Your search keyword '"protein RNA binding"' showing total 8 results

1. MYC-driven regulation of long non-coding RNA profiles in breast cancer cells

Author

Ayse Gaye Tomatir, Hakan Akca, Pervin Elvan Tokgun, Serap Kurt, and Onur Tokgun

Subjects

0301 basic medicine, miRNA gene, Carcinogenesis, complementary DNA, MCF-7 cell line, 0302 clinical medicine, lncRNA gene, oncogene, genetics, gene knockdown, Regulation of gene expression, MEG3, Gene knockdown, quantitative analysis, breast tumor, HOTAIR, General Medicine, gene expression regulation, Cell cycle, protein function, RNA analysis, Long non-coding RNA, unclassified drug, Breast Neoplasms/*genetics/pathology, Carcinogenesis/genetics, Cell Line, Tumor, Cell Proliferation/genetics, Female, Gene Expression Regulation, Neoplastic, Humans, MCF-7 Cells, Oncogenes, Proto-Oncogene Proteins c-myc/biosynthesis/*genetics, RNA, Long Noncoding/*genetics, female, priority journal, real time polymerase chain reaction, 030220 oncology & carcinogenesis, protein GAS5, RNA, Long Noncoding, lentivirus vector, Long noncoding RNA HOTAIR, protein RNA binding, cell cycle regulation, signal transduction, gene overexpression, long untranslated RNA, Breast Neoplasms, Biology, RNA gene, Article, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, Breast cancer, breast cancer, breast cancer cell line, Genetics, medicine, Long intervening noncoding RNA p21 protein, controlled study, human, tumor suppressor protein, Cell Proliferation, tumor cell line, medicine.disease, 030104 developmental biology, Myc protein, Cancer research, protein MEG3, pathology, GAS5, biosynthesis, untranslated RNA, MYC protein, human

Abstract

Aim MYC deregulation contributes to breast cancer development and progression. Deregulated expression levels of long non-coding RNAs (lncRNA) have been demonstrated to be critical players in development and/or maintenance of breast cancer. In this study we aimed to evaluate lncRNA expressions depending on MYC overexpression and knockdown in breast cancer cells. Materials and methods Cells were infected with lentiviral vectors by either knockdown or overexpression of c-MYC. LncRNA cDNA was transcribed from total RNA samples and lncRNAs were evaluated by qRT-PCR. Results Our results indicated that some of the lncRNAs having tumor suppressor (GAS5, MEG3, lincRNA-p21) and oncogenic roles (HOTAIR) are regulated by c-MYC. Conclusion We observed that c-MYC regulates lncRNAs that have important roles on proliferation, cell cycle and etc. Further studies will give us a light to identify molecular mechanisms related to MYC-lncRNA regulatory pathways in breast cancer.

Published

2019

2. Identification of the ribosome binding sites of translation initiation factor IF3 by multidimensional heteronuclear NMR spectroscopy

Author

Marco Sette, Rolf Boelens, Paul J.A. van Tilborg, Roberto Spurio, and Claudio O. Gualerzi

Subjects

Models, Molecular, Secondary, Magnetic Resonance Spectroscopy, Protein Conformation, Eukaryotic Initiation Factor-3, 30S ribosomes, NMR titrations, Protein domains, Protein synthesis, RNA- protein interaction, protein synthesis regulation, Ribosome, Protein Structure, Secondary, Protein structure, Models, Peptide Initiation Factors, RNA-Protein Interaction, Protein biosynthesis, 30S, initiation factor 3, article, protein domain, RNA-Binding Proteins, priority journal, Ribonucleoproteins, Biochemistry, ribosome subunit, protein RNA binding, Research Article, Protein Structure, Stereochemistry, Molecular Sequence Data, Protein domain, translation regulation, Biology, RNA, binding site, controlled study, escherichia coli, molecular recognition, nonhuman, Amino Acid Sequence, Bacterial Proteins, Binding Sites, Escherichia coli, Mutation, Ribosomes, Settore BIO/10, Binding site, Molecular Biology, Molecular, Ribosomal RNA

