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健康绝经前女性子宫的细胞异质性和动态变化

Cellular heterogeneity and dynamics of the human uterus in healthy premenopausal women.

作者信息

Ulrich Nicole D, Vargo Alex, Ma Qianyi, Shen Yu-Chi, Hannum D Ford, Gurczynski Stephen J, Moore Bethany B, Schon Samantha, Lieberman Richard, Shikanov Ariella, Marsh Erica E, Fazleabas Asgerally, Li Jun Z, Hammoud Saher Sue

出版信息

bioRxiv. 2024 Mar 12:2024.03.07.583985. doi: 10.1101/2024.03.07.583985.

DOI:10.1101/2024.03.07.583985
PMID:38559249
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10979868/
Abstract

UNLABELLED

The human uterus is a complex and dynamic organ whose lining grows, remodels, and regenerates in every menstrual cycle or upon tissue damage. Here we applied single-cell RNA sequencing to profile more the 50,000 uterine cells from both the endometrium and myometrium of 5 healthy premenopausal individuals, and jointly analyzed the data with a previously published dataset from 15 subjects. The resulting normal uterus cell atlas contains more than 167K cells representing the lymphatic endothelium, blood endothelium, stromal, ciliated epithelium, unciliated epithelium, and immune cell populations. Focused analyses within each major cell type and comparisons with subtype labels from prior studies allowed us to document supporting evidence, resolve naming conflicts, and to propose a consensus annotation system of 39 subtypes. We release their gene expression centroids, differentially expressed genes, and mRNA patterns of literature-based markers as a shared community resource. We find many subtypes show dynamic changes over different phases of the cycle and identify multiple potential progenitor cells: compartment-wide progenitors for each major cell type, transitional cells that are upstream of other subtypes, and potential cross-lineage multipotent stromal progenitors that may be capable of replenishing the epithelial, stromal, and endothelial compartments. When compared to the healthy premenopausal samples, a postpartum and a postmenopausal uterus sample revealed substantially altered tissue composition, involving the rise or fall of stromal, endothelial, and immune cells. The cell taxonomy and molecular markers we report here are expected to inform studies of both basic biology of uterine function and its disorders.

SIGNIFICANCE

We present single-cell RNA sequencing data from seven individuals (five healthy pre-menopausal women, one post-menopausal woman, and one postpartum) and perform an integrated analysis of this data alongside 15 previously published scRNA-seq datasets. We identified 39 distinct cell subtypes across four major cell types in the uterus. By using RNA velocity analysis and centroid-centroid comparisons we identify multiple computationally predicted progenitor populations for each of the major cell compartments, as well as potential cross-compartment, multi-potent progenitors. While the function and interactions of these cell populations remain to be validated through future experiments, the markers and their "dual characteristics" that we describe will serve as a rich resource to the scientific community. Importantly, we address a significant challenge in the field: reconciling multiple uterine cell taxonomies being proposed. To achieve this, we focused on integrating historical and contemporary knowledge across multiple studies. By providing detailed evidence used for cell classification we lay the groundwork for establishing a stable, consensus cell atlas of the human uterus.

摘要

未加标签

人类子宫是一个复杂且动态的器官,其内膜在每个月经周期或组织受损时都会生长、重塑和再生。在此,我们应用单细胞RNA测序技术,对5名健康绝经前个体的子宫内膜和肌层中的5万多个子宫细胞进行了分析,并将这些数据与之前发表的来自15名受试者的数据集进行了联合分析。由此产生的正常子宫细胞图谱包含超过16.7万个细胞,代表了淋巴管内皮细胞、血管内皮细胞、基质细胞、纤毛上皮细胞、非纤毛上皮细胞和免疫细胞群体。对每种主要细胞类型进行重点分析,并与先前研究中的亚型标签进行比较,使我们能够记录支持证据、解决命名冲突,并提出一个包含39个亚型的共识注释系统。我们发布了它们的基因表达中心、差异表达基因以及基于文献的标志物的mRNA模式,作为共享的社区资源。我们发现许多亚型在月经周期的不同阶段呈现动态变化,并鉴定出多个潜在的祖细胞:每种主要细胞类型的全区域祖细胞、其他亚型上游的过渡细胞,以及可能能够补充上皮、基质和内皮细胞区域的潜在跨谱系多能基质祖细胞。与健康绝经前样本相比,一个产后子宫样本和一个绝经后子宫样本显示出组织组成有显著改变,涉及基质细胞、内皮细胞和免疫细胞的增加或减少。我们在此报告的细胞分类法和分子标志物有望为子宫功能的基础生物学及其疾病的研究提供信息。

意义

我们展示了来自7名个体(5名健康绝经前女性、1名绝经后女性和1名产后女性)的单细胞RNA测序数据,并将这些数据与之前发表的15个单细胞RNA测序数据集进行了综合分析。我们在子宫的四种主要细胞类型中鉴定出39种不同的细胞亚型。通过使用RNA速度分析和中心与中心的比较,我们为每个主要细胞区域鉴定出多个通过计算预测的祖细胞群体,以及潜在的跨区域多能祖细胞。虽然这些细胞群体的功能和相互作用仍有待通过未来的实验进行验证,但我们所描述的标志物及其“双重特征”将为科学界提供丰富的资源。重要的是,我们解决了该领域的一个重大挑战:协调正在提出的多种子宫细胞分类法。为实现这一目标,我们专注于整合多项研究中的历史和当代知识。通过提供用于细胞分类的详细证据,我们为建立一个稳定的、共识性的人类子宫细胞图谱奠定了基础。

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