Your search keyword '"Nagata, Kyosuke"' showing total 83 results

1. Measles virus C protein facilitates transcription by the control of N protein-viral genomic RNA interaction in early phases of infection.

Author

Nishie, Tomomi and Nagata, Kyosuke

Subjects

*MEASLES virus, *VIRAL proteins, *GENETIC transcription, *MICROBIAL genomics, *RNA synthesis, *VIRUSES

Abstract

Measles virus (MV) C protein has been known a multifunctional protein involved in anti-IFN response, viral RNA synthesis, and so on. Recent studies have clarified that double-stranded RNA (dsRNA) is derived from viral genomic RNA (vRNA), and the amount of dsRNA was increased in an MV lacking C protein (MV(C-))-infected cells, suggesting that C protein blocks viral RNA synthesis. However, detailed roles of C protein in viral RNA synthesis remain unknown. Here, we have confirmed through time course experiments using Vero/hSLAM cells that as reported previously, the amount of mRNA is increased in MV(C-)-infected cells at 36 h post infection (hpi). In contrast, we found that the transcription level is lower in MV(C-)-infected cells than wild-type MV-infected cells in early phases of infection. Immunoprecipitation assays were performed to find an interactor(s) of C protein, revealed that C protein interacts with N protein in the absence of vRNA and P protein. RNA immunoprecipitation (RIP) assays showed that the interaction between N protein and vRNA was increased in MV(C-)-infected cells. These results suggest that in early phases of infection C protein facilitates viral transcription to control the formation of nascent nucleocapsid composed of N protein and vRNA. [ABSTRACT FROM AUTHOR]

Published

2015

2. Upstream binding factor-dependent and pre-rRNA transcription-independent association of pre-rRNA processing factors with rRNA gene.

Author

Ueshima, Shuhei, Nagata, Kyosuke, and Okuwaki, Mitsuru

Subjects

*RIBOSOMAL RNA, *TRANSCRIPTION factors, *CARRIER proteins, *NUCLEAR proteins, *RNA polymerases, *CHROMATIN

Abstract

Highlights: [•] Pre-rRNA processing factors associate with rRNA gene. [•] The rRNA gene association of pre-rRNA processing factors is decreased in mitosis. [•] The pre-rRNA processing factors-rRNA gene association is transcription-independent. [•] UBF is necessary for the association of pre-rRNA processing factors with rRNA gene. [ABSTRACT FROM AUTHOR]

Published

2014

3. Replication-Uncoupled Histone Deposition during Adenovirus DNA Replication.

Author

Komatsu, Tetsuro and Nagata, Kyosuke

Subjects

*ADENOVIRUSES, *VIRAL replication, *HISTONES, *DNA replication, *MOLECULAR structure of chromatin, *VIRAL genomes, *IMMUNOPRECIPITATION

Abstract

In infected cells, the chromatin structure of the adenovirus genome DNA plays critical roles in its genome functions. Previously, we reported that in early phases of infection, incoming viral DNA is associated with both viral core protein VII and cellular histones. Here we show that in late phases of infection, newly synthesized viral DNA is also associated with histones. We also found that the knockdown of CAF-1, a histone chaperone that functions in the replication-coupled deposition of histones, does not affect the level of histone H3 bound on viral chromatin, although CAF-1 is accumulated at viral DNA replication foci together with PCNA. Chromatin immunoprecipitation assays using epitope-tagged histone H3 demonstrated that histone variant H3.3, which is deposited onto the cellular genome in a replication-independent manner, is selectively associated with both incoming and newly synthesized viral DNAs. Microscopic analyses indicated that histones but not USF1, a transcription factor that regulates viral late gene expression, are excluded from viral DNA replication foci and that this is achieved by the oligomerization of the DNA binding protein (DBP). Taken together, these results suggest that histone deposition onto newly synthesized viral DNA is most likely uncoupled with viral DNA replication, and a possible role of DBP oligomerization in this replication-uncoupled histone deposition is discussed. [ABSTRACT FROM AUTHOR]

Published

2012

4. Synergistic requirement of orphan nonamer-like elements and DNA bending enhanced by HMGB1 for RAG-mediated nicking at cryptic 12-RSS but not authentic 12-RSS.

Author

Numata, Masashi and Nagata, Kyosuke

Subjects

*DNA, *SCISSION (Chemistry), *CHROMOSOMAL translocation, *GENETICS, *CHROMOSOMES, *IMMUNOASSAY

Abstract

V(D)J recombination is initiated by the specific binding of the recombination activating gene (RAG) complex to the heptamer and nonamer elements within recombination signal sequence (RSS). The break points associated with some chromosomal translocations contain cryptic RSSs, and mistargeting of RAG proteins to these less conserved elements could contribute to an aberrant V(D)J recombination. Recently, we found RAG-dependent recombination in the hotspots of TEL- AML1 t(12;21)(p13;q22) chromosomal translocation by an extrachromosomal recombination assay. Here, we describe using in vitro cleavage assays that RAG proteins directly bind to and introduce nicks into TEL and AML1 translocation regions, which contain several heptamer-like sequences. The cryptic nicking site within the TEL fragment was cleaved by RAG proteins essentially depending on a 12-RSS framework, and the nicking activity was enhanced synergistically by both HMGB1 and orphan nonamer-like (NL) sequences, which do not possess counterpart heptamers. In addition, we found that DNA bending stimulated by HMGB1 is indispensable for the HMGB1- and orphan NL element-dependent enhancement of RAG-mediated nicking at the cryptic 12-RSS. Collectively, we would propose the mechanism of HMGB1-dependent enhancement of RAG-mediated nicking at a cryptic RSS through enhanced DNA bending. [ABSTRACT FROM AUTHOR]

Published

2011

5. De novo replication of the influenza virus RNA genome is regulated by DNA replicative helicase, MCM.

Author

Kawaguchi, Atsushi and Nagata, Kyosuke

Subjects

*INFLUENZA viruses, *RNA, *GENOMES, *DNA replication, *RESPIRATORY infections

Abstract

By dissecting and reconstituting a cell-free influenza virus genome replication system, we have purified and identified the minichromosome maintenance (MCM) complex, which is thought to be a DNA replicative helicase, as one of the host factors that regulate the virus genome replication. MCM interacted with the PA subunit of the viral RNA-dependent RNA polymerase that is found to be involved in the replication genetically. The virus genome replication was decreased in MCM2 knockdown cells. The viral polymerase appeared to be a nonproductive complex, that is, it was capable of initiating replication but produced only abortive short RNA chains. MCM stimulated de novo-initiated replication reaction by stabilizing a replication complex during its transition from initiation to elongation. Based on the findings, including the result that the MCM-mediated RNA replication reaction was competed with exogenously added RNA, we propose that MCM functions as a scaffold between the nascent RNA chains and the viral polymerase. [ABSTRACT FROM AUTHOR]

Published

2007

6. The C protein of wild-type measles virus has the ability to shuttle between the nucleus and the cytoplasm

Author

Nishie, Tomomi, Nagata, Kyosuke, and Takeuchi, Kaoru

Subjects

*MEASLES virus, *MORBILLIVIRUSES, *MEASLES, *VIRUS diseases

Abstract

Abstract: Measles virus (MV) C protein is a small and basic non-structural protein, but its function is not well understood. We have found that a FLAG-tagged wild-type MV C protein expressed from cDNA was accumulated exclusively in the nucleus. To analyze the amino acid sequence important for the nuclear localization of C protein, a plasmid expressing C protein fused to the enhanced green fluorescent protein (EGFP) was generated. Mutation analysis revealed that 41PPARKRRQ48, belonging to the classical nuclear localization signal was important for nuclear localization. Analysis of the amino acid sequence of C protein revealed that it has a nuclear export signal (NES)-like sequence, 76LEKAMTTLKL85. Addition of the putative NES to the EGFP resulted in the translocation of EGFP to the cytoplasm. The Rev(1.4)-EGFP nuclear export assay showed that this putative NES has a CRM1-dependent NES activity. C-EGFP accumulated in HeLa nuclei could be translocated to NIH3T3 nuclei in heterokaryon assays. In MV-infected cells, C-EGFP was accumulated in the nuclei in early phase but in the cytoplasm in late phase. These results indicate that the putative NES is functional and that C protein has the ability to shuttle between the nucleus and the cytoplasm. [Copyright &y& Elsevier]

Published

2007

7. Template activating factor-I epigenetically regulates the TERT transcription in human cancer cells.

Author

Kato, Kohsuke, Kawaguchi, Atsushi, and Nagata, Kyosuke

Subjects

*TELOMERES, *CANCER cells, *HELA cells, *GENETIC regulation, *GENETIC transcription

Abstract

Telomere, the terminus of linear chromosome in eukaryotes, is composed of specific repeat DNA which is mainly synthesized by a protein complex called telomerase. The maintenance of telomere DNA is important for unlimited proliferative capacity of cancer cells. The telomerase activity is controlled by the expression level of telomerase reverse transcriptase (TERT), a catalytic unit of telomerase, in some species including human. Therefore, to reveal the regulatory mechanisms of the transcription of TERT gene is important for understanding the tumor development. We found that template activating factor-I (TAF-I), a multifunctional nuclear protein, is involved in the transcriptional activation of TERT for the maintenance of telomere DNA in HeLa cells. TAF-I maintains the histone H3 modifications involved in transcriptional activation and hypomethylated cytosines in CpG dinucleotides around the transcription start site (TSS) in the TERT gene locus. Collectively, TAF-I is involved in the maintenance of telomere DNA through the regulation of TERT transcription, then consequently the occurrence and/or recurrence of cancer cells. [ABSTRACT FROM AUTHOR]

Published

2021

8. Biochemical characterization of avian influenza viral polymerase containing PA or PB2 subunit from human influenza A virus.

