Requirement for Twist1 in frontonasal and skull vault development in the mouse embryo

Heidi Bildsoe; David A.F. Loebel; Vanessa J. Jones; You Tzung Chen; Richard R. Behringer; Patrick P.L. Tam

doi:10.1016/j.ydbio.2009.04.034

Requirement for Twist1 in frontonasal and skull vault development in the mouse embryo

Heidi Bildsoe, David A.F. Loebel, Vanessa J. Jones, You Tzung Chen, Richard R. Behringer, Patrick P.L. Tam

Genetics

Research output: Contribution to journal › Article › peer-review

76 Scopus citations

Abstract

Using a Cre-mediated conditional deletion approach, we have dissected the function of Twist1 in the morphogenesis of the craniofacial skeleton. Loss of Twist1 in neural crest cells and their derivatives impairs skeletogenic differentiation and leads to the loss of bones of the snout, upper face and skull vault. While no anatomically recognizable maxilla is formed, a malformed mandible is present. Since Twist1 is expressed in the tissues of the maxillary eminence and the mandibular arch, this finding suggests that the requirement for Twist1 is not the same in all neural crest derivatives. The effect of the loss of Twist1 function is not restricted to neural crest-derived bones, since the predominantly mesoderm-derived parietal and interparietal bones are also affected, presumably as a consequence of lost interactions with neural crest-derived tissues. In contrast, the formation of other mesodermal skeletal derivatives such as the occipital bones and most of the chondrocranium are not affected by the loss of Twist1 in the neural crest cells.

Original language	English (US)
Pages (from-to)	176-188
Number of pages	13
Journal	Developmental Biology
Volume	331
Issue number	2
DOIs	https://doi.org/10.1016/j.ydbio.2009.04.034
State	Published - Jul 15 2009

Keywords

Craniofacial morphogenesis
Cre
Neural crest cells
Skeletal development
Twist1
loxP

ASJC Scopus subject areas

Molecular Biology
Developmental Biology
Cell Biology

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10.1016/j.ydbio.2009.04.034

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title = "Requirement for Twist1 in frontonasal and skull vault development in the mouse embryo",

abstract = "Using a Cre-mediated conditional deletion approach, we have dissected the function of Twist1 in the morphogenesis of the craniofacial skeleton. Loss of Twist1 in neural crest cells and their derivatives impairs skeletogenic differentiation and leads to the loss of bones of the snout, upper face and skull vault. While no anatomically recognizable maxilla is formed, a malformed mandible is present. Since Twist1 is expressed in the tissues of the maxillary eminence and the mandibular arch, this finding suggests that the requirement for Twist1 is not the same in all neural crest derivatives. The effect of the loss of Twist1 function is not restricted to neural crest-derived bones, since the predominantly mesoderm-derived parietal and interparietal bones are also affected, presumably as a consequence of lost interactions with neural crest-derived tissues. In contrast, the formation of other mesodermal skeletal derivatives such as the occipital bones and most of the chondrocranium are not affected by the loss of Twist1 in the neural crest cells.",

keywords = "Craniofacial morphogenesis, Cre, Neural crest cells, Skeletal development, Twist1, loxP",

author = "Heidi Bildsoe and Loebel, {David A.F.} and Jones, {Vanessa J.} and Chen, {You Tzung} and Behringer, {Richard R.} and Tam, {Patrick P.L.}",

note = "Funding Information: We thank Robyn Jamieson for advice on the interpretation of the eye phenotype, Christine Smyth for assistance with image analysis, the CMRI BioServices Facility for maintaining the mouse stocks, Sylvie Dufor for the gift of HtPA-Cre mice and Graham Kay for the Tyr-Cre mice. Clones for riboprobe production were provided by: Fritz Meijlink (Alx3, Alx 4 and Cart1); Jen Kuei Liu (Dlx5); Gail Martin (Fgf8 and Fgf10); Vassillis Pachnis (Lhx7); Murray Hargrave (Sox10); John Rubenstein (Dlx2); Yi-Hsin Liu (Msx2); Eric Olson (Twist2); and Bill Shawlot (Twist1). Our work is supported by Mr. James Fairfax. HB is a University of Sydney and CMRI Postgraduate Scholar. DAFL is a Kimberly-Clark Research Fellow and PPLT is a Senior Principal Research Fellow of the NHMRC of Australia. ",

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AU - Jones, Vanessa J.

AU - Chen, You Tzung

AU - Behringer, Richard R.

AU - Tam, Patrick P.L.

N1 - Funding Information: We thank Robyn Jamieson for advice on the interpretation of the eye phenotype, Christine Smyth for assistance with image analysis, the CMRI BioServices Facility for maintaining the mouse stocks, Sylvie Dufor for the gift of HtPA-Cre mice and Graham Kay for the Tyr-Cre mice. Clones for riboprobe production were provided by: Fritz Meijlink (Alx3, Alx 4 and Cart1); Jen Kuei Liu (Dlx5); Gail Martin (Fgf8 and Fgf10); Vassillis Pachnis (Lhx7); Murray Hargrave (Sox10); John Rubenstein (Dlx2); Yi-Hsin Liu (Msx2); Eric Olson (Twist2); and Bill Shawlot (Twist1). Our work is supported by Mr. James Fairfax. HB is a University of Sydney and CMRI Postgraduate Scholar. DAFL is a Kimberly-Clark Research Fellow and PPLT is a Senior Principal Research Fellow of the NHMRC of Australia.

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N2 - Using a Cre-mediated conditional deletion approach, we have dissected the function of Twist1 in the morphogenesis of the craniofacial skeleton. Loss of Twist1 in neural crest cells and their derivatives impairs skeletogenic differentiation and leads to the loss of bones of the snout, upper face and skull vault. While no anatomically recognizable maxilla is formed, a malformed mandible is present. Since Twist1 is expressed in the tissues of the maxillary eminence and the mandibular arch, this finding suggests that the requirement for Twist1 is not the same in all neural crest derivatives. The effect of the loss of Twist1 function is not restricted to neural crest-derived bones, since the predominantly mesoderm-derived parietal and interparietal bones are also affected, presumably as a consequence of lost interactions with neural crest-derived tissues. In contrast, the formation of other mesodermal skeletal derivatives such as the occipital bones and most of the chondrocranium are not affected by the loss of Twist1 in the neural crest cells.

AB - Using a Cre-mediated conditional deletion approach, we have dissected the function of Twist1 in the morphogenesis of the craniofacial skeleton. Loss of Twist1 in neural crest cells and their derivatives impairs skeletogenic differentiation and leads to the loss of bones of the snout, upper face and skull vault. While no anatomically recognizable maxilla is formed, a malformed mandible is present. Since Twist1 is expressed in the tissues of the maxillary eminence and the mandibular arch, this finding suggests that the requirement for Twist1 is not the same in all neural crest derivatives. The effect of the loss of Twist1 function is not restricted to neural crest-derived bones, since the predominantly mesoderm-derived parietal and interparietal bones are also affected, presumably as a consequence of lost interactions with neural crest-derived tissues. In contrast, the formation of other mesodermal skeletal derivatives such as the occipital bones and most of the chondrocranium are not affected by the loss of Twist1 in the neural crest cells.

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KW - Skeletal development

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KW - loxP

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Requirement for Twist1 in frontonasal and skull vault development in the mouse embryo

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Keywords

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