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research article

Additive and global functions of HoxA cluster genes in mesoderm derivatives

Di-Poï, Nicolas
•
Koch, Ute  
•
Radtke, Freddy  
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2010
Developmental biology

Hox genes encode transcription factors that play a central role in the specification of regional identities along the anterior to posterior body axis. In the developing mouse embryo, Hox genes from all four genomic clusters are involved in range of developmental processes, including the patterning of skeletal structures and the formation of several organs. However, the functional redundancy observed either between paralogous genes, or among neighboring genes from the same cluster, has hampered functional analyses, in particular when synergistic, cluster-specific functions are considered. Here, we report that mutant mice lacking the entire HoxA cluster in mesodermal lineages display the expected spectrum of postnatal respiratory, cardiac and urogenital defects, previously reported for single gene mutations. Likewise, mild phenotypes are observed in both appendicular and axial skeleton. However, a striking effect was uncovered in the hematopoietic system, much stronger than that seen for Hoxa9 inactivation alone, which involves stem cells (HSCs) as well as the erythroid lineage, indicating that several Hoxa genes are necessary for normal hematopoiesis to occur. Finally, the combined deletions of Hoxa and Hoxd genes reveal abnormalities in axial elongation as well as skin morphogenesis that are likely the results of defects in epithelial-mesenchymal interactions.

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Type
research article
DOI
10.1016/j.ydbio.2010.03.006
Web of Science ID

WOS:000277404300013

Author(s)
Di-Poï, Nicolas
Koch, Ute  
Radtke, Freddy  
Duboule, Denis  
Date Issued

2010

Publisher

Elsevier

Published in
Developmental biology
Volume

341

Issue

2

Start page

488

End page

98

Subjects

HoxA

•

HoxD

•

Mesoderm

•

Hematopoiesis

•

Skeleton

•

Organs

•

Skin

•

Hematopoietic Stem-Cells

•

Homeobox Genes

•

Mutant Mice

•

Homeotic Transformations

•

Targeted Disruptions

•

Myeloid-Leukemia

•

Limb Development

•

Axial Skeleton

•

Nervous-System

•

Body Plan

Editorial or Peer reviewed

NON-REVIEWED

Written at

EPFL

EPFL units
UPDUB  
UPRAD  
Available on Infoscience
July 22, 2010
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/51821
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