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3. Global consortium for the classification of fungi and fungus-like taxa

Author

Hyde, K. D., Abdel-Wahab, M. A., Abdollahzadeh, J., Abeywickrama, P. D., Absalan, S., Afshari, N., Ainsworth, A. M., Akulov, O. Y., Aleoshin, V. V., Al-Sadi, A. M., Alvarado, P., Alves, A., Alves-Silva, G., Amalfi, M., Amira, Y., Amuhenage, T. B., Anderson, J. L., Antonín, V., Aouali, S., Aptroot, A., Apurillo, C. C. S., Araújo, J. P.M., Ariyawansa, H. A., Armand, A., Arumugam, E., Asghari, R., Assis, D. M.A., Atienza, V., Avasthi, S., Azevedo, E., Bahkali, A. H., Bakhshi, M., Banihashemi, Z., Bao, D. F., Baral, H. O., Barata, M., Barbosa, F. R., Barbosa, R. N., Barreto, R. W., Baschien, C., Belamesiatseva, D. B., Reuel, M. Bennett, Bera, I., Bezerra, J. D. P., Bezerra, J. L., Bhat, D. J., Bhunjun, C. S., Bianchinotti, M. V., Błaszkowski, J., Blondelle, A., Boekhout, T., Bonito, G., Boonmee, S., Boonyuen, N., Bregant, C., Buchanan, P., Bundhun, D., Burgaud, G., Burgess, T., Buyck, B., Cabarroi-Hernández, M., Cáceres, M. E. S., Caeiro, M. F., Cai, L., Cai, M. F., Calabon, M. S., Calaça, F. J. S., Callalli, M., Camara, M. P. S., Cano-Lira, J. F., Cantillo, T., Cao, B., Carlavilla, J. R., Carvalho, A., Castañeda-Ruiz, R. F., Castlebury, L., Castro-Jauregui, O., Catania, M. D., Cavalcanti, L. H., Cazabonne, J., Cedeño-Sanchez, M. L., Chaharmiri-Dokhaharani, S., Chaiwan, N., Chakraborty, N., Chaverri, P., Cheewangkoon, R., Chen, C., Chen, C. Y., Chen, K. H., Chen, J., Chen, Q., Chen, W. H., Chen, Y. P., Chethana, K. W. T., Coleine, C., Condé, T. O., Corazon-Guivin, M. A., Cortés-Pérez, A., Costa-Rezende, D. H., Courtecuisse, R., Crouch, J. A., Crous, P. W., Cui, B. K., Cui, Y. Y., da Silva, D. K. A., da Silva, G. A., da Silva, I. R., da Silva, R. M. F., da Silva Santos, A. C., Dai, D. Q., Dai, Y. C., Damm, U., Darmostuk, V., Zoha, Daroodi, Das, K., Davoodian, N., Davydov, E. A., Dayarathne, M. C., Decock, C., de Groot, M. D., De Kesel, A., de la Cruz, T. E. E., De Lange, R., Delgado, G., Denchev, C. M., Denchev, T. T., de Oliveira, N. T., de Silva, N. I., de Souza, F. A., Dentinger, B., Devadatha, B., Dianese, J. C., Dima, B., Diniz, A. G., Dissanayake, A. J., Dissanayake, L. S., Doğan, H. H., Doilom, M., Dolatabadi, S., Dong, W., Dong, Z. Y., Dos Santos, L. A., Drechsler-Santos, E. R., Du, T. Y., Dubey, M. K., Dutta, A. K., Egidi, E., Elliott, T. F., Elshahed, M. S., Erdoğdu, M., Ertz, D., Etayo, J., Evans, H. C., Fan, X. L., Fan, Y. G., Fedosova, A. G., Fell, J., Fernandes, I., Firmino, A. L., Fiuza, P. O., Flakus, A., de Souza, C. A.Fragoso, Frisvad, J. C., Fryar, S. C., Gabaldón, T., Gajanayake, A. J., Galindo, L. J., Gannibal, P. B., García, D., García-Sandoval, S. R., Garrido-Benavent, I., Garzoli, L., Gautam, A. K., Ge, Z. W., Gené, D. J., Gentekaki, E., Ghobad-Nejhad, M., Giachini, A. J., Gibertoni, T. B., Góes-Neto, A., Gomdola, D., de Farias, A. R. Gomes, Gorjón, S. P., Goto, B. T., Granados-Montero, M. M., Griffith, G. W., Groenewald, J. Z., Groenewald, M., Grossart, H. P., Gueidan, C., Gunarathne, A., Gunaseelan, S., Gusmão, L. F.P., Gutierrez, A. C., Guzmán-Dávalos, L., Haelewaters, D., Halling, R., Han, Y. F., Hapuarachchi, K. K., Harder, C. B., Harrington, T. C., Hattori, T., He, M. Q., He, S., He, S. H., Healy, R., Herández-Restrepo, M., Heredia, G., Hodge, K. T., Holgado-Rojas, M., Hongsanan, S., Horak, E., Hosoya, T., Houbraken, J., Huang, S. K., Huanraluek, N., Hur, J. S., Hurdeal, V. G., Hustad, V. P., Iotti, M., Iturriaga, T., Jafar, E., Janik, P., Jany, J. L., Jayalal, R. G.U., Jayasiri, S. C., Jayawardena, R. S., Jeewon, R., Jerônimo, G. H., Jesus, A. L., Jin, J., Johnston, P. R., Jones, E. B.G., Joshi, Y., Justo, A., Kaishian, P., Kakishima, M., Kaliyaperumal, M., Kang, G. P., Kang, J. C., Karakehian, J. M., Karimi, O., Karpov, S. A., Karunarathna, S. C., Kaufmann, M., Kemler, M., Kezo, K., Khyaju, S., Kirchmair, M., Kirk, P. M., Kitaura, M. J., Klawonn, I., Kolarik, M., Kong, A., Kuhar, F., Kukwa, M., Kumar, S., Kušan