Research ArticleOMERACT 11

Patient-reported Outcomes and Adult Patients’ Disease Experience in the Idiopathic Inflammatory Myopathies. Report from the OMERACT 11 Myositis Special Interest Group

Helene Alexanderson, Maria Del Grande, Clifton O. Bingham III, Ana-Maria Orbai, Catherine Sarver, Katherine Clegg-Smith, Ingrid E. Lundberg, Yeong Wook Song and Lisa Christopher-Stine
The Journal of Rheumatology March 2014, 41 (3) 581-592; DOI: https://doi.org/10.3899/jrheum.131247

Abstract

The newly formed Outcome Measures in Rheumatology (OMERACT) Myositis Special Interest Group (SIG) was established to examine patient-reported outcome measures (PROM) in myositis. At OMERACT 11, a literature review of PROM used in the idiopathic inflammatory myopathies (IIM) and other neuromuscular conditions was presented. The group examined in more detail 2 PROM more extensively evaluated in patients with IIM, the Myositis Activities Profile, and the McMaster-Toronto Arthritis Patient Preference Disability Questionnaire, through the OMERACT filter of truth, discrimination, and feasibility. Preliminary results from a qualitative study of patients with myositis regarding their symptoms were discussed that emphasized the range of symptoms experienced: pain, physical tightness/stiffness, fatigue, disease effect on emotional life and relationships, and treatment-related side effects. Following discussion of these results and following additional discussions since OMERACT 11, a research agenda was developed. The next step in evaluating PROM in IIM will require additional focus groups with a spectrum of patients with different myositis disease phenotypes and manifestations across a range of disease activity, and from multiple international settings. The group will initially focus on dermatomyositis and polymyositis in adults. Qualitative analysis will facilitate the identification of commonalities and divergent patient-relevant aspects of disease, insights that are critical given the heterogeneous manifestations of these diseases. Based on these qualitative studies, existing myositis PROM can be examined to more thoroughly assess content validity, and will be important to identify gaps in domain measurement that will be required to develop a preliminary core set of patient-relevant domains for IIM.

Key Indexing Terms:

The idiopathic inflammatory myopathies (IIM) are a heterogeneous group of diseases, but commonalities among them include proximal muscle weakness, elevated muscle enzymes, electromyogram (EMG) abnormalities including irritability, and muscle biopsies usually characterized by lymphocytic inflammation1. Evaluating people affected by IIM, which include dermatomyositis (DM), polymyositis (PM), inclusion body myositis (IBM), and immune-mediated necrotizing myopathy, is further complicated by extramuscular manifestations including interstitial lung disease (ILD), arthritis, Raynaud phenomenon, and other autoimmune features2. The cardinal clinical feature traditionally associated with IIM has been described as painless muscle weakness with limitations in activities of daily living (ADL) and quality of life (QOL)3,4, but few data are available concerning patients’ experience of the disease with detailed characterization of important symptoms and disease burden.

The International Myositis Assessment and Clinical Studies Group (IMACS) is a group of healthcare providers and researchers with experience and interest in the myositis syndromes. Represented by diverse subspecialties including rheumatology, neurology, dermatology, and physical medicine and rehabilitation, the goal of IMACS is research and discovery that improves the lives of those living with myositis. To date, through international collaborative efforts, IMACS members have developed consensus standards on the conduct and reporting of adult and juvenile myositis studies. The preliminary core set of measures of disease activity for myositis therapeutic trials developed by IMACS includes a physician global assessment of disease activity, muscle strength testing (e.g., strength, endurance), physical function, laboratory assessments [e.g., muscle enzymes such as creatine phosphokinase (CPK), imaging, biomarkers], and scoring of extramuscular disease activity5. This core set also includes several patient-reported outcome measures (PROM) such as the patient/parent report of disease activity, a measure of physical function/ADL. IMACS also recommends including a measure of health-related QOL (HRQOL), e.g., the generic Medical Outcome Study Short Form-36 survey (SF-36) in clinical studies5,6. While disease activity and damage core sets of measures have been derived and validated, no specific PROM have been developed under IMACS initiatives, although the group is undertaking an initiative to further assess fatigue in these diseases. Outcome Measures in Rheumatology (OMERACT) provides a complementary, non-overlapping approach to the IMACS work to date, uniquely bringing healthcare providers, patients, and other stakeholders together to facilitate research to evaluate, develop, and validate PROM under a well-established framework. Increasingly it has been emphasized that clinical trials and observational studies should include an assessment of the outcomes that matter most to patients. OMERACT has contributed substantially to this effort over the last decade, with the identification by patients of fatigue as a recommended core set measure in rheumatoid arthritis (RA) and the development of recommendations for a process of patient-reported outcome (PRO) domain selection7,8,9. Additional recommendations through the World Health Organization, regulatory agencies including the European Medicines Agency, and the US Food and Drug Administration through the critical pathway initiative, and the newly established patient-centered outcomes research institute in the USA have also emphasized the importance of PROM inclusion10,11,12,13. Most outcome measures in IIM to date, however, have focused on the pathophysiologic manifestations of these diseases (e.g., physical strength testing, EMG, CPK). Although PROM are widely used and applied in different disease areas in rheumatology and neurology, they have not been extensively studied in patients with IIM. While IMACS has recommended inclusion of certain PROM as part of their core set (patient global assessment, physical function), the extent to which these include the aspects of the disease most important to patients has not been well studied. In a Swedish study of 28 patients with myositis using the McMaster-Toronto Arthritis Patient Preference Disability Questionnaire (MACTAR) semistructured interview, several areas of health that were prioritized by patients, including sexual activity, social activities, and sleep, were not covered by items in standard assessments of physical function14 used most in myositis studies to date: the Health Assessment Questionnaire (HAQ)15, and the Myositis Activities Profile (MAP)16. OMERACT groups working in other diseases have demonstrated that patients and healthcare providers weigh domains differently in terms of perceived importance17,18,19.

The purpose of the Myositis Special Interest Group (SIG) is to evaluate existing PRO assessments used in IIM and to better understand the patient-valued aspects of the disease that will allow the delineation of domains that reflect important disease features. This will help inform subsequent PROM identification, development, and validation for IIM, which can then provide a more comprehensive assessment of IIM disease activity and burden.

METHODS

Overview of the OMERACT Myositis SIG

An organizing OMERACT Myositis SIG group meeting was held at the American College of Rheumatology (ACR) annual meeting in Chicago in 2011. Twenty-five attendees representing 8 countries were present. A 90-min SIG meeting was held at the OMERACT 11 conference in Pinehurst, North Carolina, USA, in May 2012 and was attended by 20 participants representing 5 countries (USA, Canada, Sweden, UK, and Japan), including 1 patient with myositis. The group met again at the European League Against Rheumatism (EULAR) June 2012 meeting in Berlin, Germany, with an expanded discussion on ensuring international representation of the group and further developing a research agenda. Individuals from 4 countries and 3 continents were represented. At the ACR meeting in Washington, DC, USA, the group met again to discuss how to move forward with a standardized focus group discussion guide that could be used across different nationalities.

