Article Text
Abstract
Objectives Fatigue is prevalent in people with inflammatory rheumatic and musculoskeletal diseases (I-RMDs) and recognised as one of the most challenging symptoms to manage. The existence of multiple factors associated with driving and maintaining fatigue, and the evidence about what improves fatigue has led to a multifaceted approach to its management. However, there are no recommendations for fatigue management in people with I-RMDs. This lack of guidance is challenging for those living with fatigue and health professionals delivering clinical care. Therefore, our aim was to develop EULAR recommendations for the management of fatigue in people with I-RMDs.
Methods A multidisciplinary taskforce comprising 26 members from 14 European countries was convened, and two systematic reviews were conducted. The taskforce developed the recommendations based on the systematic review of evidence supplemented with taskforce members’ experience of fatigue in I-RMDs.
Results Four overarching principles (OAPs) and four recommendations were developed. OAPs include health professionals’ awareness that fatigue encompasses multiple biological, psychological and social factors which should inform clinical care. Fatigue should be monitored and assessed, and people with I-RMDs should be offered management options. Recommendations include offering tailored physical activity and/or tailored psychoeducational interventions and/or, if clinically indicated, immunomodulatory treatment initiation or change. Patient-centred fatigue management should consider the individual’s needs and preferences, their clinical disease activity, comorbidities and other psychosocial and contextual factors through shared decision-making.
Conclusions These 2023 EULAR recommendations provide consensus and up-to-date guidance on fatigue management in people with I-RMDs.
- health services research
- rehabilitation
- therapeutics
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Introduction
Inflammatory rheumatic and musculoskeletal diseases (I-RMDs) encompass several long-term conditions, including rheumatoid arthritis (RA), psoriatic arthritis, axial spondyloarthritis, systemic lupus erythematosus and Sjögren’s syndrome, among others. Fatigue is prevalent in people with I-RMDs and is one of the most challenging symptoms to cope with due to its invisible, pervasive and unpredictable nature.1–4 Although there is no single conceptualisation or definition of fatigue, it is recognised that fatigue in I-RMDs is different to normal feelings of tiredness.5 People with I-RMDs describe fatigue as overwhelming, intrusive, distressing and draining them of physical and mental energy.6 It can impact all areas of their daily lives and can leave people feeling alone as they withdraw from social interactions and their lives become increasingly restricted.7 Survey evidence with over 6000 people with I-RMDs found that one out of every two was severely fatigued, scoring≤35 on the 36-item Short Form Vitality Scale.8
At an individual level, fatigue is strongly associated with a poor quality of life for people with I-RMDs.9 10 At a societal level, fatigue in I-RMDs is associated with increased clinical care costs, primary care consultations, employment loss and high levels of absenteeism, presenteeism and work disability.11–13 People with I-RMDs report debilitating fatigue during flares and in low disease activity and remission states.14–17 In those with early RA, one of the most common I-RMDs, fatigue is associated with perceived non-improvement in health in those with favourable treatment outcomes, and fatigue has been identified as one of the most important outcome domains in defining disease remission.18 19 In rheumatology, people with I-RMDs and health professionals have identified access to fatigue interventions as an unmet need and priority.20–22 Rheumatology health professionals recognise that fatigue is important, but few routinely offer advice, interventions or support to manage the symptom.19 23 24
Part of the challenge of providing support for fatigue in I-RMDs is that the causes and maintaining factors are unclear and multifaceted and that there is no curative treatment. Research indicates that the immune system, the central and autonomic nervous systems and the neuroendocrine system might have a role in the induction and maintenance of fatigue in I-RMDs.25 Evidence is also emerging that sleep, genetic susceptibility, metabolic disturbances and other biological and physiological mechanisms might contribute to fatigue.26 However, this evidence is inconclusive. In addition, an array of other biopsychosocial and contextual variables are associated with fatigue in I-RMDs, including physical functioning and physical activity, comorbidities, pain, obesity, anxiety and depression, stress and relationships and work roles.27–29 Although the inter-relationships between these diverse factors and fatigue are not clearly understood or defined, there is general agreement that fatigue in I-RMDs is likely to involve multiple biological, psychological and social mechanisms.30 It has been proposed that these mechanisms can change over time and are likely to vary between people.31 This body of evidence indicates that optimal fatigue management requires a tailored, flexible and holistic approach. However, there are no recommendations to support people with I-RMDs and health professionals with fatigue management. Acknowledging this current lack of guidance, we convened a taskforce to develop EULAR recommendations for the management of fatigue in people with I-RMDs.
