Buhimschi Catalin S, Norwitz Errol R, Funai Edmund, Richman Susan, Guller Seth, Lockwood Charles J, Buhimschi Irina A
Department of Obstetrics, Gynecology and Reproductive Science, Yale University, New Haven, CT 06520, USA.
Am J Obstet Gynecol. 2005 Mar;192(3):734-41. doi: 10.1016/j.ajog.2004.12.052.
Serum levels of soluble fms-like tyrosine kinase 1 (sFlt-1), vascular endothelial growth factor (VEGF), and placental growth factor (PlGF) are altered in women with clinical preeclampsia. We sought to identify whether similar alterations in urinary levels of these proteins cluster hypertensive disorders in pregnancy, and identify women with severe preeclampsia (sPE).
Free urinary levels of sFlt-1, VEGF, and PlGF were measured by immunoassay in 68 women enrolled prospectively in the following groups: nonpregnant reproductive age (NP-CTR n = 14), healthy pregnant control (P-CTR n = 16), pregnant hypertensive and proteinuric women who did not meet criteria for severe preeclampsia (pHTN n = 21), and women with sPE (n = 17).
There was no difference in gestational age at the time of enrollment among groups (median [range]: sPE: 31 [24-40], pHTN: 34 [16-40], P-CTR: 28 [7-39] wks). Urinary excretion of VEGF was significantly increased in sPE women compared with NP-CTR (P = .023), but did not differ among pregnant groups. Urinary PlGF levels were significantly increased in pregnant compared with nonpregnant women, but were decreased in all hypertensive women compared with healthy P-CTR (P < .001). Urinary sFlt-1 concentrations were significantly increased in women with sPE relative to all other groups (P < .001). pHTN women had higher sFlt-1 urinary output compared with P-CTR group (P = .001). A cutoff >2.1 in the ratio log [sFlt-1/PlGF] had 88.2% sensitivity and 100% specificity in differentiating women with sPE from normotensive controls. We also described that the log[sFlt-1/PlGF] ratio identified women with sPE better than proteinuria alone (P = .03). Our regression model revealed that uric acid correlated best with log[sFlt-1/PlGF] ratio (r = 0.628; P = .005).
sPE is associated with increased urinary output of the antiangiogenic factor sFlt-1 and a decreased output of PlGF at the time of clinical manifestation, providing a rapid noninvasive screening of hypertensive women based on a sFlt/PlGF ratio. This ratio may be used as representation for severity of the disease, and appears to be superior to random urinary protein measurements.
临床子痫前期女性的血清可溶性fms样酪氨酸激酶1(sFlt-1)、血管内皮生长因子(VEGF)和胎盘生长因子(PlGF)水平会发生改变。我们试图确定这些蛋白质的尿水平的类似改变是否会将妊娠期高血压疾病聚类,并识别出重度子痫前期(sPE)女性。
通过免疫测定法测量了前瞻性纳入以下组别的68名女性的尿中游离sFlt-1、VEGF和PlGF水平:非孕生育年龄组(NP-CTR,n = 14)、健康妊娠对照组(P-CTR,n = 16)、未达到重度子痫前期标准的妊娠高血压和蛋白尿女性(pHTN,n = 21)以及sPE女性(n = 17)。
各组入组时的孕周无差异(中位数[范围]:sPE:31[24 - 40],pHTN:34[16 - 40],P-CTR:28[7 - 39]周)。与NP-CTR相比,sPE女性的VEGF尿排泄量显著增加(P = 0.023),但妊娠组之间无差异。与非妊娠女性相比,妊娠女性的尿PlGF水平显著增加,但与健康P-CTR相比,所有高血压女性的尿PlGF水平均降低(P < 0.001)。相对于所有其他组,sPE女性的尿sFlt-1浓度显著增加(P < 0.001)。与P-CTR组相比,pHTN女性的尿sFlt-1排泄量更高(P = 0.001)。log[sFlt-1/PlGF]比值>2.1在区分sPE女性与血压正常对照组时具有88.2%的敏感性和100%的特异性。我们还描述了log[sFlt-1/PlGF]比值在识别sPE女性方面比单独的蛋白尿更好(P = 0.03)。我们的回归模型显示尿酸与log[sFlt-1/PlGF]比值相关性最好(r = 0.628;P = 0.005)。
sPE与抗血管生成因子sFlt-1的尿排泄量增加以及临床表现时PlGF的排泄量减少有关,基于sFlt/PlGF比值为高血压女性提供了一种快速无创的筛查方法。该比值可作为疾病严重程度的指标,并且似乎优于随机尿蛋白测量。
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