Enhancer timing of Hox gene expression: deletion of the endogenous Hoxc8 early enhancer

doi:10.1242/dev.00672

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First published online 13 August 2003
doi: 10.1242/dev.00672

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Development 130, 4823-4834 (2003)
Copyright © 2003 The Company of Biologists Limited

Enhancer timing of Hox gene expression: deletion of the endogenous Hoxc8 early enhancer

Aster H. Juan and Frank H. Ruddle^*

Department of Molecular, Cellular, and Developmental Biology, Yale University, New Haven, CT 06520, USA

^* Author for correspondence (e-mail: frank.ruddle{at}yale.edu)

Accepted 13 June 2003

The proper expression of Hox genes is necessary for the accuratepatterning of the body plan. The elucidation of the developmentalgenetic basis of transcriptional regulation of Hox genes bythe study of their cis-regulatory elements provides crucialinformation regarding the establishment of axial specification.In this report, we investigate the role of the early enhancer (EE)of the murine Hoxc8 gene to better understand its role in patternformation. Previous reports show that knockouts of the endogenous Hoxc8coding region result in a combination of neural, behavioraland skeletal phenotypes. In this report, we limit ourselvesto a consideration of the skeletal abnormalities. Early reportsfrom our laboratory based on exogenous transgenic reporter constructsimplicate a 200 bp non-coding element 3 kb upstream of the Hoxc8promoter as a crucial enhancer that regulates the transcriptionof Hoxc8. In the present work, we have deleted this regulatoryregion from the endogenous genome using embryonic stem celltechnology. Our results show that the deletion of the EE resultsin a significant delay in the temporal expression of Hoxc8.We also show that the deletion of the EE does not eliminatethe expression of the Hoxc8 protein, but delays the attainmentof control levels of expression and anterior and posterior boundariesof expression on the AP axis. The temporal delay in Hoxc8 expressionis sufficient to produce phenocopies of many of the axial skeletaldefects associated with the complete absence of Hoxc8 gene productas previously reported for the Hoxc8-null mutation. Our resultsare consistent with emerging evidence that the precise temporalexpression of Hox genes is crucial for the establishment ofregional identities. The fact that the EE deletion does noteliminate Hoxc8 expression indicates the existence of a Hoxc8transcriptional regulatory apparatus independent to some degreeof the Hoxc8 EE. In a comparison of our results with those reportedpreviously by others investigating temporal control of Hox geneexpression, we have discovered a structural similarity betweenthe Hoxc8 EE reported here and a transcriptional control elementlocated in the Hoxd11 region. We speculate that a distributedsystem of expression timing control may exist that is similarthe one we propose for Hoxc8. Last, our data is consistent withthe position that disparate regulatory pathways are responsiblefor the expression of Hoxc8 in the organogenesis of somites,neural tube and limb bud.

Key words: Enhancer, Hoxc8, Gene regulation, Mouse

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