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一项动态表达调查确定了与小鼠消化道发育相关的转录因子。

A dynamic expression survey identifies transcription factors relevant in mouse digestive tract development.

作者信息

Choi Michael Y, Romer Anthony I, Hu Michael, Lepourcelet Maina, Mechoor Ambili, Yesilaltay Ayce, Krieger Monty, Gray Paul A, Shivdasani Ramesh A

机构信息

Dana-Farber Cancer Institute, 44 Binney Street, Boston, MA 02115, USA.

出版信息

Development. 2006 Oct;133(20):4119-29. doi: 10.1242/dev.02537. Epub 2006 Sep 13.

DOI:10.1242/dev.02537
PMID:16971476
Abstract

Tissue-restricted transcription factors (TFs), which confer specialized cellular properties, are usually identified through sequence homology or cis-element analysis of lineage-specific genes; conventional modes of mRNA profiling often fail to report non-abundant TF transcripts. We evaluated the dynamic expression during mouse gut organogenesis of 1381 transcripts, covering nearly every known and predicted TF, and documented the expression of approximately 1000 TF genes in gastrointestinal development. Despite distinctive structures and functions, the stomach and intestine exhibit limited differences in TF genes. Among differentially expressed transcripts, a few are virtually restricted to the digestive tract, including Nr2e3, previously regarded as a photoreceptor-specific product. TFs that are enriched in digestive organs commonly serve essential tissue-specific functions, hence justifying a search for other tissue-restricted TFs. Computational data mining and experimental investigation focused interest on a novel homeobox TF, Isx, which appears selectively in gut epithelium and mirrors expression of the intestinal TF Cdx2. Isx-deficient mice carry a specific defect in intestinal gene expression: dysregulation of the high density lipoprotein (HDL) receptor and cholesterol transporter scavenger receptor class B, type I (Scarb1). Thus, integration of developmental gene expression with biological assessment, as described here for TFs, represents a powerful tool to investigate control of tissue differentiation.

摘要

赋予细胞特殊性质的组织限制性转录因子(TFs)通常是通过对谱系特异性基因进行序列同源性分析或顺式元件分析来鉴定的;传统的mRNA分析模式往往无法检测到低丰度的TF转录本。我们评估了1381个转录本在小鼠肠道器官发生过程中的动态表达,这些转录本几乎涵盖了所有已知和预测的TF,并记录了大约1000个TF基因在胃肠道发育中的表达情况。尽管胃和肠具有不同的结构和功能,但它们在TF基因方面的差异有限。在差异表达的转录本中,有一些实际上仅限于消化道,包括Nr2e3,它以前被认为是光感受器特异性产物。在消化器官中富集的TF通常具有重要的组织特异性功能,因此有理由寻找其他组织限制性TF。通过计算数据挖掘和实验研究,人们将兴趣集中在一种新型的同源盒TF——Isx上,它选择性地出现在肠道上皮中,并且反映了肠道TF Cdx2的表达。Isx基因敲除小鼠在肠道基因表达方面存在特定缺陷:高密度脂蛋白(HDL)受体和胆固醇转运蛋白B类I型清道夫受体(Scarb1)的表达失调。因此,如本文针对TFs所描述的,将发育基因表达与生物学评估相结合,是研究组织分化调控的有力工具。

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