Literature DB >> 21903590

MYC protein inhibits transcription of the microRNA cluster MC-let-7a-1~let-7d via noncanonical E-box.

Zifeng Wang1, Sheng Lin, Julia Jun Li, Zhenhua Xu, Hong Yao, Xiao Zhu, Dan Xie, Zan Shen, Johnny Sze, Kui Li, Gang Lu, Danny Tat-Ming Chan, Wai Sang Poon, Hsiang-fu Kung, Marie Chia-mi Lin.   

Abstract

The human microRNA cluster MC-let-7a-1let-7d, with three members let-7a-1, let-7f-1, and let-7d, is an important cluster of the let-7 family. These microRNAs play critical roles in regulating development and carcinogenesis. Therefore, precise control of MC-let-7a-1let-7d level is critical for cellular functions. In this study, we first showed that the expression of these three members was significantly reduced in human hepatocellular carcinoma HepG2 cells as compared with the immortalized human liver L02 cells. We demonstrated that the MC-let-7a-1let-7d cluster was encoded by a single polycistronic transcript driven by a 10-kb upstream promoter, with two MYC-binding sites. Importantly, MYC inhibited MC-let-7a-1let-7d promoter activity via binding to the noncanonical E-box 3 downstream of the transcription start sites, whereas it enhanced promoter activity by binding to the canonical E-box 2 upstream of the transcription start sites. We found that although the binding affinity of MYC to E-box 2 was stronger than E-box 3, the binding quantum of MYC to E-box 3 was significantly higher in cancerous HepG2 cells as compared with the noncancerous L02 cells. In addition, forced expression of let-7 could reverse the MYC-mediated cell proliferation. These findings suggested that in L02 cells with a low level of MYC, MYC binds mainly to E-box 2 to enhance MC-let-7a-1let-7d expression. However, in HepG2 cells with an elevated MYC, the extra MYC could bind to E-box 3 to suppress the transcription of MC-let-7a-1let-7d and thus enable HepG2 cells to maintain a high level of MYC and a low level of let-7 microRNAs simultaneously.

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Year:  2011        PMID: 21903590      PMCID: PMC3220549          DOI: 10.1074/jbc.M111.293126

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  60 in total

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  33 in total

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7.  MicroRNAs As Biomarkers For Clinical Features Of Lung Cancer.

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Review 8.  MYC cofactors: molecular switches controlling diverse biological outcomes.

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9.  LIN28 Selectively Modulates a Subclass of Let-7 MicroRNAs.

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10.  MYCN-driven regulatory mechanisms controlling LIN28B in neuroblastoma.

Authors:  Anneleen Beckers; Gert Van Peer; Daniel R Carter; Moritz Gartlgruber; Carl Herrmann; Saurabh Agarwal; Hetty H Helsmoortel; Kristina Althoff; Jan J Molenaar; Belamy B Cheung; Johannes H Schulte; Yves Benoit; Jason M Shohet; Frank Westermann; Glenn M Marshall; Jo Vandesompele; Katleen De Preter; Frank Speleman
Journal:  Cancer Lett       Date:  2015-06-26       Impact factor: 8.679

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