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用于端粒酶研究的小鼠模型。

Mouse models for the study of telomerase.

作者信息

Blasco M A, Lee H W, Rizen M, Hanahan D, DePinho R, Greider C W

机构信息

Department of Immunology and Oncology, Centro Nacional de Biotecnología, Madrid, Spain.

出版信息

Ciba Found Symp. 1997;211:160-70; discussion 170-6. doi: 10.1002/9780470515433.ch11.

Abstract

The ends of chromosomes, or telomeres, consist of short repeated sequences that are synthesized by a ribonucleoprotein-DNA polymerase called telomerase. The RNA component of telomerase is essential for enzyme activity. The maintenance of telomere length by telomerase has been proposed to be essential for cellular viability and to play an important role in cellular senescence and immortalization. We are interested in using the mouse as a model system for the study of telomerase. We studied telomerase activity and expression of the mouse telomerase RNA component (mTR) in two different transgenic mouse models of multistage tumorigenesis: models of islet cell carcinoma and squamous cell carcinoma. In both tumour models, telomerase activity was detected only in late-stage tumours, whereas the telomerase RNA was present at higher than normal levels in pre-neoplastic stages and increased further in late-stage tumours. However, the RNA levels did not parallel the amounts of telomerase activity detected, suggesting that regulation of telomerase activity does not correlate with the regulation of its RNA component. These results establish a direct correlation between progression to late-stage tumours and induction of telomerase activity, and suggest that the initial upregulation of telomerase RNA is an early event. To address the role of telomerase during normal mouse development and tumour formation, we have constructed a knockout mouse for the mouse telomerase RNA, mTR-/-. These mice and the cell lines derived from them are telomerase deficient.

摘要

染色体末端,即端粒,由短的重复序列组成,这些序列由一种称为端粒酶的核糖核蛋白-DNA聚合酶合成。端粒酶的RNA成分对酶活性至关重要。有人提出,端粒酶维持端粒长度对细胞活力至关重要,并在细胞衰老和永生化过程中发挥重要作用。我们有兴趣将小鼠作为研究端粒酶的模型系统。我们在两种不同的多阶段肿瘤发生转基因小鼠模型中研究了端粒酶活性和小鼠端粒酶RNA成分(mTR)的表达:胰岛细胞癌模型和鳞状细胞癌模型。在这两种肿瘤模型中,仅在晚期肿瘤中检测到端粒酶活性,而端粒酶RNA在肿瘤前阶段的水平高于正常水平,并在晚期肿瘤中进一步增加。然而,RNA水平与检测到的端粒酶活性量并不平行,这表明端粒酶活性的调节与其RNA成分的调节不相关。这些结果建立了进展到晚期肿瘤与端粒酶活性诱导之间的直接关联,并表明端粒酶RNA的初始上调是一个早期事件。为了研究端粒酶在正常小鼠发育和肿瘤形成过程中的作用,我们构建了一种小鼠端粒酶RNA基因敲除小鼠,即mTR-/-。这些小鼠及其衍生的细胞系均缺乏端粒酶。

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