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  4. Notch1 is essential for postnatal hair follicle development and homeostasis
 
research article

Notch1 is essential for postnatal hair follicle development and homeostasis

Vauclair, S.
•
Nicolas, M.  
•
Barrandon, Y.  
Show more
2005
Developmental Biology

Notch genes encode evolutionarily conserved large, single transmembrane receptors, which regulate many cell fate decisions and differentiation processes during fetal and postnatal life. Multiple Notch receptors and ligands are expressed in both developing and adult epidermis and hair follicles. Proliferation and differentiation of these two ectodermal-derived structures have been proposed to be controlled in part by the Notch pathway. Whether Notch signaling is involved in postnatal hair homeostasis is currently unknown. Here, we investigate and compare the role of the Notch1 receptor during embryonic hair follicle development and postnatal hair homeostasis using Cre-loxP based tissue specific and inducible loss-of-function approaches. During embryonic development, tissue-specific ablation of Notch1 does not perturb formation and patterning of hair follicle placodes. However, Notch1 deficient hair follicles invaginate prematurely into the dermis. Embryonic as well as postnatal inactivation of Notch1 shortly after birth or in adult mice results in almost complete hair loss followed by cyst formation. The first hair cycle of Notch1 deficient mice is characterized by shortened anagen and a premature entry into catagen. These data show that Notch1 is essential for late stages of hair follicle development during embryogenesis as well as for post-natal hair follicle development and hair homeostasis.

  • Details
  • Metrics
Type
research article
DOI
10.1016/j.ydbio.2005.05.018
Web of Science ID

WOS:000231352800015

PubMed ID

15978571

Author(s)
Vauclair, S.
Nicolas, M.  
Barrandon, Y.  
Radtke, F.  
Date Issued

2005

Published in
Developmental Biology
Volume

284

Issue

1

Start page

184

End page

93

Subjects

Animals

•

Comparative Study

•

DNA Primers

•

Gene Deletion

•

Hair Follicle/embryology/*growth & development/metabolism/ultrastructure

•

Immunohistochemistry

•

In Situ Hybridization

•

Integrases

•

Mice

•

Microscopy

•

Electron

•

Scanning

•

Polymerase Chain Reaction

•

Receptor

•

Notch1/*metabolism

•

Research Support

•

Non-U.S. Gov't

•

Signal Transduction/*physiology

•

beta-Galactosidase

Note

Ludwig Institute for Cancer Research, Lausanne Branch, University of Lausanne, 1066 Epalinges, Switzerland.

Journal Article

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
UPRAD  
Available on Infoscience
December 5, 2006
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/237332
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