Literature review of PRO used in IIM

We searched MEDLINE and trial registries from inception until June 2012. The search terms included “patient related outcome,” “patient reported outcome,” “patient centered outcome,” “assessment,” AND “dermatomyositis,” “juvenile dermatomyositis,” “polymyositis,” “immune-mediated necrotizing myopathy,” “inclusion body myositis,” and “idiopathic inflammatory myopathies.” Given the paucity of IIM-related PROM, we then broadened the search to additional neuromuscular diseases: “centronuclear myopathy,” “progressive muscular atrophy,” “spinal muscular atrophy,” “sarcopenia,” “Charcot-Marie-Tooth disease,” “muscular dystrophy,” “Duchenne muscular dystrophy,” “multiple sclerosis,” and “myasthenia gravis.” Articles that included only non-patient-centered outcomes were excluded. This approach was reviewed and agreed upon by the OMERACT Myositis SIG members at the ACR Annual Meeting, in November 2011 in Chicago. Additional articles known to the investigators and from the references in a review on outcome measures in myositis20 supplemented the above search. All retrieved data were summarized into a tabulated format according to the OMERACT criteria of truth, discrimination, and feasibility in the setting of myositis21.

Focus group

A 90-min focus group discussion was conducted with 7 patients with IIM seen at the Johns Hopkins Myositis Center. This study was conducted under the auspices of the Johns Hopkins Institutional Review Board, and all patients signed informed consent prior to any questionnaire completion or discussions. Patients completed a short questionnaire before the focus group that included demographics, disease duration, global assessment, pain, stiffness, fatigue, and the HAQ. The focus group was led by a qualitative researcher and a rheumatologist not involved with the care of the patients. Initial questions were non-directive, encouraging patients to discuss freely the way the disease affected their lives. Topics of great interest for multiple participants in the focus group were then prioritized. The focus group was recorded and transcribed, and all patient identifiers were removed to maintain anonymity. Data analysis was largely inductive and exploratory, with a goal of identifying and reporting on major thematic elements pertaining to patients’ experience of living with and being treated for myositis. The analytic process included use of qualitative software Atlas.ti. for data management as well as to facilitate an iterative consensus process among a team of clinical and behavioral scientists to identify common themes and consider their potential importance for understanding and improving patient experiences22.

Patient inclusion

One patient with DM and ILD participated in the Baltimore focus group and attended the OMERACT 11 Meeting in Pinehurst as a patient research partner (PRP). During the Myositis SIG meeting, she shared her detailed experience of living with inflammatory myopathy and the effect of the disease on her life, as well as her experience as a participant in the focus group and as a PRP at OMERACT 11.

RESULTS

Literature review

We reviewed the literature concerning PROM in IIM with regard to use and validation. In our initial analysis we found that the spectrum of PRO domains studied in patients with IIM was limited to patient/parent global assessment, physical function, HRQOL, pain, and fatigue. When the search was expanded to other neuromuscular conditions, we found that many additional domains had been studied. These included psychological function (mood, including depression) and the effect of IIM on pain interference, sleep, coping, cognitive functioning, occupational and leisure activities, satisfaction with life roles and activities, social supports, health utilities (European Quality of Life), and a number of disease-specific QOL and functional status measures (data not shown). Several short forms reflecting domains within the Patient Reported Outcome Measurement Information System framework including pain interference, sleep, fatigue, depression, and satisfaction with social roles have been evaluated in multiple sclerosis and muscular dystrophy23. Table 1 outlines the domains that have been used in IIM and evaluates instruments in the context of the OMERACT Filter 1.0. Most of the instruments that have been evaluated in IIM were generic instruments or were adopted from use in other rheumatic or neuromuscular diseases. We identified only 1 instrument, the MAP, that was created specifically for adult PM and DM16 and 1, the MACTAR14, that was adapted for these 2 diagnoses. In addition, the IBM Functional Rating Scale (IBMFRS) was created and validated for patients with IBM while the QOL scores Individualized Neuromuscular Quality of Life Questionnaire and Childhood Health Questionnaire (CHQ), and activity limitation scales such as Child Health Assessment Questionnaire (CHAQ) and parent’s global assessment, were validated for juvenile myositis24,25,26,27. Other scores that have been used in these disorders include the Neuromuscular Symptom and Disability Functional Score, the Amyotrophic Lateral Sclerosis Functional Rating Scale, and the Barthel’s ADL Index28,29,30.

View this table:
Table 1.

Patient-reported outcomes used in idiopathic inflammatory myopathies outlined according to the OMERACT Filter 1.0 (numerals in parentheses are references).

The OMERACT Filter 1.0 was created to set a standard for the validation process and applicability of PROM and can be summarized as truth, discrimination, and feasibility21. The 22 PROM that were identified and used in juvenile or adult myositis are outlined in Table 1 according to the OMERACT Filter components in myositis with definitions of “low,” “moderate,” or “high” validity or reliability. High content validity reflects patient involvement from qualitative research, moderate as patients being partly involved, and low with no patient input. Spearman correlation coefficients for analysis of construct or criterion validity were defined as rs 0–0.25 (no or very low correlation), 0.26–0.49 (low), 0.50–0.69 (moderate), 0.70–0.89 (good), and 0.90–1.00 (very high correlation)31. For analysis of item fit within their subscale, Cronbach’s alpha coefficients < 0.70 were defined as inadequate32. Test-retest reliability was defined as weighted kappa coefficients of 0–0.20 (no or low agreement), 0.21–0.40 (fair), 0.41–0.60 (moderate), 0.61–0.80 (substantial), and 0.81–1.00 (almost perfect agreement)33. We defined high sensitivity to change as demonstrating clinically relevant and statistically significant changes, moderate sensitivity showing only statistically significant changes, and low sensitivity to change as no significant changes. We defined examiner burden as low when scores can be calculated by hand in a short time and high when a software program is not available to score complicated scores. Examiner burden also involved costs of requiring measures or software limiting feasibility. High respondent burden was defined as more than 10 min to complete. We indicated only the languages in which the outcome was used in myositis.

The PROM used in juvenile myositis (e.g., CHAQ and CHQ) have been more extensively validated than those for adult IIM. The SF-36 and HAQ-DI were not validated in IIM; however, the SF-36 has good construct and criterion validity, according to our definition, and good feasibility, but discrimination is not defined20. HAQ-DI has only good feasibility and fair construct validity. Only 1 PROM used in myositis was specifically developed for adult PM or DM (MAP)16, and 1 was validated for adult PM and DM (MACTAR semistructured interview)14.

Truth, discrimination, and feasibility of PRO in myositis. OMERACT Filter 1.0: MAP and MACTAR

Only 2 nongeneric, validated PRO have been validated in adult PM and DM, the MAP16; and the MACTAR14, according to the OMERACT Filter21. Alexanderson, et al created the disease-specific MAP questionnaire to assess limitations, difficulty, and importance in daily activities of PM and DM in adult patients in Sweden16. The MAP consists of 31 items divided into 4 subscales (movement, moving around, personal hygiene, domestic) and 4 single items (social activities, avoiding overexertion, work/school, leisure activities). Each subscale is scored separately. The MAP has been translated into English and studied in US patients with PM and DM34.

The MACTAR was originally developed for patients with RA as a self-administered questionnaire35. A French version was also used in systemic sclerosis36. The MACTAR was later adapted into a semistructured interview format that requires administration by a trained interviewer. Its validity and responsiveness was demonstrated in a multi-center randomized trial of RA37. The MACTAR interview consists of 1 patient-preference part, in which patients are asked to identify disabilities in relation to their rheumatic condition that they deem important to improve, and a second part with predefined items relating to global health, QOL, physical function, social function, and emotional function14,37. In contrast to traditional fixed-item questionnaires, the ability to rank items by importance is felt by some to provide a more individualized assessment of function. The MACTAR was translated into Swedish and adapted to the Swedish context14 according to the process described by Guillemin38 and was recently found to be responsive in detecting improvements in patient preference following intensive endurance exercise in established PM and DM39.

