首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >A targeted mutation in the mouse E-cadherin gene results in defective preimplantation development.
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A targeted mutation in the mouse E-cadherin gene results in defective preimplantation development.

机译:小鼠E-钙粘着蛋白基因中的靶向突变导致有缺陷的植入前发育。

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摘要

The Ca(2+)-dependent cell adhesion molecule E-cadherin functions in the establishment and maintenance of epithelial cell morphology during embryogenesis and adulthood. Downregulation or complete shut-down of E-cadherin expression and mutation of the gene are observed during the progression of tumors of epithelial origin (carcinomas) and correlate with the metastatic potential. We have introduced a targeted mutation into the E-cadherin gene by homologous recombination in mouse embryonic stem cells. The mutation removes E-cadherin sequences essential for Ca2+ binding and for adhesive function. These embryonic stem cells were used to generate mice carrying the mutation. Heterozygous mutant animals appear normal and are fertile. However, the homozygous mutation is not compatible with life: E-cadherin -/- embryos show severe abnormalities before implantation. Particularly, the adhesive cells of the morula dissociate shortly after compaction has occurred, and their morphological polarization is then destroyed. Interestingly, the blastomers are still able to form desmosomes and tight junctions at sites of distorted cell-cell contact. Thus, maternal E-cadherin suffices for initial compaction of the morula but not for further preimplantation development to occur.
机译:Ca(2+)依赖细胞粘附分子E-钙粘着蛋白在胚胎发生和成年过程中建立和维持上皮细胞形态的功能。在上皮起源的肿瘤(癌)的进展过程中观察到E-钙粘着蛋白表达的下调或完全关闭以及基因的突变,并且与转移潜力相关。我们已经在小鼠胚胎干细胞中通过同源重组将靶向突变引入到E-钙粘蛋白基因中。该突变去除了对钙离子结合和粘附功能必不可少的E-钙粘着蛋白序列。这些胚胎干细胞用于产生携带突变的小鼠。杂合突变动物看起来正常并且可育。但是,纯合突变与生命不相容:E-钙粘着蛋白-/-胚胎在植入前显示出严重异常。特别地,在压实发生后不久,桑ula的粘附细胞解离,然后破坏其形态极化。有趣的是,卵裂球仍然能够在变形的细胞间接触部位形成桥粒和紧密连接。因此,母体E-钙粘着蛋白足以满足骨的初始压紧作用,但不能满足植入前进一步发展的需要。

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