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8. Abstracts for the Tenth International Conference on Brain Tumour Research and Therapy: Stalheim Hotel, Voss, Norway, September 6–9, 1993

Author

Abrahamsen, Tore G., Wesenberg, Finn, Mørk, Sverre, Allen, Jeffrey, Hayes, Roberta, DaRosso, Robert, Nirenberg, Anita, Ali-Osman, Francis, Akande, Nike, Amberger, V., Seulberger, H., Paganetti, P. A., Schwab, M. E., Schwab, M. E., Arita N., Ohnishi T., Hiraga S., Yamamoto H., Taki T., Izumoto S., Higuchi M., Hayakawa T., Kusakabe M., Sakakura T., Baldwin, N. G., Rice, C. D., Merchant, R. E., Ashmore, Sally M., Darling, J. L., Bailey, C. C., Balmaceda C., Diez B., Villablanca J., Walker R., Finlay J., Bergenheim, A. Tommy, Hartman, Magdalena, Bergh, Jonas, Ridderheim, PerÅke, Henriksson, Roger, Berens, Michael E., Rief, Monique D., Giese, Alf, Zackrisson, Björn, Elfversson, Jörgen, Bernstein, Mark, Cabantog, Alberto, Glen, Jennifer, Mikulis, David, Bjerkvig, Rolf, Pedersen, Paal-Henning, Mathisen, Berit, Mahesparan, Rupavathana, Haugland, Hans Kristian, Bernstein, Mark, Laperriere, Normand, Thomason, Cindy, Leung, Phil, Bobola M. S., Berger M. S., Silber J. R., Bongcam-Rudloff, Erik, Wang, Jia-Lun, Nistér, Monica, Westermark, Bengt, Brem, Steven, Breslow, Gary, Ho, Jason, Gately, Stephen, Takano, Shingo, Ward, William, Brada, M., Laing, R., Warrington, J., Brem, Steven, Engelhard, Herbert, Takano, Shingo, Gately, Stephen, Brem, Steven, Landau, Barry, Kwaan, Hau, Verrusio, Elaine, Buckner, J. C., Cascino, T. L., Schomberg, P. S., O'Fallon, J. R., Dinapoli, R. P., Burch, P. A., Shaw, E. G., Broaddus, William C., Hager-Loudon, Kathryn, Merchant, Randall E., Loudon, William, Couldwell, William T., Jiang, Jack B., Burns, David, Couldwell, William T., Weiss, Martin H., Apuzzo, Michael L. J., Desbaillets I., Tada M., de Tribolet N., Van Meir, E., Davis, R. L., Onda, K., Prados, M. D., Dolan, M. Eileen, Fleig, Matthew J., Friedman, Henry S., Ekstrand, A. Jonas, Longo, Nicola, James, C. David, Chou, D., Wijnhoven, B., Bellinzona, M., Nakagawa, M., Feuerstein B. G., Basu H. S., Dolan M. E., Bergeron C., Pellarm M., Deen D. F., Marton L. J., Finlay, Jonathan, Fulton D. S., Urtasun R. C., Giese, Alf, Scheck, Adrienne C., Geddes, J., Vowles, G. M., Ashmore, S. M., Gillespie, G. Y., Goldman, C. K., Tucker, M. T., Lyon, E., Tsai, J. -C., Gobbel, G. T., Chan, P. H., Greenberg, Hairy S., Chandler, W. F., Ensminger, W. D., Junck, L., Sandler, H., Bromberg, J., McKeever, P., Gonzalez G. G., Sarkar A., Basu H., Feuerstein B. G., Deen D. F., Haugland, Kr., Tysnes, Ole-Bjørn, Hiraga, Shoju, Arita, Norio, Ohnishi, Takanori, Taki, Takuyu, Yamamoto, Hiroshi, Higuchi, Masahide, Hayakawa, Toru, Isern, Erik, Unsgaard, Geirmund, Marthinsen, Anne Beate Langeland, Strickert, Trond, Helseth, Eirik, Hochberg F., Cosgrove R., Valenzuela R., Pardo F., Zervas N., Jenkins, Robert B., Ritland, Steven R., Hailing, Kevin C., Thibodeau, Stephen N., Juillerat L., Darekar P., Janzer R. C., Hamou M. F., Kato, Tsutomu, Sawamura, Yutaka, Tada, Mitsuhiro, Sakuma, Shirou, Sudo, Masako, Abe, Hiroshi, Kallio M., Leppää J., Nikula T., Nikkinen P., Gylling H., Färkkilä M., Hiltunen J., Jääskeläinen J., Liewendahl K., Keles, G. Evren, Berger, Mitchel S., Deliganis, Anna, Kellie S. J., De Graaf S. S. N., Bloemhof H., Johnston I., Uges D. D. R., Besser M., Chaseling R. W., Ouvrier R. A., Kitchen, N. D., Hughes, S., Beaney, R., Thomas, D. G. T., Kim D. H., Maeda T., Mohapatra G., Park S., Waldman F. W., Gray J. W., Koala, D., Silber, J., Berger, M., Krauseneck P., Müller B., Strik H., Warmuth-Metz M., Kuratsu, Jun-ichi, Takeshima, Hideo, Ushio, Yukitaka, Kretschmar, C., Grodman, H., Linggood, R., Kyritsis, A. P., Bondy, M., Cunningham, J., Xiao, M., Levin, V., Leeds, N., Bruner, J., Yung, W. K. A., Saya, H., Lampson, L. A., Nichols, M. R., Lampson, M. A., Dunne, A. D., Li, Hong, Hamou, Marie-France, Jaufeerally, Rehana, Diserens, Annie-Claire, Van Meir, Erwin, de Tribolet, Nicolas, Levin, V. A., Maor, M., Sawaya, R., Leavens, M., Woo, S., Thall, P., Gleason, M. J., Liang, Bertrand C., Ross, D. A., Meltzer, P. S., Trent, J. M., Greenberg, H. S., Lillehei K. O., Kong Q., DeMasters B. K., Withrow S. J., Macdonald D. R., Cairncross J. G., Ludwin S., Lee D., Cascino T., Buckner J., Dropcho E., Fulton D., Stewart D., Schold C., Wainman N., Eisenhauer E., Kirby S., Fisher B. J., Magrassi, L., Butti, G., Pezzotta, S., Milanesi∘, G., Matsutani, Masao, Marienhagen, Kirsten, Laerum, Ole Didrik, Baldwin, N. G., Merzak, Abderrahim, Koocheckpour, Shahriar, Roxanis, Yannis, Pilktngton, Geoffrey J., Nagai, Masakatsu, Watanabe, Kunihiko, Narita, Jun-ichi, Hagiwara, Hideaki, Noble, Mark, Nomura, K., Oyama, H., Motoo, M., Shibui, S., Tokuue, K., Akine, Y., Ohnishi, T., Arita, N., Hiraga, S., Hayakawa, T., Nygaard, Svein J. Tjoflaat, Tysnes, Ole-Bjørn, Pardo, F. S., Hsu, D. W., Hedley-Whyte, E. T., Efird, J., Schmidt, E. V., Marienhagen, Paal-Henning Pedersenl Kirsten, Pilkington, Geoffrey J., Clarke, Tracey M., Yu, Hui Tian, Rogers, Joan P., Stern, Robert, Phuphanich, Surasak, Greenberg, Harvey, Murtagh, R., Viloria, Jesus, Ransohoff, Joseph, Martin, Kimberly, Hatva, V. Erika, Rao, Jasti S., Mohanam, S., Rempel, Sandra A., Schwechheimer, Karl, Davis, Richard L., Cavenee, Webster K., Rosenblum, Mark L., Reifenberger, Guido, Liu, Lu, Ichimura, Koichi, Schmidt, Esther E., Collins, V. Peter, Revesz T., Scaravilli F., Cockburn H., Thomas D. G. T., Rice, C. D., Biron, R. T., Merchant, R. E., McKerrow, James, Sloane, Bonnie, Mikkelsen, Tom, Roosen, Norbert, Coopersmith, Peter, Smith, Robert, Rooprai, Harcharan Kaur, Maidment, Steven, Rucklidge, Garry, Volovsek, Anton, Rutka J. T., Smith S. L., Matsuzawa K., Sankar, A. A., Darling, J. L., Williams, S. R., Fukuyama K., Marton L. J., Ikeda, Jun, Selker, R. G., Vertosick, F. T., Goldenberg, M. T., Bindal, R., Diez B., Taratuto A., Picco P., Monges J., Martinez M., Pacheco G., Gamboni M., Schultz M., Silber J. R., Mueller B. A., Ewers T. G., Berger M. S., Shiraishi, T., Tabuchi, K., Nakagawa, S., Kihara, S., Stewart, D. J., Eapen, L., Agboola, O., Popovic, P., Goel, R., Raaphorst, P., Wong, P. T. T., Shimokawa, S., Oh-uchida, M., Hori, K., Markert C., Pflughaupt K. -W., Tada M., Diserens A. -C., Jauferrally R., Desbaillets I., Hamou M. -F., de Tribolet N., Takeshima H., Mochizuki H., Clifford J. L., Nishi T., Levin V. A., Lotan R., Saya H., Terzis, A. J. A., Arnold, H., Laerum, O. D., Bjerkvig, R., Taratuto A. L., Sevlever G., Diaz D., Di Tella M., Cuccia V., Pomata H., Gallo G., Dietze, A., Knopp, U., Thomas, R., Brada, M., Carnochan, P., Flux, G., Kitchen, N., Thomas, D., Zalutsky, M., Bigner, D., Tofilon, Philip, Borchardt, Paul, Torp, Sverre H., Dalen, Are, Tohyama, Takashi, Kubo, Osami, Takakura, Kintomo, Lee, Virginia M. -Y., Trojanowski, John Q., Nygaard, Svein, Urtasun, R. C., Parliament, M. B., McEwan, A. J., Mannan, R. H., Weibe, L. I., Unsgårp, G., Sonnewald, U., Gribbestad, I., Isern, E., Petersen, S. B., Wang J., Delgado D. A., Warr, Tracy J., Sheer, Denise, Gorman, Pat, Yamaguchi, F., Westphal, M., Anker, L., Hamel, W., Lücke, M., Shepard, M., Kleihues, P., Herrmann, H. D., Yung, W. K. Alfred, Taylor, Scott, and Steck, Peter A.