Abstract

Titrations of Escherichia coli translation initiation factor IF3, isotopically labeled with 15 N, with 30S ribosomal subunits were followed by NMR by recording two-dimensional ( 15 N, 1 H)-HSQC spectra. In the titrations, intensity changes are observed for cross peaks belonging to amides of individual amino acids. At low concentrations of ribosomal subunits, only resonances belonging to amino acids of the C-domain of IF3 are affected, whereas all those attributed to the N-domain are still visible. Upon addition of a larger amount of 30S subunits cross peaks belonging to residues of the N-terminal domain of the protein are also selectively affected. Our results demonstrate that the two domains of IF3 are functionally independent, each interacting with a different affinity with the ribosomal subunits, thus allowing the identification of the individual residues of the two domains involved in this interaction. Overall, the C-domain interacts with the 30S subunits primarily through some of its loops and a-helices and the residues involved in ribosome binding are distributed rather symmetrically over a fairly large surface of the domain, while the N-domain interacts mainly via a small number of residues distributed asymmetrically in this domain. The spatial organization of the active sites of IF3, emerging through the comparison of the present data with the previous chemical modification and mutagenesis data, is discussed in light of the ribosomal localization of IF3 and of the mechanism of action of this factor.

Published

1999

3. Gar1p Binds to the Small Nucleolar RNAs snR10 and snR30 in Vitro through a Nontypical RNA Binding Element

Author

Bruno Lapeyre and Claudia Bagni

Subjects

cell nucleolus ribonucleic acid, fibrillarin, nuclear protein, pseudouridine, ribosome rna, rna, unclassified drug, article, cell growth, controlled study, genetic transcription, immunoprecipitation, nonhuman, nucleolus, priority journal, protein rna binding, rna cleavage, rna processing, rna translation, saccharomyces cerevisiae, Amino Acid Sequence, Fungal Proteins, Molecular Sequence Data, Nuclear Proteins, Protein Binding, Ribonucleoproteins, Small Nucleolar, RNA, Small Nuclear, RNA-Binding Proteins, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, Sequence Deletion, Sequence Homology, Amino Acid, Heterogeneous nuclear ribonucleoprotein, Sequence Homology, Plasma protein binding, yeast, Biochemistry, Preribosomal RNA, Small nucleolar RNA, heterogeneous nuclear ribonucleoprotein, Ribonucleoprotein, preribosomal rna, Settore BIO/13, glycine-rich, Cell biology, Amino Acid, Ribonucleoproteins, saccharomyces-cerevisiae, recognition, Pseudouridine synthesis, Biology, Small Nuclear, gene, Molecular Biology, Small Nucleolar, Fibrillarin, urogenital system, RNA, Cell Biology, Molecular biology, pre-ribosomal-rna, protein gar1, identification

Abstract

The nucleolar proteins Gar1p and fibrillarin possess a typical nucleolar glycine/arginine-rich domain and belong to ribonucleoprotein particles. Both proteins are essential for yeast cell growth and are required for pre-rRNA processing. In addition, Gar1p is involved in pre-rRNA pseudouridylation, whereas fibrillarin is required for pre-rRNA methylation. Gar1p and fibrillarin are each associated with a different subset of the small nucleolar RNAs (snoRNAs). Gar1p is co-immunoprecipitated with the H/ACA family of snoRNAs, whereas fibrillarin is co-immunoprecipitated with the C/D family. However, attempts to demonstrate direct interactions between fibrillarin and snoRNAs have failed, and such interactions between Gar1p and the H/ACA snoRNAs had not get been reported. Among the H/ACA snoRNAs associated with Gar1p, one can distinguish a large group of snoRNAs that are not essential in yeast and serve as guides for pseudouridine synthesis onto the pre-rRNA molecule. In contrast, the two snoRNAs snR10 and snR30 are required for normal cell growth and for pre-rRNA cleavage. We show here that Gar1p interacts in vitro directly and specifically with these two snoRNAs, Deletion analysis of Gar1p indicates that a major RNA binding element, which is extremely well conserved throughout evolution, lies in the middle of the protein. However, this domain alone binds poorly to the target RNAs and an accessory domain is required to restore efficient binding. The accessory domain can be either one of the glycine/arginine-rich domains or a second element of the core of the protein that is highly conserved between different species. ispartof: Journal of biological chemistry vol:273 issue:18 pages:10868-10873 ispartof: location:United States status: published

