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新生儿的铜代谢适应了乳铜蓝蛋白作为铜的营养来源:对现有数据的综述。

Copper Metabolism of Newborns Is Adapted to Milk Ceruloplasmin as a Nutritive Source of Copper: Overview of the Current Data.

机构信息

Laboratory of Trace Elements Metabolism, ITMO University, Kronverksky av., 49, 197101 St.-Petersburg, Russia.

Department of Molecular Genetics, Research Institute of Experimental Medicine, Acad. Pavlov str., 12, 197376 St.-Petersburg, Russia.

出版信息

Nutrients. 2018 Oct 30;10(11):1591. doi: 10.3390/nu10111591.

Abstract

Copper, which can potentially be a highly toxic agent, is an essential nutrient due to its role as a cofactor for cuproenzymes and its participation in signaling pathways. In mammals, the liver is a central organ that controls copper turnover throughout the body, including copper absorption, distribution, and excretion. In ontogenesis, there are two types of copper metabolism, embryonic and adult, which maintain the balance of copper in each of these periods of life, respectively. In the liver cells, these types of metabolism are characterized by the specific expression patterns and activity levels of the genes encoding ceruloplasmin, which is the main extracellular ferroxidase and copper transporter, and the proteins mediating ceruloplasmin metalation. In newborns, the molecular genetic mechanisms responsible for copper homeostasis and the ontogenetic switch from embryonic to adult copper metabolism are highly adapted to milk ceruloplasmin as a dietary source of copper. In the mammary gland cells, the level of ceruloplasmin gene expression and the alternative splicing of its pre-mRNA govern the amount of ceruloplasmin in the milk, and thus, the amount of copper absorbed by a newborn is controlled. In newborns, the absorption, distribution, and accumulation of copper are adapted to milk ceruloplasmin. If newborns are not breast-fed in the early stages of postnatal development, they do not have this natural control ensuring alimentary copper balance in the body. Although there is still much to be learned about the neonatal consequences of having an imbalance of copper in the mother/newborn system, the time to pay attention to this problem has arrived because the neonatal misbalance of copper may provoke the development of copper-related disorders.

摘要

铜是一种潜在的高毒性物质,但由于其作为铜酶辅助因子的作用及其在信号通路中的参与,铜也是一种必需的营养物质。在哺乳动物中,肝脏是控制全身铜周转的重要器官,包括铜的吸收、分布和排泄。在个体发生过程中,有两种类型的铜代谢,即胚胎期和成人期,它们分别维持着生命中每个时期的铜平衡。在肝细胞中,这两种代谢类型的特征是编码铜蓝蛋白的基因的特定表达模式和活性水平,铜蓝蛋白是主要的细胞外亚铁氧化酶和铜转运蛋白,以及介导铜蓝蛋白金属化的蛋白质。在新生儿中,负责铜稳态的分子遗传机制和从胚胎期到成人期铜代谢的发育转变高度适应于乳铜蓝蛋白作为铜的膳食来源。在乳腺细胞中,铜蓝蛋白基因表达水平和其前体 mRNA 的选择性剪接控制着乳中的铜蓝蛋白含量,从而控制新生儿吸收的铜量。在新生儿中,铜的吸收、分布和积累都适应于乳铜蓝蛋白。如果新生儿在出生后早期没有母乳喂养,他们就没有这种天然的控制机制来确保体内铜的营养平衡。尽管关于母儿系统中铜失衡对新生儿的影响还有很多需要了解的地方,但现在是关注这个问题的时候了,因为新生儿铜的失衡可能会引发与铜相关的疾病的发展。

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