Published
1993
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11. LAB-RADIOBIOLOGY

Author

Floyd, S. R., primary, Pacold, M. E., additional, Clarke, S. M., additional, Blake, E., additional, Fydrych, A., additional, Ho, R., additional, Lee, M. J., additional, Root, D. E., additional, Carpenter, A. E., additional, Sabatini, D. M., additional, French, C. A., additional, Bradner, J. E., additional, Chen, C. C., additional, Yaffe, M. B., additional, Le Rhun, E., additional, Massin, F., additional, Lefevre, A., additional, Bonneterre, J., additional, Bittencourt, M. d. C., additional, Faure, G., additional, Hiramatsu, R., additional, Kawabata, S., additional, Yamada, Y., additional, Miyatake, S.-I., additional, Kuroiwa, T., additional, Li, S., additional, Chou, A. P., additional, Chen, W., additional, Chen, R., additional, Deng, Y., additional, Phillips, H. S., additional, Faull, K. F., additional, Cloughesy, T., additional, Liau, L. M., additional, Lai, A., additional, Mori, K., additional, Ishikura, R., additional, Tomogane, Y., additional, Izumoto, S., additional, Arita, N., additional, Piao, J., additional, Auyeung, G., additional, Policarpio, E., additional, Tabar, V., additional, Yeung, T. P. C., additional, Morrison, L., additional, Hoffman, L., additional, Lee, T.-Y., additional, Bauman, G., additional, Yartsev, S., additional, Ryu, S., additional, Kolozsvary, A., additional, Lapanowski, M., additional, Jenrow, K., additional, Brown, S., additional, Kim, J. H., additional, Brown, R. J., additional, Love, J., additional, Warburton, D., additional, McBride, W., additional, Bluml, S., additional, Ren, X., additional, Vanderwaal, B., additional, Jaboin, J., additional, Baldock, A. L., additional, Anh, S., additional, Rockne, R., additional, Neal, M., additional, Clark-Swanson, K., additional, Sterin, G., additional, Trister, A. D., additional, Malone, H., additional, Ebiana, V., additional, Sonabend, A. M., additional, Mrugala, M., additional, Rockhill, J. K., additional, Silbergeld, D. L., additional, McKhann, G. M., additional, Bruce, J. N., additional, Rostomily, R., additional, Canoll, P., additional, Swanson, K. R., additional, Hawkins-Daarud, A., additional, Baldock, A., additional, Bridge, C., additional, Corwin, D., additional, Mrugala, M. M., additional, Yagle, K., additional, Born, D., additional, and Swanson, P., additional

Published
2012
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12. BIOLOGY

Author

Kim, J. H., primary, Song, H. B., additional, Kim, D. H., additional, Park, K. D., additional, Kim, J. H., additional, Lee, B. J., additional, Khatua, S., additional, Kalkan, E., additional, Brown, R., additional, Pearlman, M., additional, Vats, T., additional, Abela, L., additional, Fiaschetti, G., additional, Shalaby, T., additional, Grunder, E., additional, Ma, M., additional, Grahlert, J., additional, Baumgartner, M., additional, Siler, U., additional, Nonoguchi, N., additional, Ohgaki, H., additional, Grotzer, M., additional, Adachi, J.-i., additional, Suzuki, T., additional, Fukuoka, K., additional, Yanagisawa, T., additional, Mishima, K., additional, Koga, T., additional, Matsutani, M., additional, Nishikawa, R., additional, Sardi, I., additional, Giunti, L., additional, Bresci, C., additional, Cardellicchio, S., additional, Da Ros, M., additional, Buccoliero, A. M., additional, Farina, S., additional, Arico, M., additional, Genitori, L., additional, Massimino, M., additional, Filippi, L., additional, Erdreich-Epstein, A., additional, Zhou, H., additional, Ren, X., additional, Schur, M., additional, Davidson, T. B., additional, Ji, L., additional, Sposto, R., additional, Asgharzadeh, S., additional, Tong, Y., additional, White, E., additional, Murugesan, M., additional, Nimmervoll, B., additional, Wang, M., additional, Marino, D., additional, Ellison, D., additional, Finkelstein, D., additional, Pounds, S., additional, Malkin, D., additional, Gilbertson, R., additional, Eden, C., additional, Ju, B., additional, Phoenix, T., additional, Poppleton, H., additional, Lessman, C., additional, Taylor, M., additional, la Marca, G., additional, Malvagia, S., additional, Fratoni, V., additional, Giovannini, M. G., additional, Giangaspero, F., additional, Badiali, M., additional, Gleize, V., additional, Paris, S., additional, Moi, L., additional, Elhouadani, S., additional, Arcella, A., additional, Morace, R., additional, Antonelli, M., additional, Buttarelli, F., additional, Mokhtari, K., additional, Sanson, M., additional, Smith, S., additional, Ward, J., additional, Wilson, M., additional, Rahman, C., additional, Rose, F., additional, Peet, A., additional, Macarthur, D., additional, Grundy, R., additional, Rahman, R., additional, Venkatraman, S., additional, Birks, D., additional, Balakrishnan, I., additional, Alimova, I., additional, Harris, P., additional, Patel, P., additional, Foreman, N., additional, Vibhakar, R., additional, Wu, H., additional, Zhou, Q., additional, Wang, D., additional, Wang, G., additional, Dang, D., additional, Pencreach, E., additional, Nguyen, A., additional, Guerin, E., additional, Lasthaus, C., additional, Guenot, D., additional, Entz-Werle, N., additional, Unland, R., additional, Schlosser, S., additional, Farwick, N., additional, Plagemann, T., additional, Richter, G., additional, Juergens, H., additional, Fruehwald, M., additional, Chien, C.-L., additional, Lee, Y.-H., additional, Lin, C.-I., additional, Hsieh, J.-Y., additional, Lin, S.-C., additional, Wong, T.-T., additional, Ho, D. M.-T., additional, Wang, H.-W., additional, Lagah, S., additional, Tan, I.-L., additional, Malcolm, S., additional, Majani, Y., additional, van Vuurden, D. G., additional, Aronica, E., additional, Wedekind, L. E., additional, Hulleman, E., additional, Biesmans, D., additional, Bugiani, M., additional, Vandertop, W. P., additional, Kaspers, G. J. L., additional, Wurdinger, T., additional, Noske, D. P., additional, Van der Stoop, P. M., additional, Shukla, S., additional, Kuipers, G. K., additional, Slotman, B. J., additional, Cloos, J., additional, Sun, T., additional, Warrington, N., additional, Luo, J., additional, Ganzhorn, S., additional, Tabori, U., additional, Druley, T., additional, Gutmann, D., additional, Rubin, J., additional, Castelo-Branco, P., additional, Choufani, S., additional, Mack, S., additional, Galagher, D., additional, Zhang, C., additional, Lipman, T., additional, Zhukova, N., additional, Martin, D., additional, Merino, D., additional, Wasserman, J., additional, Samuel, C., additional, Alon, N., additional, Hitzler, J., additional, Wang, J. C. Y., additional, Keller, G., additional, Dirks, P. B., additional, Pfister, S., additional, Taylor, M. D., additional, Weksberg, R., additional, Leblond, P., additional, Meignan, S., additional, Dewitte, A., additional, Le Tinier, F., additional, Wattez, N., additional, Lartigau, E., additional, Lansiaux, A., additional, Hanson, R., additional, Gordon, I., additional, Zhao, S., additional, Camphausen, K., additional, Warren, K., additional, Warrington, N. M., additional, Gutmann, D. H., additional, Rubin, J. B., additional, Jaillet, M., additional, Kovacs, Z., additional, Martin-Fiori, E., additional, Bernasconi, M., additional, Werner, B., additional, Dyberg, C., additional, Baryawno, N., additional, Milosevic, J., additional, Wickstrom, M., additional, Northcott, P. A., additional, Kool, M., additional, Kogner, P., additional, Johnsen, J. I., additional, Reynolds, G., additional, Davies, N., additional, Arvanitis, T., additional, Zoghbi, A., additional, Meisterernst, M., additional, Fruehwald, M. C., additional, Kerl, K., additional, Orr, B., additional, Haffner, M., additional, Nelson, W., additional, Yegnasubramanian, S., additional, Eberhart, C., additional, Fotovati, A., additional, Abu-Ali, S., additional, Wang, P.-S., additional, Deleyrolle, L., additional, Lee, C., additional, Triscott, J., additional, Chen, J., additional, Franciosi, S., additional, Nakamura, Y., additional, Sugita, Y., additional, Uchiumi, T., additional, Kuwano, M., additional, Leavitt, B., additional, Singh, S., additional, Jury, A., additional, Jones, C., additional, Wakimoto, H., additional, Reynolds, B., additional, Pallen, C., additional, Dunn, S., additional, Fletcher, S., additional, Levine, J., additional, Li, M., additional, Kagawa, N., additional, Hirayama, R., additional, Chiba, Y., additional, Kijima, N., additional, Arita, H., additional, Kinoshita, M., additional, Hashimoto, N., additional, Izumoto, S., additional, Maruno, M., additional, and Yoshimine, T., additional