Author

Pham, Phu Tran Vinh, Turan, Kadir, Nagata, Kyosuke, and Kawaguchi, Atsushi

Subjects

*GENETIC mutation, *AVIAN influenza A virus, *ENDONUCLEASES, *BIOLOGICAL adaptation, *MEDICAL care

Abstract

Adaptive mutations in viral polymerase, which is composed of PB1, PB2, and PA, of avian influenza viruses are major genetic determinants of the host range. In this study, to elucidate the molecular mechanism of mammalian adaptation of avian viral polymerase, we performed cell-based vRNP reconstitution assays and biochemical analyses using purified recombinant viral polymerase complexes. We found that avian viral polymerase from A/duck/Pennsylvania/10,218/84 (DkPen) enhances the viral polymerase activity in mammalian cells by replacing the PA or PB2 gene with that from human influenza virus A/WSN/33 (WSN). Chimeric constructs between DkPen PA and WSN PA showed that the N-terminal endonuclease domain of WSN PA was essential for the mammalian adaptation of DkPen viral polymerase. We also found that the cap-snatching activity of purified DkPen viral polymerase was more than 5 times weaker than that of WSN in vitro in a PB2 Glu627-dependent manner. However, the cap-snatching activity of DkPen viral polymerase was hardly increased by replacing DkPen PA to WSN PA. These results suggest that the activity of viral genome replication may be enhanced in the DkPen reassortant containing WSN PA. [ABSTRACT FROM AUTHOR]

Published

2018

9. Selective regulation of type II interferon‐inducible genes by NPM1/nucleophosmin.

Author

Abe, Mayumi, Lin, Jianhuang, Nagata, Kyosuke, and Okuwaki, Mitsuru

Subjects

*NUCLEOPHOSMIN, *TRANSCRIPTION factors, *NUCLEAR proteins, *GENETIC regulation, *INTERFERONS, *GENE expression

Abstract

Nucleophosmin (NPM1) is a multifunctional nucleolar protein. Here, we analyze the role of NPM1 in gene expression using our previous microarray data and find a relationship between NPM1 and interferon (IFN)‐γ‐inducible genes. We show that NPM1 selectively regulates the expression of a subset of IFN‐γ‐inducible genes and directly binds to two important transcription factors in the type II IFN pathway: signal transducer and activator of transcription 1 and interferon regulatory factor 1 (IRF1). Furthermore, NPM1 is found to regulate the IFN‐γ‐inducible promoter activity of major histocompatibility complex class II transactivator (CIITA), and mutation of the IRF1‐binding site on the CIITA promoter abolishes the effect of NPM1. Our results suggest a novel mechanism for IFN‐γ‐mediated gene expression by NPM1. [ABSTRACT FROM AUTHOR]

Published

2018

10. A small RNA system ensures accurate homologous pairing and unpaired silencing of meiotic chromosomes.

Author

Tabara, Hiroaki, Mitani, Shohei, Mochizuki, Megumi, Kohara, Yuji, and Nagata, Kyosuke

Subjects

*NON-coding RNA, *CHROMOSOMES, *HOMOLOGOUS chromosomes, *ARGONAUTE proteins, *COHESINS, *TRANSPOSONS, *LINCRNA

Abstract

During meiosis, chromosomes with homologous partners undergo synaptonemal complex (SC)‐mediated pairing, while the remaining unpaired chromosomes are heterochromatinized through unpaired silencing. Mechanisms underlying homolog recognition during SC formation are still unclear. Here, we show that the Caenorhabditis elegans Argonaute proteins, CSR‐1 and its paralog CSR‐2, interacting with 22G‐RNAs, are required for synaptonemal complex formation with accurate homology. CSR‐1 in nuclei and meiotic cohesin, constituting the SC lateral elements, were associated with nonsimple DNA repeats, including minisatellites and transposons, and weakly associated with coding genes. CSR‐1‐associated CeRep55 minisatellites were expressing 22G‐RNAs and long noncoding (lnc) RNAs that colocalized with synaptonemal complexes on paired chromosomes and with cohesin regions of unpaired chromosomes. CeRep55 multilocus deletions reduced the efficiencies of homologous pairing and unpaired silencing, which were supported by the csr‐1 activity. Moreover, CSR‐1 and CSR‐2 were required for proper heterochromatinization of unpaired chromosomes. These findings suggest that CSR‐1 and CSR‐2 play crucial roles in homology recognition, achieving accurate SC formation between chromosome pairs and condensing unpaired chromosomes by targeting repeat‐derived lncRNAs. Synopsis: It remains unclear how the homologous sequences of meiotic chromosomes, excluding the pairing center regions, are recognized during synaptonemal complex (SC) formation. This study describes a new model where an Argonaute‐dependent small RNA system is involved in homolog recognition during SC formation in C. elegans. Argonaute protein CSR‐1 and its paralog CSR‐2 interacting with 22G‐RNAs are required for SC formation between chromosome pairs with accurate homology.CSR‐1 and CSR‐2 are also involved in the condensation of unpaired chromosomes.CSR‐1 in nuclei and meiotic cohesin containing COH‐3/4 are associated with non‐simple DNA repeats and weakly with coding genes.CSR‐1 plays pleiotropic roles in the endogenous and exogenous RNAi pathways. [ABSTRACT FROM AUTHOR]

Published

2023

11. Histone H1 chaperone activity of TAF-I is regulated by its subtype-dependent intramolecular interaction.

Author

Kajitani, Kaori, Kato, Kohsuke, and Nagata, Kyosuke

Subjects

*MOLECULAR structure of histones, *MOLECULAR chaperones, *INTRAMOLECULAR forces, *MOLECULAR interactions, *DIMERIZATION, *C-terminal residues

Abstract

Linker histone H1 is involved in the regulation of gene activity through the maintenance of higher-order chromatin structure. Previously, we have shown that template activating factor-I ( TAF-I or protein SET) is involved in linker histone H1 dynamics as a histone H1 chaperone. In human and murine cells, two TAF-I subtypes exist, namely TAF-Iα and TAF-Iβ. TAF-I has a highly acidic amino acid cluster in its C-terminal region and forms homo- or heterodimers through its dimerization domain. Both dimer formation and the C-terminal region of TAF-I are essential for the histone chaperone activity. TAF-Iα exhibits less histone chaperone activity compared with TAF-Iβ even though TAF-Iα and β differ only in their N-terminal regions. However, it is unclear how subtype-specific TAF-I activities are regulated. Here, we have shown that the N-terminal region of TAF-Iα autoinhibits its histone chaperone activity via intramolecular interaction with its C-terminal region. When the interaction between the N- and C-terminal regions of TAF-Iα is disrupted, TAF-Iα shows a histone chaperone activity similar to that of TAF-Iβ. Taken together, these results provide mechanistic insights into the concept that fine tuning of TAF-I histone H1 chaperone activity relies on the subtype compositions of the TAF-I dimer. [ABSTRACT FROM AUTHOR]

Published

2017

12. Zinc binding of a Cys2His2-type zinc finger protein is enhanced by the interaction with DNA.

Author

Hajdu, Bálint, Hunyadi-Gulyás, Éva, Kato, Kohsuke, Kawaguchi, Atsushi, Nagata, Kyosuke, and Gyurcsik, Béla

Subjects

*ZINC-finger proteins, *DNA-binding proteins, *PEPTIDES, *STABILITY constants, *DNA, *NUCLEOTIDE sequence

Abstract

Zinc finger proteins specifically recognize DNA sequences and, therefore, play a crucial role in living organisms. In this study the Zn(II)-, and DNA-binding of 1MEY#, an artificial zinc finger protein consisting of three finger units was characterized by multiple methods. Fluorimetric, circular dichroism and isothermal calorimetric titrations were applied to determine the accurate stability constant of a zinc finger protein. Assuming that all three zinc finger subunits behave identically, the obtained thermodynamic data for the Zn(II) binding were ΔHbinding site = − (23.5 − 28.0) kcal/mol (depending on the applied protonation state of the cysteines) and logβ'pH 7.4 = 12.2 ± 0.1, being similar to those of the CP1 consensus zinc finger peptide. The specific DNA binding of the protein can be characterized by logβ'pH 7.4 = 8.20 ± 0.08, which is comparable to the affinity of the natural zinc finger proteins (Sp1, WT1, TFIIIA) toward DNA. This value is ~ 1.9 logβ' unit higher than those determined for semi- or nonspecific DNA binding. Competitive circular dichroism and electrophoretic mobility shift measurements revealed that the conditional stability constant characteristic for Zn(II) binding of 1MEY# protein increased by 3.4 orders of magnitude in the presence of its target DNA sequence. [ABSTRACT FROM AUTHOR]

Published

2023

13. pp32, an INHAT component, is a transcription machinery recruiter for maximal induction of IFN-stimulated genes.

