTS
    • DISCUSSION
    • REFERENCES
  • Figures & Data
  • Info & Metrics
  • References
  • PDF
  • eLetters

Keywords

PSORIATIC ARTHRITIS
REMISSION
COMPOSITE INDICES
BIOLOGIC THERAPY
DMARD

Related Articles

Cited By...

More in this TOC Section

  • Sex-Based Differences in Sonographic and Clinical Findings Among Patients With Psoriatic Arthritis
  • Women With Psoriatic Arthritis Experience Higher Disease Burden Than Men: Findings From a Real-World Survey in the United States and Europe
  • Doppler Signal and Bone Erosions at the Enthesis Are Independently Associated With Ultrasound Joint Erosive Damage in Psoriatic Arthritis
Show more Psoriatic Arthritis

Similar Articles

Keywords

  • psoriatic arthritis
  • remission
  • COMPOSITE INDICES
  • biologic therapy
  • DMARD

Content

  • First Release
  • Current
  • Archives
  • Collections
  • Audiovisual Rheum
  • COVID-19 and Rheumatology

Resources

  • Guide for Authors
  • Submit Manuscript
  • Author Payment
  • Reviewers
  • Advertisers
  • Classified Ads
  • Reprints and Translations
  • Permissions
  • Meetings
  • FAQ
  • Policies

Subscribers

  • Subscription Information
  • Purchase Subscription
  • Your Account
  • Terms and Conditions

More

  • About Us
  • Contact Us
  • My Alerts
  • My Folders
  • Privacy/GDPR Policy
  • RSS Feeds
The Journal of Rheumatology
The content of this site is intended for health care professionals.
Copyright © 2022 by The Journal of Rheumatology Publishing Co. Ltd.
Print ISSN: 0315-162X; Online ISSN: 1499-2752
Powered by HighWire