Cartilage collagen neoepitope C2C in urine as an integrative diagnostic marker for early knee osteoarthritis

Abstract Objective To investigate the suitability of urinary collagen type-II C-terminal cleavage neoepitope (uC2C) as a marker for early knee osteoarthritis (kOA). Design We examined 302 Estonian subjects (mean age, 49 years): 186 subjects with and 20 control subjects without knee symptoms, and 96 patients treated by arthroscopy. For the latter, cartilage lesions were characterized using Societe Francaise d'Arthroscopie (SFA) scores. Standardized radiographs of bilateral tibiofemoral (TF) and patellofemoral (PF) joints were assessed for osteoarthritis (OA) features. Osteophytes (Ophs) and joint space narrowing (JSN) were graded separately. uC2C was measured by the uC2C-HUSA assay. Logistic and linear regression models were used for data analysis. Results Of the kOA cases, 50% were isolated (TF or PF) grade 1; 10% were grade 2. JSN with Ophs was more frequent in females than in males (52% vs. 34%, p = 0.01). Increased uC2C level was associated with gradual increase in the risk of kOA grade of severity (odds ratio = 2.14–3.7) including grade 1 vs. 0. TF-OA and PF-OA equally predicted uC2C concentration (R2 = 0.33–0.35). uC2C prediction was better for females than for males (R2 = 0.42 vs. 0.22 by TF-OA). The best predictive model for uC2C level (R2 = 0.75) included three OA features: macroscopic cartilage lesions, TF Ophs, and PF-JSN. Conclusions uC2C as an integrative marker of kOA is associated with cartilage degradation and Oph formation in the PF- and TF-joints. Increased uC2C concentration could be used as an early diagnostic marker for kOA in clinical studies.