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新生小鼠表皮生长因子内源性合成的起始

Onset of endogenous synthesis of epidermal growth factor in neonatal mice.

作者信息

Popliker M, Shatz A, Avivi A, Ullrich A, Schlessinger J, Webb C G

出版信息

Dev Biol. 1987 Jan;119(1):38-44. doi: 10.1016/0012-1606(87)90204-1.

Abstract

We have analyzed mouse fetuses and neonates for the presence of epidermal growth factor (EGF)-specific mRNA. No detectable EGF-specific mRNA was found in fetuses, fetal membranes, or placentae from Day 9 of gestation through birth or in the early neonatal period. While the kidneys begin to produce EGF specific transcripts by two weeks postpartum, the salivary glands begin to produce detectable levels of EGF mRNA only after weaning and even then at levels far below the adult amount. Reports of EGF and EGF-related material in rodent fetuses failed to determine whether this material was of maternal or fetal origin. We now conclude that authentic EGF in these embryos is probably of maternal origin. We have performed experiments designed to determine whether EGF can be transported into the fetus. A small percentage of 125I-EGF administered to pregnant females either systemically or directly into the uterine arteries reached the fetus itself. The uterus and the placenta attained a high level of labeling, whereas the amniotic fluid and yolk sac were virtually devoid of the tracer. In the neonatal period, milk may be the physiologically relevant source of EGF. We have found that 125I-EGF ingested by neonates was absorbed into the circulation, reached many internal organs, and was eventually excreted in the urine. Previously demonstrated EGF receptors in mouse embryonic cell types may be activated by either alpha type transforming growth factor or maternal EGF transported via the placenta.

摘要

我们已对小鼠胎儿和新生儿进行分析,以检测表皮生长因子(EGF)特异性mRNA的存在。从妊娠第9天直至出生或新生儿早期,在胎儿、胎膜或胎盘中均未检测到EGF特异性mRNA。产后两周时肾脏开始产生EGF特异性转录本,而唾液腺仅在断奶后才开始产生可检测水平的EGF mRNA,且即便如此,其水平也远低于成年时的量。关于啮齿类动物胎儿中EGF及EGF相关物质的报告未能确定该物质是母体来源还是胎儿来源。我们现在得出结论,这些胚胎中的真实EGF可能来源于母体。我们已开展实验以确定EGF是否能够转运至胎儿体内。给怀孕母鼠全身给药或直接向子宫动脉注射125I-EGF后,仅有一小部分到达了胎儿自身。子宫和胎盘有很高的放射性标记水平,而羊水和卵黄囊几乎没有这种示踪剂。在新生儿期,乳汁可能是EGF的生理相关来源。我们发现,新生儿摄入的125I-EGF被吸收进入循环系统,到达许多内部器官,并最终经尿液排出。先前在小鼠胚胎细胞类型中证实的EGF受体可能被α型转化生长因子或经胎盘转运的母体EGF激活。

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