Literature DB >> 27197193

Systematic Analysis of AU-Rich Element Expression in Cancer Reveals Common Functional Clusters Regulated by Key RNA-Binding Proteins.

Edward Hitti1, Tala Bakheet1, Norah Al-Souhibani1, Walid Moghrabi1, Suhad Al-Yahya1, Maha Al-Ghamdi1, Maher Al-Saif1, Mohamed M Shoukri2, András Lánczky3, Renaud Grépin4, Balázs Győrffy5, Gilles Pagès6, Khalid S A Khabar7.   

Abstract

Defects in AU-rich elements (ARE)-mediated posttranscriptional control can lead to several abnormal processes that underlie carcinogenesis. Here, we performed a systematic analysis of ARE-mRNA expression across multiple cancer types. First, the ARE database (ARED) was intersected with The Cancer Genome Atlas databases and others. A large set of ARE-mRNAs was over-represented in cancer and, unlike non-ARE-mRNAs, correlated with the reversed balance in the expression of the RNA-binding proteins tristetraprolin (TTP, ZFP36) and HuR (ELAVL1). Serial statistical and functional enrichment clustering identified a cluster of 11 overexpressed ARE-mRNAs (CDC6, KIF11, PRC1, NEK2, NCAPG, CENPA, NUF2, KIF18A, CENPE, PBK, TOP2A) that negatively correlated with TTP/HuR mRNA ratios and was involved in the mitotic cell cycle. This cluster was upregulated in a number of solid cancers. Experimentally, we demonstrated that the ARE-mRNA cluster is upregulated in a number of tumor breast cell lines when compared with noninvasive and normal-like breast cancer cells. RNA-IP demonstrated the association of the ARE-mRNAs with TTP and HuR. Experimental modulation of TTP or HuR expression led to changes in the mitosis ARE-mRNAs. Posttranscriptional reporter assays confirmed the functionality of AREs. Moreover, TTP augmented mitotic cell-cycle arrest as demonstrated by flow cytometry and histone H3 phosphorylation. We found that poor breast cancer patient survival was significantly associated with low TTP/HuR mRNA ratios and correlated with high levels of the mitotic ARE-mRNA signature. These results significantly broaden the role of AREs and their binding proteins in cancer, and demonstrate that TTP induces an antimitotic pathway that is diminished in cancer. Cancer Res; 76(14); 4068-80. ©2016 AACR. ©2016 American Association for Cancer Research.

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Year:  2016        PMID: 27197193     DOI: 10.1158/0008-5472.CAN-15-3110

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  31 in total

Review 1.  The Untranslated Regions of mRNAs in Cancer.

Authors:  Samantha L Schuster; Andrew C Hsieh
Journal:  Trends Cancer       Date:  2019-03-22

2.  [Tristetraprolin inhibits autophagy in cultured lung cancer cells via the nuclear factor-κB pathway].

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Review 3.  Dysregulation of TTP and HuR plays an important role in cancers.

Authors:  Hao Wang; Nannan Ding; Jian Guo; Jiazeng Xia; Yulan Ruan
Journal:  Tumour Biol       Date:  2016-09-19

4.  Human coronaviruses disassemble processing bodies.

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Journal:  PLoS Pathog       Date:  2022-08-23       Impact factor: 7.464

Review 5.  Post-transcriptional regulation of cytokine and growth factor signaling in cancer.

Authors:  Irina Vlasova-St Louis; Paul R Bohjanen
Journal:  Cytokine Growth Factor Rev       Date:  2016-12-02       Impact factor: 7.638

Review 6.  Polyamines in Gut Epithelial Renewal and Barrier Function.

Authors:  Jaladanki N Rao; Lan Xiao; Jian-Ying Wang
Journal:  Physiology (Bethesda)       Date:  2020-09-01

7.  Targeting the HuR Oncogenic Role with a New Class of Cytoplasmic Dimerization Inhibitors.

Authors:  Natalia Filippova; Xiuhua Yang; Subramaniam Ananthan; Jennifer Calano; Vibha Pathak; Larry Bratton; Rakesh H Vekariya; Sixue Zhang; Edward Ofori; Emily N Hayward; David Namkoong; David K Crossman; Michael R Crowley; Peter H King; James Mobley; Louis B Nabors
Journal:  Cancer Res       Date:  2021-02-18       Impact factor: 13.312

Review 8.  The control of inflammation via the phosphorylation and dephosphorylation of tristetraprolin: a tale of two phosphatases.

Authors:  Andrew R Clark; Jonathan L E Dean
Journal:  Biochem Soc Trans       Date:  2016-10-15       Impact factor: 5.407

9.  A novel mechanism for variable phenotypic expressivity in Mendelian diseases uncovered by an AU-rich element (ARE)-creating mutation.

Authors:  Nisha Patel; Arif O Khan; Maher Al-Saif; Walid N Moghrabi; Balsam M AlMaarik; Niema Ibrahim; Firdous Abdulwahab; Mais Hashem; Tarfa Alshidi; Eman Alobeid; Rana A Alomar; Saad Al-Harbi; Mohamed Abouelhoda; Khalid S A Khabar; Fowzan S Alkuraya
Journal:  Genome Biol       Date:  2017-07-28       Impact factor: 13.583

Review 10.  Cell cycle RNA regulons coordinating early lymphocyte development.

Authors:  Alison Galloway; Martin Turner
Journal:  Wiley Interdiscip Rev RNA       Date:  2017-02-23       Impact factor: 9.957

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