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钙网蛋白在维持细胞稳态和功能中的作用(综述)

Role of regucalcin in maintaining cell homeostasis and function (review).

作者信息

Yamaguchi Masayoshi

机构信息

Laboratory of Endocrinology and Molecular Metabolism, Graduate School of Nutritional Sciences, University of Shizuoka, Shizuoka 422-8526, Japan.

出版信息

Int J Mol Med. 2005 Mar;15(3):371-89.

Abstract

Regucalcin was discovered in 1978 as a Ca(2+)-binding protein that does not contain EF-hand motif of Ca(2+)-binding domain. The name regucalcin was proposed for this Ca2(2+)binding protein, which can regulate liver cell functions related to Ca(2+). The regucalcin gene is localized on chromosome X, and the organization of the regucalcin gene consists of seven exons and six introns. AP-1 and NFI-A1 can bind to the promoter region of the rat regucalcin gene to mediate the Ca(2+) response for transcriptional activation. Regucalcin plays a pivotal role in maintaining intracellular Ca(2+) homeostasis due to activating Ca(2+) pump enzymes in the plasma membrane (basolateral membrane), microsomes (endoplasmic reticulum) and mitochondria of many cell types. Regucalcin has a suppressive effect on Ca(2+) signaling from the cytoplasm to the nucleus in the proliferative cells. Also, regucalcin has been demonstrated to transport to nucleus, and it can inhibit nuclear protein kinase, protein phosphatase, and deoxyribonucleic acid (DNA) and ribonucleic acid (RNA) synthesis. Regucalcin can control enhancement of cell proliferation due to hormonal stimulation. Moreover, overexpression of regucalcin suppresses cell death and apoptosis in the cloned rat hepatoma cells induced by various signaling factors. Regucalcin plays a multifunctional role in the regulation of cellular function in liver, kidney cortex, heart and brain. Moreover, regucalcin-overexpressing rat has been shown to induce bone loss and hyperlipidemia with increasing age, indicating a pathophysiologic role. Regucalcin transgenic rat may be useful as an animal model in osteoporosis and hyperlipidemia. Thus, regucalcin plays a pivotal role in maintaining cell homeostasis and function. Regucalcin gene expression-related diseases may be found in human.

摘要

调钙素于1978年被发现,是一种不含有钙结合结构域的EF手基序的钙结合蛋白。该钙结合蛋白被命名为调钙素,它可以调节与钙相关的肝细胞功能。调钙素基因定位于X染色体,其基因结构由7个外显子和6个内含子组成。AP - 1和NFI - A1可以结合大鼠调钙素基因的启动子区域,介导钙反应以进行转录激活。调钙素在维持细胞内钙稳态方面起着关键作用,因为它能激活多种细胞类型的质膜(基底外侧膜)、微粒体(内质网)和线粒体中的钙泵酶。调钙素对增殖细胞中从细胞质到细胞核的钙信号传导具有抑制作用。此外,调钙素已被证明可转运至细胞核,并且它可以抑制核蛋白激酶、蛋白磷酸酶以及脱氧核糖核酸(DNA)和核糖核酸(RNA)的合成。调钙素可以控制因激素刺激引起的细胞增殖增强。此外,调钙素的过表达可抑制由各种信号因子诱导的克隆大鼠肝癌细胞中的细胞死亡和凋亡。调钙素在肝脏、肾皮质、心脏和大脑的细胞功能调节中发挥着多功能作用。此外,过表达调钙素的大鼠已被证明随着年龄增长会导致骨质流失和高脂血症,表明其具有病理生理作用。调钙素转基因大鼠可能作为骨质疏松症和高脂血症的动物模型。因此,调钙素在维持细胞稳态和功能方面起着关键作用。在人类中可能会发现与调钙素基因表达相关的疾病。

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