BMP4 substitutes for loss of BMP7 during kidney development

Leif Oxburgh; Andrew T. Dudley; Robert E. Godin; Chad H. Koonce; Ayesha Islam; Dorian C. Anderson; Elizabeth K. Bikoff; Elizabeth J. Robertson

doi:10.1016/j.ydbio.2005.08.024

BMP4 substitutes for loss of BMP7 during kidney development

Leif Oxburgh, Andrew T. Dudley, Robert E. Godin, Chad H. Koonce, Ayesha Islam, Dorian C. Anderson, Elizabeth K. Bikoff, Elizabeth J. Robertson

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

63 Scopus citations

Abstract

Functional inactivation of divergent bone morphogenetic proteins (BMPs) causes discrete disturbances during mouse development. BMP4-deficient embryos display mesodermal patterning defects at early post-implantation stages, whereas loss of BMP7 selectively disrupts kidney and eye morphogenesis. Whether these distinct phenotypes simply reflect differences in expression domains, or alternatively intrinsic differences in the signaling properties of these ligands remains unknown. To address this issue, we created embryos exclusively expressing BMP4 under control of the BMP7 locus. Surprisingly, this novel knock-in allele efficiently rescues kidney development. These results demonstrate unequivocally that these structurally divergent BMP family members, sharing only minimal sequence similarity can function interchangeably to activate all the essential signaling pathways for growth and morphogenesis of the kidney. Thus, we conclude that partially overlapping expression patterns of BMPs serve to modulate strength of BMP signaling rather than create discrete fields of ligands with intrinsically different signaling properties.

Original language	English (US)
Pages (from-to)	637-646
Number of pages	10
Journal	Developmental Biology
Volume	286
Issue number	2
DOIs	https://doi.org/10.1016/j.ydbio.2005.08.024
State	Published - Oct 15 2005
Externally published	Yes

Keywords

BMP
Bone morphogenetic protein
Kidney development

ASJC Scopus subject areas

Molecular Biology
Developmental Biology
Cell Biology

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10.1016/j.ydbio.2005.08.024

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title = "BMP4 substitutes for loss of BMP7 during kidney development",

abstract = "Functional inactivation of divergent bone morphogenetic proteins (BMPs) causes discrete disturbances during mouse development. BMP4-deficient embryos display mesodermal patterning defects at early post-implantation stages, whereas loss of BMP7 selectively disrupts kidney and eye morphogenesis. Whether these distinct phenotypes simply reflect differences in expression domains, or alternatively intrinsic differences in the signaling properties of these ligands remains unknown. To address this issue, we created embryos exclusively expressing BMP4 under control of the BMP7 locus. Surprisingly, this novel knock-in allele efficiently rescues kidney development. These results demonstrate unequivocally that these structurally divergent BMP family members, sharing only minimal sequence similarity can function interchangeably to activate all the essential signaling pathways for growth and morphogenesis of the kidney. Thus, we conclude that partially overlapping expression patterns of BMPs serve to modulate strength of BMP signaling rather than create discrete fields of ligands with intrinsically different signaling properties.",

keywords = "BMP, Bone morphogenetic protein, Kidney development",

author = "Leif Oxburgh and Dudley, {Andrew T.} and Godin, {Robert E.} and Koonce, {Chad H.} and Ayesha Islam and Anderson, {Dorian C.} and Bikoff, {Elizabeth K.} and Robertson, {Elizabeth J.}",

note = "Funding Information: We would like to thank Debbie Pelusi for genotyping assistance and Drs Daniel Constam and Ray Dunn for insightful comments on the work. L. O. was supported by a fellowship from the Wenner-Gren Foundation. This work was supported by a grant from the NIH to E. J. R. ",

year = "2005",

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day = "15",

doi = "10.1016/j.ydbio.2005.08.024",

language = "English (US)",

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AU - Oxburgh, Leif

AU - Dudley, Andrew T.

AU - Godin, Robert E.

AU - Koonce, Chad H.

AU - Islam, Ayesha

AU - Anderson, Dorian C.

AU - Bikoff, Elizabeth K.

AU - Robertson, Elizabeth J.

N1 - Funding Information: We would like to thank Debbie Pelusi for genotyping assistance and Drs Daniel Constam and Ray Dunn for insightful comments on the work. L. O. was supported by a fellowship from the Wenner-Gren Foundation. This work was supported by a grant from the NIH to E. J. R.

PY - 2005/10/15

Y1 - 2005/10/15

N2 - Functional inactivation of divergent bone morphogenetic proteins (BMPs) causes discrete disturbances during mouse development. BMP4-deficient embryos display mesodermal patterning defects at early post-implantation stages, whereas loss of BMP7 selectively disrupts kidney and eye morphogenesis. Whether these distinct phenotypes simply reflect differences in expression domains, or alternatively intrinsic differences in the signaling properties of these ligands remains unknown. To address this issue, we created embryos exclusively expressing BMP4 under control of the BMP7 locus. Surprisingly, this novel knock-in allele efficiently rescues kidney development. These results demonstrate unequivocally that these structurally divergent BMP family members, sharing only minimal sequence similarity can function interchangeably to activate all the essential signaling pathways for growth and morphogenesis of the kidney. Thus, we conclude that partially overlapping expression patterns of BMPs serve to modulate strength of BMP signaling rather than create discrete fields of ligands with intrinsically different signaling properties.

AB - Functional inactivation of divergent bone morphogenetic proteins (BMPs) causes discrete disturbances during mouse development. BMP4-deficient embryos display mesodermal patterning defects at early post-implantation stages, whereas loss of BMP7 selectively disrupts kidney and eye morphogenesis. Whether these distinct phenotypes simply reflect differences in expression domains, or alternatively intrinsic differences in the signaling properties of these ligands remains unknown. To address this issue, we created embryos exclusively expressing BMP4 under control of the BMP7 locus. Surprisingly, this novel knock-in allele efficiently rescues kidney development. These results demonstrate unequivocally that these structurally divergent BMP family members, sharing only minimal sequence similarity can function interchangeably to activate all the essential signaling pathways for growth and morphogenesis of the kidney. Thus, we conclude that partially overlapping expression patterns of BMPs serve to modulate strength of BMP signaling rather than create discrete fields of ligands with intrinsically different signaling properties.

KW - BMP

KW - Bone morphogenetic protein

KW - Kidney development

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BMP4 substitutes for loss of BMP7 during kidney development

Abstract

Keywords

ASJC Scopus subject areas

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