Published
2012
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13. PATHOLOGY

Author

Hobbs, J., primary, Fardo, D. W., additional, Cieply, K., additional, Dacic, S., additional, Hamilton, R. L., additional, Horbinski, C., additional, Giannini, C., additional, Bernardo, M. C., additional, Menke, J., additional, Radford, J. G., additional, Hallemeier, C., additional, Boes, C. J., additional, Lewis, M., additional, Scheithauer, B. W., additional, Kim, S. H., additional, Change, W. S., additional, Kim, J. P., additional, Chang, J. H., additional, Chen, Z.-p., additional, Chen, Y.-S., additional, Mihalcik, S. A., additional, Jentoft, M., additional, Scheithauer, B., additional, Laack, N., additional, Mori, K., additional, Fujita, S., additional, Tomogane, Y., additional, Izumoto, S., additional, Arita, N., additional, Pollo, B., additional, Maderna, E., additional, Calatozzolo, C., additional, Nunziata, R., additional, Silvani, A., additional, Eoli, M., additional, Salmaggi, A., additional, Finocchiaro, G., additional, Wesseling, P., additional, Boots-Sprenger, S., additional, Bleeker, F., additional, Sijben, A., additional, Rijntjes, J., additional, Gijtenbeek, A., additional, Jeuken, J., additional, Kirsch, M., additional, Mackenroth, L., additional, Geiger, K., additional, Schackert, G., additional, Steiner, G., additional, Engler, J., additional, Robinson, A., additional, Gupta, N., additional, James, C. D., additional, Phillips, J. J., additional, Cole, V. R., additional, Kennedy, L. D., additional, and Lesser, G., additional

Published
2011
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23. Control of Chemical Waves by Fluid Stretching and Compression.

Author

Izumoto S, Escala DM, Heyman J, Le Borgne T, and De Wit A

Abstract

Oscillatory kinetics coupled to diffusion can produce traveling waves as observed in physical, chemical, and biological systems. We show experimentally that the properties of such waves can be controlled by fluid stretching and compression in a hyperbolic flow. Localized packet waves consisting in a train of parallel waves can develop due to a balance between diffusive broadening and advective compression along the unstable manifold. At a given distance from the stagnation point, the parallel waves transform into planelike waves and smeared waves where the transverse parabolic flow profile disturbs the patterns in the gap width. Once a wave packet has been obtained, it imprints a privileged direction that is maintained even if the compression rate is decreased. The width of the wave packet then scales inversely with the compression rate.

Published
2024
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24. Spontaneous high clonal expansion of Wilms' tumor gene 1-specific cytotoxic T-lymphocytes in patients with Wilms' tumor gene 1-expressing solid tumor.

Author

Morimoto S, Tanaka Y, Nakata J, Fujiki F, Hasegawa K, Nakajima H, Nishida S, Tsuboi A, Hosen N, Kagawa N, Maruno M, Myoui A, Enomoto T, Izumoto S, Sekimoto M, Hashimoto N, Yoshimine T, Kumanogoh A, Oji Y, Oka Y, and Sugiyama H

Subjects
Humans, Male, Female, Middle Aged, Adult, Aged, Neoplasms immunology, Neoplasms genetics, HLA-A2 Antigen immunology, HLA-A2 Antigen genetics, Wilms Tumor immunology, Wilms Tumor genetics, T-Lymphocytes, Cytotoxic immunology, WT1 Proteins immunology, WT1 Proteins genetics
Abstract

Wilms' tumor protein 1 (WT1)-targeted immunotherapy has been used in patients with leukemia and solid tumors. However, the spontaneous WT1-specific immune response before WT1 peptide vaccination in patients with WT1-expressing tumors (PTs) remains unclear. Therefore, we investigated whether WT1-specific cytotoxic CD8 + T-lymphocytes (CTLs) are clonally expanded in the peripheral blood outside of tumor sites. Clonal expansion of WT1 126 peptide (a.a.126-134)-specific CTLs (WT1 126 -CTLs) was compared between seven PTs and five healthy volunteers (HVs), and their T-cell receptors (TCRs) were analyzed at the single-cell level. Overall, 433 and 351 TCR β-chains of WT1 126 -CTLs were detected from PTs and HVs, respectively, and complementarity-determining region 3 was sequenced for clonality analysis. The frequencies of WT1 126 -CTLs were higher in human leukocyte antigen (HLA)-A*02:01 + PTs than in HLA-A*02:01 + HVs, although the difference was not statistically significant. WT1 126 -CTLs of differentiated types, including memory and effector, were higher in PTs than in HVs; whereas, those of the naïve type were higher in HVs than in PTs. WT1 126 -CTL clonality was significantly higher in PTs than in HVs. Furthermore, the frequency of effector WT1 126 -CTLs positively correlated with WT1 126 -CTL clonality in PTs; whereas, the frequency of naïve phenotype WT1 126 -CTLs tended to be negatively correlated with clonality. In conclusion, these results suggest that the WT1 protein in tumor cells is highly immunogenic, thereby stimulating endogenous naïve-type WT1 126 -CTLs and enabling them to clonally expand and differentiate into effector-type WT1 126 -CTLs., (© 2024. The Author(s).)

Published
2024
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25. Perampanel for Treatment of People with a Range of Epilepsy Aetiologies in Clinical Practice: Evidence from the PERMIT Extension Study.

Author

Strzelczyk A, Maschio M, Pensel MC, Coppola A, Takahashi S, Izumoto S, Trinka E, Cappucci S, Sainz-Fuertes R, and Villanueva V

Abstract

Introduction: It is important to assess the effectiveness of an antiseizure medication in treating different epilepsy aetiologies to optimise individualised therapeutic approaches. Data from the PERaMpanel pooled analysIs of effecTiveness and tolerability (PERMIT) Extension study were used to assess the effectiveness and safety/tolerability of perampanel (PER) when used to treat individuals with a range of epilepsy aetiologies in clinical practice., Methods: A post hoc analysis was conducted of PERMIT Extension data from individuals with a known aetiology. Retention was assessed after 3, 6 and 12 months. Effectiveness was assessed after 3, 6 and 12 months and at the last visit (last observation carried forward). Effectiveness assessments included responder rate (≥ 50% seizure frequency reduction) and seizure freedom rate (no seizures since at least the prior visit). Safety/tolerability was assessed by evaluating adverse events (AEs) and AEs leading to discontinuation., Results: PERMIT Extension included 1945 individuals with structural aetiology, 1012 with genetic aetiology, 93 with an infectious aetiology, and 26 with an immune aetiology. Retention rates at 12 months were 61.1% (structural), 65.9% (genetic), 56.8% (infectious) and 56.5% (immune). At the last visit, responder rates (total seizures) were 43.3% (structural), 68.3% (genetic), 37.0% (infectious) and 20.0% (immune), and corresponding seizure freedom rates were 15.8%, 46.5%, 11.1% and 5.0%, respectively. AE incidence rates were 58.0% (structural), 46.5% (genetic), 51.1% (infectious) and 65.0% (immune), and corresponding rates of discontinuation due to AEs over 12 months were 18.9%, 16.4%, 18.5% and 21.7%, respectively. The types of AEs reported were generally consistent across aetiology subgroups, with no idiosyncratic AEs emerging., Conclusion: Although PER was effective and generally well tolerated when used to treat individuals with a range of epilepsy aetiologies in clinical practice, variability in its effectiveness and tolerability across the subgroups indicates that PER may be particularly useful for individuals with specific epilepsy aetiologies., (© 2024. The Author(s).)

Published
2024
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26. Pore-Scale Mechanisms for Spectral Induced Polarization of Calcite Precipitation Inferred from Geo-Electrical Millifluidics.

Author

Izumoto S, Huisman JA, Zimmermann E, Heyman J, Gomez F, Tabuteau H, Laniel R, Vereecken H, Méheust Y, and Le Borgne T

Subjects
Chemical Precipitation, Porosity, Calcium Carbonate chemistry, Electricity
Abstract

Spectral induced polarization (SIP) has the potential for monitoring reactive processes in the subsurface. While strong SIP responses have been measured in response to calcite precipitation, their origin and mechanism remain debated. Here we present a novel geo-electrical millifluidic setup designed to observe microscale reactive transport processes while performing SIP measurements. We induced calcite precipitation by injecting two reactive solutions into a porous medium, which led to highly localized precipitates at the mixing interface. Strikingly, the amplitude of the SIP response increased by 340% during the last 7% increase in precipitate volume. Furthermore, while the peak frequency in SIP response varied spatially over 1 order of magnitude, the crystal size range was similar along the front, contradicting assumptions in the classical grain polarization model. We argue that the SIP response of calcite precipitation in such mixing fronts is governed by Maxwell-Wagner polarization due to the establishment of a precipitate wall. Numerical simulations of the electric field suggested that spatial variation in peak frequency was related to the macroscopic shape of the front. These findings provide new insights into the SIP response of calcite precipitation and highlight the potential of geoelectrical millifluidics for understanding and modeling electrical signatures of reactive transport processes.

Published
2022
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27. A 48-Year-Old Man Presenting as an Emergency with Severe Back Pain, a Large Anterior Paravertebral Hematoma, and Spontaneous Rupture of the Right 9th Intercostal Artery Successfully Managed by Transcatheter Arterial Embolization: A Case Report.

