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Your search keyword '"Hwang, K"' showing total 65 results
Start Over Author "Hwang, K" Publisher elsevier b.v.
65 results on '"Hwang, K"'

2. Search for the Higgs boson decays to a ρ0, ϕ, or K⁎0 meson and a photon in proton-proton collisions at [formula omitted]

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Hayrapetyan, A., Tumasyan, A., Adam, W., Andrejkovic, J.W., Bergauer, T., Chatterjee, S., Damanakis, K., Dragicevic, M., Hussain, P.S., Jeitler, M., Krammer, N., Li, A., Liko, D., Mikulec, I., Schieck, J., Schöfbeck, R., Schwarz, D., Sonawane, M., Waltenberger, W., Wulz, C.-E., Janssen, T., Van Laer, T., Van Mechelen, P., Breugelmans, N., D'Hondt, J., Dansana, S., De Moor, A., Delcourt, M., Heyen, F., Lowette, S., Makarenko, I., Müller, D., Tavernier, S., Tytgat, M., Van Onsem, G.P., Van Putte, S., Vannerom, D., Bilin, B., Clerbaux, B., Das, A.K., De Lentdecker, G., Evard, H., Favart, L., Gianneios, P., Jaramillo, J., Khalilzadeh, A., Khan, F.A., Lee, K., Mahdavikhorrami, M., Malara, A., Paredes, S., Shahzad, M.A., Thomas, L., Vanden Bemden, M., Vander Velde, C., Vanlaer, P., De Coen, M., Dobur, D., Gokbulut, G., Hong, Y., Knolle, J., Lambrecht, L., Marckx, D., Mota Amarilo, K., Skovpen, K., Van Den Bossche, N., van der Linden, J., Wezenbeek, L., Benecke, A., Bethani, A., Bruno, G., Caputo, C., De Favereau De Jeneret, J., Delaere, C., Donertas, I.S., Giammanco, A., Guzel, A.O., Jain, Sa., Lemaitre, V., Lidrych, J., Mastrapasqua, P., Tran, T.T., Wertz, S., Alves, G.A., Alves Gallo Pereira, M., Coelho, E., Correia Silva, G., Hensel, C., Menezes De Oliveira, T., Mora Herrera, C., Moraes, A., Rebello Teles, P., Soeiro, M., Vilela Pereira, A., Aldá Júnior, W.L., Barroso Ferreira Filho, M., Brandao Malbouisson, H., Carvalho, W., Chinellato, J., Da Costa, E.M., Da Silveira, G.G., De Jesus Damiao, D., Fonseca De Souza, S., Gomes De Souza, R., Laux Kuhn, T., Macedo, M., Martins, J., Mundim, L., Nogima, H., Pinheiro, J.P., Santoro, A., Sznajder, A., Thiel, M., Bernardes, C.A., Calligaris, L., Fernandez Perez Tomei, T.R., Gregores, E.M., Maietto Silverio, I., Mercadante, P.G., Novaes, S.F., Orzari, B., Padula, Sandra S., Aleksandrov, A., Antchev, G., Hadjiiska, R., Iaydjiev, P., Misheva, M., Shopova, M., Sultanov, G., Dimitrov, A., Litov, L., Pavlov, B., Petkov, P., Petrov, A., Shumka, E., Keshri, S., Laroze, D., Thakur, S., Cheng, T., Javaid, T., Yuan, L., Hu, Z., Liang, Z., Liu, J., Chen, G.M., Chen, H.S., Chen, M., Iemmi, F., Jiang, C.H., Kapoor, A., Liao, H., Liu, Z.-A., Sharma, R., Song, J.N., Tao, J., Wang, C., Wang, J., Wang, Z., Zhang, H., Zhao, J., Agapitos, A., Ban, Y., Deng, S., Guo, B., Jiang, C., Levin, A., Li, C., Li, Q., Mao, Y., Qian, S., Qian, S.J., Qin, X., Sun, X., Wang, D., Yang, H., Zhang, L., Zhao, Y., Zhou, C., Yang, S., You, Z., Jaffel, K., Lu, N., Bauer, G., Li, B., Yi, K., Zhang, J., Gao, X., Li, Y., Lin, Z., Lu, C., Xiao, M., Avila, C., Barbosa Trujillo, D.A., Cabrera, A., Florez, C., Fraga, J., Reyes Vega, J.A., Ramirez, F., Rendón, C., Rodriguez, M., Ruales Barbosa, A.A., Ruiz Alvarez, J.D., Giljanovic, D., Godinovic, N., Lelas, D., Sculac, A., Kovac, M., Petkovic, A., Sculac, T., Bargassa, P., Brigljevic, V., Chitroda, B.K., Ferencek, D., Jakovcic, K., Starodumov, A., Susa, T., Attikis, A., Christoforou, K., Hadjiagapiou, A., Leonidou, C., Mousa, J., Nicolaou, C., Paizanos, L., Ptochos, F., Razis, P.A., Rykaczewski, H., Saka, H., Stepennov, A., Finger, M., Finger, M., Jr., Kveton, A., Ayala, E., Carrera Jarrin, E., Abdelalim, A.A., Elgammal, S., Ellithi Kamel, A., Mahmoud, M.A., Mohammed, Y., Ehataht, K., Kadastik, M., Lange, T., Nandan, S., Nielsen, C., Pata, J., Raidal, M., Tani, L., Veelken, C., Kirschenmann, H., Osterberg, K., Voutilainen, M., Bharthuar, S., Bin Norjoharuddeen, N., Brücken, E., Garcia, F., Inkaew, P., Kallonen, K.T.S., Lampén, T., Lassila-Perini, K., Lehti, S., Lindén, T., Myllymäki, M., Rantanen, M.m., Siikonen, H., Tuominiemi, J., Luukka, P., Petrow, H., Besancon, M., Couderc, F., Dejardin, M., Denegri, D., Faure, J.L., Ferri, F., Ganjour, S., Gras, P., Hamel de Monchenault, G., Kumar, M., Lohezic, V., Malcles, J., Orlandi, F., Portales, L., Rosowsky, A., Sahin, M.Ö., Savoy-Navarro, A., Simkina, P., Titov, M., Tornago, M., Beaudette, F., Boldrini, G., Busson, P., Cappati, A., Charlot, C., Chiusi, M., Damas, F., Davignon, O., De Wit, A., Ehle, I.T., Fontana Santos Alves, B.A., Ghosh, S., Gilbert, A., Granier de Cassagnac, R., Hakimi, A., Harikrishnan, B., Kalipoliti, L., Liu, G., Nguyen, M., Ochando, C., Salerno, R., Sauvan, J.B., Sirois, Y., Urda Gómez, L., Vernazza, E., Zabi, A., Zghiche, A., Agram, J.-L., Andrea, J., Apparu, D., Bloch, D., Brom, J.-M., Chabert, E.C., Collard, C., Falke, S., Goerlach, U., Haeberle, R., Le Bihan, A.