Skip to main content
Download PDF
  • Research article
  • Open access
  • Published:

Absence of ultrasound inflammation in patients presenting with arthralgia rules out the development of arthritis

Arthritis Research & Therapy volume 19, Article number: 202 (2017) Cite this article

Abstract

Background

To decrease the burden of disease of rheumatoid arthritis (RA), patients at risk for RA need to be identified as early as possible, preferably when no clinically apparent synovitis can be detected. Up to now, it has been fairly difficult to identify those patients with arthralgia who develop inflammatory arthritis (IA), but recent studies using ultrasound (US) suggest that earlier detection is possible. We aimed to identify patients with arthralgia developing IA within 1 year using US to detect subclinical synovitis at first consultation.

Methods

In a multi-centre cohort study, we followed patients with arthralgia with at least two painful joints of the hands, feet or shoulders without clinical synovitis over 1 year. Symptom duration was < 1 year, and symptoms were not explained by other conditions. At baseline and at 6 and 12 months, data were collected for physical examinations, laboratory values and diagnoses. At baseline, we examined 26 joints ultrasonographically (bilateral metacarpophalangeal joints 2–5, proximal interphalangeal joints 2–5, wrist and metatarsophalangeal joints 2–5). Scoring was done semi-quantitatively on greyscale (GS; 0–3) and power Doppler (PD; 0–3) images. US synovitis was defined as GS ≥ 2 and/or PD ≥ 1. IA was defined as clinical soft tissue swelling. Sensitivity and specificity were used to assess the diagnostic value of US for the development of IA. Univariate logistic regression was used to analyse the association between independent variables and the incidence of IA. For multivariate logistic regression, the strongest variables (p < 0.157) were selected. Missing values for independent variables were imputed.

Results

A total of 196 patients were included, and 159 completed 12 months of follow-up. Thirty-one (16%) patients developed IA, of whom 59% showed US synovitis at baseline. The sensitivity and specificity of US synovitis were 59% and 68%, respectively. If no joints were positive on US, negative predictive value was 89%. In the multivariate logistic regression, age (OR 1.1), the presence of morning stiffness for > 30 minutes (OR 3.3) and PD signal (OR 3.4) were associated with incident IA.

Conclusions

The presence of PD signal, morning stiffness for > 30 minutes and age at baseline were independently associated with the development of IA. Regarding the value of US in the diagnostic workup of patients with early arthralgia at risk for IA, US did perform well in ruling out IA in patients who did not have US synovitis.

Background

Rheumatoid arthritis (RA) is a debilitating chronic autoimmune disease. Early initiation of effective disease-modifying drugs can slow disease progression and diminish joint damage [1, 2]. It could be that starting disease-modifying anti-rheumatic drug (DMARD) therapy in the arthralgia phase or even before that could lead to better patient outcomes [3, 4]. Until now, it has been fairly difficult to identify those patients with arthralgia who would benefit from such early initiation of DMARD therapy because only those who would have subsequently developed inflammatory arthritis (IA) related to a chronic inflammatory joint disease would benefit from such an early intervention. Recent technical developments in magnetic resonance imaging (MRI) and ultrasound (US) suggest that earlier detection of inflammation should be possible before clinical manifestation [5].

We know from previous research that 15% of patients with arthralgia who presented without clinical signs of inflammation at baseline would be diagnosed with IA 1 year later, half of whom were anti-citrullinated protein antibody (ACPA)-positive [6]. Although ACPA positivity is a very good predictor for those patients who will develop IA within 1 year, it is still difficult to identify the exact individuals who will develop IA, because any ACPA-positive individual has an a priori chance of 50% of developing IA. In seronegative patients, the prediction of IA is even more difficult, because only 5% develop IA within the subsequent year. Imaging techniques have been shown to be able to detect synovitis before its clinical appearance and could be of help in identifying those at risk of IA [5, 7]. MRI and US are both available in the daily rheumatology clinic. MRI has the disadvantage of being time-consuming, thereby constraining the number of joints which that can be assessed. In addition, MRI is expensive and not accessible for everyone (e.g., joint replacement, pacemaker). US is more operator-dependent because, owing to probe position, multiple examiners can make different observations. However, US is more flexible and easily applied in the clinic. In this study, we aimed to identify which patients with arthralgia will develop clinically apparent IA within 1 year using US to detect subclinical synovitis at first consultation added to demographic and clinical variables.