Author

Izumoto S, Abe T, Koroki T, Furukoji E, Masuda R, and Ochiai H

Subjects
Arteries, Back Pain, Hematoma diagnostic imaging, Hematoma etiology, Hematoma therapy, Humans, Male, Middle Aged, Rupture, Spontaneous, Vascular Surgical Procedures, Embolization, Therapeutic
Abstract

BACKGROUND The rupture of an intercostal artery is rare and is usually associated with trauma, neurofibromatosis type 1, or coarctation of the aorta. Transcatheter arterial embolization is a minimally invasive vascular surgical procedure used to control hemorrhage of an intercostal artery. This report describes a case of a 48-year-old man who presented with severe back pain. This was due to a large anterior paravertebral hematoma following the spontaneous rupture of the right 9th intercostal artery. The rupture was successfully managed by transcatheter arterial embolization. CASE REPORT A 48-year-old man suddenly felt severe back pain while walking. He had no previous medical history and he had not experienced any external injury. On arrival, he was tachycardic and hypertensive. He did not have abnormal physical findings. His chest radiograph, 12-lead electrocardiogram, ultrasonography, and blood test findings were unremarkable. A chest computed tomography scan with contrast media was performed, which revealed a 4.3×2.7×7.0 cm mass, enhanced with contrast media, anterior to the 9th vertebral body. The patient was diagnosed with spontaneous rupture of the right ninth intercostal artery. The lesion was embolized with 8 microcoils. The patient was discharged on the 8th hospital day without complications. CONCLUSIONS This report presents a rare case of the rupture of an intercostal artery in which no cause was identified. It highlights the role of imaging as an important diagnostic tool. Furthermore, this report shows the benefits of the timely use of emergency transcatheter arterial embolization, which in this instance resulted in a successful outcome.

Published
2022
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28. Evaluation of the Safety and Effectiveness of Coil Embolization for Anterior Communicating and Anterior Cerebral Artery Aneurysms.

Author

Nakagawa N, Fukawa N, Tsuji K, Furukawa K, Watanabe A, and Izumoto S

Abstract

Objective: Endovascular coil embolization for anterior communicating artery (ACoA) and anterior cerebral artery (ACA) aneurysms is associated with high total and near-total occlusion rates, but the complication rate is high. The development of newer endovascular technologies may improve the clinical outcomes. This study investigated the status of endovascular treatment of ACoA and ACA aneurysms by comparing our results with past reports., Methods: Between January 2006 and December 2018, we investigated 50 patients who were followed for 12 months or longer to clarify the outcomes of coil embolization. The outcomes of embolization were evaluated using time-of-flight MRA. The safety was evaluated based on procedure-related complications that affected clinical outcomes., Results: Initial assessments demonstrated complete obliteration in 84% (42 of 50 patients) and a residual neck in 14% (7 of 50 patients). Procedure-related complications developed in 12% (6 of 50 patients). The procedure-related morbidity rate was 2% (1 of 50 patients) and there was no procedure-related death. Recanalization was noted in 14% (7 of 50 patients, median follow-up period, 57 months). The recanalized aneurysms were significantly smaller than the stable aneurysms in maximum size (4.3 mm vs. 5.8 mm; p = 0.017) and height (3.7 mm vs. 4.3 mm; p = 0.035)., Conclusion: We demonstrated the safety and effectiveness of endovascular coil embolization for ACoA and ACA aneurysms. The small size of aneurysms may be related to recanalization., Competing Interests: All authors have no conflicts of interest to declare., (©2022 The Japanese Society for Neuroendovascular Therapy.)

Published
2022
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29. Maintenance of WT1 expression in tumor cells is associated with a good prognosis in malignant glioma patients treated with WT1 peptide vaccine immunotherapy.

Author

Yokota C, Kagawa N, Takano K, Chiba Y, Kinoshita M, Kijima N, Oji Y, Oka Y, Sugiyama H, Tsuboi A, Izumoto S, Kishima H, and Hashimoto N

Subjects
Adult, Biomarkers, Tumor biosynthesis, CD3 Complex biosynthesis, CD4-Positive T-Lymphocytes cytology, Cancer Vaccines, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, Female, Gene Expression Profiling, Histocompatibility Antigens Class I immunology, Humans, Male, Middle Aged, Peptides chemistry, Prognosis, Proportional Hazards Models, Brain Neoplasms diagnosis, Brain Neoplasms metabolism, Gene Expression Regulation, Neoplastic, Glioma diagnosis, Glioma metabolism, Immunotherapy methods, WT1 Proteins biosynthesis
Abstract

We have previously revealed the overexpression of Wilms' tumor gene 1 (WT1) in malignant glioma and developed WT1 peptide vaccine cancer immunotherapy. A phase II clinical trial indicated the clinical efficacy of the WT1 peptide vaccine for recurrent malignant glioma. Here, we aimed to investigate the immunological microenvironment in glioma tissues before and after WT1 peptide vaccine treatment. Paired tissue samples were obtained from 20 malignant glioma patients who had received the WT1 peptide vaccine for > 3 months and experienced tumor progression, confirmed radiographically and/or clinically, during vaccination. We discovered that the expression of WT1 and HLA class I antigens in the tumor cells significantly decreased after vaccination. Maintenance of WT1 expression, which is the target molecule of immunotherapy, in tumor cells during the vaccination period was significantly associated with a longer progression-free and overall survival. A high expression of HLA class I antigens and low CD4 + /CD8 + tumor-infiltrating lymphocytes (TIL) ratio in pre-vaccination specimens, were also associated with a good prognosis. No statistically significant difference existed in the number of infiltrating CD3 + or CD8 + T cells between the pre- and post-vaccination specimens, whereas the number of infiltrating CD4 + T cells significantly decreased in the post-vaccination specimens. This study provides insight into the mechanisms of intra-tumoral immune reaction/escape during WT1 peptide vaccine treatment and suggests potential clinical strategies for cancer immunotherapy., (© 2021. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published
2022
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30. Cardiac Strangulation Due to Partial Pericardial Defect Presenting as Acute Myocardial Infarction.

Author

Izumoto S, Oguri N, Koyama S, Matsuura Y, Komatsu H, Asada Y, and Iwakiri H

Abstract

A 79-year-old man with chest pain and dyspnea underwent emergency percutaneous coronary intervention for acute myocardial infarction. However, he died 17 days later due to refractory heart failure. An autopsy revealed cardiac strangulation caused by herniation of the apical heart through a pericardial defect due to partial absence of the pericardium. ( Level of Difficulty: Advanced. )., Competing Interests: The authors have reported that they have no relationships relevant to the contents of this paper to disclose., (© 2021 The Authors.)

Published
2021
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31. Necessity for craniospinal irradiation of germinoma with positive cytology without spinal lesion on MR imaging-A controversy.

Author

Kanamori M, Takami H, Suzuki T, Tominaga T, Kurihara J, Tanaka S, Hatazaki S, Nagane M, Matsuda M, Yoshino A, Natsumeda M, Yamaoka M, Kagawa N, Akiyama Y, Fukai J, Negoto T, Shibahara I, Tanaka K, Inoue A, Mase M, Tomita T, Kuga D, Kijima N, Fukami T, Nakahara Y, Natsume A, Yoshimoto K, Keino D, Tokuyama T, Asano K, Ujifuku K, Abe H, Nakada M, Matsuda KI, Arakawa Y, Ikeda N, Narita Y, Shinojima N, Kambe A, Nonaka M, Izumoto S, Kawanishi Y, Kanaya K, Nomura S, Nakajima K, Yamamoto S, Terashima K, Ichimura K, and Nishikawa R

Abstract

Background: Cerebrospinal fluid (CSF) cytology and spinal MR imaging are routinely performed for staging before treatment of intracranial germinoma. However, the interpretation of the results of CSF cytology poses 2 unresolved clinical questions: (1) Does positive CSF cytology correlate with the presence of spinal lesion before treatment? and (2) Is craniospinal irradiation (CSI) necessary for patients with positive CSF cytology in the absence of spinal lesion?, Methods: Multicenter retrospective analyses were performed based on a questionnaire on clinical features, spinal MR imaging finding, results of CSF cytology, treatments, and outcomes which was sent to 86 neurosurgical and 35 pediatrics departments in Japan. Pretreatment frequencies of spinal lesion on MR imaging were compared between the patients with positive and negative cytology. Progression-free survival (PFS) rates were compared between patients with positive CSF cytology without spinal lesion on MR imaging treated with CSI and with whole brain or whole ventricular irradiation (non-CSI)., Results: A total of 92 germinoma patients from 45 institutes were evaluated by both CSF cytology and spinal MR images, but 26 patients were excluded because of tumor markers, the timing of CSF sampling or incomplete estimation of spinal lesion. Of the remaining 66 germinoma patients, spinal lesions were equally identified in patients with negative CSF cytology and positive cytology (4.9% and 8.0%, respectively). Eleven patients treated with non-CSI had excellent PFS comparable to 11 patients treated with CSI., Conclusion: CSI is unnecessary for germinoma patients with positive CSF cytology without spinal lesions on MR imaging., (© The Author(s) 2021. Published by Oxford University Press, the Society for Neuro-Oncology and the European Association of Neuro-Oncology.)

Published
2021
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32. So-called bifocal tumors with diabetes insipidus and negative tumor markers: are they all germinoma?

