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转录因子同源物通过与多个共因子的上下文相关合作来协调替代基因调控网络。

Transcription factor paralogs orchestrate alternative gene regulatory networks by context-dependent cooperation with multiple cofactors.

机构信息

Department of Biochemistry and Molecular Biophysics, Columbia University, New York, NY, USA.

Mortimer B. Zuckerman Mind Brain Behavior Institute, Columbia University, New York, NY, USA.

出版信息

Nat Commun. 2022 Jul 1;13(1):3808. doi: 10.1038/s41467-022-31501-2.

Abstract

In eukaryotes, members of transcription factor families often exhibit similar DNA binding properties in vitro, yet orchestrate paralog-specific gene regulatory networks in vivo. The serially homologous first (T1) and third (T3) thoracic legs of Drosophila, which are specified by the Hox proteins Scr and Ubx, respectively, offer a unique opportunity to address this paradox in vivo. Genome-wide analyses using epitope-tagged alleles of both Hox loci in the T1 and T3 leg imaginal discs, the precursors to the adult legs and ventral body regions, show that ~8% of Hox binding is paralog-specific. Binding specificity is mediated by interactions with distinct cofactors in different domains: the Hox cofactor Exd acts in the proximal domain and is necessary for Scr to bind many of its paralog-specific targets, while in the distal leg domain, the homeodomain protein Distal-less (Dll) enhances Scr binding to a different subset of loci. These findings reveal how Hox paralogs, and perhaps paralogs of other transcription factor families, orchestrate alternative downstream gene regulatory networks with the help of multiple, context-specific cofactors.

摘要

在真核生物中,转录因子家族的成员通常在体外表现出相似的 DNA 结合特性,但在体内却调控着特定于旁系同源基因的调控网络。果蝇的串联同源的第一(T1)和第三(T3)胸腿,分别由 Hox 蛋白 Scr 和 Ubx 决定,这为在体内解决这一悖论提供了独特的机会。使用 Hox 基因座的表位标记等位基因在 T1 和 T3 腿的 imaginal 盘(成虫腿和腹部区域的前体)中进行全基因组分析,显示约 8%的 Hox 结合是旁系同源特异性的。结合特异性由不同结构域中的不同共因子相互作用介导:Hox 共因子 Exd 在近端结构域中起作用,是 Scr 结合其许多旁系同源特异性靶标的必要条件,而在远端腿结构域中,同源域蛋白 Distal-less (Dll) 增强了 Scr 对不同亚群基因座的结合。这些发现揭示了 Hox 旁系同源物,以及其他转录因子家族的旁系同源物,如何在多个特定于上下文的共因子的帮助下,协调替代的下游基因调控网络。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/21a7/9249852/24dc5e49b85e/41467_2022_31501_Fig1_HTML.jpg

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