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Series GSE528 Query DataSets for GSE528
Status Public on Jul 13, 2003
Title NK2 model of congenital heart disease
Organism Mus musculus
Experiment type Expression profiling by array
Summary Lack of the conserved NK2-domain of the cardiac transcription factor Nkx2.5 causes multiple heart defects .

The NK2 family of homeobox genes constitutes a family of transcription factors that play an important role in different developmental processes. Members of this group are characterized by two highly conserved protein domains: the homeodomain, conferring DNA binding activity, and the NK2-specific domain (NK2-SD) of yet unknown function. One of the best characterized members of this group is the early cardiogenic marker Nkx2.5. Loss of function of Nkx2.5 leads to embryonic lethality around E10.5 due to an arrest of heart development at the looping stage. We have further dissected the function of Nkx2.5 in vivo by creating a knockout mouse line harboring an in frame deletion of the NK2-SD by Cre/loxP mediated excision. Homozygous mutant mice die at E14.5 due to severe cardiac malformations, e.g. common AV canal, DORV, and VSD. Lack of the NK2-SD leads to downregulation of the ventricular markers MLC-2v and Irx4 specifically in the right ventricle, and is accompanied with reduced right ventricular function. This function of Nkx2.5 seems to be independent of its ability to bind target DNA, since lack of the NK2-SD does not alter the DNA binding activity of Csx/Nkx2.5 in vitro. Heterozygous mutant mice show a spectrum of cardiac defects related to cardiac septation and valve morphogenesis, but lack conduction system defects as reported for heterozygous Nkx2.5 mice. The phenotype observed in NK2-SD mutant mice shows that Nkx2.5 is not only crucial during early steps of cardiogenesis but also plays an important role at later developmental stages.

Embryos were isolated at embryonic day 12.5. The entire embryo heart was taken and isolated in ice-cold PBS and immediately frozen on dry-ice. Total RNA was extracted from pooled samples of wildtype, heterozygous and mutant embryos.
Keywords = congenital heart disease, Csx, Nkx2.5
Keywords: other
 
 
Contributor(s) Schinke M, Riggi LE, Chen I, Izumo S
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Submission date Jul 11, 2003
Last update date Jul 08, 2016
Contact name Martina Schinke
URL http://www.cardiogenomics.org
Organization name Harvard University
Department Bauer Center for Genomic Research
Lab Cardiogenomics
Street address 7 Divinity Ave
City Cambridge
State/province MA
ZIP/Postal code 02138
Country USA
 
Platforms (2)
GPL75 [Mu11KsubA] Affymetrix Murine 11K SubA Array
GPL76 [Mu11KsubB] Affymetrix Murine 11K SubB Array
Samples (26)
GSM7760 PGA-Nk2-sd_het_12A-m4
GSM7761 PGA-Nk2-sd_het_5A-m4
GSM7762 PGA-Nk2-sd_het_6A-m4
Relations
BioProject PRJNA85533

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