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Series GSE110614 Query DataSets for GSE110614
Status Public on Dec 03, 2019
Title Coronary arterial development is regulated by a Dll4-Jag1-EphrinB2 signaling cascade
Organism Mus musculus
Experiment type Expression profiling by high throughput sequencing
Summary Coronaries are essential for myocardial growth and heart function. Notch is crucial for mouse embryonic angiogenesis, but its role in coronary development remains uncertain. We show Jag1, Dll4 and activated Notch1 receptor expression in sinus venosus (SV) endocardium. Endocardial Jag1 removal blocks SV capillary sprouting, while Dll4 inactivation stimulates excessive capillary growth, suggesting that ligand antagonism regulates coronary primary plexus formation. Later endothelial ligand removal, or forced expression of Dll4 or the glycosyltransferase MFng, blocks coronary plexus remodeling, arterial differentiation, and perivascular cell maturation. Endocardial deletion of Efnb2 phenocopies the coronary arterial defects of Notch mutants. Angiogenic rescue experiments in ventricular explants, or in primary human endothelial cells, indicate that EphrinB2 is a critical effector of antagonistic Dll4 and Jag1 functions in arterial morphogenesis. Thus, coronary arterial precursors are specified in the SV prior to primary coronary plexus formation and subsequent arterial differentiation depends on a Dll4-Jag1-EphrinB2 signaling cascade.




 
Overall design RNA was isolated at E12.5, from whole hearts, for WT (4 replicate samples, pooling 4 embryos) and Jag1flox;Nfatc1-Cre embryos(4 replicate samples, pooling 4 embryos), and for WT (4 replicate samples, pooling 4 embryos) and Dll4flox;Nfatc1-Cre (4 replicate samples, pooling 4 embryos). It was isolated at E15.5, from heart ventricles, for WT (4 replicate samples, pooling 3 embryos) and Dll4flox; Cdh5(PAC)-CreERT (3 replicate samples, pooling 3 embryos) and for WT (4 replicate samples, pooling 3 embryos) and Dll4GOF;Tie2-Cre (3 replicate samples, pooling 3 embryos). Finally, it was isolated at E16.5, from heart ventricles, for WT (4 replicate samples, from one embryo) and Efnb2flox;Nfatc1-Cre (4 replicate samples, from one embryo).
 
Contributor(s) Travisano SI, MacGrogan D, Pompa JL
Citation(s) 31789590
Submission date Feb 14, 2018
Last update date Sep 08, 2022
Contact name Jose Luis de la Pompa
E-mail(s) jlpompa@cnic.es
Organization name Centro Nacional de Investigaciones Cardiovasculares Carlos III (CNIC).
Lab Intercellular Signalling in Cardiovascular Development & Disease
Street address Melchor Fernández Almagro 3
City Madrid
ZIP/Postal code 28029
Country Spain
 
Platforms (1)
GPL17021 Illumina HiSeq 2500 (Mus musculus)
Samples (36)
GSM3004185 J1Pan_KO1
GSM3004186 J1Pan_KO2
GSM3004187 J1Pan_KO3
Relations
BioProject PRJNA434109
SRA SRP132873

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE110614_D4Gof_matrix_table.xls.gz 1.0 Mb (ftp)(http) XLS
GSE110614_D4Pan_matrix_table.xls.gz 954.2 Kb (ftp)(http) XLS
GSE110614_D4VE_matrix_table.xls.gz 1021.9 Kb (ftp)(http) XLS
GSE110614_Epb2_matrix_table.xls.gz 1.1 Mb (ftp)(http) XLS
GSE110614_Jag1Pan_matrix_table.xls.gz 1.2 Mb (ftp)(http) XLS
SRA Run SelectorHelp
Raw data are available in SRA
Processed data are available on Series record

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