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小鼠端粒酶RNA的结构特征导致小鼠端粒酶的活性低于人类端粒酶。

Structural features of mouse telomerase RNA are responsible for the lower activity of mouse telomerase versus human telomerase.

作者信息

Garforth Scott J, Wu Yan Yun, Prasad Vinayaka R

机构信息

Department of Microbiology and Immunology, Albert Einstein College of Medicine, 1300 Morris Park Avenue, GB401, Bronx, NY 10461, USA.

出版信息

Biochem J. 2006 Aug 1;397(3):399-406. doi: 10.1042/BJ20060456.

Abstract

Human and mouse telomerases show a high degree of similarity in both the protein and RNA components. Human telomerase is more active and more processive than the mouse telomerase. There are two key differences between hTR [human TR (telomerase RNA)] and mTR (mouse TR) structures. First, the mouse telomerase contains only 2 nt upstream of its template region, whereas the human telomerase contains 45 nt. Secondly, the template region of human telomerase contains a 5-nt alignment domain, whereas that of mouse has only 2 nt. We hypothesize that these differences are responsible for the differential telomerase activities. Mutations were made in both the hTR and mTR, changing the template length and the length of the RNA upstream of the template, and telomerase was reconstituted in vitro using mouse telomerase reverse transcriptase generated by in vitro translation. We show that the sequences upstream of the template region, with a potential to form a double-stranded helix (the P1 helix) as in hTR, increase telomerase activity. The longer alignment domain increases telomerase activity only in the context of the P1 helix. Thus the TR contributes to regulating the level of activity of mammalian telomerases.

摘要

人类和小鼠的端粒酶在蛋白质和RNA成分上都表现出高度的相似性。人类端粒酶比小鼠端粒酶更具活性且持续性更强。人类端粒酶RNA(hTR)和小鼠端粒酶RNA(mTR)的结构存在两个关键差异。首先,小鼠端粒酶在其模板区域上游仅含有2个核苷酸,而人类端粒酶含有45个核苷酸。其次,人类端粒酶的模板区域包含一个5个核苷酸的比对结构域,而小鼠的只有2个核苷酸。我们推测这些差异导致了端粒酶活性的不同。对hTR和mTR都进行了突变,改变了模板长度和模板上游RNA的长度,并使用体外翻译产生的小鼠端粒酶逆转录酶在体外重建端粒酶。我们发现,如hTR中那样,模板区域上游具有形成双链螺旋(P1螺旋)潜力的序列会增加端粒酶活性。更长的比对结构域仅在P1螺旋的情况下会增加端粒酶活性。因此,端粒酶RNA有助于调节哺乳动物端粒酶的活性水平。

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