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首页> 外文期刊>AJRI: American Journal of Reproductive Immunology >Maternal plasma proteomics in a rat model of pregnancy complications reveals immune and pro‐coagulant gene pathway activation
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Maternal plasma proteomics in a rat model of pregnancy complications reveals immune and pro‐coagulant gene pathway activation

机译:孕产妇血浆蛋白质组学在妊娠并发症的大鼠模型中揭示了免疫和亲凝血基因途径活化

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摘要

Abstract Problem The Brown Norway (BN) rat is a model of T‐helper 2 immune diseases, and also a model of pregnancy disorders that include placental insufficiency, fetal loss, and pre‐eclampsia‐like symptoms. The aim of this study was to investigate the plasma proteomic/cytokine profile of pregnant BN rats in comparison to that of the Lewis (LEW) rat strain. Method of study Plasma proteomics differences were studied at day 13 of pregnancy in pooled plasma samples by differential in‐gel electrophoresis, and protein identification was performed by mass spectrometry. Key protein findings and predicted cytokine differences were validated by ELISA using plasma from rats at various pregnancy stages. Proteomics data were used for ingenuity pathway analysis (IPA). Results In‐gel analysis revealed 74 proteins with differential expression between BN and LEW pregnant dams. ELISA studies confirmed increased maternal plasma levels of complement 4, prothrombin, and C‐reactive protein in BN compared to LEW pregnancies. LEW pregnancies showed higher maternal plasma levels of transthyretin and haptoglobin than BN pregnancies. Ingenuity pathway analysis revealed that BN pregnancies are characterized by activation of pro‐coagulant, reactive oxygen species, and immune‐mediated chronic inflammation pathways, and suggested increased interleukin 6 and decreased transforming growth factor‐β1 as potential upstream events. Plasma cytokine analysis revealed that pregnant BN dams have a switch from anti‐ to pro‐inflammatory cytokines with the opposite switch observed in pregnant LEW dams. Conclusion Brown Norway rats show a maternal pro‐inflammatory response to pregnancy that likely contributes to the reproductive outcomes observed in this rat strain.
机译:摘要问题褐色挪威(BN)RAT是T-Helper 2免疫疾病的模型,以及妊娠障碍模型,包括胎盘不足,胎儿损失和异普拉姆类症状的症状。该研究的目的是研究怀孕BN大鼠的血浆蛋白质组学/细胞因子谱与Lewis(Lew)大鼠菌株的血浆。研究血浆蛋白质组学差异在妊娠血浆样品的第13天通过差异凝胶电泳进行了研究,并且通过质谱法进行蛋白质鉴定。 ELISA使用来自各种妊娠阶段的大鼠的血浆验证了关键蛋白质发现和预测的细胞因子差异。蛋白质组学数据用于互联途径分析(IPA)。结果In-Gel分析显示了BN和Lew怀孕水坝之间具有差异表达的74个蛋白质。 ELISA研究证实,与LEW妊娠相比,BN中的补体4,凝血酶原和C反应蛋白的母体血浆水平增加。 Lew妊娠表现出较高的母体血浆水平的Transthyretin和Haptoglobin比BN怀孕。 Ingenuey途径分析显示,BN妊娠的特征在于激活促凝血剂,活性氧物质和免疫介导的慢性炎症途径,并提出了白细胞介素6的增加,并降低了转化生长因子-β1作为潜在上游事件。血浆细胞因子分析显示,怀孕的BN坝具有从抗促炎细胞因子的开关,在怀孕的lew水坝中观察到的相反开关。结论棕褐色挪威大鼠对妊娠的母体促炎反应可能有助于在该大鼠菌株中观察到的生殖结果。

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