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HoxC5 和 miR-615-3p 靶向新进化的基因组区域,抑制 hTERT 并抑制肿瘤发生。

HoxC5 and miR-615-3p target newly evolved genomic regions to repress hTERT and inhibit tumorigenesis.

机构信息

Cancer and Stem Cell Biology Program, Duke-NUS Medical School, 8 College Road, Singapore, 169857, Singapore.

Cancer Therapeutics and Stratified Oncology, Genome Institute of Singapore, 60 Biopolis Street, Singapore, 138672, Singapore.

出版信息

Nat Commun. 2018 Jan 8;9(1):100. doi: 10.1038/s41467-017-02601-1.

Abstract

The repression of telomerase activity during cellular differentiation promotes replicative aging and functions as a physiological barrier for tumorigenesis in long-lived mammals, including humans. However, the underlying mechanisms remain largely unclear. Here we describe how miR-615-3p represses hTERT expression. mir-615-3p is located in an intron of the HOXC5 gene, a member of the highly conserved homeobox family of transcription factors controlling embryogenesis and development. Unexpectedly, we found that HoxC5 also represses hTERT expression by disrupting the long-range interaction between hTERT promoter and its distal enhancer. The 3'UTR of hTERT and its upstream enhancer region are well conserved in long-lived primates. Both mir-615-3p and HOXC5 are activated upon differentiation, which constitute a feed-forward loop that coordinates transcriptional and post-transcriptional repression of hTERT during cellular differentiation. Deregulation of HOXC5 and mir-615-3p expression may contribute to the activation of hTERT in human cancers.

摘要

在细胞分化过程中,端粒酶活性受到抑制,促进了复制性衰老,并作为包括人类在内的长寿哺乳动物肿瘤发生的生理屏障。然而,其潜在机制在很大程度上仍不清楚。在这里,我们描述了 miR-615-3p 如何抑制 hTERT 的表达。miR-615-3p 位于 HOXC5 基因的内含子中,HOXC5 基因是高度保守的同源盒转录因子家族的成员,该家族控制着胚胎发生和发育。出乎意料的是,我们发现 HoxC5 还通过破坏 hTERT 启动子与其远端增强子之间的长距离相互作用来抑制 hTERT 的表达。hTERT 的 3'UTR 及其上游增强子区域在长寿灵长类动物中高度保守。miR-615-3p 和 HOXC5 在分化时均被激活,构成了一个正反馈回路,在细胞分化过程中协调 hTERT 的转录和转录后抑制。HOXC5 和 mir-615-3p 表达的失调可能导致人类癌症中 hTERT 的激活。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/de6f/5758779/2e254f04ca32/41467_2017_2601_Fig1_HTML.jpg

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