Methods

This study was a multi-centre (three centres) prospective cohort study in which we followed patients with inflammatory joint complaints for 1 year.

Patients

Patients with inflammatory joint complaints of the hands, feet or shoulders without clinically apparent synovitis in any joint were recruited from the outpatient clinic. Patients had a symptom duration < 1 year which could not be explained by other conditions, such as IA, fibromyalgia, overuse or trauma. To distinguish inflammatory arthralgia from other forms of arthralgia, patients had to have at least two painful joints in hands, feet or shoulders and two of the following criteria adapted from the Rotterdam Early Arthritis Cohort (REACH) trial [8]: morning stiffness for more than 1 h, unable to clench a fist in the morning, pain when shaking someone’s hand, pins and needles in the fingers, difficulties wearing rings or shoes, family history of RA and/or unexplained fatigue for < 1 year. Patients had to be able to understand, speak and write in Dutch. Patients received treatment as the rheumatologists saw fit, but no DMARDs were prescribed at first consultation. Written informed consent was obtained from the participants according to the Declaration of Helsinki. The study was approved by the medical ethics committee of Erasmus MC, University Medical Centre Rotterdam, Rotterdam, The Netherlands (MEC-2010-353) and was assessed for feasibility by the local ethical bodies of Maasstad Hospital and Vlietland Hospital.

Clinical examination

A trained research nurse collected data about articular symptoms, extra-articular symptoms, family history and previous medical history. Data collection at baseline and at 6-month and 12-month follow-up included a detailed medical examination (swollen joint count in 44 joints, tender joint count in 44 joints), laboratory variables (ACPA, rheumatoid factor [RF], erythrocyte sedimentation rate), diagnosis and medications used. Observed soft tissue swelling needed to be confirmed as an arthritis by the treating rheumatologist. Because substantial loss to follow-up was expected at the start of the study due to the nature of recovering arthralgia for the majority of patients, a telephone interview was scheduled if patients did not want to return to the clinic for their 6- and 12-month evaluations. Patients were asked about their clinical symptoms. If the interviewer doubted the potential presence of clinical synovitis, patients were asked to return to the outpatient clinic for clinical evaluation.

US examination

At baseline, trained US examiners blinded to the participants’ clinical details performed US following the European League Against Rheumatism (EULAR) guidelines concerning patient position and scanning planes [9]. To minimise inter-variability, US examiners followed a standardised scanning protocol regarding acquisition and scoring. The US machine used was the MyLab60 (Esaote, Genoa, Italy) with a high-frequency linear array probe (LA435, 10–18 MHz). Twenty-six joints were evaluated using greyscale (GS) and power Doppler (PD) imaging. We scanned metatarsophalangeal joints (MTP) 2–5 (dorsal aspect), metacarpophalangeal joints (MCP) 2–5, proximal interphalangeal joints (PIP) 2–5 (dorsal and palmar aspects) and the wrist (radiocarpal and intercarpal joints). A single midline (longitudinal 12 o’clock position) scan perpendicular to the bone surface was used as advised by the Outcome Measures in Rheumatology (OMERACT) US working group [10]. The following PD settings were used. Colour gain was set at the disappearance of colour noise. The pulse repetition frequency was set as low as possible to have maximum sensitivity but minimising noise, which resulted in a frequency of 750 Hz. We adjusted the size and position of the colour box to include the subcutaneous tissue to recognize artefacts caused by vessels above the joint [11]. PD signals were measured only in joints with a GS score ≥ 1. The total scanning time was ½ h per patient per session. The treating rheumatologist and the research nurse were blinded to the results of the US examinations at baseline.

