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成年小鼠成纤维细胞保留器官特异性转录组特征。

Adult mouse fibroblasts retain organ-specific transcriptomic identity.

作者信息

Forte Elvira, Ramialison Mirana, Nim Hieu T, Mara Madison, Li Jacky Y, Cohn Rachel, Daigle Sandra L, Boyd Sarah, Stanley Edouard G, Elefanty Andrew G, Hinson John Travis, Costa Mauro W, Rosenthal Nadia A, Furtado Milena B

机构信息

The Jackson Laboratory, Bar Harbor, United States.

Australian Regenerative Medicine Institute, Monash University, Clayton, Australia.

出版信息

Elife. 2022 Mar 16;11:e71008. doi: 10.7554/eLife.71008.

DOI:10.7554/eLife.71008
PMID:35293863
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8959603/
Abstract

Organ fibroblasts are essential components of homeostatic and diseased tissues. They participate in sculpting the extracellular matrix, sensing the microenvironment, and communicating with other resident cells. Recent studies have revealed transcriptomic heterogeneity among fibroblasts within and between organs. To dissect the basis of interorgan heterogeneity, we compare the gene expression of murine fibroblasts from different tissues (tail, skin, lung, liver, heart, kidney, and gonads) and show that they display distinct positional and organ-specific transcriptome signatures that reflect their embryonic origins. We demonstrate that expression of genes typically attributed to the surrounding parenchyma by fibroblasts is established in embryonic development and largely maintained in culture, bioengineered tissues and ectopic transplants. Targeted knockdown of key organ-specific transcription factors affects fibroblast functions, in particular genes involved in the modulation of fibrosis and inflammation. In conclusion, our data reveal that adult fibroblasts maintain an embryonic gene expression signature inherited from their organ of origin, thereby increasing our understanding of adult fibroblast heterogeneity. The knowledge of this tissue-specific gene signature may assist in targeting fibrotic diseases in a more precise, organ-specific manner.

摘要

器官成纤维细胞是稳态组织和患病组织的重要组成部分。它们参与塑造细胞外基质、感知微环境并与其他驻留细胞进行通讯。最近的研究揭示了器官内部和之间的成纤维细胞存在转录组异质性。为了剖析器官间异质性的基础,我们比较了来自不同组织(尾巴、皮肤、肺、肝脏、心脏、肾脏和性腺)的小鼠成纤维细胞的基因表达,并表明它们呈现出独特的位置和器官特异性转录组特征,反映了它们的胚胎起源。我们证明,成纤维细胞通常归因于周围实质组织的基因表达在胚胎发育过程中建立,并在培养、生物工程组织和异位移植中基本维持。关键器官特异性转录因子的靶向敲低会影响成纤维细胞功能,特别是参与纤维化和炎症调节的基因。总之,我们的数据表明,成年成纤维细胞维持着从其起源器官继承而来的胚胎基因表达特征,从而增进了我们对成年成纤维细胞异质性的理解。这种组织特异性基因特征的知识可能有助于以更精确、器官特异性的方式靶向纤维化疾病。

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Adult mouse fibroblasts retain organ-specific transcriptomic identity.成年小鼠成纤维细胞保留器官特异性转录组特征。
Elife. 2022 Mar 16;11:e71008. doi: 10.7554/eLife.71008.
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Epigenomic landscape of single vascular cells reflects developmental origin and disease risk loci.单个血管细胞的表观基因组景观反映发育起源和疾病风险位点。
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2
Cardiac endothelial cells maintain open chromatin and expression of cardiomyocyte myofibrillar genes.心脏内皮细胞维持开放染色质和心肌细胞肌原纤维基因的表达。
Elife. 2020 Dec 14;9:e55730. doi: 10.7554/eLife.55730.
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Fibrosis: from mechanisms to medicines.纤维化:从机制到药物
通过共培养系统揭示诱导多能干细胞衍生的成纤维细胞中的组织特异性转录适应性。
Stem Cell Res Ther. 2025 Jul 30;16(1):413. doi: 10.1186/s13287-025-04537-6.
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Cellular Reprogramming by PHF7 Enhances Cardiac Function Following Myocardial Infarction.PHF7介导的细胞重编程增强心肌梗死后的心功能
Circulation. 2025 Jul 9. doi: 10.1161/CIRCULATIONAHA.124.072733.
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Establishing Primary and Stable Cell Lines from Frozen Wing Biopsies for Cellular, Physiological, and Genetic Studies in Bats.从冷冻的翅膀活检组织中建立原代稳定细胞系,用于蝙蝠的细胞、生理和遗传研究。
Curr Protoc. 2024 Sep;4(9):e1123. doi: 10.1002/cpz1.1123.
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Bacterial Ribosomes Induce Plasticity in Mouse Adult Fibroblasts.细菌核糖体诱导成年小鼠成纤维细胞发生可塑性。
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