, I., Lado, C., Larsson, K. H., Latha, K. P.D., Lee, H. B., Leonardi, M., Leontyev, D. L., Lestari, A. S., Li, C. J.Y., Li, D. W., Li, H. Y., Li, L., Li, Q. R., Li, W. L., Li, Y., Li, Y. C., Liao, C. F., Liimatainen, K., Lim, Y. W., Lin, C. G., Linaldeddu, B. T., Linde, C. C., Linn, M. M., Liu, F., Liu, J. K., Liu, N. G., Liu, S., Liu, X. F., Liu, X. Z., Liu, Z. B., Lu, L., Lu, Y. Z., Luangharn, T., Luangsa-ard, J. J., Lumbsch, H. T., Lumyong, S., Luo, L., Luo, M., Luo, Z. L., Ma, J., Machado, A. R., Madagammana, A. D., Madrid, H., Magurno, F., Magyar, D., Mahadevan, N., Maharachchikumbura, S. S.N., Maimaiti, Y., Malosso, E., Manamgoda, D. S., Manawasinghe, I. S., Mapook, A., Marasinghe, D. S., Mardones, M., Marin-Felix, Y., Márquez, R., Masigol, H., Matočec, N., May, T. W., McKenzie, E. H.C., Meiras-Ottoni, A., Melo, R. F.R., Mendes-Alvarenga, R. L., Mendieta, S., Meng, Q. F., Menkis, A., Menolli, N., Mešić, A., Calvo, J. G.Meza, Mikhailov, K. V., Miller, S. L., Moncada, B., Moncalvo, J. M., Monteiro, J. S., Monteiro, M., Mora-Montes, H. M., Moreau, P. A., Mueller, G. M., Mukhopadyay, S., Murugadoss, R., Nagy, L. G., Najafiniya, M., Nanayakkara, C. M., Nascimento, C. C., Nei, Y., Neves, M. A., Neuhauser, S., Niego, A. G.T., Nilsson, R. H., Niskanen, T., Niveiro, N., Noorabadi, M. T., Noordeloos, M. E., Norphanphoun, C., Otaño, N. B.Nuñez, O’Donnell, R. P., Oehl, F., Olariaga, I., Orlando, O. P., Pang, K. L., Papp, V., Pawłowska, J., Peintner, U., Pem, D., Pereira, O. L., Perera, R. H., Perez-Moreno, J., Perez-Ortega, S., Péter, G., Phillips, A. J.L., Phonemany, M., Phukhamsakda, C., Phutthacharoen, K., Piepenbring, M., Pires-Zottarelli, C. L.A., Poinar, G., Pošta, A., Prieto, M., Promputtha, I., Quandt, C. A., Radek, R., Rahnama, K., Raj, K. N.A., Rajeshkumar, K. C., Rämä, T., Rambold, G., Ramírez-Cruz, V., Rasconi, S., Rathnayaka, A. R., Raza, M., Ren, G. C., Robledo, G. L., Rodriguez-Flakus, P., Ronikier, A., Rossi, W., Ryberg, M., Ryvarden, L. R., Salvador-Montoya, C. A., Samant, B., Samarakoon, B. C., Samarakoon, M. C., Sánchez-Castro, I., Sánchez-García, M., Sandoval-Denis, M., Santamaria, B., Santiago, A. L.C.M.A., Sarma, V. V., Savchenko, A., Savchenko, K., Saxena, R. K., Scholler, M., Schoutteten, N., Seifollahi, E., Selbmann, L., Selcuk, F., Senanayake, I. C., Shabashova, T. G., Shen, H. W., Shen, Y. M., Silva-Filho, A. G.S., Simmons, D. R., Singh, R., Sir, E. B., Song, C. G., Souza-Motta, C. M., Sruthi, O. P., Stadler, M., Stchigel, A. M., Stemler, J., Stephenson, S. L., Strassert, J. F.H., Su, H. L., Su, L., Suetrong, S., Sulistyo, B., Sun, Y. R., Svantesson, S., Sysouphanthong, P., Takamatsu, S., Tan, T. H., Tanaka, K., Tang, A. M.C., Tang, X., Tanney, J. B., Tavakol, N. M., Taylor, J. E., Taylor, P. W.J., Tedersoo, L., Tennakoon, D. S., Thamodini, G. K., Thines, M., Thiyagaraja, V., Thongklang, N., Tiago, P. V., Tian, Q., Tian, W. H., Tibell, L., Tibell, S., Tibpromma, S., Tkalčec, Z., Tomšovský, M., Toome-Heller, M., Torruella, G., Tsurykau, A., Udayanga, D., Ulukapi, M., Untereiner, W. A., Uzunov, B. A., Valle, L. G., Van Caenegem, W., Van den Wyngaert, S., Van Vooren, N., Velez, P., Verma, R. K., Vieira, L. C., Vieira, W. A.S., Vizzini, A., Walker, A., Walker, A. K., Wanasinghe, D. N., Wang, C. G., Wang, K., Wang, S. X., Wang, X. Y., Wang, Y., Wannasawang, N., Wartchow, F., Wei, D. P., Wei, X. L., White, J. F., Wijayawardene, N. N., Wijesinghe, S. N., Wijesundara, D. S.A., Wisitrassameewong, K., Worthy, F. R., Wu, F., Wu, G., Wu, H. X., Wu, N., Wu, W. P., Wurzbacher, C., Xiao, Y. P., Xiong, Y. R., Xu, B., Xu, L. J., Xu, R., Xu, T. M., Yakovchenko, L., Yan, J. Y., Yang, H. D., Yang, J., Yang, Z. L., Yang, Y. H., Yapa, N., Yasanthika, E., Youssef, N. H., Yu, F. M., Yu, Q., Yu, X. D., Yu, Y. X., Yu, Z. F., Yuan, H. S., Yuan, Y., Yurkov, A., Zafari, D., Zamora, J. C., Zare, R., Zeng, M., Zeng, N. K., Zeng, X. Y., Zhang, F., Zhang, H., Zhang, J. F., Zhang, J. Y., Zhang, Q. Y., Zhang, S. N., Zhang, W., Zhang, Y., Zhao, C. L., Zhao, H., Zhao, Q., Zhao, R. L., Zhou, L. W., Zhou, M., Zhurbenko, M. P., Zin, H. H., Zucconi, L., Hyde, K. D., Abdel-Wahab, M. A., Abdollahzadeh, J., Abeywickrama, P. D., Absalan, S., Afshari, N., Ainsworth, A. M., Akulov, O. Y., Aleoshin, V. V., Al-Sadi, A. M., Alvarado, P., Alves, A., Alves-Silva, G., Amalfi, M., Amira, Y., Amuhenage, T. B., Anderson, J. L., Antonín, V., Aouali, S., Aptroot, A., Apurillo, C. C. S., Araújo, J. P.M., Ariyawansa, H. A., Armand, A., Arumugam, E., Asghari, R., Assis, D. M.A., Atienza, V., Avasthi, S., Azevedo, E., Bahkali, A. H., Bakhshi, M., Banihashemi, Z., Bao, D. F., Baral, H. O., Barata, M., Barbosa, F. R., Barbosa, R. N., Barreto, R. W., Baschien, C., Belamesiatseva, D. B., Reuel, M. Bennett, Bera, I., Bezerra, J. D. P., Bezerra, J. L., Bhat, D. J., Bhunjun, C. S., Bianchinotti, M. V., Błaszkowski, J., Blondelle, A., Boekhout, T., Bonito, G., Boonmee, S., Boonyuen, N., Bregant, C., Buchanan, P., Bundhun, D., Burgaud, G., Burgess, T., Buyck, B., Cabarroi-Hernández, M., Cáceres, M. E. S., Caeiro, M. F., Cai, L., Cai, M. F., Calabon, M. S., Calaça, F. J. S., Callalli, M., Camara, M. P. S., Cano-Lira, J. F., Cantillo, T., Cao, B., Carlavilla, J. R., Carvalho, A., Castañeda-Ruiz, R. F., Castlebury, L., Castro-Jauregui, O., Catania, M. D., Cavalcanti, L. H., Cazabonne, J., Cedeño-Sanchez, M. L., Chaharmiri-Dokhaharani, S., Chaiwan, N., Chakraborty, N., Chaverri, P., Cheewangkoon, R., Chen, C., Chen, C. Y., Chen, K. H., Chen, J., Chen, Q., Chen, W. H., Chen, Y. P., Chethana, K. W. T., Coleine, C., Condé, T. O., Corazon-Guivin, M. A., Cortés-Pérez, A., Costa-Rezende, D. H., Courtecuisse, R., Crouch, J. A., Crous, P. W., Cui, B. K., Cui, Y. Y., da Silva, D. K. A., da Silva, G. A., da Silva, I. R., da Silva, R. M. F., da Silva Santos, A. C., Dai, D. Q., Dai, Y. C., Damm, U., Darmostuk, V., Zoha, Daroodi, Das, K., Davoodian, N., Davydov, E. A., Dayarathne, M. C., Decock, C., de Groot, M. D., De Kesel, A., de la Cruz, T. E. E., De Lange, R., Delgado, G., Denchev, C. M., Denchev, T. T., de Oliveira, N. T., de Silva, N. I., de Souza, F. A., Dentinger, B., Devadatha, B., Dianese, J. C., Dima, B., Diniz, A. G., Dissanayake, A. J., Dissanayake, L. S., Doğan, H. H., Doilom, M., Dolatabadi, S., Dong, W., Dong, Z. Y., Dos Santos, L. A., Drechsler-Santos, E. R., Du, T. Y., Dubey, M. K., Dutta, A. K., Egidi, E., Elliott, T. F., Elshahed, M. S., Erdoğdu, M., Ertz, D., Etayo, J., Evans, H. C., Fan, X. L., Fan, Y. G., Fedosova, A. G., Fell, J., Fernandes, I., Firmino, A. L., Fiuza, P. O., Flakus, A., de Souza, C. A.Fragoso, Frisvad, J. C., Fryar, S. C., Gabaldón, T., Gajanayake, A. J., Galindo, L. J., Gannibal, P. B., García, D., García-Sandoval, S. R., Garrido-Benavent, I., Garzoli, L., Gautam, A. K., Ge, Z. W., Gené, D. J., Gentekaki, E., Ghobad-Nejhad, M., Giachini, A. J., Gibertoni, T. B., Góes-Neto, A., Gomdola, D., de Farias, A. R. Gomes, Gorjón, S. P., Goto, B. T., Granados-Montero, M. M., Griffith, G. W., Groenewald, J. Z., Groenewald, M., Grossart, H. P., Gueidan, C., Gunarathne, A., Gunaseelan, S., Gusmão, L. F.P., Gutierrez, A. C., Guzmán-Dávalos, L., Haelewaters, D., Halling, R., Han, Y. F., Hapuarachchi, K. K., Harder, C. B., Harrington, T. C., Hattori, T., He, M. Q., He, S., He, S. H., Healy, R., Herández-Restrepo, M., Heredia, G., Hodge, K. T., Holgado-Rojas, M., Hongsanan, S., Horak, E., Hosoya, T., Houbraken, J., Huang, S. K., Huanraluek, N., Hur, J. S., Hurdeal, V. G., Hustad, V. P., Iotti, M., Iturriaga, T., Jafar, E., Janik, P., Jany, J. L., Jayalal, R. G.U., Jayasiri, S. C., Jayawardena, R. S., Jeewon, R., Jerônimo, G. H., Jesus, A. L., Jin, J., Johnston, P. R., Jones, E. B.G., Joshi, Y., Justo, A., Kaishian, P., Kakishima, M., Kaliyaperumal, M., Kang, G. P., Kang, J. C., Karakehian, J. M., Karimi, O., Karpov, S. A., Karunarathna, S. C., Kaufmann, M., Kemler, M., Kezo, K., Khyaju, S., Kirchmair, M., Kirk, P. M., Kitaura, M. J., Klawonn, I., Kolarik, M., Kong, A., Kuhar, F., Kukwa, M., Kumar, S., Kušan, I., Lado, C., Larsson, K. H., Latha, K. P.D., Lee, H. B., Leonardi, M., Leontyev, D. L., Lestari, A. S., Li, C. J.Y., Li, D. W., Li, H. Y., Li, L., Li, Q. R., Li, W. L., Li, Y., Li, Y. C., Liao, C. F., Liimatainen, K., Lim, Y. W., Lin, C. G., Linaldeddu, B. T., Linde, C. C., Linn, M. M., Liu, F., Liu, J. K., Liu, N. G., Liu, S., Liu, X. F., Liu, X. Z., Liu, Z. B., Lu, L., Lu, Y. Z., Luangharn, T., Luangsa-ard, J. J., Lumbsch, H. T., Lumyong, S., Luo, L., Luo, M., Luo, Z. L., Ma, J., Machado, A. R., Madagammana, A. D., Madrid, H., Magurno, F., Magyar, D., Mahadevan, N., Maharachchikumbura, S. S.N., Maimaiti, Y., Malosso, E., Manamgoda, D. S., Manawasinghe, I. S., Mapook, A., Marasinghe, D. S., Mardones, M., Marin-Felix, Y., Márquez, R., Masigol, H., Matočec, N., May, T. W., McKenzie, E. H.C., Meiras-Ottoni, A., Melo, R. F.R., Mendes-Alvarenga, R. L., Mendieta, S., Meng, Q. F., Menkis, A., Menolli, N., Mešić, A., Calvo, J. G.Meza, Mikhailov, K. V., Miller, S. L., Moncada, B., Moncalvo, J. M., Monteiro, J. S., Monteiro, M., Mora-Montes, H. M., Moreau, P. A., Mueller, G. M., Mukhopadyay, S., Murugadoss, R., Nagy, L. G., Najafiniya, M., Nanayakkara, C. M., Nascimento, C. C., Nei, Y., Neves, M. A., Neuhauser, S., Niego, A. G.T., Nilsson, R. H., Niskanen, T., Niveiro, N., Noorabadi, M. T., Noordeloos, M. E., Norphanphoun, C., Otaño, N. B.Nuñez, O’Donnell, R. P., Oehl, F., Olariaga, I., Orlando, O. P., Pang, K. L., Papp, V., Pawłowska, J., Peintner, U., Pem, D., Pereira, O. L., Perera, R. H., Perez-Moreno, J., Perez-Ortega, S., Péter, G., Phillips, A. J.L., Phonemany, M., Phukhamsakda, C., Phutthacharoen, K., Piepenbring, M., Pires-Zottarelli, C. L.A., Poinar, G., Pošta, A., Prieto, M., Promputtha, I., Quandt, C. A., Radek, R., Rahnama, K., Raj, K. N.A., Rajeshkumar, K. C., Rämä, T., Rambold, G., Ramírez-Cruz, V., Rasconi, S., Rathnayaka, A. R., Raza, M., Ren, G. C., Robledo, G. L., Rodriguez-Flakus, P., Ronikier, A., Rossi, W., Ryberg, M., Ryvarden, L. R., Salvador-Montoya, C. A., Samant, B., Samarakoon, B. C., Samarakoon, M. C., Sánchez-Castro, I., Sánchez-García, M., Sandoval-Denis, M., Santamaria, B., Santiago, A. L.C.M.A., Sarma, V. V., Savchenko, A., Savchenko, K., Saxena, R. K., Scholler, M., Schoutteten, N., Seifollahi, E., Selbmann, L., Selcuk, F., Senanayake, I. C., Shabashova, T. G., Shen, H. W., Shen, Y. M., Silva-Filho, A. G.S., Simmons, D. R., Singh, R., Sir, E. B., Song, C. G., Souza-Motta, C. M., Sruthi, O. P., Stadler, M., Stchigel, A. M., Stemler, J., Stephenson, S. L., Strassert, J. F.H., Su, H. L., Su, L., Suetrong, S., Sulistyo, B., Sun, Y. R., Svantesson, S., Sysouphanthong, P., Takamatsu, S., Tan, T. H., Tanaka, K., Tang, A. M.C., Tang, X., Tanney, J. B., Tavakol, N. M., Taylor, J. E., Taylor, P. W.J., Tedersoo, L., Tennakoon, D. S., Thamodini, G. K., Thines, M., Thiyagaraja, V., Thongklang, N., Tiago, P. V., Tian, Q., Tian, W. H., Tibell, L., Tibell, S., Tibpromma, S., Tkalčec, Z., Tomšovský, M., Toome-Heller, M., Torruella, G., Tsurykau, A., Udayanga, D., Ulukapi, M., Untereiner, W. A., Uzunov, B. A., Valle, L. G., Van Caenegem, W., Van den Wyngaert, S., Van Vooren, N., Velez, P., Verma, R. K., Vieira, L. C., Vieira, W. A.S., Vizzini, A., Walker, A., Walker, A. K., Wanasinghe, D. N., Wang, C. G., Wang, K., Wang, S. X., Wang, X. Y., Wang, Y., Wannasawang, N., Wartchow, F., Wei, D. P., Wei, X. L., White, J. F., Wijayawardene, N. N., Wijesinghe, S. N., Wijesundara, D. S.A., Wisitrassameewong, K., Worthy, F. R., Wu, F., Wu, G., Wu, H. X., Wu, N., Wu, W. P., Wurzbacher, C., Xiao, Y. P., Xiong, Y. R., Xu, B., Xu, L. J., Xu, R., Xu, T. M., Yakovchenko, L., Yan, J. Y., Yang, H. D., Yang, J., Yang, Z. L., Yang, Y. H., Yapa, N., Yasanthika, E., Youssef, N. H., Yu, F. M., Yu, Q., Yu, X. D., Yu, Y. X., Yu, Z. F., Yuan, H. S., Yuan, Y., Yurkov, A., Zafari, D., Zamora, J. C., Zare, R., Zeng, M., Zeng, N. K., Zeng, X. Y., Zhang, F., Zhang, H., Zhang, J. F., Zhang, J. Y., Zhang, Q. Y., Zhang, S. N., Zhang, W., Zhang, Y., Zhao, C. L., Zhao, H., Zhao, Q., Zhao, R. L., Zhou, L. W., Zhou, M., Zhurbenko, M. P., Zin, H. H., and Zucconi, L.

