Department of Obstetrics, Gynecology and Reproductive Science, Yale University, New Haven, CT 06520, USA.
BJOG. 2010 Feb;117(3):321-30. doi: 10.1111/j.1471-0528.2009.02434.x. Epub 2009 Nov 26.
Endoglin, an anti-angiogenic glycoprotein expressed on endothelial cells, has been proposed recently as a biomarker of pre-eclampsia (PE). Given that PE is characterised by an imbalance of angiogenic factors, we sought to determine the clinical utility of urinary soluble endoglin, relative to the soluble fms-like tyrosine kinase 1 to placental growth factor (PlGF) ratio, in the diagnosis of PE during gestation.
Prospective observational cohort.
Tertiary referral university hospital.
Two hundred and thirty-four pregnant women were enrolled prospectively in the following groups: healthy controls, n = 63; gestational age (GA), median (interquartile range), 33 weeks (27-39 weeks); chronic hypertension, n = 27; GA, 33 weeks (30-36 weeks); mild PE, n = 38; GA, 37 weeks (34-40 weeks); severe PE, n = 106; GA, 32 weeks (29-37 weeks).
Free urinary levels of soluble endoglin, soluble fms-like tyrosine kinase 1 and PlGF were measured by sensitive and specific immunoassay. Levels for all urinary analytes were normalised to creatinine.
Urinary soluble endoglin, and the soluble fms-like tyrosine kinase 1 to PlGF ratio.
In healthy controls, urinary soluble endoglin levels were increased significantly at term relative to those earlier in gestation. Severe PE was characterised by an increased urinary level of soluble endoglin, soluble fms-like tyrosine kinase 1, protein to creatinine ratio and soluble fms-like tyrosine kinase 1 to PlGF ratio compared with all other groups. There was a direct correlation between urinary soluble endoglin and proteinuria that remained after GA correction (R = 0.382, P < 0.001). Urinary soluble endoglin could not differentiate mild PE from severe preterm PE. Overall, soluble endoglin had the ability to discriminate PE from chronic hypertension and healthy controls only in women who were evaluated at <37 weeks of GA. The sensitivity, specificity and accuracy of urinary soluble endoglin alone in the diagnosis of PE or in the identification of women with PE requiring a mandated delivery before 37 weeks of gestation were 70%, 86% and 76%, respectively. These values were inferior to those of the soluble fms-like tyrosine kinase 1 to PlGF ratio (P < 0.001). The addition of urinary soluble endoglin did not improve the diagnostic accuracy of the soluble fms-like tyrosine kinase 1 to PlGF ratio alone.
We have provided evidence that soluble endoglin is present and elevated in the urine of women who develop preterm PE. Urinary soluble endoglin has only limited ability to determine the severity of PE and to distinguish between PE and chronic hypertension both preterm and at term. Compared with urinary soluble endoglin, the soluble fms-like tyrosine kinase 1 to PlGF ratio remains a better marker of disease presence, severity and outcome.
内皮细胞表达的抗血管生成糖蛋白内胚琳(endoglin)最近被提出作为先兆子痫(PE)的生物标志物。鉴于 PE 的特征是血管生成因子失衡,我们试图确定尿可溶性内胚琳相对于可溶性 fms 样酪氨酸激酶 1 至胎盘生长因子(PlGF)比值在妊娠期诊断 PE 的临床效用。
前瞻性观察队列。
三级转诊大学医院。
234 名孕妇前瞻性纳入以下组:健康对照组,n = 63;孕龄(GA)中位数(四分位数范围),33 周(27-39 周);慢性高血压,n = 27;GA,33 周(30-36 周);轻度 PE,n = 38;GA,37 周(34-40 周);重度 PE,n = 106;GA,32 周(29-37 周)。
通过敏感和特异性免疫测定法测量游离尿可溶性内胚琳、可溶性 fms 样酪氨酸激酶 1 和 PlGF 的水平。所有尿分析物的水平均用肌酐归一化。
尿可溶性内胚琳和可溶性 fms 样酪氨酸激酶 1 至 PlGF 比值。
在健康对照组中,与妊娠早期相比,足月时尿可溶性内胚琳水平显著升高。与所有其他组相比,重度 PE 特征为尿可溶性内胚琳、可溶性 fms 样酪氨酸激酶 1、蛋白与肌酐比和可溶性 fms 样酪氨酸激酶 1 至 PlGF 比值升高。尿可溶性内胚琳与蛋白尿之间存在直接相关性,即使在 GA 校正后仍然存在(R = 0.382,P < 0.001)。尿可溶性内胚琳不能区分轻度 PE 与严重早产 PE。总体而言,可溶性内胚琳仅在 GA <37 周评估的女性中具有将 PE 与慢性高血压和健康对照组区分开来的能力。单独使用尿可溶性内胚琳诊断 PE 或识别需要在 37 周前强制分娩的 PE 女性的敏感性、特异性和准确性分别为 70%、86%和 76%。这些值低于可溶性 fms 样酪氨酸激酶 1 至 PlGF 比值(P < 0.001)。添加尿可溶性内胚琳并不能提高可溶性 fms 样酪氨酸激酶 1 至 PlGF 比值的诊断准确性。
我们提供的证据表明,早产 PE 妇女的尿液中存在并升高了可溶性内胚琳。尿可溶性内胚琳只能有限地确定 PE 的严重程度,并区分早产和足月时的 PE 和慢性高血压。与尿可溶性内胚琳相比,可溶性 fms 样酪氨酸激酶 1 至 PlGF 比值仍然是疾病存在、严重程度和结局的更好标志物。
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