Abstract:ObjectiveTo use statistical methods to establish a threshold for individual response in patient‐reported outcomes (PROs) in patients with rheumatoid arthritis.MethodsWe used an analysis of variance model in patients on stable therapy (discovery cohort) to establish critical differences (dcrit) for the minimum change associated with a significant individual patient response (beyond normal variation) in the PRO measures of pain (0–10), fatigue (0–10), and function (Funktionsfragebogen Hannover questionnaire; 0–1… Show more
“…However, the strong association with pain is more surprising and supports the clinical relevance of a DAS28-d crit response as a surrogate for outcomes important to patients. The mean change in pain during tocilizumab and anti-TNF treatment exceeded the individual pain-d crit response value of 30 mm (corresponding to 3 points on a scale of 0 to 10 as calculated by Scharbatke et al [6]) in the DAS28-d crit responder group, but not in the group that did not achieve a DAS28-d crit response, suggesting that changes in pain associated with a DAS28-d crit response were clinically meaningful to patients. Patients with a DAS28-d crit response also showed strong improvements in patient-reported function as assessed by the HAQ-DI.…”
Section: Discussionmentioning
confidence: 63%
“…Previous studies have found that DAS28-d crit responses are associated with improvements in function as assessed by the Funktionsfragebogen Hannover patient questionnaire [3] and that patients with DAS28-d crit responses are more likely to achieve individual responses in PROs than patients who do not achieve a DAS28-d crit response [6]. In this study, we extend these observations by showing that DAS28-d crit responses were closely associated with In this study, the FACIT fatigue scale was reversed (0 = best; 52 = worst) so that lower scores were better, in keeping with other patient-reported outcomes.…”
Section: Discussionmentioning
confidence: 98%
“…In RA patients receiving stable therapy with conventional or biologic DMARDs during routine clinical care, the DAS28-d crit corresponded to a DAS28 decrease (improvement) ≥ 1.8 [3]; this value was confirmed in patients on tocilizumab monotherapy [4] in the non-interventional ICHIBAN study [5]. DAS28-d crit responses are more closely correlated with patient-reported improvements in functional capacity than EULAR responses [3] and are associated with significant improvements in patient-reported outcomes (PROs) [6], thereby demonstrating the clinical relevance of this response criterion. The validation study focused on change from baseline in an observational cohort initiating treatment with a biologic therapy [3].…”
Assessment of individual therapeutic responses provides valuable information concerning treatment benefits in individual patients. We evaluated individual therapeutic responses as determined by the Disease Activity Score-28 joints critical difference for improvement (DAS28-d crit ) in rheumatoid arthritis (RA) patients treated with intravenous tocilizumab or comparator anti-tumor necrosis factor (TNF) agents. The previously published DAS28-d crit value [DAS28 decrease (improvement) ≥ 1.8] was retrospectively applied to data from two studies of tocilizumab in RA, the 52-week ACT-iON observational study and the 24-week ADACTA randomized study. Data were compared within (not between) studies. DAS28 was calculated with erythrocyte sedimentation rate as the inflammatory marker. Stability of DAS28-d crit responses and European League Against Rheumatism (EULAR) good responses was determined by evaluating repeated responses at subsequent timepoints. A logistic regression model was used to calculate p values for differences in response rates between active agents. Patient-reported outcomes (PROs; pain, global health, function, and fatigue) in DAS28-d crit responder versus non-responder groups were compared with an ANCOVA model. DAS28-d crit individual response rates were 78.2% in tocilizumab-treated patients and 58.2% in anti-TNF-treated patients at week 52 in the ACT-ion study (p = 0.0001) and 90.1% versus 59.1% at week 24 in the ADACTA study (p < 0.0001). DAS28-d crit responses showed greater stability over time (up to 52 weeks) than EULAR good responses. For both active treatments, DAS28-d crit responses were associated with statistically significant improvements in mean PRO values compared with non-responders. The DAS28-d crit response criterion provides robust assessments of individual responses to RA therapy and may be useful for discriminating between active agents in clinical studies and guiding treat-to-target decisions in daily practice.