Author

Kadota, Shinichi and Nagata, Kyosuke

Subjects

*ANTIVIRAL agents, *INTERFERONS, *ACETYLTRANSFERASES, *HISTONE deacetylase, *TYROSINE, *PHOSPHORYLATION

Abstract

Type I interferon (IFN) plays a crucial role in establishing the cellular antiviral state by inducing transcription of IFN-stimulated genes (ISGs). Generally, histone acetyltransferases (HATs) are positive regulators of transcription, but histone deacetylase (HDAC) activity is essential for transcriptional induction of ISGs. pp32 is known to be a key component of the inhibitor of acetyltransferase (INHAT) complex that inhibits HAT-dependent transcriptional activation. Here, we show that pp32 is involved in the positive regulation of ISG transcription. pp32 interacted with signal transducer and activator of transcription 1 (STAT1) and STAT2 in an IFN-dependent manner. pp32 was not required for tyrosine phosphorylation and nuclear translocation of STATs, but was needed for binding of transcriptional complexes with ISG promoters and, thereby, for maximal transcription activation. pp32 was found to be associated with ISG promoters in IFN-untreated cells, and its binding amount fluctuated as a function of time after IFN treatment. short interfering RNA (siRNA)-mediated knockdown of pp32 expression reduced the histone acetylation level on ISG promoters, suggesting that pp32 plays a role in ISG transcription by a function other than that of INHAT. Taking these findings together, we propose that pp32 is involved in the formation of ISG transcription initiation complexes, possibly as their recruiter. [ABSTRACT FROM AUTHOR]

Published

2011

14. Functional characterization and efficient detection of Nucleophosmin/NPM1 oligomers.

Author

Lin, Jianhuang, Hisaoka, Miharu, Nagata, Kyosuke, and Okuwaki, Mitsuru

Subjects

*NUCLEOPHOSMIN, *CELL culture, *OLIGOMERIZATION, *RENILLA luciferase, *BIOLUMINESCENCE

Abstract

NPM1/nucleophosmin is a multifunctional and oligomeric phosphoprotein. A number of observations have suggested that changes in the oligomer formation of NPM1 could influence its biological functions, especially its oncogenic functions. To understand the functional meaning of oligomerization of NPM1/nucleophosmin, we have established a novel method to monitor protein oligomerization in cells. We utilized the split synthetic Renilla luciferase protein fragment-assisted complementation (SRL-PFAC) bioluminescence activity and observed the change of NPM1 oligomer levels under various cell culture conditions. Our study provides a method for systematic characterization of NPM1 oligomer formation changes and for screening inhibitors of NPM1 oligomerization. [ABSTRACT FROM AUTHOR]

Published

2016

15. Imaging analysis of nuclear antiviral factors through direct detection of incoming adenovirus genome complexes.

Author

Komatsu, Tetsuro, Will, Hans, Nagata, Kyosuke, and Wodrich, Harald

Subjects

*ANTIVIRAL agents, *ADENOVIRUSES, *DEFENSE reaction (Physiology), *NUCLEAR DNA, *VIRUS diseases, *IMAGE analysis

Abstract

Recent studies involving several viral systems have highlighted the importance of cellular intrinsic defense mechanisms through nuclear antiviral proteins that restrict viral propagation. These factors include among others components of PML nuclear bodies, the nuclear DNA sensor IFI16, and a potential restriction factor PHF13/SPOC1. For several nuclear replicating DNA viruses, it was shown that these factors sense and target viral genomes immediately upon nuclear import. In contrast to the anticipated view, we recently found that incoming adenoviral genomes are not targeted by PML nuclear bodies. Here we further explored cellular responses against adenoviral infection by focusing on specific conditions as well as additional nuclear antiviral factors. In line with our previous findings, we show that neither interferon treatment nor the use of specific isoforms of PML nuclear body components results in co-localization between incoming adenoviral genomes and the subnuclear domains. Furthermore, our imaging analyses indicated that neither IFI16 nor PHF13/SPOC1 are likely to target incoming adenoviral genomes. Thus our findings suggest that incoming adenoviral genomes may be able to escape from a large repertoire of nuclear antiviral mechanisms, providing a rationale for the efficient initiation of lytic replication cycle. [ABSTRACT FROM AUTHOR]

Published

2016

16. Glucocorticoids facilitate the transcription from the human cytomegalovirus major immediate early promoter in glucocorticoid receptor- and nuclear factor-I-like protein-dependent manner.

Author

Inoue-Toyoda, Maki, Kato, Kohsuke, Nagata, Kyosuke, and Yoshikawa, Hiroyuki

Subjects

*GLUCOCORTICOID receptors, *TRANSCRIPTION factors, *CYTOMEGALOVIRUSES, *PROMOTERS (Genetics), *NUCLEAR factor of activated T-cells, *DEXAMETHASONE

Abstract

Human cytomegalovirus (HCMV) is a common and usually asymptomatic virus agent in healthy individuals. Initiation of HCMV productive infection depends on expression of the major immediate early (MIE) genes. The transcription of HCMV MIE genes is regulated by a diverse set of transcription factors. It was previously reported that productive HCMV infection is triggered probably by elevation of the plasma hydroxycorticoid level. However, it is poorly understood whether the transcription of MIE genes is directly regulated by glucocorticoid. Here, we found that the dexamethasone (DEX), a synthetic glucocorticoid, facilitates the transcription of HCMV MIE genes through the MIE promoter and enhancer in a glucocorticoid receptor (GR)-dependent manner. By competitive EMSA and reporter assays, we revealed that an NF-I like protein is involved in DEX-mediated transcriptional activation of the MIE promoter. Thus, this study supports a notion that the increased level of hydroxycorticoid in the third trimester of pregnancy reactivates HCMV virus production from the latent state. [ABSTRACT FROM AUTHOR]

Published

2015

17. Identification of a Novel and Unique Transcription Factor in the Intraerythrocytic Stage of Plasmodium falciparum.

Author

Komaki-Yasuda, Kanako, Okuwaki, Mitsuru, Nagata, Kyosuke, Kawazu, Shin-ichiro, and Kano, Shigeyuki

Subjects

*TRANSCRIPTION factors, *PLASMODIUM falciparum, *GENE expression, *LUCIFERASES, *CHROMATOGRAPHIC analysis, *RNA, *TROPHOZOITES

Abstract

The mechanisms of stage-specific gene regulation in the malaria parasite Plasmodium falciparum are largely unclear, with only a small number of specific regulatory transcription factors (AP2 family) having been identified. In particular, the transcription factors that function in the intraerythrocytic stage remain to be elucidated. Previously, as a model case for stage-specific transcription in the P. falciparum intraerythrocytic stage, we analyzed the transcriptional regulation of pf1-cys-prx, a trophozoite/schizont-specific gene, and suggested that some nuclear factors bind specifically to the cis-element of pf1-cys-prx and enhance transcription. In the present study, we purified nuclear factors from parasite nuclear extract by 5 steps of chromatography, and identified a factor termed PREBP. PREBP is not included in the AP2 family, and is a novel protein with four K-homology (KH) domains. The KH domain is known to be found in RNA-binding or single-stranded DNA-binding proteins. PREBP is well conserved in Plasmodium species and partially conserved in phylum Apicomplexa. To evaluate the effects of PREBP overexpression, we used a transient overexpression and luciferase assay combined approach. Overexpression of PREBP markedly enhanced luciferase expression under the control of the pf1-cys-prx cis-element. These results provide the first evidence of a novel transcription factor that activates the gene expression in the malaria parasite intraerythrocytic stage. These findings enhance our understanding of the evolution of specific transcription machinery in Plasmodium and other eukaryotes. [ABSTRACT FROM AUTHOR]

Published

2013

18. Tamiflu-Resistant but HA-Mediated Cell-to-Cell Transmission through Apical Membranes of Cell-Associated Influenza Viruses.

Author

Mori, Kotaro, Haruyama, Takahiro, and Nagata, Kyosuke

Subjects

*INFLUENZA viruses, *NEURAMINIDASE, *PROTEASE inhibitors, *ION channels, *ENDOSOMES, *VIRUS disease transmission

Abstract

The infection of viruses to a neighboring cell is considered to be beneficial in terms of evasion from host anti-virus defense systems. There are two pathways for viral infection to ''right next door'': one is the virus transmission through cell-cell fusion by forming syncytium without production of progeny virions, and the other is mediated by virions without virus diffusion, generally designated cell-to-cell transmission. Influenza viruses are believed to be transmitted as cell-free virus from infected cells to uninfected cells. Here, we demonstrated that influenza virus can utilize cell-to-cell transmission pathway through apical membranes, by handover of virions on the surface of an infected cell to adjacent host cells. Live cell imaging techniques showed that a recombinant influenza virus, in which the neuraminidase gene was replaced with the green fluorescence protein gene, spreads from an infected cell to adjacent cells forming infected cell clusters. This type of virus spreading requires HA activation by protease treatment. The cell-to-cell transmission was also blocked by amantadine, which inhibits the acidification of endosomes required for uncoating of influenza virus particles in endosomes, indicating that functional hemagglutinin and endosome acidification by M2 ion channel were essential for the cell-to-cell influenza virus transmission. Furthermore, in the cell-to-cell transmission of influenza virus, progeny virions could remain associated with the surface of infected cell even after budding, for the progeny virions to be passed on to adjacent uninfected cells. The evidence that cell-to-cell transmission occurs in influenza virus lead to the caution that local infection proceeds even when treated with neuraminidase inhibitors. [ABSTRACT FROM AUTHOR]

Published

2011

19. Role of Template Activating Factor-I as a chaperone in linker histone dynamics.

Author

Kato, Kohsuke, Okuwaki, Mitsuru, and Nagata, Kyosuke

Subjects

*MOLECULAR chaperones, *HISTONES, *CHROMATIN, *SOMATIC cells, *CHROMOSOMAL proteins

Abstract

Linker histone H1 is a fundamental chromosomal protein involved in the maintenance of higher-ordered chromatin organization. The exchange dynamics of histone H1 correlates well with chromatin plasticity. A variety of core histone chaperones involved in core histone dynamics has been identified, but the identity of the linker histone chaperone in the somatic cell nucleus has been a longstanding unanswered question. Here we show that Template Activating Factor-I (TAF-I, also known as protein SET) is involved in histone H1 dynamics as a linker histone chaperone. Among previously identified core histone chaperones and linker histone chaperone candidates, only TAF-I was found to be associated specifically with histone H1 in mammalian somatic cell nuclei. TAF-I showed linker histone chaperone activity in vitro. Fluorescence recovery after photobleaching analyses revealed that TAF-I is involved in the regulation of histone H1 dynamics in the nucleus. Therefore, we propose that TAF-I is a key molecule that regulates linker histone-mediated chromatin assembly and disassembly. [ABSTRACT FROM AUTHOR]

Published

2011

20. RAG-dependent recombination at cryptic RSSs within TEL–AML1 t(12;21)(p13;q22) chromosomal translocation region

Author

Numata, Masashi, Saito, Shoko, and Nagata, Kyosuke

Subjects

*CHROMOSOMAL translocation, *CHROMOSOMES, *ENDONUCLEASES, *NUCLEOTIDE sequence, *PROTEINS, *IMMUNOGLOBULINS, *T cell receptors