Abstract

The Global Consortium for the Classification of Fungi and fungus-like taxa is an international initiative of more than 550 mycologists to develop an electronic structure for the classification of these organisms. The members of the Consortium originate from 55 countries/regions worldwide, from a wide range of disciplines, and include senior, mid-career and early-career mycologists and plant pathologists. The Consortium will publish a biannual update of the Outline of Fungi and fungus-like taxa, to act as an international scheme for other scientists. Notes on all newly published taxa at or above the level of species will be prepared and published online on the Outline of Fungi website (https://www.outlineoffungi.org/), and these will be finally published in the biannual edition of the Outline of Fungi and fungus-like taxa. Comments on recent important taxonomic opinions on controversial topics will be included in the biannual outline. For example, 'to promote a more stable taxonomy in Fusarium given the divergences over its generic delimitation', or 'are there too many genera in the Boletales?' and even more importantly, 'what should be done with the tremendously diverse 'dark fungal taxa?' There are undeniable differences in mycologists' perceptions and opinions regarding species classification as well as the establishment of new species. Given the pluralistic nature of fungal taxonomy and its implications for species concepts and the nature of species, this consortium aims to provide a platform to better refine and stabilise fungal classification, taking into consideration views from different parties. In the future, a confidential voting system will be set up to gauge the opinions of all mycologists in the Consortium on important topics. The results of such surveys will be presented to the International Commission on the Taxonomy of Fungi (ICTF) and the Nomenclature Committee

Published
2023

5. Neural Decoding of Visual Information Across Different Neural Recording Modalities and Approaches

Author

Zhang, Y-J, Yu, Z-F, Liu, JK, and Huang, T-J

Abstract

Vision plays a peculiar role in intelligence. Visual information, forming a large part of the sensory information, is fed into the human brain to formulate various types of cognition and behaviours that make humans become intelligent agents. Recent advances have led to the development of brain-inspired algorithms and models for machine vision. One of the key components of these methods is the utilization of the computational principles underlying biological neurons. Additionally, advanced experimental neuroscience techniques have generated different types of neural signals that carry essential visual information. Thus, there is a high demand for mapping out functional models for reading out visual information from neural signals. Here, we briefly review recent progress on this issue with a focus on how machine learning techniques can help in the development of models for contending various types of neural signals, from fine-scale neural spikes and single-cell calcium imaging to coarse-scale electroencephalography (EEG) and functional magnetic resonance imaging recordings of brain signals.

Published
2022

8. Design and validation of micro-vibration isolator for reaction wheels in consideration of launch environment of satellite.

Author

Jie Huang and Yu, Z. F.

Subjects
ARTIFICIAL satellite launching, RANDOM vibration, SYSTEM safety, REMOTE-sensing images, WHEELS, TELECOMMUNICATION satellites, EARTHQUAKE resistant design
Abstract

Micro-vibration is an important factor that influences the imager orientation accuracy and even deteriorates the quality of image of high-resolution satellite. To eliminate the influences of micro-vibration, a passive micro-vibration isolationmethod is proposed for reaction wheels (RWs) of satellite. At the same time, the launch environment is fully considered in the design of isolation system to guarantee the safety of both RWs. The isolation efficiency and orientation stability experiment results show that, without isolators, the peak value of the torque output reaches more than 10 Nm that is sharply depressed with isolation system operating mode. Without isolators, four clear peak values located at 10 Hz, 41 Hz, 47 Hz, 83 Hz are found in the orientation oscillation of RW. The random vibration experiments showthat the maximal acceleration output 34.61 g is much lower than the RWdesign value 49 g which guarantees the safety of RW under harsh launch environment. The isolating efficiency is higher than 75% which is suitable for the requirement of the imager onboard the SDLT-1 satellite. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Cognitive endpoints for therapy development for neuronopathic mucopolysaccharidoses: Results of a consensus procedure

Author

Lee, J.H. (Johanna) van der, Morton, J. (Jonathan), Adams, H.R. (Heather R.), Clarke, L.A. (L.), Ebbink, B.J. (Johanneke), Escolar, M.L. (Maria L.), Giugliani, R. (Roberto), Harmatz, P. (Paul), Hogan, M. (Melissa), Jones, S.A. (Simon), Kearney, S. (Shauna), Muenzer, J. (Joseph), Rust, S. (Stewart), Semrud-Clikeman, M. (Margaret), Wijburg, F.A. (Frits), Yu, Z.-F. (Zi-fan), Janzen, D. (Darren), Shapiro, E. (Elsa), Lee, J.H. (Johanna) van der, Morton, J. (Jonathan), Adams, H.R. (Heather R.), Clarke, L.A. (L.), Ebbink, B.J. (Johanneke), Escolar, M.L. (Maria L.), Giugliani, R. (Roberto), Harmatz, P. (Paul), Hogan, M. (Melissa), Jones, S.A. (Simon), Kearney, S. (Shauna), Muenzer, J. (Joseph), Rust, S. (Stewart), Semrud-Clikeman, M. (Margaret), Wijburg, F.A. (Frits), Yu, Z.-F. (Zi-fan), Janzen, D. (Darren), and Shapiro, E. (Elsa)

Abstract

The design and conduct of clinical studies to evaluate the effects of novel therapies on central nervous system manifestations in children with neuronopathic mucopolysaccharidoses is challenging. Owing to the rarity of these disorders, multinational studies are often needed to recruit enough patients to provide meaningful data and statistical power. This can make the consistent collection of reliable data across study sites difficult. To address these challenges, an International MPS Consensus Conference for Cognitive Endpoints was convened to discuss approaches for evaluating cognitive and adaptive function in patients with mucopolysaccharidoses. The goal was to develop a consensus on best practice for the design and conduct of clinical studies investigating novel therapies for these conditions, with particular focus on the most appropriate outcome measures for cognitive function and adaptive behavior. The outcomes from the consensus panel discussion are reported here.

Published
2017
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19. Spin-orbit torque induced magnetization switching in ferrimagnetic Heusler alloy D022-Mn3Ga with large perpendicular magnetic anisotropy.

Author

Zhao, X. P., Lu, J., Mao, S. W., Yu, Z. F., Wei, D. H., and Zhao, J. H.

