4.5 Article

Complement activation in patients with immune thrombocytopenic purpura according to phases of disease course

Journal

CLINICAL AND EXPERIMENTAL IMMUNOLOGY
Volume 201, Issue 3, Pages 258-265

Publisher

WILEY
DOI: 10.1111/cei.13475

Keywords

Anti-platelet antibody; C1q; complement system; immunoglobulin; ITP; sC5b-9; thrombocytopenia

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Immune thrombocytopenic purpura (ITP) is an autoimmune thrombocytopenia with shortened platelet survival and relative bone marrow failure. The pathogenesis involves antibody production, cytokine release, T cell impairment, complement activation and clearance of platelets. We measured plasma levels of C3, C4, C1q and sC5b-9 in 80 ITP patients in acute phase, 50 ITP patients in complete (CR) or partial (PR) remission and 50 age- and sex-matched healthy volunteers. Statistical analyses showed that acute ITP patients had higher plasma levels of sC5b-9 and C1q than CR or PR patients (median = sC5b-9: 200 versus 98 mg/dl,P-value < 0 center dot 001) (median C1q = 2 center dot 11versus1 center dot 00 mg/dl,P-value < 0 center dot 001). CR and PR ITP patients had sC5b-9 and C1q plasma levels comparable to those observed in healthy volunteers. There was a significant correlation between sC5b-9 and C1q plasma levels (Spearman's rho correlation index on 130 ITP patients equal to 0 center dot 58,P-value < 0 center dot 001). We also found that sC5b-9 plasma level is inversely correlated with the number of platelets. Furthermore, we divided acute ITP patients into subjects with detectable (24 of 80, 30%) or undetectable (56 of 80, 70%) anti-platelet antibodies; patients with detectable anti-platelet antibodies have significantly higher plasma levels of C1q and sC5b-9. This research will potentially offer novel therapeutic strategies in light of new drugs affecting complement activation for monitoring therapy response.

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