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Resolution of defective dorsal aortae patterning in Sema3E-deficient mice occurs via angiogenic remodeling

机译:通过血管生成重塑发生Sema3e缺陷小鼠的缺陷背部Aortae的分辨率进行分辨率

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Background: Neuronal guidance cues influence endothelial cell (EC) behavior to shape the embryonic vascular system. The repulsive neuronal guidance cue, Semaphorin 3E (Sema3E), is critical for creating avascular zones that instruct and subsequently pattern the first embryonic vessels, the paired dorsal aortae (DA). Sema3E-/- embryos develop highly branched plexus-like vessels during vasculogenesis, instead of smooth paired vessels. Unexpectedly, despite these severe DA patterning defects, mutant mice are viable throughout adulthood. Results: Examination of Sema3E-/- mice reveals that the plexus-like DA resolve into single, unbranched vessels between embryonic day (E) E8.25 and E8.75. Although fusion of Sema3E-/- DA occurs slightly earlier than in heterozygotes, the DA are otherwise indistinguishable, suggesting a complete "rescue" in their development. Resolution of the DA null plexuses occurs by remodeling rather than by means of changes in cell proliferation or death. Conclusions: Normalization of Sema3E-/- DA patterning defects demonstrates resilience of embryonic vascular patterning programs. Additional repulsive guidance cues within the lateral plate mesoderm likely re-establish avascular zones lost in Sema3E-/- embryos and guide resolution of mutant plexus into branchless, parallel aortae. Our observations explain how Sema3E-/- mice survive throughout development and into adulthood, despite severe initial vascular defects.
机译:背景:神经元引导提示影响内皮细胞(EC)行为来塑造胚胎血管系统。令人厌恶的神经元引导提示,信号素3e(Sema3e)对于产生指导和随后图案的血管区,对第一胚胎血管的缺血区至关重要,配对背部Aortae(DA)。 SEMA3E - / - 胚胎在血管生成期间在血管生成期间形成高度分枝状葡萄球菌,而不是光滑的配对容器。出乎意料的是,尽管这些严重的DA图案化缺陷,但突变小鼠在整个成年期都是可行的。结果:SEMA3E的检查 - / - 小鼠揭示了Plexus样Da在胚胎天(e)e8.25和e8.75之间分离成单一的非支链血管。虽然SEMA3E - / - DA的融合比杂合子略要略高,但DA否则无法区分,表明他们在发展中完全“救援”。通过重塑而不是通过细胞增殖或死亡的变化发生的DA零族丛的分辨率。结论:SEMA3E的标准化 - / - DA图案化缺陷证明了胚胎血管图案设计的恢复力。横向板中的额外排斥指导提示Mesoderm可能重新建立Sema3e - / - 胚胎中损失的血管区,并将突变丛导向分离为无树枝,平行的Aortae。我们的观察结果解释了SEMA3E - / - 小鼠在整个开发过程中如何生存,并且尽管严重的血管缺陷,但仍然存在于成年期。

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