-C., Meena, M., Poncet, O., Saha, G., Sessini, M.A., Van Hove, P., Vaucelle, P., Di Florio, A., Amram, D., Beauceron, S., Blancon, B., Boudoul, G., Chanon, N., Contardo, D., Depasse, P., Dozen, C., El Mamouni, H., Fay, J., Gascon, S., Gouzevitch, M., Greenberg, C., Grenier, G., Ille, B., Jourd‘huy, E., Laktineh, I.B., Lethuillier, M., Mirabito, L., Perries, S., Purohit, A., Vander Donckt, M., Verdier, P., Xiao, J., Lomidze, I., Toriashvili, T., Tsamalaidze, Z., Botta, V., Consuegra Rodríguez, S., Feld, L., Klein, K., Lipinski, M., Meuser, D., Pauls, A., Pérez Adán, D., Röwert, N., Teroerde, M., Diekmann, S., Dodonova, A., Eich, N., Eliseev, D., Engelke, F., Erdmann, J., Erdmann, M., Fackeldey, P., Fischer, B., Hebbeker, T., Hoepfner, K., Ivone, F., Jung, A., Lee, M.y., Mausolf, F., Merschmeyer, M., Meyer, A., Mukherjee, S., Noll, D., Nowotny, F., Pozdnyakov, A., Rath, Y., Redjeb, W., Rehm, F., Reithler, H., Sarkisovi, V., Schmidt, A., Seth, C., Sharma, A., Spah, J.L., Stein, A., Torres Da Silva De Araujo, F., Wiedenbeck, S., Zaleski, S., Dziwok, C., Flügge, G., Kress, T., Nowack, A., Pooth, O., Stahl, A., Ziemons, T., Zotz, A., Aarup Petersen, H., Aldaya Martin, M., Alimena, J., Amoroso, S., An, Y., Bach, J., Baxter, S., Bayatmakou, M., Becerril Gonzalez, H., Behnke, O., Belvedere, A., Blekman, F., Borras, K., Campbell, A., Cardini, A., Cheng, C., Colombina, F., Eckerlin, G., Eckstein, D., Estevez Banos, L.I., Filatov, O., Gallo, E., Geiser, A., Guglielmi, V., Guthoff, M., Hinzmann, A., Jeppe, L., Kaech, B., Kasemann, M., Kleinwort, C., Kogler, R., Komm, M., Krücker, D., Lange, W., Leyva Pernia, D., Lipka, K., Lohmann, W., Lorkowski, F., Mankel, R., Melzer-Pellmann, I.-A., Mendizabal Morentin, M., Meyer, A.B., Milella, G., Moral Figueroa, K., Mussgiller, A., Nair, L.P., Niedziela, J., Nürnberg, A., Otarid, Y., Park, J., Ranken, E., Raspereza, A., Rastorguev, D., Rübenach, J., Rygaard, L., Saggio, A., Scham, M., Schnake, S., Schütze, P., Schwanenberger, C., Selivanova, D., Sharko, K., Shchedrolosiev, M., Stafford, D., Vazzoler, F., Ventura Barroso, A., Walsh, R., Wang, Q., Wen, Y., Wichmann, K., Wiens, L., Wissing, C., Yang, Y., Zimermmane Castro Santos, A., Albrecht, A., Albrecht, S., Antonello, M., Bein, S., Benato, L., Bollweg, S., Bonanomi, M., Connor, P., El Morabit, K., Fischer, Y., Garutti, E., Grohsjean, A., Haller, J., Jabusch, H.R., Kasieczka, G., Keicher, P., Klanner, R., Korcari, W., Kramer, T., Kuo, C.c., Kutzner, V., Labe, F., Lange, J., Lobanov, A., Matthies, C., Moureaux, L., Mrowietz, M., Nigamova, A., Nissan, Y., Paasch, A., Pena Rodriguez, K.J., Quadfasel, T., Raciti, B., Rieger, M., Savoiu, D., Schindler, J., Schleper, P., Schröder, M., Schwandt, J., Sommerhalder, M., Stadie, H., Steinbrück, G., Tews, A., Wolf, M., Brommer, S., Burkart, M., Butz, E., Chwalek, T., Dierlamm, A., Droll, A., Elicabuk, U., Faltermann, N., Giffels, M., Gottmann, A., Hartmann, F., Hofsaess, R., Horzela, M., Husemann, U., Kieseler, J., Klute, M., Koppenhöfer, R., Lawhorn, J.M., Link, M., Lintuluoto, A., Maier, S., Mitra, S., Mormile, M., Müller, Th., Neukum, M., Oh, M., Pfeffer, E., Presilla, M., Quast, G., Rabbertz, K., Regnery, B., Shadskiy, N., Shvetsov, I., Simonis, H.J., Sowa, L., Stockmeier, L., Tauqeer, K., Toms, M., Trevisani, N., Von Cube, R.F., Wassmer, M., Wieland, S., Wittig, F., Wolf, R., Zuo, X., Anagnostou, G., Daskalakis, G., Kyriakis, A., Papadopoulos, A., Stakia, A., Kontaxakis, P., Melachroinos, G., Painesis, Z., Papavergou, I., Paraskevas, I., Saoulidou, N., Theofilatos, K., Tziaferi, E., Vellidis, K., Zisopoulos, I., Bakas, G., Chatzistavrou, T., Karapostoli, G., Kousouris, K., Papakrivopoulos, I., Siamarkou, E., Tsipolitis, G., Zacharopoulou, A., Adamidis, K., Bestintzanos, I., Evangelou, I., Foudas, C., Kamtsikis, C., Katsoulis, P., Kokkas, P., Kosmoglou Kioseoglou, P.G., Manthos, N., Papadopoulos, I., Strologas, J., Hajdu, C., Horvath, D., Márton, K., Rádl, A.J., Sikler, F., Veszpremi, V., Csanád, M., Farkas, K., Fehérkuti, A., Gadallah, M.M.A., Kadlecsik, Á., Major, P., Pásztor, G., Veres, G.I., Ujvari, B., Zilizi, G., Bencze, G., Czellar, S., Molnar, J., Szillasi, Z., Csorgo, T., Nemes, F., Novak, T., Bansal, S., Beri, S.B., Bhatnagar, V., Chaudhary, G., Chauhan, S., Dhingra, N., Kaur, A., Kaur, H., Kaur, M., Kumar, S., Sheokand, T., Singh, J.B., Singla, A., Ahmed, A., Bhardwaj, A., Chhetri, A., Choudhary, B.C., Kumar, A., Naimuddin, M., Ranjan, K., Saini, M.K., Saumya, S., Baradia, S., Barman, S., Bhattacharya, S., Das Gupta, S., Dutta, S., Sarkar, S., Ameen, M.M., Behera, P.K., Behera, S.C., Dash, G., Jana, P., Kalbhor, P., Kamble, S., Komaragiri, J.R., Kumar, D., Mishra, T., Parida, B., Pujahari, P.R., Saha, N.R., Sikdar, A.K., Singh, R.K., Verma, P., Verma, S., Vijay, A., Dugad, S., Mohanty, G.B., Shelake, M., Suryadevara, P., Bala, A., Banerjee, S., Chatterjee, R.M., Guchait, M., Jain, Sh., Jaiswal, A., Majumder, G., Mazumdar, K., Parolia, S., Thachayath, A., Bahinipati, S., Kar, C., Maity, D., Mal, P., Muraleedharan