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单细胞和空间转录组学揭示了胎盘植入谱系障碍中侵袭部位滋养层细胞的改变以及子宫肌层免疫微环境的紊乱。

Single-cell and spatial transcriptomics reveal alterations in trophoblasts at invasion sites and disturbed myometrial immune microenvironment in placenta accreta spectrum disorders.

作者信息

Ji Kaiyuan, Chen Yunshan, Pan Xiuyu, Chen Lina, Wang Xiaodi, Wen Bolun, Bao Junjie, Zhong Junmin, Lv Zi, Zheng Zheng, Liu Huishu

机构信息

Guangzhou Key Laboratory of Maternal-Fetal Medicine, Guangzhou Women and Children's Medical Center, Guangzhou Medical University, No. 9 Jinsui Road, Guangzhou, China.

Institute of Reproductive Health and Perinatology, Guangzhou Women and Children's Medical Center, Guangzhou Medical University, Guangzhou, China.

出版信息

Biomark Res. 2024 Jun 3;12(1):55. doi: 10.1186/s40364-024-00598-6.

Abstract

BACKGROUND

Placenta accreta spectrum disorders (PAS) are a severe complication characterized by abnormal trophoblast invasion into the myometrium. The underlying mechanisms of PAS involve a complex interplay of various cell types and molecular pathways. Despite its significance, both the characteristics and intricate mechanisms of this condition remain poorly understood.

METHODS

Spatial transcriptomics (ST) and single-cell RNA sequencing (scRNA-seq), were performed on the tissue samples from four PAS patients, including invasive tissues (ST, n = 3; scRNA-seq, n = 4), non-invasive normal placenta samples (ST, n = 1; scRNA-seq, n = 2). Three healthy term pregnant women provided normal myometrium samples (ST, n = 1; scRNA-seq, n = 2). ST analysis characterized the spatial expression landscape, and scRNA-seq was used to identify specific cellular components in PAS. Immunofluorescence staining was conducted to validate the findings.

RESULTS

ST slices distinctly showed the myometrium in PAS was invaded by three subpopulations of trophoblast cells, extravillous trophoblast cells, cytotrophoblasts, and syncytiotrophoblasts, especially extravillous trophoblast cells. The pathways enriched by genes in trophoblasts, smooth muscle cells (SMC), and immune cells of PAS were mainly associated with immune and inflammation. We identified elevated expression of the angiogenesis-stimulating gene PTK2, alongside the cell proliferation-enhancing gene EGFR, within the trophoblasts of PAS group. Trophoblasts mainly contributed the enhancement of HLA-G and EBI3 signaling, which is crucial in establishing immune escape. Meanwhile, SMC regions in PAS exhibited upregulation of immunomodulatory markers such as CD274, HAVCR2, and IDO1, with CD274 expression experimentally verified to be increased in the invasive SMC areas of the PAS group.

CONCLUSIONS

This study provided information of cellular composition and spatial organization in PAS at single-cell and spatial level. The dysregulated expression of genes in PAS revealed a complex interplay between enhanced immune escape in trophoblasts and immune tolerance in SMCs during invasion in PAS. These findings will enhance our understanding of PAS pathogenesis for developing potential therapeutic strategies.

摘要

背景

胎盘植入谱系疾病(PAS)是一种严重的并发症,其特征是滋养层细胞异常侵入子宫肌层。PAS的潜在机制涉及多种细胞类型和分子途径的复杂相互作用。尽管其具有重要意义,但这种疾病的特征和复杂机制仍知之甚少。

方法

对4例PAS患者的组织样本进行了空间转录组学(ST)和单细胞RNA测序(scRNA-seq),包括侵袭性组织(ST,n = 3;scRNA-seq,n = 4)、非侵袭性正常胎盘样本(ST,n = 1;scRNA-seq,n = 2)。3名足月健康孕妇提供了正常子宫肌层样本(ST,n = 1;scRNA-seq,n = 2)。ST分析表征了空间表达格局,scRNA-seq用于识别PAS中的特定细胞成分。进行免疫荧光染色以验证研究结果。

结果

ST切片清楚地显示,PAS中的子宫肌层被三种滋养层细胞亚群侵入,即绒毛外滋养层细胞、细胞滋养层细胞和合胞体滋养层细胞,尤其是绒毛外滋养层细胞。PAS中滋养层细胞、平滑肌细胞(SMC)和免疫细胞中基因富集的途径主要与免疫和炎症相关。我们发现在PAS组的滋养层细胞中,促血管生成基因PTK2以及增强细胞增殖的基因EGFR表达升高。滋养层细胞主要促成了HLA-G和EBI3信号的增强,这在建立免疫逃逸中至关重要。同时,PAS中的SMC区域表现出免疫调节标志物如CD274、HAVCR2和IDO1的上调,实验证实PAS组侵袭性SMC区域中CD274表达增加。

结论

本研究在单细胞和空间水平上提供了PAS中细胞组成和空间组织的信息。PAS中基因的失调表达揭示了PAS侵袭过程中滋养层细胞免疫逃逸增强与SMC免疫耐受之间的复杂相互作用。这些发现将增进我们对PAS发病机制的理解,以制定潜在的治疗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec20/11149369/69916b91aab0/40364_2024_598_Fig1_HTML.jpg

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