p53 cooperates with DNA methylation and a suicidal interferon response to maintain epigenetic silencing of repeats and noncoding RNAs

Leonova, Katerina I.; Brodsky, Leonid; Lipchick, Brittany C.; Pal, Mahadeb; Novototskaya, Liliya R.; Chenchik, Alex; Sen, Ganes C.; Komarova, Elena A.; Gudkov, Andrei V.

doi:10.1073/pnas.1216922110

Cited by 231 publications

(274 citation statements)

References 61 publications

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“…Endogenous dsRNA species are some of the primary activators of the interferon response (Leonova et al , 2013; Mannion et al , 2014; White et al , 2014; Chiappinelli et al , 2015; Liddicoat, 2015; Roulois et al , 2015; Goel et al , 2017). Recent studies showed transcriptional activations of the ERVs triggered by several anti‐tumor drugs, which in turn resulted in ERV‐originated dsRNA accumulation, potent interferon responses, and significant tumor inhibition (Chiappinelli et al , 2015; Roulois et al , 2015; Goel et al , 2017).…”

Section: Discussionmentioning

confidence: 99%

Function of HNRNPC in breast cancer cells by controlling the dsRNA‐induced interferon response

et al. 2018

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Elevated expression of RNA binding protein HNRNPC has been reported in cancer cells, while the essentialness and functions of HNRNPC in tumors were not clear. We showed that repression of HNRNPC in the breast cancer cells MCF7 and T47D inhibited cell proliferation and tumor growth. Our computational inference of the key pathways and extensive experimental investigations revealed that the cascade of interferon responses mediated by RIG‐I was responsible for such tumor‐inhibitory effect. Interestingly, repression of HNRNPC resulted in accumulation of endogenous double‐stranded RNA (dsRNA), the binding ligand of RIG‐I. These up‐regulated dsRNA species were highly enriched by Alu sequences and mostly originated from pre‐mRNA introns that harbor the known HNRNPC binding sites. Such source of dsRNA is different than the recently well‐characterized endogenous retroviruses that encode dsRNA. In summary, essentialness of HNRNPC in the breast cancer cells was attributed to its function in controlling the endogenous dsRNA and the down‐stream interferon response. This is a novel extension from the previous understandings about HNRNPC in binding with introns and regulating RNA splicing.

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Section: Discussionmentioning

confidence: 99%

Function of HNRNPC in breast cancer cells by controlling the dsRNA‐induced interferon response

et al. 2018

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“…But such LTRs are highly involved in the emergence of new regulatory networks, such as the origin of the placenta (Bièche et al 2003;Chuong et al 2013;Emera and Wagner 2012;Harris 1998;Nakagawa et al 2013) (re-regulating 1500 genes) Lynch et al 2011Lynch et al , 2012 or in the African primates where alteration of 320,000 LTR p53 binding sites occurred onto the p53 cell cycle control network (Wang et al 2007). These primate p53 network changes also relate to (co-operate with) changes in brain specific microRNAs (Le et al 2009), alterations to DNA methylation involved in controlling SINE-derived RNA transcription (Leonova et al 2013), as well as Alu-derived transcription (Zemojtel et al 2009 In proposing the qs-c concept, it was argued that agent diversity (not errors) was essential for the capacity of a collective of RNA agents to function co-operatively (Villarreal and Witzany 2013b). Thus, an identity group of sub-functional RNA agents would be the predecessors of RNA-based life (not a functioning individual).…”

Section: Retroviral Network Regulate Evolution and Developmentmentioning

confidence: 97%

When Competing Viruses Unify: Evolution, Conservation, and Plasticity of Genetic Identities

Villarreal

Witzany

2015

J Mol Evol

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In the early 1970s, Manfred Eigen and colleagues developed the quasispecies model (qs) for the population-based origin of RNAs representing the early genetic code. The Eigen idea is basically that a halo of mutants is generated by error-prone replication around the master fittest type which will behave similarly as a biological population. But almost from the start, very interesting and unexpected observations were made regarding competition versus co-operation which suggested more complex interactions. It thus became increasingly clear that although viruses functioned similar to biological species, their behavior was much more complex than the original theory could explain, especially adaptation without changing the consensus involving minority populations. With respect to the origin of natural codes, meaning, and code-use in interactions (communication), it also became clear that individual fittest type-based mechanisms were likewise unable to explain the origin of natural codes such as the genetic code with their context-and consortia-dependence (pragmatic nature). This, instead, required the participation of groups of agents competent in the code and able to edit code because natural codes do not code themselves. Three lines of inquiry, experimental virology, quasispecies theory, and the study of natural codes converged to indicate that consortia of cooperative RNA agents such as viruses must be involved in the fitness of RNA and its involvement in communication, i.e., code-competent interactions. We called this co-operative form quasispecies consortia (qs-c). They are the essential agents that constitute the possibility of evolution of biological group identity. Finally, the basic interactional motifs for the emergence of group identity, communication, and cooperation-together with its opposing functions-are explained by the ''Gangen'' hypothesis.

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“…Therefore, we included a DNA-demethylating agent, 5-aza-2 0 -deoxycytidine (5-AZA), which was recently shown to be an effective chemotherapeutic agent in satellite DNA overexpressing cells. 28 Interestingly, we discovered that only WT PTEN cells had reduced sensitivity to 5-AZA (Fig. 4F).…”

Section: C-terminal Truncated Pten Mutant Does Not Function As a Tumomentioning

confidence: 99%

Nuclear PTEN tumor-suppressor functions through maintaining heterochromatin structure

et al. 2015

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The tumor suppressor, PTEN, is one of the most commonly mutated genes in cancer. Recently, PTEN has been shown to localize in the nucleus and is required to maintain genomic stability. Here, we show that nuclear PTEN, independent of its phosphatase activity, is essential for maintaining heterochromatin structure. Depletion of PTEN leads to loss of heterochromatic foci, decreased chromatin compaction, overexpression of heterochromatic genes, and reduced protein stability of heterochromatin protein 1 a. We found that the C-terminus of PTEN is required to maintain heterochromatin structure. Additionally, cancer-associated PTEN mutants lost their tumor-suppressor function when their heterochromatin structure was compromised. We propose that this novel role of PTEN accounts for its function in guarding genomic stability and suppressing tumor development.

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p53 cooperates with DNA methylation and a suicidal interferon response to maintain epigenetic silencing of repeats and noncoding RNAs

Cited by 231 publications

References 61 publications

Function of HNRNPC in breast cancer cells by controlling the dsRNA‐induced interferon response

Function of HNRNPC in breast cancer cells by controlling the dsRNA‐induced interferon response

When Competing Viruses Unify: Evolution, Conservation, and Plasticity of Genetic Identities

Nuclear PTEN tumor-suppressor functions through maintaining heterochromatin structure

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