Methods
We developed the recommendations following the 2014 updated EULAR standardised operating procedures.32 The convenor (ED) and the methodologist (PMM) submitted a proposal to the EULAR Executive Committee (now designated EULAR Council). Once the proposal had been approved, PMM and ED set up a steering group with the two fellows (EJFS and BF) and invited the proposed taskforce members. The taskforce comprised 26 clinicians, academics, methodologists and experts by experience from 14 European countries. EULAR representatives from the health professionals committee, People with Arthritis/Rheumatism across Europe and EMerging EUlar NETwork were included, and five members were recruited through an open call to EULAR countries via a competitive application process. Taskforce members were patient partners, nurses, physicians (rheumatology consultants and registrars), occupational therapists, psychologists and physiotherapists, all with personal and/or professional experience of fatigue in I-RMDs. The diverse, multidisciplinary taskforce reflects the complex nature of fatigue and the multifaceted approach to its management. The recommendations were developed over 2-day-long meetings held online via MS Teams and co-facilitated by PMM and ED. As required by the EULAR SOP, all members disclosed their conflicts of interest upfront.
At the first meeting, taskforce members discussed which groups could benefit from fatigue management recommendations. These include people living with I-RMDs and those in their support systems, such as family, carers and friends; the multidisciplinary rheumatology team, which is often hospital based; primary care physicians; health professionals in other clinical areas and settings, for example, community based; healthcare funders, commissioners, insurers and providers; healthcare educators and trainers; charities and organisations that support people with I-RMDs; employers, educational institutions and occupational health providers; and pharmaceutical companies.
The taskforce then formulated questions for the systematic literature review (SLR) that would provide the evidence to underpin the recommendations. The questions were:
Which pharmacological interventions are efficacious in reducing fatigue (in a broad sense) in people with I-RMDs?
Which non-pharmacological interventions are efficacious in reducing fatigue (in a broad sense) in people with I-RMDs?
Which pharmacological and non-pharmacological interventions are safe in reducing fatigue in people with I-RMDs?
After the meeting, the steering group drafted an SLR protocol that was registered with PROSPERO (reference: CRD42021282899). As the initial searches returned large numbers of abstracts, the steering group decided to conduct two SLRs. EJFS led the review of non-pharmacological interventions, and BF led the review of pharmacological interventions. Both reviews were conducted according to the Cochrane Handbook proposed method and reported following the Preferred Reporting Items for Systematic Reviews and Meta-Analysis guidelines.33 34 The steering group drafted potential overarching principles (OAPs) and recommendations based on these results.
At the second taskforce meeting, EJFS and BF presented the results from the SLRs. The main findings included evidence that physical activity or exercise, psychoeducational interventions and several pharmacological interventions are efficacious (and generally safe) in reducing fatigue in people with I-RMDs.35 36 Physical activity or exercise was found to be efficacious in reducing fatigue, with a small effect size in RA (standardised mean difference (SMD)=−0.23), a moderate effect size in systemic lupus erythematosus (SLE) and a large effect size in spondyloarthritis (SpA) (SMD=−0.94).36 Psychoeducational interventions were also found to be efficacious in reducing fatigue in RA, showing a small effect size (SMD=−0.32). However, it is important to note that these effect sizes are challenging to interpret and compare due to the heterogeneity of studies in terms of inclusion criteria, intervention types, study design and the number of studies included in the meta-analyses. PMM and ED then presented the steering group’s potential OAPs and recommendations, one by one, which were modified through discussion and voting. OPAs and recommendations were edited live according to the comments made, followed by formal anonymised voting using the poll function in MS Teams. Consensus was reached if either ≥75% of the members voted in favour of the recommendations in the first, ≥67% in the second or ≥50% in a third round. If multiple rounds of voting were necessary, a discussion took place in between voting rounds to refine the drafted statements.
