2013
DOI: 10.1038/ncb2862
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Heart field origin of great vessel precursors relies on nkx2.5-mediated vasculogenesis

Abstract: The pharyngeal arch arteries (PAAs) are transient embryonic blood vessels that make indispensable contributions to the carotid arteries and great vessels of the heart, including the aorta and pulmonary artery1, 2. During embryogenesis, the PAAs appear in a craniocaudal sequence to connect pre-existing segments of the primitive circulation after de novo vasculogenic assembly from angioblast precursors3, 4. Despite the unique spatiotemporal characteristics of PAA development, the embryonic origins of PAA angiobl… Show more

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Cited by 67 publications
(117 citation statements)
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“…To test this idea, we analyzed the formation of the ventral head endothelium in tcf21 mutant, nkx2.5 mutant, and tcf21 ; nkx2.5 double mutant embryos transgenic for flk:mCherry to label endothelial cells and nkx2.5:ZsYellow to label pPAA progenitors. In contrast to nkx2.5 morpholino knockdown experiments [8], which have recently been reported to be error prone [37], we find that the pPAAs are present at 60 hpf in tcf21 mutant, nkx2.5 mutant, and tcf21 ; nkx2.5 double mutant embryos, although pPAAs occasionally failed to lumenize in nkx2.5 mutant, tcf21 mutant, and tcf21 ; nkx2.5 double mutant embryos (Figure 5R). This result indicates, unexpectedly, that tcf21 and nkx2.5 are not required for pPAA formation.…”
Section: Resultscontrasting
confidence: 82%
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“…To test this idea, we analyzed the formation of the ventral head endothelium in tcf21 mutant, nkx2.5 mutant, and tcf21 ; nkx2.5 double mutant embryos transgenic for flk:mCherry to label endothelial cells and nkx2.5:ZsYellow to label pPAA progenitors. In contrast to nkx2.5 morpholino knockdown experiments [8], which have recently been reported to be error prone [37], we find that the pPAAs are present at 60 hpf in tcf21 mutant, nkx2.5 mutant, and tcf21 ; nkx2.5 double mutant embryos, although pPAAs occasionally failed to lumenize in nkx2.5 mutant, tcf21 mutant, and tcf21 ; nkx2.5 double mutant embryos (Figure 5R). This result indicates, unexpectedly, that tcf21 and nkx2.5 are not required for pPAA formation.…”
Section: Resultscontrasting
confidence: 82%
“…Consistent with observations in chicken and mice [2022], we find that the transcription factor tcf21 (Epicardin/Capsulin/Pod1) is expressed bilaterally at the 12-somite stage (15 hpf) in two domains within the head mesoderm—an anterior domain and a posterior domain (Figure 1A). Using tcf21:mCherry-NTR (referred to as tcf21:mCherry if not indicated otherwise), a transcriptional reporter for tcf21 + cells [23], we find that at the 14-somite stage (16 hpf), the anterior tcf21 expression domain is bounded anteriorly by the prechordal plate mesoderm marked by pitx2 [24] and overlaps posteriorly with the cardiac mesoderm marked by a transcriptional reporter for nkx2.5 ( nkx2.5: ZsYellow ) [8, 25] (Figures 1D, 1J, and 1K). The posterior domain of tcf21 expression overlaps anteriorly with the nkx2.5 -expressing domain (Figures 1D and 1E; Movie S3).…”
Section: Resultsmentioning
confidence: 99%
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“…Chromatin was immunoprecipitated using specific antibodies. Five primer pairs 1, 2, 3, 4, 5 were designed to cover the 1.6‐kb genomic region of the downstream enhancer. Results are shown as the fold enrichment of each protein in every genomic segment.…”
Section: Resultsmentioning
confidence: 99%