Subjects
PERPENDICULAR magnetic anisotropy, FERRIMAGNETIC materials, SPIN-orbit interactions, HEUSLER alloys, ANOMALOUS Hall effect, MAGNETIZATION, ELECTRIC potential measurement, TORQUE
Abstract

Magnetization switching induced by spin–orbit torque is of fundamental interest for developing spintronic devices with low-power consumption and nonvolatility. Here, we report on the spin–orbit torque induced magnetization switching behavior of (001) oriented tetragonal Heusler alloy D022-Mn3Ga films with an intrinsic ferrimagnetic spin structure grown on the GaAs(001) substrate by molecular-beam epitaxy. The out-of-plane hysteresis loop and anomalous Hall effect demonstrated a large perpendicular magnetic anisotropy and low saturation magnetization of D022-Mn3Ga thin films. The spin–orbit torque induced magnetization switching has been realized in D022-Mn3Ga/Pt heterostructure based Hall devices under an in-plane external field. It is found that the critical switching current density Jc is much smaller than that of the L10-MnGa/heavy metal system. Besides, both a dampinglike effective field HDL and a fieldlike effective field HFL are quantified by performing harmonic Hall voltage measurements. All these results indicate that ferrimagnetic D022-Mn3Ga can be a promising candidate material for realizing high-density and energy-efficient spintronic devices. [ABSTRACT FROM AUTHOR]

Published
2019
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28. Comparison between Transareola Singlesite Endoscopic Thyroidectomy and Minimally Invasive Video-assisted Thyroidectomy

Author

Shana, Y-Z, Zhoua, L-M, Yu, Z-F, Wang, S-G, Gao, G-L, Shen, Y, and Zhang, X-L

Abstract

OBJECTIVES: To compare surgical outcomes between transareola single-site endoscopic thyroidectomy (TASSET) and minimally invasive video-assisted thyroidectomy (MIVAT).Methods: Patients with thyroid nodules were randomized to TASSET (n = 24) or MIVAT (n = 24). Surgical outcomes and patient-rated cosmetic results, based on numerical (0 [worst], 10 [best]) and verbal (1 [poor], 4 [excellent]) response scales, were compared.Results: There were no significant differences between groups for age, sex, indication for operation, estimated blood loss, postoperative pain and length of postoperative stay. TASSET was associated with a significantly longer mean ± SD operative time than MIVAT (156.84 ± 41.42 vs. 66.38 ± 17.58 min), and significantly improved cosmetic results according to the numerical (9.63 ± 0.60 vs 7.90 ± 1.38) and verbal response (3.8 ± 0.5 vs 3.1 ± 0.7) scales. Postoperative complaints were comparable between the two approaches, although MIVAT involved a shorter operation time.Conclusions: Patients treated with TASSET had superior cosmetic results compared with those treated with MIVAT.

Published
2012
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30. [Analysis on the status quo of the awareness rate of core knowledge of cancer prevention and treatment and its influencing factors among residents in Liaoning Province in 2021].

Author

Li MD, Ni P, Yu HH, Yu ZF, Sun JX, Bai MY, Bai S, An XX, Shi YH, and Liu YY

Subjects
Adult, Female, Humans, Male, Middle Aged, China, Surveys and Questionnaires, Adolescent, Young Adult, Aged, Health Knowledge, Attitudes, Practice, Neoplasms prevention & control
Abstract

Objective: To analyze the status quo of the knowledge and related factors of cancer prevention and treatment among residents in Liaoning Province in 2021. Methods: From August to November 2021, through network sampling method, 17 474 permanent residents aged 15-69 years in Liaoning Province were surveyed. The WeChat public account was used to collect information such as demographic characteristics and core knowledge of cancer prevention and treatment. The Chi-square test was used to compare the difference of the level of the cancer prevention and treatment knowledge among different groups. The multivariate logistic regression model was used to analyze the related factors. Results: Among the 17 474 subjects, 43.1% (7 528) were male and 58.7% (10 262) were urban residents. The overall awareness rate was 72.3%, and the awareness rate of cancer cognition, prevention, early diagnosis and treatment, cancer management and rehabilitation were 71.4%, 67.6%, 72.7%, 83.4% and 63.5%, respectively. The multivariate logistic regression model showed that the residents who were man ( OR : 0.850, 95% CI : 0.781-0.925), in rural areas ( OR : 0.753, 95% CI : 0.694-0.817), 55-59 years old ( OR : 0.851, 95% CI : 0.751-0.963), quitters ( OR : 0.721, 95% CI : 0.640-0.813) and smoker ( OR : 0.724, 95% CI : 0.654-0.801) had lower awareness rates, while the residents who were 35-54 years old ( OR : 1.312, 95% CI : 1.202-1.432), with an educational level of junior high school/senior high school/college degree or above ( OR : 1.834-5.130, 95% CI : 1.575-6.047), technical personnel ( OR : 1.592, 95% CI : 1.367-1.854), civil servant/institution staff ( OR : 1.282, 95% CI : 1.094-1.503), enterprise/business/service staff ( OR : 1.218, 95% CI : 1.071-1.385), retired ( OR : 1.324, 95% CI : 1.114-1.573) and with family history of cancer ( OR : 1.369, 95% CI : 1.266-1.481) had higher awareness rates. Conclusion: The level of the awareness of core knowledge of cancer prevention and treatment among residents in Liaoning Province has met the requirements of the Healthy China Action. Region, gender, education level, age, family history of cancer and smoking are relevant factors.

Published
2023
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31. [Open hepatectomy versus laparoscopic in the treatment of primary left-sided hepatolithiasis: a propensity, long-term follow-up analysis at a single center].