US evaluation

Image evaluation followed the recommendations of the Spanish Society of Rheumatology, which is a modified version of the previously developed OMERACT definitions of sonographic pathology [12]. Joints were graded according to a semi-quantitative scoring system (0–3) for both GS and PD images. For GS, all joints were graded as follows: 0 = no capsular distention; 1 = hypoechoic material only at the level of the joint margins; 2 = partial distention of the whole capsule, which appears mostly concave or flat; and 3 = complete distention of the whole capsule, which appears mostly convex. Synovial vascularisation was measured using PD and graded as follows: 0 = absent, 1 = mild single-vessel signal or isolated signal, 2 = moderate confluent vessels, and 3 = marked vessel signals in more than half of the intra-articular area [13]. US synovitis was defined as GS grade 2 or 3 and/or presence of PD (grade 1, 2 or 3).

Outcome

One-year incident IA was defined as clinical soft tissue swelling. Observed soft tissue swelling needed to be confirmed as an arthritis by the treating rheumatologist, who was unaware of the US findings.

Statistical analysis

If patients had no clinical evaluation for both their 6- and 12-month visits, they were classified as lost to follow-up and not included in the analysis. Simple descriptions were used to report baseline characteristics and the US findings. Depending on the distribution of the data, we used the independent t test or Wilcoxon-Mann-Whitney test to examine differences between cases and non-cases. Frequencies were compared using a chi-square test. Sensitivity and specificity were used to assess the diagnostic value of US for the development of IA.

After consideration of the available literature [14, 15], we identified the following variables as relevant in the association with emerging IA: demographic characteristics (age, sex), clinical characteristics (tender joint count, high positive autoantibodies [ACPA, RF], morning stiffness lasting ≥ 30 minutes) and US findings (presence of US synovitis, positive PD signal in at least one joint) [14,15,16]. These variables were tested for their association with IA using univariate logistic regression. For multivariate logistic regression, we used a backward stepwise model procedure to select the strongest predictors (p = 0.157) [17]. A p value of 0.157 is equal to the Akaike information criterion for predictors with one regression coefficient and is recommended for use in stepwise selection of predictors [18]. Missing values of independent variables were handled by multiple imputation using the STATA multiple imputation by chained equations routine (M = 20) [19]. Analysis was done using STATA 14 software (StataCorp, College Station, TX, USA).

Results

In total, 297 patients were recruited to participate. The flowchart in Fig. 1 shows the distribution of patients during follow-up. At baseline, 196 patients met the inclusion criteria. One hundred seventy-eight patients (91%) returned for their clinical evaluation at 6 months, and 159 patients (81%) had their 12-month assessment. We could determine our primary outcome for 174 patients (89%).

Fig. 1
figure 1

Flowchart showing the distribution of patients during follow-up

Full size image

In total, 31 (16%) patients had developed IA within 1 year of follow-up, of whom 15 had started DMARD therapy. Twenty-two patients had no definite diagnosis: 12 patients had mono-arthritis, and 10 patients had poly-arthritis. A definite diagnosis after 12 months was given for nine patients (RA: n = 4; psoriatic arthritis: n = 4; spondyloarthritis: n = 1). Baseline characteristics of patients with IA and non-IA patients are shown in Table 1. We found a statistically significant difference in baseline characteristics between the IA and non-IA groups for age (mean 50 vs 44 years; p = 0.005). In addition, US synovitis was found more often in patients with IA than in non-IA subjects (59% vs 32%; p = 0.007), and PD signal was present in 31% of the patients with IA vs 12% of the non-IA patients (p = 0.012).

