Structural Insights into Parasite eIF4E Binding Specificity for m7G and m2,2,7G mRNA Caps

Liu, Weizhi; Zhao, Rui; McFarland, Craig; Kieft, Jeffrey S.; Niedzwiecka, Anna; Jankowska-Anyszka, Marzena; Stępiński, Janusz; Darżynkiewicz, Edward; Jones, David N. M.; Davis, Richard E.

doi:10.1074/jbc.m109.049858

Cited by 33 publications

(43 citation statements)

References 64 publications

(85 reference statements)

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“…The large number of residues that undergo CSPs is in agreement with the enclosure of the cap structure into the core of the eIF4E protein (Matsuo et al 1997;Kinkelin et al 2012). In agreement with the limited (Tomoo et al 2005;Liu et al 2009;Peter et al 2015) show that the position of the first nucleotide of the RNA body (pink) is not well defined. This indicates that the interaction between eIF4e and the mRNA is mediated almost exclusively through the m 7 GTP part of the cap-0 structure.…”

Section: Nmr Studies Of the Capped Rnamentioning

confidence: 56%

A general method for rapid and cost-efficient large-scale production of 5′ capped RNA

Fuchs

Neu

Sprangers

2016

RNA

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The eukaryotic mRNA 5 ′ cap structure is indispensible for pre-mRNA processing, mRNA export, translation initiation, and mRNA stability. Despite this importance, structural and biophysical studies that involve capped RNA are challenging and rare due to the lack of a general method to prepare mRNA in sufficient quantities. Here, we show that the vaccinia capping enzyme can be used to produce capped RNA in the amounts that are required for large-scale structural studies. We have therefore designed an efficient expression and purification protocol for the vaccinia capping enzyme. Using this approach, the reaction scale can be increased in a cost-efficient manner, where the yields of the capped RNA solely depend on the amount of available uncapped RNA target. Using a large number of RNA substrates, we show that the efficiency of the capping reaction is largely independent of the sequence, length, and secondary structure of the RNA, which makes our approach generally applicable. We demonstrate that the capped RNA can be directly used for quantitative biophysical studies, including fluorescence anisotropy and highresolution NMR spectroscopy. In combination with 13 C-methyl-labeled S-adenosyl methionine, the methyl groups in the RNA can be labeled for methyl TROSY NMR spectroscopy. Finally, we show that our approach can produce both cap-0 and cap-1 RNA in high amounts. In summary, we here introduce a general and straightforward method that opens new means for structural and functional studies of proteins and enzymes in complex with capped RNA.

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Section: Nmr Studies Of the Capped Rnamentioning

confidence: 56%

A general method for rapid and cost-efficient large-scale production of 5′ capped RNA

Fuchs

Neu

Sprangers

2016

RNA

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“…The development of respective, parasite-specific drugs could prove difficult if they are directed against the splicing process itself, since trans-splicing is carried out by the canonical spliceosome, the components of which are highly conserved between cestodes and mammals (Tsai et al, 2013). However, as already suggested previously (Liu et al, 2009), the eukaryotic translation initiation factor 4E (eIF4E), which initiates translation by binding to the mRNA cap structure, could be a promising target. In mammals, eIF4E only recognises 7mG cap structures, whereas in the trans-splicing schistosomes an eIF4E is present that recognises both 7mG and TMG caps (Liu et al, 2009).…”

Section: Echinococcus Genomicsmentioning

confidence: 95%

“…However, as already suggested previously (Liu et al, 2009), the eukaryotic translation initiation factor 4E (eIF4E), which initiates translation by binding to the mRNA cap structure, could be a promising target. In mammals, eIF4E only recognises 7mG cap structures, whereas in the trans-splicing schistosomes an eIF4E is present that recognises both 7mG and TMG caps (Liu et al, 2009). The E. multilocularis genome contains one single copy gene for eIF4E and it is reasonable to assume that this factor also recognises both types of caps.…”

Section: Echinococcus Genomicsmentioning

confidence: 95%

“…One striking difference in gene expression mechanisms between flatworm parasites and their hosts, which has already been suggested to be exploitable for drug development (Liu et al, 2009), is spliced-leader trans-splicing (SL-TS). Originally described in trypanosomes and nematodes (Hastings, 2005), SL-TS has later also been shown to occur in all parasitic and free-living lineages of flatworms (Brehm et al, 2002(Brehm et al, , 2000aDavis et al, 1995;Zayas et al, 2005).…”

Section: Echinococcus Genomicsmentioning

confidence: 99%

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Recent advances in Echinococcus genomics and stem cell research

Koziol

Brehm

2015

Veterinary Parasitology

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Alveolar and cystic echinococcosis, caused by the metacestode larval stages of the tapeworms Echinococcus multilocularis and Echinococcus granulosus, respectively, are life-threatening diseases and very difficult to treat. The introduction of benzimidazole-based chemotherapy, which targets parasite β-tubulin, has significantly improved the life-span and prognosis of echinococcosis patients. However, benzimidazoles show only parasitostatic activity, are associated with serious adverse side effects and have to be administered for very long time periods, underlining the need for new drugs. Very recently, the nuclear genomes of E. multilocularis and E. granulosus have been characterised, revealing a plethora of data for gaining a deeper understanding of host-parasite interaction, parasite development and parasite evolution. Combined with extensive transcriptome analyses of Echinococcus life cycle stages these investigations also yielded novel clues for targeted drug design. Recent years also witnessed significant advancements in the molecular and cellular characterisation of the Echinococcus 'germinative cell' population, which forms a unique stem cell system that differs from stem cells of other organisms in the expression of several genes associated with the maintenance of pluripotency. As the only parasite cell type capable of undergoing mitosis, the germinative cells are central to all developmental transitions of Echinococcus within the host and to parasite expansion via asexual proliferation. In the present article, we will briefly introduce and discuss recent advances in Echinococcus genomics and stem cell research in the context of drug design and development. Interestingly, it turns out that benzimidazoles seem to have very limited effects on Echinococcus germinative cells, which could explain the high recurrence rates observed after chemotherapeutic treatment of echinococcosis patients. This clearly indicates that future efforts into the development of parasitocidal drugs should also target the parasite's stem cell system.

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“…[37][38][39]. Total lysates, washed beads after m 7 GTP co-capture, and the supernatants were Western-blotted for eIF4E, 4E-BP, or eIF4G.…”

Section: Methodsmentioning

confidence: 99%

The Soy Isoflavone Equol May Increase Cancer Malignancy via Up-regulation of Eukaryotic Protein Synthesis Initiation Factor eIF4G

Parra

Otero-Franqui

Martínez-Montemayor

et al. 2012

Journal of Biological Chemistry

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Background: The molecular mechanisms of soy isoflavones in metastatic cancer remain to be elucidated. Results: Equol, a daidzein metabolite, regulates eIF4G-mediated cap-independent protein synthesis initiation of proteins relevant for cancer malignancy. Conclusion: Equol is a potent regulator of the cancer promoting effects of dietary daidzein. Significance: Consumption of soy may not be advisable for patients with aggressive breast cancer.

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Structural Insights into Parasite eIF4E Binding Specificity for m7G and m2,2,7G mRNA Caps

Cited by 33 publications

References 64 publications

A general method for rapid and cost-efficient large-scale production of 5′ capped RNA

A general method for rapid and cost-efficient large-scale production of 5′ capped RNA

Recent advances in Echinococcus genomics and stem cell research

The Soy Isoflavone Equol May Increase Cancer Malignancy via Up-regulation of Eukaryotic Protein Synthesis Initiation Factor eIF4G

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