NO TREATMENT EFFECTS OF ORAL GLUCOSAMINE FOR SUBGROUPS OF KNEE AND HIP OSTEOARTHRITIS PATIENTS; AN INDIVIDUAL PATIENT DATA META-ANALYSIS FROM THE OA TRIAL BANK

Abstract

Background The effectiveness of oral glucosamine for symptoms of osteoarthritis (OA) is debated. Individual trials are not powered to show effects within subgroups of patients.

Objectives To evaluate the effectiveness of oral glucosamine in clinical relevant subgroups of hip and knee OA patients based on pain severity, BMI, sex, structural abnormalities and inflammation, using individual patient data from published trials.

Methods A systematic search for published randomized controlled trials on the effectiveness of any oral glucosamine substance in patients with clinically or radiologically defined knee or hip OA was performed. Additionally, trail registries were searched for ongoing studies. All authors and institutions of all eligible studies were approached and asked to share the trial data. All shared trials were assessed for their risk of bias, using the criteria recommended by the Cochrane. Missing data for covariates and outcome measures were imputed, using multiple imputation methods, within each original study. Subgroup factors were dichotomized, based on consensus of the OA Trial Bank Steering Committee. A multilevel regression analysis was performed to estimate the magnitude of the effect of glucosamine over the control intervention in the different subgroups with the individuals nested within each study. Pain at short-term (3 months) and long-term (24 months) served as primary outcomes measure, function as secondary. Outcome measures measured on different scales were standardized to a 0–100 scale to pool the data. All analyses were performed with and without stratifying for affected joint and type of glucosamine substance.

Results Out of 21 eligible studies, six studies (N=1663) shared their trial data with the OA Trial Bank. Only one of these studies (N=40) was industry driven. All six studies had a low risk of bias, of which five trials (all not industry driven) compared glucosamine to placebo. These five studies represented 50% of the total number of randomized subjects in all published trials for this comparison. No main effects of glucosamine were found on pain or function at short-term (mean difference 0.31 95% CI [-2.02 to 2.64] and 1.56 [-0.56 to 3.69], respectively) and at long-term follow-up (0.98 [-1.76 to 3.73] and 1.40 [-1.27 to 4.06], respectively). Also, no significant interactions with treatment were found for subgroups based on pain severity (WOMAC pain <70 vs. ≥70), BMI (<27 kg/m2 vs. ≥27kg/m2), sex (male vs. female) and structural abnormalities (KL-grade 0–2 vs. 3–4), see Table. Stratification for knee OA patients only and for type of glucosamine did not result in any differences in the outcomes. No data was available to adequately form subgroups based on degree of inflammation.