Nair Bindhu, V.K., Naskar, K., Nayak, A., Nayak, S., Pal, K., Sadangi, P., Swain, S.K., Varghese, S., Vats, D., Acharya, S., Alpana, A., Dube, S., Gomber, B., Hazarika, P., Kansal, B., Laha, A., Sahu, B., Sharma, S., Vaish, K.Y., Bakhshiansohi, H., Jafari, A., Zeinali, M., Bashiri, S., Chenarani, S., Etesami, S.M., Hosseini, Y., Khakzad, M., Khazaie, E., Mohammadi Najafabadi, M., Tizchang, S., Felcini, M., Grunewald, M., Abbrescia, M., Colaleo, A., Creanza, D., D'Anzi, B., De Filippis, N., De Palma, M., Elmetenawee, W., Fiore, L., Iaselli, G., Longo, L., Louka, M., Maggi, G., Maggi, M., Margjeka, I., Mastrapasqua, V., My, S., Nuzzo, S., Pellecchia, A., Pompili, A., Pugliese, G., Radogna, R., Ramos, D., Ranieri, A., Silvestris, L., Simone, F.M., Sözbilir, Ü., Stamerra, A., Troiano, D., Venditti, R., Verwilligen, P., Zaza, A., Abbiendi, G., Battilana, C., Bonacorsi, D., Capiluppi, P., Castro, A., Cavallo, F.R., Cuffiani, M., Dallavalle, G.M., Diotalevi, T., Fabbri, F., Fanfani, A., Fasanella, D., Giacomelli, P., Giommi, L., Grandi, C., Guiducci, L., Lo Meo, S., Lorusso, M., Lunerti, L., Marcellini, S., Masetti, G., Navarria, F.L., Paggi, G., Perrotta, A., Primavera, F., Rossi, A.M., Rossi Tisbeni, S., Rovelli, T., Siroli, G.P., Costa, S., Di Mattia, A., Lapertosa, A., Potenza, R., Tricomi, A., Tuve, C., Assiouras, P., Barbagli, G., Bardelli, G., Camaiani, B., Cassese, A., Ceccarelli, R., Ciulli, V., Civinini, C., D'Alessandro, R., Focardi, E., Kello, T., Latino, G., Lenzi, P., Lizzo, M., Meschini, M., Paoletti, S., Papanastassiou, A., Sguazzoni, G., Viliani, L., Benussi, L., Bianco, S., Meola, S., Piccolo, D., Chatagnon, P., Ferro, F., Robutti, E., Tosi, S., Benaglia, A., Brivio, F., Cetorelli, F., De Guio, F., Dinardo, M.E., Dini, P., Gennai, S., Gerosa, R., Ghezzi, A., Govoni, P., Guzzi, L., Lucchini, M.T., Malberti, M., Malvezzi, S., Massironi, A., Menasce, D., Moroni, L., Paganoni, M., Palluotto, S., Pedrini, D., Perego, A., Pinolini, B.S., Pizzati, G., Ragazzi, S., Tabarelli de Fatis, T., Buontempo, S., Cagnotta, A., Carnevali, F., Cavallo, N., Fabozzi, F., Iorio, A.O.M., Lista, L., Paolucci, P., Rossi, B., Ardino, R., Azzi, P., Bacchetta, N., Bisello, D., Bortignon, P., Bortolato, G., Bragagnolo, A., Bulla, A.C.M., Carlin, R., Checchia, P., Dorigo, T., Gasparini, F., Gasparini, U., Giorgetti, S., Lusiani, E., Margoni, M., Meneguzzo, A.T., Migliorini, M., Montecassiano, F., Pazzini, J., Ronchese, P., Rossin, R., Simonetto, F., Tosi, M., Triossi, A., Ventura, S., Zotto, P., Zucchetta, A., Zumerle, G., Braghieri, A., Calzaferri, S., Fiorina, D., Montagna, P., Re, V., Riccardi, C., Salvini, P., Vai, I., Vitulo, P., Ajmal, S., Ascioti, M.E., Bilei, G.M., Carrivale, C., Ciangottini, D., Fanò, L., Magherini, M., Mariani, V., Menichelli, M., Moscatelli, F., Rossi, A., Santocchia, A., Spiga, D., Tedeschi, T., Aimè, C., Alexe, C.A., Asenov, P., Azzurri, P., Bagliesi, G., Bhattacharya, R., Bianchini, L., Boccali, T., Bossini, E., Bruschini, D., Castaldi, R., Ciocci, M.A., Cipriani, M., D'Amante, V., Dell'Orso, R., Donato, S., Giassi, A., Ligabue, F., Marini, A.C., Matos Figueiredo, D., Messineo, A., Mishra, S., Musich, M., Palla, F., Rizzi, A., Rolandi, G., Roy Chowdhury, S., Sarkar, T., Scribano, A., Spagnolo, P., Tenchini, R., Tonelli, G., Turini, N., Vaselli, F., Venturi, A., Verdini, P.G., Baldenegro Barrera, C., Barria, P., Basile, C., Cavallari, F., Cunqueiro Mendez, L., Del Re, D., Di Marco, E., Diemoz, M., Errico, F., Gargiulo, R., Longo, E., Martikainen, L., Mijuskovic, J., Organtini, G., Pandolfi, F., Paramatti, R., Quaranta, C., Rahatlou, S., Rovelli, C., Santanastasio, F., Soffi, L., Amapane, N., Arcidiacono, R., Argiro, S., Arneodo, M., Bartosik, N., Bellan, R., Bellora, A., Biino, C., Borca, C., Cartiglia, N., Costa, M., Covarelli, R., Demaria, N., Finco, L., Grippo, M., Kiani, B., Legger, F., Luongo, F., Mariotti, C., Markovic, L., Maselli, S., Mecca, A., Menzio, L., Meridiani, P., Migliore, E., Monteno, M., Mulargia, R., Obertino, M.M., Ortona, G., Pacher, L., Pastrone, N., Pelliccioni, M., Ruspa, M., Siviero, F., Sola, V., Solano, A., Staiano, A., Tarricone, C., Trocino, D., Umoret, G., White, R., Babbar, J., Belforte, S., Candelise, V., Casarsa, M., Cossutti, F., De Leo, K., Della Ricca, G., Dogra, S., Hong, J., Kim, B., Kim, J., Lee, D., Lee, H., Lee, S.W., Moon, C.S., Oh, Y.D., Ryu, M.S., Sekmen, S., Tae, B., Yang, Y.C., Kim, M.S., Bak, G., Gwak, P., Kim, H., Moon, D.H., Asilar, E., Choi, J., Kim, D., Kim, T.J., Merlin, J.A., Ryou, Y., Choi, S., Han, S., Hong, B., Lee, K.S., Lee, S., Yoo, J., Goh, J., Kim, H.S., Kim, Y., Almond, J., Bhyun, J.H., Jun, W., Kim, Y.W., Ko, S., Kwon, H., Lee, J., Oh, B.H., Oh, S.B., Seo, H., Yang, U.K., Yoon, I., Jang, W., Kang, D.Y., Kang, Y., Kim, S., Ko, B., Lee, J.S.H., Lee, Y., Park, I.C., Roh, Y., Watson, I.J., Ha, S., Hwang, K., Yoo, H.D., Choi, M., Kim, M.R., Yu, I., Beyrouthy, T., Gharbia, Y., Alazemi, F., Dreimanis, K., Gaile, A., Munoz