Abstract

Abstract: The recombination activating gene (RAG) is a lymphoid-specific endonuclease involved in the V(D)J recombination. It has long been proposed that mis-targeting of RAG proteins is one of the factors contributing to lymphoid chromosomal translocation bearing authentic recombination signal sequences (RSSs) in immunoglobulin (Ig) and T cell receptor (TCR) gene loci or cryptic RSSs (cRSSs). However, it is unclear whether primary sequence-dependent targeting mistake involved in the chromosomal translocation bearing no Ig/TCR gene loci is mediated by RAG proteins. Using an extrachromosomal recombination assay, we found RAG-dependent recombination in the regions dense in breakpoints within TEL and AML1 gene loci related to acute lymphoid leukemia-associated t(12;21)(p13;q22) chromosomal translocation. Sequence analyses revealed several heptamer-like sequences located in the vicinity of RAG-dependent recombination sites. By chromatin immunoprecipitation (ChIP) and ligation-mediated PCR (LM-PCR) assays, we have shown that RAG proteins bind to and cleave the TEL translocation region dense in breakpoints. These results suggest that mis-targeting of RAG proteins to cRSSs within TEL and AML1 translocation regions might be responsible for the t(12;21)(p13;q22) chromosomal translocation not bearing Ig/TCR regions. [ABSTRACT FROM AUTHOR]

Published

2010

21. Development of tetraphenylethylene-based fluorescent oligosaccharide probes for detection of influenza virus

Author

Kato, Tomohisa, Kawaguchi, Atsushi, Nagata, Kyosuke, and Hatanaka, Kenichi

Subjects

*BIOSENSORS, *INFLUENZA viruses, *STYRENE, *OLIGOSACCHARIDES, *FLUORESCENT probes, *ALKYNES, *LIGANDS (Biochemistry), *DETECTION of microorganisms

Abstract

Abstract: Tetraphenylethylene (TPE) derivatives have strong fluorescence in aggregated state. We designed and synthesized a tetraphenylethylene derivative bearing alkyne groups which were used for combination by click chemistry. The new TPE compound bearing alkyne groups was used to synthesize fluorescence oligosaccharide probes which have lactosyl and 6′-sialyllactosyl moieties as ligands. We found that the TPE compounds bearing lactosyl and 6′-sialyllactosyl moieties were useful for detection of RCA120 and SSA lectins, respectively. Moreover, we have shown that TPE-based fluorescent oligosaccharide probe bearing 6′-sialyllactose moiety can be utilized as a “turn-on” fluorescent sensor for detection of influenza virus. [Copyright &y& Elsevier]

Published

2010

22. Functional characterization of human nucleosome assembly protein 1-like proteins as histone chaperones.

Author

Okuwaki, Mitsuru, Kato, Kohsuke, and Nagata, Kyosuke

Subjects

*MOLECULAR chaperones, *HISTONES, *NUCLEOPROTEINS, *CYTOPLASM, *DIMERS

Abstract

Nucleosome Assembly Protein 1 (NAP1) is a highly conserved histone chaperone protein suspected to be involved in the dynamical regulation of the histone H2A-H2B hetero-dimer. However, the exact mechanism by which NAP1-like proteins act is currently unknown. In this work, we characterized the biochemical properties of two human NAP1-like proteins, hNAP1L1 and hNAP1L4, including a previously uncharacterized subtype, with the aim of determining their exact mechanistic role. Both hNAP1L1 and hNAP1L4 were found to be localized mainly to the cytoplasm and a minor population of them was suggested to be in the nucleus. Biochemical analyses demonstrated that both hNAP1L1 and hNAP1L4 mediated nucleosome formation. In addition, hNAP1L1 was shown to possess a significantly greater nucleosome disassembly activity than hNAP1L4, suggesting that hNAP1L1 and hNAP1L4 may play distinct roles in the regulation of histone dynamics. Building upon this initial discovery we also found that histone H2A-H2B and various histone H2A variants-H2B dimers were found to associate with both hNAP1L1 and hNAP1L4 in cell extracts. These results suggest that human NAP1-like proteins play overlapping roles in transport and deposition of histone H2A-H2B or H2A variants-H2B dimers on chromatin and nonoverlapping roles in nucleosome disassembly. [ABSTRACT FROM AUTHOR]

Published

2010

23. Previously Unrecognized Amino Acid Substitutions in the Hemagglutinin and Fusion Proteins of Measles Virus Modulate Cell-Cell Fusion, Hemadsorption, Virus Growth, and Penetration Rate.

Author

Okada, Hiromi, Itoh, Masae, Nagata, Kyosuke, and Takeuchi, Kaoru

Subjects

*MEASLES virus, *MORBILLIVIRUSES, *PROTEINS, *BIOMOLECULES, *VIRUSES, *AMINO acids, *NUCLEOTIDE sequence

Abstract

Wild-type measles virus (MV) isolated in B95a cells could be adapted to Vero cells after several blind passages. In this study, we have determined the complete nucleotide sequences of the genomes of the wild type (T11wild) and its Vero cell-adapted (T11Ve-23) MV strain and identified amino acid substitutions R516G, E271K, D439E and G464W (D439E/G464W), N481Y/H495R, and Y187H/L204F in the nucleocapsid, V, fusion (F), hemagglutinin (H), and large proteins, respectively. Expression of mutated H and F proteins from cDNA revealed that the H495R substitution, in addition to N481Y, in the H protein was necessary for the wild-type H protein to use CD46 efficiently as a receptor and that the G464W substitution in the F protein was important for enhanced cell-cell fusion. Recombinant wild-type MV strains harboring the F protein with the mutations D439E/G464W [F(D439E/G464W)] and/or H(N481Y/H495R) protein revealed that both mutated F and H proteins were required for efficient syncytium formation and virus growth in Vero cells. Interestingly, a recombinant wild-type MV strain harboring the H(N481Y/H495R) protein penetrated slowly into Vero cells, while a recombinant wild-type MV strain harboring both the F(D439E/G464W) and H(N481Y/H495R) proteins penetrated efficiently into Vero cells, indicating that the F(D439E/G464W) protein compensates for the inefficient penetration of a wild-type MV strain harboring the H(N481Y/H495R) protein. Thus, the F and H proteins synergistically function to ensure efficient wild-type MV growth in Vero cells. [ABSTRACT FROM AUTHOR]

Published

2009

24. Sp1-mediated transcription regulation of TAF-Iα gene encoding a histone chaperone

Author

Asaka, Masamitsu N., Murano, Kensaku, and Nagata, Kyosuke

Subjects

*GENETIC transcription, *GENETIC code, *HISTONES, *TRANSCRIPTION factors

Abstract

Abstract: TAF-I, one of histone chaperones, consists of two subtypes, TAF-Iα and TAF-Iβ. The histone chaperone activity of TAF-I is regulated by dimer patterns of these subtypes. TAF-Iβ is expressed ubiquitously, while the expression level of TAF-Iα with less activity than TAF-Iβ differs among cell types. It is, therefore, assumed that the expression level of TAF-Iα in a cell is important for the TAF-I activity level. Here, we found that TAF-Iα and TAF-Iβ genes are under the control of distinct promoters. Reporter assays and gel shift assays demonstrated that Sp1 binds to three regions in the TAF-Iα promoter and two or all mutaions of the three Sp1 binding regions reduced the TAF-Iα promoter activity. ChIP assays demonstrated that Sp1 binds to the TAF-Iα promoter in vivo. Furthermore, the expression level of TAF-Iα mRNA was reduced by knockdown of Sp1 using siRNA method. These studies indicated that the TAF-Iα promoter is under the control of Sp1. [Copyright &y& Elsevier]

Published

2008

25. Involvement of Influenza Virus PA Subunit in Assembly of Functional RNA Polymerase Complexes.

Author

Kawaguchi, Atsushi, Naito, Tadasuke, and Nagata, Kyosuke

Subjects

*INFLUENZA viruses, *RNA polymerases, *RNA, *RESPIRATORY infections, *TRANSFERASES, *MESSENGER RNA, *AMINO acids, *VIROLOGY, *RECOMBINANT viruses

Abstract

The RNA-dependent RNA polymerase of influenza virus consists of three subunits, PB1, PB2, and PA, and synthesizes three kinds of viral RNAs, vRNA, cRNA, and mRNA. PB1 is a catalytic subunit; PB2 recognizes the cap structure for generation of the primer for transcription; and PA is thought to be involved in viral RNA replication. However, the process of polymerase complex assembly and the exact nature of polymerase complexes involved in synthesis of the three different RNA species are not yet clear, ts53 virus is a temperature-sensitive (ts) mutant derived from A/WSN/33 (A. Sugiura, M. Ueda, K. Tobita, and C. Enomoto, Virology 65:363-373, 1975). We confirmed that the mRNA synthesis level of ts53 remains unaffected at the nonpermissive temperature, whereas vRNA synthesis is largely reduced. Sequencing of the gene encoding ts53 PA and recombinant virus rescue experiments revealed that an amino acid change from Leu to Pro at amino acid position 226 is causative of temperature sensitivity. By glycerol density gradient analyses of nuclear extracts prepared from wild-type virus-infected cells, we found that polymerase proteins sediment in three fractions: one (H fraction) consists of RNP complexes, another (M fraction) contains active polymerases but not viral RNA, and the other (L fraction) contains inactive forms of polymerases. Pulse-chase experiments showed that polymerases in the L fraction are converted to those in the M fraction. In ts53-infected cells, polymerases accumulated in the L fraction. These results strongly suggest that PA is involved in the assembly of functional viral RNA polymerase complexes from their inactive intermediates. [ABSTRACT FROM AUTHOR]

Published

2005

26. SET‐NUP214 and MLL cooperatively regulate the promoter activity of the HoxA10 gene.

Author

Cigdem, Sadik, Saito, Shoko, Nishikata, Daiki, Nagata, Kyosuke, and Okuwaki, Mitsuru

Subjects

*GENE fusion, *LYMPHOBLASTIC leukemia, *PROMOTERS (Genetics), *GENES, *ACUTE leukemia

Abstract

SET‐Nup214 is a recurrent fusion gene that is mainly observed in T‐cell acute lymphoblastic leukemia (T‐ALL). Dysregulation of homeobox (Hox) genes is frequently observed in patients with leukemia. Consistent with this, HoxA genes are upregulated in the SET‐Nup214+ T‐ALL cell line and patients. Although SET‐Nup214 has been reported to be recruited to the promoter regions of HoxA genes, the detailed mechanisms of how SET‐Nup214 specifically binds to HoxA gene promoters and regulates HoxA gene expression are not known. In this study, we demonstrated that SET‐Nup214 interacts with MLL via the SET acidic region of SET‐Nup214. SET‐Nup214 and MLL cooperatively enhance the promoter activity of the HoxA10 gene. Neither the SET region alone nor the Nup214 region alone sufficiently enhanced the HoxA10 gene promoter. Our results indicated that the SET portion of the SET‐Nup214‐fusion protein is important for interactions with MLL and transcription enhancement of the HoxA10 gene. Thus, our study will contribute to the understanding of how SET‐Nup214 and MLL disturb the expression of HoxA10 gene in leukemia. [ABSTRACT FROM AUTHOR]

Published

2021

27. RNA-recognition motifs and glycine and arginine-rich region cooperatively regulate the nucleolar localization of nucleolin.

