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小鼠乳腺中羧基酯脂肪酶基因调控的研究。

Studies of the regulation of the mouse carboxyl ester lipase gene in mammary gland.

作者信息

Kannius-Janson M, Lidberg U, Hultén K, Gritli-Linde A, Bjursell G, Nilsson J

机构信息

Department of Molecular Biology, Göteborg University, Box 462, 405 30 Göteborg, Sweden.

出版信息

Biochem J. 1998 Dec 15;336 ( Pt 3)(Pt 3):577-85. doi: 10.1042/bj3360577.

Abstract

The lactating mammary gland and pancreas of mouse constitute the main tissues for synthesis and secretion of a bile-salt-stimulated lipase called carboxyl ester lipase (CEL). In this paper we have analysed the endogenous CEL gene expression in mammary gland. It is shown that the gene is expressed at day 14 of pregnancy, which is synchronous with that of the whey acidic protein (WAP) gene. Even though the CEL and WAP genes are induced at the same time during mammary gland differentiation, their regulation is different with respect to dependence on lactogenic hormones. The high induction of the WAP gene expression due to the activation of signal transducer and activator of transcription (STAT)5 by prolactin has not been observed for the CEL gene, even though it has been demonstrated that both STAT5 isoforms interact with one of the gamma-interferon activation sequence sites in the promoter of the CEL gene. Hence we have demonstrated that the prolactin/STAT5 signal is not involved in a general and significant activation of 'milk genes'. Instead of a direct effect of the lactogenic hormones, the up-regulation of the CEL gene is correlated with an increase in the number of differentiated epithelial cells. Furthermore, promoter studies using the mammary-gland-derived cell line, HC11, show that a major positive element in the CEL gene promoter interacts with a member(s) of the CCAAT-binding transcription factor/nuclear factor 1 family, binding to a palindromic site. Binding of this factor(s) is important for the tissue-specific activation of the CEL gene in the mammary gland, because no activation by this factor(s) was seen in cells of pancreatic origin.

摘要

小鼠的泌乳乳腺和胰腺是合成与分泌一种名为羧基酯脂肪酶(CEL)的胆汁盐刺激脂肪酶的主要组织。在本文中,我们分析了乳腺中内源性CEL基因的表达情况。结果表明,该基因在妊娠第14天表达,这与乳清酸性蛋白(WAP)基因的表达同步。尽管CEL和WAP基因在乳腺分化过程中同时被诱导,但它们在对泌乳激素的依赖性方面调控不同。催乳素通过激活信号转导子和转录激活子(STAT)5导致WAP基因表达的高度诱导,而CEL基因并未观察到这种情况,尽管已经证明两种STAT5同工型都与CEL基因启动子中的一个γ-干扰素激活序列位点相互作用。因此,我们证明催乳素/STAT5信号不参与“乳基因”的普遍且显著的激活。CEL基因的上调与分化上皮细胞数量的增加相关,而非泌乳激素的直接作用。此外,使用源自乳腺的细胞系HC11进行的启动子研究表明,CEL基因启动子中的一个主要正向元件与CCAAT结合转录因子/核因子1家族的一个成员相互作用,该成员结合到一个回文位点。该因子的结合对于乳腺中CEL基因的组织特异性激活很重要,因为在胰腺来源的细胞中未观察到该因子的激活作用。

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