Diaz, C., Osite, D., Pikurs, G., Potrebko, A., Seidel, M., Sidiropoulos Kontos, D., Strautnieks, N.R., Ambrozas, M., Juodagalvis, A., Rinkevicius, A., Tamulaitis, G., Yusuff, I., Zolkapli, Z., Benitez, J.F., Castaneda Hernandez, A., Encinas Acosta, H.A., Gallegos Maríñez, L.G., León Coello, M., Murillo Quijada, J.A., Sehrawat, A., Valencia Palomo, L., Ayala, G., Castilla-Valdez, H., Crotte Ledesma, H., De La Cruz-Burelo, E., Heredia-De La Cruz, I., Lopez-Fernandez, R., Mejia Guisao, J., Mondragon Herrera, C.A., Sánchez Hernández, A., Oropeza Barrera, C., Ramirez Guadarrama, D.L., Ramírez García, M., Bautista, I., Pedraza, I., Salazar Ibarguen, H.A., Uribe Estrada, C., Bubanja, I., Raicevic, N., Butler, P.H., Ahmad, A., Asghar, M.I., Awais, A., Awan, M.I.M., Hoorani, H.R., Khan, W.A., Avati, V., Grzanka, L., Malawski, M., Bialkowska, H., Bluj, M., Górski, M., Kazana, M., Szleper, M., Zalewski, P., Bunkowski, K., Doroba, K., Kalinowski, A., Konecki, M., Krolikowski, J., Muhammad, A., Pozniak, K., Zabolotny, W., Araujo, M., Bastos, D., Beirão Da Cruz E Silva, C., Boletti, A., Bozzo, M., Camporesi, T., Da Molin, G., Faccioli, P., Gallinaro, M., Hollar, J., Leonardo, N., Marozzo, G.B., Niknejad, T., Petrilli, A., Pisano, M., Seixas, J., Varela, J., Wulff, J.W., Adzic, P., Milenovic, P., Devetak, D., Dordevic, M., Milosevic, J., Nadderd, L., Rekovic, V., Alcaraz Maestre, J., Bedoya, Cristina F., Brochero Cifuentes, J.A., Carretero, Oliver M., Cepeda, M., Cerrada, M., Colino, N., De La Cruz, B., Delgado Peris, A., Escalante Del Valle, A., Fernández Del Val, D., Fernández Ramos, J.P., Flix, J., Fouz, M.C., Gonzalez Lopez, O., Goy Lopez, S., Hernandez, J.M., Josa, M.I., Llorente Merino, J., Martin Viscasillas, E., Moran, D., Morcillo Perez, C.M., Navarro Tobar, Á., Perez Dengra, C., Pérez-Calero Yzquierdo, A., Puerta Pelayo, J., Redondo, I., Sánchez Navas, S., Sastre, J., Vazquez Escobar, J., de Trocóniz, J.F., Alvarez Gonzalez, B., Cuevas, J., Fernandez Menendez, J., Folgueras, S., Gonzalez Caballero, I., Leguina, P., Palencia Cortezon, E., Prado Pico, J., Ramón Álvarez, C., Rodríguez Bouza, V., Soto Rodríguez, A., Trapote, A., Vico Villalba, C., Vischia, P., Bhowmik, S., Blanco Fernández, S., Cabrillo, I.J., Calderon, A., Duarte Campderros, J., Fernandez, M., Gomez, G., Lasaosa García, C., Lopez Ruiz, R., Martinez Rivero, C., Martinez Ruiz del Arbol, P., Matorras, F., Matorras Cuevas, P., Navarrete Ramos, E., Piedra Gomez, J., Scodellaro, L., Vila, I., Vizan Garcia, J.M., Kailasapathy, B., Wickramarathna, D.D.C., Dharmaratna, W.G.D., Liyanage, K., Perera, N., Abbaneo, D., Amendola, C., Auffray, E., Auzinger, G., Baechler, J., Barney, D., Bermúdez Martínez, A., Bianco, M., Bin Anuar, A.A., Bocci, A., Borgonovi, L., Botta, C., Brondolin, E., Caillol, C., Cerminara, G., Chernyavskaya, N., d'Enterria, D., Dabrowski, A., David, A., De Roeck, A., Defranchis, M.M., Deile, M., Dobson, M., Franzoni, G., Funk, W., Giani, S., Gigi, D., Gill, K., Glege, F., Hegeman, J., Heikkilä, J.K., Huber, B., Innocente, V., James, T., Janot, P., Kaluzinska, O., Karacheban, O., Laurila, S., Lecoq, P., Leutgeb, E., Lourenço, C., Malgeri, L., Mannelli, M., Matthewman, M., Mehta, A., Meijers, F., Mersi, S., Meschi, E., Milosevic, V., Monti, F., Moortgat, F., Mulders, M., Neutelings, I., Orfanelli, S., Pantaleo, F., Petrucciani, G., Pfeiffer, A., Pierini, M., Qu, H., Rabady, D., Ribeiro Lopes, B., Rovere, M., Sakulin, H., Sanchez Cruz, S., Scarfi, S., Schwick, C., Selvaggi, M., 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Warden, A., Afanasiev, S., Alexakhin, V., Budkouski, D., Golutvin, I., Gorbunov, I., Karjavine, V., Korenkov, V., Lanev, A., Malakhov, A., Matveev, V., Palichik, V., Perelygin, V., Savina, M., Shalaev, V., Shmatov, S., Shulha, S., Smirnov, V., Teryaev, O., Voytishin, N., Yuldashev, B.S., Zarubin, A., Zhizhin, I., Gavrilov, G., Golovtcov, V., Ivanov, Y., Kim, V., Levchenko, P., Murzin, V., Oreshkin, V., Sosnov, D., Sulimov, V., Uvarov, L., Vorobyev, A., Andreev, Yu., Dermenev, A., Gninenko, S., Golubev, N., Karneyeu, A., Kirpichnikov, D., Kirsanov, M., Krasnikov, N., Tlisova, I., Toropin, A., Aushev, T., Gavrilov, V., Lychkovskaya, N., Nikitenko, A., Popov, V., Zhokin, A., Chadeeva, M., Chistov, R., Polikarpov, S., Andreev, V., Azarkin, M., Kirakosyan, M., Terkulov, A., Boos, E., Bunichev, V., Dubinin, M., Dudko, L., Ershov, A., Gribushin, A., Klyukhin, V., Kodolova, O., Obraztsov, S., Petrushanko, S., Savrin, V., Snigirev, A., Blinov, V., Dimova, T., Kozyrev, A., Radchenko, O., Skovpen, Y., Kachanov, V., Konstantinov, D., Slabospitskii, S., Uzunian, A., Babaev, A., Borshch, V., Druzhkin, D., Chekhovsky, V., and Makarenko, V.

