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促成小鼠表皮分化和屏障形成的分子与机械特征。

Molecular and mechanical signatures contributing to mouse epidermal differentiation and barrier formation.

作者信息

Prado-Mantilla Alexandra, Ning Wenxiu, Lechler Terry

机构信息

Department of Dermatology, Duke University Medical Center, Durham, United States.

Department of Cell Biology, Duke University Medical Center, Durham, United States.

出版信息

Elife. 2025 Aug 7;13:RP100961. doi: 10.7554/eLife.100961.

Abstract

Formation of the skin barrier requires rapid proliferation coupled with differentiation and stratification of the embryonic epidermis. Basal progenitors give rise to progeny throughout development - first to intermediate cells, a transient proliferative suprabasal cell population, and later to spinous cells. Neither the function nor the differentiation trajectory of intermediate cells has been documented. We generated transcriptomes of intermediate and spinous cells and identified specific markers that distinguish these two populations. Further, we found that intermediate cells express a subset of genes in common with granular cells of the epidermis - the terminal living cell type that helps establish the barrier. Lineage tracing revealed that most intermediate cells directly transition to granular cells without expressing markers specific to spinous cells, thus revealing a distinct lineage pathway leading to granular fate. In addition to their transcriptional similarities, intermediate and granular cells both had hallmarks of increased actomyosin contractility. We found that rather than simply lying downstream of cell fate pathways, contractility was sufficient to suppress spinous fate and promote granular gene expression. Together, these data establish the molecular and mechanical characteristics of the developing epidermis that allow this tissue to rapidly develop barrier activity.

摘要

皮肤屏障的形成需要胚胎表皮快速增殖并伴随分化和分层。基底祖细胞在整个发育过程中产生后代——首先产生中间细胞,这是一种短暂增殖的基底上层细胞群体,随后产生棘状细胞。中间细胞的功能和分化轨迹均未被记录。我们生成了中间细胞和棘状细胞的转录组,并鉴定出区分这两种细胞群体的特异性标志物。此外,我们发现中间细胞表达的一部分基因与表皮颗粒细胞相同,表皮颗粒细胞是有助于建立屏障的终末活细胞类型。谱系追踪显示,大多数中间细胞直接转变为颗粒细胞,而不表达棘状细胞特异性标志物,从而揭示了一条通向颗粒细胞命运的独特谱系途径。除了转录相似性外,中间细胞和颗粒细胞均具有肌动球蛋白收缩性增加的特征。我们发现,收缩性并非简单地处于细胞命运途径的下游,它足以抑制棘状细胞命运并促进颗粒细胞基因表达。总之,这些数据确定了发育中表皮的分子和力学特征,这些特征使该组织能够快速发展屏障活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eab4/12331242/54f11f73b724/elife-100961-fig1.jpg

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