TY - JOUR
T1 - BMP7 acts in murine lens placode development
AU - Wawersik, Stefan
AU - Purcell, Patricia
AU - Rauchman, Michael
AU - Dudley, Andrew T.
AU - Robertson, Elizabeth J.
AU - Maas, Richard
N1 - Funding Information:
We thank Drs. Andrew Lassar, Andrew McMahon, and Mark Mercola and members of the Maas lab for critical comments on this work, and Drs. Yasuhide Furuta and Brigid Hogan for sharing results prior to publication. We also thank Dr. Gerard Karsenty for providing an additional independent Bmp7 mutant allele. We are also grateful to Drs. Claudio Basilico, Andrew McMahon, A. F. Parlow, Forbes Porter, and Kuber Sampath for providing us with reagents. This work was supported by a grant from the NIH (EY10123) to R.M.
PY - 1999/3/1
Y1 - 1999/3/1
N2 - Targeted inactivation of the Bmp7 gene in mouse leads to eye defects with late onset and variable penetrance (A. T. Dudley et al., 1995, Genes Dev. 9, 2795-2807; G. Luo et al., 1995, Genes Dev. 9, 2808-2820). Here we report that the expressivity of the Bmp7 mutant phenotype markedly increases in a C3H/He genetic background and that the phenotype implicates Bmp7 in the early stages of lens development. Immunolocalization experiments show that BMP7 protein is present in the head ectoderm at the time of lens placode induction. Using an in vitro culture system, we demonstrate that addition of BMP7 antagonists during the period of lens placode induction inhibits lens formation, indicating a role for BMP7 in lens placode development. Next, to integrate Bmp7 into a developmental pathway controlling formation of the lens placode, we examined the expression of several early lens placode-specific markers in Bmp7 mutant embryos. In these embryos, Pax6 head ectoderm expression is lost just prior to the time when the lens placode should appear, while in Pax6-deficient (Sey/Sey) embryos, Bmp7 expression is maintained. These results could suggest a simple linear pathway in placode induction in which Bmp7 functions upstream of Pax6 and regulates lens placode induction. At odds with this interpretation, however, is the finding that expression of secreted Frizzled Related Protein-2 (sFRP-2), a component of the Wnt signaling pathway which is expressed in prospective lens placode, is absent in Sey/Sey embryos but initially present in Bmp7 mutants. This suggests a different model in which Bmp7 function is required to maintain Pax6 expression after induction, during a preplacodal stage of lens development. We conclude that Bmp7 is a critical component of the genetic mechanism(s) controlling lens placode formation.
AB - Targeted inactivation of the Bmp7 gene in mouse leads to eye defects with late onset and variable penetrance (A. T. Dudley et al., 1995, Genes Dev. 9, 2795-2807; G. Luo et al., 1995, Genes Dev. 9, 2808-2820). Here we report that the expressivity of the Bmp7 mutant phenotype markedly increases in a C3H/He genetic background and that the phenotype implicates Bmp7 in the early stages of lens development. Immunolocalization experiments show that BMP7 protein is present in the head ectoderm at the time of lens placode induction. Using an in vitro culture system, we demonstrate that addition of BMP7 antagonists during the period of lens placode induction inhibits lens formation, indicating a role for BMP7 in lens placode development. Next, to integrate Bmp7 into a developmental pathway controlling formation of the lens placode, we examined the expression of several early lens placode-specific markers in Bmp7 mutant embryos. In these embryos, Pax6 head ectoderm expression is lost just prior to the time when the lens placode should appear, while in Pax6-deficient (Sey/Sey) embryos, Bmp7 expression is maintained. These results could suggest a simple linear pathway in placode induction in which Bmp7 functions upstream of Pax6 and regulates lens placode induction. At odds with this interpretation, however, is the finding that expression of secreted Frizzled Related Protein-2 (sFRP-2), a component of the Wnt signaling pathway which is expressed in prospective lens placode, is absent in Sey/Sey embryos but initially present in Bmp7 mutants. This suggests a different model in which Bmp7 function is required to maintain Pax6 expression after induction, during a preplacodal stage of lens development. We conclude that Bmp7 is a critical component of the genetic mechanism(s) controlling lens placode formation.
KW - Bmp7
KW - Eye development
KW - Lens placode
KW - Pax6
UR - http://www.scopus.com/inward/record.url?scp=0033105981&partnerID=8YFLogxK
U2 - 10.1006/dbio.1998.9153
DO - 10.1006/dbio.1998.9153
M3 - Article
C2 - 10049573
AN - SCOPUS:0033105981
SN - 0012-1606
VL - 207
SP - 176
EP - 188
JO - Developmental Biology
JF - Developmental Biology
IS - 1
ER -