Table 1 Baseline characteristics (n = 174)
Full size table

US findings

US findings are described in more detail in Table 2. In total, 72 patients with arthralgia (37%) had US synovitis, of whom 29 had a positive PD signal. Wrists (26%) and MTP (11%) were most commonly involved, which was also observed if only PD was taken into consideration. The distribution of US synovitis over the different joint groups between patients who developed IA and those who did not develop IA was comparable, except for the MTP, which were more involved in the IA group.

Table 2 Distribution of ultrasound findings
Full size table

Diagnostic value of US

The sensitivity and specificity of US synovitis in relation to the incidence of IA if one joint was positive on US were 59% and 68%, respectively. Positive predictive value (PPV) was 26%, and negative predictive value (NPV) was 74%. When we required two joints to be US-positive to identify an IA case, sensitivity decreased to 28% and specificity increased to 86% (PPV 27%, NPV 73%). For the presence of PD signal, sensitivity was 31% and specificity was 88% for one positive PD joint (PPV 33%, NPV 67%). When two joints were required, sensitivity decreased to 14% and specificity increased to 95% (PPV 38%, NPV 63%). If no joints were positive on US, the NPV was 89%.

Association of independent variables with development of IA

To quantify the associations between baseline characteristics and incident IA at follow-up, we performed univariate and multivariate logistic regression after multiple imputation (M = 20). Results are presented in Table 3. Age (OR 1.06, 95% CI 1.03–1.09), morning stiffness > 30 minutes (OR 2.39, 95% CI 1.20–4.73) and positive ACPA (OR 2.08, 95% CI 1.07–4.07) were associated with IA in univariate analysis. Other clinical and demographic characteristics did not differentiate patients with IA from non-IA patients. For the presence of US synovitis in at least one joint, the OR was 3.03 (95% CI 1.69–5.41), and for the presence of PD signal in at least one joint, the OR was 3.12 (95% CI 1.61–6.03). In the multivariate logistic regression analysis, age (OR 1.06, 95% CI 1.03–1.10), morning stiffness > 30 minutes (OR 2.80, 95% CI 1.33–5.90), positive ACPA (OR 2.35, 95% CI 1.13–4.87) and US synovitis (OR 2.65, 95% CI 1.44–4.88) remained associated with the development of arthritis during 1 year of follow-up. If we replaced US synovitis with the presence of PD signal (OR 3.44, 95% CI 1.71–6.95), the ORs for age and morning stiffness were similar, but positive ACPA was not associated with the development of arthritis.

Table 3 Association between baseline characteristics and development of inflammatory arthritis using univariate logistic regression analysis and multivariate logistic regression analysis after multiple imputation (n = 174)
Full size table

Discussion

Sixteen percent of patients with early arthralgia developed IA after 1 year of follow-up, of whom 59% showed US synovitis at baseline. Age, morning stiffness > 30 minutes and positive PD signal were all significantly associated with the development of IA after 1 year in a multivariate model. Regarding the value of US in the diagnostic workup of patients with early arthralgia at risk for IA, US did not perform well in ruling in IA (PPV 26%), but it did perform well in ruling out IA in patients who did not have US synovitis (NPV 89%).

Up to now, researchers in few studies had investigated subclinical synovitis in patients with arthralgia by making use of imaging modalities. In an autoantibody-positive arthralgia cohort, patients with positive US had an increased risk for IA [14, 15]. This was confirmed in our study, although only 15% of the patients were ACPA-positive, and 24% was RF-positive. In another study in which investigators evaluated patients with very early hand symptoms, the presence of PD signal was associated with IA in addition to clinical features (e.g., swollen joints) and laboratory tests (e.g., serology, RF, ACPA) [20]. For MRI, the results are not conclusive. Among a seropositive arthralgia population, changes on MRI indicative of MCP and PIP inflammation were not associated with the development of arthritis at 3-year follow-up [21]. In contrast, MRI findings in the most affected hand in patients with clinically suspect arthralgia showed that subclinical MRI inflammation preceded clinical arthritis by a few months. This was also found in a subanalysis in a seronegative arthralgia population [22, 23].

