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Investigation of the angiogenic programme with tissue-specific and inducible genetic approaches in mice

机译:小鼠组织特异性和诱导诱导方法对血管生成计划的研究

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Blood vessels form a highly organi2ed hierarchical network throughout the vertebrate body, integrate functionally into very different tissue environments and remain remarkably adaptable to changing local requirements. The importance of a correctly formed and functional vascular network is highlighted by numerous human pathologies, which involve defects such as compromised blood circulation, destabiliza-tion of vessel walls or deregulated angiogenesis. Genetically modified mice are powerful tools for the functional characterization of genes, and can also serve as models of human diseases. However, targeted inactivation of genes essential for blood vessel morphogenesis is usually incompatible with embryonic survival, so studies In adult mice are precluded. Moreover, mutant phenotypes can be a complex combination of defects in different tissues and cell types. Tissue-specific and Inducible genetic approaches allow us to overcome many of these limitations. In particular, it is possible to perform manipulations in a spatially (i.e. cell type-specific) and temporally controlled fashion, which makes possible studies throughout development and in adults. We have generated several transgenic Cre and tamoxifen-induble CreERT2 lines that enable the selective targeting of vascular cell populations. Here, 1 will discuss the characterization of these lines and present examples of their application in the analysis of vascular development.
机译:血管在整个脊椎动物体内形成高度有机的分层网络,在功能上集成到非常不同的组织环境中,并保持显着适应改变局部要求。众多人类病理突出了正确形成和功能性血管网络的重要性,这涉及缺陷,例如受损的血液循环,血管壁的破坏壁或损失血管生成。基因改性小鼠是基因功能表征的强大工具,也可以作为人类疾病的模型。然而,针对血管形态发生的基因的靶向失活通常与胚胎生存率不相容,因此预先抑制成年小鼠的研究。此外,突变表型可以是不同组织和细胞类型中的缺陷的复杂组合。组织特异性和诱导遗传遗传方法允许我们克服许多这些限制。特别地,可以在空间(即细胞类型特异性)和时间上控制的时装中进行操纵,这使得在整个发育和成人中进行了可能的研究。我们产生了几种转基因Cre和Tamoxifen-Induble Creert2线,其能够选择性靶向血管细胞群。这里,1将讨论这些系列的表征,并在血管发育分析中存在其应用的实例。

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