Author

Kanamori M, Takami H, Yamaguchi S, Sasayama T, Yoshimoto K, Tominaga T, Inoue A, Ikeda N, Kambe A, Kumabe T, Matsuda M, Tanaka S, Natsumeda M, Matsuda KI, Nonaka M, Kurihara J, Yamaoka M, Kagawa N, Shinojima N, Negoto T, Nakahara Y, Arakawa Y, Hatazaki S, Shimizu H, Yoshino A, Abe H, Akimoto J, Kawanishi Y, Suzuki T, Natsume A, Nagane M, Akiyama Y, Keino D, Fukami T, Tomita T, Kanaya K, Tokuyama T, Izumoto S, Nakada M, Kuga D, Yamamoto S, Anei R, Uzuka T, Fukai J, Kijima N, Terashima K, Ichimura K, and Nishikawa R

Subjects
Biomarkers, Tumor, Child, Humans, Male, Retrospective Studies, Brain Neoplasms, Diabetes Insipidus etiology, Diabetes Mellitus, Germinoma complications, Germinoma diagnosis, Pineal Gland
Abstract

Background: The Delphi consensus statements on the management of germ cell tumors (GCTs) failed to reach agreements on the statement that the cases with (i) pineal and neurohypophyseal bifocal lesion, (ii) with diabetes insipidus, and (iii) with negative tumor markers can be diagnosed as germinoma without histological verification. To answer this, multicenter retrospective analysis was performed., Methods: A questionnaire on clinical findings, histological diagnosis, and details of surgical procedures was sent to 86 neurosurgical and 35 pediatrics departments in Japan., Results: Fifty-one institutes reported 132 cases that fulfilled the 3 criteria. Tissue sampling was performed in 91 cases from pineal (n = 44), neurohypophyseal (n = 32), both (n = 6), and distant (n = 9) lesions. Histological diagnosis was established in 89 cases: pure germinoma or germinoma with syncytiotrophoblastic giant cells in 82 (92.1%) cases, germinoma and mature teratoma in 2 cases, and granulomatous inflammation in 2 cases. Histological diagnosis was not established in 2 cases. Although no tumors other than GCTs were identified, 3 (3.4%) patients had non-germinomatous GCTs (NGGCTs). None of the patients developed permanent complications after endoscopic or stereotactic biopsy. Thirty-nine patients underwent simultaneous procedure for acute hydrocephalus without permanent complications, and hydrocephalus was controlled in 94.9% of them., Conclusion: All patients who fulfilled the 3 criteria had GCTs or granulomatous inflammation, but not other types of tumors. However, no fewer than 3.4% of the patients had NGGCTs. Considering the safety and the effects of simultaneous procedures for acute hydrocephalus, biopsy was recommended in such patients., (© The Author(s) 2020. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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33. Complement Activation in Human Sepsis is Related to Sepsis-Induced Disseminated Intravascular Coagulation.

Author

Abe T, Kubo K, Izumoto S, Shimazu S, Goan A, Tanaka T, Koroki T, Saito K, Kawana R, and Ochiai H

Subjects
Aged, Complement Activation physiology, Female, Humans, Intensive Care Units, Male, Middle Aged, Prognosis, Prospective Studies, Complement Membrane Attack Complex metabolism, Disseminated Intravascular Coagulation blood, Disseminated Intravascular Coagulation etiology, Sepsis blood, Sepsis complications
Abstract

Introduction: In human sepsis, little is known about the relationships between complement activation and the clinical characteristics of sepsis, including disseminated intravascular coagulation (DIC), interventions, and prognosis., Patients and Methods: Adult patients with sepsis admitted from November 2016 to December 2018 were included. We used the plasma levels of soluble C5b-9 (SC5b-9) as a marker of complement activation. We compared the clinical characteristics and complement components between patients with and without DIC. We also compared the clinical characteristics and each DIC parameter across quartile groups for the SC5b-9 value., Results: Forty-nine sepsis patients were eligible. Thirty-four patients developed DIC, and eight patients died. The median (interquartile range) SC5b-9 value was 342 (261-501) ng/mL. Compared with patients without DIC, patients with DIC showed lower C3 levels (mean, 95.7 vs. 70.4 mg/dL, P < 0.01) and higher SC5b-9 levels (median, 287 vs. 400 ng/mL, P = 0.01). Patients were stratified by SC5b-9 quartile (ng/mL: low: < 260, moderate: 260-342, high: 343-501, highest: > 501). The mean Sequential Organ Failure Assessment score varied across these groups (P = 0.02). In the high and highest groups, many more patients received vasopressors and developed DIC. In the highest group, the coagulation parameters were severe, and thrombocytopenia was prolonged. In-hospital mortality tended to be high (33%) in the highest group., Conclusions: The degree of complement activation is related to DIC, severity, intensive interventions, and mortality. Further studies are needed to confirm the usefulness of SC5b-9 for stratifying sepsis patients.

Published
2020
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34. [A Case of Primary Central Nervous System Lymphomatoid Granulomatosis that was Completely Ameliorated by Corticosteroid Treatment].

Author

Nakao T, Izumoto S, Tsuyuguchi N, Kato A, Yokoo H, and Enoki E

Subjects
Adult, Female, Herpesvirus 4, Human, Humans, Magnetic Resonance Imaging, Adrenal Cortex Hormones therapeutic use, Brain Neoplasms diagnostic imaging, Brain Neoplasms drug therapy, Lymphomatoid Granulomatosis diagnostic imaging, Lymphomatoid Granulomatosis drug therapy
Abstract

Lymphomatoid granulomatosis (LYG) is an angiocentric, angiodestructive lymphoreticular proliferative disease that usually affects the lungs but it has been speculated to also effect the central nervous system (CNS). However, unique primary LYG of the CNS has rarely been reported in the literature. Herein, we describe a clinical case of a 37-year-old female patient with grade 1 primary CNS-LYG having a good prognosis owing to corticosteroid treatment. The aforesaid patient, presented with a headache and left leg weakness with no evidence of a systemic disease. MRI revealed multiple small enhancing nodules in the right hemisphere with diffuse high-intensity lesions on T 2 / FLAIR image. A brain biopsy showed lymphohistiocytic cells with blood vessels infiltrated with CD3+ and CD20+. The Epstein-Barr virus encoded small RNA-ISH test was negative. Based on the above findings, grade 1 primary CNS-LYG was diagnosed. Following the administration of oral corticosteroids, a systemic high-dose corticosteroid therapy was administrated. Complete remission was achieved and maintained for 24 months following treatment. Grade 1 primary CNS-LYG is a rare disease that is not apparently associated with the Epstein-Barr virus (EBV) and possibly yields much better prognosis than the frequently EBV-positive systemic LYG with CNS localization. (Received November 5, 2019; Accepted November 20, 2019; Published February 1, 2020).

Published
2020
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35. Prediction of IDH and TERT promoter mutations in low-grade glioma from magnetic resonance images using a convolutional neural network.

Author

Fukuma R, Yanagisawa T, Kinoshita M, Shinozaki T, Arita H, Kawaguchi A, Takahashi M, Narita Y, Terakawa Y, Tsuyuguchi N, Okita Y, Nonaka M, Moriuchi S, Takagaki M, Fujimoto Y, Fukai J, Izumoto S, Ishibashi K, Nakajima Y, Shofuda T, Kanematsu D, Yoshioka E, Kodama Y, Mano M, Mori K, Ichimura K, Kanemura Y, and Kishima H

Subjects
Biomarkers, Tumor, Female, Humans, Image Processing, Computer-Assisted, Male, Neoplasm Grading, Neoplasm Staging, Reproducibility of Results, Glioma diagnosis, Glioma genetics, Isocitrate Dehydrogenase genetics, Magnetic Resonance Imaging methods, Mutation, Neural Networks, Computer, Promoter Regions, Genetic, Telomerase genetics
Abstract

Identification of genotypes is crucial for treatment of glioma. Here, we developed a method to predict tumor genotypes using a pretrained convolutional neural network (CNN) from magnetic resonance (MR) images and compared the accuracy to that of a diagnosis based on conventional radiomic features and patient age. Multisite preoperative MR images of 164 patients with grade II/III glioma were grouped by IDH and TERT promoter (pTERT) mutations as follows: (1) IDH wild type, (2) IDH and pTERT co-mutations, (3) IDH mutant and pTERT wild type. We applied a CNN (AlexNet) to four types of MR sequence and obtained the CNN texture features to classify the groups with a linear support vector machine. The classification was also performed using conventional radiomic features and/or patient age. Using all features, we succeeded in classifying patients with an accuracy of 63.1%, which was significantly higher than the accuracy obtained from using either the radiomic features or patient age alone. In particular, prediction of the pTERT mutation was significantly improved by the CNN texture features. In conclusion, the pretrained CNN texture features capture the information of IDH and TERT genotypes in grade II/III gliomas better than the conventional radiomic features.

Published
2019
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36. Intravascular Lymphoma Presenting as a Cavernous Sinus Tumor.

Author

Kawai S, Okuda T, Fukui A, Sanada Y, Yoshikawa K, Morikawa M, Kuwahara M, Maenishi O, Morita Y, Izumoto S, Kato A, Matsumura I, and Kusunoki S

Subjects
Adult, Female, Humans, Rare Diseases pathology, Rare Diseases surgery, Treatment Outcome, Cavernous Sinus pathology, Eye Neoplasms pathology, Eye Neoplasms surgery, Lymphoma, Large B-Cell, Diffuse pathology, Lymphoma, Large B-Cell, Diffuse surgery, Vascular Neoplasms pathology, Vascular Neoplasms surgery
Abstract

Intravascular lymphoma (IVL) is a malignant lymphoma that lacks the expression of cell surface adhesion molecules so that cells fluidly migrate within the blood vessels. The patient in the present study had restricted eye movement caused by IVL, mimicking a cavernous sinus tumor. Because the cavernous sinus lumen is divided into multiple compartments by trabeculae and venous channels, IVL tumor cells were trapped in these compartments, thus forming a mass, which subsequently extended into the contralateral cavernous sinus via the anterior and posterior intercavernous sinuses. This is a rare case of IVL forming a mass inside the cavernous sinus.

Published
2019
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37. Significance of molecular classification of ependymomas: C11orf95-RELA fusion-negative supratentorial ependymomas are a heterogeneous group of tumors.

