Patient global assessment in measuring disease activity in rheumatoid arthritis: a review of the literature

Patient-reported outcomes (PROs) are increasingly recognized for their value in providing the patient’s perspective on aspects of their condition or their overall health status. Their incorporation into clinical practice and in research in rheumatoid arthritis (RA) is widely supported by international organizations and professional bodies [1, 2], including the European Patients’ Academy on Therapeutic Innovations (EUPATI; http://​www.​patientsacademy.​eu/​index.​php/​en/​) and the Patient-Centered Outcomes Research Institute (PCORI; http://​www.​pcori.​org/​research-results) in the United States, as well as regulatory agencies such as the Food and Drug Administration (http://​www.​fda.​gov/​) and the European Medicines Agency (http://​www.​ema.​europa.​eu/​ema/​), all of whom recognize the patient’s unique position in providing direct feedback on their disease.

Patient global assessment (PGA) is one of the most widely reported PROs in RA. The considerable burden of RA on the individual is related to both inflammation and damage but also to broader aspects of disease, including psychological and societal impact. The use of PROs like the widely used Health Assessment Questionnaire (HAQ) or the PGA allows a more holistic assessment of disease beyond objective measures of inflammation or structural damage, such as acute phase reactants or radiographic damage. Experts from the American College of Rheumatology (ACR), the European League Against Rheumatism (EULAR), and the Outcome Measures in Rheumatology Clinical Trials (OMERACT) have endorsed a “core set” of data for use in RA clinical trials which includes PGA [3, 4]. In recent randomized controlled trials and observational studies in RA, PGA has been reported in 49 % of studies, making it the second most frequently collected PRO after physical function (68 %) [5]. PGA is also incorporated into several of the major outcome and disease activity scores in RA, often as the only PRO: these include the ACR/EULAR remission criteria, the 28-joint count Disease Activity Score (DAS28), the Simplified Disease Activity Index (SDAI), the Clinical Disease Activity Index (CDAI), and the Routine Assessment of Patient Index Data (RAPID3).

However, the use of PGA in RA presents many challenges and limitations. The several possible ways of measuring PGA, including the intended assessment or underlying concept (i.e., global health versus disease activity) and variations in wording/phrasing and time period assessed may lead to differences in interpretation of PGA. Discordance with objective RA measures is also an issue that needs to be addressed. The latter is particularly important in the context of treating to target aiming for remission and shared decision-making [6, 7]. What the different formulations of PGA are, their impact, and justifications for their use remain to be clarified.

To provide readers with a complete overview regarding PGA in RA, a review of the literature was undertaken based on a hierarchical literature search including hand searches and expert opinion searches covering key publications in the field. The objectives were to explore the value of PGA as an outcome measure in RA, focusing on its psychometric properties (feasibility, validity, reliability, and sensitivity to change). Specifically, this review discusses the validity and impact of different wordings/phrasings and time period assessed as part of PGA on patients’ assessment of disease, as well as discordance between physician global assessment and PGA.

The main strengths and weaknesses of PGA are summarized in Table 2. Below, we review each psychometric property of PGA.

The heterogeneity in the wording/phrasing of PGA requires caution when interpreting the results [34]. The DAS28 is one of the most commonly used composite scores in routine clinical practice; the PGA component of the score carries a small weighting of 0.014, which may still result in differences to the overall DAS28 score (the maximum difference being 1.4 when holding the other variables constant and using first a PGA-VAS score of 0 mm, then of 100 mm). French et al. [11] performed a study where DAS28 was calculated in the same patients when using different PGAs. Five different versions of the PGA-VAS were assessed based on: (1) “Feeling” (“How do you feel concerning your arthritis over the last week?”); (2) Disease activity (“How active has your disease been this week?”); (3) “Well-being” (“How has your overall well-being been this week?”); (4) “Best/worst” (“If 0 is the best you have ever been and 100 is the worst you have ever been, where do you think you have been over the last week?”); and (5) “Arthritis impact measurement scales” (AIMS; “Considering all the ways your arthritis affects you….”). All PGA-VAS versions correlated strongly with each other (rho = 0.67–0.87, p < 0.0001) [11]. However, when the phrasing of PGA varied there was a difference in DAS28 scores, the largest being 0.63 points. Such differences in score, though small, could have clinical implications, i.e., on the eligibility for biologic disease-modifying anti-rheumatic drugs in countries where access to these drugs is restricted based on strict DAS28 cutoffs.