Author

Okuwaki, Mitsuru, Saotome-Nakamura, Ai, Yoshimura, Masashi, Saito, Shoko, Hirawake-Mogi, Hiroko, Sekiya, Takeshi, and Nagata, Kyosuke

Subjects

*NUCLEAR proteins, *NUCLEOLIN, *MUTANT proteins, *GLYCINE, *RIBOSOMAL RNA, *CLARITHROMYCIN, *NUCLEOPHOSMIN

Abstract

Nucleolin (NCL) is a nucleolar protein i.e. involved in the regulation of the nucleolar structure and functions, and consists of three distinct regions: the N-terminal region; the middle region, which contains four RNA-recognition motifs (RRMs); and the C-terminal glycine- and arginine-rich (GAR) region. The primary function of the RRMs and GAR is thought to be specific RNA binding. However, it is not well understood how these RNA-binding regions of NCL separately or cooperatively regulate its nucleolar localization and functions. To address this issue, we constructed mutant proteins carrying point mutations at the four RRMs individually or deletion of the C-terminal GAR region. We found that the GAR deletion and the mutations in the fourth RRM (RRM4) decreased the nucleolar localization of NCL. Biochemical analyses showed that NCL interacted directly with ribosomal RNAs (rRNAs) and G-rich oligonucleotides, and that this interaction was decreased by mutations at RRM1 and RRM4 and GAR deletion. Although GAR deletion decreased the rRNA-binding activity of NCL, the mutant was efficiently coprecipitated with rRNAs and nucleolar proteins from cell extracts. These contradictory results suggest that NCL stably localizes to the nucleoli via the interactions with rRNAs and nucleolar proteins via GAR, RRM1 and RRM4. [ABSTRACT FROM AUTHOR]

Published

2021

28. Jdp2-deficient granule cell progenitors in the cerebellum are resistant to ROS-mediated apoptosis through xCT/Slc7a11 activation.

Author

Ku, Chia-Chen, Wuputra, Kenly, Kato, Kohsuke, Lin, Wen-Hsin, Pan, Jia-Bin, Tsai, Shih-Chieh, Kuo, Che-Jung, Lee, Kan-Hung, Lee, Yan-Liang, Lin, Ying-Chu, Saito, Shigeo, Noguchi, Michiya, Nakamura, Yukio, Miyoshi, Hiroyuki, Eckner, Richard, Nagata, Kyosuke, Wu, Deng-Chyang, Lin, Chang-Shen, and Yokoyama, Kazunari K.

Subjects

*GRANULE cells, *CEREBELLUM, *APOPTOSIS, *GLUTAMIC acid, *AMINO acids

Abstract

The Jun dimerization protein 2 (Jdp2) is expressed predominantly in granule cell progenitors (GCPs) in the cerebellum, as was shown in Jdp2-promoter-Cre transgenic mice. Cerebellum of Jdp2-knockout (KO) mice contains lower number of Atoh-1 positive GCPs than WT. Primary cultures of GCPs from Jdp2-KO mice at postnatal day 5 were more resistant to apoptosis than GCPs from wild-type mice. In Jdp2-KO GCPs, the levels of both the glutamate‒cystine exchanger Sc7a11 and glutathione were increased; by contrast, the activity of reactive oxygen species (ROS) was decreased; these changes confer resistance to ROS-mediated apoptosis. In the absence of Jdp2, a complex of the cyclin-dependent kinase inhibitor 1 (p21Cip1) and Nrf2 bound to antioxidant response elements of the Slc7a11 promoter and provide redox control to block ROS-mediated apoptosis. These findings suggest that an interplay between Jdp2, Nrf2, and p21Cip1 regulates the GCP apoptosis, which is one of critical events for normal development of the cerebellum. [ABSTRACT FROM AUTHOR]

Published

2020

29. Formation of adenovirus DNA replication compartments and viral DNA accumulation sites by host chromatin regulatory proteins including NPM1.

Author

Genoveso, Michelle Jane, Hisaoka, Miharu, Komatsu, Tetsuro, Wodrich, Harald, Nagata, Kyosuke, and Okuwaki, Mitsuru

Subjects

*VIRAL proteins, *CELL nuclei, *VIRAL genomes, *DNA, *NUCLEOLIN, *NUCLEOPHOSMIN, *DNA replication

Abstract

The adenovirus (Ad) genome is believed to be packaged into the virion by forming a chromatin‐like structure. The replicated viral genome is likely to be condensed through binding with viral core proteins before encapsidation. Replicated viral genomes accumulate in the central region of the nucleus, which we termed virus‐induced postreplication (ViPR) body. However, the molecular mechanism by which the nuclear structure is reorganized and its functional significance in virus production are currently not understood. In this study, we found that viral packaging protein IVa2, but not capsid proteins, accumulated in the ViPR body. In addition, nucleolar chromatin regulatory proteins, nucleophosmin 1 (NPM1), upstream binding factor, and nucleolin accumulated in the ViPR body in late‐stage Ad infection. NPM1 depletion increased the nuclease‐resistant viral genome and delayed the ViPR body formation. These results suggested that structural changes in the infected cell nucleus depend on the formation of viral chromatin by host chromatin regulatory proteins. Because NPM1 depletion decreases production of the infectious virion, we propose that host factor‐mediated viral chromatin remodeling and concomitant ViPR body formation are prerequisites for efficient encapsidation of Ad chromatin. [ABSTRACT FROM AUTHOR]

Published

2020

30. Function of Nup98 subtypes and their fusion proteins, Nup98-TopIIβ and Nup98-SETBP1 in nuclear-cytoplasmic transport.

Author

Saito, Shoko, Yokokawa, Takafumi, Iizuka, Gemmei, Cigdem, Sadik, Okuwaki, Mitsuru, and Nagata, Kyosuke

Subjects

*NUCLEAR pore complex, *CHIMERIC proteins, *NEOPLASTIC cell transformation, *CELL migration, *CHROMOSOMAL translocation, *HEMATOLOGIC malignancies

Abstract

Nup98 is a component of the nuclear pore complex. The nup98 -fusion genes derived by chromosome translocations are involved in hematopoietic malignancies. Here, we investigated the functions of Nup98 isoforms and two unexamined Nup98-fusion proteins, Nup98-TopIIβ and Nup98-SETBP1. We first demonstrated that two Nup98 isoforms are expressed in various mouse tissues and similarly localized in the nucleus and the nuclear envelope. We also showed that Nup98-TopIIβ and Nup98-SETBP1 are localized in the nucleus and partially co-localized with full-length Nup98 and a nuclear export receptor XPO1. We demonstrated that Nup98-TopIIβ and Nup98-SETBP1 negatively regulate the XPO1-mediated protein export. Our results will contribute to the understanding of the molecular mechanism by which the Nup98-fusion proteins induce tumorigenesis. [ABSTRACT FROM AUTHOR]

Published

2017

31. Replication-Coupled and Host Factor-Mediated Encapsidation of the Influenza Virus Genome by Viral Nucleoprotein.

Author

Kawaguchi, Atsushi, Momose, Fumitaka, and Nagata, Kyosuke

Subjects

*INFLUENZA viruses, *NUCLEOPROTEINS, *CELLULAR mechanics, *RNA polymerases, *MOLECULAR chaperones

Abstract

The influenza virus RNA-dependent RNA polymerase is capable of initiating replication but mainly catalyzes abortive RNA synthesis in the absence of viral and host regulatory factors. Previously, we reported that IREF-1/minichromosome maintenance (MCM) complex stimulates a de novo initiated replication reaction by stabilizing an initiated replication complex through scaffolding between the viral polymerase and nascent cRNA to which MCM binds. In addition, several lines of genetic and biochemical evidence suggest that viral nucleoprotein (NP) is involved in successful replication. Here, using cell-free systems, we have shown the precise stimulatory mechanism of virus genome replication by NP. Stepwise cell-free replication reactions revealed that exogenously added NP free of RNA activates the viral polymerase during promoter escape while it is incapable of encapsidating the nascent cRNA. However, we found that a previously identified cellular protein, RAF-2p48/NPI-5/UAP56, facilitates replication reaction-coupled encapsidation as an NP molecular chaperone. These findings demonstrate that replication of the virus genome is followed by its encapsidation by NP in collaboration with its chaperone. [ABSTRACT FROM AUTHOR]

Published

2011

32. Tracking adenovirus genomes identifies morphologically distinct late DNA replication compartments.

Author

Komatsu, Tetsuro, Robinson, Derrick R., Hisaoka, Miharu, Ueshima, Shuhei, Okuwaki, Mitsuru, Nagata, Kyosuke, and Wodrich, Harald

