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系统性红斑狼疮患者低疾病活动度时的内皮功能障碍:通过定量和鉴定循环内皮微颗粒评估,抗内皮细胞抗体的作用。

Endothelial dysfunction in systemic lupus patients with low disease activity: evaluation by quantification and characterization of circulating endothelial microparticles, role of anti-endothelial cell antibodies.

机构信息

AP-HP, Internal Medicine Department, Hôpital Européen Georges Pompidou, France.

出版信息

Rheumatology (Oxford). 2010 Jun;49(6):1049-55. doi: 10.1093/rheumatology/keq041. Epub 2010 Mar 7.

DOI:10.1093/rheumatology/keq041
PMID:20211868
Abstract

OBJECTIVE

We attempted to evaluate endothelial dysfunction and the role of AECAs in systemic lupus (SL) with low disease activity. We quantified endothelial microparticles (EMps) and attempted to find the best flow cytometry method for that purpose.

METHODS

CD105, CD144 and CD146 were tested, individually or in combination, on EMp-enriched plasma. Twenty-three healthy blood donors and 27 SL patients were evaluated. SL patients with a SLEDAI <10 (median 2.6) were evaluated in our outpatient clinic. For each patient, EMps (CD105-CD146(+), CD45(-)) and AECAs were quantified and characterized.

RESULTS

The monochrome composite marker CD105-CD146 appeared to be the most efficient in detecting EMps. SL patients had more circulating EMps than healthy donors: respective median values were 2575 and 130 EMps/microl (P < 0.001). SL patients had more CD54(+) and CD54(-) EMps than healthy donors (496 vs 34 EMps CD54(+)/microl, P < 0.0001; 1875 vs 89 EMps CD54(-)/microl, P < 0.0001). The ratio CD54(+) EMps/total EMps was lower for lupus patients than for healthy individuals (20.3 vs 33.7%, P = 0.03). Twenty-four patients (89%) were positive for AECAs. EMp counts were not significantly higher for patients with AECAs.

CONCLUSION

Monochrome composite marker is efficient in detecting the whole population of EMps using flow cytometry. SL patients with low disease activity have a marked endothelial dysfunction. EMps released from the endothelium originate from activated and non-activated cells. AECAs do not seem to be the main cause of endothelial dysfunction in this population.

摘要

目的

我们试图评估低疾病活动度的系统性红斑狼疮(SLE)中的内皮功能障碍和 AECA 的作用。我们量化了内皮细胞微颗粒(EMps),并尝试找到为此目的的最佳流式细胞术方法。

方法

单独或组合测试了 CD105、CD144 和 CD146 在富含 EMp 的血浆上的表达。评估了 23 名健康献血者和 27 名 SLE 患者。在我们的门诊诊所评估了 SLEDAI<10(中位数 2.6)的 SLE 患者。为每位患者定量和表征 EMps(CD105-CD146(+),CD45(-))和 AECA。

结果

单色复合标志物 CD105-CD146 似乎是检测 EMps 的最有效方法。SLE 患者的循环 EMps 多于健康供体:分别的中位数分别为 2575 和 130 EMps/microl(P<0.001)。SLE 患者的 CD54(+)和 CD54(-) EMps 多于健康供体(496 与 34 EMps CD54(+)/microl,P<0.0001;1875 与 89 EMps CD54(-)/microl,P<0.0001)。狼疮患者的 CD54(+) EMps/总 EMps 比值低于健康个体(20.3 与 33.7%,P=0.03)。24 名患者(89%)为 AECA 阳性。AECA 阳性患者的 EMp 计数没有显著升高。

结论

单色复合标志物使用流式细胞术高效地检测到整个 EMps 群体。低疾病活动度的 SLE 患者存在明显的内皮功能障碍。从内皮细胞释放的 EMps 来自激活和非激活的细胞。AECA 似乎不是该人群中内皮功能障碍的主要原因。

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