Maternal obesogenic diet disrupts mid-gestation decidual immune and vascular homeostasis without impairing spiral artery remodelling

Christian J. Bellissimo, Erica Yeo, Tatiane A. Ribeiro, Patrycja A. Jazwiec, Chethana Ellewela, Jaskiran Bains, Ali A. Ashkar, Alexander G. Beristain, Dawn M.E. Bowdish, Deborah M. Sloboda
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Abstract

Excess maternal adiposity (i.e., overweight and obesity) during pregnancy has been linked to impaired uteroplacental perfusion, compromised placental development, and a higher risk of adverse pregnancy outcomes. Owing to the nature of chronic inflammation and immune dysregulation accompanying excess adiposity, disruption of leukocyte-mediated tissue remodelling and immunoregulation within the decidua have emerged as likely drivers contributing to suboptimal placental function in pregnancies impacted by maternal overweight or obesity. However, the impacts of excess adiposity on major populations of innate lymphoid cells (ILCs) and macrophages which orchestrate these processes and the environment that these cells occupy remain vastly understudied. Here, we used a mouse model of chronic high-fat, high-sucrose (HFHS) diet-feeding to characterize the impacts of an obesogenic milieu on decidual immune dynamics during placental development at mid-gestation (E10.5). HFHS pregnancies exhibited marked increases in total decidual leukocyte abundance, driven by population-level increases in tissue-resident and conventional NK cells, and MHC-II+ macrophages. This was not associated with abnormalities in implantation site morphology or decidual spiral artery remodelling but was coincident with histological patterns of local inflammation. In line with this, expression of canonical proinflammatory cytokines and chemokines were moderately upregulated in bulk decidual tissue of HFHS dams. This was accompanied by more potent elevations in multiple mediators of angiogenesis, endothelial activation, and coagulation in HFHS decidual tissue. Collectively, these findings point towards pathological vascular inflammation and possibly dysregulated decidual angiogenesis in the first half of pregnancy as factors predisposing to reduced placental efficiency, malperfusion, and inflammation seen in pregnancies affected by maternal overweight and obesity.
母体肥胖饮食会破坏妊娠中期蜕膜免疫和血管稳态,但不会影响螺旋动脉重塑
妊娠期母体脂肪过多(即超重和肥胖)与子宫胎盘灌注受损、胎盘发育受损和不良妊娠结局的风险较高有关。由于伴随着过度肥胖的慢性炎症和免疫失调的性质,蜕膜内白细胞介导的组织重塑和免疫调节的破坏已成为导致受母体超重或肥胖影响的孕妇胎盘功能不佳的可能驱动因素。然而,过多的脂肪对先天性淋巴细胞(ILCs)和巨噬细胞等主要细胞群的影响以及这些细胞所处的环境仍未得到充分研究。在这里,我们利用长期高脂肪、高蔗糖(HFHS)饮食喂养的小鼠模型来描述肥胖环境对妊娠中期(E10.5)胎盘发育过程中蜕膜免疫动态的影响。在组织驻留细胞、常规 NK 细胞和 MHC-II+ 巨噬细胞群体水平增加的驱动下,HFHS 妊娠显示出蜕膜白细胞总丰度的显著增加。这与植入部位形态或蜕膜螺旋动脉重塑的异常无关,但与局部炎症的组织学模式相吻合。与此相一致的是,HFHS 母体的大量蜕膜组织中,典型促炎细胞因子和趋化因子的表达中度上调。与此同时,HFHS蜕膜组织中血管生成、内皮活化和凝血的多种介质也出现了更强的升高。总之,这些研究结果表明,妊娠前半期病理血管炎症和蜕膜血管生成失调可能是导致胎盘效率降低、灌注不良和炎症的因素,这在受孕妇超重和肥胖影响的妊娠中很容易见到。
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