肝细胞生长因子/分散因子敲除小鼠胚胎致死性的恢复。

IF 1.5 4区 生物学 Q3 Biochemistry, Genetics and Molecular Biology
Genesis Pub Date : 2000-07-01
Y Uehara, C Mori, T Noda, K Shiota, N Kitamura
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引用次数: 0

摘要

虽然有针对性地破坏基因是研究该基因生理功能的有力工具,但破坏胚胎发生所必需的基因会导致胚胎死亡。修复导致胚胎死亡的缺陷应该会促进存活,从而允许进一步评估该基因在以后的发育过程中所起的作用。小鼠肝细胞生长因子/分散因子(HGF/SF)基因的破坏导致胎盘发育缺陷导致中期胚胎死亡。本研究报道,在胚胎第9.5天(E9.5)向HGF/SF(-/-)胚胎的羊膜腔内单次注射HGF/SF可挽救胎盘缺损,并使胚胎存活至足月。组织学分析表明,HGF/SF在组织器官发生的发育后期也是必需的。因此,注射分泌因子可作为挽救胚胎致死性缺陷的有效方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Rescue of embryonic lethality in hepatocyte growth factor/scatter factor knockout mice.

While the targeted disruption of a gene is a powerful tool for investigating the physiological functions of that gene, disruption of a gene essential for embryogenesis leads to embryonic death. Rescue of the defect(s) causing embryonic death should promote survival, thus permitting further evaluation of the roles that the gene plays later in the developmental process. Disruption of the gene for mouse hepatocyte growth factor/scatter factor (HGF/SF) leads to middle-stage embryonic lethality because of a defect in placental development. Here we report that a single injection of HGF/SF at embryonic day 9.5 (E9.5) into the amniotic cavity of HGF/SF(-/-) embryos rescued the placental defect and resulted in the survival of the embryos until term. Histological analysis suggested that HGF/SF is also required at the late stage of development for tissue organogenesis. Thus, injection of a secreted factor can be a useful method to rescue the defects causing embryonic lethality.

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来源期刊
Genesis
Genesis DEVELOPMENTAL BIOLOGY-GENETICS & HEREDITY
CiteScore
3.90
自引率
0.00%
发文量
19
期刊介绍: As of January 2000, Developmental Genetics was renamed and relaunched as genesis: The Journal of Genetics and Development, with a new scope and Editorial Board. The journal focuses on work that addresses the genetics of development and the fundamental mechanisms of embryological processes in animals and plants. With increased awareness of the interplay between genetics and evolutionary change, particularly during developmental processes, we encourage submission of manuscripts from all ecological niches. The expanded numbers of genomes for which sequencing is being completed will facilitate genetic and genomic examination of developmental issues, even if the model system does not fit the “classical genetic” mold. Therefore, we encourage submission of manuscripts from all species. Other areas of particular interest include: 1) the roles of epigenetics, microRNAs and environment on developmental processes; 2) genome-wide studies; 3) novel imaging techniques for the study of gene expression and cellular function; 4) comparative genetics and genomics and 5) animal models of human genetic and developmental disorders. genesis presents reviews, full research articles, short research letters, and state-of-the-art technology reports that promote an understanding of the function of genes and the roles they play in complex developmental processes.
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