Foxo3 circular RNA retards cell cycle progression via forming ternary complexes with p21 and CDK2

Du, William W.; Yang, Weining; Liu, Elizabeth; Yang, Zhen-Guo; Dhaliwal, Preet; Yang, Burton B.

doi:10.1093/nar/gkw027

Cited by 1,305 publications

(1,062 citation statements)

References 34 publications

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“…Another study by the same research group showed that circ-Foxo3 could also bind to the cell cycle proteins cyclin-dependent kinase 2 (CDK2) and cyclin-dependent kinase inhibitor 1 (p21), resulting in the formation of a ternary complex. 49 The formation of this circ-Foxo3-p21-CDK2 ternary complex arrested the function of CDK2 and blocked cell cycle progression, adding support to circ-Foxo3 acting as a protein's scaffold to modulate certain cellular activities. In summary, circ-Foxo3 seems to be able to bind to many different proteins.…”

Section: Protein Interactionmentioning

confidence: 99%

The emerging role and clinical implication of human exonic circular RNA

Lyu

Huang

2016

RNA Biology

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Circular RNA from backspliced exons (or exonic circular RNA, circRNA) is a type of covalently closed noncolinear RNA that was recently rediscovered in eukaryotes. Although circRNAs are often expressed at low levels, emerging evidence indicates that many circRNAs are linked to physiological development and various diseases. Notably, circRNAs have been shown to serve as oncogenic stimuli or tumor suppressors in cancer. circRNAs may regulate gene expression through different mechanisms. In addition, circRNAs have been shown to be useful as biomarkers of diseases due to their stability, specific expression and relation to diseases both in cells and in extracellular fluid. This review summarizes current knowledge of human circRNAs and discusses the emerging role and clinical implication of these multifarious transcripts.

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Section: Protein Interactionmentioning

confidence: 99%

The emerging role and clinical implication of human exonic circular RNA

Lyu

Huang

2016

RNA Biology

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“…17,21 Second, pioneering studies have now showed functionality of specific circRNAs in both normal physiology and disease. 18,[22][23][24][25] Third, circRNAs are cytoplasmic, whereas most (if not all) undesired splicing products accumulate at the site of transcription. 26 Fourth, circRNAs are evolutionarily conserved at both their sequence level and their pattern of expression, in particular in the brain.…”

Section: Circrnas: a New Regulation Layer Of Gene Expressionmentioning

confidence: 99%

“…CircFOXO3 inhibits cell cycle progression by forming a ternary complex with cyclin-dependent kinase 2 (CDK2) and cyclin-dependent kinase inhibitor 1 (p21). 23 CircH-IPK3 directly binds and inhibits miR-124 activity, and silencing it results in arrested cell growth. 22 In addition, we recently reported that the splicing factor muscleblind (mbl) hosts a circRNA which is involved in the auto-regulation of this RNA-binding protein.…”

Section: Circrnas: a New Regulation Layer Of Gene Expressionmentioning

confidence: 99%

“…48 Indeed, circRNAs have already been shown to be good biomarkers for different types of cancers. 23,24,49 Future prospects and concluding remarks Many neuronal genes generate multiple circRNAs. These "hotspots" for circRNA production usually involve splicing with one specific exon, either at the splice donor or splice acceptor.…”

Section: Circrnas In Neurodegenerationmentioning

confidence: 99%

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CircRNAs in the brain

2016

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Circular RNAs (circRNAs) are highly abundant and evolutionarily conserved non-coding RNAs produced by circularization of specific exons. Since their re-discovery as potential regulators of gene expression, thousands of circRNAs were detected in different tissues and cell types across most organisms. Accumulating data suggest key roles for them in the central nervous system. Neuronal-expressed RNAs are diverted to yield highly enriched CircRNAs in human, mouse, pig and flies, with many of them enriched in neuronal tissues. CircRNA levels are dynamically modulated in neurons, both during differentiation and following bursts of electrical activity, and accumulate with age, and many of them are enriched in synapses. Together, available data suggest that circRNAs have important roles in synaptic plasticity and neuronal function. This review covers current advances in the field and lays out hypotheses regarding functions of circRNAs in the brain as well as their putative involvement in initiation and progression of neurodegenerative processes.

