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首页> 外文期刊>Mechanisms of Development >Hox cluster polarity in early transcriptional availability: a high order regulatory level of clustered Hox genes in the mouse
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Hox cluster polarity in early transcriptional availability: a high order regulatory level of clustered Hox genes in the mouse

机译:早期转录可用性中的Hox簇极性:小鼠中簇状Hox基因的高水平调控水平

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摘要

The molecular mechanism underlying the 3' to 5' polarity of induction of mouse Hox genes is still elusive. While relief from a cluster-encompassing repression was shown to lead to all Hoxd genes being expressed like the 3' most of them, Hoxd1 (Kondoand Duboule, 1999), the molecular basis of initial activation of this 3' most gene, is not understood yet. We show that, already before primitive streak formation, prior to initial expression of the first Hox gene, a dramatic transcriptional stimulationof the 3' most genes, Hoxb1 and Hoxb2, is observed upon a short pulse of exogenous retinoic acid (RA), whereas it is not in the case for more 5', cluster-internal, RA-responsive Hoxb genes. In contrast, the RA-responding Hoxb1lacZ transgene that faithfully mimics the endogenous gene (Marshall et al., 1994) did not exhibit the sensitivity of Hoxb1 to precocious activation. We conclude that polarity in initial activation of Hoxb genes reflects a greater availability of 3' Hox genes for transcription, suggesting a pre-existing (susceptibility to) opening of the chromatin structure at the 3' extremity of the cluster. We discuss the data in the context of prevailing models involving differential chromatin opening in the directionality of clustered Hox genetranscription, and regarding the importance of the cluster context for correct timing of initial Hox gene expression. Interestingly, Cdx1 manifested the same early transcriptional availability as Hoxb1.
机译:诱导小鼠Hox基因3'到5'极性的分子机制仍然难以捉摸。尽管从包围簇的抑制中的缓解显示导致所有Hoxd基因都像它们中的大多数3'一样被表达,但人们并不了解Hoxd1(Kondoand Duboule,1999),这是该3'最多数基因的初始激活的分子基础。然而。我们显示,在原始条纹形成之前,在第一个Hox基因的初始表达之前,在短时间的外源视黄酸(RA)脉冲中观察到了3'大多数基因Hoxb1和Hoxb2的戏剧性转录刺激,而对于更多的5',内部簇,RA反应性Hoxb基因则不是这种情况。相反,忠实地模拟内源基因的RA响应Hoxb1lacZ转基因(Marshall等,1994)没有表现出Hoxb1对性早熟的敏感性。我们得出的结论是,Hoxb基因的初始激活中的极性反映了3'Hox基因转录的更大可用性,这表明在簇3'末端的染色质结构开放(存在)。我们讨论了在流行的模型的上下文中的数据,这些模型涉及在成簇的Hox基因转录的方向性上的差异染色质开放,以及关于集群上下文对于初始Hox基因表达正确时机的重要性。有趣的是,Cdx1表现出与Hoxb1相同的早期转录可用性。

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