Risk assessment for prolonged sickness absence due to musculoskeletal disorders: protocol for a prospective cohort study

The primary outcomes in the present study will be sickness absence and costs related to health care and sickness absence. Sickness absence will be operationalized in different ways and includes 1) total number of absence days during 6- and 12-month follow-up adjusted for percentage of work and percentage of sickness absence, 2) the time until full sustainable RTW, i.e. at least 4 weeks without relapse during 12-months follow-up, and 3) probability of working (i.e. not receiving medical benefits) each month during 12 months of follow-up, measured as repeated events, and 4) proportion of people with sustainable RTW (at least 4 weeks) at 6 and 12 months. Data on sickness absence will be collected from the NAV registry, containing dates and grading of sickness absence as well as the diagnostic codes related to the absence. The use of health care will be collected from public registries including the Norwegian Patient Registry (NPR), the Municipal Patient and User Registry (KPR), and the Control and Payment of Health Refunds (KUHR). Periods of sickness absence and use of health care will be collected 12 months before inclusion and 6 and 12 months after inclusion in the study (Table 1).

Secondary outcomes will be musculoskeletal health status, health-related quality of life, productivity loss (Table 1). Musculoskeletal health will be measured with the Musculoskeletal health questionnaire (MSK-HQ), which is developed to capture musculoskeletal health status through 15 questions embracing a broad range of musculoskeletal disorders [18]. The first 14 questions are scored on a 0–4-point scale and summed up to a score between 0 and 56 points, with a higher score indicating better musculoskeletal health status. Health-related quality of life will be measured with the EuroQol 5 Dimensions (EQ-5D-5 L) [21], which covers five domains: mobility, self-care, activities of daily living, pain/discomfort, and anxiety/depression. The EQ-5D-5 L is scored on a 5-point scale from 1 (no problems) to 5 (extreme problems). Responses can be transformed into an index value ranging from − 0.59 to 1, where − 0.59 represents worst possible state and 1 represents perfect health. The EQ-5D Visual Analogue Scale (VAS) is also included as a measure of health-related quality of life and consists of a single question asking about the respondent’s self-rated health on a vertical 0 to 100 VAS, with 100 indicating best health. Productivity loss will be measured with The institute of Medical Technology Assessment Productivity Cost Questionnaire (iPCQ), which is used to measure and value health-related productivity loss for both paid and unpaid work. The instrument is found to be suitable for measuring absenteeism from paid work and productivity loss related to unpaid labor [20].

Measurement properties of the translated questionnaires will be evaluated based on the COnsensus-based Standards for the selection of health Measurement INstruments (COSMIN) guidelines [28, 29]. Construct validity of the Keele STarT MSK and the MSK-HQ will be assessed by testing a priori hypotheses about the relationship with the same and other constructs. For acceptable construct validity, 75% of the hypotheses need to be confirmed. Reliability will be assessed with intraclass correlation coefficient (ICC) using two-way random, average agreement, and smallest detectable change (SDC_95%) [28]. Criterion validity of self-reported productivity loss (by iPCQ) compared to registered sickness absence will be assessed by Cohen’s unweighted Kappa for dichotomous variables of the iPCQ and by ICC for the index score of absenteeism. According to COSMIN, acceptable level of ICC is > 0.70 [28]. The Kappa values are according to Altman judged as follows: poor (0 to 0.2), fair (0.21 to 0.40), moderate (0.41 to 0.60), good (0.61 to 0.80) and very good (0.81 to 1.00) [30].

The predictive ability of the Keele STarT MSK, the ÖMPSQ-SF and other established risk factors for long-term sickness absence for detecting people at risk of prolonged sickness absence at 6 and 12 months will be compared by using multivariate logistic analysis. These analyses will be adjusted for age and sex, and duration of sick leave. The optimal cut-off value for the Keele STarT MSK and ÖMPSQ-SF tools in detecting people at high risk of prolonged sickness absence at 6 and 12 months will be determined using Receiver Operating Curve (ROC) analyses. In addition, values for sensitivity, specificity, positive and negative predictive value of RTW at 6 and 12 months will be compared using the optimal cut-off values.

A prognostic model for the risk of prolonged sickness absence, assessing risk factors listed in Table 1, will be developed according to the PROGRESS framework using multiple linear and logistic regression. The model will be externally validated in other materials in Norway, e.g. the work package 3 of the MI-NAV project and a similar project in Trondheim [31].

Multivariate logistic regression analysis will also be used to assess predictors for health care costs, and to assess if these vary across different risk profile groups.

Finally, latent class modelling will be used in order to explore if clusters of people on sick leave due to musculoskeletal disorders with regard to work-related disability and sickness absence trajectories, can be identified [32].

Separate statistical analysis plans will be developed before the data collection is finished and the database is locked. A biostatistician will contribute in the statistical analyses.