Subjects

*ADENOVIRUSES, *VIRAL genomes, *DNA replication, *CHROMATIN, *CELL morphology, *NUCLEOSIDES

Abstract

In adenoviral virions, the genome is organized into a chromatin-like structure by viral basic core proteins. Consequently viral DNAs must be replicated, chromatinized and packed into progeny virions in infected cells. Although viral DNA replication centers can be visualized by virtue of viral and cellular factors, the spatiotemporal regulation of viral genomes during subsequent steps remains to be elucidated. In this study, we used imaging analyses to examine the fate of adenoviral genomes and to track newly replicated viral DNA as well as replication-related factors. We show de novo formation of a subnuclear domain, which we termed Virus-induced Post-Replication ( ViPR) body, that emerges concomitantly with or immediately after disintegration of initial replication centers. Using a nucleoside analogue, we show that viral genomes continue being synthesized in morphologically distinct replication compartments at the periphery of ViPR bodies and are then transported inward. In addition, we identified a nucleolar protein Mybbp1a as a molecular marker for ViPR bodies, which specifically associated with viral core protein VII. In conclusion, our work demonstrates the formation of previously uncharacterized viral DNA replication compartments specific for late phases of infection that produce progeny viral genomes accumulating in ViPR bodies. [ABSTRACT FROM AUTHOR]

Published

2016

33. C-terminal acidic domain of histone chaperone human NAP1 is an efficient binding assistant for histone H2A-H2B, but not H3-H4.

Author

Ohtomo, Hideaki, Akashi, Satoko, Moriwaki, Yoshihito, Okuwaki, Mitsuru, Osakabe, Akihisa, Nagata, Kyosuke, Kurumizaka, Hitoshi, and Nishimura, Yoshifumi

Subjects

*CHROMATIN, *MOLECULAR chaperones, *C-terminal binding proteins, *DIMERS, *CALORIMETRY

Abstract

Nucleosome assembly protein 1 ( NAP1) binds both the (H3-H4)2 tetramer and two H2A-H2B dimers, mediating their sequential deposition on DNA. NAP1 contains a C-terminal acidic domain ( CTAD) and a core domain that promotes dimer formation. Here, we have investigated the roles of the core domain and CTAD of human NAP1 in binding to H2A-H2B and H3-H4 by isothermal calorimetry and native mass spectrometry and compared them with the roles of yeast NAP1. We show that the hNAP1 and yNAP1 dimers bind H2A-H2B by two different modes: a strong endothermic interaction and a weak exothermic interaction. A mutant hNAP1, but not yNAP1, dimer lacking CTAD loses the exothermic interaction and shows greatly reduced H2A-H2B binding activity. The isolated CTAD of hNAP1 binds H2A-H2B only exothermically with relatively stronger binding as compared with the exothermic interaction observed for the full-length hNAP1 dimer. Thus, the two CTADs in the hNAP1 dimer seem to provide binding assistance for the strong endothermic interaction of the core domain with H2A-H2B. By contrast, in the relatively weaker binding of hNAP1 to H3-H4 as compared with yNAP1, CTAD of hNAP1 has no significant role. To our knowledge, this is the first distinct role identified for the hNAP1 CTAD. [ABSTRACT FROM AUTHOR]

Published

2016

34. Influenza Virus Induces Cholesterol-Enriched Endocytic Recycling Compartments for Budozone Formation via Cell Cycle-Independent Centrosome Maturation.

Author

Kawaguchi, Atsushi, Hirohama, Mikako, Harada, Yoshimi, Osari, Suguru, and Nagata, Kyosuke

Subjects

*INFLUENZA viruses, *CELL cycle, *BIOLOGICAL rhythms, *CELL membranes, *CELL envelope (Biology), *CENTROSOMES

Abstract

Influenza virus particles are assembled at the plasma membrane in concert with incorporation of the virus genome, but the details of its spatio-temporal regulation are not understood. Here we showed that influenza virus infection induces the assembly of pericentrosomal endocytic recycling compartment (ERC) through the activation of Rab11a GTPase and cell cycle-independent maturation of centrosome by YB-1, a multifunctional protein that is involved in mitotic division, RNA metabolism and tumorigenesis. YB-1 is recruited to the centrosome in infected cells and is required for anchoring microtubules to the centrosome. We also found that viral infection accumulates cholesterol in ERC and is dependent on YB-1. Depletion of YB-1 shows reduced cholesterol-enriched ERC and prevented budozone formation at the plasma membrane. These results suggest that cholesterol in recycling endosomes, which are emanated from ERC, may trigger the virus assembly concomitantly with the packaging of the virus genome. We propose that the virus genome is transported to the plasma membrane by cholesterol-enriched recycling endosomes through cell cycle-independent activation of the centrosome by YB-1. [ABSTRACT FROM AUTHOR]

Published

2015

35. A Method for Visualization of Incoming Adenovirus Chromatin Complexes in Fixed and Living Cells.

Author

Komatsu, Tetsuro, Dacheux, Denis, Kreppel, Florian, Nagata, Kyosuke, and Wodrich, Harald

Subjects

*VISUALIZATION, *ADENOVIRUSES, *CHROMATIN, *COMPLEX compounds, *SPATIO-temporal variation

Abstract

Inside the adenovirus virion, the genome forms a chromatin-like structure with viral basic core proteins. Core protein VII is the major DNA binding protein and was shown to remain associated with viral genomes upon virus entry even after nuclear delivery. It has been suggested that protein VII plays a regulatory role in viral gene expression and is a functional component of viral chromatin complexes in host cells. As such, protein VII could be used as a maker to track adenoviral chromatin complexes in vivo. In this study, we characterize a new monoclonal antibody against protein VII that stains incoming viral chromatin complexes following nuclear import. Furthermore, we describe the development of a novel imaging system that uses Template Activating Factor-I (TAF-I/SET), a cellular chromatin protein tightly bound to protein VII upon infection. This setup allows us not only to rapidly visualize protein VII foci in fixed cells but also to monitor their movement in living cells. These powerful tools can provide novel insights into the spatio-temporal regulation of incoming adenoviral chromatin complexes. [ABSTRACT FROM AUTHOR]

Published

2015

36. Substrate binding activates the designed triple mutant of the colicin E7 metallonuclease.

Author

Németh, Eszter, Körtvélyesi, Tamás, Kožíšek, Milan, Thulstrup, Peter, Christensen, Hans, Asaka, Masamitsu, Nagata, Kyosuke, and Gyurcsik, Béla

Subjects

*BINDING sites, *GENETIC mutation, *COLICINS, *NUCLEASES, *CATALYTIC activity, *GEL electrophoresis, *CIRCULAR dichroism

Abstract

The nuclease domain of colicin E7 (NColE7) cleaves DNA nonspecifically. The active center is a Zn-containing HNH motif at the C-terminus. The N-terminal loop is essential for the catalytic activity providing opportunity for allosteric modulation of the enzyme. To identify the key residues responsible for the structural integrity of NColE7, a virtual alanine scan was performed on a semiempirical quantum chemical level within the 25 residue long N-terminal sequence (446-470). Based on the calculations the T454A/K458A/W464A-NColE7 triple mutant (TKW) was expressed and purified. According to the agarose gel electrophoresis experiments and linear dichroism spectra the catalytic activity of the TKW mutant decreased in comparison with wild-type NColE7. The distorted structure and weakened Zn binding may account for this as revealed by circular dichroism spectra, mass spectrometry, fluorescence-based thermal analysis and isothermal microcalorimetric titrations. Remarkably, the substrate induced the folding of the mutant protein. [ABSTRACT FROM AUTHOR]

Published

2014

37. Reconstitution of human rRNA gene transcription in mouse cells by a complete SL1 complex.

Author

Murano, Kensaku, Okuwaki, Mitsuru, Momose, Fumitaka, Kumakura, Michiko, Ueshima, Shuhei, Newbold, Robert F., and Nagata, Kyosuke

Subjects

*RIBOSOMAL RNA, *RNA polymerases, *REPORTER genes, *MESSENGER RNA

Abstract

An important characteristic of the transcription of a ribosomal RNA gene (rDNA) mediated by DNA-dependent RNA polymerase (Pol) I is its stringent species specificity. SL1/TIF-IB is a key complex for species specificity, but its functional complex has not been reconstituted. Here, we established a novel and highly sensitive monitoring system for Pol I transcription to reconstitute the SL1 activity in which a transcript harboring a reporter gene synthesized by Pol I is amplified and converted into translatable mRNA by the influenza virus RNA-dependent RNA polymerase. Using this monitoring system, we reconstituted Pol I transcription from the human rDNA promoter in mouse cells by expressing four human TATA-binding protein (TBP)-associated factors (TAF[sub I]s) in the SL1 complex. The reconstituted SL1 also re-activated human rDNA transcription in mouse A9 cells carrying an inactive human chromosome 21 that contains the rDNA cluster. Chimeric SL1 complexes containing human and mouse TAF[sub I]s could be formed, but these complexes were inactive for human rDNA transcription. We conclude that four human TAF[sub I]s are necessary and sufficient to overcome the barrier of species specificity for human rDNA transcription in mouse cells. [ABSTRACT FROM AUTHOR]

Published

2014

38. Long Noncoding RNA NEAT1-Dependent SFPQ Relocation from Promoter Region to Paraspeckle Mediates IL8 Expression upon Immune Stimuli.

