Nkx2-5 pathways and congenital heart disease: Loss of ventricular myocyte lineage specification leads to progressive cardiomyopathy and complete heart block

Mohammad Pashmforoush; Jonathan T. Lu; Hanying Chen; Tara St. Amand; Richard Kondo; Sylvain Pradervand; Sylvia M. Evans; Bob Clark; James R. Feramisco; Wayne Giles; Siew Yen Ho; D. Woodrow Benson; Michael Silberbach; Weinian Shou; Kenneth R. Chien

doi:10.1016/S0092-8674(04)00405-2

Nkx2-5 pathways and congenital heart disease: Loss of ventricular myocyte lineage specification leads to progressive cardiomyopathy and complete heart block

Mohammad Pashmforoush, Jonathan T. Lu, Hanying Chen, Tara St. Amand, Richard Kondo, Sylvain Pradervand, Sylvia M. Evans, Bob Clark, James R. Feramisco, Wayne Giles, Siew Yen Ho, D. Woodrow Benson, Michael Silberbach, Weinian Shou, Kenneth R. Chien

Pediatrics

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

367 Scopus citations

Abstract

Human mutations in Nkx2-5 lead to progressive cardiomyopathy and conduction defects via unknown mechanisms. To define these pathways, we generated mice with a ventricular-restricted knockout of Nkx2-5, which display no structural defects but have progressive complete heart block, and massive trabecular muscle overgrowth found in some patients with Nkx2-5 mutations. At birth, mutant mice display a hypoplastic atrioventricular (AV) node and then develop selective dropout of these conduction cells. Transcriptional profiling uncovered the aberrant expression of a unique panel of atrial and conduction system-restricted target genes, as well as the ectopic, high level BMP-10 expression in the adult ventricular myocardium. Further, BMP-10 is shown to be necessary and sufficient for a major component of the ventricular muscle defects. Accordingly, loss of ventricular muscle cell lineage specification into trabecular and conduction system myocytes is a new mechanistic pathway for progressive cardiomyopathy and conduction defects in congenital heart disease.

Original language	English (US)
Pages (from-to)	373-386
Number of pages	14
Journal	Cell
Volume	117
Issue number	3
DOIs	https://doi.org/10.1016/S0092-8674(04)00405-2
State	Published - Apr 30 2004

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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Pashmforoush, M., Lu, J. T., Chen, H., St. Amand, T., Kondo, R., Pradervand, S., Evans, S. M., Clark, B., Feramisco, J. R., Giles, W., Ho, S. Y., Benson, D. W., Silberbach, M., Shou, W., & Chien, K. R. (2004). Nkx2-5 pathways and congenital heart disease: Loss of ventricular myocyte lineage specification leads to progressive cardiomyopathy and complete heart block. Cell, 117(3), 373-386. https://doi.org/10.1016/S0092-8674(04)00405-2

Pashmforoush, M, Lu, JT, Chen, H, St. Amand, T, Kondo, R, Pradervand, S, Evans, SM, Clark, B, Feramisco, JR, Giles, W, Ho, SY, Benson, DW, Silberbach, M, Shou, W & Chien, KR 2004, 'Nkx2-5 pathways and congenital heart disease: Loss of ventricular myocyte lineage specification leads to progressive cardiomyopathy and complete heart block', Cell, vol. 117, no. 3, pp. 373-386. https://doi.org/10.1016/S0092-8674(04)00405-2

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title = "Nkx2-5 pathways and congenital heart disease: Loss of ventricular myocyte lineage specification leads to progressive cardiomyopathy and complete heart block",

abstract = "Human mutations in Nkx2-5 lead to progressive cardiomyopathy and conduction defects via unknown mechanisms. To define these pathways, we generated mice with a ventricular-restricted knockout of Nkx2-5, which display no structural defects but have progressive complete heart block, and massive trabecular muscle overgrowth found in some patients with Nkx2-5 mutations. At birth, mutant mice display a hypoplastic atrioventricular (AV) node and then develop selective dropout of these conduction cells. Transcriptional profiling uncovered the aberrant expression of a unique panel of atrial and conduction system-restricted target genes, as well as the ectopic, high level BMP-10 expression in the adult ventricular myocardium. Further, BMP-10 is shown to be necessary and sufficient for a major component of the ventricular muscle defects. Accordingly, loss of ventricular muscle cell lineage specification into trabecular and conduction system myocytes is a new mechanistic pathway for progressive cardiomyopathy and conduction defects in congenital heart disease.",