However, although there are differences at the individual level according to the concepts, wordings/phrasing used, and time period assessed, these differences do not always reflect differences at the group level [11, 12]. Direct comparison between studies is limited due to differences in techniques used to assess the PGA and the population used. Although this has not been explored, it is possible PGA interpretation may be different in clinical trials versus in “clinical practice”, in particular given population selection and the often multiple use of PROs in studies.

Table 4 summarizes the main aspects of the PGA and key messages presented in this review.

Both DAS28-based remission and ACR/EULAR defined remission criteria incorporate PGA into their scores [2, 35]. ACR/EULAR Boolean-based remission is defined as PGA ≤1 using a 0–10 VAS. Therefore, PGA plays a major role in determining fulfillment of remission criteria in RA [6, 7, 35, 36]. In fact, PGA appears to be often a limiting factor for remission—i.e., in patients with no visible inflammation, remission may not be reached because of PGA. In a study based on the DREAM remission induction cohort, ACR/EULAR remission was present in 20.1 % of the patients. In 108 out of 512 patients, the PGA score was >1 using a 0–10 VAS despite fulfillment of the remaining criteria (TJC28, SJC28, and C-reactive protein in mg/dl ≤1). The specific wording of questions and anchors used for the PGA were: “Considering all of the ways your arthritis affects you, mark “X” on the scale for how well you are doing” (“very well” to “very poor”)” [37]. Similarly, close to half the patients without visible inflammation in the ESPOIR cohort did not achieve ACR/EULAR remission because of PGA levels above 1/10 cm [38]. Thus, near-remission defined as three of the four criteria (PGA excluded) is the most frequent status [36‐39]. Many of these patients have a PGA above 1 but still quite low (usual values are around 2/10) [40], perhaps suggesting a need for revising the remission cutoff value for PGA. Another question relates to the phrasing of PGA in the remission criteria: would using the “disease activity” formulation make more sense than using the “global health” formulation? Unpublished results based on the ESPOIR French early arthritis cohort indicate that the disease activity wording will lead to less states of near-remission.

Overall, the high frequency of near-remission raises the question of whether the way remission is defined needs to be better clarified, i.e., should it reflect absence of inflammation alone or absence of inflammation and symptoms? The current amalgamation of joint counts and C-reactive protein with PGA indeed leads to some difficulties of interpretation, particularly in cases of near-remission. Furthermore, the predictive validity of near-remission is of clear importance, predicting long-term outcomes of these patients. Our unpublished results indicate near-remission predicts radiographic progression over 3 years in early RA, as well as ACR/EULAR remission, in the ESPOIR cohort, suggesting near-remission is a possible valid and even sufficient predictive outcome in early RA [40, 41]. In the context of treating to target, more work is needed on how to best interpret levels of PGA when aiming for remission.

PGA is a wide-reaching measure which may mean different things for different people. Data are available on the main drivers of PGA at the group level. PGA reflects both disease activity and other factors. Given PGA is assessed to provide information additional to joint counts or acute phase reactants, it is expected there might be some but not complete overlap.

It is interesting to compare PGA to another global, “gestalt” assessment of disease, which is the physician global assessment. Physician global assessment is a well-validated outcome which is recognized as part of the RA core set [3]. Evidence suggests that discordance exists between patient and physician assessment of RA disease activity, with studies consistently showing that PGA is very often scored higher than physician global assessment [13, 43, 46‐49]. Discordance in most studies is defined as a difference of ≥3/10 points between the PGA and physician global assessment [12]. The prevalence of discordance using this definition was found to be around 43 % in a recent meta-analysis, indicating a different understanding or perspective of the same general concept [48].