“…However, the strong association with pain is more surprising and supports the clinical relevance of a DAS28-d crit response as a surrogate for outcomes important to patients. The mean change in pain during tocilizumab and anti-TNF treatment exceeded the individual pain-d crit response value of 30 mm (corresponding to 3 points on a scale of 0 to 10 as calculated by Scharbatke et al [6]) in the DAS28-d crit responder group, but not in the group that did not achieve a DAS28-d crit response, suggesting that changes in pain associated with a DAS28-d crit response were clinically meaningful to patients. Patients with a DAS28-d crit response also showed strong improvements in patient-reported function as assessed by the HAQ-DI.…”
Section: Discussionmentioning
confidence: 63%
“…Previous studies have found that DAS28-d crit responses are associated with improvements in function as assessed by the Funktionsfragebogen Hannover patient questionnaire [3] and that patients with DAS28-d crit responses are more likely to achieve individual responses in PROs than patients who do not achieve a DAS28-d crit response [6]. In this study, we extend these observations by showing that DAS28-d crit responses were closely associated with In this study, the FACIT fatigue scale was reversed (0 = best; 52 = worst) so that lower scores were better, in keeping with other patient-reported outcomes.…”
Section: Discussionmentioning
confidence: 98%
“…In RA patients receiving stable therapy with conventional or biologic DMARDs during routine clinical care, the DAS28-d crit corresponded to a DAS28 decrease (improvement) ≥ 1.8 [3]; this value was confirmed in patients on tocilizumab monotherapy [4] in the non-interventional ICHIBAN study [5]. DAS28-d crit responses are more closely correlated with patient-reported improvements in functional capacity than EULAR responses [3] and are associated with significant improvements in patient-reported outcomes (PROs) [6], thereby demonstrating the clinical relevance of this response criterion. The validation study focused on change from baseline in an observational cohort initiating treatment with a biologic therapy [3].…”
Assessment of individual therapeutic responses provides valuable information concerning treatment benefits in individual patients. We evaluated individual therapeutic responses as determined by the Disease Activity Score-28 joints critical difference for improvement (DAS28-d crit ) in rheumatoid arthritis (RA) patients treated with intravenous tocilizumab or comparator anti-tumor necrosis factor (TNF) agents. The previously published DAS28-d crit value [DAS28 decrease (improvement) ≥ 1.8] was retrospectively applied to data from two studies of tocilizumab in RA, the 52-week ACT-iON observational study and the 24-week ADACTA randomized study. Data were compared within (not between) studies. DAS28 was calculated with erythrocyte sedimentation rate as the inflammatory marker. Stability of DAS28-d crit responses and European League Against Rheumatism (EULAR) good responses was determined by evaluating repeated responses at subsequent timepoints. A logistic regression model was used to calculate p values for differences in response rates between active agents. Patient-reported outcomes (PROs; pain, global health, function, and fatigue) in DAS28-d crit responder versus non-responder groups were compared with an ANCOVA model. DAS28-d crit individual response rates were 78.2% in tocilizumab-treated patients and 58.2% in anti-TNF-treated patients at week 52 in the ACT-ion study (p = 0.0001) and 90.1% versus 59.1% at week 24 in the ADACTA study (p < 0.0001). DAS28-d crit responses showed greater stability over time (up to 52 weeks) than EULAR good responses. For both active treatments, DAS28-d crit responses were associated with statistically significant improvements in mean PRO values compared with non-responders. The DAS28-d crit response criterion provides robust assessments of individual responses to RA therapy and may be useful for discriminating between active agents in clinical studies and guiding treat-to-target decisions in daily practice.
“…One contributing factor to this variation in treatment is when patients resist (refuse to adopt, avoid initiating/implementing, or discontinue) DMARD medication regimens recommended or prescribed by physicians . Patients’ resistance to DMARD treatment regimens can increase the risk of suboptimal treatment, prolong time spent with painful symptoms, and lead to progression of joint damage, diminishing patients’ current and future quality of life .This qualitative study contributes to a better understanding of the role that feelings play in how patients with chronic conditions weigh the benefits and costs of medication treatments.For the rheumatoid arthritis (RA) patients in our study, feelings such as pain, loss, helplessness, shame, fear, protectiveness, anger, disappointment, and anxiety played an important role in motivating decisions to accept or resist disease‐modifying antirheumatic drug treatment regimens.Feelings in response to experiences of illness symptoms, medication side effects, identity as an RA patient, the act of taking medication, and the decision‐making process itself affected patients’ willingness to accept prescribed or recommended treatment.…”
Feelings in response to experiences and information played a major role in how patients weighed the benefits and costs of treatment options, suggesting that addressing patients' feelings may be important when rheumatologists counsel about therapeutic options. Further research is needed to learn how best to address patients' feelings throughout the treatment decision-making process.
“…Clinical trials have shown that employing a T2T strategy leads to lower disease activity and reduction of progressive joint damage, compared to routine care . Furthermore, studies have demonstrated that improvements in these disease‐specific outcomes are associated with reduced pain and improved physical function, health‐related quality of life, and work productivity , suggesting that minimizing the amount of time RA patients spend with MHDAS is beneficial. Even brief periods of MHDAS (<3 months) are associated with progression of joint damage and worsened short‐term and long‐term pain and functional deterioration .…”
Adjusting DMARDs within 90 days was associated with shorter times to LDAS, but many patients with persistent MHDAS waited >90 days to adjust DMARDs. Interventions are needed to address the timeliness of DMARD adjustments for RA patients with MHDAS.
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