Published
2025
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3. Dissemination of meticillin-resistant Staphylococcus aureus sequence type 8 (USA300) in Taiwan.

Author

Huang, Y-C., Chen, C-J., Kuo, A-J., Hwang, K-R., Chien, C-C., Lee, C-Y., Wu, T-H., Ko, W-C., and Hsueh, P-R.

Abstract

In Taiwan, sequence type (ST) 239 and ST59 were two major clones among meticillin-resistant Staphylococcus aureus (MRSA) clinical isolates in the past two decades. USA300 (ST8) prevailed in the Americas but not in outside areas. Recently USA300 (ST8) emerged and was increasingly identified in Taiwan; we thus conducted an island-wide study to explore the role of USA300 among MRSA isolates. One hundred MRSA bloodstream isolates identified in 2020 from each of the six participating hospitals in Taiwan were collected and characterized. The first 10 ST8 isolates from each hospital were further analysed by whole-genome sequencing. Of the 590 confirmed MRSA isolates, a total of 22 pulsotypes and 21 STs were identified. The strain of pulsotype AI/ST8 was the most common lineage identified, accounting for 187 isolates (31.7%) and dominating in five of six hospitals, followed by pulsotype A/ST239 (14.7%), pulsotype C/ST59 (13.9%) and pulsotype D/ST59 (9.2%). Of the 187 pulsotype AI/ST8 isolates, 184 isolates were characterized as USA300 and clustered in three major sub-pulsotypes, accounting for 78%. Ninety per cent of the 60 ST8 isolates for whole-genome sequencing were clustered in three major clades. In 2020, USA300 became the most common clone of MRSA in Taiwan, accounting for >30% of MRSA bloodstream isolates island wide. Most of USA300 isolates circulating in Taiwan might have been imported on multiple occasions and evolved into at least three successful local clades. MRSA USA300 has successfully established its role in Taiwan, an area outside of the Americas. [ABSTRACT FROM AUTHOR]

Published
2024
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12. Effects of soy sauce on physicochemical and textural properties of tumbled chicken breast.

Author

Kim, H. W., Hwang, K. E., Song, D. H., Kim, Y. J., Lim, Y. B., Choi, J. H., Choi, Y. S., Kim, H. Y., and Kim, C. J.

Subjects
*SOY sauce, *CHICKEN as food, *DISTILLED water, *LACTIC acid, *SALT, *MARINADES, *SOLUBILITY
Abstract

The objective of this study was to evaluate the effects of soy sauce on the physicochemical and textural properties of tumbled chicken breasts. Chicken breasts marinated with distilled water (Con), 4% NaCl solution, 4% NaCl and lactic acid solution (pH 4.9), and soy sauce solution (4% salt concentration and pH 4.9) were vacuum tumbled at 3°C for 60 min. The chicken breast marinated with soy sauce solution showed lower lightness and higher redness and yellowness due to the color of the soy sauce. The acidic marinades led to a decrease in pH value of tumbled chicken breast. The acidic marinades increased collagen solubility of sample compared with 4% NaCl solution, resulting in decreased shear force. Water-holding capacity, marination and cooking yields, and solubility of myofibrillar proteins were mainly affected by the presence of salt in the marinade, rather than by pH alternation. Our results suggested that soy sauce marination can improve the tenderness of tumbled chicken breast. [ABSTRACT FROM PUBLISHER]

Published
2014
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13. Evaluation of the antioxidant effect of ganghwayakssuk (Artemisia princeps Pamp.) extract alone and in combination with ascorbic acid in raw chicken patties.

Author

Hwang, K. E., Kim, H. W., Choi, Y. S., Lee, S. Y., Yeo, E. J., Ham, Y. K., Choi, S. M., Lee, M. A., and Kim, C. J.

Subjects
*ARTEMISIA, *PLANT extracts, *ANTIOXIDANTS, *VITAMIN C in animal nutrition, *OXIDATIVE stress, *LIPID metabolism
Abstract

We investigated the inhibition of lipid oxi-dation of raw chicken patties by the antioxidants ascor-bic acid (Aa), ganghwayakssuk ex tracts (GE), and their combination (Aa + GE). All antioxidant combinations were effective at delaying lipid oxidation compared with the control or Aa. A combination of Aa + GE (0.05% Aa + 0.2% GE) was the most effective for delaying lipid oxidation (TBA reactive substances, conjugated dienes, and peroxide formation). The color values of all samples were significantly affected by adding GE. Additionally, the redness, color difference, and hue values of all treatments, except for Aa, were lower than those of the control as the amount of GE increased. The total viable bacterial counts of samples with GE 0.2 and Aa + GE 0.2 were significantly affected during storage (P < 0.05). The results suggest that adding an antioxidant combination reduced the oxidative stress and microbial growth of raw chicken patties stored for 12 d under nor-mal refrigeration temperature, which may extend the shelf life of chicken patties. [ABSTRACT FROM AUTHOR]

Published
2013
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14. Identification and characterization of a novel mouse and human MOPT gene containing MORN-motif protein in testis

Author

Choi, Y-J., Hwang, K-C., Park, J-Y., Park, K-K., Kim, J-H., Park, S-B., Hwang, S., Park, H., and Park, C.

Subjects
*LABORATORY mice, *TESTIS, *PROTEINS, *CELL membranes, *CHROMOSOMES, *SPERMIOGENESIS in animals, *GENE expression
Abstract

Abstract: A novel testis-derived membrane occupation and recognition nexus (MORN)-motif protein was identified in mouse testis (MOPT) by subtraction screening methods and found to be localized on chromosome 17E3, spanning approximately 7kb. Sequence analysis showed that MOPT contains 669 base pair nucleotides of open reading frame and the corresponding 79 amino acids. The protein is predicted to have theoretical molecular mass of 9000 Da and an expected isoelectric point of 5.8 and seems to have unique sequences except for MORN-motif domain. The transcript of MOPT is highly and specifically expressed in adult testis as well as skeletal muscle. Moreover, MOPT transcript and protein are confined mainly to round and elongated spermatids, except for a few individual dispersed spermatocytes, and increase in abundance at subsequent stages. MOPT first appeared in the proacrosomic vesicles of the early Golgi phase spermatids and was translocated from the head cap of elongated spermatid to the nucleus of mature spermatozoa at the final stage of spermiogenesis. Our study suggests that MOPT may play an important role in dynamic regulation of acrosome biogenesis during late spermiogenesis. [Copyright &y& Elsevier]

Published
2010
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15. Anatomic variations of the infraorbital fat compartment.

