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首页> 外文期刊>Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology >Complement activation in patients with immune thrombocytopenic purpura according to phases of disease course
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Complement activation in patients with immune thrombocytopenic purpura according to phases of disease course

机译:根据疾病课程阶段的免疫血小板减薄紫癜患者的补体激活

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摘要

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.
机译:免疫血小板减少紫癜(ITP)是一种自身免疫性血小板减少症,血小板存活缩短和相对骨髓衰竭。该发病机制涉及抗体产生,细胞因子释放,T细胞损伤,补体激活和血小板的间隙。我们在80个ITP患者中测量了C3,C4,C1Q和SC5B-9的血浆水平,完全(CR)或部分(PR)缓解和50岁和性别匹配的健康志愿者。统计学分析表明,急性ITP患者的SC5B-9和C1Q的血浆水平高于Cr或PR患者(中位数= SC5B-9:200与98mg / DL,P值<0中心点001)(中位C1Q = 2中心点11Versus1中心点00 mg / dl,p值<0中心点001)。 CR和PR ITP患者的SC5B-9和C1Q等离子水平与健康志愿者观察到的人相当。 SC5B-9和C1Q等离子体水平之间存在显着相关性(Spearman的RHO相关指数在130 ITP患者等于0中心点58,P值<0中心点001)。我们还发现SC5B-9等离子体水平与血小板数量相反。此外,我们将急性ITP患者分为可检测的(24个,30%,30%)或未检测到的受试者(80,70%,70%)的抗血小板抗体;可检测的抗血小板抗体的患者具有显着更高的C1Q和SC5B-9的血浆水平。本研究将鉴于影响互补激活的新药,潜在提供新的治疗策略,用于监测治疗响应。

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