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首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Differences of soluble CD40L in sera and plasma: Implications on CD40L assay as a marker of thrombotic risk.
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Differences of soluble CD40L in sera and plasma: Implications on CD40L assay as a marker of thrombotic risk.

机译:血清和血浆中可溶性CD40L的差异:作为血栓风险标志物的CD40L分析的意义。

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Introduction: Soluble CD40L (sCD40L) ELISA has emerged as a promising predictor of poor outcomes in acute coronary syndrome. Yet many blood processing techniques have been used with little consideration of their effect on the results. Methods: We measured sCD40L by ELISA in 10 patients with thrombocytopenia and 12 with normal or high platelet counts and 8 healthy controls using three sampling techniques: serum clotted on ice (serum-I) or at room temperature (serum-RT) and platelet poor plasma (PPP). Results: Serum-RT samples, compared to serum-I, gave significantly higher CD40L values (p=0.003), demonstrating that ex vivo sCD40L release by activated platelets is inhibited by cold temperature. Although serum-I and PPP were comparable in patients with normal platelet counts, serum-I gave significantly higher values than PPP in the thrombocytosis group (p=0.01), suggesting that cold inhibition is insufficient in the latter group. To estimate the fraction of sCD40L that was microparticle-bound CD40L (mp-CD40L), 16 samples underwent 0.1-microm filtration. 50.6% of sCD40L was mp-CD40L in serum-RT, whereas 21.3% and 29.9% were observed in serum-I and PPP, respectively. Lastly, plasma sCD40L was assayed in 46 patients with and 35 without thrombosis. Plasma sCD40L did not correlate with platelet count in non-thrombotic, non-inflammatory patients but did (p<0.01) in those with thrombosis. Conclusions: Sample processing and temperature profoundly affect sCD40L assay. Serum-I and PPP minimize the release of sCD40L ex vivo and better represent sCD40L in vivo. However, PPP may be preferable particularly in patients with thrombocytosis. The existence of mp-CD40L highlights the importance of centrifuge conditions.
机译:简介:可溶性CD40L(sCD40L)ELISA已成为急性冠脉综合征预后不良的有希望的预测指标。然而,已经使用了许多血液处理技术,而很少考虑其对结果的影响。方法:我们采用三种采样技术,通过ELISA在10例血小板减少症患者和12例血小板计数正常或较高的患者以及12例健康对照的sCD40L中使用三种采样技术:冰凝结的血清(血清I)或室温(血清RT)和血小板贫血等离子(PPP)。结果:与血清I相比,血清RT样品的CD40L值明显更高(p = 0.003),表明活化的血小板离体sCD40L的释放受到低温的抑制。尽管血小板计数正常的患者血清I和PPP具有可比性,但血小板增多症患者血清I的值明显高于PPP(p = 0.01),这表明后者的冷抑制作用不足。为了估计与微粒结合的CD40L(mp-CD40L)的sCD40L的比例,对16个样品进行了0.1微米的过滤。血清RT中sCD40L的50.6%是mp-CD40L,而血清I和PPP中分别观察到21.3%和29.9%。最后,在46例有血栓形成的患者和35例无血栓形成的患者中检测了血浆sCD40L。在非血栓性,非炎性患者中,血浆sCD40L与血小板计数无关,而在血栓形成性患者中,血浆sCD40L与血小板计数无关(p <0.01)。结论:样品处理和温度深刻影响sCD40L测定。血清-I和PPP使sCD40L的离体释放最小化,并更好地代表sCD40L在体内。但是,PPP可能尤其适用于血小板增多症患者。 mp-CD40L的存在凸显了离心条件的重要性。

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