Epithelial and ectomesenchymal role of the type I TGF-beta receptor ALK5 during facial morphogenesis and palatal fusion

Dudas, Marek; Kim, Jieun; Li, Wai-Yee; Nagy, Andre; Larsson, Jonas; Karlsson, Stefan; Chai, Yang; Kaartinen, Vesa

Epithelial and ectomesenchymal role of the type I TGF-beta receptor ALK5 during facial morphogenesis and palatal fusion

Mark

Dudas, Marek ; Kim, Jieun ; Li, Wai-Yee ; Nagy, Andre ; Larsson, Jonas ^LU ; Karlsson, Stefan ^LU

; Chai, Yang and Kaartinen, Vesa (2006) In Developmental Biology 296(2). p.298-314

Abstract: Transforming growth factor beta (TGF-beta) proteins play important roles in morphogenesis of many cramofacial tissues; however, detailed biological mechanisms of TGF-beta action, particularly in vivo, are still poorly understood. Here, we deleted the TGF-beta type I receptor gene Alk5 specifically in the embryonic ectodermal and neural crest cell lineages. Failure in signaling via this receptor, either in the epithelium or in the mesenchyme, caused severe craniofacial defects including cleft palate. Moreover, the facial phenotypes of neural crest-specific Alk5 mutants included devastating facial cleft and appeared significantly more severe than the defects seen in corresponding mutants lacking the TGF-beta type II receptor (TGF beta II), a... (More); Transforming growth factor beta (TGF-beta) proteins play important roles in morphogenesis of many cramofacial tissues; however, detailed biological mechanisms of TGF-beta action, particularly in vivo, are still poorly understood. Here, we deleted the TGF-beta type I receptor gene Alk5 specifically in the embryonic ectodermal and neural crest cell lineages. Failure in signaling via this receptor, either in the epithelium or in the mesenchyme, caused severe craniofacial defects including cleft palate. Moreover, the facial phenotypes of neural crest-specific Alk5 mutants included devastating facial cleft and appeared significantly more severe than the defects seen in corresponding mutants lacking the TGF-beta type II receptor (TGF beta II), a prototypical binding partner of ALK5. Our data indicate that ALK5 plays unique, non-redundant cell-autonomous roles during facial development. Remarkable divergence between Tgfbr2 and A1k5 phenotypes, together with our biochemical in vitro data, imply that (1) ALK5 mediates signaling of a diverse set of ligands not limited to the three isoforms of TGF-beta, and (2) ALK5 acts also in conjunction with type II receptors other than TGF beta RII. (c) 2006 Elsevier Inc. All rights reserved. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/395240

author

Dudas, Marek ; Kim, Jieun ; Li, Wai-Yee ; Nagy, Andre ; Larsson, Jonas ^LU ; Karlsson, Stefan ^LU

; Chai, Yang and Kaartinen, Vesa

organization

Division of Molecular Medicine and Gene Therapy

publishing date

2006

type

Contribution to journal

publication status

published

subject

Hematology

keywords

mandible, malformation, craniofacial, cranial neural crest, cleft palate, ALK5, cleft face, palatal fusion

in

Developmental Biology

volume

296

issue

2

pages

298 - 314

publisher

Elsevier

external identifiers

pmid:16806156
wos:000239980200002
scopus:33747078200
pmid:16806156

ISSN

1095-564X

DOI

10.1016/j.ydbio.2006.05.030

language

English

LU publication?

yes

id

3581fbbe-cd47-4ac5-a978-d197f4e7a08b (old id 395240)

date added to LUP

2016-04-01 11:56:22

date last changed

2022-03-20 21:06:31

@article{3581fbbe-cd47-4ac5-a978-d197f4e7a08b,
  abstract     = {{Transforming growth factor beta (TGF-beta) proteins play important roles in morphogenesis of many cramofacial tissues; however, detailed biological mechanisms of TGF-beta action, particularly in vivo, are still poorly understood. Here, we deleted the TGF-beta type I receptor gene Alk5 specifically in the embryonic ectodermal and neural crest cell lineages. Failure in signaling via this receptor, either in the epithelium or in the mesenchyme, caused severe craniofacial defects including cleft palate. Moreover, the facial phenotypes of neural crest-specific Alk5 mutants included devastating facial cleft and appeared significantly more severe than the defects seen in corresponding mutants lacking the TGF-beta type II receptor (TGF beta II), a prototypical binding partner of ALK5. Our data indicate that ALK5 plays unique, non-redundant cell-autonomous roles during facial development. Remarkable divergence between Tgfbr2 and A1k5 phenotypes, together with our biochemical in vitro data, imply that (1) ALK5 mediates signaling of a diverse set of ligands not limited to the three isoforms of TGF-beta, and (2) ALK5 acts also in conjunction with type II receptors other than TGF beta RII. (c) 2006 Elsevier Inc. All rights reserved.}},
  author       = {{Dudas, Marek and Kim, Jieun and Li, Wai-Yee and Nagy, Andre and Larsson, Jonas and Karlsson, Stefan and Chai, Yang and Kaartinen, Vesa}},
  issn         = {{1095-564X}},
  keywords     = {{mandible; malformation; craniofacial; cranial neural crest; cleft palate; ALK5; cleft face; palatal fusion}},
  language     = {{eng}},
  number       = {{2}},
  pages        = {{298--314}},
  publisher    = {{Elsevier}},
  series       = {{Developmental Biology}},
  title        = {{Epithelial and ectomesenchymal role of the type I TGF-beta receptor ALK5 during facial morphogenesis and palatal fusion}},
  url          = {{http://dx.doi.org/10.1016/j.ydbio.2006.05.030}},
  doi          = {{10.1016/j.ydbio.2006.05.030}},
  volume       = {{296}},
  year         = {{2006}},
}

Lund University Publications

LUND UNIVERSITY LIBRARIES

Epithelial and ectomesenchymal role of the type I TGF-beta receptor ALK5 during facial morphogenesis and palatal fusion