Author

Imamura, Katsutoshi, Imamachi, Naoto, Akizuki, Gen, Kumakura, Michiko, Kawaguchi, Atsushi, Nagata, Kyosuke, Kato, Akihisa, Kawaguchi, Yasushi, Sato, Hiroki, Yoneda, Misako, Kai, Chieko, Yada, Tetsushi, Suzuki, Yutaka, Yamada, Toshimichi, Ozawa, Takeaki, Kaneki, Kiyomi, Inoue, Tsuyoshi, Kobayashi, Mika, Kodama, Tatsuhiko, and Wada, Youichiro

Subjects

*NON-coding RNA, *GENE expression, *GENETIC engineering, *PROLINE, *INTERLEUKIN-8, *TOLL-like receptors, *GENETIC transcription, *IMMUNE response

Abstract

Summary: Although thousands of long noncoding RNAs (lncRNAs) are localized in the nucleus, only a few dozen have been functionally characterized. Here we show that nuclear enriched abundant transcript 1 (NEAT1), an essential lncRNA for the formation of nuclear body paraspeckles, is induced by influenza virus and herpes simplex virus infection as well as by Toll-like receptor3-p38 pathway-triggered poly I:C stimulation, resulting in excess formation of paraspeckles. We found that NEAT1 facilitates the expression of antiviral genes including cytokines such as interleukin-8 (IL8). We found that splicing factor proline/glutamine-rich (SFPQ), a NEAT1-binding paraspeckle protein, is a repressor of IL8 transcription, and that NEAT1 induction relocates SFPQ from the IL8 promoter to the paraspeckles, leading to transcriptional activation of IL8. Together, our data show that NEAT1 plays an important role in the innate immune response through the transcriptional regulation of antiviral genes by the stimulus-responsive cooperative action of NEAT1 and SFPQ. [ABSTRACT FROM AUTHOR]

Published

2014

39. Involvement of the N-terminal portion of influenza virus RNA polymerase subunit PB1 in nucleotide recognition.

Author

Binh, Nguyen Trong, Wakai, Chitose, Kawaguchi, Atsushi, and Nagata, Kyosuke

Subjects

*N-terminal residues, *INFLUENZA viruses, *VIRAL genomes, *RNA polymerases, *NUCLEOTIDES, *RIBAVIRIN, *DRUG resistance

Abstract

Highlights: [•] Isolation of a ribavirin-resistant influenza virus polymerase. [•] Asp27-to-Asn mutation of PB1 contributes to the ribavirin resistance. [•] Asp27 of PB1 is involved in the nucleotide recognition. [ABSTRACT FROM AUTHOR]

Published

2014

40. Crystallization and preliminary crystallographic analysis of an Escherichia coli-selected mutant of the nuclease domain of the metallonuclease colicin E7.

Author

Czene, Anikó, Tóth, Eszter, Gyurcsik, Béla, Otten, Harm, Poulsen, Jens-Christian N., Lo Leggio, Leila, Larsen, Sine, Christensen, Hans E. M., and Nagata, Kyosuke

Subjects

*CRYSTALLIZATION, *BACTERIAL genetics, *ESCHERICHIA coli, *NUCLEASES, *BACTERIOPHAGES, *ALLOSTERIC regulation, *CATALYTIC activity

Abstract

The metallonuclease colicin E7 is a member of the HNH family of endonucleases. It serves as a bacterial toxin in Escherichia coli, protecting the host cell from other related bacteria and bacteriophages by degradation of their chromosomal DNA under environmental stress. Its cell-killing activity is attributed to the nonspecific nuclease domain (NColE7), which possesses the catalytic ββα-type metal ion-binding HNH motif at its C-terminus. Mutations affecting the positively charged amino acids at the N-terminus of NColE7 (444-576) surprisingly showed no or significantly reduced endonuclease activity [Czene et al. (2013), J. Biol. Inorg. Chem. 18, 309-321]. The necessity of the N-terminal amino acids for the function of the C-terminal catalytic centre poses the possibility of allosteric activation within the enzyme. Precise knowledge of the intramolecular interactions of these residues that affect the catalytic activity could turn NColE7 into a novel platform for artificial nuclease design. In this study, the N-terminal deletion mutant ΔN4-NColE7-C* of the nuclease domain of colicin E7 selected by E. coli was overexpressed and crystallized at room temperature by the sitting-drop vapour-diffusion method. X-ray diffraction data were collected to 1.6 Å resolution and could be indexed and averaged in the trigonal space group P3121 or P3221, with unit-cell parameters a = b = 55.4, c = 73.1 Å. Structure determination by molecular replacement is in progress. [ABSTRACT FROM AUTHOR]

Published

2013

41. The role of the N-terminal loop in the function of the colicin E7 nuclease domain.

Author

Czene, Anikó, Németh, Eszter, Zóka, István, Jakab-Simon, Noémi, Körtvélyesi, Tamás, Nagata, Kyosuke, Christensen, Hans, and Gyurcsik, Béla

Subjects

*COLICINS, *NUCLEASES, *ESCHERICHIA coli toxins, *METAL ions, *MASS spectrometry, *QUANTUM chemistry, *GENE expression in bacteria

Abstract

Colicin E7 (ColE7) is a metallonuclease toxin of Escherichia coli belonging to the HNH superfamily of nucleases. It contains highly conserved amino acids in its HHXNXHXH ββα-type metal ion binding C-terminal active centre. However, the proximity of the arginine at the N-terminus of the nuclease domain of ColE7 (NColE7, 446-576) is necessary for the hydrolytic activity. This poses a possibility of allosteric activation control in this protein. To obtain more information on this phenomenon, two protein mutants were expressed, i.e. four and 25 N-terminal amino acids were removed from NColE7. The effect of the N-terminal truncation on the Zn ion and DNA binding as well as on the activity was investigated in this study by mass spectrometry, synchrotron-radiation circular dichroism and fluorescence spectroscopy and agarose gel mobility shift assays. The dynamics of protein backbone movement was simulated by molecular dynamics. Semiempirical quantum chemical calculations were performed to obtain better insight into the structure of the active centre. The longer protein interacted with both Zn ion and DNA more strongly than its shorter counterpart. The results were explained by the structural stabilization effect of the N-terminal amino acids on the catalytic centre. In agreement with this, the absence of the N-terminal sequences resulted in significantly increased movement of the backbone atoms compared with that in the native NColE7: in ΔN25-NColE7 the amino acid strings between residues 485-487, 511-515 and 570-571, and in ΔN4-NColE7 those between residues 467-468, 530-535 and 570-571. [ABSTRACT FROM AUTHOR]

Published

2013

42. YB-1 Functions as a Porter To Lead Influenza Virus Ribonucleoprotein Complexes to Microtubules.

Author

Kawaguchi, Atsushi, Matsumoto, Ken, and Nagata, Kyosuke

Subjects

*CARRIER proteins, *INFLUENZA viruses, *NUCLEOPROTEINS, *MICROTUBULES, *RIBONUCLEASES, *CYTOPLASM, *CELL membranes, *CELLULAR signal transduction

Abstract

De novo-synthesized RNAs are under the regulation of multiple posttranscriptional processes by a variety of RNA-binding proteins. The influenza virus genome consists of single-stranded RNAs and exists as viral ribonucleoprotein (vRNP) complexes. After the replication of vRNP in the nucleus, it is exported to the cytoplasm and then reaches the budding site beneath the cell surface in a process mediated by Rab11a-positive recycling endosomes along microtubules. However, the regulatory mechanisms of the postreplicational processes of vRNP are largely unknown. Here we identified, as a novel vRNP-interacting protein, Y-box-binding protein 1 (YB-1), a cellular protein that is involved in regulation of cellular transcription and translation. YB-1 translocated to the nucleus from the cytoplasm and accumulated in PML nuclear bodies in response to influenza virus infection. vRNP assembled into the exporting complexes with YB-1 at PML nuclear bodies. After nuclear export, using YB-1 knockdown cells and in vitro reconstituted systems, YB-1 was shown to be required for the interaction of vRNP exported from the nucleus with microtubules around the microtubule-organizing center (MTOC), where Rab11a-positive recycling endosomes were located. Further, we also found that YB-1 overexpression stimulates the production of progeny virions in an Rab11a-dependent manner. Taking these findings together, we propose that YB-1 is a porter that leads vRNP to microtubules from the nucleus and puts it into the vesicular trafficking system. [ABSTRACT FROM AUTHOR]

Published

2012

43. Critical Role of an Antiviral Stress Granule Containing RIG-I and PKR in Viral Detection and Innate Immunity.

Author

Onomoto, Koji, Jogi, Michihiko, Yoo, Ji-Seung, Narita, Ryo, Morimoto, Shiho, Takemura, Azumi, Sambhara, Suryaprakash, Kawaguchi, Atushi, Osari, Suguru, Nagata, Kyosuke, Matsumiya, Tomoh, Namiki, Hideo, Yoneyama, Mitsutoshi, Fujita, Takashi, and Kanai, Akio

Subjects

*TRETINOIN, *RNA, *INTERFERON inducers, *VIRUS diseases, *IMMUNOHISTOCHEMISTRY, *MORPHOLOGY, *GENE transfection

Abstract

Retinoic acid inducible gene I (RIG-I)-like receptors (RLRs) function as cytoplasmic sensors for viral RNA to initiate antiviral responses including type I interferon (IFN) production. It has been unclear how RIG-I encounters and senses viral RNA. To address this issue, we examined intracellular localization of RIG-I in response to viral infection using newly generated anti- RIG-I antibody. Immunohistochemical analysis revealed that RLRs localized in virus- induced granules containing stress granule (SG) markers together with viral RNA and antiviral proteins. Because of similarity in morphology and components, we termed these aggregates antiviral stress granules (avSGs). Influenza A virus (IAV) deficient in non-structural protein 1 (NS1) efficiently generated avSGs as well as IFN, however IAV encoding NS1 produced little. Inhibition of avSGs formation by removal of either the SG component or double-stranded RNA (dsRNA)- dependent protein kinase (PKR) resulted in diminished IFN production and concomitant enhancement of viral replication. Furthermore, we observed that transfection of dsRNA resulted in IFN production in an avSGs-dependent manner. These results strongly suggest that the avSG is the locus for non-self RNA sensing and the orchestration of multiple proteins is critical in the triggering of antiviral responses. [ABSTRACT FROM AUTHOR]

