| Literature DB >> 25600850 |
Nalinie Joharatnam1, Daniel F McWilliams2, Deborah Wilson3, Maggie Wheeler4, Ira Pande5, David A Walsh6,7,8.
Abstract
INTRODUCTION: Pain remains the most important problem for people with rheumatoid arthritis (RA). Active inflammatory disease contributes to pain, but pain due to non-inflammatory mechanisms can confound the assessment of disease activity. We hypothesize that augmented pain processing, fibromyalgic features, poorer mental health, and patient-reported 28-joint disease activity score (DAS28) components are associated in RA.Entities:
Mesh:
Year: 2015 PMID: 25600850 PMCID: PMC4363056 DOI: 10.1186/s13075-015-0525-5
Source DB: PubMed Journal: Arthritis Res Ther ISSN: 1478-6354 Impact factor: 5.156
Participant characteristics
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| 50 | 24 | 26 | |
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| 76% | 75% | 77% | |
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| 60 (54–69) | 58 (54–66) | 63 (54–70) | |
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| 21% | 26% | 17% | |
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| Any | 69% | 71% | 65% |
| Paracetamol | 63% | 71% | 54% | |
| NSAID | 16% | 17% | 15% | |
| Opiate | 37% | 38% | 35% | |
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| Methotrexate | 59% | 50% | 65% |
| Sulfasalazine | 22% | 15% | 25% | |
| Other nonbiologic DMARD | 36% | 40% | 30% | |
| Combination nonbiologic DMARD | 24% | 29% | 15% | |
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| 12% | 8% | 16% | |
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| 31% | 33% | 27% | |
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| 20% | 15% | 21% | |
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| Knee | 173 (119–287) | 133 (58–181)** | 239 (169–470) | |
| Tibia | 140 (98–246) | 108 (61–167)** | 187 (122–337) | |
| Sternum | 155 (85–211) | 111 (70–175)** | 179 (149–256) | |
Demographics of the entire study group and a comparison between participants that did or did not satisfy fibromyalgia-classification criteria. Other nonbiologic DMARDs were azathioprine (n = 2), leflunomide (n = 4), gold (n = 3), hydroxychloroquine (n = 6), and cyclosporin (n = 3). Biologic therapies were antitumor-necrosis factor agents (n=4), rituximab (n=1), or abatacept (n=1). Combination DMARDs; two or more biologic or nonbiologic DMARDs. **P < 0.01 (compared with participants who did not satisfy criteria for fibromyalgia).
Associations of clinical characteristics with pressure pain-detection thresholds
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| −0.62** | −0.62** | −0.60** | ||
| TJC | −0.53** | −0.50** | −0.48** | ||
| VAS-GH | −0.52** | −0.46** | −0.52** | ||
| SJC | −0.04 | 0.03 | −0.04 | ||
| ESR | −0.12 | −0.21 | −0.14 | ||
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| −0.46** | −0.41** | −0.41** | ||
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| McGill Pain Questionnaire | Continuous | −0.43** | −0.60** | −0.47** |
| Intermittent | −0.41** | −0.41** | −0.40** | ||
| Neuropathic | −0.45** | −0.49** | −0.38** | ||
| Affective | −0.30* | −0.43** | −0.33* | ||
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| −0.47** | −0.57** | −0.46** | ||
| ICOAP | Constant | −0.34** | −0.39** | −0.35* | |
| Intermittent | −0.35* | −0.56** | −0.41** | ||
| Knee pain | −0.53** | −0.49** | −0.46** | ||
| Widespread Pain Index | −0.36* | −0.40** | −0.33* | ||
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| Fatigue Severity Scale | −0.27 | −0.33* | −0.27 | |
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| Beck Depression Index II | −0.40** | −0.35* | −0.36* | |
| State-Trait Anxiety Index | −0.24 | −0.16 | −0.12 | ||
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| −0.28* | −0.30* | −0.27* | ||
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| −0.44** | −0.41** | −0.39** | ||
Negative values indicate that higher levels of trait are associated with lower PPTs (more sensitive). Unadjusted correlation coefficients for log-transformed PPT are shown. Fibromyalgia is calculated from Widespread Pain Index + Somatic Symptoms Scale. **P < 0.01, *P < 0.05 for significance of association.