Truth:

The first draft of the MAP included 81 activities from the International Classification of Functioning Disability and Handicap40. These activities were selected by healthcare providers involved in the clinical care of patients with myositis as being the most relevant for individuals living in the Western world and affected with these conditions. Ten patients, selected to represent men and women and various disease duration, disease activity, and life situations, rated their difficulty with each activity and the importance of being able to perform each in daily life; as well, they were encouraged to add any important activities. Separate visual analog scales (VAS) for difficulty and importance were combined to a median value ranging from 0–10, with 10 as severe difficulty/very high importance. Thirty-seven items met or exceeded a cutoff of ≥ 6, and were taken forward to a second draft. Altogether, 6 activities were omitted because of internal redundancy or poor internal consistency, resulting in a third draft containing 31 items, which was tested in 32 consecutive patients with PM or DM with other referent physical function questionnaires. The MAP correlated best with HAQ and Arthritis Impact Measurement Scales Health Status Questionnaire41, with Spearman correlation coefficients ranging from 0.51–0.70. Lower correlations were observed for measures of muscle impairment42, disease effect on well-being (assessed on a 100 mm VAS), and serum CPK. The MAP was translated into English and evaluated in 64 US patients with PM and DM and validated according to the same process as the original Swedish MAP, with the only difference that patients rated difficulty and importance of all the 31 included items, while also adding any activity of choice in an open question at the end of the questionnaire. This process revealed a slightly lower cutoff for combined difficulty and importance of activities of > 5 for inclusion in the second draft of the MAP, which was found valid and reliable34.

The MACTAR interview has not been presented to patients with myositis for evaluation of content validity, and no analyses of internal redundancy or internal consistency have been performed14. Twenty-eight patients with established, stable PM and DM performed the MACTAR interview; Spearman correlation analysis revealed moderate to high correlation to SF-36 domains: mental health, social functioning, and role-emotional (0.67–0.73), with lower correlations to measures of ADL (the HAQ and MAP), muscle impairment by manual muscle testing, a strength test of 8 muscle groups43, Functional Index-244, and disease activity (6-item core set)5.

Discrimination:

Seventeen of the 31 patients with stable myositis disease activity completed the third draft of the MAP twice within 1 week for test-retest evaluation of reliability. Weighted kappa coefficients ranged between 0.56–0.77 for subscales and single items without systematic variations. MAP was used in 1 small 7-week resistance training study in patients with PM and DM leading to improved muscle function and reduced disease activity45, but no statistically significant change was obtained on a group level compared to baseline. However, 2 patients were responders according to criteria defined as improvement in at least 2 scale steps in at least 1 subscale or single item45. There are no data on specificity, error of measurement, or cutoff scores of the MAP. The weighted kappa coefficient of the Swedish MACTAR interview total score was 0.68 without systematic variation, and the intraclass correlation coefficient was 0.83, revealing a measurement error of 3.28 in PM and DM. There are to date no data published on responsiveness of the MACTAR in myositis.

Feasibility:

The MAP has low patient and observer burden; it only takes about 5 min to complete and about 5 min to calculate by hand. The MAP is available free of charge, but so far only in Swedish and American English. It has been validated as to content and construct validity, and test-retest reliability for a US context, also demonstrating good item fit according to Cronbach’s alpha analysis34. The MACTAR interview takes about 15 min to complete; however, the need for a trained interviewer and a complicated scoring system hamper its feasibility14.

The relative strengths and weaknesses of the MAP and the MACTAR were discussed during the SIG session at OMERACT 11. One advantage of the MAP is that patients were involved in the development process; however, the originating list of items presented to patients came from experts selecting items from the International Classification of Functioning, Disability and Health framework, although patients were encouraged to add any activities of choice in an open question. It is possible that qualitative studies may have been useful for revealing additional important areas. Presenting the questionnaire to patients again would further strengthen the validity of the MAP. Further, CPK was used as a surrogate marker for myositis disease activity; the relevance of CPK as an anchor can be questioned.

When the Swedish MAP was developed, the IMACS consensus 6-item core sets for disease activity measures20 were not yet available. However, the American MAP was validated using the IMACS 6-item core set. The MAP was considered an easy-to-use measure, but feasibility is hampered to date because it has not yet been adapted to several languages and cultures. A limitation of the MACTAR is that patients were not involved in the development process, neither in the original nor the Swedish version. This measure also needs to be presented to patients for evaluation of relevance. It is important to note that each of these measures is primarily focused on activities and physical function, although the MAP includes additional areas.

Myositis patients’ perspectives of symptoms

While it is imperative to derive the PRO-related information directly from patients, the majority of PRO are created by physicians and based on their point of view, including physicians’ understanding of their patients’ experiences.

Patient research partner perspective

A PRP who participated in the focus group conducted at Johns Hopkins and who attended the OMERACT 11 meeting in May 2012 shared with the OMERACT attendees her experience of living with myositis over 4 years. She discussed the effect of initial uncertainties in diagnosis, 47 days of hospitalizations and intensive care unit requirements, challenges in identifying medications to control her symptoms, and specific symptoms and changes in her life as a result of her condition. Her comments were directly transcribed.

With my muscle issues, the hardest thing has been dealing with how my life has changed, seemingly overnight, and adjusting to the fact that I have to have an oxygen bottle with me wherever I go and the slowness of my movement and the fatigue. It’s been hard to deal with my loss of my vitality.

She also poignantly discussed the effects of her illness on her family and social network: “I don’t think I could’ve survived or be as well as I am now, if I did not have their [my family’s] help and support.” She emphasized the shared experience of patients with myositis in the focus group she attended.

I found it to be very liberating to sit and talk with people that know what it’s like to have this disease and deal with it. The things we discussed [in the focus group included] pain, fatigue, shortness of breath, personal outlooks, and again the loss of vitality that each one of us share in such a personal way.

She said she was at times overwhelmed by her experience as a new OMERACT attendee, but that she had improved her understanding of the research process and nomenclature: “I think that the objectives of the doctors are very sound and a lot of goodwill comes from their research.”

Focus group results

The initial focus group of patients with myositis comprised 6 women and 1 man ranging in age from 33 to 69 years (mean 45 yrs). Six patients were white and 1 was Asian; disease duration ranged from 2 to 24 years. Patient global assessment, pain, fatigue, and stiffness were recorded on a 100 mm VAS. The mean scores were 35.7 for patient global assessment, 15.4 for pain, 54.6 for fatigue, and 40.9 for stiffness; the mean HAQ score for the group was 0.61 (range 0–1.5). In this initial focus group, high-level themes identified included pain, physical tightness/stiffness and flexibility, fatigue, emotional consequence of the illness, the effect of the disease on relationships, and treatment-related side effects. It is notable that with the exception of fatigue, and to some extent the social effects as measured in the MAP, these domains have not been previously evaluated in patients with IIM.

As noted, healthcare providers are traditionally taught that “typical” symptoms in IIM are painless weakness. However, there was widespread acknowledgment by the patients with myositis in the focus groups and from our PRP that pain was an important component of many patients’ disease experiences. Quotes illustrative of the identified theme of pain: “There is plenty of pain.” “But it’s a pain; it’s a better way to say it. It’s not stiffness; it’s…a bone thing. It’s like tightening up…” “…the pain is one my body would feel like someone just either scalded you with red-hot water, just constant burning…” “Another feeling in a different area, depending where I was complaining about, felt like someone just had a thousand straight pins and just stuck it, just brutal pain.” “And I always think of…a board with a million needles on it and someone’s just like pressing on my legs or…because when your leg falls asleep you think of pins and needles, but it’s not that pins and needles of being asleep.”

