Your search keyword '"Seiji Hongo"' showing total 7 results

1. Stability of the seven hexon hypervariable region sequences of adenovirus types 1–6 isolated in Yamagata, Japan between 1988 and 2007

Author

Seiji Hongo, Hidekazu Nishimura, Noriko Katsushima, Hitoshi Oshitani, Tadayuki Ahiko, Akira Suzuki, Yuki Furuse, Katsumi Mizuta, Hirokazu Kimura, Michiko Okamoto, Akira Ohmi, Tsutomu Itagaki, Masahiro Noda, and Yoko Matsuzaki

Subjects

Serotype, Cancer Research, Sequence analysis, Molecular Sequence Data, Biology, Adenoviridae, Cell Line, Adenovirus Infections, Human, Japan, Phylogenetics, Virology, Genetic variation, Humans, Amino Acid Sequence, Child, Peptide sequence, Gene, Phylogeny, Genetics, Phylogenetic tree, Genetic Variation, Sequence Analysis, DNA, Hypervariable region, Infectious Diseases, DNA, Viral, Capsid Proteins

Abstract

Seven hexon hypervariable regions (HVRs) of adenoviruses (Ads) were identified by comparing the regions among different serotypes; however, no one has compared HVR sequences among the identical serotypes, except for adenovirus type 3 (Ad3). To examine a variability between the HVRs for each serotype, we compared the sequences of Ad1-6 isolates, respectively, isolated between 1988 and 2007 in Yamagata, Japan. We selected 23-43 isolates randomly and sequenced 894-987 bp regions. Except for strains with insertions and deletions, the sequence identities among Ad1-6 were 99-100%, excluding that between the two Ad5 groups (approx. 94%). Even the insertions and deletions were likely to be established, as these changes were repeatedly observed. The obtained phylogenetic tree indicated that Ad isolates and reference strains branched depending on serotype. The Yamagata isolates had similar sequences or amino acid arrangements to the reference strains as well as to other strains isolated in different areas. HVRs have been stably conserved as serotype-specific regions for a long period with only minor genomic variations. Therefore, we herein recommend that these regions be hereafter referred to as "serotype-specific regions", which might be a more appropriate title with which to characterize the epidemiological nature of these sites than the current "HVRs".

Published

2009

2. Location of a linear epitope recognized by monoclonal antibody S16 on the hemagglutinin-esterase glycoprotein of influenza C virus

Author

Emi Takashita, Seiji Hongo, Kanetsu Sugawara, Kiyoto Nakamura, Fumio Kitame, Yoko Matsuzaki, and Yasushi Muraki

Subjects

Cancer Research, Influenzavirus C, medicine.drug_class, Antigens, Polyomavirus Transforming, Genetic Vectors, Gene Expression, Hemagglutinins, Viral, Chick Embryo, Simian virus 40, Cross Reactions, Antibodies, Viral, Monoclonal antibody, Virus, Epitope, Cell Line, Virology, Chlorocebus aethiops, medicine, Animals, Peptide sequence, Glycoproteins, Recombination, Genetic, Linear epitope, Hemagglutinin esterase, biology, Antibodies, Monoclonal, Molecular biology, Infectious Diseases, Mutagenesis, COS Cells, biology.protein, Epitopes, B-Lymphocyte, Antibody, Influenza C Virus, Viral Fusion Proteins, Epitope Mapping

Abstract

We reported previously that monoclonal antibody S16, which had been raised against the hemagglutinin-esterase (HE) glycoprotein of influenza C/Ann Arbor/1/50 (AA/50) virus, recognizes a linear epitope present on the HE molecules of all influenza C viruses examined except for viruses belonging to a lineage represented by Aichi/1/81 (AI/81). Comparison of the deduced amino acid sequence of HE between viruses on the AI/81-related lineage and those on the others suggests that the epitope recognized by S16 is located in a region containing amino acid residue 403 and that a change from Glu to Lys at this position causes the loss of reactivity with the antibody. To prove it, the wild type (WT) HEs of AA/50 and AI/81 as well as their mutants with an amino acid substitution at residue 403 were expressed in CV-1 cells from the recombinant simian virus 40 (SV40) and tested for reactivity with S16 by immunoprecipitation. The results showed that the AA/50 virus WT and AI/81 virus mutant HEs (both having Glu at residue 403) were reactive with S16 whereas the AI/81 virus WT and AA/50 virus mutant HEs (both having Lys at residue 403) were not. Furthermore, we examined the reactivity of S16 with two synthetic peptides (corresponding to residues 397–409) that possess Glu and Lys at position 403, respectively, by enzyme-linked immunosorbent assays. The results demonstrated that the former peptide but not the latter was reactive with S16. These observations support strongly the notion described above. During this study it was also found that S16 cross-reacts with large T antigen of SV40.