Published

1998

4. Genome-wide analysis reveals characteristics of off-target sites bound by the Cas9 endonuclease

Author

Mazhar Adli, Jeremy Thorpe, Sevki Arslan, Ritambhara Singh, and Cem Kuscu

Subjects

genetic processes, Applied Microbiology and Biotechnology, endonuclease, Clinical research, Endonuclease, protein cleavage, Guide RNA, indel mutation, Cells, Cultured, genome analysis, Genetics, High-throughput sequencing, Genome, biology, article, food and beverages, Chromosome Mapping, unclassified drug, enzyme activity, Nucleic acids, priority journal, HEK293 cell line, Gene Targeting, Molecular Medicine, enzyme binding, protein RNA binding, cas9 endonuclease, Biotechnology, Background level, Base Sequence, Binding Sites, CRISPR-Cas Systems/*genetics, Deoxyribonuclease I/*genetics, Embryonic Stem Cells/*physiology, Gene Targeting/*methods, Genome/*genetics, HEK293 Cells, Humans, Models, Genetic, Molecular Sequence Data, Biomedical Engineering, Genome wide analysis, embryo, Bioengineering, Genomics, RNA sequence, Computational biology, chromatin immunoprecipitation, Molecular engineering, high throughput sequencing, Deoxyribonuclease I, natural sciences, controlled study, human, Indel, Embryonic Stem Cells, catalysis, Cas9, binding site, human cell, nucleotide sequence, Endonucleases, guide RNA, Genes, biology.protein, chromatin, CRISPR-Cas Systems

Abstract

RNA-guided genome editing with the CRISPR-Cas9 system has great potential for basic and clinical research, but the determinants of targeting specificity and the extent of off-target cleavage remain insufficiently understood. Using chromatin immunoprecipitation and high-throughput sequencing (ChIP-seq), we mapped genome-wide binding sites of catalytically inactive Cas9 (dCas9) in HEK293T cells, in combination with 12 different single guide RNAs (sgRNAs). The number of off-target sites bound by dCas9 varied from â ̂1/410 to >1,000 depending on the sgRNA. Analysis of off-target binding sites showed the importance of the PAM-proximal region of the sgRNA guiding sequence and that dCas9 binding sites are enriched in open chromatin regions. When targeted with catalytically active Cas9, some off-target binding sites had indels above background levels in a region around the ChIP-seq peak, but generally at lower rates than the on-target sites. Our results elucidate major determinants of Cas9 targeting, and we show that ChIP-seq allows unbiased detection of Cas9 binding sites genome-wide. © 2014 Nature America, Inc.

Published

2014

5. Development of RNA stiffness parameters and analysis on protein-RNA binding specificity: Comparison with DNA

Author

Gromiha, M.M.

Subjects

hydrogen bond, PP7 coat protein, atom, DNA, nucleotide, protein DNA binding, RBD1 protein, dissociation constant, trinucleotide, unclassified drug, U1A protein, RNA stiffness, priority journal, rigidity, coat protein, hydrogen, binding affinity, RNA, elasticity, molecular recognition, protein RNA binding, protein, RNA structure

Abstract

It has been well established that the elastic character of DNA plays an important role in protein-DNA binding specificity. In this work, we have analyzed the role of elasticity to understand the binding specificity of protein-RNA complexes. We have developed a sequence dependent stiffness scale for the trinucleotides in RNA and revealed the similarities and differences compared with DNA. We found that the stiffness of 15 trinucleotides has inverse effects and nine nucleotides are significantly different between RNA and DNA. The analysis on the relationship between RNA stiffness and RNA-binding specificity shows that the influence of elasticity is minimal in protein-RNA recognition, whereas it plays an important role in protein-DNA binding specificity. We observed a moderate correlation between stiffness and dissociation constant in U1A RBD1 protein and PP7 coat protein, whereas the correlation is poor for many other complexes. These results show that along with RNA stiffness, other interactions, such as shape complementarity, electrostatic interactions, hydrogen bonds and direct contacts between RNA and protein atoms are important for protein-RNA recognition. � 2012 Bentham Science Publishers.

Published

2012

6. Methionine sulfoxide reductases protect Ffh from oxidative damages in Escherichia coli

Author

Régis Grimaud, Daniéle Moinier, Frédéric Barras, Benjamin Ezraty, Mohammed El Hassouni, Laboratoire Electronique, Informatique et Image [UMR6306] (Le2i), Université de Bourgogne (UB)-École Nationale Supérieure d'Arts et Métiers (ENSAM), Arts et Métiers Sciences et Technologies, HESAM Université (HESAM)-HESAM Université (HESAM)-Arts et Métiers Sciences et Technologies, HESAM Université (HESAM)-HESAM Université (HESAM)-AgroSup Dijon - Institut National Supérieur des Sciences Agronomiques, de l'Alimentation et de l'Environnement-Centre National de la Recherche Scientifique (CNRS), Institut de biologie et chimie des protéines [Lyon] (IBCP), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), Laboratoire Electronique, Informatique et Image ( Le2i ), Université de Bourgogne ( UB ) -AgroSup Dijon - Institut National Supérieur des Sciences Agronomiques, de l'Alimentation et de l'Environnement-Centre National de la Recherche Scientifique ( CNRS ), Institut de biologie et chimie des protéines [Lyon] ( IBCP ), Université Claude Bernard Lyon 1 ( UCBL ), and Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique ( CNRS )

