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1. Genetic Reassortment in a Child Coinfected with Two Influenza B Viruses, B/Yamagata Lineage and B/Victoria-Lineage Strains.

Author

Matsuzaki, Yoko, Sugawara, Kanetsu, Kidoguchi, Yuko, Kadowaki, Yoko, Shimotai, Yoshitaka, Katsushima, Yuriko, Katsushima, Fumio, Tanaka, Shizuka, Matoba, Yohei, Komabayashi, Kenichi, Aoki, Yoko, and Mizuta, Katsumi

Subjects
*INFLUENZA viruses, *INFLUENZA B virus, *GENETIC variation
Abstract

We identified a child coinfected with influenza B viruses of B/Yamagata and B/Victoria lineages, in whom we analyzed the occurrence of genetic reassortment. Plaque purification was performed using a throat swab specimen from a 9-year-old child, resulting in 34 well-isolated plaques. The genomic composition of eight gene segments (HA, NA, PB1, PB2, PA, NP, M, and NS genes) for each plaque was determined at the lineage level. Of the 34 plaques, 21 (61.8%) had B/Phuket/3073/2013 (B/Yamagata)-like sequences in all gene segments, while the other 13 (38.2%) were reassortants with B/Texas/02/2013 (B/Victoria)-like sequences in 1–5 of the 8 segments. The PB1 segment had the most B/Victoria lineage genes (23.5%; 8 of 34 plaques), while PB2 and PA had the least (2.9%; 1 of 34 plaques). Reassortants with B/Victoria lineage genes in 2–5 segments showed the same level of growth as viruses with B/Yamagata lineage genes in all segments. However, reassortants with B/Victoria lineage genes only in the NA, PB1, NP, or NS segments exhibited reduced or undetectable growth. We demonstrated that various gene reassortments occurred in a child. These results suggest that simultaneous outbreaks of two influenza B virus lineages increase genetic diversity and could promote the emergence of new epidemic strains. [ABSTRACT FROM AUTHOR]

Published
2024
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6. A two-year survey of the oseltamivir-resistant influenza A(H1N1) virus in Yamagata, Japan and the clinical effectiveness of oseltamivir and zanamivir

Author

Itagaki Tsutomu, Takashita Emi, Sugawara Kanetsu, Sanjoh Kanako, Abiko Chieko, Suto Asuka, Aoki Yoko, Mizuta Katsumi, Matsuzaki Yoko, Katsushima Yuriko, Ujike Makoto, Obuchi Masatsugu, Odagiri Takato, and Tashiro Masato

Subjects
Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background Oseltamivir is the preferred antiviral drug for influenza, but oseltamivir-resistant A(H1N1) viruses have circulated worldwide since the 2007-2008 influenza season. We aimed to determine the rate of oseltamivir resistance among A(H1N1) isolates from Yamagata, Japan, to compare the virological characteristics between isolates from the 2007-2008 and 2008-2009 seasons, and to evaluate the clinical effectiveness of oseltamivir. Results Oseltamivir resistance, determined by detecting the H275Y mutation in the neuraminidase (NA) gene, was observed in 2.5% (2 of 79) and 100% (77 of 77) of isolates from the 2007-2008 and 2008-2009 seasons, respectively. Antigenic analysis suggested that antigenically different variants of A(H1N1) viruses circulated in the 2008-2009 season. Growth testing demonstrated that the ability of the 2008-2009 isolates to replicate in MDCK cells was similar to those of the oseltamivir-susceptible isolates from the 2007-2008 season. A phylogenetic analysis revealed that two oseltamivir-resistant viruses isolated in the 2007-2008 season were closely related to other oseltamivir-susceptible viruses in Yamagata but were different from oseltamivir-resistant viruses isolated in Europe and North America in the 2007-2008 season. The oseltamivir-resistant viruses isolated in Japan in the 2008-2009 season were phylogenetically similar to oseltamivir-resistant isolates from Europe and North America during the 2007-2008 season. Furthermore, the median duration of fever after the start of oseltamivir treatment was significantly longer in oseltamivir-resistant cases (2 days; range 1-6 days) than in oseltamivir-susceptible cases (1.5 days: range 1-2 days) (P = 0.0356). Conclusion Oseltamivir-resistant A(H1N1) isolates from Yamagata in the 2007-2008 season might have acquired resistance through the use of oseltamivir, and the 2008-2009 oseltamivir-resistant isolates might have been introduced into Japan and circulated throughout the country. Influenza surveillance to monitor oseltamivir-resistance would aid clinicians in determining an effective antiviral treatment strategy.

Published
2010
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9. Development of a high-throughput assay to detect antibody inhibition of low pH induced conformational changes of influenza virus hemagglutinin

Author

Trost, Jessica F., primary, LeMasters, Elizabeth H., additional, Liu, Feng, additional, Carney, Paul, additional, Lu, Xiuhua, additional, Sugawara, Kanetsu, additional, Hongo, Seiji, additional, Stevens, James, additional, Steinhauer, David A., additional, Tumpey, Terrence, additional, Katz, Jacqueline M., additional, Levine, Min Z., additional, and Li, Zhu-Nan, additional

Published
2018
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13. Epitope Mapping of the Hemagglutinin Molecule of A/(H1N1)pdm09 Influenza Virus by Using Monoclonal Antibody Escape Mutants

Author

Matsuzaki, Yoko, primary, Sugawara, Kanetsu, additional, Nakauchi, Mina, additional, Takahashi, Yoshimasa, additional, Onodera, Taishi, additional, Tsunetsugu-Yokota, Yasuko, additional, Matsumura, Takayuki, additional, Ato, Manabu, additional, Kobayashi, Kazuo, additional, Shimotai, Yoshitaka, additional, Mizuta, Katsumi, additional, Hongo, Seiji, additional, Tashiro, Masato, additional, and Nobusawa, Eri, additional

