Maternal Innate Immune Reprogramming After Complicated Pregnancy

IF 2.5 3区医学 Q3 IMMUNOLOGY

American Journal of Reproductive Immunology Pub Date : 2024-08-09 DOI:10.1111/aji.13908

Nakeisha A. Lodge-Tulloch, Jean-François Paré, Camille Couture, Elsa Bernier, Tiziana Cotechini, Sylvie Girard, Charles H. Graham

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Abstract

Problem

Preeclampsia (PE) and fetal growth restriction (FGR) are often associated with maternal inflammation and an increased risk of cardiovascular and metabolic disease in the affected mothers. The mechanism responsible for this increased risk of subsequent disease may involve reprogramming of innate immune cells, characterized by epigenetic modifications.

Method of Study

Circulating monocytes from women with PE, FGR, or uncomplicated pregnancies (control) were isolated before labor. Cytokine release from monocytes following exposure to lipopolysaccharide (LPS) and the presence of lysine 4-trimethylated histone 3 (H3K4me3) within TNF promoter sequences were evaluated. Single-cell transcriptomic profiles of circulating monocytes from women with PE or uncomplicated pregnancies were assessed.

Results

Monocytes from women with PE or FGR exhibited increased IL-10 secretion and decreased IL-1β and GM-CSF secretion in response to LPS. While TNFα secretion was not significantly different in cultures of control monocytes versus those from complicated pregnancies with or without LPS exposure, monocytes from complicated pregnancies had significantly decreased levels of H3K4me3 associated with TNF promoter sequences. Cluster quantification and pathway analysis of differentially expressed genes revealed an increased proportion of anti-inflammatory myeloid cells and a lower proportion of inflammatory non-classical monocytes among the circulating monocyte population in women with PE.

Conclusions

Monocytes from women with PE and FGR exhibit an immune tolerance phenotype before initiation of labor. Further investigation is required to determine whether this tolerogenic phenotype persists after the affected pregnancy and contributes to increased risk of subsequent disease.

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妊娠并发症后母体先天性免疫重编程

问题：子痫前期（PE）和胎儿生长受限（FGR）通常与母体炎症以及受影响母亲罹患心血管疾病和代谢疾病的风险增加有关。导致这种后续疾病风险增加的机制可能涉及先天性免疫细胞的重编程，其特点是表观遗传修饰：研究方法：在分娩前分离患有 PE、FGR 或无并发症妊娠（对照组）的妇女的循环单核细胞。研究评估了单核细胞暴露于脂多糖（LPS）后细胞因子的释放情况以及 TNF 启动子序列中赖氨酸 4-三甲基化组蛋白 3（H3K4me3）的存在情况。对患有 PE 或无并发症妊娠的妇女的循环单核细胞的单细胞转录组图谱进行了评估：结果：PE 或 FGR 孕妇的单核细胞对 LPS 的反应是 IL-10 分泌增加，IL-1β 和 GM-CSF 分泌减少。虽然对照组单核细胞与有或无 LPS 暴露的难治性妊娠单核细胞的 TNFα 分泌无显著差异，但难治性妊娠单核细胞与 TNF 启动子序列相关的 H3K4me3 水平显著下降。差异表达基因的聚类定量和通路分析表明，在 PE 妇女的循环单核细胞群中，抗炎髓系细胞的比例增加，而炎症性非典型单核细胞的比例降低：结论：患有 PE 和 FGR 的妇女的单核细胞在分娩开始前表现出免疫耐受表型。结论：患有 PE 和 FGR 的妇女的单核细胞在分娩开始前表现出免疫耐受表型，需要进一步研究以确定这种耐受表型是否会在受影响妊娠后持续存在并导致后续疾病风险的增加。

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来源期刊

American Journal of Reproductive Immunology 医学-免疫学

CiteScore

6.20

自引率

5.60%

发文量

314

审稿时长

2 months

期刊介绍： The American Journal of Reproductive Immunology is an international journal devoted to the presentation of current information in all areas relating to Reproductive Immunology. The journal is directed toward both the basic scientist and the clinician, covering the whole process of reproduction as affected by immunological processes. The journal covers a variety of subspecialty topics, including fertility immunology, pregnancy immunology, immunogenetics, mucosal immunology, immunocontraception, endometriosis, abortion, tumor immunology of the reproductive tract, autoantibodies, infectious disease of the reproductive tract, and technical news.