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从早发型子痫前期妇女中分离的胎盘来源循环细胞外囊泡的差异蛋白质组学研究揭示了异常的固有免疫和止血过程。

Differential proteomics of circulating extracellular vesicles of placental origin isolated from women with early-onset preeclampsia reveal aberrant innate immune and hemostasis processes.

机构信息

Innate Immunity Department, ICMR-National Institute for Research in Reproductive and Child Health (ICMR-NIRRCH), Mumbai, India.

Biomedical Informatics Centre, ICMR-National Institute for Research in Reproductive and Child Health (ICMR-NIRRCH), Mumbai, India.

出版信息

Am J Reprod Immunol. 2024 Jun;91(6):e13860. doi: 10.1111/aji.13860.

Abstract

PROBLEM

Early-onset preeclampsia (EOPE) is a severe gestational hypertensive disorder with significant feto-maternal morbidity and mortality due to uteroplacental insufficiency. Circulating extracellular vesicles of placental origin (EV-P) are known to be involved in the pathophysiology of EOPE and might serve as an ideal reservoir for its specific biomarkers. Therefore, we aimed to characterize and perform comparative proteomics of circulating EV-P from healthy pregnant and EOPE women before delivery.

METHOD OF STUDY

The EV-P from both groups were isolated using immunoaffinity and were characterized using transmission electron microscopy, dynamic light scattering, nanoparticle tracking analysis, and immunoblotting. Following IgG albumin depletion, the pooled proteins that were isolated from EV-P of both groups were subjected to quantitative TMT proteomics.

RESULTS

Circulating term EV-P isolated from both groups revealed ∼150 nm spherical vesicles containing CD9 and CD63 along with placental PLAP and HLA-G proteins. Additionally, the concentration of EOPE-derived EV-P was significantly increased. A total of 208 proteins were identified, with 26 among them being differentially abundant in EV-P of EOPE women. This study linked the pathophysiology of EOPE to 19 known and seven novel proteins associated with innate immune responses such as complement and TLR signaling along with hemostasis and oxygen homeostasis.

CONCLUSION

The theory suggesting circulating EVs of placental origin could mimic molecular information from the parent organ-"the placenta"-is strengthened by this study. The findings pave the way for possible discovery of novel prognostic and predictive biomarkers as well as provide insight into the mechanisms driving the pathogenesis of EOPE.

摘要

问题

早发型子痫前期(EOPE)是一种严重的妊娠高血压疾病,由于胎盘功能不全,导致胎儿和母亲发病率和死亡率显著增加。胎盘来源的细胞外囊泡(EV-P)已被证实参与 EOPE 的病理生理过程,并且可能作为其特异性生物标志物的理想来源。因此,我们旨在对健康孕妇和 EOPE 孕妇分娩前的循环 EV-P 进行特征描述和比较蛋白质组学分析。

研究方法

使用免疫亲和法分离两组的 EV-P,并通过透射电子显微镜、动态光散射、纳米颗粒跟踪分析和免疫印迹进行表征。在 IgG 白蛋白耗尽后,将从两组 EV-P 中分离的混合蛋白进行定量 TMT 蛋白质组学分析。

结果

从两组中分离出的足月 EV-P 显示出含有 CD9 和 CD63 的约 150nm 球形囊泡,以及胎盘 PLAP 和 HLA-G 蛋白。此外,EOPE 来源的 EV-P 的浓度明显增加。共鉴定出 208 种蛋白质,其中 26 种在 EOPE 妇女的 EV-P 中丰度差异显著。本研究将 EOPE 的病理生理学与已知的 19 种和 7 种与先天免疫反应(如补体和 TLR 信号转导)以及止血和氧平衡相关的新型蛋白联系起来。

结论

本研究进一步证实了循环胎盘来源的 EV 可以模拟来自母源器官“胎盘”的分子信息的理论。这些发现为发现新的预后和预测生物标志物铺平了道路,并深入了解了驱动 EOPE 发病机制的机制。

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