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妊娠向泌乳的同源适应:大鼠从妊娠向泌乳过渡过程中乳腺、肝脏和脂肪组织的比较转录组分析。

Homeorhetic adaptation to lactation: comparative transcriptome analysis of mammary, liver, and adipose tissue during the transition from pregnancy to lactation in rats.

机构信息

Department of Cell and Molecular Biology, Grand Valley State University, Allendale, MI 49401, USA.

出版信息

Funct Integr Genomics. 2011 Mar;11(1):193-202. doi: 10.1007/s10142-010-0193-0. Epub 2010 Sep 18.

Abstract

Tissue-specific shifts in a dam's metabolism to support fetal and neonatal growth during pregnancy and lactation are controlled by differential expression of regulatory genes. The goal of this study was to identify a more detailed cohort of genes in mammary, liver, and adipose tissue that are transcriptionally controlled during the pregnancy to lactation evolution and explore the relationship of these genes to core clock genes. Total RNA was isolated from mammary, liver and adipose tissues collected from rat dams on day 20 of pregnancy (P20) and day 1 of lactation (L1) and gene expression was measured using Rat 230 2.0 Affymetrix GeneChips. Gene functional analysis revealed that pathway associated metabolism (carbohydrate, amino acid, lipid, cholesterol, protein) were enriched (P < 0.001) in the mammary gland during P20 to L1 transition. Approximately 50% of the genes associated with solute transport, as well as lipogenesis were up-regulated in the mammary gland during P20 to L1 transition compared to 10% in liver and 15% in adipose tissue. Genes engaged in conveying glucose (INSR, GLUT1, GLUT4, SGLT1, and SGLT2), bicarbonate (SLC4), sodium (SLC9), zinc (SLC30), copper (SLC31), iron (SLC40) in tandem with rate-limiting lipogenic genes (ACACA, FASN, PRLR, SREBP2, THRSP) were specifically enriched in the mammary gland during the P20 to L1 evolution. Our results provide insight into a cross-tissue transcriptional repertoire that is associated with homeorhetic adaptation needed to support lactation, and at the onset of lactation the mammary gland becomes a factory for macromolecular biosynthesis through inducing genes participating in nutrient transfer and lipid biosynthesis.

摘要

组织特异性代谢变化以支持妊娠和哺乳期胎儿和新生儿的生长是由调节基因的差异表达控制的。本研究的目的是鉴定更多在妊娠到哺乳期进化过程中受转录调控的乳腺、肝脏和脂肪组织中的基因,并探讨这些基因与核心时钟基因的关系。从妊娠第 20 天(P20)和第 1 天(L1)的大鼠母鼠的乳腺、肝脏和脂肪组织中分离总 RNA,并使用 Rat 230 2.0 Affymetrix GeneChips 测量基因表达。基因功能分析表明,与代谢途径(碳水化合物、氨基酸、脂质、胆固醇、蛋白质)相关的基因在 P20 到 L1 过渡期间在乳腺中富集(P<0.001)。与 10%在肝脏和 15%在脂肪组织中相比,大约 50%与溶质转运以及脂肪生成相关的基因在 P20 到 L1 过渡期间在乳腺中上调。参与葡萄糖(INSR、GLUT1、GLUT4、SGLT1 和 SGLT2)、碳酸氢盐(SLC4)、钠(SLC9)、锌(SLC30)、铜(SLC31)、铁(SLC40)传递的基因与限速脂肪生成基因(ACACA、FASN、PRLR、SREBP2、THRSP)一起在 P20 到 L1 进化期间在乳腺中特异性富集。我们的结果提供了对与支持哺乳所需的同源适应相关的跨组织转录组的深入了解,并且在哺乳期开始时,乳腺通过诱导参与营养转移和脂质生物合成的基因成为大分子生物合成的工厂。

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