Published

1999

3. Phosphorylation of influenza C virus CM2 protein

Author

Yoko Matsuzaki, Seiji Hongo, Yuichiro Tada, Kanetsu Sugawara, Fumio Kitame, Yasushi Muraki, and Kiyoto Nakamura

Subjects

inorganic chemicals, Cancer Research, Influenzavirus C, Golgi Apparatus, Oligosaccharides, Chick Embryo, macromolecular substances, Biology, Endoplasmic Reticulum, environment and public health, Phosphoamino acid analysis, Viral Matrix Proteins, Serine, chemistry.chemical_compound, symbols.namesake, Virology, Tumor Cells, Cultured, Animals, Humans, Protein phosphorylation, Phosphorylation, Endoplasmic reticulum, Virion, Biological Transport, Tunicamycin, Brefeldin A, Golgi apparatus, enzymes and coenzymes (carbohydrates), Infectious Diseases, chemistry, Biochemistry, symbols, bacteria, Protein Processing, Post-Translational

Abstract

Labeling of influenza C virus-infected HMV-II cells with [32P]orthophosphate showed that the CM2 protein is posttranslationally modified by phosphorylation. The unglycosylated form of CM2 synthesized in the presence of tunicamycin was found to be highly phosphorylated. This result, together with the finding that digestion of CM2 with peptide-N-glycosidase F failed to remove the 32P label from the glycosylated form of CM2, indicated that phosphorylation occurs in the polypeptide backbone and not in the oligosaccharide chain. Furthermore, phosphoamino acid analysis revealed that phosphorylation occurs exclusively on serine residues. Treatment of infected cells with brefeldin A resulted in a complete inhibition of phosphorylation, showing that phosphorylation of CM2 occurs after its migration from the endoplasmic reticulum to the Golgi apparatus. Phosphorylation of CM2 was also inhibited strongly, although not completely, by monensin treatment, suggesting that CM2 is phosphorylated predominantly after its movement from medial to trans Golgi cisternae. Finally, we found that the CM2 protein incorporated into the progeny virion is phosphorylated, which indicates that there is no strictly selective incorporation of the unphosphorylated form of CM2 into the virion.

Published

1998

4. Interspecies transmission of influenza C virus between humans and pigs

Author

Hiroshi Kimura, Yoshio Numazaki, Gao Peng, Yasushi Muraki, Kanetsu Sugawara, Hiroshi Suzuki, Seiji Hongo, Chieko Abiko, Katsumi Mizuta, Fumio Kitame, and Kiyoto Nakamura

Subjects

Cancer Research, Influenzavirus C, Swine, Molecular Sequence Data, Hemagglutinins, Viral, Biology, Virus, Interspecies transmission, Viral Proteins, Species Specificity, Antigen, Virology, Influenza, Human, Animals, Humans, Antigens, Viral, Phylogeny, Glycoproteins, chemistry.chemical_classification, Base Sequence, Molecular epidemiology, Antigenic analysis, Infectious Diseases, chemistry, DNA, Viral, RNA, Viral, Influenza C Virus, Glycoprotein, Viral Fusion Proteins

Abstract

The antigenic and genetic characteristics of the 18 human strains of influenza C virus isolated in Yamagata and Sendai Cities, Japan between January 1991 and February 1993 were investigated. Antigenic analysis with monoclonal antibodies to the hemagglutinin-esterase glycoprotein showed that the isolates could be divided into three distinct groups closely related to C/Yamagata/26/81, C/Aichi/1/81 and C/Mississippi/80, respectively. T1-oligonucleotide fingerprinting of total vRNA revealed that the six isolates belonging to the C.Yamagata/26/81 virus group had the genomes greatly similar to one another but considerably different from those of the 1988/1990 isolates (except C/Yamagata/10/89) of the same antigenic group. Comparison of total or partial nucleotide sequences of the seven RNA segments of the three strains (C/Miyagi/3/91, C/Miyagi/9/91 and C/Miyagi/2/92) representative of the 1991/1993 strains of the C/Yamagata/26/81 virus group with those of the previous influenza C isolates obtained from humans and pigs during 1980/1989 showed that the 1991/1993 strains, like C/Yamagata/10/89, are more closely related to viruses isolated from pigs in Beijing, China in 1981/1982 than to any of the isolates from humans. This observation suggests strongly that interspecies transmission of influenza C virus between humans and pigs has occurred in nature, although it is not known whether the virus has been transmitted from pigs to humans or from humans to pigs.

Published

1997

5. Comparison of receptor-binding properties among influenza C virus isolates

Author

Yasushi Muraki, Masami Matsuzaki, Yoko Matsuzaki, Fumio Kitame, Seiji Hongo, Kiyoto Nakamura, and Kanetsu Sugawara

Subjects

Cancer Research, Erythrocytes, Influenzavirus C, Hemagglutinins, Viral, Biology, Receptor binding site, Mice, Structure-Activity Relationship, Viral Proteins, Virology, Animals, Humans, Amino Acids, Peptide sequence, Glycoproteins, chemistry.chemical_classification, Hemagglutinin esterase, Hemagglutination, Molecular biology, Amino acid, Agglutination (biology), Titer, Infectious Diseases, chemistry, Receptors, Virus, Influenza C Virus, Chickens, Viral Fusion Proteins