Author

Fukuoka K, Kanemura Y, Shofuda T, Fukushima S, Yamashita S, Narushima D, Kato M, Honda-Kitahara M, Ichikawa H, Kohno T, Sasaki A, Hirato J, Hirose T, Komori T, Satomi K, Yoshida A, Yamasaki K, Nakano Y, Takada A, Nakamura T, Takami H, Matsushita Y, Suzuki T, Nakamura H, Makino K, Sonoda Y, Saito R, Tominaga T, Matsusaka Y, Kobayashi K, Nagane M, Furuta T, Nakada M, Narita Y, Hirose Y, Ohba S, Wada A, Shimizu K, Kurozumi K, Date I, Fukai J, Miyairi Y, Kagawa N, Kawamura A, Yoshida M, Nishida N, Wataya T, Yamaoka M, Tsuyuguchi N, Uda T, Takahashi M, Nakano Y, Akai T, Izumoto S, Nonaka M, Yoshifuji K, Kodama Y, Mano M, Ozawa T, Ramaswamy V, Taylor MD, Ushijima T, Shibui S, Yamasaki M, Arai H, Sakamoto H, Nishikawa R, and Ichimura K

Subjects
Adolescent, Adult, Aged, Carrier Proteins metabolism, Child, Child, Preschool, DNA Methylation, Female, Genetic Techniques, Histones metabolism, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Humans, Infant, Infant, Newborn, Male, Middle Aged, Nerve Tissue Proteins metabolism, Proteins metabolism, RNA, Messenger metabolism, Receptors, Dopamine D4 metabolism, Transcription Factor RelA metabolism, Young Adult, Central Nervous System Neoplasms classification, Central Nervous System Neoplasms genetics, Ependymoma classification, Ependymoma genetics, Mutation genetics, Proteins genetics, Transcription Factor RelA genetics
Abstract

Extensive molecular analyses of ependymal tumors have revealed that supratentorial and posterior fossa ependymomas have distinct molecular profiles and are likely to be different diseases. The presence of C11orf95-RELA fusion genes in a subset of supratentorial ependymomas (ST-EPN) indicated the existence of molecular subgroups. However, the pathogenesis of RELA fusion-negative ependymomas remains elusive. To investigate the molecular pathogenesis of these tumors and validate the molecular classification of ependymal tumors, we conducted thorough molecular analyses of 113 locally diagnosed ependymal tumors from 107 patients in the Japan Pediatric Molecular Neuro-Oncology Group. All tumors were histopathologically reviewed and 12 tumors were re-classified as non-ependymomas. A combination of RT-PCR, FISH, and RNA sequencing identified RELA fusion in 19 of 29 histologically verified ST-EPN cases, whereas another case was diagnosed as ependymoma RELA fusion-positive via the methylation classifier (68.9%). Among the 9 RELA fusion-negative ST-EPN cases, either the YAP1 fusion, BCOR tandem duplication, EP300-BCORL1 fusion, or FOXO1-STK24 fusion was detected in single cases. Methylation classification did not identify a consistent molecular class within this group. Genome-wide methylation profiling successfully sub-classified posterior fossa ependymoma (PF-EPN) into PF-EPN-A (PFA) and PF-EPN-B (PFB). A multivariate analysis using Cox regression confirmed that PFA was the sole molecular marker which was independently associated with patient survival. A clinically applicable pyrosequencing assay was developed to determine the PFB subgroup with 100% specificity using the methylation status of 3 genes, CRIP1, DRD4 and LBX2. Our results emphasized the significance of molecular classification in the diagnosis of ependymomas. RELA fusion-negative ST-EPN appear to be a heterogeneous group of tumors that do not fall into any of the existing molecular subgroups and are unlikely to form a single category.

Published
2018
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38. Characteristics and outcomes of elderly patients with diffuse gliomas: a multi-institutional cohort study by Kansai Molecular Diagnosis Network for CNS Tumors.

Author

Sasaki T, Fukai J, Kodama Y, Hirose T, Okita Y, Moriuchi S, Nonaka M, Tsuyuguchi N, Terakawa Y, Uda T, Tomogane Y, Kinoshita M, Nishida N, Izumoto S, Nakajima Y, Arita H, Ishibashi K, Shofuda T, Kanematsu D, Yoshioka E, Mano M, Fujita K, Uematsu Y, Nakao N, Mori K, and Kanemura Y

Subjects
Aged, Aged, 80 and over, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Brain Neoplasms genetics, Brain Neoplasms mortality, DNA Methylation, DNA Modification Methylases genetics, DNA Modification Methylases metabolism, DNA Repair Enzymes genetics, DNA Repair Enzymes metabolism, Female, Glioma genetics, Glioma mortality, Humans, Isocitrate Dehydrogenase genetics, Japan, Male, Mutation, Neoplasm Grading, Prognosis, Retrospective Studies, Telomerase genetics, Tumor Suppressor Proteins genetics, Tumor Suppressor Proteins metabolism, Brain Neoplasms metabolism, Brain Neoplasms therapy, Glioma metabolism, Glioma therapy
Abstract

Introduction: This study investigates the current state of clinical practice and molecular analysis for elderly patients with diffuse gliomas and aims to elucidate treatment outcomes and prognostic factors of patients with glioblastomas., Methods: We collected elderly cases (≥ 70 years) diagnosed with primary diffuse gliomas and enrolled in Kansai Molecular Diagnosis Network for CNS Tumors. Clinical and pathological characteristics were analyzed retrospectively. Various factors were evaluated in univariate and multivariate models to examine their effects on overall survival., Results: Included in the study were 140 elderly patients (WHO grade II: 7, III: 19, IV: 114), median age was 75 years. Sixty-seven patients (47.9%) had preoperative Karnofsky Performance Status score of ≥ 80. All patients underwent resection (gross-total: 20.0%, subtotal: 14.3%, partial: 39.3%, biopsy: 26.4%). Ninety-six of the patients (68.6%) received adjuvant treatment consisting of radiotherapy (RT) with temozolomide (TMZ). Seventy-eight of the patients (75.0%) received radiation dose of ≥ 50 Gy. MGMT promoter was methylated in 68 tumors (48.6%), IDH1/2 was wild-type in 129 tumors (92.1%), and TERT promoter was mutated in 78 of 128 tumors (60.9%). Median progression-free and overall survival of grade IV cases was 8.2 and 13.6 months, respectively. Higher age (≥ 80 years) and TERT promoter mutated were associated with shorter survival. Resection and adjuvant RT + TMZ were identified as independent factors for good prognosis., Conclusions: This community-based study reveals characteristics and outcomes of elderly glioma patients in a real-world setting. Elderly patients have several potential factors for poor prognosis, but resection followed by RT + TMZ could lengthen duration of survival.

Published
2018
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39. Lesion location implemented magnetic resonance imaging radiomics for predicting IDH and TERT promoter mutations in grade II/III gliomas.

Author

Arita H, Kinoshita M, Kawaguchi A, Takahashi M, Narita Y, Terakawa Y, Tsuyuguchi N, Okita Y, Nonaka M, Moriuchi S, Takagaki M, Fujimoto Y, Fukai J, Izumoto S, Ishibashi K, Nakajima Y, Shofuda T, Kanematsu D, Yoshioka E, Kodama Y, Mano M, Mori K, Ichimura K, and Kanemura Y

Subjects
Adult, Brain Neoplasms diagnostic imaging, Brain Neoplasms genetics, Brain Neoplasms mortality, Female, Glioma mortality, Humans, Kaplan-Meier Estimate, Male, Mutation genetics, Young Adult, Glioma diagnostic imaging, Glioma genetics, Isocitrate Dehydrogenase genetics, Magnetic Resonance Imaging methods, Promoter Regions, Genetic genetics, Telomerase genetics
Abstract

Molecular biological characterization of tumors has become a pivotal procedure for glioma patient care. The aim of this study is to build conventional MRI-based radiomics model to predict genetic alterations within grade II/III gliomas attempting to implement lesion location information in the model to improve diagnostic accuracy. One-hundred and ninety-nine grade II/III gliomas patients were enrolled. Three molecular subtypes were identified: IDH1/2-mutant, IDH1/2-mutant with TERT promoter mutation, and IDH-wild type. A total of 109 radiomics features from 169 MRI datasets and location information from 199 datasets were extracted. Prediction modeling for genetic alteration was trained via LASSO regression for 111 datasets and validated by the remaining 58 datasets. IDH mutation was detected with an accuracy of 0.82 for the training set and 0.83 for the validation set without lesion location information. Diagnostic accuracy improved to 0.85 for the training set and 0.87 for the validation set when lesion location information was implemented. Diagnostic accuracy for predicting 3 molecular subtypes of grade II/III gliomas was 0.74 for the training set and 0.56 for the validation set with lesion location information implemented. Conventional MRI-based radiomics is one of the most promising strategies that may lead to a non-invasive diagnostic technique for molecular characterization of grade II/III gliomas.

Published
2018
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40. Monitoring of methane emission from a landfill site in daily and hourly time scales using an automated gas sampling system.

Author

Izumoto S, Hamamoto S, Kawamoto K, Nagamori M, and Nishimura T

Subjects
Environmental Monitoring instrumentation, Japan, Refuse Disposal, Soil chemistry, Time Factors, Water analysis, Air Pollutants analysis, Environmental Monitoring methods, Methane analysis, Waste Disposal Facilities
Abstract

Landfill sites are significant sources of methane gas globally. Understanding the temporal variabilities of methane emissions from landfill sites is necessary for estimating such emissions. In this study, an automated monitoring system was used to monitor methane emission flux and concentration on daily and hourly time scales at a landfill site. Measured methane emission fluxes were almost negligible in the studied area. However, methane concentration at landfill surface at nighttime was significantly higher than those in the daytime, which demonstrates the importance of investigating methane emissions at an hourly time scale, including during nighttime. The daily and hourly variations in methane concentration were well correlated with either soil temperature or volumetric water content near the surface. The obtained relations indicate that the automated monitoring system measurements can facilitate a more comprehensive understanding of the methane emission mechanisms at different time scales.