After the meeting, the levels of evidence and grades of recommendation derived from the SLRs following the standards of the Oxford Center for Evidence Based Medicine were added by the steering committee to each of the recommendations.37 Finally, each taskforce member anonymously indicated their level of agreement (LoA) through an online survey (numerical rating scale ranging from 0=‘do not agree at all’ to 10=‘fully agree’). The mean and SD of the LoA, as well as the percentage of agreement≥8, are presented.
The taskforce also discussed important areas for future research on fatigue in I-RMDs that were not addressed in the current SLRs and where there is a lack of evidence. The draft of the manuscript was sent to all taskforce members for review. All authors and the EULAR Council approved the final manuscript.
Results
The taskforce agreed on four OAPs and four recommendations (table 1). These are based on evidence from the two SLRs, combined with the taskforce members’ expert opinions. LoA was very high for all OAPs and recommendations, ranging from 9.4 to 9.9 average LoA on 0–10 scale, strengthening the validity and robustness of the agreed statements.
Overarching principles
During the analysis of the evidence and expert discussion, the taskforce identified four key general themes across all recommendations. These were formulated and agreed as OAPs. They provide a set of crucial principles in managing fatigue in people with I-RMDs, reflecting state-of-the-art management.
Health professionals should be aware that fatigue encompasses multiple and mutually interacting biological, psychological and social factors
This OAP provides a conceptual framework to inform health professionals’ understanding of fatigue and their communication about this symptom with people with I-RMDs. It is important that the complexity of fatigue is recognised and that health professionals are aware of the potentially wide range of biopsychosocial factors that can drive and maintain fatigue and the implications of this for people’s physical and mental health.26 27 30 31 This awareness should facilitate discussions with people who have I-RMDs about which specific factors might be pertinent for them as individuals. People with I-RMDs have reported that being asked about their fatigue can be validating and make them feel less isolated; for some, it can be the first step to self-management.38 39
Fatigue should be routinely monitored in people with I-RMDs, and management options should be offered as part of their clinical care
Fatigue in I-RMDs is a prevalent, often non-resolving symptom that needs to be considered in the long term. Monitoring fatigue as part of clinical care acknowledges that the symptom is frequently present and has a detrimental impact on people with I-RMDs. In some settings, monitoring might comprise the completion of patient-reported outcome measures so that health professionals can gauge fatigue in people with I-RMDs at individual and population levels, for example, as part of national registries.11 14 17 40–42
Management options should be offered as part of clinical care. The taskforce recognises that various health professionals in different healthcare systems undertake responsibility for offering management options. In addition, not all fatigue management options are widely available and not all health professionals have the knowledge, skills and confidence to provide support. However, at a minimum, health professionals can provide information and signpost to resources, such as those provided by patient organisations. In multidisciplinary teams, health professionals can consider referrals to colleagues who might be better placed to offer appropriate support.43 44 Together, monitoring and offering management options should normalise fatigue which is likely to be helpful to people with I-RMDs.