Abstract

A total of 10 influenza C virus strains isolated recently in Yamagata City, Japan and shown to belong to the same lineage was compared for the ability to agglutinate chicken and mouse erythrocytes under various conditions. C/Yamagata/10/89 was unique in lacking the ability to agglutinate chicken erythrocytes at a temperatureor = 4 degrees C. This isolate also agglutinated native mouse erythrocytes only very inefficiently, although the high agglutination titer was obtained with the glutaraldehyde-fixed cells. Furthermore, it was found that C/Yamagata/4/88, unlike the other isolates, agglutinated erythrocytes from chickens to lower titers than those from mice, even when assayed at 0 degree C. Comparison of the deduced amino acid sequence of hemagglutinin-esterase among the 6 representative strains including two older isolates, C/Yamagata/26/81 and C/Nara/2/85, suggested that the failures of C/Yamagata/10/89 to agglutinate chicken erythrocytes ator = 4 degrees C and unfixed mouse erythrocytes to high titers may be due to amino acid changes at residues 337 (Glu--Lys) and 340 (Thr--Tyr), respectively, and that a change at residue 347 (Leu--Ser) may be responsible for the decreased ability of C/Yamagata/4/88 to agglutinate chicken erythrocytes.

Published

1995

6. Palmitoylation of CM2 is dispensable to influenza C virus replication

Author

Seiji Hongo, Yoko Matsuzaki, Kanetsu Sugawara, Takako Okuwa, Yasushi Muraki, Yoshiro Ohara, Takatoshi Furukawa, and Toshiki Himeda

Subjects

Cancer Research, Influenzavirus C, viruses, Eggs, Lipoylation, Biology, Virus Replication, Virus, Viral Matrix Proteins, Viral Proteins, Palmitoylation, Virology, Cell Line, Tumor, Animals, Humans, Recombination, Genetic, Viral matrix protein, Infectious Diseases, Viral replication, Membrane protein, Cell culture, RNA, Viral, Influenza C Virus, Chickens

Abstract

CM2 is the second membrane protein of influenza C virus. The significance of the posttranslational modifications of CM2 remains to be clarified in the context of viral replication, although the positions of the modified amino acids on CM2 have been determined. In the present study, using reverse genetics we generated rCM2-C65A, a recombinant influenza C virus lacking CM2 palmitoylation site, in which cysteine at residue 65 of CM2 was mutated to alanine, and examined viral growth and viral protein synthesis in the recombinant-infected cells. The rCM2-C65A virus grew as efficiently as did the parental virus in cultured HMV-II cells as well as in embryonated chicken eggs. The synthesis and biochemical features of HEF, NP, M1 and mutant CM2 in the rCM2-C65A-infected HMV-II cells were similar to those in the parental virus-infected cells. Furthermore, membrane flotation analysis of the infected cells revealed that equal amount of viral proteins was recovered in the plasma membrane fractions of the rCM2-C65A-infected cells to that in the parental virus-infected cells. These findings indicate that defect in palmitoylation of CM2 does not affect transport and maturation of HEF, NP and M1 as well as CM2 in virus-infected cells, and palmitoylation of CM2 is dispensable to influenza C virus replication.

Published

2010

7. Conformational maturation of the nucleoprotein synthesized in influenza C virus-infected cells

Author

Emi Takashita, Yasushi Muraki, Kanetsu Sugawara, Yoko Matsuzaki, and Seiji Hongo

Subjects

Cancer Research, Influenzavirus C, medicine.drug_class, Protein Conformation, Biology, Monoclonal antibody, Antibodies, Viral, Cell Line, Epitopes, Viral Proteins, Dogs, Antigen, Virology, Complementary DNA, Chlorocebus aethiops, medicine, Centrifugation, Density Gradient, Animals, Nucleocapsid, Cell Nucleus, Viral matrix protein, Linear epitope, Antibodies, Monoclonal, Molecular biology, Nucleoprotein, Protein Transport, Infectious Diseases, Nucleoproteins, Influenza C Virus, Protein Processing, Post-Translational, Conformational epitope, Protein Binding

Abstract

The conformational maturation of the influenza C virus nucleoprotein (NP) synthesized in infected cells was investigated. Monoclonal antibodies (mAbs) that have previously been characterized [Sugawara, K., Nishimura, H., Hongo, S., Kitame, F., Nakamura, K., 1991. Antigenic characterization of the nucleoprotein and matrix protein of influenza C virus with monoclonal antibodies. J. Gen. Virol. 72, 103-109] enabled this molecular maturation to be detected. Both pulse-labeled and chased NPs could equally retain high reactivity with H31 mAb recognizing a linear epitope on the NP molecule. However, pulse-labeled NP showed three- to four-fold lower reactivity with H27 mAb recognizing a conformational epitope, compared to chased NP. Sedimentation analyses by sucrose gradient centrifugation revealed that the mature NP could readily participate in nucleocapsid formation while the immature NP was free. The immature NP was rapidly transported into the nucleus and its maturation seemed to occur after or during translocation into the nucleus. A single expression of NP cDNA in COS-1 cells demonstrated that the NP maturation was an intrinsic feature of the NP molecule without relation to other viral components.

Published

2006