Translational Obstetrics Group Mercy Hospital for Women Heidelberg Victoria Australia.
Department of Obstetrics and Gynaecology Mercy Hospital for Women University of Melbourne Heidelberg Victoria Australia.
J Am Heart Assoc. 2022 Apr 5;11(7):e024536. doi: 10.1161/JAHA.121.024536. Epub 2022 Mar 24.
Background Preeclampsia is pregnancy specific, involving significant maternal endothelial dysfunction. Predictive biomarkers are lacking. We evaluated the biomarker potential, expression, and function of PSG7 (pregnancy-specific β-1 glycoprotein 7) and PSG9 (pregnancy-specific β-1 glycoprotein 9) in preeclampsia. Methods and Results At 36 weeks gestation preceding term preeclampsia diagnosis, PSG7 and PSG9 (in Australian cohorts of n=918 and n=979, respectively) were significantly increased before the onset of term preeclampsia (PSG7, =0.013; PSG9, =0.0011). In samples collected at 28 to 32 weeks from those with preexisting cardiovascular disease and at high risk of preeclampsia (Manchester Antenatal Vascular Service, UK cohort, n=235), both PSG7 and PSG9 were also significantly increased preceding preeclampsia onset (PSG7, <0.0001; PSG9, =0.0003) relative to controls. These changes were validated in the plasma and placentas of patients with established preeclampsia who delivered at <34 weeks gestation (PSG7, =0.0008; PSG9, <0.0001). To examine whether PSG7 and PSG9 are associated with increasing disease severity, we measured them in a cohort from South Africa stratified for this outcome, the PROVE (Preeclampsia Obstetric Adverse Events) cohort (n=72). PSG7 (=0.0027) and PSG9 (=0.0028) were elevated among patients who were preeclamptic with severe features (PROVE cohort), but not significantly changed in those without severe features or with eclampsia. In syncytialized first trimester cytotrophoblast stem cells, exposure to TNFα (tumor necrosis factor α) or IL-6 (interleukin 6) significantly increased the expression and secretion of PSG7 and PSG9. In contrast, when we treated primary endothelial cells with recombinant PSG7 and PSG9, we only observed modest changes in (FMS-like tyrosine kinase-1) expression and (placental growth factor) expression, and no other effects on proangiogenic/antiangiogenic or endothelial dysfunction markers were observed. Conclusions Circulating PSG7 and PSG9 are increased before preeclampsia onset and among those with established disease with their production and release potentially driven by placental inflammation.
子痫前期是一种与妊娠相关的疾病,涉及到母体内皮功能的显著障碍。目前缺乏预测生物标志物。我们评估了 PSG7(妊娠特异性β-1 糖蛋白 7)和 PSG9(妊娠特异性β-1 糖蛋白 9)在子痫前期中的生物标志物潜力、表达和功能。
在澳大利亚队列中,在妊娠 36 周时进行了前瞻性研究,在早产子痫前期诊断前,PSG7 和 PSG9 明显升高(PSG7,=0.013;PSG9,=0.0011)。在英国曼彻斯特产前血管服务队列中,在 28 至 32 周时采集了有心血管疾病病史且子痫前期风险较高的样本(英国曼彻斯特产前血管服务队列,n=235),在子痫前期发作前,PSG7 和 PSG9 也明显升高(PSG7,<0.0001;PSG9,=0.0003)。在在 34 周前分娩的确诊子痫前期患者的血浆和胎盘组织中也验证了这些变化(PSG7,=0.0008;PSG9,<0.0001)。为了研究 PSG7 和 PSG9 是否与疾病严重程度有关,我们在南非的 PROVE(子痫前期产科不良事件)队列中对分层的患者进行了测量(n=72)。PSG7(=0.0027)和 PSG9(=0.0028)在有严重特征的子痫前期患者中升高,但在无严重特征或子痫患者中无明显变化。在合体滋养层干细胞中,TNFα(肿瘤坏死因子α)或 IL-6(白细胞介素 6)的暴露显著增加了 PSG7 和 PSG9 的表达和分泌。相比之下,当我们用重组 PSG7 和 PSG9 处理原代内皮细胞时,我们只观察到 FMS 样酪氨酸激酶-1(FMS-like tyrosine kinase-1)和胎盘生长因子(placental growth factor)表达的适度变化,并且没有观察到其他对促血管生成/抗血管生成或内皮功能障碍标志物的影响。
循环 PSG7 和 PSG9 在子痫前期发作前升高,在已确诊的疾病患者中升高,其产生和释放可能是由胎盘炎症驱动的。
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