Abstract

Subclinical synovitis occur long before clinical haemophilic arthropathy (HA). New biomarkers are needed for early detection of HA. To compare the levels of tissue inhibitors of metalloproteinase-1 (TIMP-1) and vascular endothelial growth factor (VEGF)in severe haemophilia A boys on prophylaxis and on-demand therapy to healthy boys and correlate them with the haemophilia joint health score (HJHS) & the Denver magnetic resonance imaging (MRI) scale; hence, determine their values in early detection of HA. Haemophilia joint health score, serum TIMP-1, VEGF and Denver MRI score were assessed in 50 boys with severe haemophilia A (31 on prophylactic factor VIII therapy (62%) with a dose of 15IU/kg/twice weekly) and 50 age-matched healthy boys. Boys with severe haemophilia A had significantly higher TIMP-1 240ng/mL, SD200-350 (P<.001) and VEGF 600pg/mL, SD400-1100 (P<.001). Their mean HJHS was 4.5±3.0 (0-11) and their mean Denver MRI score was 5.55±1.6 (2.00-8.00). A significant positive correlation was found between TIMP-1 and VEGF (P<.001), BMI Z-score (P=.029), HJHS (P=.041)and total MRI score (<.001). Significant correlations were found between VEGF and age (P<.001), HJHS (P=.003) and total MRI score (P<.001). Boys with severe haemophilia A on prophylaxis therapy had significantly lower HJHS (P=.021), VEGF (P<.001), TIMP-1 (P=.002) and total MRI score (P=.021) than those on on-demand therapy. Receiver operating characteristic curve, defined a cut-off value of 160ng/mL for TIMP-1 with a sensitivity of 90% and specificity of 60% and that of 350pg/mL for VEGF with a sensitivity of 78% and specificity of 88% for discrimination between severe haemophilia A and healthy boys. Vascular endothelial growth factor and TIMP-1 can be used for early detection of HA. Further prospective studies should include larger study populations. In addition, studies should address the role of various anti-VEGFs as potential therapy for HA and their impact on prevention and treatment of HA.

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