Decisions on managing fatigue should be shared and agreed on, between the person with an I-RMD and the professionals providing care for their health and well-being
Patient-centred care includes listening to, informing and involving patients in ways that are meaningful and valuable to the individual, with the goal of empowering them to become active participants in their care. Shared decision-making is central to implementing patient-centred care. Therefore, as part of delivering patient-centred care in rheumatology, decisions about fatigue management need to be shared between the person with an I-RMD and the health professional.45 This involves collaboration based on health professionals’ expertise (eg, knowledge about management options, including evidence, risks and benefits) and people with I-RMDs’ expertise (eg, knowledge of their preferences, circumstances, goals, values and beliefs). Shared decision-making should be undertaken to support people to make decisions about their fatigue management that are right for them at that time. Shared decision-making allows people to choose the extent to which they want to collaborate with health professionals and includes acknowledging that some people prefer not to take an active role in making decisions . However, it is important that all people with I-RMDs are offered the opportunity to engage in shared decision-making and that their needs and preferences determine the degree of collaboration.
As with the previous OAP, the taskforce discussed how healthcare systems differ in the care pathways available to people with I-RMDs and in who provides support for fatigue. The use of ‘health and well-being professionals’ reflects this breadth and includes a range of sources of support from multidisciplinary rheumatology teams to individual practitioners such as mental health therapists and/or fitness and exercise instructors. It is important to mobilise all available resources that might benefit people with I-RMDs and to recognise that elements of fatigue support might derive from shared decisions taken in both clinical and non-clinical settings.46
In managing fatigue, the needs and preferences of people with I-RMDs should be considered together with their clinical disease activity, comorbidities and other individual psychosocial and/or contextual factors
Current evidence suggests that fatigue may be caused and maintained by an array of biopsychosocial factors, which vary between and within individuals over time. This conceptualisation of fatigue underpins OAP1 and needs to be reflected in managing the symptom, which should be tailored to individuals with I-RMDs. Providing tailored fatigue management options includes considering the needs and preferences of people with I-RMDs, which will contribute to the shared decision-making underpinning OAP3. Management of fatigue also needs to be set in the context of exploring which factors might be contributing to an individual’s fatigue. This could include stress, disease activity, pain, sleep quality, comorbid long-term conditions, obesity, deconditioning and low levels of physical activity, low mood and withdrawal and ‘boom and bust’ activity patterns, among others.26 47
Recommendations
Health professionals should incorporate regular assessment of fatigue severity, impact and coping strategies into clinical consultations
Addressing fatigue should be part of usual clinical care for people with I-RMDs and incorporating regular assessment of fatigue is an important part of this process. People with I-RMDs have reported fatigue when their disease activity levels are not only high but also when they are in remission or low disease states, with fatigue being severe in about half of the cases.27 48 Therefore, it is important to conduct regular assessments of fatigue over time and not make assumptions about when someone might be impacted by fatigue or when discussions about fatigue might be relevant. A strategic option for clinical practice may be to use a single-item instrument as a screening tool (eg, BRAF-NRS and RAID-F, among others), which could be supplemented by additional multidimensional assessments if significant levels of fatigue are identified by the screening tool.49 It is important that responsibility for raising the issue of fatigue does not lie solely with the person with an I-RMD.
Not only might fatigue itself fluctuate over time but also how it affects people and how they respond can change. Central to this recommendation is that assessment should include not only the level or severity of fatigue but also the impact of the symptom on daily life and how someone is coping with it.50 51 These assessments should inform the clinical consultations of people with I-RMDs and lead to discussions about management options.
As part of their clinical care, people with I-RMDs and fatigue should be offered access to tailored physical activity interventions and encouraged to engage in long-term physical activity
According to the results of our SLR, there is evidence that supervised physical activity interventions can help reduce fatigue in people with I-RMDs. Existing EULAR recommendations on physical activity also emphasise its importance in disease management based on proven efficacy, feasibility and safety.52 As such, tailored physical activity that considers a person’s current sedentary and exercise behaviours; their disease activity, disease damage, comorbidities and disability; and their preferences and goals should be offered to people with I-RMDs and fatigue as part of their clinical care. However, there is also evidence of the benefits of unsupervised physical activity outside clinical care settings.53–56 Therefore, long-term physical activity as a lifestyle change should be encouraged. There was consensus in the taskforce that the role of health professionals is to engage in shared decision-making about options and to facilitate access to physical activity interventions.