Subjects

methionine sulfoxide reductase b, methionine sulfoxide reductase a, protein synthesis, [SDV]Life Sciences [q-bio], Mutant, animal cell, Negibacteria, reactive oxygen metabolite, medicine.disease_cause, Mass Spectrometry, Substrate Specificity, chemistry.chemical_compound, chemistry.chemical_classification, 0303 health sciences, General Neuroscience, Escherichia coli Proteins, 030302 biochemistry & molecular biology, article, aerobic metabolism, protein domain, unclassified drug, Protein Transport, Biochemistry, priority journal, Methionine sulfoxide reductase, protein RNA binding, Oxidoreductases, Oxidation-Reduction, MSRA, Protein Binding, oxidation, Molecular Sequence Data, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, medicine, Escherichia coli, protein targeting, Animalia, controlled study, Amino Acid Sequence, Molecular Biology, 030304 developmental biology, methionine, Methionine, nonhuman, [ SDV ] Life Sciences [q-bio], General Immunology and Microbiology, Methionine sulfoxide, RNA, Membrane Proteins, protein ffh, Oxidative Stress, Enzyme, chemistry, Methionine Sulfoxide Reductases, methionine sulfoxide reductase, Mutation, Signal Recognition Particle

Abstract

cited By 46; International audience; In proteins, methionine residues are primary targets for oxidation. Methionine oxidation is reversed by methionine sulfoxide reductases A and B, a class of highly conserved enzymes. Ffh protein, a component of the ubiquitous signal recognition particle, contains a methionine-rich domain, interacting with a small 4.5S RNA. In vitro analyses reported here show that: (i) oxidized Ffh is unable to bind 4.5S RNA, (ii) oxidized Ffh contains methionine sulfoxide residues, (iii) oxidized Ffh is a substrate for MsrA and MsrB enzymes; and (iv) MsrA/B repairing activities allow oxidized Ffh to recover 4.5S RNA-binding abilities. In vivo analyses reveal that: (i) Ffh synthesized in the msrA msrB mutant contains methionine sulfoxide residues and is unstable, (ii) msrA msrB mutant requires high levels of Ffh synthesis for growth and (iii) msrA msrB mutation leads to defects in Ffh-dependent targeting of MalF. We conclude that MsrA and MsrB are required to repair Ffh oxidized by reactive oxygen species produced by aerobic metabolism, establishing an as-yet undescribed link between protein targeting and oxidation.

Published

2004

7. La protein has a positive effect on the translation of TOP mRNAs in vivo

Author

Claudia Crosio, Francesco Amaldi, Fabrizio Loreni, Pietro Pilo Boyl, and Paola Pierandrei-Amaldi

Subjects

pyrimidine, sequence analysis, Xenopus, Messenger, Gene Expression, animal cell, Autoantigens, Xenopus laevis, nucleic acid binding protein, Gene expression, Translational regulation, Protein biosynthesis, Ribonucleoprotein, messenger RNA, oligonucleotide, ribosome protein, 5' untranslated region, amino acid sequence, article, cell strain, controlled study, gene expression regulation, genetic transfection, human, human cell, nonhuman, plasmid, priority journal, protein expression, protein processing, protein RNA binding, reporter gene, translation regulation, 5' Untranslated Regions, Animals, Cell Line, Protein Biosynthesis, Pyrimidines, Ribonucleoproteins, RNA, Messenger, Transfection, Animalia, Vertebrata, Settore BIO/11, Translation (biology), Biology, Ribosomal protein, Genetics, Gene, Messenger RNA, Molecular biology, RNA

Abstract

In vertebrates, the mRNAs encoding ribosomal proteins, as well as other proteins implicated in translation, are characterized by a 5′-untranslated region (5′-UTR), including a stretch of pyrimidines at the 5′-end. The 5′-terminal oligopyrimidine (5′-TOP) sequence, which is involved in the growth-dependent translational regulation characteristic of this class of genes (so-called TOP genes), has been shown to specifically bind the La protein in vitro, suggesting that La might be implicated in translational regulation in vivo. In order to substantiate this hypothesis, we have examined the effect of La on TOP mRNA translational control in both stable and transient transfection experiments. In particular we have constructed and analyzed three stably transfected Xenopus cell lines inducible for overexpression of wild-type La or of putative dominant negative mutated forms. Moreover, La-expressing plasmids have been transiently co-transfected together with a plasmid expressing a reporter TOP mRNA in a human cell line. Our results suggest that in vivo La protein plays a positive role in the translation of TOP mRNA. They also suggest that the function of La is to counteract translational repression exerted by a negative factor, possibly cellular nucleic acid binding protein (CNBP), which has been previously shown to bind the 5′-UTR downstream from the 5′-TOP sequence.

