Association of Tumor Suppressor Protein Pdcd4 With Ribosomes Is Mediated by Protein-Protein and Protein-RNA Interactions

Wedeken, Lena; Ohnheiser, Johanna; Hirschi, Benjamin; Wethkamp, Nils; Klempnauer, Karl‐Heinz

doi:10.1177/1947601910364227

Cited by 29 publications

(41 citation statements)

References 31 publications

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“…Initially, in vitro binding experiments using nonspecific RNA suggested that the N-terminal part of Pdcd4 is involved in RNA binding (Bo¨hm et al, 2003). More recently, we have shown that the Pdcd4 RNAbinding domain is required for the association of Pdcd4 with ribosomal complexes in vivo, providing the first evidence for a role of RNA binding in targeting Pdcd4 to the translation machinery (Wedeken et al, 2010). The identification of a 'Pdcd4-response region' in c-myb mRNA has allowed, for the first time, to study RNA binding of Pdcd4 in the context of a physiological RNA target site.…”

Section: Discussionmentioning

confidence: 99%

“…Previous work has shown that the amino terminal domain of Pdcd4 binds to RNA and that its RNA-binding activity is mediated by two clusters of basic amino acids. Mutation of both clusters (which are referred to as RBM1 and 2) results in a complete loss of the RNAbinding activity (Bo¨hm et al, 2003;Wedeken et al, 2010). As shown in Figure 5, mutant Pdcd4 carrying mutations of the basic amino acid clusters inhibited c-Myb translation less strongly than wild-type Pdcd4, Nco, E, X, N, S and B refer to restriction sites for NcoI, EcoRI, XmaI, NaeI, SalI and BglII, respectively.…”

Section: C-myb Mrna Is a Translational Target Of Pdcd4mentioning

confidence: 99%

“…pCMVluc was obtained by inserting the CMV promoter into pGL3-basic (Promega, Mannheim, Germany). Expression vectors for hemagglutinin-tagged chicken Pdcd4 and wild-type human Pdcd4 have been described (Schlichter et al, 2001a;Waters et al, 2007) pCDNA4-hPdcd4-mutRBM1 þ 2 encodes a mutant Pdcd4 protein with amino-acid substitutions of several basic amino acids in the N-terminal part of Pdcd4 (Wedeken et al, 2010). Bacterial expression vectors for GST-Pdcd4 and GST-Pdcd4 mutRBM1 þ 2 have been described (Wedeken et al, 2010).…”

Section: Expression Vectorsmentioning

confidence: 99%

“…Density gradient centrifugation was performed as described (Wedeken et al, 2010). Ribosomal RNAs were visualized by agarose gel electrophoresis.…”

Section: Sucrose Density Gradientsmentioning

confidence: 99%

“…The RNA was extracted with TriZOL, ethanolprecipitated and dissolved in diethylpyrocarbonate-treated water. GST-Pdcd4-wt and GST-Pdcd4-mutRBM1 þ 2 have been described (Wedeken et al, 2010). The proteins were purified by binding to GST sepharose in buffer containing 1 Â phosphate-buffered saline, 1% NP-40, 2 mM DTT, 1 mM phenylmethanesulfonylfluoride and a protease inhibitor cocktail containing pepstatin A, leupeptin and aprotinin.…”

Section: Electrophoretic Mobility Shift Assaymentioning

confidence: 99%

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Pdcd4 directly binds the coding region of c-myb mRNA and suppresses its translation

