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首页> 外文期刊>The Journal of Nutritional Biochemistry >Glucose as a fetal nutrient: dynamic regulation of several glucose transporter genes by DNA methylation in the human placenta across gestation.
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Glucose as a fetal nutrient: dynamic regulation of several glucose transporter genes by DNA methylation in the human placenta across gestation.

机译:葡萄糖作为胎儿的营养物质:整个妊娠过程中人胎盘中的DNA甲基化可动态调节几种葡萄糖转运蛋白基因。

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摘要

The human placenta ensures proper fetal development through the regulation of nutrient and gas transfer from the mother to the fetus and the removal of waste products from the fetal circulation. Glucose is one of the major nutrients for the growing fetus. Its transport across the placenta to the fetus is mediated by a family of facilitative transporter proteins, known as the glucose transporters (GLUTs), encoded by the SLC2A family of genes. There are 14 members of this gene family, and the expression of several of these has been shown in human placenta; however, aside from GLUT1 and GLUT3, little is known about the role of these proteins in placental function, fetal development and disease. In this study, we analysed previously generated genome-scale DNA methylation and gene expression data to examine the role of methylation in GLUT expression throughout gestation. We found evidence that DNA methylation regulates expression of GLUT3 and GLUT10, while the constitutively expressed GLUT1 showed no promoter methylation. We further analysed the level of DNA methylation across the promoter region of GLUT3, previously shown to be involved in glucose back-flux from the fetal circulation into the placenta. Using the Sequenom EpiTYPER platform, we found increasing DNA methylation of this gene in association with decreasing expression as gestation progresses, thereby highlighting the role of epigenetic modifications in regulating the GLUT family of genes in the placenta during pregnancy. These findings warrant a reexamination of the role of additional GLUT family members in the placenta in pregnancy and disease. All rights reserved, Elsevier.
机译:人类胎盘通过调节从母亲到胎儿的营养和气体转移以及从胎儿循环中清除废物来确保胎儿的正常发育。葡萄糖是胎儿成长的主要营养物质之一。 SLC2A基​​因家族编码的一系列便利转运蛋白(称为葡萄糖转运蛋白(GLUT))介导了其跨胎盘转运至胎儿的过程。该基因家族有14个成员,其中一些在人胎盘中已表达。但是,除了GLUT1和GLUT3以外,关于这些蛋白在胎盘功能,胎儿发育和疾病中的作用知之甚少。在这项研究中,我们分析了先前生成的基因组规模的DNA甲基化和基因表达数据,以检查整个妊娠过程中甲基化在GLUT表达中的作用。我们发现证据表明,DNA甲基化调节GLUT3和GLUT10的表达,而组成型表达的GLUT1没有启动子甲基化。我们进一步分析了GLUT3启动子区域的DNA甲基化水平,该区域先前已显示参与从胎儿循环到胎盘的葡萄糖反流。使用Sequenom EpiTYPER平台,我们发现该基因的DNA甲基化增加与妊娠进程中表达的降低有关,从而突显了表观遗传修饰在妊娠期间调节胎盘中GLUT基因家族中的作用。这些发现需要重新检查其他GLUT家族成员在妊娠和疾病的胎盘中的作用。保留所有权利,Elsevier。

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