Estimating minimally important differences for the PROMIS pain interference scales: results from 3 randomized clinical trials

Chen, Chen X.Kroenke, KurtStump, Timothy E.Kean, JacobCarpenter, Janet S.Krebs, Erin E.Bair, Matthew J.Damush, Teresa M.Monahan, Patrick O.2019-08-052019-08-052018-04Chen, C. X., Kroenke, K., Stump, T. E., Kean, J., Carpenter, J. S., Krebs, E. E., … Monahan, P. O. (2018). Estimating minimally important differences for the PROMIS pain interference scales: results from 3 randomized clinical trials. Pain, 159(4), 775–782. doi:10.1097/j.pain.0000000000001121https://hdl.handle.net/1805/20191Minimally important difference (MID) refers to the smallest meaningful difference that carries implications for patient care. Minimally important differences are necessary to help interpret patient-reported pain outcomes in research and clinical practice. The PROMIS pain interference scales were validated across diverse samples; however, more information about their MIDs could improve their interpretability. The purpose of this study was to estimate MIDs for 4 fixed-length PROMIS pain interference scales, including the 6-item Pain Short Form and the 4-, 6-, and 8-item pain interference scales used in the PROMIS profile instruments. Data were analyzed from 3 randomized controlled trials (N = 759). The 3 samples, respectively, consisted of patients with chronic low back pain (n = 261), chronic back pain or hip/knee osteoarthritis pain (n = 240), and a history of stroke (n = 258). For each sample, anchor- and distribution-based approaches were used to estimate MIDs. Standard error of measurement and effect sizes were used as distribution-based MID estimates. Anchor-based MID estimates were established by mapping PROMIS pain interference scores onto established anchor measures, including the Brief Pain Inventory, and retrospective and prospective global ratings of change. The distribution- and anchor-based MID estimates showed convergence. For the pain samples, MID estimates ranged from 2 to 3 T-score points. For the nonpain sample, MID estimates ranged from 3.5 to 4.5 T-score points. The MID estimates were comparable across the 4 fixed-length scales. These MIDs can be used to evaluate treatment effects in research and clinical care and to calculate estimates for powering clinical trials.en-USPublisher PolicyChronic painDisability evaluationPain measurement -- methodsPatient reported outcome measuresEstimating minimally important differences for the PROMIS pain interference scales: results from 3 randomized clinical trialsArticle