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偶数跳动基因evx1的靶向破坏导致小鼠胚胎植入后早期死亡。

Targeted disruption of the even-skipped gene, evx1, causes early postimplantation lethality of the mouse conceptus.

作者信息

Spyropoulos D D, Capecchi M R

机构信息

Howard Hughes Medical Institute, Department of Human Genetics, University of Utah School of Medicine, Salt Lake City 84112.

出版信息

Genes Dev. 1994 Aug 15;8(16):1949-61. doi: 10.1101/gad.8.16.1949.

Abstract

Implantation within the mammalian uterus elicits dramatic changes in the growth, differentiation, and morphogenesis of the conceptus. This process is interrupted in mice carrying a targeted disruption of the murine evx1 gene, a homolog of the Drosophila even-skipped (eve) gene. Upon implantation, presumptive evx1- homozygotes elicit a decidual response, invade the uterine epithelium, and attach to the basement membrane between uterine stroma and epithelium, but fail to differentiate extraembryonic tissues or to form egg cylinders prior to resorption. Retrograde analysis of embryo genotypes demonstrates that homozygotes could be isolated as free-floating blastocysts but not as gastrulating egg cylinders. Homozygous mutant blastocysts appeared normal and, when grown in vitro, attach, proliferate, and form trophoblastic giant cells surrounding a growing inner cell mass before rapidly degenerating. In situ hybridization analysis demonstrates evx1 gene expression within the visceral endoderm after implantation and prior to gastrulation, at a time in which the mutant phenotype is first detected.

摘要

在哺乳动物子宫内着床会引发孕体在生长、分化和形态发生方面的显著变化。这一过程在携带小鼠evx1基因靶向缺失的小鼠中被打断,evx1基因是果蝇even-skipped(eve)基因的同源物。着床时,假定的evx1纯合子引发蜕膜反应,侵入子宫上皮,并附着于子宫基质和上皮之间的基底膜,但在吸收前无法分化胚外组织或形成卵柱。对胚胎基因型的逆向分析表明,纯合子可以作为游离的囊胚分离出来,但不能作为原肠胚形成的卵柱分离出来。纯合突变囊胚看起来正常,在体外培养时,会附着、增殖并形成围绕不断生长的内细胞团的滋养层巨细胞,然后迅速退化。原位杂交分析表明,在着床后和原肠胚形成前,在内脏内胚层中可检测到evx1基因表达,此时首次检测到突变表型。

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