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在氨基酸饥饿后,永生化下丘脑细胞系N25/2中众多溶质载体转运蛋白的基因表达发生了改变。

The gene expression of numerous SLC transporters is altered in the immortalized hypothalamic cell line N25/2 following amino acid starvation.

作者信息

Hellsten Sofie V, Lekholm Emilia, Ahmad Tauseef, Fredriksson Robert

机构信息

Department of Pharmaceutical Bioscience, Molecular Neuropharmacology Uppsala University Sweden; Department of Neuroscience, Functional Pharmacology Uppsala University Sweden.

Department of Pharmaceutical Bioscience, Molecular Neuropharmacology Uppsala University Sweden.

出版信息

FEBS Open Bio. 2017 Jan 11;7(2):249-264. doi: 10.1002/2211-5463.12181. eCollection 2017 Feb.

Abstract

Amino acids are known to play a key role in gene expression regulation, and in mammalian cells, amino acid signaling is mainly mediated via two pathways, the mammalian target of rapamycin complex 1 (mTORC1) pathway and the amino acid responsive (AAR) pathway. It is vital for cells to have a system to sense amino acid levels, in order to control protein and amino acid synthesis and catabolism. Amino acid transporters are crucial in these pathways, due to both their sensing and transport functions. In this large-scale study, an immortalized mouse hypothalamic cell line (N25/2) was used to study the gene expression changes following 1, 2, 3, 5 or 16 h of amino acid starvation. We focused on genes encoding solute carriers (SLCs) and putative SLCs, more specifically on amino acid transporters. The microarray contained 28 270 genes and 86.2% of the genes were expressed in the cell line. At 5 h of starvation, 1001 genes were upregulated and 848 genes were downregulated, and among these, 47 genes from the SLC superfamily or atypical SLCs were found. Of these, 15 were genes encoding amino acid transporters and 32 were genes encoding other SLCs or atypical SLCs. Increased expression was detected for genes encoding amino acid transporters from system A, ASC, L, N, T, xc-, and y+. Using GO annotations, genes involved in amino acid transport and amino acid transmembrane transporter activity were found to be most upregulated at 3 h and 5 h of starvation.

摘要

已知氨基酸在基因表达调控中起关键作用,在哺乳动物细胞中,氨基酸信号主要通过两条途径介导,即雷帕霉素复合物1(mTORC1)途径和氨基酸应答(AAR)途径。细胞拥有感知氨基酸水平的系统对于控制蛋白质和氨基酸的合成及分解代谢至关重要。氨基酸转运体在这些途径中至关重要,这是由于它们兼具感知和转运功能。在这项大规模研究中,使用永生化小鼠下丘脑细胞系(N25/2)来研究氨基酸饥饿1、2、3、5或16小时后的基因表达变化。我们重点关注编码溶质载体(SLC)和假定SLC的基因,更具体地说是氨基酸转运体。微阵列包含28270个基因,其中86.2%的基因在该细胞系中表达。饥饿5小时时,1001个基因上调,848个基因下调,其中发现了来自SLC超家族或非典型SLC的47个基因。其中,15个是编码氨基酸转运体的基因,32个是编码其他SLC或非典型SLC的基因。检测到来自A、ASC、L、N、T、xc-和y+系统的氨基酸转运体编码基因表达增加。使用基因本体注释发现,参与氨基酸转运和氨基酸跨膜转运体活性的基因在饥饿3小时和5小时时上调最为明显。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9163/5292668/97a578d2bf3b/FEB4-7-249-g001.jpg

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