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AGO2 promotes telomerase activity and interaction between the telomerase components TERT and TERC

机译:前2促进端粒酶活性和端粒酶组分Tert和Terc之间的相互作用

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Telomerase reverse transcriptase (TERT) and telomerase RNA component (TERC) constitute the core telomerase enzyme that maintains the length of telomeres. Telomere maintenance is affected in a broad range of cancer and degenerative disorders. Taking advantage of gain-and loss-of-function approaches, we show that Argonaute 2 (AGO2) promotes telomerase activity and stimulates the association between TERT and TERC. AGO2 depletion results in shorter telomeres as well as in lower proliferation rates in vitro and in vivo. We also demonstrate that AGO2 interacts with TERC and with a newly identified sRNA (terc-sRNA), arising from the H/ACA box of TERC. Notably, terc-sRNA is sufficient to enhance telomerase activity when overexpressed. Analyses of sRNA-Seq datasets show that terc-sRNA is detected in primary human tissues and increases in tumors as compared to control tissues. Collectively, these data uncover a new layer of complexity in the regulation of telomerase activity by AGO2 and might lay the foundation for new therapeutic targets in tumors and telomere diseases.
机译:端粒酶逆转录酶(TERT)和端粒酶RNA组分(TERC)构成维持端粒长度的核心端粒酶酶。端粒维持在广泛的癌症和退行性障碍中受到影响。利用增益和功能丧失的方法,我们表明Argonaute 2(前)促进端粒酶活性,并刺激TERT和TERC之间的关联。前2次耗尽导致缩短端粒,以及体外较低的增殖率。我们还证明,AGO2与TERC和NEW识别的SRNA(TERC-SRNA)相互作用,由TERC的H / ACA盒产生。值得注意的是,TERC-SRNA足以在过表达时增强端粒酶活性。 SRNA-SEQ数据集的分析表明,与对照组织相比,在一次人体组织中检测到TERC-SRNA并增加肿瘤。统称,这些数据在以往2的调节中发现了一种新的复杂性层,可能为肿瘤和端粒疾病的新治疗靶标的基础。

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