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功能性替代端粒酶RNA组分基因在小鼠大脑和运动神经元细胞中的表达可抵御氧化应激。

Expression of functional alternative telomerase RNA component gene in mouse brain and in motor neurons cells protects from oxidative stress.

作者信息

Eitan Erez, Tamar Admoni, Yossi Grin, Peleg Refael, Braiman Alex, Priel Esther

机构信息

The Shraga Segal Department Microbiology, Immunology & Genetics, Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel.

出版信息

Oncotarget. 2016 Nov 29;7(48):78297-78309. doi: 10.18632/oncotarget.13049.

Abstract

Telomerase, a ribonucleoprotein, is highly expressed and active in many tumor cells and types, therefore it is considered to be a target for anti-cancer agents. On the other hand, recent studies demonstrated that activation of telomerase is a potential therapeutic target for age related diseases. Telomerase mainly consists of a catalytic protein subunit with a reverse transcription activity (TERT) and an RNA component (TERC), a long non-coding RNA, which serves as a template for the re-elongation of telomeres by TERT. We previously showed that TERT is highly expressed in distinct neuronal cells of the mouse brain and its expression declined with age. To understand the role of telomerase in non-mitotic, fully differentiated cells such neurons we here examined the expression of the other component, TERC, in mouse brain. Surprisingly, by first using bioinformatics analysis, we identified an alternative TERC gene (alTERC) in the mouse genome. Using further experimental approaches we described the presence of a functional alTERC in the mouse brain and spleen, in cultures of motor neurons- like cells and neuroblastoma tumor cells. The alTERC is similar (87%) to mouse TERC (mTERC) with a deletion of 18 bp in the TERC conserved region 4 (CR4). This alTERC gene is expressed and its product interacts with the endogenous mTERT protein and with an exogenous human TERT protein (hTERT) to form an active enzyme. Overexpression of the alTERC and the mTERC genes, in mouse motor neurons like cells, increased the activity of TERT without affecting its protein level. Under oxidative stress conditions, alTERC significantly increased the survival of motor neurons cells without altering the level of TERT protein or its activity.The results suggest that the expression of the alTERC gene in the mouse brain provides an additional way for regulating telomerase activity under normal and stress conditions and confers protection to neuronal cells from oxidative stress.

摘要

端粒酶是一种核糖核蛋白,在许多肿瘤细胞及肿瘤类型中高表达且具有活性,因此它被视为抗癌药物的一个靶点。另一方面,最近的研究表明,端粒酶的激活是与年龄相关疾病的一个潜在治疗靶点。端粒酶主要由具有逆转录活性的催化蛋白亚基(TERT)和RNA组分(TERC)组成,TERC是一种长链非编码RNA,作为TERT重新延长端粒的模板。我们之前发现TERT在小鼠大脑的特定神经元细胞中高表达,且其表达随年龄下降。为了解端粒酶在诸如神经元这类非有丝分裂、完全分化细胞中的作用,我们在此检测了小鼠大脑中另一组分TERC的表达。令人惊讶的是,通过首先进行生物信息学分析,我们在小鼠基因组中鉴定出一个替代性TERC基因(alTERC)。使用进一步的实验方法,我们描述了功能性alTERC在小鼠大脑和脾脏、运动神经元样细胞培养物及神经母细胞瘤肿瘤细胞中的存在情况。alTERC与小鼠TERC(mTERC)相似(87%),在TERC保守区域4(CR4)中缺失18个碱基对。这个alTERC基因表达,其产物与内源性mTERT蛋白以及外源性人TERT蛋白(hTERT)相互作用形成一种活性酶。在小鼠运动神经元样细胞中过表达alTERC和mTERC基因,增加了TERT的活性而不影响其蛋白水平。在氧化应激条件下,alTERC显著提高了运动神经元细胞的存活率,而不改变TERT蛋白水平或其活性。结果表明,alTERC基因在小鼠大脑中的表达为在正常和应激条件下调节端粒酶活性提供了另一种方式,并赋予神经元细胞对氧化应激的保护作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/69e2/5346639/cf715204f008/oncotarget-07-78297-g001.jpg

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