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Myc蛋白支持食管上皮基底细胞的自我更新。

Myc Supports Self-Renewal of Basal Cells in the Esophageal Epithelium.

作者信息

Hishida Tomoaki, Vazquez-Ferrer Eric, Hishida-Nozaki Yuriko, Takemoto Yuto, Hatanaka Fumiyuki, Yoshida Kei, Prieto Javier, Sahu Sanjeeb Kumar, Takahashi Yuta, Reddy Pradeep, O'Keefe David D, Rodriguez Esteban Concepcion, Knoepfler Paul S, Nuñez Delicado Estrella, Castells Antoni, Campistol Josep M, Kato Ryuji, Nakagawa Hiroshi, Izpisua Belmonte Juan Carlos

机构信息

Gene Expression Laboratory, Salk Institute for Biological Studies, La Jolla, CA, United States.

Laboratory of Biological Chemistry, School of Pharmaceutical Sciences, Wakayama Medical University, Wakayama, Japan.

出版信息

Front Cell Dev Biol. 2022 Mar 4;10:786031. doi: 10.3389/fcell.2022.786031. eCollection 2022.

Abstract

It is widely believed that cellular senescence plays a critical role in both aging and cancer, and that senescence is a fundamental, permanent growth arrest that somatic cells cannot avoid. Here we show that Myc plays an important role in self-renewal of esophageal epithelial cells, contributing to their resistance to cellular senescence. Myc is homogeneously expressed in basal cells of the esophageal epithelium and Myc positively regulates their self-renewal by maintaining their undifferentiated state. Indeed, Myc knockout induced a loss of the undifferentiated state of esophageal epithelial cells resulting in cellular senescence while forced MYC expression promoted oncogenic cell proliferation. A superoxide scavenger counteracted Myc knockout-induced senescence, therefore suggesting that a mitochondrial superoxide takes part in inducing senescence. Taken together, these analyses reveal extremely low levels of cellular senescence and senescence-associated phenotypes in the esophageal epithelium, as well as a critical role for Myc in self-renewal of basal cells in this organ. This provides new avenues for studying and understanding the links between stemness and resistance to cellular senescence.

摘要

人们普遍认为,细胞衰老在衰老和癌症中都起着关键作用,并且衰老是体细胞无法避免的一种基本的、永久性的生长停滞。在此我们表明,Myc在食管上皮细胞的自我更新中起重要作用,有助于其抵抗细胞衰老。Myc在食管上皮的基底细胞中均匀表达,并且Myc通过维持其未分化状态来正向调节它们的自我更新。事实上,Myc基因敲除导致食管上皮细胞未分化状态丧失,从而引起细胞衰老,而强制表达MYC则促进致癌性细胞增殖。一种超氧化物清除剂可抵消Myc基因敲除诱导的衰老,因此表明线粒体超氧化物参与诱导衰老。综上所述,这些分析揭示了食管上皮中极低水平的细胞衰老和衰老相关表型,以及Myc在该器官基底细胞自我更新中的关键作用。这为研究和理解干性与抵抗细胞衰老之间的联系提供了新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0854/8931341/3972840220b5/fcell-10-786031-g001.jpg

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