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Retinol dehydrogenase 10 is a feedback regulator of retinoic acid signalling during axis formation and patterning of the central nervous system.

机译:视黄醇脱氢酶10是在轴形成和中枢神经系统图案化期间视黄酸信号传导的反馈调节剂。

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摘要

Retinoic acid (RA) is an important morphogen that regulates many biological processes, including the development of the central nervous system (CNS). Its synthesis from vitamin A (retinol) occurs in two steps, with the second reaction - catalyzed by retinal dehydrogenases (RALDHs) - long considered to be crucial for tissue-specific RA production in the embryo. We have recently identified the Xenopus homologue of retinol dehydrogenase 10 (XRDH10) that mediates the first step in RA synthesis from retinol to retinal. XRDH10 is specifically expressed in the dorsal blastopore lip and in other domains of the early embryo that partially overlap with XRALDH2 expression. We show that endogenous RA suppresses XRDH10 gene expression, suggesting negative-feedback regulation. In mRNA-injected Xenopus embryos, XRDH10 mimicked RA responses, influenced the gene expression of organizer markers, and synergized with XRALDH2 in posteriorizing the developing brain. Knockdown of XRDH10 and XRALDH2 by specific antisense morpholino oligonucleotides had the opposite effects on organizer gene expression, and caused a ventralized phenotype and anteriorization of the brain. These data indicate that the conversion of retinol into retinal is a developmentally controlled step involved in specification of the dorsoventral and anteroposterior body axes, as well as in pattern formation of the CNS. We suggest that the combinatorial gene expression and concerted action of XRDH10 and XRALDH2 constitute a ;biosynthetic enzyme code' for the establishment of a morphogen gradient in the embryo.
机译:维甲酸(RA)是重要的形态发生素,可调节许多生物过程,包括中枢神经系统(CNS)的发育。它由维生素A(视黄醇)合成分为两个步骤,第二个反应-视网膜脱氢酶(RALDHs)催化-长期以来被认为对胚胎中组织特异性RA的产生至关重要。我们最近确定了视黄醇脱氢酶10(XRDH10)的非洲爪蟾同源物,介导了从视黄醇到视网膜的RA合成的第一步。 XRDH10特异地在背胚芽孔唇和早期胚胎中与XRALDH2表达部分重叠的其他域中表达。我们显示内源性RA抑制XRDH10基因表达,提示负反馈调节。在注射了mRNA的非洲爪蟾胚胎中,XRDH10模仿RA反应,影响组织标志物的基因表达,并与XRALDH2协同作用,使发育中的脑部恶化。特定的反义吗啉代寡核苷酸敲低XRDH10和XRALDH2对组织基因的表达具有相反的作用,并导致腹侧表型和大脑前位化。这些数据表明,视黄醇向视网膜的转化是发育受控的步骤,涉及背腹和前后体轴的规范以及中枢神经系统的模式形成。我们建议,XRDH10和XRALDH2的组合基因表达和协同作用构成了一个“生物合成酶代码”,用于在胚胎中建立形态发生子梯度。

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