As part of their clinical care, people with I-RMDs and fatigue should be offered access to structured and tailored psychoeducational interventions
There is evidence that psychoeducational interventions can help reduce fatigue in people with I-RMDs. This evidence is for structured, time-limited interventions. Typically, these go beyond information provision alone and explore the thoughts, feelings (physical and emotional) and behaviours of the person with an I-RMD in relation to their fatigue. As with recommendation 2, the role of health professionals is to engage in shared decision-making with the person with an I-RMD and fatigue and to facilitate access to psychoeducational interventions. It cannot be assumed that people with I-RMDs have achieved optimal benefits from participating in a single ‘one-off’ psychoeducational intervention or that helpful behaviour changes will be maintained for a certain length of time. Therefore, access to psychoeducational interventions should be discussed periodically and should be needs based and not restricted based on previous offers and/or uptake. Fatigue-specific and/or other biopsychosocial and contextual factors can change over time, both within and between people with I-RMDs and fatigue. As such, psychoeducational interventions might be helpful to people at different points in their I-RMD trajectory.
The presence or worsening of fatigue should trigger evaluation of inflammatory disease activity status and consideration of immunomodulatory treatment initiation or change, if clinically indicated
There is evidence that pharmacological interventions that reduce disease activity are also efficacious in reducing fatigue in people with I-RMDs, especially biologic agents.35 These interventions are indicated and licensed to treat high disease activity levels, and recommendation 4 needs to be understood within the context of regulatory restrictions. A level of fatigue can always be present for some people with I-RMDs. However, if someone’s fatigue is distressing and impactful or it worsens, this should trigger an evaluation of their disease activity. This evaluation might be more than calculating an individual’s disease activity score and include procedures such as MRI of their sacroiliac joints or spine to assess the presence of inflammatory/acute lesions or an ultrasound of their joints to check for synovitis. If high levels of (inflammatory) disease activity are present and are subsequently treated by starting and/or changing an immunomodulatory drug, fatigue will likely decrease. This includes disease modifying antirheumatic drugs such as biologics and other drugs such as prednisolone. It is unclear whether the improvement comes from a direct action of these interventions on fatigue or indirectly through reduction in inflammation or disease activity.
Research agenda
The SLRs conducted to inform these recommendations highlighted existing gaps in the literature, which, together with key discussion points raised during the taskforce meetings, resulted in our proposed research agenda (box 1).
Research agenda
The development of recommendations for instruments to measure fatigue across I-RMDs. This should include summaries of what individual instruments capture and their psychometric properties, plus identification of any missing domains. Ultimately, it would be helpful to standardise fatigue measurement in research and clinical practice (ie, define a gold standard).
Understanding of the mechanisms of fatigue interventions, including the efficacy of single modalities or components in non-pharmacological interventions such as sleep hygiene training, physical activity, pacing, cognitive-behavioural management or weight reduction in case of obesity, plus predictors of improvement and long-term adherence.
Understanding the efficacy and safety of interventions in specific I-RMDs where evidence is still scarce, for example, systemic sclerosis, idiopathic inflammatory myopathies and giant cell arteritis.
Understanding tailoring and implementation of fatigue support in different contexts, including what works, for whom and under what circumstances. This research should be pragmatic and wide-ranging and involve investigation of modes of delivery, content and structure designed to address varying levels of therapeutic intensity, health literacy, cultural appropriateness and inclusivity.
Related to the point above, there is a need for innovative trial designs that can provide insight into tailored intervention effects at the individual level as well as the group level.
Further research to understand the underlying biology of fatigue.
