TY - JOUR
T1 - Transgenic analysis of the atrialnatriuretic factor (ANF) promoter
T2 - Nkx2-5 and GATA-4 binding sites are required for atrial specific expression of ANF
AU - Small, Eric M.
AU - Krieg, Paul A.
N1 - Funding Information:
We thank Mike King for providing the Xenopus genomic library, Tim Mohun and Branko Latinkic for technical assistance with transgenesis methods and valuable discussions, and Steve Vokes and Jessica Wandelt for comments on the manuscript. P.A.K. is the Allan C. Hudson and Helen Lovaas Endowed Professor of the Sarver Heart Center at the University of Arizona College of Medicine. This work was supported by the Sarver Heart Center and by the NHLBI of the NIH, Grant HL63926 (to P.A.K.).
PY - 2003/9/1
Y1 - 2003/9/1
N2 - The atrial natriuretic factor (ANF) gene is initially expressed throughout the myocardial layer of the heart, but during subsequent development, expression becomes limited to the atrial chambers. Mouse knockout and mammalian cell culture studies have shown that the ANF gene is regulated by combinatorial interactions between Nkx2-5, GATA-4, Tbx5, and SRF; however, the molecular mechanisms leading to chamber-specific expression are currently unknown. We have isolated the Xenopus ANF promoter in order to examine the temporal and spatial regulation of the ANF gene in vivo using transgenic embryos. The mammalian and Xenopus ANF promoters show remarkable sequence similarity, including an Nkx2-5 binding site (NKE), two GATA sites, a T-box binding site (TBE), and two SRF binding sites (SREs). Our transgenic studies show that mutation of either SRE, the TBE or the distal GATA element, strongly reduces expression from the ANF promoter. However, mutations of the NKE, the proximal GATA, or both elements together, result in relatively minor reductions in transgene expression within the myocardium. Surprisingly, mutation of these elements results in ectopic ANF promoter activity in the kidneys, facial muscles, and aortic arch artery-associated muscles, and causes persistent expression in the ventricle and outflow tract of the heart. We propose that the NKE and proximal GATA elements serve as crucial binding sites for assembly of a repressor complex that is required for atrial-specific expression of the ANF gene.
AB - The atrial natriuretic factor (ANF) gene is initially expressed throughout the myocardial layer of the heart, but during subsequent development, expression becomes limited to the atrial chambers. Mouse knockout and mammalian cell culture studies have shown that the ANF gene is regulated by combinatorial interactions between Nkx2-5, GATA-4, Tbx5, and SRF; however, the molecular mechanisms leading to chamber-specific expression are currently unknown. We have isolated the Xenopus ANF promoter in order to examine the temporal and spatial regulation of the ANF gene in vivo using transgenic embryos. The mammalian and Xenopus ANF promoters show remarkable sequence similarity, including an Nkx2-5 binding site (NKE), two GATA sites, a T-box binding site (TBE), and two SRF binding sites (SREs). Our transgenic studies show that mutation of either SRE, the TBE or the distal GATA element, strongly reduces expression from the ANF promoter. However, mutations of the NKE, the proximal GATA, or both elements together, result in relatively minor reductions in transgene expression within the myocardium. Surprisingly, mutation of these elements results in ectopic ANF promoter activity in the kidneys, facial muscles, and aortic arch artery-associated muscles, and causes persistent expression in the ventricle and outflow tract of the heart. We propose that the NKE and proximal GATA elements serve as crucial binding sites for assembly of a repressor complex that is required for atrial-specific expression of the ANF gene.
KW - ANF
KW - Atrium
KW - Heart
KW - Nkx2-5
KW - Transcription factor
KW - Transgenesis
KW - Xenopus laevis
UR - http://www.scopus.com/inward/record.url?scp=0041661957&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=0041661957&partnerID=8YFLogxK
U2 - 10.1016/S0012-1606(03)00306-3
DO - 10.1016/S0012-1606(03)00306-3
M3 - Article
C2 - 12941624
AN - SCOPUS:0041661957
SN - 0012-1606
VL - 261
SP - 116
EP - 131
JO - Developmental biology
JF - Developmental biology
IS - 1
ER -