Our results should be interpreted in the light of the choices we made. As explained in the Background section above, we aimed for very early identification of IA. For this study, we restricted the population to patients with at least two painful joints as well as two criteria related to inflammation to be surer of the inflammatory component. These inclusion criteria may have driven the selection to a population at increased risk for polyarthritis. We missed those patients who might be at risk for IA but had only one painful (large) joint. However, our inclusion criteria are in line with other arthralgia cohorts and with the new EULAR guidelines regarding clinically suspect arthralgia [22, 24]. Other forms of selection may have occurred due to rheumatologists who recruited clinically suspected patients with possibly more severe symptoms [25]. In addition, 38 patients decided not to participate without giving specific reasons, which could have introduced a bias toward patients with more severe complaints. These patients did not differ in age and sex compared with the responders, but we do not know whether their clinical symptoms differed. Information bias could have occurred because some patients were lost to follow-up (14%). This was anticipated at the start of the study, so we included a telephone service if patients did not respond to their initial invitation for follow-up. If those patients did not wish to return, they were asked a small set of questions to establish whether they were at risk of IA. We saw no differences in their baseline characteristics compared with those returning to the clinic. We did not include these patients in the analysis. Other bias could have been introduced by not blinding the clinical examination and US examination, because we included only patients with arthralgia. This could have led unconsciously to less sensitive assessment of clinical and US synovitis. However, at baseline, several patients were excluded because of clinically apparent arthritis confirmed by a trained research nurse. Another item to take into account is that US is still considered operator-dependent; therefore, the US examiners scanned patients following the US study protocol as training prior to the start of the study. In addition, US examiners followed a protocol regarding acquisition and scoring. Previous research regarding inter-reliability confirmed that a consensus scoring system combined with a standardised acquisition protocol provided good inter-reliability [26, 27]. In our definition of US synovitis, we combined GS abnormalities with PD signal. Studies showed that GS abnormalities also occur in non-arthritic individuals, and especially the discriminative value of GS score 1 is debatable [14, 28]. Therefore, we used a threshold score of 2 for GS US abnormalities.

Conclusions

Sixteen percent of the patients with arthralgia developed IA after 1 year of follow-up, of whom 59% showed US synovitis at baseline. Positive PD signal, morning stiffness and age were independently associated with the development of IA after 1 year. Given the high NPV, US has added value to identify which patients would not develop into IA. Further research is recommended to confirm our results regarding the diagnostic value of US synovitis to predict the progression to IA in patients with early arthralgia.

Abbreviations

ACPA:

Anti-citrullinated protein antibody

BMI:

Body mass index

DAS28:

Disease Activity Score in 28 joints

DMARD:

Disease-modifying anti-rheumatic drug

ESR:

Erythrocyte sedimentation rate

EULAR:

European League Against Rheumatism

GS:

Greyscale

IA:

Inflammatory arthritis

MCP:

Metacarpophalangeal joint

MTP:

Metatarsophalangeal joint

MRI:

Magnetic resonance imaging

NPV:

Negative predictive value

OMERACT:

Outcome Measures in Rheumatology

PD:

Power Doppler

PIP:

Proximal interphalangeal joint

PPV:

Positive predictive value

RF:

Rheumatoid factor

SJC:

Swollen joint count

TJC:

Tender joint count

US:

Ultrasound

References

  1. Finckh A, Liang MH, van Herckenrode CM, de Pablo P. Long-term impact of early treatment on radiographic progression in rheumatoid arthritis: a meta-analysis. Arthritis Rheum. 2006;55:864–72.

    Article  PubMed  Google Scholar 

  2. Verstappen SM, McCoy MJ, Roberts C, Dale NE, Hassell AB, Symmons DP, et al. Beneficial effects of a 3-week course of intramuscular glucocorticoid injections in patients with very early inflammatory polyarthritis: results of the STIVEA trial. Ann Rheum Dis. 2010;69:503–9.

