Validity and contributions to pain from the central aspects of pain questionnaire in rheumatoid arthritis.

Smith, SL.; Georgopoulos, V.; Ifesemen, OS.; James, R.; Ferguson, E.; Wakefield, RJ.; Wilson, D.; Buckley, P.; Platts, D.; Ledbury, S.; Choy, E.; Pickles, T.; Rutter-Locher, Z.; Kirkham, B.; Walsh, DA.; McWilliams, DF.

Validity and contributions to pain from the central aspects of pain questionnaire in rheumatoid arthritis.

All Authors

Smith, SL.

Georgopoulos, V.

Ifesemen, OS.

James, R.

Ferguson, E.

Wakefield, RJ.

Wilson, D.

Buckley, P.

Platts, D.

Ledbury, S.

Show 6 more

LTHT Author

Wakefield, Richard

LTHT Department

Rheumatology
NIHR Leeds Biomedical Research Centre

Publication Date

2025

Item Type

Journal Article

Abstract

Introduction: The central nervous system (CNS) contributes to pain perception across musculoskeletal conditions. The central aspects of pain (CAP) questionnaire captures a single score associated with quantitative sensory testing (QST) evidence of CNS dysfunction validated in knee osteoarthritis. Objectives: Given the different pathophysiology of rheumatoid arthritis (RA), an inflammatory polyarthritis, this cross-sectional study assessed CAP's psychometric properties and its association with pain in RA. Methods: Adults with RA were recruited from Nottinghamshire, London, and Cardiff. Participants completed CAP and reported pain using a numerical rating scale. A subgroup underwent additional assessments, including quantitative sensory testing (QST; Pressure Pain detection Threshold, Temporal Summation, Conditioned Pain Modulation), Disease Activity Score-28, C-reactive protein, questionnaires addressing pain and related characteristics, and Central Sensitization Inventory short form (CSI-9). Cronbach alpha, confirmatory factor (CFA), and Rasch measurement theory assessed CAP's reliability and validity. Multivariable linear regression modelled contributions to pain by inflammation indices and CAP or CSI-9. Results: The 380 participants (73% female, median 63 years) reported average pain over the past 4 weeks of 6/10 and a CAP score of 9/16. Central aspects of pain demonstrated acceptable reliability (ICC(2,1) = 0.71), CFA fit (comparative fit index = 0.99, Tucker-Lewis index = 0.99, root mean square error of approximation = 0.034, standardized root mean residuals = 0.03), and internal consistency (alpha = 0.82). Central aspects of pain was significantly associated with pain (0.50 <= beta <= 0.57) but not QST. Central aspects of pain explained 33% of pain variance, rising to 42% with inflammation, age, sex, and body mass index. Central Sensitization Inventory-9 correlated with pain, not QST and explained less pain variance than CAP. Conclusion: Central aspects of pain is reliable and valid for use with people with RA and explains RA pain variance better than inflammation or CSI-9.