Pain is the most prominent symptom in most musculoskeletal diseases, but there has been limited evaluation of this symptom in patients with myositis. These dramatic descriptions of pain from this first focus group suggest that this is a manifestation that requires further study. It highlights that domains identified as important by healthcare providers to assess in myositis do not necessarily reflect areas that are most important to patients. While these are preliminary data derived from a single focus group, additional focus groups are currently under way internationally, and analyses will be conducted to better describe and understand the range and nature of patient perspectives.

In moving toward a comprehensive PRO assessment in myositis, foundational qualitative studies are needed to develop a conceptual framework for the patient’s experience. Adding to the complexity of myositis is the greater heterogeneity in terms of extramuscular manifestations of disease that may also affect various aspects of HRQOL.

Discussion and voting

At the Myositis SIG meeting, there was consensus that the MAP does not meet the OMERACT Filter 1.0 because of the absence of direct patient input on item selection, and that the MAP will need to be presented to patients at a future SIG meeting to strengthen content validity. There was overwhelming support that the Myositis SIG was worthwhile to continue, but that voting on specific PROM at this preliminary stage was premature.

It was decided that we should begin by including only PM and DM and to have focus groups that have representations from both rather than separate the groups by disease phenotype. Because IBM differs clinically and is likely to yield a different set of PRO (e.g., distal muscle weakness), it was decided that IBM would be studied after PRO were defined for PM and DM. It was also decided that children would not be included at this time, given the additional expertise and resources required for PROM development and validation in children, but that this would remain a future consideration. Further discussion at the 2012 annual meeting of the EULAR suggested that future focus groups should be constructed to include male participants, disease presence for at least 1 year, varied employment and educational status, and varied levels of education when possible. As DM and PM often coexist with ILD2, it was felt that patients with severe ILD with oxygen dependence should not be initially included given the difficulty in distinguishing outcomes related to ILD and those related to the underlying myositis (e.g., fatigue). Thus, this important comorbidity will be addressed specifically by the connective tissue disease (CTD)-ILD group. It was suggested that groups should last about 1.5 to 2 h with an anticipation of 90 min of active discussion. While free discussion was encouraged, the group intends to provide all focus group leaders with a set of potential questions to prompt discussion.

DISCUSSION

Most studies and PROM have focused on physical function measures largely generated by healthcare providers in the absence of patients. Recently, an extensive review on outcome measures in IIM outlined the measurement properties of a large number of clinical outcome measures used in myositis, of which 6 were PROM, confirming that there are very limited data on measurement properties of the often-used HAQ and SF-36 in adult myositis, but that the CHAQ has been extensively studied in juvenile dermatomyositis20. Our preliminary results from 1 focus group suggest that while not usually considered as a symptom in reference to myositis, pain is frequently reported by patients. Other important themes included the identification of fatigue as a central issue that affects the ability to perform activities and to participate in social roles. Preliminary descriptive statistics from studies in myositis have reported that fatigue is frequently encountered in patients with PM and DM46,47,48.

Symptoms in myositis

There was consensus among SIG meeting participants that extensive qualitative work is needed, specifically additional focus groups to understand the patient perspective on myositis and define core domains for myositis. These focus groups are planned at multiple centers in the United States and in countries in Europe and Asia. The results will be discussed at future group meetings. These investigations will guide the development or use of clinical outcome measures in myositis and will likely reveal symptoms previously unappreciated by providers.

Disease-specific and validated PRO for myositis

The MAP had been available only in Swedish, but the American adaptation has been published34. To meet the Filter 1.0, the Swedish and American MAP should be again presented to patients to ensure content validity. To further validate responsiveness, the Swedish MAP is currently used as a complement to the HAQ in standard clinical care and research in Sweden and for the same purpose the American MAP should also be included in US-led clinical trials. To broaden the availability of the MAP, translation to other languages and adaptation to other cultures is needed. Otherwise, to date, myositis-specific indices are limited to IBM in the form of the IBMFRS24. A similar effort to translate the IBMFRS and adapt it for other cultures, followed by inclusion in trials where possible, should be a research priority, given that IBM is expected to be added later as a separate group.

Finally, as stated, ILD can coexist with myositis, as in the case of our PRP. Because there is ongoing OMERACT work in CTD-ILD in which patients with myositis have participated, it is reasonable to consider reviewing those transcripts specifically to determine whether other themes regarding myositis may have emerged. The presentations at OMERACT and subsequent discussions have allowed the group to develop an active research agenda (Table 2).

View this table:
Table 2.

Research agenda.

The Filter 1.0 framework provided a useful construct in which to evaluate the extant PRO that have been used in myositis and related neuromuscular disorders, with only 2 instruments ever validated specifically in inflammatory muscle disease. The expanded Filter 2.0 framework provides a more overarching approach to development of core sets of outcome measures. The work of this SIG has been concentrated under the conceptual area of effect of health conditions, more specifically within the core area of life effect measures to better understand how (and what) to measure from the patient’s perspective of living with myositis and its comorbidities. The group elected to first focus on 2 key diseases, DM and PM. Although our work was initiated before development of the OMERACT Filter 2, we followed the outline that has subsequently been delineated toward the development of core domain sets, in our case a core domain set of PROM. We initiated our studies with a review of current domains and instruments used to evaluate HRQOL in myositis. Because we focused on patient perspective, there was obligatory inclusion of patients in the initial identification of relevant domains, which we have begun to obtain through our qualitative studies. The next steps toward the development of a draft core domain set will require additional studies in patients with IIM that are representative of different aspects of the disease (e.g., with and without lung disease, level of disability, disease duration) in order to ensure that all potentially relevant domains are identified. The IMACS group has separately engaged healthcare providers in the identification of important areas.

Our preliminary qualitative studies have identified a number of relevant contextual factors that will be important to address in future studies, including the influence of disease-related and individual contextual factors (e.g., the coexistence of ILD, disease duration, social support, and coping strategies). As the work of this SIG moves forward, the development of a conceptual framework of the patient’s experience of myositis will be important to determine the optimal domains and instruments to measure relevant aspects.

With this framework in mind, we plan to start at the level of the patient to identify the most important domains and develop psychometrically grounded items and anchors based on cognitively debriefing.

Because we have highlighted the problems with a generic HRQOL instrument (e.g., determining which subscores of the SF-36 are most applicable), we will move toward appreciation of participation and disease effect17,18. Patient ranking and appreciation of patient relevant versus healthcare-provider rated are highly valued; however, they will be examined through an iterative Delphi process, to achieve consensus between proportional groups (e.g., physician and PRP). It is hoped that the work of this OMERACT SIG will distill those aspects of health that are most important to patients with myositis. This may then help to inform a conceptual framework for IIM, within which patient-relevant domains can be identified, instruments developed/tested, and measures validated in randomized controlled trials and longitudinal observational study settings. This information will provide a much needed and richer understanding of these complex illnesses from the patient’s perspective.

Footnotes

  • The Myositis Special Interest Group received financial support from Crescent Health Care and NuFactor. Qualitative studies reported were supported through the Ira Fine Discovery Fund, the Sibley Hospital Memorial Fund, and the Johns Hopkins Arthritis Center Discovery Fund. H. Alexanderson was supported by the Centre for Care Science (Centrum för Vårdvetenskap), Karolinska Institutet and the Association Myopathie Francaise. A-M. Orbai is supported by US National Institutes of Health (NIH) T32-AR48522 and was supported to attend OMERACT 11 by the American College of Rheumatology and the Johns Hopkins Arthritis Center Discovery Fund. C.O. Bingham has received research grants and/or served as a consultant to Abbott, Amgen, American College of Rheumatology, Bristol Myers Squibb, Celgene, Genentech/Roche, Janssen/Johnson and Johnson/Centocor, NIH, Pfizer, and UCB. L. Christopher-Stine is supported by The Huayi and Siuling Zhang Discovery Fund; she has received research grants or served as a consultant to Novartis, MedImmune, Biogen Idec, URL, Questcor, Crescent Healthcare, and NIH.