    Article  CAS  PubMed  Google Scholar 

  3. Hazes JM, Luime JJ. The epidemiology of early inflammatory arthritis. Nat Rev Rheumatol. 2011;7:381–90.

    Article  PubMed  Google Scholar 

  4. van Steenbergen HW, Huizinga TW, van der Helm-van Mil AH. The preclinical phase of rheumatoid arthritis: what is acknowledged and what needs to be assessed? Arthritis Rheum. 2013;65:2219–32.

    Article  PubMed  Google Scholar 

  5. Wakefield RJ, Freeston JE, O’Connor P, Reay N, Budgen A, Hensor EM, et al. The optimal assessment of the rheumatoid arthritis hindfoot: a comparative study of clinical examination, ultrasound and high field MRI. Ann Rheum Dis. 2008;67:1678–82.

    Article  CAS  PubMed  Google Scholar 

  6. Alves C. Early detection of patients at risk for rheumatoid arthritis: a challenge for primary and secondary care. Rotterdam, The Netherlands: Erasmus University Rotterdam; 6 Feb 2015. http://hdl.handle.net/1765/78432. Accessed 20 Nov 2015.

  7. Colebatch AN, Edwards CJ, Ostergaard M, van der Heijde D, Balint PV, D’Agostino MA, et al. EULAR recommendations for the use of imaging of the joints in the clinical management of rheumatoid arthritis. Ann Rheum Dis. 2013;72:804–14.

    Article  PubMed  Google Scholar 

  8. Geuskens GA, Burdorf A, Evers AW, Hazes JM. Clear associations between demographic and psychosocial factors and health-related quality of life in patients with early inflammatory joint complaints. J Rheumatol. 2008;35:1754–61.

    PubMed  Google Scholar 

  9. Backhaus M, Burmester GR, Gerber T, Grassi W, Machold KP, Swen WA, et al. Guidelines for musculoskeletal ultrasound in rheumatology. Ann Rheum Dis. 2001;60:641–9.

    Article  CAS  PubMed  PubMed Central  Google Scholar 

  10. Naredo E, Moller I, Moragues C, de Agustin JJ, Scheel AK, Grassi W, et al. Interobserver reliability in musculoskeletal ultrasonography: results from a “Teach the Teachers” rheumatologist course. Ann Rheum Dis. 2006;65:14–9.

    Article  CAS  PubMed  Google Scholar 

  11. Torp-Pedersen ST, Terslev L. Settings and artefacts relevant in colour/power Doppler ultrasound in rheumatology. Ann Rheum Dis. 2008;67:143–9.

    Article  CAS  PubMed  Google Scholar 

  12. Wakefield RJ, Balint PV, Szkudlarek M, Filippucci E, Backhaus M, D’Agostino MA, et al. Musculoskeletal ultrasound including definitions for ultrasonographic pathology. J Rheumatol. 2005;32:2485–7.

    PubMed  Google Scholar 

  13. Szkudlarek M, Court-Payen M, Jacobsen S, Klarlund M, Thomsen HS, Ostergaard M. Interobserver agreement in ultrasonography of the finger and toe joints in rheumatoid arthritis. Arthritis Rheum. 2003;48:955–62.

    Article  PubMed  Google Scholar 

  14. van de Stadt LA, Bos WH, Meursinge Reynders M, Wieringa H, Turkstra F, van der Laken CJ, et al. The value of ultrasonography in predicting arthritis in auto-antibody positive arthralgia patients: a prospective cohort study. Arthritis Res Ther. 2010;12:R98.

    Article  PubMed  PubMed Central  Google Scholar 

  15. Rakieh C, Nam JL, Hunt L, Hensor EM, Das S, Bissell LA, et al. Predicting the development of clinical arthritis in anti-CCP positive individuals with non-specific musculoskeletal symptoms: a prospective observational cohort study. Ann Rheum Dis. 2015;74:1659–66.