Author

Oh, C.S., Chung, I.H., Kim, Y.S., Hwang, K., and Nam, K.I.

Subjects
SURGICAL excision, FAT, BLEPHAROPLASTY, EYELID surgery, PLASTIC surgery
Abstract

Summary: Resection of the infraorbital fat is performed in blepharoplasty of the lower eyelid, however, the previous anatomical reports on its compartmentalization have been in disagreement. The aim of this study was to classify the infraorbital fat based on the extent of compartmentalization, and to clarify its topographic relationship with the surrounding structures. Sixty orbits from 30 cadavers were dissected. The infraorbital fat was classified into four types based on its compartmentalization. In type I, which was the most common type (60.0%), the infraorbital fat was compartmentalised into three encapsulated medial, central, and lateral parts, which were side by side. In type II (11.7%), the medial or lateral compartment, or both compartments were under the central fat compartment. In type III (26.7%), there were two compartments, the medial and remaining part or the lateral and remaining part. In type IV (1.7%), the fat was not compartmentalised, but presented as a single pad. The average heights from the inferior orbital rim, the average widths, and the average distances from the fornix were 7.3, 17.2, and 7.1mm in the medial compartment, 8.9, 24.2, and 8.0mm in the central compartment, and 8.1, 17.2, and 6.9mm in the lateral compartment, respectively. The average distance from the end of the margin of the stretched lower eyelid to the most cephalic point in the compartments was 8.6mm. These results are relevant to blepharoplasty with removal of the infraorbital fat. [Copyright &y& Elsevier]

Published
2006
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16. Expression of Inflammatory Cytokines in Pigs Experimentally Infected with Mycoplasma hyopneumoniae.

Author

Choi, C., Kwon, D., Jung, K., Ha, Y., Lee, Y.-H., Kim, O., Park, H.-K., Kim, S.-H., Hwang, K.-K., and Chae, C.

Subjects
CYTOKINES, CELLULAR immunity, LUNGS, TUMORS
Abstract

Summary: The expression of interleukin-1 (IL-1), tumour necrosis factor-α (TNF-α) and IL-6 were studied over a period of 35 days in the lungs of pigs experimentally infected with Mycoplasma hyopneumoniae, by semiquantitative reverse transcription-polymerase chain reaction (RT-PCR), morphometric analysis and in-situ hybridization. Fifteen colostrum-deprived pigs aged 14 days were inoculated intranasally with M. hyopneumoniae. IL-1, TNF-α and IL-6 were detected by RT-PCR in the lungs of the infected pigs from 7 days post-inoculation (dpi) onwards, but not in the uninfected control pigs. Concurrent expression of all three cytokines was always observed, in association with lung lesions. Inflammatory cytokine-positive cells were detected in the lungs at 7 dpi, their number increasing at 21dpi, and decreasing thereafter. The results suggest that such cytokines play a role in mediating and regulating inflammation in M. hyopneumoniae infection. [Copyright &y& Elsevier]

Published
2006
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17. Synthetic Peptide-derived Antibody-based Immunohistochemistry for the Detection of Porcine Circovirus 2 in Pigs with Postweaning Multisystemic Wasting Syndrome.

Author

Ha, Y., Jung, K., Choi, C., Hwang, K.-K., and Chae, C.

Subjects
SWINE diseases, VIRUSES, FORMALDEHYDE, PARAFFIN wax, LYMPH nodes
Abstract

Summary: Porcine circovirus 2 (PCV2) was detected consistently in formalin-fixed paraffin wax-embedded lymph node and spleen from experimentally and naturally infected pigs by synthetic peptide-derived polyclonal antibody-based immunohistochemistry. Synthetic peptides were generated from open reading frame 2 of PCV2 by solid-phase peptide synthesis, purified by high performance liquid chromatography, and injected into rabbits to produce polyclonal antibody. Positive cells had large nuclei with abundant cytoplasm, and resembled macrophages. In serial sections, a similar distribution of PCV2 antigen and DNA was confirmed in virus-infected cells by immunohistochemistry and in-situ hybridization, respectively. The immunohistochemical method described was successfully applied to formalin-fixed, paraffin wax-embedded tissues and should prove helpful in diagnosing postweaning multisystemic wasting syndrome. [Copyright &y& Elsevier]

Published
2005
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18. Active insulin infusion using optimal and derivative-weighted control

Author

Lam, Z.-H., Hwang, K.-S., Lee, J.-Y., Chase, J.G., and Wake, G.C.

Subjects
*DIABETES, *INSULIN
Abstract

Close control of blood glucose levels significantly reduces vascular complications in Type I diabetes. A control method for the automation of insulin infusion that utilizes emerging technologies in blood glucose biosensors is presented. The controller developed provides tighter, more optimal control of blood glucose levels, while accounting for variation in patient response, insulin employed and sensor bandwidth. Particular emphasis is placed on controller simplicity and robustness necessary for medical devices and implants.A PD controller with heavy emphasis on the derivative term is found to outperform the typically used proportional-weighted controllers in glucose tolerance and multi-meal tests. Simulation results show reductions of over 50% in the magnitude and duration of blood glucose excursions from basal levels. A closed-form steady state optimal solution is also developed as a benchmark, and results in a flat glucose response. The impact and trade-offs associated with sensor bandwidth, sensor lag and proportional versus derivative-based control methods are illustrated. Overall, emerging blood glucose sensor technologies that enable frequent measurement are shown to enable more effective, automated control of blood glucose levels within a tight, acceptable range for Type I and II diabetic individuals. [Copyright &y& Elsevier]

Published
2002
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20. 5PLong-term prognostic effect of hormone receptor subtype on breast cancer.

Author

Hwang, K-T

Subjects
*HORMONE receptors, *BREAST cancer, *PROGESTERONE receptors, *ESTROGEN receptors, *HORMONE receptor positive breast cancer, *CANCER-related mortality
Abstract