REFERENCES

  1. 1.
    1. Khan S,
    2. Christopher-Stine L
    . Polymyositis, dermatomyositis, and autoimmune necrotizing myopathy: clinical features. Rheum Dis Clin North Am 2011;37:14358.
    OpenUrlCrossRefPubMed
  2. 2.
    1. Christopher-Stine L,
    2. Plotz PH
    . Adult inflammatory myopathies. Best Pract Res Clin Rheumatol 2004;18:33144.
    OpenUrlCrossRefPubMed
  3. 3.
    1. Ponyi A,
    2. Borgulya G,
    3. Constantin T,
    4. Vancsa A,
    5. Gergely L,
    6. Danko K
    . Functional outcome and quality of life in adult patients with idiopathic inflammatory myositis. Rheumatology 2005;44:838.
    OpenUrlAbstract/FREE Full Text
  4. 4.
    1. Alexanderson H,
    2. Lundberg IE
    . Inflammatory muscle disease: clinical presentation and assessment of patients. Curr Rheumatol Rep 2007;9:2739.
    OpenUrlCrossRefPubMed
  5. 5.
    1. Miller FW,
    2. Rider LG,
    3. Chung YL,
    4. Cooper R,
    5. Danko K,
    6. Farewell V,
    7. et al.
    Proposed preliminary core set measures for disease outcome assessment in adult and juvenile idiopathic inflammatory myopathies. Rheumatology 2001;40:126273.
    OpenUrlAbstract/FREE Full Text
  6. 6.
    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;30:47383.
    OpenUrlCrossRefPubMed
  7. 7.
    1. Kirwan JR,
    2. Ahlmen M,
    3. de Wit M,
    4. Heiberg T,
    5. Hehir M,
    6. Hewlett S,
    7. et al.
    Progress since OMERACT 6 on including patient perspective in rheumatoid arthritis outcome assessment. J Rheumatol 2005;32:22469.
    OpenUrlAbstract/FREE Full Text
  8. 8.
    1. Kirwan JR,
    2. Newman S,
    3. Tugwell PS,
    4. Wells GA,
    5. Hewlett S,
    6. Idzera L,
    7. et al.
    Progress on incorporating the patient perspective in outcome assessment in rheumatology and the emergence of life impact measures at OMERACT 9. J Rheumatol 2009;36:20716.
    OpenUrlAbstract/FREE Full Text
  9. 9.
    1. Kirwan JR,
    2. Hewlett SE,
    3. Heiberg T,
    4. Hughes RA,
    5. Carr M,
    6. Hehir M,
    7. et al.
    Incorporating the patient perspective into outcome assessment in rheumatoid arthritis—progress at OMERACT 7. J Rheumatol 2005;32:22506.
    OpenUrlAbstract/FREE Full Text
  10. 10.
    1. Committee of Medicinal Products for Human Use. European Medicines Agency
    . Reflection Paper on the Regulatory Guidance for the Use of Health-related Quality of Life (HRQOL) Measures in the Evaluation of Medicinal Products, London, 27 July, 2005. [Internet. Accessed November 18, 2013.] Available from: http://www.ema.europa.eu/docs/en_GB/document_library/Scientific_guideline/2009/09/WC500003637.pdf
  11. 11.
    1. US Food and Drug Administration
    . Guidance for Industry – patient-reported outcome measures: use in medical product development to support labeling claims. 2012 [Internet. Accessed November 18, 2013.] Available from: http://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/UCM183282.pdf).
  12. 12.
    1. Critical Path Institute (cPATH)
    . Patient Reported Outcomes (PRO) Consortium. [Internet.] Available from://c-path.org/PRO.cfm).
  13. 13.
    1. Stucki G,
    2. Kostanjsek N,
    3. Ustun B,
    4. Cieza A
    . ICF-based classification and measurement of functioning. Eur J Phys Rehabil Med 2008;44:31528.
    OpenUrlPubMed
  14. 14.
    1. Alemo Munters L,
    2. van Vollenhoven RF,
    3. Alexanderson H
    . Patient preference assessment reveals disease aspects not covered by recommended outcomes in polymyositis and dermatomyositis. ISRN Rheumatol 2011;2011:463124.
    OpenUrlPubMed
  15. 15.
    1. Fries JF,
    2. Spitz P,
    3. Kraines RG,
    4. Holman HR
    . Measurement of patient outcome in arthritis. Arthritis Rheum 1980;23:13745.
    OpenUrlCrossRefPubMed
  16. 16.
    1. Alexanderson H,
    2. Lundberg IE,
    3. Stenstrom CH
    . Development of the myositis activities profile—validity and reliability of a self-administered questionnaire to assess activity limitations in patients with polymyositis/dermatomyositis. J Rheumatol 2002;29:238692.
    OpenUrlAbstract/FREE Full Text
  17. 17.
    1. Bartlett SJ,
    2. Hewlett S,
    3. Bingham CO 3rd.,
    4. Woodworth TG,
    5. Alten R,
    6. Pohl C,
    7. et al.
    Identifying core domains to assess flare in rheumatoid arthritis: an OMERACT international patient and provider combined Delphi consensus. Ann Rheum Dis 2012;71:185560.
    OpenUrlAbstract/FREE Full Text
  18. 18.
    1. Bingham CO 3rd.,
    2. Alten R,
    3. Bartlett SJ,
    4. Bykerk VP,
    5. Brooks PM,
    6. Choy E,
    7. et al.
    Identifying preliminary domains to detect and measure rheumatoid arthritis flares: report of the OMERACT 10 RA Flare Workshop. J Rheumatol 2011;38:17518.
    OpenUrlAbstract/FREE Full Text
  19. 19.
    1. Hewlett S,
    2. Sanderson T,
    3. May J,
    4. Alten R,
    5. Bingham CO 3rd.,
    6. Cross M,
    7. et al.
    ‘I’m hurting, I want to kill myself’: rheumatoid arthritis flare is more than a high joint count—an international patient perspective on flare where medical help is sought. Rheumatology 2012;51:6976.
    OpenUrlAbstract/FREE Full Text
  20. 20.
    1. Rider LG,
    2. Werth VP,
    3. Huber AM,
    4. Alexanderson H,
    5. Rao AP,
    6. Ruperto N,
    7. et al.
    Measures of adult and juvenile dermatomyositis, polymyositis, and inclusion body myositis: Physician and Patient/Parent Global Activity, Manual Muscle Testing (MMT), Health Assessment Questionnaire (HAQ)/HAQ, Childhood Myositis Assessment Scale (CMAS), Myositis Disease Activity Assessment Tool (MDAAT), Disease Activity Score (DAS), Short Form 36 (SF-36), Child Health Questionnaire (CHQ), physician global damage, Myositis Damage Index (MDI), Quantitative Muscle Testing (QMT), Myositis Functional Index-2 (FI-2), Myositis Activities Profile (MAP), Inclusion Body Myositis Functional Rating Scale (IBMFRS), Cutaneous Dermatomyositis Disease Area and Severity Index (CDASI), Cutaneous Assessment Tool (CAT), Dermatomyositis Skin Severity Index (DSSI), Skindex, and Dermatology Life Quality Index (DLQI). Arthritis Care Res 2011;63 Suppl 11:S11857.
    OpenUrlCrossRef
  21. 21.
    1. Boers M,
    2. Brooks P,
    3. Strand CV,
    4. Tugwell P
    . The OMERACT filter for Outcome Measures in Rheumatology. J Rheumatol 1998;25:1989.
