p53 and MicroRNA-34 Are Suppressors of Canonical Wnt Signaling

Kim, Nam Hee; Kim, Hyun Sil; Kim, Nam Gyun; Lee, Inhan; Choi, Hyung Seok; Li, Xiao Yan; Kang, Shi Eun; Young, So; Ryu, Joo Kyung; Na, Jung Min; Park, Changbum; Kim, Kunhong; Lee, Sanghyuk; Gumbiner, Barry M.; Yook, Jong In; Weiss, Stephen J.

doi:10.1126/scisignal.2001744

Cited by 273 publications

(278 citation statements)

References 70 publications

(178 reference statements)

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“…Interestingly, miR‐1205 and let‐7i are positively regulated by p53,29, 30 and miR‐885‐5p and miR‐449b activate the p53 pathway 31, 32. Therefore, our results further strengthen the idea that the regulation of beta‐catenin by miRNAs is linked to p53 signaling 17. We noticed that the exon 3 deletion in HepG2 cells made mutated beta‐catenin more resistant to miRNAs, confirming previous data with miR‐483‐3p in colon cancer cells 18.…”

Section: Discussionsupporting

confidence: 79%

“…2D). Very surprisingly, several previously reported miRNAs with a regulatory effect on beta‐catenin, such as miR‐34a and miR‐200a,16, 17 had no such regulatory effect in HBL cells (Fig. 2).…”

Section: Discussionmentioning

confidence: 78%

“…2A‐D; Supporting Fig. S2, dark gray bars) 16, 17. Nine out of 26 miRNA candidates significantly decreased beta‐catenin protein expression in Huh6 cells, which carry the beta‐catenin missense G34V mutation (Fig.…”

Section: Resultsmentioning

confidence: 94%

“…This characteristic of miRNAs is an advantage for cancer therapy since tumors display specific signaling pathway alterations that can be controlled by single miRNAs 11, 12. Many miRNAs have been reported to target beta‐catenin: mature miRNA (miR)‐200a in human meningioma,16 members of the miR‐34 family in lung and breast carcinomas,17 miR‐483‐3p in breast and colon cancers,18 and miR‐214 in HCC 19. However, it is unknown if one of these miRNAs targets beta‐catenin in HBL.…”

Section: Introductionmentioning

confidence: 99%

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MicroRNA therapy inhibits hepatoblastoma growth in vivo by targeting β‐catenin and Wnt signaling

Indersie

Lesjean

Hooks

et al. 2017

Hepatology Communications

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Hepatoblastoma (HBL) is the most common pediatric liver cancer. In this malignant neoplasm, beta‐catenin protein accumulates and increases Wnt signaling due to recurrent activating mutations in the catenin‐beta 1 (CTNNB1) gene. Therefore, beta‐catenin is a key therapeutic target in HBL. However, controlling beta‐catenin production with therapeutic molecules has been challenging. New biological studies could provide alternative therapeutic solutions for the treatment of HBL, especially for advanced tumors and metastatic disease. In this study, we identified microRNAs (miRNAs) that target beta‐catenin and block HBL cell proliferation in vitro and tumor growth in vivo. Using our dual‐fluorescence‐FunREG system, we screened a library of 1,712 miRNA mimics and selected candidates inhibiting CTNNB1 expression through interaction with its untranslated regions. After validating the regulatory effect of nine miRNAs on beta‐catenin in HBL cells, we measured their expression in patient samples. Let‐7i‐3p, miR‐449b‐3p, miR‐624‐5p, and miR‐885‐5p were decreased in tumors compared to normal livers. Moreover, they inhibited HBL cell growth and Wnt signaling activity in vitro partly through beta‐catenin down‐regulation. Additionally, miR‐624‐5p induced cell senescence in vitro, blocked experimental HBL growth in vivo, and directly targeted the beta‐catenin 3′‐untranslated region. Conclusion: Our results shed light on how beta‐catenin‐regulating miRNAs control HBL progression through Wnt signaling inactivation. In particular, miR‐624‐5p may constitute a promising candidate for miRNA replacement therapy for HBL patients. (Hepatology Communications 2017;1:168‐183)