Discussion
Existing EULAR recommendations include self-management advice in routine clinical care and the role of health professionals such as nurses to support self-management skills to increase the sense of control, self-efficacy and empowerment of people with I-RMDs.57 58 Patient education recommendations highlight the importance of an approach tailored to individual needs, including activity regulation, physical activity and behaviour change.59 These recommendations can potentially help people with I-RMDs cope with the impact of symptoms. In this EULAR taskforce, we developed four OAPs and four recommendations for managing fatigue in people with I-RMDs. The OAPs are based on theoretical reasons, clinical experience and models of patient-centred healthcare, while the recommendations incorporate the evidence from two SLRs. The low number of recommendations reflects the limited evidence available at the time.
Historically, the scientific uncertainty about the pathogenesis of fatigue and the absence of a curative treatment has led to a reluctance to discuss fatigue in clinical practice. These OAPs and recommendations are intended to address this. They are premised on understanding fatigue as multifactorial and the need to communicate this to people with I-RMDs and to help them reflect on potential underlying drivers. Related to this is the understanding that fatigue is a long-term challenge for many people with I-RMDs, so access to support should be reviewed regularly. The taskforce recognises that some healthcare systems, insurers and providers might challenge ongoing access to support provision. However, the consensus is to recommend optimal care.
Regular assessment of fatigue severity, impact and coping strategies should be part of usual care and used to facilitate discussions between people with I-RMDs and health professionals. These discussions require knowledge, and the taskforce understands that health professionals may need to acquire skills, for example, how to explore individual fatigue drivers and coping strategies. Assessment of fatigue raises the issue of measurement.49 In 2007, the OMERACT group agreed that fatigue should be measured in RA clinical trials whenever possible,60 but there are no recommendations about which instruments to use in research and clinical practice across I-RMDs. Addressing this complex issue is beyond the scope of this taskforce. However, we have included a list of which instruments were used (box 2) in the two SLRs.35 36
List of instruments to measure fatigue*
Functional Assessment of Chronic Illness Therapy (FACIT).
FACIT Fatigue Subscale (FACIT-F).
Fatigue Severity Scale (FSS).
Fatigue Self-Efficacy Scale (FSES).
Multidimensional Assessment of Fatigue (MAF).
Global Fatigue Index (GBI).
Fatigue Impact Scale (FIS).
EULAR Primary Sjogren’s Syndrome Patient-Reported Index Score-Fatigue Scale (ESSPRI).
Multidimensional Fatigue Inventory (MFI).
MAC Fatigue Scale.
Profile of Mood States Fatigue Scale (POMS).
VAS-Fatigue.
Vitality Scale Short Form 36 (SF-36).
Fatigue Scale of the Checklist Individual Strength (CIS).
Bristol Rheumatoid Arthritis Fatigue-Multi-Dimensional Questionnaire (BRAF-MDQ).
BRAF Effect Numerical Rating Scale (NRS).
Multidimensional Fatigue Inventory (MFI-20).
Patient-Reported Outcome Measurement Information System Fatigue Short Form (PROMIS).
Item Checklist of Individual Strengths (CIS-20).
Rheumatoid Arthritis Impact of Disease questionnaire (RAID-F).
Bath Ankylosing Spondylitis Disease Activity Index-Fatigue (BASDAI-F).
Fatigue-Profile of Fatigue Questionnaire (ProF).
Chalder Fatigue Scale (CFS).
Fatigue Numerical Rating Scales (NRS).
Fatigue Assessment Scale (FAS).
Health Assessment Questionnaire (HAQ) fatigue domain.
*This list is based on the instruments used to measure fatigue in the two systematic reviews undertaken to inform these recommendations.
