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大鼠肝脏、肾脏和肺中肝细胞生长因子mRNA及其受体的发育变化。

Developmental changes in hepatocyte growth factor mRNA and its receptor in rat liver, kidney and lung.

作者信息

Kagoshima M, Kinoshita T, Matsumoto K, Nakamura T

机构信息

Department of Biology, Faculty of Science, Kyushu University, Fukuoka, Japan.

出版信息

Eur J Biochem. 1992 Nov 15;210(1):375-80. doi: 10.1111/j.1432-1033.1992.tb17431.x.

Abstract

Hepatocyte growth factor (HGF) is a mesenchymal-derived factor which induces mitosis, cell movement and morphogenesis of tissue-like structure. We analyzed changes in HGF mRNA and its receptor, the c-met proto-oncogene product, in the liver, kidney and lung during late fetal and postnatal development in rats. In the liver, the HGF-mRNA level was very low during late gestation and in neonates, it increased remarkably and reached a maximum two weeks postnatally, to be followed by a decrease to 33% of the maximum. HGF mRNA in the kidney and lung was either undetectable or very low during late gestation and the neonatal period and increased markedly to reach a maximum, respectively, 3-4 weeks postnatally. HGF-mRNA level in the adult rat lung was fivefold higher than that in the liver and kidney. The number of HGF receptors on plasma membranes of these tissues was low in neonates but there was a rapid increase after birth and a maximum was reached within three weeks. The number of HGF receptors/ng plasma membrane protein at the maximal level was highest in the liver and lowest in the lung. c-met/HGF-receptor mRNA in the liver was also low during late-gestation or in early neonatal periods and increased postnatally. Since HGF-mRNA and HGF-receptor levels changed differently in liver, kidney and lung, the expression of HGF and its receptor may be independently regulated in each organ. However, in these organs, HGF mRNA and the HGF receptor increased within a few weeks of birth, HGF may play roles in organ growth, organ maturation and the maintenance of tissue homeostasis during the postnatal period, presumably through its potential to act as mitogen, motogen and morphogen.

摘要

肝细胞生长因子(HGF)是一种间充质来源的因子,可诱导有丝分裂、细胞运动以及组织样结构的形态发生。我们分析了大鼠胎儿后期及出生后发育过程中肝脏、肾脏和肺中HGF mRNA及其受体(c-met原癌基因产物)的变化。在肝脏中,妊娠后期和新生儿期HGF-mRNA水平非常低,出生后显著升高,在出生后两周达到峰值,随后降至峰值的33%。妊娠后期和新生儿期,肾脏和肺中的HGF mRNA检测不到或水平极低,出生后分别在3 - 4周显著升高并达到峰值。成年大鼠肺中HGF-mRNA水平比肝脏和肾脏高五倍。这些组织质膜上HGF受体的数量在新生儿期较低,但出生后迅速增加,在三周内达到峰值。最高水平时每纳克质膜蛋白中HGF受体的数量在肝脏中最高,在肺中最低。肝脏中c-met/HGF受体mRNA在妊娠后期或新生儿早期也较低,出生后增加。由于HGF-mRNA和HGF受体水平在肝脏、肾脏和肺中的变化不同,HGF及其受体的表达可能在每个器官中独立调节。然而,在这些器官中,HGF mRNA和HGF受体在出生后几周内增加,HGF可能在出生后时期的器官生长、器官成熟和组织稳态维持中发挥作用,大概是通过其作为促有丝分裂原、促运动原和形态发生原的潜力。

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