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自维持的长期 3D 上皮样培养物揭示了食管上皮克隆扩张的驱动因素。

Self-sustaining long-term 3D epithelioid cultures reveal drivers of clonal expansion in esophageal epithelium.

机构信息

Wellcome Sanger Institute, Hinxton, UK.

Department of Biomedical Sciences, Universitat de Barcelona, Barcelona, Spain.

出版信息

Nat Genet. 2024 Oct;56(10):2158-2173. doi: 10.1038/s41588-024-01875-8. Epub 2024 Sep 23.

Abstract

Aging epithelia are colonized by somatic mutations, which are subjected to selection influenced by intrinsic and extrinsic factors. The lack of suitable culture systems has slowed the study of this and other long-term biological processes. Here, we describe epithelioids, a facile, cost-effective method of culturing multiple mouse and human epithelia. Esophageal epithelioids self-maintain without passaging for at least 1 year, maintaining a three-dimensional structure with proliferative basal cells that differentiate into suprabasal cells, which eventually shed and retain genomic stability. Live imaging over 5 months showed that epithelioids replicate in vivo cell dynamics. Epithelioids support genetic manipulation and enable the study of mutant cell competition and selection in three-dimensional epithelia, and show how anti-cancer treatments modulate competition between transformed and wild-type cells. Finally, a targeted CRISPR-Cas9 screen shows that epithelioids recapitulate mutant gene selection in aging human esophagus and identifies additional drivers of clonal expansion, resolving the genetic networks underpinning competitive fitness.

摘要

衰老的上皮细胞被体细胞突变定植,这些突变受到内在和外在因素影响的选择。缺乏合适的培养系统减缓了对这一现象和其他长期生物学过程的研究。在这里,我们描述了上皮细胞类器官,这是一种简便、经济有效的培养多种小鼠和人类上皮细胞的方法。食管上皮细胞类器官无需传代即可自我维持至少 1 年,保持具有增殖性基底细胞的三维结构,这些基底细胞分化为基底上层细胞,最终脱落并保持基因组稳定性。经过 5 个月的活体成像观察表明,上皮细胞类器官在体内复制了细胞动力学。上皮细胞类器官支持遗传操作,并能够在三维上皮组织中研究突变细胞竞争和选择,还展示了抗癌治疗如何调节转化细胞和野生型细胞之间的竞争。最后,一个靶向 CRISPR-Cas9 筛选显示,上皮细胞类器官重现了衰老人类食管中突变基因的选择,并确定了克隆扩增的其他驱动因素,解析了竞争适应性的遗传网络。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3fc8/11525200/55030f4b163e/41588_2024_1875_Fig1_HTML.jpg

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