Published
2014
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16. A two-year survey of the oseltamivir-resistant influenza A(H1N1) virus in Yamagata, Japan and the clinical effectiveness of oseltamivir and zanamivir

Author

Matsuzaki, Yoko, primary, Mizuta, Katsumi, additional, Aoki, Yoko, additional, Suto, Asuka, additional, Abiko, Chieko, additional, Sanjoh, Kanako, additional, Sugawara, Kanetsu, additional, Takashita, Emi, additional, Itagaki, Tsutomu, additional, Katsushima, Yuriko, additional, Ujike, Makoto, additional, Obuchi, Masatsugu, additional, Odagiri, Takato, additional, and Tashiro, Masato, additional

Published
2010
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19. A Nationwide Epidemic of Influenza C Virus Infection in Japan in 2004

Author

Matsuzaki, Yoko, primary, Abiko, Chieko, additional, Mizuta, Katsumi, additional, Sugawara, Kanetsu, additional, Takashita, Emi, additional, Muraki, Yasushi, additional, Suzuki, Hiroshi, additional, Mikawa, Masahide, additional, Shimada, Shinichi, additional, Sato, Katsuhiko, additional, Kuzuya, Mitsutaka, additional, Takao, Shinichi, additional, Wakatsuki, Kiyoko, additional, Itagaki, Tsutomu, additional, Hongo, Seiji, additional, and Nishimura, Hidekazu, additional

Published
2007
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31. An Assay for the Receptor‐Destroying Activity of Influenza C Virus

Author

Sugawara, Kanetsu, Kitame, Fumio, Homma, Morio, and Nakamura, Kiyoto

Abstract

We have developed a convenient method for assaying the receptor‐destroying enzyme (RDE) activity of influenza C virus. This method measures the ability of the RDE to destroy the hemagglutination‐inhibition activity of a potent inhibitor present in rat serum. Some physico‐chemical properties of the RDE of influenza C virus were investigated by using this method. The temperature optimum for maximal activity of this enzyme was found to be 45 C to 53 C. There was little difference in thermostability between the RDE and hemagglutinating activities of influenza C virus. When influenza C virions were treated with various concentrations of trypsin, the RDE activity decreased in parallel with the decrease in the amount of residual gp88 glycoprotein, suggesting association of RDE with this glycoprotein.

Published
1985
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32. Distribution of the Antibody to Influenza C Virus in Dogs and Pigs in Yamagata Prefecture, Japan

Author

Ohwada, Kazuo, Kitame, Fumio, Sugawara, Kanetsu, Nishimura, Hidekazu, Homma, Morio, and Nakamura, Kiyoto

Abstract

The distribution of the antibody to influenza C virus in the dogs and pigs in Yamagata prefecture, Japan was investigated by using three different serological methods: hemagglutination‐inhibition (HI), radioimmunoprecipitation (RIP), and immunoblotting. The antibody against influenza C virus glycoprotein (gp88) was detected in 5 out of 112 sera collected from mongrel dogs, three by RIP test and two by any of the three methods, suggesting that the virus can cause natural infection in dogs. Significant levels of HI activity were found in 58 out of 269 sera collected from domestic pigs, but none of them showed positive reaction in the more sensitive method, RIP, which suggests that the inhibitors against the hemagglutination by influenza C virus rather than the antibody to gp88 are responsible for the observed HI activity. It appears, therefore, that at least in the Yamagata area, pigs do not play significant roles in the spread of influenza C virus in humans.

Published
1987
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33. Prevalence of the Antibody to Influenza C Virus in a Northern Luzon Highland Village, Philippines

Author

Nishimura, Hidekazu, Sugawara, Kanetsu, Kitame, Fumio, Nakamura, Kiyoto, and Sasaki, Hideo

Abstract

A total of 101 serum samples were collected from the persons (1 to 85 years of age) living in a Philippine mountain village where the contact with other communities has largely been restricted. These sera were tested for the presence of antibody to influenza C virus with hemagglutination‐inhibition and radioimmunoprecipitation tests. The results showed that all the subjects, including the persons who had never been outside the village, contained the antibody to the surface glycoprotein of the virus, and that the age of acquisition of the antibody was significantly lower in this village than in any of the previously studied communities. Thus it appeared that infection with influenza C virus was prevalent even in this small mountain village, presumably with a higher incidence than in the larger, industrialized communities.

Published
1987
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34. Intrinsic Temperature Sensitivity of Influenza C Virus Hemagglutinin-Esterase-Fusion Protein.

Author

Takashita, Emi, Muraki, Yasushi, Sugawara, Kanetsu, Asao, Hironobu, Nishimura, Hidekazu, Suzuki, Koji, Tsuji, Takashi, Hongo, Seiji, Ohara, Yoshihiro, Kawaoka, Yoshihiro, Ozawa, Makoto, and Matsuzaki, Yoko

Subjects
*INFLUENZAVIRUS C, *HEMAGGLUTININ, *ESTERASES, *MEMBRANE glycoproteins, *PHYSIOLOGICAL effects of temperature, *MEMBRANE fusion
Abstract

Influenza C virus replicates more efficiently at 33°C than at 37°C. To determine whether hemagglutinin-esterase-fusion protein (HEF), a surface glycoprotein of influenza C virus, is a restricting factor for this temperature sensitivity, we analyzed the biological and biochemical properties of HEF at 33°C and 37°C. We found that HEF exhibits intrinsic temperature sensitivities for surface expression and fusion activity. [ABSTRACT FROM AUTHOR]

Published
2012
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