Background To determine the long-term prognostic role of hormone receptor subtype in breast cancer using the Surveillance, Epidemiology, and End Results (SEER) database. Methods Data of 810,587 female operable invasive breast cancer patients from SEER database with a mean follow-up period of 94.2 months (range, 0-311 months) were analyzed. Hormone receptor subtype was classified into four groups based on estrogen receptor (ER) and progesterone receptor (PR) statuses: ER(+)/PR(+), ER(+)/PR(-), ER(-)/PR(+), and ER(-)/PR(-). Results Numbers of subjects with ER(+)/PR(+), ER(+)/PR(-), ER(-)/PR(+), ER(-)/PR(-), and unknown were 496,279 (61.2%), 86,858 (10.7%), 11,545 (1.4%), 135,441 (16.7%), and 80,464 (9.9%), respectively. The ER(+)/PR(+) subtype showed the best breast cancer specific survival, followed by ER(+)/PR(-), ER(-)/PR(+), and ER(-)/PR(-) subtypes in order (all p < 0.001). Survival difference among hormone receptor subtypes was maintained in subgroup analysis according to anatomic stage, race, age group, and year of diagnosis. Hormone receptor subtype was a significant independent prognostic factor in multivariable analyses (p < 0.001). Hazard ratios of ER(+)/PR(-), ER(-)/PR(+), and ER(-)/PR(-) for breast cancer specific mortality risk were 1.419 (95% confidence interval [CI], 1.383-1.456), 1.630 (95% CI, 1.537-1.729), and 1.811 (95% CI, 1.773-1.848), respectively, with ER(+)/PR(+) as reference. Conclusions Hormone receptor subtype is a significant independent prognostic factor in female operable invasive breast cancer with long-term effect. The ER(+)/PR(+) subtype shows the most favorable prognosis, followed by ER(+)/PR(-), ER(-)/PR(+), and ER(-)/PR(-) subtypes in order. Prognostic impacts of hormone receptor subtypes are also maintained in subgroup analysis according to anatomic stage, race, age, and year of diagnosis. Legal entity responsible for the study The author. Funding Has not received any funding. Disclosure The author has declared no conflicts of interest. [ABSTRACT FROM AUTHOR]

Published
2019
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37. Short communication: retinoic acid plus prolactin to synergistically increase specific casein gene expression in MAC-T cells.

Author

Lee, H. Y., Heo, Y. T., Lee, S. E., Hwang, K. C., Lee, H. G., Choi, S. H., and Kim, N. H.

Subjects
*TRETINOIN, *EPITHELIAL cells, *CELL lines, *CASEINS, *PROLACTIN, *GENE expression
Abstract

Mammary alveolar (MAC-T) cells, an established bovine mammary epithelial cell line, are frequently used to investigate differentiation. A lactogenic phenotype in these cells is induced by treatment with a combination of hydrocortisone, insulin, and prolactin (PRL). The effect of the vitamin A derivative retinoic acid (RA), which induces differentiation in many cells, has not been studied in MAC-T cells. The objective of this study was to evaluate the differentiation potential of RA (1 µM) in MAC-T cells and to examine the effect of combined treatment with RA (1 µM) and PRL (5 µg/ mL). Although RA treatment alone inhibited MAC-T cell proliferation, co-treatment of RA with PRL increased cell growth compared with the control group (treated with 1 µg/mL hydrocortisone and 5 µg/mL insulin). The ratio of Bcl to Bax mRNA was decreased in the RA treatment compared with RA+PRL or control. Retinoic acid--induced differentiation of MAC-T cells was associated with an increase in the mRNA expression of αS1-casein (3.9-fold), αS2-casein (4.5-fold), and β-casein (4.4-fold) compared with the control group. Expression of αS1-casein, αS2-casein, and β-casein was increased 12.9-fold, 11.9-fold, and 19.3-fold, respectively, following treatment with RA and PRL combined compared with the control group. These results demonstrate that RA induces differentiation of MAC-T cells and acts synergistically with PRL to increase specific casein gene expression. [ABSTRACT FROM AUTHOR]

Published
2013
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42. Effects of rigor state, thawing temperature, and processing on the physicochemical properties of frozen duck breast muscle.

Author

Kim, H. W., Lee, S. H., Choi, J. H., Choi, Y. S., Kim, H. Y., Hwang, K. E., Park, J. H., Song, D. H., and Kim, C. J.

Subjects
*MUSCLE analysis, *THAWING, *MEAT quality, *PHYSIOLOGICAL effects of temperature, *DUCKS, *EDIBLE fats & oils, *MEAT storage, *PHYSIOLOGY
Abstract

The objectives of this study were to evaluate effects of rigor state, thawing temperature, and processing on the physicochemical properties of intact frozen duck breast muscle and homogenates prepared with the frozen-thawed muscles. Prerigor breast muscle was frozen at --25°C and thawed at 4 and 15°C, and the physicochemical properties of duck breast frozen prerigor compared with those in frozen postrigor and 4°C chilled postrigor muscles. The homogenates prepared with duck breast frozen prerigor showed similar physicochemical properties as the frozen-thawed postrigor muscle homogenate. The thawing temperature did not affect the physicochemical properties of homogenates prepared with duck breast muscle frozen prerigor. Also, no significant differences (P > 0.05) in the ultimate pH value and color parameters were observed among the frozen-thawed treatments despite the differences in rigor state and thawing temperature. However, a higher thawing temperature of the intact frozen prerigor muscle resulted in an increase in thawing loss and shear force due to excessive muscle shortening. In this study, the intact duck breast that has undergone thaw-rigor showed main problems associated with thaw-rigor, such as higher thawing loss and shear force, regardless of thawing temperature. However, the processing (grinding and salting) decreased the difference in physico-chemical properties due to rigor state before freezing and thawing temperature. Therefore, the frozen-thawed duck breast muscle used to manufacture ground-type meat product may be frozen before rigor onset. [ABSTRACT FROM AUTHOR]

Published
2012
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43. Human infection with novel G3P[25] rotavirus strain in Taiwan.

Author

Wu, F.-T., Bányai, K., Huang, J. C., Wu, H.-S., Chang, F.-Y., Hsiung, C. A., Huang, Y.-C., Lin, J.-S., Hwang, K.-P., Jiang, B., and Gentsch, J. R.

Subjects
*ROTAVIRUSES, *GENES, *PHYLOGENY, *GASTROENTERITIS
Abstract

Clin Microbiol Infect 2011; 17: 1570-1573 Abstract Genotype P[25] rotaviruses are rare and to date have been reported to occur only in a few countries of mainland Asia. Here we report the molecular characterization of a novel human rotavirus genotype combination, G3P[25], detected in a 17-month-old child hospitalized due to severe gastroenteritis during 2009 in central Taiwan. Sequencing and phylogenetic analysis of the VP4 gene demonstrated a distinct origin from other strains bearing the P[25] VP4 gene, whereas the VP7, VP6 and NSP4 gene phylogenies identified common origins with cognate genes of other, presumed human-porcine reassortment Taiwanese strains. These results suggest that interactions between human and animal strains appear to contribute to the generation of genetic and antigenic diversity of rotavirus strains, with potential public health importance in Taiwan. [ABSTRACT FROM AUTHOR]

Published
2011
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44. Peripheral venous pressure as an alternative to central venous pressure in patients undergoing laparoscopic colorectal surgery.

Author

Kim, S. H., Park, S. Y., Cui, J., Lee, J. H., Cho, S. H., Chae, W. S., Jin, H. C., and Hwang, K. H.

