Endotrophin, an extracellular hormone, in combination with neoepitope markers of von Willebrand factor improves prediction of mortality in the ECLIPSE COPD cohort

The study design of Evaluation of COPD Longitudinally to Identify Predictive Surrogate End-points (ECLIPSE) (clinicaltrials.​gov identifier NCT00292552; GSK study code SCO104960) has been fully described previously [15]. The current analysis was based on a three-year clinical follow-up and performed on a subpopulation of the full ECLIPSE study of 1000 COPD consisting of the 500 patients progressing the most and the 500 patients progressing the least as defined as FEV₁ decline. For the present post hoc analysis, we used clinical and biomarker data from 898 patients obtained at month six, year one, and year three. The study complied with the declaration of Helsinki and good clinical practice guidelines and was approved by the relevant ethics and review boards. All participants provided informed consent.

Serum and heparin plasma samples were prepared from participants in the fasting state and stored at − 80 °C until analyzed. PRO-C6 was measured in month six serum samples while VWF-A and VWF-N were measured in year one plasma samples. Competitive ELISAs, utilizing monoclonal antibodies recognizing specific neo-epitopes, were used to assess endotrophin/type VI collagen formation (PRO-C6), VWF formation/ endothelial release (VWF-N), and activated VWF (VWF-A) [16, 17] (Nordic Bioscience A/S, Herlev, Denmark). Measurements were performed previously in a blinded manner, according to the manufacturer’s instructions [18, 19].

Baseline characteristics for survivors and deceased are listed in Table 1. The survivors are significantly younger, have a lower modified medical research council (mMRC) score, more are currently smoking, but their smoking pack-years history is lower.

PRO-C6, VWF-A, and VWF-N have already been shown to be independent predictors of all-cause mortality [18, 19]. To investigate if PRO-C6 combined with biomarkers of VWF processing could provide additional prognostic value, we multiplied the biomarkers. Data were dichotomized by a ROC analysis based on mortality data. The ROC curve for PRO-C6 multiplied by VWF-A (PRO-C6*VWF-A) had an area under the curve (AUC) of 0.735 (p < 0.0001) and provided a cut-off 116.5ng²/mL² for the identification of participants who died during the total follow-up time with a sensitivity of 55.6 and a specificity of 88.3 (data not shown). The ROC for PRO-C6 multiplied with VWF-N (PRO-C6*VWF-N) had an AUC of 0.788 (p < 0.0001) with the cut-off 50.7 ng²/mL² for identification of subjects who died. This curve had a sensitivity of 81.5 and specificity of 76 (data not shown). Based on the ROC analyses, data were dichotomized and analyzed by the Kaplan-Meier survival curves (Fig. 1). Kaplan-Meier survival analysis and hazard ratios evaluated the prognostic value of biomarkers alone or in combination for all-cause mortality after 3 years. Previously it was shown that high levels of PRO-C6, VWF-A, and VWF-N were associated with a higher risk of mortality with hazard ratios of 5.6 (95% CI 2.4–13.1), 4.6 (95% CI 2.2–9.6) and 3.7 (95% CI 1.8–7.6), respectively [18, 19]. These values were significantly increased when combining PRO-C6 with the VWF processing biomarkers VWF-A 8.8 (2.8–27.7) or VWF-N to hazard ratios of 8.8 (95% CI 2.8–27.7) and 13.3 (95% CI 5.6–32.0), respectively. The hazard ratios are displayed in Fig. 2 for the single biomarkers and composite biomarkers. All hazard ratios were tested for cofounders and were found to be independent predictors of all-cause mortality (data not shown).