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抑制糖鞘脂生物合成不会损害植入后小鼠胚胎的生长或形态发生。

Inhibition of glycosphingolipid biosynthesis does not impair growth or morphogenesis of the postimplantation mouse embryo.

作者信息

Brigande J V, Platt F M, Seyfried T N

机构信息

Department of Biology, Boston College, Chestnut Hill, Massachusetts 02167, USA.

出版信息

J Neurochem. 1998 Feb;70(2):871-82. doi: 10.1046/j.1471-4159.1998.70020871.x.

Abstract

Whole embryo culture (WEC) of organogenesis-stage mouse embryos was adapted for glycosphingolipid (GSL) metabolic studies to evaluate the hypothesis that de novo GSL biosynthesis is a prerequisite for growth and morphogenesis of the early postimplantation embryo. WEC supports the growth and development of postimplantation mouse embryos to stages that are indistinguishable from those achieved in vivo. N-Butyldeoxygalactonojirimycin (NB-DGJ) is an N-alkylated imino sugar that specifically inhibits biosynthesis of all glucosylceramide-based GSLs. NB-DGJ inhibited glucosylceramide and lactosylceramide biosynthesis nearly completely and inhibited ganglioside biosynthesis approximately 90% in both the embryo and visceral yolk sac. NB-DGJ also significantly reduced total ganglioside content in both the embryo and visceral yolk sac as estimated by the cholera toxin immunooverlay technique. A shift in expression from the structurally simple to the structurally complex gangliosides was also observed in NB-DGJ-treated embryos and yolk sacs. Despite causing major changes in GSL biosynthesis and composition, NB-DGJ had no effect on embryo viability, growth, or morphology. The findings suggest that de novo GSL biosynthesis may not be a prerequisite for the growth and morphogenesis of the organogenesis-stage mouse embryo.

摘要

将器官发生期小鼠胚胎的全胚胎培养(WEC)方法应用于糖鞘脂(GSL)代谢研究,以评估如下假说:从头合成GSL是植入后早期胚胎生长和形态发生的先决条件。WEC支持植入后小鼠胚胎生长发育至与体内发育阶段无法区分的阶段。N-丁基脱氧半乳糖野茉莉霉素(NB-DGJ)是一种N-烷基化亚氨基糖,可特异性抑制所有基于葡萄糖神经酰胺的GSL的生物合成。NB-DGJ几乎完全抑制了葡萄糖神经酰胺和乳糖神经酰胺的生物合成,并在胚胎和内脏卵黄囊中抑制了约90%的神经节苷脂生物合成。通过霍乱毒素免疫印迹技术估计,NB-DGJ还显著降低了胚胎和内脏卵黄囊中总神经节苷脂的含量。在经NB-DGJ处理的胚胎和卵黄囊中,还观察到了从结构简单的神经节苷脂到结构复杂的神经节苷脂的表达转变。尽管NB-DGJ引起了GSL生物合成和组成的重大变化,但对胚胎活力、生长或形态没有影响。这些发现表明,从头合成GSL可能不是器官发生期小鼠胚胎生长和形态发生的先决条件。

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