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单细胞 RNA 测序重新定义了小鼠子宫内膜的间质细胞图谱。

Single-cell RNA sequencing redefines the mesenchymal cell landscape of mouse endometrium.

机构信息

Centre for Inflammation Research, University of Edinburgh, Edinburgh, United Kingdom.

MRC Human Genetics Unit, Institute of Genetics and Molecular Medicine, University of Edinburgh, Edinburgh, United Kingdom.

出版信息

FASEB J. 2021 Apr;35(4):e21285. doi: 10.1096/fj.202002123R.

Abstract

The endometrium is a dynamic tissue that exhibits remarkable resilience to repeated episodes of differentiation, breakdown, regeneration, and remodeling. Endometrial physiology relies on a complex interplay between the stromal and epithelial compartments with the former containing a mixture of fibroblasts, vascular, and immune cells. There is evidence for rare populations of putative mesenchymal progenitor cells located in the perivascular niche of human endometrium, but the existence of an equivalent cell population in mouse is unclear. We used the Pdgfrb-BAC-eGFP transgenic reporter mouse in combination with bulk and single-cell RNA sequencing to redefine the endometrial mesenchyme. In contrast to previous reports we show that CD146 is expressed in both PDGFRβ + perivascular cells and CD31 + endothelial cells. Bulk RNAseq revealed cells in the perivascular niche which express the high levels of Pdgfrb as well as genes previously identified in pericytes and/or vascular smooth muscle cells (Acta2, Myh11, Olfr78, Cspg4, Rgs4, Rgs5, Kcnj8, and Abcc9). scRNA-seq identified five subpopulations of cells including closely related pericytes/vascular smooth muscle cells and three subpopulations of fibroblasts. All three fibroblast populations were PDGFRα+/CD34 + but were distinct in their expression of Ngfr/Spon2/Angptl7 (F1), Cxcl14/Smoc2/Rgs2 (F2), and Clec3b/Col14a1/Mmp3 (F3), with potential functions in the regulation of immune responses, response to wounding, and organization of extracellular matrix, respectively. Immunohistochemistry was used to investigate the spatial distribution of these populations revealing F1/NGFR + cells in most abundance beside epithelial cells. We provide the first definitive analysis of mesenchymal cells in the adult mouse endometrium identifying five subpopulations providing a platform for comparisons between mesenchymal cells in endometrium and other adult tissues which are prone to fibrosis.

摘要

子宫内膜是一种具有显著再生能力的动态组织,能够反复经历分化、破裂、再生和重塑。子宫内膜的生理机能依赖于基质和上皮细胞之间的复杂相互作用,前者包含混合的成纤维细胞、血管和免疫细胞。有证据表明,在人类子宫内膜的血管周围龛位中存在罕见的假定间充质祖细胞群体,但在小鼠中是否存在类似的细胞群体尚不清楚。我们使用 Pdgfrb-BAC-eGFP 转基因报告小鼠,结合批量和单细胞 RNA 测序,重新定义了子宫内膜间充质。与之前的报道相比,我们发现 CD146 在 PDGFRβ+血管周围细胞和 CD31+内皮细胞中均有表达。批量 RNAseq 揭示了血管周围龛位中的细胞高水平表达 Pdgfrb,以及先前在周细胞和/或血管平滑肌细胞中鉴定出的基因(Acta2、Myh11、Olfr78、Cspg4、Rgs4、Rgs5、Kcnj8 和 Abcc9)。scRNA-seq 鉴定出了包括密切相关的周细胞/血管平滑肌细胞在内的五个细胞亚群,以及三个成纤维细胞亚群。所有三个成纤维细胞群体均为 PDGFRα+/CD34+,但在 Ngfr/Spon2/Angptl7(F1)、Cxcl14/Smoc2/Rgs2(F2)和 Clec3b/Col14a1/Mmp3(F3)的表达上存在差异,它们分别具有调节免疫反应、对创伤的反应和细胞外基质组织的功能。免疫组织化学用于研究这些群体的空间分布,发现 F1/NGFR+细胞在大多数上皮细胞旁边最为丰富。我们首次对成年小鼠子宫内膜中的间充质细胞进行了明确分析,鉴定出了五个亚群,为比较子宫内膜和其他容易纤维化的成年组织中的间充质细胞提供了一个平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec50/9328940/3b61fed058d6/FSB2-35-0-g006.jpg

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