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发育中大鼠氨代谢酶mRNA的表达模式:肝细胞异质性的个体发生

Expression patterns of mRNAs for ammonia-metabolizing enzymes in the developing rat: the ontogenesis of hepatocyte heterogeneity.

作者信息

Moorman A F, De Boer P A, Das A T, Labruyère W T, Charles R, Lamers W H

机构信息

Department of Anatomy and Embryology, Academic Medical Centre, Amsterdam, The Netherlands.

出版信息

Histochem J. 1990 Sep;22(9):457-68. doi: 10.1007/BF01007229.

Abstract

The expression patterns of the mRNAs for the ammonia-metabolizing enzymes carbamoylphosphate synthetase (CPS), glutamine synthetase (GS) and glutamate dehydrogenase (GDH) were studied in developing pre- and neonatal rat liver by in situ hybridization. In the period of 11 to 14 embryonic days (ED) the concentrations of GS and GDH mRNA increases rapidly in the liver, whereas a substantial rise of CPS mRNA in the liver does not occur until ED 18. Hepatocyte heterogeneity related to the vascular architecture can first be observed at ED 18 for GS mRNA, at ED 20 for GDH mRNA and three days after birth for CPS mRNA. The adult phenotype is gradually established during the second neonatal week, i.e. GS mRNA becomes confined to a pericentral compartment of one to two hepatocytes thickness, CPS mRNA to a large periportal compartment being no longer expressed in the pericentral compartment and GDH mRNA is expressed over the entire porto-central distance, decreasing in concentration going from central to portal. Comparison of the observed mRNA distribution patterns in the perinatal liver, with published data on the distribution of the respective proteins, points to the occurrence of posttranslational, in addition to pretranslational control mechanisms in the period of ontogenesis of hepatocyte heterogeneity. Interestingly, during development all three mRNAS are expressed outside the liver to a considerable extent and in a highly specific way, indicating that several organs are involved in the developmentally regulated expression of the mRNAs for the ammonia-metabolizing enzymes, that were hitherto not recognized as such.

摘要

通过原位杂交技术,研究了氨代谢酶氨基甲酰磷酸合成酶(CPS)、谷氨酰胺合成酶(GS)和谷氨酸脱氢酶(GDH)的mRNA在发育中的新生大鼠肝脏中的表达模式。在胚胎第11至14天(ED)期间,肝脏中GS和GDH mRNA的浓度迅速增加,而肝脏中CPS mRNA直到ED 18才大幅上升。与血管结构相关的肝细胞异质性,对于GS mRNA最早在ED 18时可观察到,对于GDH mRNA在ED 20时可观察到,而对于CPS mRNA在出生后三天可观察到。成年表型在新生儿第二周逐渐形成,即GS mRNA局限于一到两个肝细胞厚度的中央周围区域,CPS mRNA局限于一个大的门静脉周围区域,不再在中央周围区域表达,而GDH mRNA在整个门静脉-中央区域均有表达,浓度从中央到门静脉逐渐降低。将围产期肝脏中观察到的mRNA分布模式与已发表的关于相应蛋白质分布的数据进行比较,表明在肝细胞异质性发生过程中,除了翻译前控制机制外,还存在翻译后控制机制。有趣的是,在发育过程中,所有三种mRNA在肝脏外也有相当程度的表达,且具有高度特异性,这表明几个器官参与了氨代谢酶mRNA的发育调控表达,而这些器官此前未被认为有此作用。

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