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“…9 Recently, we showed that the circular RNA circ-Foxo3 could function by binding to proteins in related signal pathways. 10,11 In the present study, we used computational approach to elucidate the interaction of circ-Foxo3 with MDM2 and p53. The RING-finger domain in the carboxyl terminal of the MDM2 is known to bind RNA specifically in a sequence-specific manner, 12 whereas p53 interacts with RNA via its C-terminal regulatory domain.…”

mentioning

confidence: 99%

Induction of tumor apoptosis through a circular RNA enhancing Foxo3 activity

et al. 2016

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Circular RNAs are a class of non-coding RNAs that are receiving extensive attention. Despite reports showing circular RNAs acting as microRNA sponges, the biological functions of circular RNAs remain largely unknown. We show that in patient tumor samples and in a panel of cancer cells, circ-Foxo3 was minimally expressed. Interestingly, during cancer cell apoptosis, the expression of circ-Foxo3 was found to be significantly increased. We found that silencing endogenous circ-Foxo3 enhanced cell viability, whereas ectopic expression of circ-Foxo3 triggered stress-induced apoptosis and inhibited the growth of tumor xenografts. Also, expression of circ-Foxo3 increased Foxo3 protein levels but repressed p53 levels. By binding to both, circ-Foxo3 promoted MDM2-induced p53 ubiquitination and subsequent degradation, resulting in an overall decrease of p53. With low binding affinity to Foxo3 protein, circ-Foxo3 prevented MDM2 from inducing Foxo3 ubiquitination and degradation, resulting in increased levels of Circular RNAs are a large class of non-coding RNAs that are circularized by joining free 3'-to 5'-ends, forming a circular structure. 1-4Although circular RNAs were initially characterized over 30 years ago, their functions in mammalian cells are still largely unknown. Most circular RNAs are predominantly found in the cytoplasm and contain exons, known as circRNAs.5 A relatively smaller group of circular RNAs that contain both exons and introns are known as EIciRNAs, and are predominantly found in the nucleus. 6 Recent studies have indicated that some circular RNAs contain miRNA binding sites and may function as sponges to arrest miRNA functions. 7,8 It has further been reported that EIciRNAs increase the transcription of their parental genes.9 Recently, we showed that the circular RNA circ-Foxo3 could function by binding to proteins in related signal pathways. 10,11 In the present study, we used computational approach to elucidate the interaction of circ-Foxo3 with MDM2 and p53. The RING-finger domain in the carboxyl terminal of the MDM2 is known to bind RNA specifically in a sequence-specific manner, 12 whereas p53 interacts with RNA via its C-terminal regulatory domain. 13 Our study comprised of computer-aided RNA structure modeling of circ-Foxo3 employing minimum free energy algorithm and machine translation system followed by its molecular interaction with MDM2 (RING-finger domain) and p53 (C-terminal regulatory domain) that includes docking, scoring, clustering, and refinement of the most promising models. The interaction was further confirmed by an approach of molecular experiments to explicate the biological functions of circ-Foxo3. ResultsDecreased expression of circ-Foxo3 in tumors and cancer cells. Downregulation of Foxo3 is often observed in cancer development.14,15 Both circ-Foxo3 and Foxo3 mRNA are encoded by the FOXO3 gene. 16 We found that the levels of circ-Foxo3 in tumor specimen were significantly lower than in the adjacent benign tissue (Figure 1a). We examined circ-Foxo3 expression and detected s...

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Foxo3 circular RNA retards cell cycle progression via forming ternary complexes with p21 and CDK2

Cited by 1,305 publications

References 34 publications

The emerging role and clinical implication of human exonic circular RNA

The emerging role and clinical implication of human exonic circular RNA

CircRNAs in the brain

Induction of tumor apoptosis through a circular RNA enhancing Foxo3 activity

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