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首页> 外文期刊>Stem Cells >Stage-specific conditional mutagenesis in mouse embryonic stem cell-derived neural cells and postmitotic neurons by direct delivery of biologically active Cre recombinase.
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Stage-specific conditional mutagenesis in mouse embryonic stem cell-derived neural cells and postmitotic neurons by direct delivery of biologically active Cre recombinase.

机译:通过直接递送具有生物活性的Cre重组酶,在小鼠胚胎干细胞衍生的神经细胞和有丝分裂后神经元中进行阶段特异性条件诱变。

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摘要

Conditional mutagenesis using Cre/loxP recombination is a powerful tool to investigate genes involved in neural development and function. However, the efficient delivery of biologically active Cre recombinase to neural cells, particularly to postmitotic neurons, represents a limiting factor. In this study, we devised a protocol enabling highly efficient conditional mutagenesis in ESC-derived neural progeny. Using a stepwise in vitro differentiation paradigm, we demonstrate that recombinant cell-permeable Cre protein can be used to efficiently induce recombination at defined stages of neural differentiation. Recombination rates of more than 90% were achieved in multipotent pan-neural and glial precursors derived from the Z/EG reporter mouse ESC line, in which Cre recombination activates enhanced green fluorescent proteinexpression. Recombined precursor cells displayed a normal phenotype and were able to differentiate into neurons and/or glial cells, indicating that Cre treatment has no overt side effects on proliferation and neural differentiation. Our data further demonstrate that recombination via Cre protein transduction is not restricted to dividing cells but can even be applied to postmitotic neurons. The ability to conduct Cre/loxP recombination at defined stages of stem cell differentiation in an expression-independent manner provides new prospects for studying the role of individual genes under stringent temporal control.
机译:使用Cre / loxP重组进行条件诱变是研究涉及神经发育和功能的基因的强大工具。然而,将生物活性Cre重组酶有效递送至神经细胞,特别是有丝分裂后神经元,是限制因素。在这项研究中,我们设计了一种协议,可以在ESC衍生的神经后代中进行高效的条件诱变。使用逐步体外分化的范式,我们证明重组细胞可渗透的Cre蛋白可用于有效地诱导神经分化的定义阶段的重组。在源自Z / EG报告基因小鼠ESC系的全能泛神经和神经胶质前体中,重组率达到90%以上,其中Cre重组激活增强的绿色荧光蛋白表达。重组的前体细胞表现出正常的表型,并且能够分化为神经元和/或神经胶质细胞,表明Cre治疗对增殖和神经分化没有明显的副作用。我们的数据进一步证明,通过Cre蛋白转导的重组不仅限于分裂细胞,甚至可以应用于有丝分裂后的神经元。在干细胞分化的确定阶段以表达独立的方式进行Cre / loxP重组的能力为研究单个基因在严格的时间控制下的作用提供了新的前景。

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