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十二指肠上皮细胞对慢性代谢性酸中毒反应的基因表达谱

Gene expression profile of duodenal epithelial cells in response to chronic metabolic acidosis.

作者信息

Wongdee Kannikar, Teerapornpuntakit Jarinthorn, Riengrojpitak Suda, Krishnamra Nateetip, Charoenphandhu Narattaphol

机构信息

Consortium for Calcium and Bone Research, Faculty of Science, Mahidol University, Bangkok, Thailand.

出版信息

Mol Cell Biochem. 2009 Jan;321(1-2):173-88. doi: 10.1007/s11010-008-9931-1. Epub 2008 Nov 4.

Abstract

Chronic metabolic acidosis (CMA) affects ion transport, permeability, and metabolism of the intestinal absorptive cells. Most effects of CMA on the intestine are long-term adaptations at genomic level. To identify the CMA-regulated genes, the Illumina's microarray featuring high-performance BeadArray technology was performed on RNA samples from the rat duodenal epithelial cells exposed to long-standing acidemia. After 21 days of CMA, we found 423 transcripts upregulated and 261 transcripts downregulated. Gene ontology analysis suggested effects of CMA on cellular processes, such as cell adhesion, proliferation, fuel metabolism, and biotransformation. Interestingly, 27 upregulated transcripts (e.g., Aqp1, Cacnb1, Atp1a2, Kcnab2, and Slc2a1) and 13 downregulated transcripts (e.g., Slc17a7, Slc9a4, and Slc30a3) are involved in the absorption of water, ions, and nutrients. Some upregulated genes, such as Slc38a5 and Slc1a7 encoding glutamine transporters, may be parts of the total body adaptation to alleviate negative nitrogen balance. Therefore, the present results provided a novel genome-wide information for further investigations of the mechanism of CMA effect on the intestine.

摘要

慢性代谢性酸中毒(CMA)会影响肠道吸收细胞的离子转运、通透性和代谢。CMA对肠道的大多数影响是基因组水平上的长期适应性变化。为了鉴定受CMA调控的基因,我们使用具有高性能BeadArray技术的Illumina微阵列,对长期处于酸血症状态的大鼠十二指肠上皮细胞的RNA样本进行检测。在CMA处理21天后,我们发现423个转录本上调,261个转录本下调。基因本体分析表明,CMA对细胞过程有影响,如细胞黏附、增殖、能量代谢和生物转化。有趣的是,27个上调的转录本(如Aqp1、Cacnb1、Atp1a2、Kcnab2和Slc2a1)和13个下调的转录本(如Slc17a7、Slc9a4和Slc30a3)参与水、离子和营养物质的吸收。一些上调的基因,如编码谷氨酰胺转运蛋白的Slc38a5和Slc1a7,可能是全身适应性变化的一部分,以减轻负氮平衡。因此,本研究结果为进一步研究CMA对肠道影响的机制提供了全新的全基因组信息。

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