et al. 2011

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Pdcd4 is a novel tumor suppressor protein that functions in the nucleus and the cytoplasm, and appears to be involved in the regulation of transcription and translation. In the cytoplasm, Pdcd4 has been implicated in the suppression of translation of mRNAs containing structured 5 0 -untranslated regions; however, the mechanisms that recruit Pdcd4 to specific target mRNAs and the identities of these mRNAs are mostly unknown. In this study, we have identified c-myb mRNA as the first natural translational target mRNA of Pdcd4. We have found that translational suppression of c-myb mRNA by Pdcd4 is dependent on sequences located within the c-myb-coding region. Furthermore, we have found that the N-terminal domain of Pdcd4 has an important role in targeting Pdcd4 to c-myb RNA by mediating preferential RNA binding to the Pdcd4-responsive region of c-myb mRNA. Overall, our work demonstrates for the first time that Pdcd4 is directly involved in translational suppression of a natural mRNA and provides the first evidence for a key role of the RNA-binding domain in targeting Pdcd4 to a specific mRNA.

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Section: Discussionmentioning

confidence: 99%

Section: C-myb Mrna Is a Translational Target Of Pdcd4mentioning

confidence: 99%

Section: Expression Vectorsmentioning

confidence: 99%

“…Density gradient centrifugation was performed as described (Wedeken et al, 2010). Ribosomal RNAs were visualized by agarose gel electrophoresis.…”

Section: Sucrose Density Gradientsmentioning

confidence: 99%

Section: Electrophoretic Mobility Shift Assaymentioning

confidence: 99%

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Pdcd4 directly binds the coding region of c-myb mRNA and suppresses its translation

et al. 2011

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Pdcd4

Yang

Wang

Bajer

et al. 2014

Translation and Its Regulation in Cancer Biology and Medicine

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PDCD4 Simultaneously Promotes Microglia Activation via PDCD4–MAPK–NF-κB Positive Loop and Facilitates Neuron Apoptosis During Neuroinflammation

et al. 2021

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Neuroinflammation and neuron injury are common features of the central nervous system (CNS) diseases. It is of great significance to identify their shared key regulatory molecules and thus explore the potential therapeutic targets. Programmed cell death factor 4 (PDCD4), an apoptosis-related molecule, extensively participates in tumorigenesis and inflammatory diseases, but its expression and biological function during CNS neuroinflammation remain unclear. In the present study, utilizing the lipopolysaccharide (LPS)-induced neuroinflammation model in mice, we reported an elevated expression of PDCD4 both in injured neurons and activated microglia of the inflamed brain. A similar change in PDCD4 expression was observed in vitro in the microglial activation model. Silencing PDCD4 by shRNA significantly inhibited the phosphorylation of MAPKs (p38, ERK, and JNK), prevented the phosphorylation and nuclear translocation of NF-κB p65, and thus attenuated the LPS-induced microglial inflammatory activation. Interestingly, LPS also required the MAPK/NF-κB signaling activation to boost PDCD4 expression in microglia, indicating the presence of a positive loop. Moreover, a persistent elevation of PDCD4 expression was detected in the H 2 O 2 -induced neuronal oxidative damage model. Knocking down PDCD4 significantly inhibited the expression of pro-apoptotic proteins BAX and Cleaved-PARP, suggesting the proapoptotic activity of PDCD4 in neurons. Taken together, our data indicated that PDCD4 may serve as a hub regulatory molecule that simultaneously promotes the microglial inflammatory activation and the oxidative stress-induced neuronal apoptosis within CNS. The microglial PDCD4-MAPK-NF-κB positive feedback loop may act as pivotal signaling for neuroinflammation which subsequently exaggerates neuronal injury, and thus may become a potential therapeutic target for neuroinflammatory diseases.

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Association of Tumor Suppressor Protein Pdcd4 With Ribosomes Is Mediated by Protein-Protein and Protein-RNA Interactions

Cited by 29 publications

References 31 publications

Pdcd4 directly binds the coding region of c-myb mRNA and suppresses its translation

Pdcd4 directly binds the coding region of c-myb mRNA and suppresses its translation

Pdcd4

PDCD4 Simultaneously Promotes Microglia Activation via PDCD4–MAPK–NF-κB Positive Loop and Facilitates Neuron Apoptosis During Neuroinflammation

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