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Section: Discussionsupporting

confidence: 79%

Section: Discussionmentioning

confidence: 78%

Section: Resultsmentioning

confidence: 94%

Section: Introductionmentioning

confidence: 99%

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MicroRNA therapy inhibits hepatoblastoma growth in vivo by targeting β‐catenin and Wnt signaling

Indersie

Lesjean

Hooks

et al. 2017

Hepatology Communications

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“…We reason that circulating miRNAs may be downregulating Wnt signaling in target tissues prone to uncontrolled cell proliferation and development of cancer. Indeed, several genes in the Wnt/β‐catenin signaling network have been found negatively correlated with age and tightly regulated by miRNAs (e.g., miR‐34 family; Kim et al ., 2011). …”

Section: Discussionmentioning

confidence: 99%

Circulating microRNA signature of genotype‐by‐age interactions in the long‐lived Ames dwarf mouse

et al. 2015

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SummaryRecent evidence demonstrates that serum levels of specific miRNAs significantly change with age. The ability of circulating sncRNAs to act as signaling molecules and regulate a broad spectrum of cellular functions implicates them as key players in the aging process. To discover circulating sncRNAs that impact aging in the long‐lived Ames dwarf mice, we conducted deep sequencing of small RNAs extracted from serum of young and old mice. Our analysis showed genotype‐specific changes in the circulating levels of 21 miRNAs during aging [genotype‐by‐age interaction (GbA)]. Genotype‐by‐age miRNAs showed four distinct expression patterns and significant overtargeting of transcripts involved in age‐related processes. Functional enrichment analysis of putative and validated miRNA targets highlighted cellular processes such as tumor suppression, anti‐inflammatory response, and modulation of Wnt, insulin, mTOR, and MAPK signaling pathways, among others. The comparative analysis of circulating GbA miRNAs in Ames mice with circulating miRNAs modulated by calorie restriction (CR) in another long‐lived mouse suggests CR‐like and CR‐independent mechanisms contributing to longevity in the Ames mouse. In conclusion, we showed for the first time a signature of circulating miRNAs modulated by age in the long‐lived Ames mouse.

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Chemical Carcinogenesis

Hofseth,

Weston,

Harris

2017

Holland‐Frei Cancer Medicine

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Overview Human exposure to chemical carcinogens can result in cancer. What dictates this outcome is relatively predictable but highly variable. Factors governing the outcome include type of exposure, amount of exposure, time of exposure, and genetic makeup of the host (i.e., humans). The latter is comprised of variations in single nucleotides within genes (e.g., single nucleotide polymorphisms in deoxyribonucleic acid–repair genes), as well as the metabolomic, proteomic, microbiomic, transcriptomic, and epigenomic background of the individual. It is becoming increasingly clear that these endpoints can be modified by chemical carcinogens and that inflammatory load influences outcome. To this end, the past decade has seen an explosion of extremely sensitive and highly accurate technology. Linking this technology to the rapid development of bioinformatics has enabled us to begin merging the totality of lifetime exposure (exposome) with the totality of metabolomic, proteomic, microbiomic, transcriptomic, epigenomic, and other “omic” profiles. We feel optimistic that the next decade will bring the development of tools to identify an individual's weighted risk signature as a biomarker for cancer risk and develop a personalized and precise approach to cancer chemoprevention and treatment.

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p53 and MicroRNA-34 Are Suppressors of Canonical Wnt Signaling

Cited by 273 publications

References 70 publications

MicroRNA therapy inhibits hepatoblastoma growth in vivo by targeting β‐catenin and Wnt signaling

MicroRNA therapy inhibits hepatoblastoma growth in vivo by targeting β‐catenin and Wnt signaling

Circulating microRNA signature of genotype‐by‐age interactions in the long‐lived Ames dwarf mouse

Chemical Carcinogenesis

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