Author

Pan SB, Wu CL, Hou H, Zhou DC, Cui X, He L, Gu J, Wang L, Yu ZF, Dong GY, Xie SX, Xiong QR, and Geng XP

Subjects
Adult, Aged, Follow-Up Studies, Hepatectomy adverse effects, Humans, Laparoscopy, Middle Aged, Propensity Score, Retrospective Studies, Treatment Outcome, Hepatectomy methods, Lithiasis surgery, Liver Diseases surgery
Abstract

To compare short-term and long-term efficacy after laparoscopic left hepatectomy(LLR) to open left hepatectomy(OLH) for primary left-sided hepatolithiasis. Methods: Clinical data of 187 patients with left-sided hepatolithiasis and underwent laparoscopically or open left-sided hepatectomy from October 2014 to October 2019 at the Second Affiliated Hospital of Anhui Medical University were retrospectively analyzed in this propensity score matching (PSM) study and were matched in terms of age, sex, body mass index, liver function, ASA score, comorbidities, history of biliary surgery, and smoking history on the ratio of 1∶1.There were 47 cases in each group and the mean age were (54.7±12.3)years old(range:34 to 75 years old) and (53.2±12.6) years old (range: 34 to 75 years old) in open and laparoscopically group respectively. The data of operation time, intraoperative blood loss, postoperative hospital-stay, complication rate, biliary fistula rate, stone clearance rate, and stone recurrence rate were compared. The quantitative data were compared using t -test or rank-sum test. Count data were analyzed with χ(2) test or Fisher test. Results: No significant difference was observed in the clinical characteristics of included 94 patients in this study(all P> 0.05).The length of the postoperative hospital-stay after OLH was significantly higher than that in the LLH group((10.8±3.1) days vs .(8.5±2.2)days, t= 4.085, P= 0.000). LLR significantly decreased the incidence of postoperative biliary fistula compared with the OLH (6.3% vs .21.2%, χ(2)=4.374, P= 0.036) and the rates of postoperative complications in the OLH group was significantly higher than that in the LLH group (48.9% vs .27.6%, χ(2)=4.502, P= 0.034). Moreover, the stone recurrence rates in the LLH group was significantly lower than that after OLR (4.2% vs . 17.0%, χ(2)=4.029, P= 0.045). OLH (95 % CI : 1.55 to 10.75, P= 0.004) and postoperative complications (95 % CI : 1.29 to 9.52, P= 0.013) were independent risk factors for prolonged hospital stay. OLH (95 % CI : 1.428 to 44.080, P= 0.018) and residual stones (95 % CI : 1.580 to 62.379, P= 0.014) were independent risk factors for the occurrence of postoperative biliary fistula. Biliary fistula (95 % CI : 1.078 to 24.517, P= 0.040) was an independent risk factor for the recurrence of stones. Conclusion: Compared with OLH, LLH is safe and effective for the treatment of the primary left-sided hepatolithiasis with the clinical benefits of shorter hospital stay, fewer morbidity and biliary fistula occurrence, and lower stone recurrence rates.

Published
2020
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32. Antidepressant activity of aqueous extracts of Curcuma longa in mice.

Author

Yu ZF, Kong LD, and Chen Y

Subjects
Administration, Oral, Animals, Antidepressive Agents administration & dosage, Antidepressive Agents therapeutic use, Brain drug effects, Brain metabolism, Depression drug therapy, Dose-Response Relationship, Drug, Fluoxetine administration & dosage, Fluoxetine pharmacology, Fluoxetine therapeutic use, Male, Mice, Mice, Inbred ICR, Mitochondria drug effects, Mitochondria metabolism, Motor Activity drug effects, Plant Extracts administration & dosage, Plant Extracts therapeutic use, Antidepressive Agents pharmacology, Curcuma, Monoamine Oxidase metabolism, Phytotherapy, Plant Extracts pharmacology
Abstract

Curcuma longa (turmeric) is a well-known indigenous herbal medicine. The aqueous extracts, when administered orally to the mice from 140 to 560 mg/kg for 14 days, were able to elicit dose-dependent relation of immobility reduction in the tail suspension test and the forced swimming test in mice. The effects of the extracts at the dose of 560 mg/kg were more potent than that of reference antidepressant fluoxetine. The extracts, at the dose of 140 mg/kg or above for 14 days, significantly inhibited the monoamine oxidize A (MAO) activity in mouse whole brain at a dose-dependent manner, however, oral administration of the extract only at a dose of 560 mg/kg produced observable MAO B inhibitory activity in animal brain. Fluoxetine showed only a tendency to inhibit MAO A and B activity in animal brain in the study. Neither the extracts of C. longa nor fluoxetine, at the doses tested, produced significant effects on locomotor activity. These results demonstrated that C. longa had specifically antidepressant effects in vivo. The activity of C. longa in antidepression may mediated in part through MAO A inhibition in mouse brain.

Published
2002
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33. N-Methylformamide in advanced squamous cancer of the uterine cervix: an Eastern Cooperative Oncology Group phase II trial.

Author

Rajdev L, Yu ZF, Wadler S, Weller E, Kahn SB, Tormey D, Skeel R, and Wiernik PH

Subjects
Aged, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Carcinoma, Squamous Cell mortality, Carcinoma, Squamous Cell secondary, Cell Differentiation, Drug Administration Schedule, Female, Formamides administration & dosage, Formamides adverse effects, Humans, Middle Aged, Survival Rate, Treatment Outcome, Uterine Cervical Neoplasms mortality, Uterine Cervical Neoplasms pathology, Antineoplastic Agents therapeutic use, Carcinoma, Squamous Cell drug therapy, Formamides therapeutic use, Uterine Cervical Neoplasms drug therapy
Abstract

Purpose: Preclinical and clinical data support the study of polar-planar compounds such as N-Methylformamide (NMF) in advanced squamous cell carcinoma of the uterine cervix (SCC). This phase II trial sought to determine the efficacy and toxicities of NMF in patients with advanced SCC., Patients and Methods: Eligibility for this trial required bidimensionally measurable squamous or adenosquamous cell cancer of the uterine cervix incurable by surgery or radiation therapy, ECOG performance status of < or = 2, no prior NMF and no more than one prior chemotherapy regimen. Patients received NMF at 2000 mg/m2 intravenously over 15-30 minutes days 1, 8 and 15. The cycle was repeated every 42 days. A single dose escalation of 25%, 500 mg/m2 was made after the first cycle if the toxicities did not exceed grade I for hepatic toxicity and grade II for nausea and vomiting., Results: From July 1987 through September 1998, 21 patients with advanced squamous cell carcinoma of the uterine cervix were entered on study. Two patients were ineligible because there was no pretreatment SGOT on one and the other deteriorated prior to drug approval. Therefore, 19 patients were include in the analysis of response and survival. Four were inevaluable, three due to inappropriate tumor evaluation and one secondary to grade III vomiting, who went off study. These patients were included in the denominator while computing the results. There were 2 deaths, one due to pulmonary hemorrhage from perforation during central venous insertion and one due to disease. 30% (6/19) patients had toxicities, Eastern Cooperative Oncology Group (ECOG) grade III or higher and 2 of these patients suffered multiple grade III toxicities. There were no complete or partial responses., Conclusion: In this population, NMF in the dose and schedule employed exhibited no clinical activity.