author = "Mohammad Pashmforoush and Lu, {Jonathan T.} and Hanying Chen and {St. Amand}, Tara and Richard Kondo and Sylvain Pradervand and Evans, {Sylvia M.} and Bob Clark and Feramisco, {James R.} and Wayne Giles and Ho, {Siew Yen} and Benson, {D. Woodrow} and Michael Silberbach and Weinian Shou and Chien, {Kenneth R.}",

note = "Funding Information: We wish to thank Cameron Christman from the San Diego Supercomputer Center for his help with the 3D reconstruction of the AVN. We thank Stephen McMullen from Cancer Center for his excellent assistance with microscopy, Sabina Kupershmidt and Dan Roden for mink-LacZ mice. Julie Anderson and Kim Weldy provided excellent maintenance of the mouse colony. Masa Hoshijima, Yibing Qyang, and Ju Chen provided help with the preparation and critical reading of this manuscript. This work was supported by funding from the NHLBI.",

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AU - Lu, Jonathan T.

AU - Chen, Hanying

AU - St. Amand, Tara

AU - Kondo, Richard

AU - Pradervand, Sylvain

AU - Evans, Sylvia M.

AU - Clark, Bob

AU - Feramisco, James R.

AU - Giles, Wayne

AU - Ho, Siew Yen

AU - Benson, D. Woodrow

AU - Silberbach, Michael

AU - Shou, Weinian

AU - Chien, Kenneth R.

N1 - Funding Information: We wish to thank Cameron Christman from the San Diego Supercomputer Center for his help with the 3D reconstruction of the AVN. We thank Stephen McMullen from Cancer Center for his excellent assistance with microscopy, Sabina Kupershmidt and Dan Roden for mink-LacZ mice. Julie Anderson and Kim Weldy provided excellent maintenance of the mouse colony. Masa Hoshijima, Yibing Qyang, and Ju Chen provided help with the preparation and critical reading of this manuscript. This work was supported by funding from the NHLBI.

PY - 2004/4/30

Y1 - 2004/4/30

N2 - Human mutations in Nkx2-5 lead to progressive cardiomyopathy and conduction defects via unknown mechanisms. To define these pathways, we generated mice with a ventricular-restricted knockout of Nkx2-5, which display no structural defects but have progressive complete heart block, and massive trabecular muscle overgrowth found in some patients with Nkx2-5 mutations. At birth, mutant mice display a hypoplastic atrioventricular (AV) node and then develop selective dropout of these conduction cells. Transcriptional profiling uncovered the aberrant expression of a unique panel of atrial and conduction system-restricted target genes, as well as the ectopic, high level BMP-10 expression in the adult ventricular myocardium. Further, BMP-10 is shown to be necessary and sufficient for a major component of the ventricular muscle defects. Accordingly, loss of ventricular muscle cell lineage specification into trabecular and conduction system myocytes is a new mechanistic pathway for progressive cardiomyopathy and conduction defects in congenital heart disease.

AB - Human mutations in Nkx2-5 lead to progressive cardiomyopathy and conduction defects via unknown mechanisms. To define these pathways, we generated mice with a ventricular-restricted knockout of Nkx2-5, which display no structural defects but have progressive complete heart block, and massive trabecular muscle overgrowth found in some patients with Nkx2-5 mutations. At birth, mutant mice display a hypoplastic atrioventricular (AV) node and then develop selective dropout of these conduction cells. Transcriptional profiling uncovered the aberrant expression of a unique panel of atrial and conduction system-restricted target genes, as well as the ectopic, high level BMP-10 expression in the adult ventricular myocardium. Further, BMP-10 is shown to be necessary and sufficient for a major component of the ventricular muscle defects. Accordingly, loss of ventricular muscle cell lineage specification into trabecular and conduction system myocytes is a new mechanistic pathway for progressive cardiomyopathy and conduction defects in congenital heart disease.

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Nkx2-5 pathways and congenital heart disease: Loss of ventricular myocyte lineage specification leads to progressive cardiomyopathy and complete heart block

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