Multivariable associations of pressure-pain detection thresholds (PPTs) with DAS28 components
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| TJC | −0.37 | 0.030 | −0.42 | 0.017 | −0.29 | 0.092 |
| VAS-GH | −0.33 | 0.047 | −0.22 | 0.195 | −0.38 | 0.029 | |
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| SJC | −0.08 | 0.539 | −0.03 | 0.842 | −0.05 | 0.719 |
| ESR | −0.07 | 0.614 | −0.22 | 0.134 | −0.10 | 0.950 | |
Standardized β values and P values (not corrected for multiple comparisons) are shown for three regression models comparing the influence of DAS28 components on PPT. Multiple linear regression models with log-transformed PPT at each testing site as dependent variable, and TJC, VAS-GH, SJC, ESR, age, and gender as predictor variables.
Associations of clinical characteristics with fibromyalgia
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| 4.8 (4.4 – 5.3)** | 4.4 (3.8 – 4.9) | 0.46 | 0.001 | ||
| TJC | 11 (7 – 18)** | 6 (4 – 9) | 0.35 | 0.012 | ||
| VAS-GH | 70 (55 – 78)** | 42 (24 – 55) | 0.60 | <0.001 | ||
| SJC | 1 (0 – 2) | 1 (1 – 2) | −0.03 | 0.816 | ||
| ESR | 19 (8 – 29) | 17 (12 – 26) | 0.01 | 0.963 | ||
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| 0.58 (0.52 – 0.64)** | 0.50 (0.45 – 0.57) | 0.43 | 0.002 | ||
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| McGill Pain Questionnaire | Continuous | 5.3 (3.2 – 6.7)** | 2.3 (1.8 – 3.8) | 0.49 | <0.001 |
| Intermittent | 4.0 (3.0 – 5.5)** | 1.7 (0.7 – 2.8) | 0.61 | <0.001 | ||
| Neuropathic | 3.2 (2.3 – 5.7)** | 1.5 (0.8 – 3.8) | 0.54 | <0.001 | ||
| Affective | 4.0 (2.5 – 6.5)** | 1.8 (0.3 – 4.0) | 0.53 | <0.001 | ||
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| 3.8 (3.2 – 5.8)** | 2.2 (1.1 – 3.1) | 0.65 | <0.001 | ||
| ICOAP | Constant | 42 (8 – 65)** | 8 (0 – 35) | 0.45 | 0.001 | |
| Intermittent | 42 (29 – 58)** | 8 (0 – 32) | 0.57 | <0.001 | ||
| Knee pain | 7 (5 – 8)** | 3 (0 – 6) | 0.50 | <0.001 | ||
| Widespread Pain Index | 10 (7 – 13)** | 4 (2 – 4) | 0.86 | <0.001 | ||
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| Fatigue Severity Scale | 52 (38 – 61)* | 39 (25 – 57) | 0.46 | 0.001 | |
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| Beck Depression Index II | 16 (10 – 30)* | 13 (8 – 18) | 0.43 | 0.003 | |
| State-Trait Anxiety Index | 0 (−6 – 3)** | –6 (–9 – –2) | 0.39 | 0.006 | ||
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| 9 (7–10)** | 4 (3 – 7) | 0.83 | <0.001 | ||
Differences between DAS28, DAS28-P, individual score components, and mental health questionnaire scores for participants who did or did not satisfy fibromyalgia criteria, plus correlations of these variables with fibromyalgia, calculated from the summated Widespread Pain Index and Somatic Symptoms Scale scores. *P < 0.05, **P < 0.01 for differences between groups, or associations.
Figure 1Scatter plots of (A) DAS28-P indices and (B) anterior tibial PPT measurements versus fibromyalianess score (WPI + SSS). Best-fitted linear regression lines for each plot are shown. Other PPT measurements and the patient-reported components of DAS28 all showed similar plots.