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细胞角蛋白8和19在小鼠胎盘发育中的作用

Cytokeratins 8 and 19 in the mouse placental development.

作者信息

Tamai Y, Ishikawa T, Bösl M R, Mori M, Nozaki M, Baribault H, Oshima R G, Taketo M M

机构信息

Banyu Tsukuba Research Institute (Merck), Tsukuba, Ibaraki 300-2611, Japan.

出版信息

J Cell Biol. 2000 Oct 30;151(3):563-72. doi: 10.1083/jcb.151.3.563.

Abstract

To investigate the expression and biological roles of cytokeratin 19 (K19) in development and in adult tissues, we inactivated the mouse K19 gene (Krt1-19) by inserting a bacterial beta-galactosidase gene (lacZ) by homologous recombination in embryonic stem cells, and established germ line mutant mice. Both heterozygous and homozygous mutant mice were viable, fertile, and appeared normal. By 7.5-8.0 days post coitum (dpc), heterozygous mutant embryos expressed lacZ in the notochordal plate and hindgut diverticulum, reflecting the fact that the notochord and the gut endoderm are derived from the axial mesoderm-originated cells. In the adult mutant, lacZ was expressed mainly in epithelial tissues. To investigate the possible functional cooperation and synergy between K19 and K8, we then constructed compound homozygous mutants, whose embryos died approximately 10 dpc. The lethality resulted from defects in the placenta where both K19 and K8 are normally expressed. As early as 9. 5 dpc, the compound mutant placenta had an excessive number of giant trophoblasts, but lacked proper labyrinthine trophoblast or spongiotrophoblast development, which apparently caused flooding of the maternal blood into the embryonic placenta. These results indicate that K19 and K8 cooperate in ensuring the normal development of placental tissues.

摘要

为了研究细胞角蛋白19(K19)在发育过程和成年组织中的表达及生物学作用,我们通过在胚胎干细胞中进行同源重组插入细菌β-半乳糖苷酶基因(lacZ)来使小鼠K19基因(Krt1-19)失活,并建立了种系突变小鼠。杂合子和纯合子突变小鼠均存活、可育且外观正常。在交配后7.5 - 8.0天(dpc),杂合子突变胚胎在脊索板和后肠憩室中表达lacZ,这反映了脊索和肠内胚层源自轴中胚层起源的细胞这一事实。在成年突变体中,lacZ主要在上皮组织中表达。为了研究K19和K8之间可能的功能协作与协同作用,我们随后构建了复合纯合突变体,其胚胎在大约10 dpc时死亡。致死原因是胎盘缺陷,而K19和K8在正常胎盘中均有表达。早在9.5 dpc时,复合突变体胎盘就有过多的巨大滋养层细胞,但缺乏正常的迷路滋养层或海绵滋养层发育,这显然导致母体血液涌入胚胎胎盘。这些结果表明,K19和K8在确保胎盘组织正常发育方面存在协作。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7df8/2185583/3e33b82b60ae/JCB0006039.f1.jpg

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