Association of Modic change types and their short tau inversion recovery signals with clinical characteristics- a cross sectional study of chronic low back pain patients in the AIM-study

Author:

Bråten Lars Christian HaugliORCID,Schistad Elina Iordanova,Espeland Ansgar,Kristoffersen Per Martin,Haugen Anne Julsrud,Marchand Gunn Hege,Vetti Nils,Pripp Are Hugo,Kadar Thomas Istvan,Skouen Jan Sture,Grotle Margreth,Grøvle Lars,Zwart John-Anker,Brox Jens Ivar,Storheim Kjersti,Anke Audny,Wilhelmsen Maja,Fors Terese,Kjos Guro,Østhus Ida Beate,Lurud Britt Elin,Granvigen Fredrik,Andersen Hege,Nygaard Øystein Petter,Rao Vidar,Claussen Siv Krüger,Andersen Erling,Froholdt Anne,Randen Sigrun,Presberg Hilde,Wigemyr Monica,Pedersen Linda Margareth,Winsvold Bendik Slagsvold,Rolfsen Mads Peder,Helllum Christian,Gammelsrud Karianne Wiger,Vigeland Maria Dehli,Lie Benedicte Alexandra,Flåm Siri Tennebø,Vigeland Magnus Dehli,Thorsø Marianne,Huneide Knut Morten,Sørensen Veronica,Lutro Olav,Holmgard Thor Einar,

Abstract

Abstract Background Modic Changes (MCs, magnetic resonance imaging (MRI) signal changes in the vertebral bone marrow extending from the vertebral endplate) may represent a subgroup of nonspecific chronic low back pain that could benefit from a specific management. The primary aim was to compare clinical characteristics between patients with type 1 versus type 2 MCs. The secondary aim was to explore associations between clinical characteristics and MC related short tau inversion recovery (STIR) signals. Methods This cross-sectional study used baseline data prospectively collected between 2015 and 2017 on the 180 patients included in the AIM-study (Antibiotics In Modic changes), a randomized controlled trial in a Norwegian hospital out-patient setting of patients with chronic low back pain, a lumbar disc herniation within the last 2 years, low back pain intensity score ≥ 5 (on a 0–10 scale) and current type 1 or type 2 MCs at the previously herniated lumbar disc level. We used prespecified clinical characteristics including self-report measures, physiologic measures and functional measures from clinical history and examination. The diagnostic accuracy of various clinical characteristics to discriminate between patients with type 1 MCs (with or without additional type 2 MCs) and patents with type 2 MCs only (not type 1) were assessed by calculating the area under the receiver-operating curve. We assessed the correlations of clinical characteristics with details of MC related STIR signal increase. Results No clinical characteristic differed between patients with type 1 (n = 118) versus type 2 (but not type 1) (n = 62) MCs. The clinical characteristics showed no/minor differences or no/weak correlations with MC related STIR signal increase. Patients with a positive Springing test (at any lumbar level) had slightly less volume of STIR signal increase than those with a negative test (mean difference 1.3 on a 0–48 scale, 95% CI 0.3 to 2.3). Conclusion Clinical characteristics were similar for patients with type 1 MCs and patients with type 2 MCs, and showed no clinically relevant correlations with MC related STIR signal increase. Trial registration ClinicalTrials.gov NCT02323412, First registered 23 December 2014

Funder

Helse Sør-Øst RHF

Helse Vest

Publisher

Springer Science and Business Media LLC

Subject

Orthopedics and Sports Medicine,Rheumatology

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