Published

2012

44. Structure-based discovery of anti-influenza virus A compounds among medicines

Author

Fukuoka, Mayuko, Minakuchi, Moeko, Kawaguchi, Atsushi, Nagata, Kyosuke, Kamatari, Yuji O., and Kuwata, Kazuo

Subjects

*INFLUENZA A virus, *ANTI-infective agents, *PANDEMICS, *INFLUENZA prevention, *DRUG resistance in microorganisms, *ANIMAL models in research, *SURFACE plasmon resonance

Abstract

Abstract: Background: Influenza A virus (IAV) infection is nowadays a major public health concern, in particular since the 2009 H1N1 flu pandemic. The outbreak of IAV strains resistant to currently available drugs, such as oseltamivir or zanamivir targeting the neuraminidase, is a real threat for humans as well as for animals. Thus the development of anti-IAV drugs with a novel action mechanism may be an urgent theme. Methods: We performed a docking simulation targeting the interface of PA interacting with PB1 using a drug database including ~4000 compounds. We then conducted cell viability assay and plaque assay using IAV/WSN/33. Finally we examined their anti-IAV mechanism by surface plasmon resonance and IAV replicon assay. Results: We found that benzbromarone, diclazuril, and trenbolone acetate had strong anti-IAV activities. We confirmed that benzbromarone and diclazuril bound with PA subunit, and decreased the transcriptional activity of the viral RNA polymerase. Conclusions: Benzbromarone and diclazuril had strong anti-IAV activities with novel action mechanism, i.e. inhibition of viral RNA polymerase. General significance: Since benzbromarone and diclazuril are already used in public as medicines, these could be the candidates for alternatives in case of an outbreak of IAV which is resistant to pre-existing anti-IAV drugs. [Copyright &y& Elsevier]

Published

2012

45. Immobilization of fluorous oligosaccharide recognized by influenza virus on polytetrafluoroethylene filter

Author

Tojino, Mami, Mori, Masako, Kasuya, Maria Carmelita Z., Hatanaka, Kenichi, Kawaguchi, Atsushi, Nagata, Kyosuke, Shirai, Takashi, and Mizuno, Mamoru

Subjects

*POLYTEF, *OLIGOSACCHARIDES, *INFLUENZA viruses, *POLYETHYLENE glycol, *CELL culture, *GANGLIOSIDES, *CELL communication, *MEMBRANE proteins

Abstract

Abstract: The lactoside with PEG-fluorous tag was introduced to BHK-21(C-13) cells to generate a GM3-type oligosaccharide (Siaα2-3Galβ1-4Glc). The GM3-type oligosaccharide obtained was easily immobilized by spotting onto commercially available polytetrafluoroethylene (PTFE) filter through non-covalent fluorous affinity and simply assessed by dot blot method using the interaction of carbohydrate- with proteins which recognize sialic acid such as virus membrane proteins. [Copyright &y& Elsevier]

Published

2012

46. Apical Transport of Influenza A Virus Ribonucleoprotein Requires Rab11-positive Recycling Endosome.

Author

Momose, Fumitaka, Sekimoto, Tetsuya, Ohkura, Takashi, Jo, Shuichi, Kawaguchi, Atsushi, Nagata, Kyosuke, and Morikawa1, Yuko

Subjects

*NUCLEOPROTEINS, *INFLUENZA A virus, *ENDOSOMES, *APICAL dominance (Plant physiology), *RNA viruses, *RNA polymerase regulation, *FLUORESCENT antibody technique, *G proteins

Abstract

Influenza A virus RNA genome exists as eight-segmented ribonucleoprotein complexes containing viral RNA polymerase and nucleoprotein (vRNPs). Packaging of vRNPs and virus budding take place at the apical plasma membrane (APM). However, little is known about the molecular mechanisms of apical transport of newly synthesized vRNP. Transfection of fluorescent-labeled antibody and subsequent live cell imaging revealed that punctate vRNP signals moved along microtubules rapidly but intermittently in both directions, suggestive of vesicle trafficking. Using a series of Rab family protein, we demonstrated that progeny vRNP localized to recycling endosome (RE) in an active/GTP-bound Rab11- dependent manner. The vRNP interacted with Rab11 through viral RNA polymerase. The localization of vRNP to RE and subsequent accumulation to the APM were impaired by overexpression of Rab binding domains (RBD) of Rab11 family interacting proteins (Rab11-FIPs). Similarly, no APM accumulation was observed by overexpression of class II Rab11-FIP mutants lacking RBD. These results suggest that the progeny vRNP makes use of Rab11-dependent RE machinery for APM trafficking. [ABSTRACT FROM AUTHOR]

Published

2011

47. Crucial role of the influenza virus NS2 (NEP) C-terminal domain in M1 binding and nuclear export of vRNP

Author

Shimizu, Teppei, Takizawa, Naoki, Watanabe, Ken, Nagata, Kyosuke, and Kobayashi, Nobuyuki

Subjects

*INFLUENZA viruses, *NUCLEOPROTEINS, *CARRIER proteins, *POLYPEPTIDES, *CYTOPLASM, *MATURATION (Psychology)

Abstract

Abstract: The influenza virus genome replicates in the host cell nucleus, and the progeny viral ribonucleoproteins (vRNPs) are exported to the cytoplasm prior to maturation. The influenza virus NS2 protein has a nuclear export signal (NES) and binds to M1. It is therefore postulated that vRNP is exported from the nucleus by binding to NS2 through M1. However, the significance of the association between NS2 and M1 for the nuclear export of vRNP is still poorly understood. We herein demonstrate that the C-terminal domain of NS2 (residues 81–100) is essential for M1 binding and the nuclear export of progeny vRNPs. Structured summary: MINT-8057301, MINT-8057317: NS2 (uniprotkb:P03508) binds (MI:0407) to M1 (uniprotkb:P03485) by pull down (MI:0096) [ABSTRACT FROM AUTHOR]

Published

2011

48. Involvement of vesicular trafficking system in membrane targeting of the progeny influenza virus genome

Author

Jo, Shuichi, Kawaguchi, Atsushi, Takizawa, Naoki, Morikawa, Yuko, Momose, Fumitaka, and Nagata, Kyosuke

Subjects

*VIRAL genetics, *INFLUENZA viruses, *GENOMES, *BIOLOGICAL transport, *MESSENGER RNA, *CELL membranes, *DIAGNOSTIC use of fluorescence in situ hybridization, *VIRAL envelopes, *MEMBRANE proteins

Abstract

Abstract: The genome of influenza type A virus consists of single-stranded RNAs of negative polarity. Progeny viral RNA (vRNA) replicated in the nucleus is nuclear-exported, and finally transported to the budding site beneath the plasma membrane. However, the precise process of the membrane targeting of vRNA is unclear, although viral proteins and cytoskeleton are thought to play roles. Here, we have visualized the translocation process of progeny vRNA using fluorescence in situ hybridization method. Our results provide an evidence of the involvement of vesicular trafficking in membrane targeting of progeny vRNA independent of that of viral membrane proteins. [ABSTRACT FROM AUTHOR]

Published

2010

49. Sorting of influenza A virus RNA genome segments after nuclear export

Author

Takizawa, Naoki, Kumakura, Michiko, Takeuchi, Kaoru, Kobayashi, Nobuyuki, and Nagata, Kyosuke

Subjects

*INFLUENZA A virus, *RNA, *CYTOPLASM, *BIOMARKERS, *CELL fusion, *VIRAL genomes

Abstract

Abstract: The genome of the influenza A virus consists of eight different segments. These eight segments are thought to be sorted selectively in infected cells. However, the cellular compartment where segments are sorted is not known. We examined using temperature sensitive (ts) mutant viruses and cell fusion where segments are sorted in infected cells. Different cells were infected with different ts mutant viruses, and these cells were fused. In fused cells, genome segments are mixed only in the cytoplasm, because M1 prevents their re-import into the nucleus. We made a marker ts53 virus, which has silent mutations in given segments and determined the reassortment frequency on all segments using ts1 and marker ts53. In both co-infected and fused cells, all of marker ts53 segments and ts1 segments were incorporated into progeny virions in a random fashion. These results suggest that influenza virus genome segments are sorted after nuclear export. [Copyright &y& Elsevier]

Published

2010

50. Amino acid substitution at position 464 in the haemagglutinin-neuraminidase protein of a mumps virus Urabe strain enhanced the virus growth in neuroblastoma SH-SY5Y cells

Author

Ninomiya, Kengo, Kanayama, Tetsuya, Fujieda, Nao, Nakayama, Tetsuo, Komase, Katsuhiro, Nagata, Kyosuke, and Takeuchi, Kaoru

Subjects

*HEMAGGLUTININ, *THERAPEUTIC use of amino acids, *NEURAMINIDASE, *MUMPS, *NEUROBLASTOMA, *CANCER cells, *DNA replication, *MENINGITIS, CENTRAL nervous system infections

Abstract

Abstract: Mumps virus (MuV) infects various organs including central nervous system (CNS). However, the molecular basis of the neural cell specificity of MuV is not well understood. We found that the Hoshino vaccine strain rescued from cDNA replicated moderately in neuroblastoma SH-SY5Y cell line, while an Urabe strain (Ur89-250) isolated from a post-vaccination aseptic meningitis case replicated efficiently in the same cells. In order to examine the contribution of individual genes of Ur89-250 to the growth in SH-SY5Y cells, recombinant Hoshino vaccine strains in which each gene(s) was replaced with corresponding gene(s) of Ur89-250 were generated. A recombinant virus possessing the small hydrophobic and haemagglutinin-neuraminidase (HN) genes of Ur89-250 grew as efficiently in SH-SY5Y cells as Ur89-250. Further analysis indicated that an amino acid substitution at position 464 in the HN protein was most important for efficient growth. Thus, single amino acid substitution in the HN protein could affect neural cell specificity of mumps virus. [Copyright &y& Elsevier]

Published

2009