Samarut Eric, Gaudin Cyril, Hughes Sandrine, Gillet Benjamin, de Bernard Simon, Jouve Pierre-Emmanuel, Buffat Laurent, Allot Alexis, Lecompte Odile, Berekelya Liubov, Rochette-Egly Cécile, Laudet Vincent
Institut de Génomique Fonctionnelle de Lyon (E.S., C.G., S.H., B.G., L.B., V.L.), Université de Lyon, Université Lyon 1, Centre National de la Recherche Scientifique (CNRS), Ecole Normale Supérieure de Lyon, 69364 Lyon Cedex 07, France; Institut de Génétique et de Biologie Moléculaire et Cellulaire (E.S., A.A., O.L., C.R.-E.), Institut National de la Sante et de la Recherche Medicale, U596, CNRS, UMR7104, Université de Strasbourg, BP 10142, 67404 Illkirch Cedex, France.; and AltraBio SAS (S.B., P.-E.J., L.B.), Lyon, France.
Mol Endocrinol. 2014 Feb;28(2):260-72. doi: 10.1210/me.2013-1358. Epub 2014 Jan 9.
Retinoic acid (RA) controls many aspects of embryonic development by binding to specific receptors (retinoic acid receptors [RARs]) that regulate complex transcriptional networks. Three different RAR subtypes are present in vertebrates and play both common and specific roles in transducing RA signaling. Specific activities of each receptor subtype can be correlated with its exclusive expression pattern, whereas shared activities between different subtypes are generally assimilated to functional redundancy. However, the question remains whether some subtype-specific activity still exists in regions or organs coexpressing multiple RAR subtypes. We tackled this issue at the transcriptional level using early zebrafish embryo as a model. Using morpholino knockdown, we specifically invalidated the zebrafish endogenous RAR subtypes in an in vivo context. After building up a list of RA-responsive genes in the zebrafish gastrula through a whole-transcriptome analysis, we compared this panel of genes with those that still respond to RA in embryos lacking one or another RAR subtype. Our work reveals that RAR subtypes do not have fully redundant functions at the transcriptional level but can transduce RA signal in a subtype-specific fashion. As a result, we define RAR subtype-specific transcriptotypes that correspond to repertoires of genes activated by different RAR subtypes. Finally, we found genes of the RA pathway (cyp26a1, raraa) the regulation of which by RA is highly robust and can even resist the knockdown of all RARs. This suggests that RA-responsive genes are differentially sensitive to alterations in the RA pathway and, in particular, cyp26a1 and raraa are under a high pressure to maintain signaling integrity.
维甲酸(RA)通过与调节复杂转录网络的特定受体(维甲酸受体 [RARs])结合来控制胚胎发育的许多方面。脊椎动物中存在三种不同的RAR亚型,它们在转导RA信号中发挥着共同和特定的作用。每个受体亚型的特定活性与其独特的表达模式相关,而不同亚型之间的共同活性通常被认为是功能冗余。然而,在共表达多种RAR亚型的区域或器官中是否仍存在一些亚型特异性活性的问题仍然存在。我们以早期斑马鱼胚胎为模型,在转录水平上解决了这个问题。通过吗啉代敲低,我们在体内特异性地使斑马鱼内源性RAR亚型失活。通过全转录组分析建立斑马鱼原肠胚中RA反应基因列表后,我们将这组基因与在缺乏一种或另一种RAR亚型的胚胎中仍对RA有反应的基因进行了比较。我们的工作表明,RAR亚型在转录水平上没有完全冗余的功能,而是可以以亚型特异性的方式转导RA信号。因此,我们定义了与不同RAR亚型激活的基因库相对应的RAR亚型特异性转录组。最后,我们发现RA途径的基因(cyp26a1、raraa),其受RA的调控非常稳健,甚至可以抵抗所有RAR的敲低。这表明RA反应基因对RA途径的改变具有不同的敏感性,特别是cyp26a1和raraa在维持信号完整性方面面临着很大的压力。