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视黄酸改变后脑Hox编码,并诱导菱脑节2/3转变为4/5身份。

Retinoic acid alters hindbrain Hox code and induces transformation of rhombomeres 2/3 into a 4/5 identity.

作者信息

Marshall H, Nonchev S, Sham M H, Muchamore I, Lumsden A, Krumlauf R

机构信息

MRC Laboratory of Eukaryotic Molecular Genetics, National Institute for Medical Research, Mill Hill, London, UK.

出版信息

Nature. 1992;360(6406):737-41. doi: 10.1038/360737a0.

Abstract

It has been suggested that Hox genes play an important part in the patterning of limbs, vertebrae and craniofacial structures by providing an ordered molecular system of positional values, termed the Hox code. Little is known about the nature of the signals that govern the establishment and regulation of Hox genes, but retinoic acid can affect the expression of these genes in cell lines and in embryonic tissues. On the basis of experimental and clinical evidence, the hindbrain and branchial region of the head are particularly sensitive to the effects of retinoic acid but the phenotypes are complex and hard to interpret, and how and if they relate to Hox expression has not been clear. Here we follow the changes induced by retinoic acid to hindbrain segmentation and the branchial arches using transgenic mice which contain lacZ reporter genes that reveal the endogenous segment-restricted expression of the Hox-B1 (Hox-2.9), Hox-B2(Hox-2.8) and Krox-20 genes. Our results show that these genes rapidly respond to exposure to retinoic acid at preheadfold stages and undergo a progressive series of changes in segmental expression that are associated with specific phenotypes in hindbrain of first branchial arch. Together the molecular and anatomical alterations indicate that retinoic acid has induced changes in the hindbrain Hox code which result in the homeotic transformation of rhombomeres (r) 2/3 to an r4/5 identity. A main feature of this rhombomeric phenotype is that the trigeminal motor nerve is transformed to a facial identity. Furthermore, in support of this change in rhombomeric identity, neural crest cells derived from r2/3 also express posterior Hox markers suggesting that the retinoic acid-induced transformation extends to multiple components of the first branchial arch.

摘要

有人提出,Hox基因通过提供一个有序的位置值分子系统(称为Hox编码),在肢体、椎骨和颅面结构的模式形成中发挥重要作用。关于控制Hox基因建立和调控的信号的性质知之甚少,但视黄酸可以影响这些基因在细胞系和胚胎组织中的表达。基于实验和临床证据,后脑和头部的鳃区对视黄酸的作用特别敏感,但表型复杂且难以解释,它们与Hox表达的关系以及是否相关尚不清楚。在这里,我们利用含有lacZ报告基因的转基因小鼠,追踪视黄酸诱导的后脑节段化和鳃弓的变化,这些报告基因揭示了Hox-B1(Hox-2.9)、Hox-B2(Hox-2.8)和Krox-20基因的内源性节段限制性表达。我们的结果表明,这些基因在头褶前期迅速对视黄酸暴露作出反应,并在节段表达中经历一系列渐进变化,这些变化与第一鳃弓后脑的特定表型相关。分子和解剖学改变共同表明,视黄酸诱导了后脑Hox编码的变化,导致菱脑节(r)2/3向r4/5身份的同源转化。这种菱脑节表型的一个主要特征是三叉运动神经转化为面神经身份。此外,为了支持这种菱脑节身份的变化,来自r2/3的神经嵴细胞也表达后部Hox标记,这表明视黄酸诱导的转化延伸到第一鳃弓的多个组成部分。

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