Published
2018
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41. Seizures and Tumor Progression in Glioma Patients with Uncontrollable Epilepsy Treated with Perampanel.

Author

Izumoto S, Miyauchi M, Tasaki T, Okuda T, Nakagawa N, Nakano N, Kato A, and Fujita M

Subjects
Adult, Aged, Aged, 80 and over, Brain Neoplasms pathology, Disease Progression, Epilepsy etiology, Female, Glioma pathology, Humans, Male, Middle Aged, Nitriles, Retrospective Studies, Seizures drug therapy, Seizures etiology, Anticonvulsants therapeutic use, Brain Neoplasms complications, Epilepsy drug therapy, Glioma complications, Pyridones therapeutic use
Abstract

Background/aim: Excessive extracellular glutamate activates AMPA-type glutamate receptors (AMPA receptors) and induces seizures. Antagonistic activation of AMPA receptors inhibits epilepsy and glioma growth in in vitro and in vivo studies. This study was conducted to evaluate the clinical impacts of perampanel (PER), a novel AMPA receptor antagonist, on seizures and tumor progression in glioma patients with uncontrollable epilepsy., Patients and Methods: Twelve glioma patients with uncontrollable epilepsy were treated with PER. Seizure response, PER concentration, and tumor volume were assessed., Results: Obvious seizure control was observed in 10 analyzed patients (100%) and 6 patients (60%) became seizure-free. Median plasma concentrations of PER were 296 ng/ml in those with 4 mg/day PER treatment and 518 ng/ml in those with 8 mg/day PER treatment. High-intensity lesions in fluid-attenuated inversion recovery of magnetic resonance imaging (MRI) were volumetrically assessed to analyze tumor size. Volume reduction was detected within 6 months in correlation with increased plasma levels of PER., Conclusion: PER treatment was effective in uncontrollable epilepsy with gliomas. MRI images showed the inhibition of tumor growth., (Copyright© 2018, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published
2018
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42. Effects of Surgery With Salvage Stereotactic Radiosurgery Versus Surgery With Whole-Brain Radiation Therapy in Patients With One to Four Brain Metastases (JCOG0504): A Phase III, Noninferiority, Randomized Controlled Trial.

Author

Kayama T, Sato S, Sakurada K, Mizusawa J, Nishikawa R, Narita Y, Sumi M, Miyakita Y, Kumabe T, Sonoda Y, Arakawa Y, Miyamoto S, Beppu T, Sugiyama K, Nakamura H, Nagane M, Nakasu Y, Hashimoto N, Terasaki M, Matsumura A, Ishikawa E, Wakabayashi T, Iwadate Y, Ohue S, Kobayashi H, Kinoshita M, Asano K, Mukasa A, Tanaka K, Asai A, Nakamura H, Abe T, Muragaki Y, Iwasaki K, Aoki T, Watanabe T, Sasaki H, Izumoto S, Mizoguchi M, Matsuo T, Takeshima H, Hayashi M, Jokura H, Mizowaki T, Shimizu E, Shirato H, Tago M, Katayama H, Fukuda H, and Shibui S

Abstract

Purpose Whereas whole-brain radiotherapy (WBRT) has been the standard treatment of brain metastases (BMs), stereotactic radiosurgery (SRS) is increasingly preferred to avoid cognitive dysfunction; however, it has not been clearly determined whether treatment with SRS is as effective as that with WBRT or WBRT plus SRS. We thus assessed the noninferiority of salvage SRS to WBRT in patients with BMs. Patients and Methods Patients age 20 to 79 years old with performance status scores of 0 to 2-and 3 if caused only by neurologic deficits-and with four or fewer surgically resected BMs with only one lesion > 3 cm in diameter were eligible. Patients were randomly assigned to WBRT or salvage SRS arms within 21 days of surgery. The primary end point was overall survival. A one-sided α of .05 was used. Results Between January 2006 and May 2014, 137 and 134 patients were enrolled in the WBRT and salvage SRS arms, respectively. Median overall survival was 15.6 months in both arms (hazard ratio, 1.05; 90% CI, 0.83 to 1.33; one-sided P for noninferiority = .027). Median intracranial progression-free survival of patients in the WBRT arm (10.4 months) was longer than that of patients in the salvage SRS arm (4.0 months). The proportions of patients whose Mini-Mental Status Examination and performance status scores that did not worsen at 12 months were similar in both arms; however, 16.4% of patients in the WBRT arm experienced grade 2 to 4 cognitive dysfunction after 91 days postenrollment, whereas only 7.7% of those in the SRS arm did ( P = .048). Conclusion Salvage SRS is noninferior to WBRT and can be established as a standard therapy for patients with four or fewer BMs.

Published
2018
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43. Sensory axonal polyneuropathy due to 2,4-dinitrophenol.

Author

Izumoto S, Taniguchi A, Mochizuki H, Shiomi K, and Nakazato M

Subjects
Adult, Chemical and Drug Induced Liver Injury etiology, Humans, Japan, Male, Neural Conduction, Young Adult, 2,4-Dinitrophenol adverse effects, Anti-Obesity Agents adverse effects, Illicit Drugs adverse effects, Peripheral Nervous System Diseases chemically induced, Polyneuropathies chemically induced, Self Medication adverse effects, Somatosensory Disorders chemically induced
Abstract

A 24-year-old man developed subacute onset of numbness and pain in the upper and lower limbs. Physical examination demonstrated decreased pinprick sensation, but was otherwise normal. Blood and cerebrospinal fluid parameters were normal except for mild hepatic dysfunction. No data were suggestive of connective tissue disease. Nerve conduction studies demonstrated sensory neuropathy. A detailed medical interview revealed that the patient had been taking self-imported 2,4-dinitrophenol (DNP) for 2 months to decrease body weight. Six months after discontinuing DNP, subjective symptoms and liver dysfunction resolved completely, and the patient was diagnosed with drug-induced peripheral neuropathy and hepatopathy. There are no case reports of health risks posed by DNP in Japan, and even worldwide, cases of peripheral neuropathy due to DNP are rare. Obtaining a detailed drug history is important, as is providing information on the dangers of self-imported medicines.

Published
2017
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44. Efficacy of Combination Therapy with MET and VEGF Inhibitors for MET-overexpressing Glioblastoma.

Author

Okuda T, Tasaki T, Nakata S, Yamashita K, Yoshioka H, Izumoto S, Kato A, and Fujita M

Subjects
Animals, Bevacizumab pharmacology, Brain Neoplasms genetics, Cell Line, Tumor, Drug Synergism, Epithelial-Mesenchymal Transition, Gene Expression Regulation, Neoplastic drug effects, Glioblastoma genetics, Humans, Mice, Proto-Oncogene Proteins c-met antagonists & inhibitors, RNA, Small Interfering pharmacology, Treatment Outcome, Up-Regulation drug effects, Vascular Endothelial Growth Factor A genetics, Xenograft Model Antitumor Assays, Bevacizumab administration & dosage, Brain Neoplasms diet therapy, Glioblastoma drug therapy, Proto-Oncogene Proteins c-met genetics, RNA, Small Interfering administration & dosage, Vascular Endothelial Growth Factor A metabolism
Abstract

Background: Glioblastoma multiforme (GBM) is a malignant brain tumor with an extremely poor prognosis. GBM tissues frequently express mesenchymal-epithelial transition factor (MET), which induces cell division, growth and migration. In addition, angiogenesis is a significant feature of GBM, attributable to the overexpression of vascular endothelial growth factor (VEGF). Although the VEGF inhibitor bevacizumab was recently highlighted as the second-line drug for GBM treatment, GBMs often recur even with bevacizumab therapy. Based on these findings, we hypothesized that inhibition of both MET and VEGF would exhibit a synergistic effect on MET-overexpressing GBM., Materials and Methods: As we observed MET expression at high levels in some patients with GBM, we designed GL261 murine glioma-based experiments. GL261 cells were transfected with siRNAs specific for MET and VEGF in vitro, and the cell growth ratios were evaluated. Simultaneously, transfected GL261 cells were transplanted into the brain of C57BL/6 mice, and their survival was monitored., Results: GBM tissues frequently overexpressed MET protein at high levels compared with lower-grade gliomas. These GBMs at first responded to bevacizumab, but often eventually recurred. When GL261 cells were co-transfected with both MET-specific siRNA and VEGF-specific siRNA, the in vitro tumor cell growth significantly decelerated compared to single siRNA transfection. Consistently, when mice were transplanted with co-transfected GL261 cells, their survival was significantly prolonged compared to those given cells transfected with single siRNA., Conclusion: The current data indicate that the inhibition of both MET and VEGF exhibits efficient therapeutic effects of GBM-bearing hosts., (Copyright© 2017, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published
2017
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45. Association of WT1 IgG antibody against WT1 peptide with prolonged survival in glioblastoma multiforme patients vaccinated with WT1 peptide.

