MYC通过一种线粒体检查点机制被下调。

MYC is downregulated by a mitochondrial checkpoint mechanism.

作者信息

Zhang Xiaonan, Mofers Arjan, Hydbring Per, Olofsson Maria Hägg, Guo Jing, Linder Stig, D'Arcy Padraig

机构信息

Cancer Center Karolinska, Department of Oncology and Pathology, Karolinska Institute, SE-171 76 Stockholm, Sweden.

Department of Medical and Health Sciences, Linköping University, SE-581 83 Linköping, Sweden.

出版信息

Oncotarget. 2017 Oct 6;8(52):90225-90237. doi: 10.18632/oncotarget.21653. eCollection 2017 Oct 27.

DOI:10.18632/oncotarget.21653

PMID:29163823

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5685744/

Abstract

The MYC proto-oncogene serves as a rheostat coupling mitogenic signaling with the activation of genes regulating growth, metabolism and mitochondrial biogenesis. Here we describe a novel link between mitochondria and MYC levels. Perturbation of mitochondrial function using a number of conventional and novel inhibitors resulted in the decreased expression of MYC mRNA. This decrease in MYC mRNA occurred concomitantly with an increase in the levels of tumor-suppressive miRNAs such as members of the family and . Knockdown of family or could partially restore MYC levels following mitochondria damage. We also identified -dependent downregulation of the MYC mRNA chaperone, CRD-BP (coding region determinant-binding protein) as an additional control following mitochondria damage. Our data demonstrates the existence of a homeostasis mechanism whereby mitochondrial function controls MYC expression.

摘要

MYC原癌基因作为一种变阻器，将有丝分裂信号与调节生长、代谢和线粒体生物发生的基因激活相耦合。在此，我们描述了线粒体与MYC水平之间的一种新联系。使用多种传统和新型抑制剂对线粒体功能进行扰动，导致MYC mRNA表达降低。MYC mRNA的这种降低与肿瘤抑制性miRNA水平的增加同时发生，如家族成员和。敲低家族或可在一定程度上恢复线粒体损伤后的MYC水平。我们还发现，线粒体损伤后，作为一种额外的调控机制，MYC mRNA伴侣CRD-BP（编码区决定簇结合蛋白）存在依赖的下调。我们的数据证明存在一种稳态机制，通过该机制线粒体功能控制MYC表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ccf/5685744/8cd5a7cb79a7/oncotarget-08-90225-g001.jpg

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MYC通过一种线粒体检查点机制被下调。

MYC is downregulated by a mitochondrial checkpoint mechanism.

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