    OpenUrlPubMed
  22. 22.
    1. Hill C,
    2. Knox S,
    3. Thompson B,
    4. Williams E
    . Consensual qualitative research: an update. J Counsel Psychol 2005;52:196205.
    OpenUrlCrossRef
  23. 23.
    1. Cook KF,
    2. Bamer AM,
    3. Amtmann D,
    4. Molton IR,
    5. Jensen MP
    . Six patient-reported outcome measurement information system short form measures have negligible age- or diagnosis-related differential item functioning in individuals with disabilities. Arch Phys Med Rehabil 2012;93:128991.
    OpenUrlCrossRefPubMed
  24. 24.
    1. Jackson CE,
    2. Barohn RJ,
    3. Gronseth G,
    4. Pandya S,
    5. Herbelin L; and
    6. Muscle Study Group
    . Inclusion body myositis functional rating scale: a reliable and valid measure of disease severity. Muscle Nerve 2008;37:4736.
    OpenUrlCrossRefPubMed
  25. 25.
    1. Vincent KA,
    2. Carr AJ,
    3. Walburn J,
    4. Scott DL,
    5. Rose MR
    . Construction and validation of a quality of life questionnaire for neuromuscular disease (INQoL). Neurology 2007;68:10517.
    OpenUrlCrossRef
  26. 26.
    1. Landgraf J,
    2. Abetz L,
    3. Ware J
    . The CHQ users manual. 1st ed. Boston, MA: The Health Institute; 1996.
  27. 27.
    1. Huber AM,
    2. Hicks JE,
    3. Lachenbruch PA,
    4. Perez MD,
    5. Zemel SL,
    6. Rennebohm RM,
    7. et al.
    Validation of the Childhood Health Assessment Questionnaire in the juvenile idiopathic myopathies. Juvenile Dermatomyositis Disease Activity Collaborative Study Group. J Rheumatol 2001;28:110611.
    OpenUrlAbstract/FREE Full Text
  28. 28.
    1. Dalakas MC,
    2. Sonies B,
    3. Dambrosia J,
    4. Sekul E,
    5. Cupler E,
    6. Sivakumar K
    . Treatment of inclusion-body myositis with IVIg: a double-blind, placebo-controlled study. Neurology 1997;48:7126.
    OpenUrlCrossRef
  29. 29.
    The Amyotrophic Lateral Sclerosis Functional Rating Scale. Assessment of activities of daily living in patients with amyotrophic lateral sclerosis. The ALS CNTF treatment study (ACTS) phase I–II Study Group. Arch Neurol 1996;53:1417.
    OpenUrlCrossRefPubMed
  30. 30.
    1. Mahoney FI,
    2. Barthel DW
    . Functional evaluation: the Barthel Index. Md State Med J 1965;14:615.
    OpenUrlPubMed
  31. 31.
    1. Munro BH
    . Statistical methods for health care research. 3rd ed. Philadelphia: Lippincott;1997:235.
  32. 32.
    1. Nunnally J
    . Psychometric theory. New York: McGraw-Hill; 1978.
  33. 33.
    1. Landis JR,
    2. Koch GG
    . The measurement of observer agreement for categorical data. Biometrics 1977;33:15974.
    OpenUrlCrossRefPubMed
  34. 34.
    1. Alexanderson H,
    2. Reed AM,
    3. Ytterberg SR
    . The Myositis Activities Profile - initial validation for assessment of polymyositis/dermatomyositis in the USA. J Rheumatol 2012;39:213441.
    OpenUrlAbstract/FREE Full Text
  35. 35.
    1. Tugwell P,
    2. Bombardier C,
    3. Buchanan WW,
    4. Goldsmith CH,
    5. Grace E,
    6. Hanna B
    . The MACTAR Patient Preference Disability Questionnaire—an individualized functional priority approach for assessing improvement in physical disability in clinical trials in rheumatoid arthritis. J Rheumatol 1987;14:44651.
    OpenUrlPubMed
  36. 36.
    1. Mouthon L,
    2. Rannou F,
    3. Bérezné A,
    4. Pagnoux C,
    5. Guilpain P,
    6. Goldwasser F,
    7. et al.
    Patient preference disability questionnaire in systemic sclerosis: a cross-sectional survey. Arthritis Rheum 2008;59:96873.
    OpenUrlCrossRefPubMed
  37. 37.
    1. Verhoeven AC,
    2. Boers M,
    3. van der Liden S
    . Validity of the MACTAR questionnaire as a functional index in a rheumatoid arthritis clinical trial. The McMaster Toronto Arthritis. J Rheumatol 2000;27:28019.
    OpenUrlPubMed
  38. 38.
    1. Guillemin F
    . Cross-cultural adaptation and validation of health status measures. Scand J Rheumatol 1995;24:613.
    OpenUrlCrossRefPubMed
  39. 39.
    1. Alemo Munters L,
    2. Dastmalchi M,
    3. Andgren V,
    4. Emilsson C,
    5. Bergegård J,
    6. Regardt M,
    7. et al.
    Endurance exercise improves health and may reduce disease activity in patients with established polymyositis and dermatomyositis. A multicenter randomized controlled trial with a 1-year open extension follow-up. Arthritis Care Res 2013; July 16. [E-pub ahead of print]
  40. 40.
    1. World Health Organization
    . International Classification of Functioning, Disability and Health (ICF). [Internet. Accessed November 18, 2013.] Available from: http://www.who.int/classifications/icf/en/
  41. 41.
    1. Meenan RF,
    2. Mason JH,
    3. Anderson JJ,
    4. Guccione AA,
    5. Kazis LE
    . AIMS2. The content and properties of a revised and expanded Arthritis Impact Measurement Scales. Arthritis Rheum 1992;35:110.
    OpenUrlCrossRefPubMed
  42. 42.
    1. Josefson A,
    2. Romanus E,
    3. Carlsson J
    . A functional index in myositis. J Rheumatol 1996;23:13804.
    OpenUrlPubMed
  43. 43.
    1. Rider LG,
    2. Kozio D,
    3. Giannini EH,
    4. Jain MS,
    5. Smith MR,
    6. Whitney-Mahoney K,
    7. et al.
    Validation of manual muscle testing and a subset of eight muscles for adult and juvenile idiopathic inflammatory myopathies. Arthritis Care Res 2010;62:46572.
    OpenUrlCrossRef
  44. 44.
    1. Alexanderson H,
    2. Broman L,
    3. Tollbäck A,
    4. Josefson A,
    5. Lundberg IE,
    6. Stenström CH
    . Functional Index-2: Validity and reliability of a disease-specific measure of impairment in patients with polymyositis and dermatomyositis. Arthritis Rheum 2006;55:11422.
    OpenUrlCrossRefPubMed
  45. 45.
    1. Alexanderson H,
    2. Dastmalchi M,
    3. Esbjörnsson-Liljedahl M,
    4. Opava CH,
    5. Lundberg IE
    . Benefits of intensive resistance training in patients with chronic polymyositis or dermatomyositis. Arthritis Rheum 2007;57:76877.
    OpenUrlCrossRefPubMed
  46. 46.
    1. Ghazi E,
    2. Kling MA,
    3. Propart K,
    4. Okawa J,
    5. Werth VP
    . Increased depression and anxiety symptoms in a group of dermatomyositis patients [abstract]. Arthritis Rheum 2011;63 Suppl 10:S92.
    OpenUrl
  47. 47.
    1. Campbell RCJ,
    2. Scott DL,
    3. Kiely PD,
    4. Gordon P
