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由单个哺乳动物基因编码的O-连接N-乙酰葡糖胺转移酶的线粒体和核质异构体。

Mitochondrial and nucleocytoplasmic isoforms of O-linked GlcNAc transferase encoded by a single mammalian gene.

作者信息

Hanover John A, Yu Song, Lubas William B, Shin Sang Hoon, Ragano-Caracciola Maria, Kochran Jarema, Love Dona C

机构信息

Laboratory of Cell Biochemistry and Biology, NIDDK, National Institutes of Health, Building 8, Room 402, 8 Center Drive, MSC 0850, NIH, Bethesda, MD 20892-0850, USA.

出版信息

Arch Biochem Biophys. 2003 Jan 15;409(2):287-97. doi: 10.1016/s0003-9861(02)00578-7.

Abstract

O-Linked N-acetylglucosamine (GlcNAc) transferase (OGT) mediates a novel hexosamine-dependent signal transduction pathway. Yet, little is known about the regulation of ogt gene expression in mammals. We report the sequence and characterization of the mouse ogt locus and provide a comparison with the human and rat ogt genes. The mammalian ogt genes are similar in structure and exhibit approximately 80% sequence identity. The mouse and human ogt genes contain two potential promoters producing four major transcripts. By analyzing 56 human cDNA clones and other existing expressed sequence tags, we found that at least three protein products differing at their amino terminus result from alternative splicing. We used OGT-specific antisera to demonstrate the presence of these isoforms in HeLa cells. The longest form is a nucleocytoplasmic OGT (ncOGT) with 12 tetratricopeptide repeats (TPRs); a shorter form of OGT encodes a mitochondrially sequestered enzyme with 9 TPRs and an N-terminal mitochondrion-targeting sequence (mOGT). An even shorter form of OGT (sOGT) contains only 2 TPRs. The genomic organization of OGT appears to be highly conserved throughout metazoan evolution. These results provide the basis for a more detailed analysis of the significance and regulation of the nucleocytoplasmic and mitochondrial isoforms of OGT in mammals.

摘要

O-连接的N-乙酰葡糖胺(GlcNAc)转移酶(OGT)介导一种新型的己糖胺依赖性信号转导途径。然而,关于哺乳动物中ogt基因表达的调控知之甚少。我们报告了小鼠ogt基因座的序列和特征,并与人类和大鼠的ogt基因进行了比较。哺乳动物的ogt基因在结构上相似,序列同一性约为80%。小鼠和人类的ogt基因包含两个潜在启动子,产生四种主要转录本。通过分析56个人类cDNA克隆和其他现有的表达序列标签,我们发现至少有三种在氨基末端不同的蛋白质产物是由可变剪接产生的。我们使用OGT特异性抗血清来证明这些异构体在HeLa细胞中的存在。最长的形式是一种具有12个四肽重复序列(TPR)的核质OGT(ncOGT);较短形式的OGT编码一种具有9个TPR和N端线粒体靶向序列的线粒体隔离酶(mOGT)。甚至更短形式的OGT(sOGT)仅包含2个TPR。OGT的基因组组织在整个后生动物进化过程中似乎高度保守。这些结果为更详细地分析哺乳动物中OGT的核质和线粒体异构体的意义和调控提供了基础。

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