Single cell transcriptome analysis of decidua macrophages in normal and recurrent spontaneous abortion patients

Zheng, Qi-Teng; Xu, Xin; Yang, Fenglian; Gan, Haiyong; Zhao, Yongbo; Wan, Xiaoxia; Jin, Lei

doi:10.1101/2021.03.23.436615

Cited by 2 publications

(2 citation statements)

References 45 publications

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“…The overall monocyte/macrophage cluster can be identified by expression of CD14, CD16 ( FCGR3A ), CD163, and CD206 ( MRC1 ) ( Fig 6C ). These further subdivided into two subclusters named according to other transcriptional features: Mo/Mφ1 (2,012 cells), which show upregulation of IL1B , CCL20 , CXCL3 , CXCL8 , TNF , EREG , and the inflammasome sensor NLRP3 ; and Mo/Mφ2 (2,919 cells), a reparative phenotype that has been previously reported in non-vascular tissues [ 71 – 73 ]. The latter are characterized by high expression of C1QA/B/C , FOLR2 , HMOX1 , LYVE1 , RNASE1 , SELENOP , and VSIG4 ( Fig 6D and 6E , S5 File in S1 Data ).…”

Section: Resultsmentioning

confidence: 91%

The intricate cellular ecosystem of human peripheral veins as revealed by single-cell transcriptomic analysis

Rojas,

Zigmond,

Pereira-Simon

et al. 2024

PLoS ONE

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The venous system has been historically understudied despite its critical roles in blood distribution, heart function, and systemic immunity. This study dissects the microanatomy of upper arm veins at the single cell level, and how it relates to wall structure, remodeling processes, and inflammatory responses to injury. We applied single-cell RNA sequencing to 4 non-diseased human veins (3 basilic, 1 cephalic) obtained from organ donors, followed by bioinformatic and histological analyses. Unsupervised clustering of 20,006 cells revealed a complex ecosystem of endothelial cell (EC) types, smooth muscle cell (SMCs) and pericytes, various types of fibroblasts, and immune cell populations. The venous endothelium showed significant upregulation of cell adhesion genes, with arteriovenous zonation EC phenotypes highlighting the heterogeneity of vasa vasorum (VV) microvessels. Venous SMCs had atypical contractile phenotypes and showed widespread localization in the intima and media. MYH11+DESlo SMCs were transcriptionally associated with negative regulation of contraction and pro-inflammatory gene expression. MYH11+DEShi SMCs showed significant upregulation of extracellular matrix genes and pro-migratory mediators. Venous fibroblasts ranging from secretory to myofibroblastic phenotypes were 4X more abundant than SMCs and widely distributed throughout the wall. Fibroblast-derived angiopoietin-like factors were identified as versatile signaling hubs to regulate angiogenesis and SMC proliferation. An abundant monocyte/macrophage population was detected and confirmed by histology, including pro-inflammatory and homeostatic phenotypes, with cell counts positively correlated with age. Ligand-receptor interactome networks identified the venous endothelium in the main lumen and the VV as a niche for monocyte recruitment and infiltration. This study underscores the transcriptional uniqueness of venous cells and their relevance for vascular inflammation and remodeling processes. Findings from this study may be relevant for molecular investigations of upper arm veins used for vascular access creation, where single-cell analyses of cell composition and phenotypes are currently lacking.

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Section: Resultsmentioning

confidence: 91%

The intricate cellular ecosystem of human peripheral veins as revealed by single-cell transcriptomic analysis

Rojas,

Zigmond,

Pereira-Simon

et al. 2024

PLoS ONE

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“…In particular, a decrease in the dNK subset supporting embryonic growth, decrease in the dNK subset (CSF1 + CD59 + KIRs-expressing), decrease in the dNK subset with angiogenic function, increase in the dNK subset characteristic of cytotoxic and immune activation, and increase in the dNK subset (CD56 + CD16 + ) in RPL highlighted the role of dNKs in the pathogenesis of RPL; however, the function of these subsets requires further investigation. Besides dNKs, different macrophage polarization, accumulation of activated dendritic cell sub-population, and abnormal distribution of T cell subtypes were indicated in RPL [52][53][54]86,87] .…”

Section: Recurrent Pregnancy Lossmentioning

confidence: 99%

Single-cell analysis in endometrial research

Cao

Wang

Yao

et al. 2022

Reproductive and Developmental Medicine

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Human endometrium undergoes dynamic shedding, regeneration, and differentiation, with remarkable changes in gene expression across the menstrual cycle. The development of a receptive endometrium within a particular time frame (window of implantation) is critical for successful embryo implantation. To understand the role of the endometrium in human fertility and regenerative biology, transcriptomic characterization of the endometrium has traditionally been pursued at the tissue bulk level using microarray and next-generation sequencing. Owing to the rapid development of single-cell RNA sequencing technology, researchers have uncovered heterogeneous molecular activities in individual cells masked by bulk analysis. In this review, we opted to mainly focus on single-cell analysis in endometrial research and introduce basic knowledge of single-cell RNA sequencing and the isolation of single cells from endometrial cells. We also discussed how single-cell approaches are used to understand the transformation and regeneration of the endometrium physiologically and uncover endometrial factors that contribute to uterine pathology.

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Single cell transcriptome analysis of decidua macrophages in normal and recurrent spontaneous abortion patients

Cited by 2 publications

References 45 publications

The intricate cellular ecosystem of human peripheral veins as revealed by single-cell transcriptomic analysis

The intricate cellular ecosystem of human peripheral veins as revealed by single-cell transcriptomic analysis

Single-cell analysis in endometrial research

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