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不同同源域 DNA 结合特异性对果蝇胚胎中胚层细胞特异性基因表达程序的贡献。

Contribution of distinct homeodomain DNA binding specificities to Drosophila embryonic mesodermal cell-specific gene expression programs.

机构信息

Laboratory of Developmental Systems Biology, National Heart Lung and Blood Institute, National Institutes of Health, Bethesda, Maryland, United States of America.

出版信息

PLoS One. 2013 Jul 26;8(7):e69385. doi: 10.1371/journal.pone.0069385. Print 2013.

Abstract

Homeodomain (HD) proteins are a large family of evolutionarily conserved transcription factors (TFs) having diverse developmental functions, often acting within the same cell types, yet many members of this family paradoxically recognize similar DNA sequences. Thus, with multiple family members having the potential to recognize the same DNA sequences in cis-regulatory elements, it is difficult to ascertain the role of an individual HD or a subclass of HDs in mediating a particular developmental function. To investigate this problem, we focused our studies on the Drosophila embryonic mesoderm where HD TFs are required to establish not only segmental identities (such as the Hox TFs), but also tissue and cell fate specification and differentiation (such as the NK-2 HDs, Six HDs and identity HDs (I-HDs)). Here we utilized the complete spectrum of DNA binding specificities determined by protein binding microarrays (PBMs) for a diverse collection of HDs to modify the nucleotide sequences of numerous mesodermal enhancers to be recognized by either no or a single subclass of HDs, and subsequently assayed the consequences of these changes on enhancer function in transgenic reporter assays. These studies show that individual mesodermal enhancers receive separate transcriptional input from both I-HD and Hox subclasses of HDs. In addition, we demonstrate that enhancers regulating upstream components of the mesodermal regulatory network are targeted by the Six class of HDs. Finally, we establish the necessity of NK-2 HD binding sequences to activate gene expression in multiple mesodermal tissues, supporting a potential role for the NK-2 HD TF Tinman (Tin) as a pioneer factor that cooperates with other factors to regulate cell-specific gene expression programs. Collectively, these results underscore the critical role played by HDs of multiple subclasses in inducing the unique genetic programs of individual mesodermal cells, and in coordinating the gene regulatory networks directing mesoderm development.

摘要

同源结构域(HD)蛋白是一个进化上保守的转录因子(TF)大家族,具有多种发育功能,通常在同一细胞类型中发挥作用,但这个家族的许多成员却出人意料地识别相似的 DNA 序列。因此,多个家族成员有可能识别顺式调控元件中相同的 DNA 序列,因此很难确定单个 HD 或 HD 子类在介导特定发育功能中的作用。为了解决这个问题,我们将研究重点放在果蝇胚胎中胚层上,在那里 HD TF 不仅需要建立节段性身份(如 Hox TF),还需要组织和细胞命运特化和分化(如 NK-2 HD、Six HD 和身份 HD(I-HD))。在这里,我们利用蛋白结合微阵列(PBMs)确定的各种 HD 的完整 DNA 结合特异性谱,修饰许多中胚层增强子的核苷酸序列,使其被无或单个 HD 子类识别,然后在转基因报告基因检测中检测这些变化对增强子功能的影响。这些研究表明,单个中胚层增强子从 I-HD 和 Hox 子类的 HD 接收单独的转录输入。此外,我们证明了调节中胚层调控网络上游成分的增强子被 Six 类 HD 靶向。最后,我们确定了 NK-2 HD 结合序列激活多个中胚层组织中基因表达的必要性,支持 NK-2 HD TF Tinman(Tin)作为与其他因子合作调节细胞特异性基因表达程序的先驱因子的潜在作用。总之,这些结果强调了多个子类的 HD 在诱导单个中胚层细胞独特的遗传程序以及协调指导中胚层发育的基因调控网络方面发挥的关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aca5/3724861/b0f0d6948a66/pone.0069385.g001.jpg

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