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Bop1 对于颅面组织前体细胞结构域的形成是必需的。

Bop1 is required to establish precursor domains of craniofacial tissues.

机构信息

Department of Anatomy and Cell Biology, George Washington University, School of Medicine and Health Sciences, Washington, District of Columbia, USA.

Department of Veterinary and Animal Sciences, University of Massachusetts, Amherst, Massachusetts, USA.

出版信息

Genesis. 2024 Feb;62(1):e23580. doi: 10.1002/dvg.23580. Epub 2023 Nov 16.

Abstract

Bop1 can promote cell proliferation and is a component of the Pes1-Bop1-WDR12 (PeBoW) complex that regulates ribosomal RNA processing and biogenesis. In embryos, however, bop1 mRNA is highly enriched in the neural plate, cranial neural crest and placodes, and potentially may interact with Six1, which also is expressed in these tissues. Recent work demonstrated that during development, Bop1 is required for establishing the size of the tadpole brain, retina and cranial cartilages, as well as controlling neural tissue gene expression levels. Herein, we extend this work by assessing the effects of Bop1 knockdown at neural plate and larval stages. Loss of Bop1 expanded neural plate gene expression domains (sox2, sox11, irx1) and reduced neural crest (foxd3, sox9), placode (six1, sox11, irx1, sox9) and epidermal (dlx5) expression domains. At larval stages, Bop1 knockdown reduced the expression of several otic vesicle genes (six1, pax2, irx1, sox9, dlx5, otx2, tbx1) and branchial arch genes that are required for chondrogenesis (sox9, tbx1, dlx5). The latter was not the result of impaired neural crest migration. Together these observations indicate that Bop1 is a multifunctional protein that in addition to its well-known role in ribosomal biogenesis functions during early development to establish the craniofacial precursor domains.

摘要

Bop1 可以促进细胞增殖,是 Pes1-Bop1-WDR12(PeBoW)复合物的组成部分,该复合物调节核糖体 RNA 的加工和生物发生。然而,在胚胎中,bop1mRNA 在神经板、颅神经嵴和基板中高度富集,并且可能与 Six1 相互作用,Six1 也在这些组织中表达。最近的工作表明,在发育过程中,Bop1 对于建立蝌蚪脑、视网膜和颅软骨的大小以及控制神经组织基因表达水平是必需的。在此,我们通过评估神经板和幼虫阶段 Bop1 敲低的影响来扩展这项工作。Bop1 的缺失扩大了神经板基因表达域(sox2、sox11、irx1),并减少了神经嵴(foxd3、sox9)、基板(six1、sox11、irx1、sox9)和表皮(dlx5)表达域。在幼虫阶段,Bop1 敲低降低了几个耳泡基因(six1、pax2、irx1、sox9、dlx5、otx2、tbx1)和鳃弓基因(sox9、tbx1、dlx5)的表达,这些基因对于软骨发生是必需的。后者不是由于神经嵴迁移受损所致。这些观察结果表明,Bop1 是一种多功能蛋白,除了其在核糖体生物发生中的已知作用外,还在早期发育过程中发挥作用,以建立颅面前体域。

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