    Article  CAS  PubMed  Google Scholar 

  16. Bos WH, Wolbink GJ, Boers M, Tijhuis GJ, de Vries N, van der Horst-Bruinsma IE, et al. Arthritis development in patients with arthralgia is strongly associated with anti-citrullinated protein antibody status: a prospective cohort study. Ann Rheum Dis. 2010;69:490–4.

    Article  CAS  PubMed  Google Scholar 

  17. Harrell Jr FE, Lee KL, Mark DB. Multivariable prognostic models: issues in developing models, evaluating assumptions and adequacy, and measuring and reducing errors. Stat Med. 1996;15:361–87.

    Article  PubMed  Google Scholar 

  18. Ambler G, Brady AR, Royston P. Simplifying a prognostic model: a simulation study based on clinical data. Stat Med. 2002;21:3803–22.

    Article  PubMed  Google Scholar 

  19. van Buuren S, Boshuizen HC, Knook DL. Multiple imputation of missing blood pressure covariates in survival analysis. Stat Med. 1999;18:681–94.

    Article  PubMed  Google Scholar 

  20. Freeston JE, Wakefield RJ, Conaghan PG, Hensor EM, Stewart SP, Emery P. A diagnostic algorithm for persistence of very early inflammatory arthritis: the utility of power Doppler ultrasound when added to conventional assessment tools. Ann Rheum Dis. 2010;69:417–9.

    Article  CAS  PubMed  Google Scholar 

  21. Gent YY, Ter Wee MM, Ahmadi N, van Kuijk C, Voskuyl AE, van der Laken CJ, et al. Three-year clinical outcome following baseline magnetic resonance imaging in anti-citrullinated protein antibody-positive arthralgia patients: an exploratory study. Arthritis Rheumatol. 2014;66:2909–10.

    Article  PubMed  Google Scholar 

  22. van Steenbergen HW, Mangnus L, Reijnierse M, Huizinga TW, van der Helm-van Mil AH. Clinical factors, anticitrullinated peptide antibodies and MRI-detected subclinical inflammation in relation to progression from clinically suspect arthralgia to arthritis. Ann Rheum Dis. 2016;75:1824–30.

    Article  PubMed  Google Scholar 

  23. van Steenbergen HW, van Nies JA, Huizinga TW, Reijnierse M, van der Helm-van Mil AH. Subclinical inflammation on MRI of hand and foot of anticitrullinated peptide antibody-negative arthralgia patients at risk for rheumatoid arthritis. Arthritis Res Ther. 2014;16:R92.

    Article  PubMed  PubMed Central  Google Scholar 

  24. van Steenbergen H, Aletaha D, Beaart-van de Voorde L, Brouwer E, Codreanu C, Combe B, et al. THU0127. Development of draft criteria for arthralgia that is clinically suspect for progression to rheumatoid arthritis; results of phase 1 [poster]. Ann Rheum Dis. 2015;74 Suppl 2:240.

    Google Scholar 

  25. van Steenbergen HW, van der Helm-van Mil AH. Clinical expertise and its accuracy in differentiating arthralgia patients at risk for rheumatoid arthritis from other patients presenting with joint symptoms. Rheumatology (Oxford). 2016;55:1140–1.

    Article  Google Scholar 

  26. Wakefield RJ, D’Agostino MA, Iagnocco A, Filippucci E, Backhaus M, Scheel AK, et al. The OMERACT Ultrasound Group: status of current activities and research directions. J Rheumatol. 2007;34:848–51.

    PubMed  Google Scholar 

  27. D’Agostino MA, Conaghan PG, Naredo E, Aegerter P, Iagnocco A, Freeston JE, et al. The OMERACT Ultrasound Task Force — advances and priorities. J Rheumatol. 2009;36:1829–32.