What studies have shown to date is that variables that are important to patients are not the same as those valued by physicians as reflecting disease activity (Table 5). Generally, more objective measures of disease, e.g., joint counts and elevated acute phase reactants, lead to a higher physician global assessment whereas pain and altered quality of life without visible signs of inflammation, but also comorbidities and psychological distress, will lead to higher PGA (Table 5) [50]. In such cases of discordance, it is important to discuss the patient’s psychological status as well as personal life factors since the solutions will not always lie in immunosuppressive drugs but rather might depend on non-pharmacological interventions. This discordance may act as a clue to the presence of non-disease severity factors influencing the PGA.

The increasing emphasis on the patients’ perspective of health in considering priorities and making treatment choices has resulted in PROs being a core part of routine assessment of disease in RA and also an end-point in clinical trials and observational studies. Recent guidelines are characterized by a shift from the traditional approach of physician-led physical examination and investigations such as laboratory tests and radiographs (the “biomedical model”) to a more patient-centered approach to care [51]. PGA is one of the most commonly captured and reported PROs, mainly due to its simplicity and its feasibility in both clinical practice and registers as well as in clinical trial settings. It is strongly correlated with other self-reported outcomes and carries important patient information. Therefore, despite the controversy regarding the value of PROs including the PGA, these represent the only way to assess some of the aspects related to RA, for example, symptoms, justifying that clinician-reported outcomes and PROs should be considered as complementary to each other [52].

The lack of homogeneity in the concepts, wordings/phrasings, and time period assessed by PGA threatens the validity of PGA since it may lead to modified responses resulting from the diversity of formulations [15]. Such diversity can influence clinical and treatment decision-making, highlighting the importance of standardizing (where appropriate) and validating the question phrasing as part of capturing information on PGA. We suggest that emphasis is placed on reducing heterogeneity in wording/phrasing and time period of the PGA in order to enable more uniform capture (and hence interpretation) of information across clinical and research settings.

The discordance between PGA and physician global assessment demonstrated in many studies to date suggests that perceptions of disease activity by patients may be influenced by different factors, resulting in different aspects of disease being measured. Such discordance can negatively influence medical care, adherence to treatment, and disease outcomes. Despite this, the use of PROs such as PGA is particularly informative, bringing additional information and perspective, especially given the observed discordance of assessment between physicians and patients [52]. Like other PROs, it is of particular value when changes in clinical measurements or laboratory or radiographic outcomes may not translate into meaningful benefits for patients. In particular, the ease of use and feasibility of PGA, with little or no training of patients required to complete it, means that it can be easily incorporated into busy clinical settings. However, it is important that this contribution of patients to disease activity scores via the PGA is evaluated in a standardized way.

We feel the lack of a standardized definition on the concept, wording/phrasing, and time period assessed as part of PGA represents one of its weaknesses. This does not preclude the possibility of having more than one version of PGA; however, it requires clarity with regard to what version is selected and for which purpose (e.g., PGA for disease activity or PGA for global health). We advocate the use of a homogeneous wording in a specific context, e.g., for repeated measures it is important to use the same wording/phrasing. This is particularly important in routine clinical practice since it may lead to incorrect interpretations regarding, for example, response to treatment.

In terms of practical recommendations, the suggestion of the authors is that phrasing of PGA may at this stage be proposed as capturing (1) either global health or disease activity which is (2) related to arthritis and captured by the reference period of (3) today/this point in time. Examples would be the formulation proposed in the RAPID 3 score for global health or the one proposed in the EULAR/ACR remission criteria for disease activity (Table 6) [37].

The choice between the two concepts will depend on the objective of the measurement of the PGA. The global health question gives more holistic information on patient status since it includes to a wider extent elements such as comorbidities and psychological distress. The disease activity-PGA is more in line with more objective measures of disease and assesses more closely the inflammatory burden.

PGA is a key outcome measure in RA with clear validity and usefulness. However, the lack of a “gold standard” in terms of its wording/phrasing and time period assessed necessitates more research into this field in order to avoid pitfalls in interpretation and, consequently, in the achievement of treatment targets. In this review, we propose homogenized wordings which may be considered for future studies. Importantly, a clear understanding of what PGA measures and potential sources of variation in its reporting is key to accurate interpretation. Furthermore, this review gives insights into factors associated with and affecting PGA—for example, its close association with pain, mood, and fatigue and issues around discordance with physician global assessment. This may be informative in guiding interventions to improve care and overall quality of life for RA patients.