Santillan Mark K, Santillan Donna A, Scroggins Sabrina M, Min James Y, Sandgren Jeremy A, Pearson Nicole A, Leslie Kimberly K, Hunter Stephen K, Zamba Gideon K D, Gibson-Corley Katherine N, Grobe Justin L
From the Departments of Obstetrics and Gynecology (M.K.S., D.A.S., S.M.S., K.K.L., S.K.H.), Pharmacology (J.Y.M., J.A.S., N.A.P., J.L.G.), Biostatistics (G.K.D.Z.), and Pathology (K.N.G.-C.), The François M. Abboud Cardiovascular Research Center (M.K.S., J.L.G.), The Obesity Research and Education Initiative (M.K.S., J.L.G.), The Fraternal Order of Eagles' Diabetes Research Center (J.L.G.), and The Center for Hypertension Research (M.K.S., J.L.G.). University of Iowa, Iowa City.
Hypertension. 2014 Oct;64(4):852-9. doi: 10.1161/HYPERTENSIONAHA.114.03848. Epub 2014 Jul 7.
Preeclampsia, a cardiovascular disorder of late pregnancy, is characterized as a low-renin hypertensive state relative to normotensive pregnancy. Because other nonpregnant low-renin hypertensive disorders often exhibit and are occasionally dependent on elevated arginine vasopressin (AVP) secretion, we hypothesized a possible use for plasma AVP measurements in the prediction of preeclampsia. Copeptin is an inert prosegment of AVP that is secreted in a 1:1 molar ratio and exhibits a substantially longer biological half-life compared with AVP, rendering it a clinically useful biomarker of AVP secretion. Copeptin was measured throughout pregnancy in maternal plasma from preeclamptic and control women. Maternal plasma copeptin was significantly higher throughout preeclamptic pregnancies versus control pregnancies. While controlling for clinically significant confounders (age, body mass index, chronic essential hypertension, twin gestation, diabetes mellitus, and history of preeclampsia) using multivariate regression, the association of higher copeptin concentration and the development of preeclampsia remained significant. Receiver operating characteristic analyses reveal that as early as the sixth week of gestation, elevated maternal plasma copeptin concentration is a highly significant predictor of preeclampsia throughout pregnancy. Finally, chronic infusion of AVP during pregnancy (24 ng per hour) is sufficient to phenocopy preeclampsia in C57BL/6J mice, causing pregnancy-specific hypertension, renal glomerular endotheliosis, proteinuria, and intrauterine growth restriction. These data implicate AVP release as a novel predictive biomarker for preeclampsia very early in pregnancy, identify chronic AVP infusion as a novel and clinically relevant model of preeclampsia in mice, and are consistent with a potential causative role for AVP in preeclampsia in humans.
子痫前期是一种妊娠晚期的心血管疾病,其特征是相对于血压正常的妊娠而言,处于低肾素高血压状态。由于其他非妊娠低肾素高血压疾病通常表现出并偶尔依赖于精氨酸加压素(AVP)分泌升高,我们推测血浆AVP测量在子痫前期预测中可能有用。 copeptin是AVP的一种无活性前体片段,以1:1摩尔比分泌,与AVP相比具有长得多的生物半衰期,使其成为AVP分泌的一种临床有用的生物标志物。在整个孕期测量了子痫前期和对照女性母体血浆中的copeptin。与对照妊娠相比,子痫前期妊娠全程母体血浆copeptin显著更高。在使用多变量回归控制临床显著混杂因素(年龄、体重指数、慢性原发性高血压、双胎妊娠、糖尿病和子痫前期病史)时,较高的copeptin浓度与子痫前期发生之间的关联仍然显著。受试者工作特征分析显示,早在妊娠第6周,母体血浆copeptin浓度升高就是整个孕期子痫前期的一个高度显著预测指标。最后,孕期慢性输注AVP(每小时24 ng)足以在C57BL/6J小鼠中模拟子痫前期,导致妊娠特异性高血压、肾小球内皮病变、蛋白尿和宫内生长受限。这些数据表明AVP释放是妊娠早期子痫前期的一种新型预测生物标志物,确定慢性AVP输注是小鼠子痫前期的一种新型且与临床相关的模型,并且与AVP在人类子痫前期中的潜在致病作用一致。