    Article  PubMed  Google Scholar 

  28. Balsa A, de Miguel E, Castillo C, Peiteado D, Martin-Mola E. Superiority of SDAI over DAS-28 in assessment of remission in rheumatoid arthritis patients using power Doppler ultrasonography as a gold standard. Rheumatology (Oxford). 2010;49:683–90.

    Article  Google Scholar 

Download references

Acknowledgements

Not applicable.

Funding

This study was financially funded by an investigator-initiated grant from Pfizer bv.

Availability of data and materials

The dataset analysed during the present study is available from the corresponding author on reasonable request.

Author information

Authors and Affiliations

  1. Department of Rheumatology (Na609), Erasmus MC, University Medical Centre Rotterdam, PO Box 2040, 3000 CA, Rotterdam, The Netherlands

    Myrthe van der Ven, M. van der Veer-Meerkerk, D. F. Ten Cate, N. Rasappu, D. Csakvari, J. M. W. Hazes & J. J. Luime

  2. Department of Rheumatology, Zuyderland Medical Centre, Heerlen, The Netherlands

    M. van der Veer-Meerkerk

  3. Department of Rheumatology, Maasstad Hospital, Rotterdam, The Netherlands

    M. R. Kok

  4. Department of Rheumatology, Vlietland Hospital, Schiedam, The Netherlands

    A. H. Gerards

Authors
  1. Myrthe van der Ven
    View author publications

    You can also search for this author in PubMed Google Scholar

  2. M. van der Veer-Meerkerk
    View author publications

    You can also search for this author in PubMed Google Scholar

  3. D. F. Ten Cate
    View author publications

    You can also search for this author in PubMed Google Scholar

  4. N. Rasappu
    View author publications

    You can also search for this author in PubMed Google Scholar

  5. M. R. Kok
    View author publications

    You can also search for this author in PubMed Google Scholar

  6. D. Csakvari
    View author publications

    You can also search for this author in PubMed Google Scholar

  7. J. M. W. Hazes
    View author publications

    You can also search for this author in PubMed Google Scholar

  8. A. H. Gerards
    View author publications

    You can also search for this author in PubMed Google Scholar

  9. J. J. Luime
    View author publications

    You can also search for this author in PubMed Google Scholar

Contributions

MvdV carried out US examinations, analysed and interpreted the data, and drafted the manuscript. MvdVM participated in the design of the study, carried out US examinations and helped to draft the manuscript. DFTC participated in the design of the study, carried out US examinations and helped to draft the manuscript. NR helped to collect the data and draft the manuscript. MRK participated in the design of the study and helped to revise the manuscript. DC carried out US examinations and helped to draft the manuscript. JMWH helped to interpret the data and revise the manuscript. AHG participated in the design of the study and helped to revise the manuscript. JJL conceived of the study, participated in the design of the study, helped to interpret the data and revised the manuscript. All authors read and approved the final manuscript.

Corresponding author

Correspondence to Myrthe van der Ven.

Ethics declarations

Ethics approval and consent to participate

Written informed consent was obtained from the participants according to the Declaration of Helsinki. The study was approved by the medical ethics committee of Erasmus MC, University Medical Centre Rotterdam, Rotterdam, The Netherlands (MEC-2010-353) and was assessed for feasibility by the local ethical bodies of Maasstad Hospital and Vlietland Hospital.

Consent for publication

Not applicable.

Competing interests

The authors declare that they have no competing interests.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Rights and permissions

Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

Reprints and permissions

About this article

Check for updates. Verify currency and authenticity via CrossMark

Cite this article

van der Ven, M., van der Veer-Meerkerk, M., Ten Cate, D.F. et al. Absence of ultrasound inflammation in patients presenting with arthralgia rules out the development of arthritis. Arthritis Res Ther 19, 202 (2017). https://doi.org/10.1186/s13075-017-1405-y

Download citation

  • Received:

  • Accepted:

  • Published:

  • DOI: https://doi.org/10.1186/s13075-017-1405-y

Keywords

Arthritis Research & Therapy

ISSN: 1478-6362

Contact us