    . Fatigue in idiopathic inflammatory myopathies (IIM): Prevalence, impact and association with quality of life [abstract]. Arthritis Rheum 2011;63 Suppl:S89.
    OpenUrl
  48. 48.
    1. Campbell RCJ,
    2. Scott DL,
    3. Kiely PD,
    4. Gordon P
    . Predictors of experienced fatigue in idiopathic inflammatory myopathy (IIM): Psychological factors and pain are more predictive than disease activity, damage or strength [abstract]. Arthritis Rheum 2011;63 Suppl:S90.
    OpenUrl
  49. 49.
    1. Sultan SM,
    2. Ioannou Y,
    3. Moss K,
    4. Isenberg DA
    . Outcome in patients with idiopathic inflammatory myositis: morbidity and mortality. Rheumatology 2002;41:226.
    OpenUrlAbstract/FREE Full Text
  50. 50.
    1. Regardt M,
    2. Welin Henriksson E,
    3. Alexanderson H,
    4. Lundberg IE
    . Patients with polymyositis or dermatomyositis have reduced grip force and health-related quality of life in comparison with reference values: an observational study. Rheumatology 2011;50:57885.
    OpenUrlAbstract/FREE Full Text
  51. 51.
    1. Alexanderson H,
    2. Stenstrom CH,
    3. Lundberg I
    . Safety of a home exercise programme in patients with polymyositis and dermatomyositis: a pilot study. Rheumatology 1999;38:60811.
    OpenUrlAbstract/FREE Full Text
  52. 52.
    1. Alexanderson H,
    2. Stenstrom CH,
    3. Jenner G,
    4. Lundberg I
    . The safety of a resistive home exercise program in patients with recent onset active polymyositis or dermatomyositis. Scand J Rheumatol 2000;29:295301.
    OpenUrlCrossRefPubMed
  53. 53.
    1. Sadjadi R,
    2. Rose MR; and
    3. Muscle Study Group
    . What determines quality of life in inclusion body myositis? J Neurol Neurosurg Psychiatry 2010;81:11646.
    OpenUrlAbstract/FREE Full Text
  54. 54.
    1. Vojinović J,
    2. Riley P,
    3. Maillard S,
    4. Pilkington C
    . Importance of aggressive treatment in juvenile dermatomyositis [Serbian]. Srp Arh Celok Lek 2005;133 Suppl 2:11823.
    OpenUrlPubMed
  55. 55.
    1. Apaz MT,
    2. Saad-Magalhaes C,
    3. Pistorio A,
    4. Ravelli A,
    5. de Oliveira Sato J,
    6. Marcantoni MB,
    7. et al.
    Health-related quality of life of patients with juvenile dermatomyositis: results from the Pediatric Rheumatology International Trials Organisation multinational quality of life cohort study. Arthritis Rheum 2009;61:50917.
    OpenUrlCrossRefPubMed
  56. 56.
    1. Hunt SM,
    2. McKenna SP,
    3. McEwen J,
    4. Williams J,
    5. Papp E
    . The Nottingham Health Profile: subjective health status and medical consultations. Soc Sci Med A 1981;15:2219.
    OpenUrlPubMed
  57. 57.
    1. Chung YL,
    2. Mitchell HL,
    3. Houssien DA,
    4. Al-Mahrouki H,
    5. Carr AJ,
    6. Scott DL
    . A comparative study of outcome in myositis and other musculoskeletal disorders assessed using the Nottingham health profile. Clin Exp Rheumatol 2001;19:44750.
    OpenUrlPubMed
  58. 58.
    1. Varni JW
    . The PedsQL measurement model for the Pediatric Quality of Life Inventory. [Internet. Accessed November 18, 2013.] Available from: http://www.pedsql.org/
  59. 59.
    1. Butbul Aviel Y,
    2. Stremler R,
    3. Benseler SM,
    4. Cameron B,
    5. Laxer RM,
    6. Osa S,
    7. et al.
    Sleep and fatigue and the relationship to pain, disease activity and quality of life in juvenile idiopathic arthritis and juvenile dermatomyositis. Rheumatology 2011;50:205160.
    OpenUrlAbstract/FREE Full Text
  60. 60.
    1. Sansone VA,
    2. Panzeri M,
    3. Montanari M,
    4. Apolone G,
    5. Gandossini S,
    6. Rose MR,
    7. et al.
    Italian validation of INQoL, a quality of life questionnaire for adults with muscle diseases. Eur J Neurol 2010;17:117887.
    OpenUrlCrossRefPubMed
  61. 61.
    1. Sadjadi R,
    2. Vincent KA,
    3. Carr AJ,
    4. Walburn J,
    5. Brooks VL,
    6. Pandya S,
    7. et al.
    Validation of the individualized neuromuscular quality of life for the USA with comparison of the impact of muscle disease on those living in the USA versus UK. Health Qual Life Outcomes 2011;9:114.
    OpenUrlCrossRefPubMed
  62. 62.
    1. Muscle Study Group
    . Randomized pilot trial of high-dose betaINF-1a in patients with inclusion body myositis. Neurology 2004;63:71820.
    OpenUrlCrossRef
  63. 63.
    1. Rider LG,
    2. Feldman BM,
    3. Perez MD,
    4. Rennebohm RM,
    5. Lindsley CB,
    6. Zemel LS,
    7. et al.
    Development of validated disease activity and damage indices for the juvenile idiopathic inflammatory myopathies: I. Physician, parent, and patient global assessments. Juvenile Dermatomyositis Disease Activity Collaborative Study Group. Arthritis Rheum 1997;40:197683.
    OpenUrlCrossRefPubMed
  64. 64.
    1. Rider LG,
    2. Giannini EH,
    3. Harris-Love M,
    4. Joe G,
    5. Isenberg D,
    6. Pilkington C,
    7. et al.
    Defining clinical improvement in adult and juvenile myositis. J Rheumatol 2003;30:60317.
    OpenUrlAbstract/FREE Full Text
  65. 65.
    1. Chung L,
    2. Genovese MC,
    3. Fiorentino DF
    . A pilot trial of rituximab in the treatment of patients with dermatomyositis. Arch Dermatol 2007;143:7637.
    OpenUrlCrossRefPubMed
  66. 66.
    1. Ruperto N,
    2. Ravelli A,
    3. Pistorio A,
    4. Ferriani V,
    5. Calvo I,
    6. Ganser G,
    7. et al.
    The provisional Paediatric Rheumatology International Trials Organisation/American College of Rheumatology/European League Against Rheumatism Disease activity core set for the evaluation of response to therapy in juvenile dermatomyositis: a prospective validation study. Arthritis Rheum 2008;59:413.
    OpenUrlCrossRefPubMed
  67. 67.
    1. Neri R,
    2. Mosca M,
    3. Stampacchia G,
    4. Vesprini E,
    5. Tavoni A,
    6. d’Ascanio D,
    7. et al.
    Functional and isokinetic assessment of muscle strength in patients with idiopathic inflammatory myopathies. Autoimmunity 2006;39:2559.
    OpenUrlCrossRefPubMed
  68. 68.
    1. Muscle Study Group
    . A randomized, pilot trial of etanercept in dermatomyositis. Ann Neurol 2011;70:42736.
    OpenUrlCrossRefPubMed
  69. 69.
    1. Chen YJ,
    2. Wu CY,
    3. Shen JL
    . Predicting factors of interstitial lung disease in dermatomyositis and polymyositis. Acta Derm Venereol 2007;87:338.
    OpenUrlCrossRefPubMed
