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SOX2 在前肠前的缺失会导致食管在上皮和间质成分中都转变成气管和支气管。

The absence of SOX2 in the anterior foregut alters the esophagus into trachea and bronchi in both epithelial and mesenchymal components.

机构信息

Faculty of Life Sciences and Institutes for Protein Dynamics and Comprehensive Research, Kyoto Sangyo University, Kita-ku, Kyoto 603-8555, Japan.

Division of Biological Science, Graduate School of Science, Nagoya University, Chikusa-ku, Nagoya 464-8602, Japan.

出版信息

Biol Open. 2020 Feb 7;9(2):bio048728. doi: 10.1242/bio.048728.

Abstract

In the anterior foregut (AFG) of mouse embryos, the transcription factor SOX2 is expressed in the epithelia of the esophagus and proximal branches of respiratory organs comprising the trachea and bronchi, whereas NKX2.1 is expressed only in the epithelia of respiratory organs. Previous studies using hypomorphic alleles have indicated that reduced SOX2 expression causes the esophageal epithelium to display some respiratory organ characteristics. In the present study, we produced mouse embryos with AFG-specific SOX2 deficiency. In the absence of SOX2 expression, a single NKX2.1-expressing epithelial tube connected the pharynx and the stomach, and a pair of bronchi developed in the middle of the tube. Expression patterns of NKX2.1 and SOX9 revealed that the anterior and posterior halves of SOX2-deficient AFG epithelial tubes assumed the characteristics of the trachea and bronchus, respectively. In addition, we found that mesenchymal tissues surrounding the SOX2-deficient NKX2.1-expressing epithelial tube changed to those surrounding the trachea and bronchi in the anterior and posterior halves, as indicated by the arrangement of smooth muscle cells and SOX9-expressing cells and by the expression of (esophagus specific), (respiratory organ specific), and (distal bronchus specific). The impact of mesenchyme-derived signaling on the early stage of AFG epithelial specification has been indicated. Our study demonstrated an opposite trend where epithelial tissue specification causes concordant changes in mesenchymal tissues, indicating a reciprocity of epithelial-mesenchymal interactions.

摘要

在小鼠胚胎的前前肠(AFG)中,转录因子 SOX2 在前肠的食管和呼吸道近端分支(包括气管和支气管)的上皮中表达,而 NKX2.1 仅在呼吸道上皮中表达。先前使用功能减弱等位基因的研究表明,SOX2 表达减少导致食管上皮表现出一些呼吸道器官的特征。在本研究中,我们产生了 AFG 特异性 SOX2 缺陷的小鼠胚胎。在缺乏 SOX2 表达的情况下,单个 NKX2.1 表达的上皮管连接咽和胃,并且一对支气管在管的中部发育。NKX2.1 和 SOX9 的表达模式表明,SOX2 缺陷的 AFG 上皮管的前半部分和后半部分分别具有气管和支气管的特征。此外,我们发现,SOX2 缺陷的 NKX2.1 表达上皮管周围的间充质组织在前半部分和后半部分分别变为气管和支气管周围的间充质组织,如平滑肌细胞和 SOX9 表达细胞的排列以及 (食管特异性)、 (呼吸道器官特异性)和 (远端支气管特异性)的表达所表明的。间充质衍生信号对 AFG 上皮特化的早期阶段的影响已被指出。我们的研究表明了一种相反的趋势,即上皮组织特化导致间充质组织的一致变化,表明上皮-间充质相互作用的相互性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb18/7044460/3034b19c497d/biolopen-9-048728-g1.jpg

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