Assessment of fatigue and identifying people with I-RMDs who are being negatively impacted should lead to shared decision-making about the offer and uptake of management options. Although shared decision-making has been part of patient-centred models of rheumatology healthcare in recent years, it is not easy to undertake. Recent research has suggested the need for education and training that equips and empowers health professionals to apply shared decision-making, plus the need for a commitment of time, resources and financial support for national, regional and organisational initiatives to make it a reality.61 However, the taskforce agreed that shared decision-making should be an important feature because there is clinical experience that people actively involved in health management decisions are more satisfied with their care and more adherent to treatment recommendations. It has been proposed that health professionals can promote shared decision-making by communicating respect for the opinions and values of the person with an I-RMD, providing adequate information on management options and assisting them in weighing the benefits and risks of those options, including how they might be incorporated into their daily lives.62
The SLR evidence for non-pharmacological interventions for fatigue mainly concerned structured, time-limited physical activity and psychoeducational interventions. However, the taskforce reflected that there could be other non-pharmacological interventions for which there is currently insufficient evidence but which might be helpful at the level of an individual with an I-RMD due to the factors implicated in their fatigue, for example, cognitive behavioural therapy for insomnia or weight management for obesity.63 64 Structured and time-limited interventions are typically more therapeutically intensive than the provision of informational materials such as booklets and self-help guides. In a stepped model of care (whereby the most effective yet least resource-intensive treatment is delivered to patients first, only ‘stepping up’ to intensive interventions as clinically required), health professionals can consider including these less therapeutically intensive interventions as part of the management options that they offer to people with I-RMDs.
The SLR found that pharmacological interventions aimed at reducing disease activity are also efficacious and safe for managing fatigue in people with I-RMDs, particularly biologics. The evidence was robust and applicable to many I-RMDs. In virtually all RCTs, fatigue was assessed as a secondary outcome, with the primary outcome being disease-specific treatment response measures. These results suggest that control of inflammatory activity, the primary indication for treatment, coadjuvants the reduction of fatigue levels.35 Safety results of pharmacological interventions were reassuring and in line with known safety profiles and summaries of product characteristics of the respective drug. It should be noted that although the taskforce intended to review the safety of non-pharmacological interventions for fatigue, safety outcomes were often under-reported, but there was no indication that they were not safe.
In conclusion, EULAR recommendations have been developed to manage fatigue in people with I-RMDs. Central to these are regular assessment of fatigue and shared decision-making about the best management options at that time. Dissemination will focus on promoting these recommendations to people with I-RMDs and their networks, health professionals and other stakeholders involved in the provision of healthcare services, including patient organisations.
Ethics statements
Patient consent for publication
Acknowledgments
This paper was presented as an abstract at EULAR 2023 titled ‘EULAR recommendations for the management of fatigue in people with inflammatory rheumatic and musculoskeletal diseases’. https://ard.bmj.com/content/82/Suppl_1/437.
References
Footnotes
Handling editor Désirée van der Heijde
X @annamolto, @RajAmarr, @v_ritschl, @pedrommcmachado
Contributors All authors are members of the EULAR’s taskforce for the development of 2023 EULAR recommendations for the management of fatigue in people with inflammatory rheumatic diseases. EJFS and BF were the fellows. ED was the convenor. PMM was the methodologist. All authors have contributed to the work, read and finally approved the manuscript for submission.
Funding This study was funded by EULAR (Project HPR052: EULAR points to consider/recommendations for the management of fatigue in people with inflammatory rheumatic diseases).
Competing interests ED, BF, EJFS, AM, CF, CE-A, DC, EE, FE-L, IB, JP, MU, MAFJvdL, MR, PB, RA, RG, SR, SP, TT and VR: none. CH has received speaker fees from AbbVie. KH has received consulting/speaker fees from AbbVie, Novartis and Galapagos. RH has received speaker fees from AbbVie. TU has received personal consulting/speaker fees from Galapagos, Grünenthal, Novartis, Pfizer and UCB outside the submitted work. PMM has received consulting/speaker fees from AbbVie, BMS, Celgene, Eli Lilly, Galapagos, Janssen, MSD, Novartis, Orphazyme, Pfizer, Roche and UCB, all unrelated to this manuscript, and is supported by the National Institute for Health Research, University College London Hospitals and Biomedical Research Centre.
Provenance and peer review Not commissioned; externally peer reviewed.