2005
DOI: 10.1073/pnas.0502752102
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Gene targeting of VEGF-A in thymus epithelium disrupts thymus blood vessel architecture

Abstract: The thymus harbors an organ-typical dense network of branching and anastomosing blood vessels. To address the molecular basis for morphogenesis of this thymus-specific vascular pattern, we have inactivated a key vascular growth factor, VEGF-A, in thymus epithelial cells (TECs). Both Vegf-A alleles were deleted in TECs by a complementation strategy termed nude mouse [mutated in the transcription factor Foxn1 (forkhead box N1)] blastocyst complementation. Injection of Foxn1 ؉/؉ ES cells into Foxn1 nu/nu blastocy… Show more

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Cited by 73 publications
(72 citation statements)
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“…1D) that could first be ϩ stromal cells also expressed the cortical epithelium marker Ly51 (Fig. 1D); these cells may correspond to the proposed "cortical mesenchyme" population observed in a previous study (48).…”
Section: Thymic Distribution Of Mts-15supporting
confidence: 69%
“…1D) that could first be ϩ stromal cells also expressed the cortical epithelium marker Ly51 (Fig. 1D); these cells may correspond to the proposed "cortical mesenchyme" population observed in a previous study (48).…”
Section: Thymic Distribution Of Mts-15supporting
confidence: 69%
“…By flow cytometry, we identified two major mesenchymal cell populations in the adult thymus based on expression of Ly51 and gp38: Ly51 int gp38 + and Ly51 hi gp38 2 cells. Although Ly51 + mesenchymal cells are neural crest derived (16,24), to our knowledge, such division within the Ly51 + mesenchyme population has not previously been described. Functionally Ly51 int gp38 + and Ly51 hi gp38 2 cells appear distinct from one another, as only the former subset expressed Aldh1a-1, -2, and -3 and contained within it a population of cells with high ALDH activity.…”
Section: Discussionmentioning
confidence: 77%
“…Consistent with this, mice deficient in FGF-10 or the FGF-10/-7 receptor, FGFR2-IIIb, and mice expressing soluble dominant-negative FGFR2-IIIb display thymus dysgenesis (22,23) and reduced thymic epithelial proliferation (23). Mesenchymal components are found within both the cortex and medulla (16,24), raising the possibility that these cells may be capable of influencing both thymic compartments.…”
mentioning
confidence: 66%
“…In addition to thymocytes, other non-hematopoietic stromal elements, such as fibroblasts and endothelial cells, and distinct bone marrow-derived dendritic cells (DC) and macrophages also contribute to the final thymic architecture [26]. Thymic mesenchymatous cells also contribute to various structures of the thymus such as capsule or vasculature [27][28][29][30].…”
Section: Embryology Of the Thymusmentioning
confidence: 99%