Subjects
*COLON surgery, *LAPAROSCOPIC surgery, *CENTRAL venous pressure, *ARTIFICIAL pneumoperitoneum, *STATISTICAL correlation, *CONFIDENCE intervals, *HEART diseases
Abstract

Background Peripheral venous pressure (PVP) is strongly correlated with central venous pressure (CVP) during various surgeries. Laparoscopic surgery in the Trendelenburg position with pneumoperitoneum typically increases CVP. To determine whether PVP convincingly reflects changes in CVP, we evaluated the correlation between PVP and CVP in patients undergoing laparoscopic colorectal surgery. Methods Both CVP and PVP were measured simultaneously at predetermined time intervals during elective laparoscopic colorectal surgery in 42 patients without cardiac disease. The pairs of venous pressure measurements were analysed for correlation, and the Bland–Altman plots of repeated measures were used to evaluate the agreement between CVP and PVP. Results A total of 420 data pairs were obtained. The overall mean CVP was 11.3 (sd 4.5) mm Hg, which was significantly lower than the measured PVP of mean 12.1 (4.5) mm Hg (P=0.005). There was a strong positive correlation between overall CVP and PVP (correlation coefficient=0.96, P<0.0001). The mean bias (PVP–CVP) corrected for repeated measurements using random-effects modelling was 0.9 mm Hg [95% confidence interval (CI) 0.54–1.19 mm Hg] with 95% limits of agreement of −1.2 mm Hg (95% CI −1.75 to −0.62 mm Hg) to 2.9 mm Hg (95% CI 2.35–3.48 mm Hg). Conclusions PVP displays a strong correlation and agreement with CVP under the increased intrathoracic pressure of pneumoperitoneum in the Trendelenburg position and may be used as an alternative to CVP in patients without cardiac disease undergoing laparoscopic colorectal surgery. [ABSTRACT FROM AUTHOR]

Published
2011
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45. A serosurvey of Orientia tsutsugamushi from patients with scrub typhus.

Author

Kim, D. M., Lee, Y.-M., Back, J.-H., Yang, T. Y., Lee, J. H., Song, H.-J., Shim, S.-K., Hwang, K.-J., and Park, M.-Y.

Subjects
*TSUTSUGAMUSHI disease, *RICKETTSIAL diseases, *IMMUNOGLOBULINS, *SEROPREVALENCE, *IMMUNOFLUORESCENCE
Abstract

Clin Microbiol Infect 2010; 16: 447–451 Many countries where scrub typhus is endemic use their own cutoff values for antibody titres to differentiate between cured cases and current infections. To establish an antibody titre cutoff value, one needs to investigate the seroprevalence in endemic areas, and the duration of the increase in titre after complete cure. We conducted a follow-up study of anti- Orientia tsutsugamushi antibody titres using indirect immunofluorescence assays (IFA) and passive haemagglutination assays (PHA) in patients with scrub typhus. After the onset of symptoms, IgM antibody titres increased gradually over 2–3 weeks, peaked at about 4 weeks, and started to decrease rapidly between 4 and 5 weeks. At 1-year follow-up, the median IgM value was 1:10. Out of 77 patients who were tested at that time, 36 (47%) had IgM titres ≥1:20, and none had titres exceeding 1:80. Over the first 2 weeks, IgG antibody titres increased sharply, peaked at about 4 weeks and decreased rather gradually thereafter, with a median titre of 1:128 maintained up to the 18th month. At 1-year follow-up, five out of 77 patients (6.5%) had titres ≥1:1,024 and 57% had titres ≥1:128. Based on these results, a cutoff value of ≥1:160 for IgM antibody should differentiate between previous and current infections in endemic areas such as Korea and Japan, where scrub typhus occurs mainly in the autumn. [ABSTRACT FROM AUTHOR]

Published
2010
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46. Cordyceps pruinosa extracts induce apoptosis of HeLa cells by a caspase dependent pathway.

Author

Kim HG, Song H, Yoon DH, Song B, Park SM, Sung GH, Cho J, Park HI, Choi S, Song WO, Hwang K, and Kim TW

Abstract

AIM OF THE STUDY: Cordyceps is a parasitic fungus and has long been used as a traditional Chinese medicine to treat illnesses, promote longevity, increase athletic power, and relieve exhaustion and cancer. In this study, we reveal the mechanisms underlying apoptosis induced by Cordyceps pruinosa butanol fraction (CPBF) in the human cervical adenocarcinoma cell line, HeLa. MATERIALS AND METHODS: Proliferation and apoptosis of cells were examined by MTT assay, DNA fragmentation, phosphatidyl serine distribution assay, Western blot analysis, and immunocytochemistry. To determine the association between CPBF related apoptosis and ROS, electron spin resonance (ESR) trapping experiments were used. RESULTS: CPBF inhibited proliferation and induced apoptosis in HeLa cells in a dose-dependent manner using a MTT assay, DNA fragmentation, and a phosphatidyl serine distribution assay. Western blot analysis showed that apoptosis in HeLa cells was caspase-3- and -9-dependent. Proteolytic cleavage of PARP and the release of cytochrome c from the mitochondria into the cytosol were significantly increased and the Bcl-2/Bax protein ratio was decreased. Apoptosis induced by CPBF was not prevented by various antioxidants. CONCLUSIONS: These results indicate that apoptotic effects of CPBF on HeLa cells are mediated by mitochondria-dependent death-signaling pathway independent of reactive oxygen species, suggesting that CPBF might be effective as an anti-proliferative agent for cancer. [ABSTRACT FROM AUTHOR]

Published
2010
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47. Stone–Wales transformation in boron nitride nanotubes

Author

Song, J., Jiang, H., Wu, J., Huang, Y., and Hwang, K.-C.

Subjects
*BORON nitride, *NANOTUBES, *NITRIDES, *FULLERENES
Abstract

A hybrid atomistic/continuum model is used to study the Stone–Wales transformation (90° rotation of an atomic bond) in boron nitride nanotubes (BNNTs) subjected to tension. The critical strain for Stone–Wales transformation is 11.47% for (5,5) armchair and 14.23% for (10,0) zigzag BNNTs, which agree well with the atomistic simulations. The critical strain depends on the BNNT chirality for small tube radius, but this dependence gradually disappears with the increasing tube radius. [Copyright &y& Elsevier]

Published
2007
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48. Stone–Wales transformation: Precursor of fracture in carbon nanotubes

Author

Song, J., Jiang, H., Shi, D.-L., Feng, X.-Q., Huang, Y., Yu, M.-F., and Hwang, K.-C.

Subjects
*NANOTUBES, *FULLERENES, *MOLECULAR dynamics, *MOLECULAR beams
Abstract

Abstract: The fracture strain of carbon nanotubes (CNTs) obtained by molecular dynamics is about 30%, which is much higher than the experimental results (10–13%). The present study shows that this difference results mainly from defects in CNTs. As the tensile strain reaches a few percent, defects are nucleated in the form of Stone–Wales transformation (90° rotation of a bond). A bond in the vicinity of rotated bond breaks as the tensile strain reaches about 13%, which agrees well with the experimental results. Therefore, the Stone–Wales transformation is the precursor of CNT fracture. [Copyright &y& Elsevier]

Published
2006
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