  70. 70.
    1. Saito E,
    2. Koike T,
    3. Hashimoto H,
    4. Miyasaka N,
    5. Ikeda Y,
    6. Hara M,
    7. et al.
    Efficacy of high-dose intravenous immunoglobulin therapy in Japanese patients with steroid-resistant polymyositis and dermatomyositis. Mod Rheumatol 2008;18:3444.
    OpenUrlCrossRefPubMed
  71. 71.
    1. Sanner H,
    2. Gran JT,
    3. Sjaastad I,
    4. Flato B
    . Cumulative organ damage and prognostic factors in juvenile dermatomyositis: a cross-sectional study median 16.8 years after symptom onset. Rheumatology 2009;48:15417.
    OpenUrlAbstract/FREE Full Text
  72. 72.
    1. Varju C,
    2. Petho E,
    3. Kutas R,
    4. Czirjak L
    . The effect of physical exercise following acute disease exacerbation in patients with dermato/polymyositis. Clin Rehabil 2003;17:837.
    OpenUrlAbstract/FREE Full Text
  73. 73.
    1. Feldman BM,
    2. Ayling-Campos A,
    3. Luy L,
    4. Stevens D,
    5. Silverman ED,
    6. Laxer RM
    . Measuring disability in juvenile dermatomyositis: validity of the childhood health assessment questionnaire. J Rheumatol 1995;22:32631.
    OpenUrlPubMed
  74. 74.
    1. Takken T,
    2. Elst E,
    3. Spermon N,
    4. Helders PJ,
    5. Prakken AB,
    6. van der Net J
    . The physiological and physical determinants of functional ability measures in children with juvenile dermatomyositis. Rheumatology 2003;42:5915.
    OpenUrlAbstract/FREE Full Text
  75. 75.
    1. McCann LJ,
    2. Juggins AD,
    3. Maillard SM,
    4. Wedderburn LR,
    5. Davidson JE,
    6. Murray KJ,
    7. et al.
    The Juvenile Dermatomyositis National Registry and Repository (UK and Ireland)—clinical characteristics of children recruited within the first 5 yr. Rheumatology 2006;45:125560.
    OpenUrlAbstract/FREE Full Text
  76. 76.
    1. Ramanan AV,
    2. Campbell-Webster N,
    3. Ota S,
    4. Parker S,
    5. Tran D,
    6. Tyrrell PN,
    7. et al.
    The effectiveness of treating juvenile dermatomyositis with methotrexate and aggressively tapered corticosteroids. Arthritis Rheum 2005;52:35708.
    OpenUrlCrossRefPubMed
  77. 77.
    1. Ravelli A,
    2. Trail L,
    3. Ferrari C,
    4. Ruperto N,
    5. Pistorio A,
    6. Pilkington C,
    7. et al.
    Long-term outcome and prognostic factors of juvenile dermatomyositis: a multinational, multicenter study of 490 patients. Arthritis Care Res 2010;62:6372.
    OpenUrlCrossRef
  78. 78.
    1. Fix AJ,
    2. Daughton D
    . Human activity profile professional manual. Odessa, Florida: Psychological Assessment Resources, Inc.; 1988.
  79. 79.
    1. Matsunaga S,
    2. Sakou T,
    3. Onishi T,
    4. Hayashi K,
    5. Taketomi E,
    6. Sunahara N,
    7. et al.
    Prognosis of patients with upper cervical lesions caused by rheumatoid arthritis: comparison of occipitocervical fusion between c1 laminectomy and nonsurgical management. Spine 2003;28:15817.
    OpenUrlCrossRefPubMed
  80. 80.
    1. Weinstein AA,
    2. Drinkard BM,
    3. Diao G,
    4. Furst G,
    5. Dale JK,
    6. Straus SE,
    7. et al.
    Exploratory analysis of the relationships between aerobic capacity and self-reported fatigue in patients with rheumatoid arthritis, polymyositis, and chronic fatigue syndrome. PM R 2009;1:6208.
    OpenUrlCrossRefPubMed
  81. 81.
    1. Walter MC,
    2. Lochmuller H,
    3. Toepfer M,
    4. Schlotter B,
    5. Reilich P,
    6. Schröder M,
    7. et al.
    High-dose immunoglobulin therapy in sporadic inclusion body myositis: a double-blind, placebo-controlled study. J Neurol 2000;247:228.
    OpenUrlCrossRefPubMed
  82. 82.
    1. Soueidan SA,
    2. Dalakas MC
    . Treatment of inclusion-body myositis with high-dose intravenous immunoglobulin. Neurology 1993;43:8769.
    OpenUrlCrossRef
  83. 83.
    1. van de Vlekkert J,
    2. Hoogendijk JE,
    3. de Haan RJ,
    4. Algra A,
    5. van der Tweel I,
    6. van der Pol WL,
    7. et al.
    Oral dexamethasone pulse therapy versus daily prednisolone in sub-acute onset myositis, a randomised clinical trial. Neuromuscul Disord 2010;20:3829.
    OpenUrlCrossRefPubMed
  84. 84.
    1. Sancricca C,
    2. Mora M,
    3. Ricci E,
    4. Tonali PA,
    5. Mantegazza R,
    6. Mirabella M
    . Pilot trial of simvastatin in the treatment of sporadic inclusion-body myositis. Neurol Sci 2011;32:8417.
    OpenUrlCrossRefPubMed
  85. 85.
    1. Convery FR,
    2. Minteer MA,
    3. Amiel D,
    4. Connett KL
    . Polyarticular disability: a functional assessment. Arch Phys Med Rehabil 1977;58:4949.
    OpenUrlPubMed
  86. 86.
    1. Miller FW,
    2. Leitman SF,
    3. Cronin ME,
    4. Hicks JE,
    5. Leff RL,
    6. Wesley R,
    7. et al.
    Controlled trial of plasma exchange and leukapheresis in polymyositis and dermatomyositis. N Engl J Med 1992;326:13804.
    OpenUrlCrossRefPubMed
  87. 87.
    1. Villalba L,
    2. Hicks JE,
    3. Adams EM,
    4. Sherman JB,
    5. Gourley MF,
    6. Leff RL,
    7. et al.
    Treatment of refractory myositis: a randomized crossover study of two new cytotoxic regimens. Arthritis Rheum 1998;41:3929.
    OpenUrlCrossRefPubMed
  88. 88.
    1. Dalakas MC,
    2. Illa I,
    3. Dambrosia JM,
    4. Soueidan SA,
    5. Stein DP,
    6. Otero C,
    7. et al.
    A controlled trial of high-dose intravenous immune globulin infusions as treatment for dermatomyositis. N Engl J Med 1993;329:19932000.
    OpenUrlCrossRefPubMed
  89. 89.
    1. Melzack R
    . The short-form McGill Pain Questionnaire. Pain 1987;30:1917.
    OpenUrlCrossRefPubMed
  90. 90.
    1. Chalder T,
    2. Berelowitz G,
    3. Pawlikowska T,
    4. Watts L,
    5. Wessely S,
    6. Wright D,
    7. et al.
    Development of a fatigue scale. J Psychosom Res 1993;37:14753.
    OpenUrlCrossRefPubMed
  91. 91.
    1. Belza BL,
    2. Henke CJ,
    3. Yelin EH,
    4. Epstein WV,
    5. Gilliss CL
    . Correlates of fatigue in older adults with rheumatoid arthritis. Nurs Res 1993;42:939.
    OpenUrlPubMed
  92. 92.
    1. McNair DM,
    2. Lorr M,
    3. Droppleman LF
    . Manual for the profile of mood states. San Diego: Educational and Industrial Testing Service; 1971.
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Keywords

MYOSITIS
PATIENT-REPORTED OUTCOMES
OUTCOME AND PROCESS ASSESSMENT

Keywords