Mei-Shi Yeo scite author profile

Mei-Shi Yeo

4Publications

47Citation Statements Received

55Citation Statements Given

How they've been cited

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Affiliations

National University Cancer Institute, Singapore, National University of Singapore

Publications

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RNA-Binding Protein ZFP36L1 Suppresses Hypoxia and Cell-Cycle Signaling

Loh

Sun

Ding

et al. 2020

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◥ZFP36L1 is a tandem zinc-finger RNA-binding protein that recognizes conserved adenylate-uridylate-rich elements (ARE) located in 3 0 untranslated regions (UTR) to mediate mRNA decay. We hypothesized that ZFP36L1 is a negative regulator of a posttranscriptional hub involved in mRNA half-life regulation of cancer-related transcripts. Analysis of in silico data revealed that ZFP36L1 was significantly mutated, epigenetically silenced, and downregulated in a variety of cancers. Forced expression of ZFP36L1 in cancer cells markedly reduced cell proliferation in vitro and in vivo, whereas silencing of ZFP36L1 enhanced tumor cell growth. To identify direct downstream targets of ZFP36L1, systematic screening using RNA pull-down of wild-type and mutant ZFP36L1 as well as whole transcriptome sequencing of bladder cancer cells {plus minus} tet-on ZFP36L1 was performed. A network of 1,410 genes was identified as potential direct targets of ZFP36L1. These targets included a number of key oncogenic transcripts such as HIF1A, CCND1, and E2F1. ZFP36L1 specifically bound to the 3 0 UTRs of these targets for mRNA degradation, thus suppressing their expression. Dual luciferase reporter assays and RNA electrophoretic mobility shift assays showed that wild-type, but not zinc-finger mutant ZFP36L1, bound to HIF1A 3 0 UTR and mediated HIF1A mRNA degradation, leading to reduced expression of HIF1A and its downstream targets. Collectively, our findings reveal an indispensable role of ZFP36L1 as a posttranscriptional safeguard against aberrant hypoxic signaling and abnormal cellcycle progression.Significance: RNA-binding protein ZFP36L1 functions as a tumor suppressor by regulating the mRNA stability of a number of mRNAs involved in hypoxia and cell-cycle signaling.

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Molecular cloning of genes encoding toxins in the venom of Naja naja sputatrix

Jeyaseelan

Armugam

Earnest

et al. 1995

Toxicon

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Molecular cloning of a cardiotoxin structural gene from Malayan spitting cobra (Naja naja sputatrix)

Yeo

Jeyaseelan

Chung

et al. 1993

Toxicon

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Supplementary Data from RNA-Binding Protein <i>ZFP36L1</i> Suppresses Hypoxia and Cell-Cycle Signaling

Loh¹,

Sun²,

Ding³

et al. 2023

Preprint

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Mei-Shi Yeo

RNA-Binding Protein ZFP36L1 Suppresses Hypoxia and Cell-Cycle Signaling

Molecular cloning of genes encoding toxins in the venom of Naja naja sputatrix

Molecular cloning of a cardiotoxin structural gene from Malayan spitting cobra (Naja naja sputatrix)

Supplementary Data from RNA-Binding Protein <i>ZFP36L1</i> Suppresses Hypoxia and Cell-Cycle Signaling

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