Published

2000

8. Dissecting FMR1, the protein responsible for fragile X syndrome, in its structural and functional domains

Author

Giovanna Musco, Toby J. Gibson, Lelio Mazzarella, Salvatore Adinolfi, Claudia Bagni, Annalisa Pastore, Adinolfi, S., Bagni, C., Musco, G., Gibson, T., Mazzarella, Lelio, Pastore, A., Adinolfi, S, Bagni, C, Musco, G, Gibson, T, Mazzarella, L, Pastore, A, L., Mazzarellainolfi, C., Bagni, G., Musco, T., Gibson, and A., Pastore

Subjects

Protein Folding, Magnetic Resonance Spectroscopy, sequence analysis, fragile X, Sequence Homology, polyguanylic acid, RNA-binding protein, localization, Fragile X Mental Retardation Protein, Protein sequencing, Models, binding affinity, rna-binding, fragile X syndrome, FMR1, Peptide sequence, Protein secondary structure, Blotting, Circular Dichroism, Settore BIO/13, article, fragile x, protein domain, RNA-Binding Proteins, RNA analysis, structure analysis, Recombinant Proteins, unclassified drug, reaction analysis, Amino Acid, priority journal, Biochemistry, Protein folding, nuclear export, protein RNA binding, Western, kh-domain, Research Article, Protein Binding, Sequence analysis, Blotting, Western, peptide mapping, Molecular Sequence Data, Nerve Tissue Proteins, in-vitro, Biology, fmr1, ribonucleoprotein, Structure-Activity Relationship, Genetic, modular proteins, Humans, Amino Acid Sequence, gene, Molecular Biology, mental-retardation protein, carboxy terminal sequence, fragile X mental retardation protein, RNA binding protein, amino terminal sequence, binding site, molecular dynamics, protein determination, protein folding, sequence homology, Fragile X Syndrome, Models, Genetic, Mutagenesis, RNA, Sequence Homology, Amino Acid, rna-binding proteins, FMR1, fragile sites, fragile X, modular proteins, RNA-binding proteins, Molecular biology, KH domain, polyribosomes, fragile sites, mutation

Abstract

FMR1 is an RNA-binding protein that is either absent or mutated in, patients affected by the fragile X syndrome, the most common inherited cause of mental retardation in humans. Sequence analysis of the FMR1 protein has suggested that RNA binding is related to the presence of two K-homologous (KH) modules and an RGG box. However, no attempt has been so far made to map the RNA-binding sites along the protein sequence and to identify possible differential RNA-sequence specificity. In the present article, we describe work done to dissect FMR1 into regions with structurally and functionally distinct properties. A semirational approach was followed to identify four regions: an :N-terminal stretch of 200 amino acids, the two KH-regions, and a C-terminal stretch. Each region was produced as a recombinant protein, purified, and probed for its state of folding by spectroscopical techniques. Circular,dichroism and NMR spectra of the N-terminus show formation of secondary structure with a strong tendency to aggregate. Of the two homologous KH motifs, only the first one is folded whereas the second remains unfolded even when it is extended both N-and C-terminally. The C-terminus is, as expected from its amino acid composition, nonglobular. Binding assays were then performed using the 4-nt homopolymers. Our results show that only the first KH domain but not the second binds to RNA, and provide the first direct evidence for RNA binding of both the N-terminal and the C-terminal regions. RNA binding for the N-terminus could not be predicted from sequence analysis because no known RNA-binding motif is identifiable in this region. Different sequence specificity was observed for the fragments: both the N-terminus of the protein and KH1 bind preferentially to poly-(ra). The C-terminal region, which contains the RGG box, is nonspecific, as it recognizes the bases with comparable affinity. We therefore conclude that FMR1 is a protein with multiple sites of interaction with RNA: sequence specificity is most likely achieved by the whole block that comprises the first approximate to 400 residues, whereas the C-terminus provides a nonspecific binding surface. ispartof: Rna-a publication of the rna society vol:5 issue:9 pages:1248-1258 ispartof: location:United States status: published

Published

1999