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孕期、哺乳期及乳腺退化期大鼠乳腺中铜蓝蛋白基因表达谱的变化

Ceruloplasmin gene expression profile changes in the rat mammary gland during pregnancy, lactation and involution.

作者信息

Platonova Natalia A, Orlov Iurii A, Klotchenko Sergey A, Babich Victor S, Ilyechova Ekaterina Y, Babich Polina S, Garmai Yuri P, Vasin Andrey V, Tsymbalenko Nadezhda V, Puchkova Liudmila V

机构信息

Institute of Experimental Medicine, Pavlova str., 12, St., Petersburg 197376, Russia.

ITMO University, Kronverksky av., 49, St., Petersburg 197101, Russia; Peter the Great St. Petersburg Polytechnic University, Polytechnicheskaya str., 29, St., Petersburg 195251, Russia.

出版信息

J Trace Elem Med Biol. 2017 Sep;43:126-134. doi: 10.1016/j.jtemb.2016.12.013. Epub 2017 Jan 3.

Abstract

Copper metabolism disturbances in mammary gland (MG) cells have severe consequences in newborns. The mechanism that controls the balance of copper in the MG has not been thoroughly characterized. Four primary copper homeostasis genes in mammals: (1) ceruloplasmin (Cp) encoding multifunction multicopper blue (ferr)oxidase; (2) CTR1 encoding high affinity copper importer 1; and (3 and 4) two similar genes encoding Cu(I)/Cu(II)-ATPases P1 type (ATP7A and ATP7B) responsible for copper efflux from the cells and metallation of cuproenzymes formed in the Golgi complex are expressed in MG. This study aimed to characterize expression of these genes during pregnancy, lactation and forced involution in the rat MG. We found that Cp anchored to the plasma membrane and ATP7A were expressed during pregnancy and lactation. Soluble Cp and ATP7B were highly expressed in lactating MG decreasing to its ending. CTR1 activity increased during MG growth and reached its maximum at postpartum and then it decreased until the end of lactation. During early forced MG involution, Cp gene expression persisted; while a form of Cp that lacked exon 18 appeared. We suggest that Cp gene expressional changes at the transcriptional and posttranscriptional level reflect various physiological functions of Cp proteins during MG remodeling.

摘要

乳腺(MG)细胞中的铜代谢紊乱对新生儿有严重影响。控制MG中铜平衡的机制尚未得到充分阐明。哺乳动物中有四个主要的铜稳态基因:(1)编码多功能多铜蓝(铁)氧化酶的铜蓝蛋白(Cp);(2)编码高亲和力铜转运蛋白1的CTR1;以及(3和4)两个相似的基因,它们编码负责将铜从细胞中排出并参与在高尔基体复合物中形成的铜酶金属化的Cu(I)/Cu(II)-ATP酶P1型(ATP7A和ATP7B),这些基因在MG中均有表达。本研究旨在表征这些基因在大鼠MG妊娠、泌乳和强制退化过程中的表达情况。我们发现,锚定在质膜上的Cp和ATP7A在妊娠和泌乳期间表达。可溶性Cp和ATP7B在泌乳期的MG中高表达,在泌乳末期下降。CTR1活性在MG生长过程中增加,在产后达到最大值,然后在泌乳结束前下降。在早期强制MG退化过程中,Cp基因表达持续存在;同时出现了一种缺少第18外显子的Cp形式。我们认为,Cp基因在转录和转录后水平的表达变化反映了Cp蛋白在MG重塑过程中的各种生理功能。

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