Author

Oji Y, Hashimoto N, Tsuboi A, Murakami Y, Iwai M, Kagawa N, Chiba Y, Izumoto S, Elisseeva O, Ichinohasama R, Sakamoto J, Morita S, Nakajima H, Takashima S, Nakae Y, Nakata J, Kawakami M, Nishida S, Hosen N, Fujiki F, Morimoto S, Adachi M, Iwamoto M, Oka Y, Yoshimine T, and Sugiyama H

Subjects
Adult, Aged, Biomarkers, Cancer Vaccines administration & dosage, Cell Line, Tumor, Combined Modality Therapy, Enzyme-Linked Immunosorbent Assay, Female, Glioblastoma therapy, HLA-A24 Antigen immunology, Humans, Immunoglobulin G blood, Immunotherapy, Male, Middle Aged, Peptides administration & dosage, Prognosis, T-Lymphocytes, Cytotoxic immunology, T-Lymphocytes, Cytotoxic metabolism, Th1 Cells immunology, Th1 Cells metabolism, Treatment Outcome, Vaccination, WT1 Proteins chemistry, Young Adult, Cancer Vaccines immunology, Glioblastoma immunology, Glioblastoma mortality, Immunoglobulin G immunology, Peptides immunology, WT1 Proteins immunology
Abstract

We previously evaluated Wilms' tumor gene 1 (WT1) peptide vaccination in a large number of patients with leukemia or solid tumors and have reported that HLA-A*24:02 restricted, 9-mer WT1-235 peptide (CYTWNQMNL) vaccine induces cellular immune responses and elicits WT1-235-specific cytotoxic T lymphocytes (CTLs). However, whether this vaccine induces humoral immune responses to produce WT1 antibody remains unknown. Thus, we measured IgG antibody levels against the WT1-235 peptide (WT1-235 IgG antibody) in patients with glioblastoma multiforme (GBM) receiving the WT1 peptide vaccine. The WT1-235 IgG antibody, which was undetectable before vaccination, became detectable in 30 (50.8%) of a total of 59 patients during 3 months of WT1 peptide vaccination. The dominant WT1-235 IgG antibody subclass was Th1-type, IgG1 and IgG3 . WT1-235 IgG antibody production was significantly and positively correlated with both progression-free survival (PFS) and overall survival (OS). Importantly, the combination of WT1-235 IgG antibody production and positive delayed type-hypersensitivity (DTH) to the WT1-235 peptide was a better prognostic marker for long-term OS than either parameter alone. These results suggested that WT1-235 peptide vaccination induces not only WT1-235-specific CTLs as previously described but also WT1-235-specific humoral immune responses associated with antitumor cellular immune response. Our results indicate that the WT1 IgG antibody against the WT1 peptide may be a useful predictive marker, with better predictive performance in combination with DTH to WT1 peptide, and provide a new insight into the antitumor immune response induction in WT1 peptide vaccine-treated patients., (© 2016 The Authors International Journal of Cancer published by John Wiley & Sons Ltd on behalf of UICC.)

Published
2016
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47. MET Expressed in Glioma Stem Cells Is a Potent Therapeutic Target for Glioblastoma Multiforme.

Author

Tasaki T, Fujita M, Okuda T, Yoneshige A, Nakata S, Yamashita K, Yoshioka H, Izumoto S, and Kato A

Subjects
Animals, Antineoplastic Agents, Brain Neoplasms drug therapy, Brain Neoplasms mortality, Brain Neoplasms pathology, Crizotinib, Female, Glioblastoma drug therapy, Glioblastoma mortality, Glioblastoma pathology, Humans, Male, Mice, Inbred NOD, Mice, SCID, Middle Aged, Molecular Targeted Therapy, Proto-Oncogene Mas, Pyrazoles pharmacology, Pyridines pharmacology, Xenograft Model Antitumor Assays, Brain Neoplasms enzymology, Glioblastoma enzymology, Neoplastic Stem Cells enzymology, Proto-Oncogene Proteins c-met metabolism
Abstract

Background: Glioblastoma multiforme (GBM) is the most frequent and the most malignant tumor among adult brain tumors. Previous reports led us to hypothesize that the proto-oncogene mesenchymal-epithelial transition (MET) expressed in glioma stem cell-like cells (GSCs) would be a potent therapeutic target for GBM., Patients and Methods: To address this question, we analyzed 113 original samples of tumors from patients based on immunohistochemistry. During this process, we were able to establish GSC lines from patients with GBM that were MET-positive and MET-negative. Using these cells, we tested the therapeutic impact of a MET inhibitor, crizotinib, both in vitro and in vivo., Results: Patients with MET-positive GBM exhibited poor survival. GSC-based experiments revealed that treatment with crizotinib, both in vitro and in vivo, exhibited therapeutic efficacy particularly against MET-positive GSCs., Conclusion: Based on these findings, we conclude that MET expressed in GSCs might be a potent therapeutic target for GBM., (Copyright© 2016 International Institute of Anticancer Research (Dr. John G. Delinassios), All rights reserved.)

Published
2016

48. Wilms tumor 1 peptide vaccination combined with temozolomide against newly diagnosed glioblastoma: safety and impact on immunological response.

Author

Hashimoto N, Tsuboi A, Kagawa N, Chiba Y, Izumoto S, Kinoshita M, Kijima N, Oka Y, Morimoto S, Nakajima H, Morita S, Sakamoto J, Nishida S, Hosen N, Oji Y, Arita N, Yoshimine T, and Sugiyama H

Subjects
Adult, Antineoplastic Combined Chemotherapy Protocols adverse effects, Brain Neoplasms drug therapy, Brain Neoplasms immunology, Cohort Studies, Combined Modality Therapy, Dacarbazine administration & dosage, Dacarbazine adverse effects, Disease Progression, Female, Glioblastoma drug therapy, Glioblastoma immunology, Humans, Male, Middle Aged, Temozolomide, WT1 Proteins adverse effects, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Brain Neoplasms therapy, Cancer Vaccines administration & dosage, Dacarbazine analogs & derivatives, Glioblastoma therapy, WT1 Proteins administration & dosage, WT1 Proteins immunology
Abstract

To investigate the safety of combined Wilms tumor 1 peptide vaccination and temozolomide treatment of glioblastoma, a phase I clinical trial was designed. Seven patients with histological diagnosis of glioblastoma underwent concurrent radiotherapy and temozolomide therapy. Patients first received Wilms tumor 1 peptide vaccination 1 week after the end of combined concurrent radio/temozolomide therapy, and administration was continued once per week for 7 weeks. Temozolomide maintenance was started and performed for up to 24 cycles, and the observation period for safety encompassed 6 weeks from the first administration of maintenance temozolomide. All patients showed good tolerability during the observation period. Skin disorders, such as grade 1/2 injection-site reactions, were observed in all seven patients. Although grade 3 lymphocytopenia potentially due to concurrent radio/temozolomide therapy was observed in five patients (71.4 %), no other grade 3/4 hematological or neurological toxicities were observed. No autoimmune reactions were observed. All patients are still alive, and six are on Wilms tumor 1 peptide vaccination without progression, yielding a progression-free survival from histological diagnosis of 5.2-49.1 months. Wilms tumor 1 peptide vaccination was stopped in one patient after 12 injections by the patient's request. The safety profile of the combined Wilms tumor 1 peptide vaccination and temozolomide therapy approach for treating glioblastoma was confirmed.

Published
2015
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50. The translation elongation factor eEF2 is a novel tumor‑associated antigen overexpressed in various types of cancers.

Author

Oji Y, Tatsumi N, Fukuda M, Nakatsuka S, Aoyagi S, Hirata E, Nanchi I, Fujiki F, Nakajima H, Yamamoto Y, Shibata S, Nakamura M, Hasegawa K, Takagi S, Fukuda I, Hoshikawa T, Murakami Y, Mori M, Inoue M, Naka T, Tomonaga T, Shimizu Y, Nakagawa M, Hasegawa J, Nezu R, Inohara H, Izumoto S, Nonomura N, Yoshimine T, Okumura M, Morii E, Maeda H, Nishida S, Hosen N, Tsuboi A, Oka Y, and Sugiyama H

Subjects
Antigens, Neoplasm metabolism, Cell Line, Tumor, Elongation Factor 2 Kinase metabolism, Gene Expression Regulation, Neoplastic, Gene Knockdown Techniques, Humans, Immunoglobulin G immunology, MCF-7 Cells, Neoplasms pathology, Sequence Analysis, DNA, T-Lymphocytes, Cytotoxic immunology, Antigens, Neoplasm genetics, Elongation Factor 2 Kinase genetics, Neoplasms genetics, Neoplasms immunology
Abstract

Recent studies have shown that cancer immunotherapy could be a promising therapeutic approach for the treatment of cancer. In the present study, to identify novel tumor-associated antigens (TAAs), the proteins expressed in a panel of cancer cells were serologically screened by immunoblot analysis and the eukaryotic elongation factor 2 (eEF2) was identified as an antigen that was recognized by IgG autoantibody in sera from a group of patients with head and neck squamous cell carcinoma (HNSCC) or colon cancer. Enzyme-linked immunosorbent assay showed that serum eEF2 IgG Ab levels were significantly higher in colorectal and gastric cancer patients compared to healthy individuals. Immunohistochemistry experiments showed that the eEF2 protein was overexpressed in the majority of lung, esophageal, pancreatic, breast and prostate cancers, HNSCC, glioblastoma multiforme and non-Hodgkin's lymphoma (NHL). Knockdown of eEF2 by short hairpin RNA (shRNA) significantly inhibited the growth in four eEF2-expressing cell lines, PC14 lung cancer, PCI6 pancreatic cancer, HT1080 fibrosarcoma and A172 glioblastoma cells, but not in eEF2-undetectable MCF7 cells. Furthermore, eEF2-derived 9-mer peptides, EF786 (eEF2 786-794 aa) and EF292 (eEF2 292-300 aa), elicited cytotoxic T lymphocyte (CTL) responses in peripheral blood mononuclear cells (PBMCs) from an HLA-A*24:02- and an HLA-A*02:01-positive healthy donor, respectively, in an HLA-A-restricted manner. These results indicated that the eEF2 gene is overexpressed in the majority of several types of cancers and plays an oncogenic role in cancer cell growth. Moreover, the eEF2 gene product is immunogenic and a promising target molecule of cancer immunotherapy for several types of cancers.

Published
2014
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