TY - JOUR
T1 - Exploring the effects of gene dosage on mandible shape in mice as a model for studying the genetic basis of natural variation
AU - Boell, Louis
AU - Pallares, Luisa F.
AU - Brodski, Claude
AU - Chen, Yiping
AU - Christian, Jan L.
AU - Kousa, Youssef A.
AU - Kuss, Pia
AU - Nelsen, Sylvia
AU - Novikov, Orna
AU - Schutte, Brian C.
AU - Wang, Ying
AU - Tautz, Diethard
N1 - Funding Information: Acknowledgments The authors are indebted to Christine Pfeifle and Heike Harre for their help with mouse breeding. The work was funded by institutional resources of the Max-Planck Society to DT. Financial support to BCS (#DE13513) and YAK (#1F31DE022696-01) came from the NIH National Institute of Dental and Craniofacial Research. Financial support to CB came from the Israel Science Foundation (grant no. 1391/11). LFP is a member of the International Max Planck Research School (IMPRS) for Evolutionary Biology.
PY - 2013/9/1
Y1 - 2013/9/1
N2 - Mandible shape in the mouse is a complex trait that is influenced by many genetic factors. However, little is known about the action of single genes on adult mandible shape so far, since most developmentally relevant genes are already required during embryogenesis, i.e., knockouts lead to embryonic death or severe deformations, before the mandible is fully formed. We employ here a geometric morphometric approach to identify subtle phenotypic differences caused by dosage effects of candidate genes. We use mouse strains with specific gene modifications (knockouts and knockins) to compare heterozygous animals with controls from the same stock, which is expected to be equivalent to a change of gene expression of the respective locus. Such differences in expression level are also likely to occur as part of the natural variation. We focus on Bmp pathway genes (Bmp4, its antagonist Noggin, and combinations of Bmp5-7 genotypes), but include also two other developmental control genes suspected to affect mandible development in some way (Egfr and Irf6). In addition, we study the effects of Hoxd13, as well as an extracellular matrix constituent (Col2a1). We find that subtle but significant shape differences are caused by differences in gene dosage of several of these genes. The changes seen for Bmp4 and Noggin are partially compatible with the action of these genes known from birds and fish. We find significant shape changes also for Hoxd13, although this gene has so far only been implicated in skeletal patterning processes of the limbs. Comparing the effect sizes of gene dosage changes to the variation found in natural populations of mice as well as quantitative trait loci (QTL) effects on mandible shape, we find that the effect sizes caused by gene dosage changes are at the lower end of the spectrum of natural variation, but larger than the average additive effects found in QTL studies. We conclude that studying gene dosage effects have the potential to provide new insights into aspects of craniofacial development, variation, and evolution.
AB - Mandible shape in the mouse is a complex trait that is influenced by many genetic factors. However, little is known about the action of single genes on adult mandible shape so far, since most developmentally relevant genes are already required during embryogenesis, i.e., knockouts lead to embryonic death or severe deformations, before the mandible is fully formed. We employ here a geometric morphometric approach to identify subtle phenotypic differences caused by dosage effects of candidate genes. We use mouse strains with specific gene modifications (knockouts and knockins) to compare heterozygous animals with controls from the same stock, which is expected to be equivalent to a change of gene expression of the respective locus. Such differences in expression level are also likely to occur as part of the natural variation. We focus on Bmp pathway genes (Bmp4, its antagonist Noggin, and combinations of Bmp5-7 genotypes), but include also two other developmental control genes suspected to affect mandible development in some way (Egfr and Irf6). In addition, we study the effects of Hoxd13, as well as an extracellular matrix constituent (Col2a1). We find that subtle but significant shape differences are caused by differences in gene dosage of several of these genes. The changes seen for Bmp4 and Noggin are partially compatible with the action of these genes known from birds and fish. We find significant shape changes also for Hoxd13, although this gene has so far only been implicated in skeletal patterning processes of the limbs. Comparing the effect sizes of gene dosage changes to the variation found in natural populations of mice as well as quantitative trait loci (QTL) effects on mandible shape, we find that the effect sizes caused by gene dosage changes are at the lower end of the spectrum of natural variation, but larger than the average additive effects found in QTL studies. We conclude that studying gene dosage effects have the potential to provide new insights into aspects of craniofacial development, variation, and evolution.
KW - Dosage effects
KW - Mandible development
KW - Morphometry
KW - Mus musculus
KW - Shape analysis
UR - http://www.scopus.com/inward/record.url?scp=84882830825&partnerID=8YFLogxK
U2 - https://doi.org/10.1007/s00427-013-0443-y
DO - https://doi.org/10.1007/s00427-013-0443-y
M3 - Article
SN - 0949-944X
VL - 223
SP - 279
EP - 287
JO - Development Genes and Evolution
JF - Development Genes and Evolution
IS - 5
ER -