Published
2001
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34. Pivotal role for acidic sphingomyelinase in cerebral ischemia-induced ceramide and cytokine production, and neuronal apoptosis.

Author

Yu ZF, Nikolova-Karakashian M, Zhou D, Cheng G, Schuchman EH, and Mattson MP

Subjects
Animals, Apoptosis, Brain pathology, Bridged-Ring Compounds pharmacology, Calcium metabolism, Cell Survival, Cerebral Cortex pathology, Cerebral Infarction pathology, Cerebral Infarction physiopathology, Disease Models, Animal, Enzyme Activation drug effects, Homeostasis, Ischemic Attack, Transient enzymology, Ischemic Attack, Transient genetics, Kinetics, Mice, Mice, Knockout, Neurons cytology, Neurons pathology, Norbornanes, Phosphodiesterase Inhibitors pharmacology, Second Messenger Systems, Sphingomyelin Phosphodiesterase deficiency, Sphingomyelin Phosphodiesterase genetics, Thiocarbamates, Thiones pharmacology, Ceramides metabolism, Cerebral Cortex enzymology, Cytokines biosynthesis, Ischemic Attack, Transient physiopathology, Neurons physiology, Sphingomyelin Phosphodiesterase metabolism
Abstract

Stroke is a major cause of long-term disability, the severity of which is directly related to the numbers of neurons that succumb to the ischemic insult. The signaling cascades activated by cerebral ischemia that may either promote or protect against neuronal death are not well understood. One injury-responsive signaling pathway that has recently been characterized in studies of non-neural cells involves cleavage of membrane sphingomyelin by acidic and/or neutral sphingomyelinase (ASMase) resulting in generation of the second messenger ceramide. We now report that transient focal cerebral ischemia induces large increases in ASMase activity, ceramide levels, and production of inflammatory cytokines in wild-type mice, but not in mice lacking ASMase. The extent of brain tissue damage is decreased and behavioral outcome improved in mice lacking ASMase. Neurons lacking ASMase exhibit decreased vulnerability to excitotoxicity and hypoxia, which is associated with decreased levels of intracellular calcium and oxyradicals. Treatment of mice with a drug that inhibits ASMase activity and ceramide production reduces ischemic neuronal injury and improves behavioral outcome, suggesting that drugs that inhibit this signaling pathway may prove beneficial in stroke patients.

Published
2000
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35. Apoptotic and antiapoptotic mechanisms in stroke.

Author

Mattson MP, Culmsee C, and Yu ZF

Subjects
Animals, Apoptosis Regulatory Proteins, Brain anatomy & histology, Brain metabolism, Brain physiopathology, Brain Ischemia genetics, Brain Ischemia pathology, Brain Ischemia physiopathology, Calcium physiology, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Nucleus genetics, Cell Nucleus physiology, Cell Nucleus ultrastructure, Cytokines physiology, Gene Expression, Humans, Mice, Mitochondria physiology, Models, Biological, Nerve Growth Factors physiology, Neurons cytology, Neurons metabolism, Neurons physiology, Rats, Reactive Oxygen Species physiology, Signal Transduction, Stroke genetics, Stroke pathology, Apoptosis physiology, Intracellular Signaling Peptides and Proteins, Stroke physiopathology
Abstract

Apoptosis is a form of programmed cell death that occurs in neurons during development of the nervous system and may also be a prominent form of neuronal death in chronic neurodegenerative disorders such as Alzheimer's and Parkinson's diseases. Recent findings also implicate apoptosis in neuronal degeneration after ischemic brain injury in animal models of stroke. Activation of both apoptotic and antiapoptotic signaling cascades occurs in neurons in animal and cell culture models of stroke. Apoptotic cascades involve: increased levels of intracellular oxyradicals and calcium; induction of expression of proteins such as Par-4 (prostate apoptosis response-4), which act by promoting mitochondrial dysfunction and suppressing antiapoptotic mechanisms; mitochondrial membrane depolarization, calcium uptake, and release of factors (e.g., cytochrome c) that ultimately induce nuclear DNA condensation and fragmentation; activation of cysteine proteases of the caspase family; activation of transcription factors such as AP-1 that may induce expression of "killer genes." Antiapoptotic signaling pathways are activated by neurotrophic factors, certain cytokines, and increases in oxidative and metabolic stress. Such protective pathways include: activation of the transcription factors (e.g., nuclear factor-kappa B, NF-kappa B) that induce expression of stress proteins, antioxidant enzymes, and calcium-regulating proteins; phosphorylation-mediated modulation of ion channels and membrane transporters; cytoskeletal alterations that modulate calcium homeostasis; and modulation of proteins that stabilize mitochondrial function (e.g., Bcl-2). Intervention studies in experimental stroke models have identified a battery of approaches of potential benefit in reducing neuronal death in stroke patients, including administration of antioxidants, calcium-stabilizing agents, caspase inhibitors, and agents that activate NF-kappa B. Interestingly, recent studies suggest novel dietary approaches (e.g., food restriction and supplementation with antioxidants) that may reduce brain damage following stroke.

Published
2000
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36. Dietary restriction and 2-deoxyglucose administration reduce focal ischemic brain damage and improve behavioral outcome: evidence for a preconditioning mechanism.

Author

Yu ZF and Mattson MP

Subjects
Animals, Cells, Cultured, Cerebral Infarction pathology, Cerebral Infarction prevention & control, Energy Intake, Heat-Shock Proteins metabolism, Hippocampus cytology, Hippocampus drug effects, Hypoxia, Brain prevention & control, Ischemic Attack, Transient diet therapy, Ischemic Attack, Transient drug therapy, Male, Neurons drug effects, Rats, Rats, Sprague-Dawley, Reperfusion Injury therapy, Behavior, Animal drug effects, Deoxyglucose therapeutic use, Ischemic Attack, Transient therapy, Ischemic Preconditioning, Neuroprotective Agents therapeutic use
Abstract

Stroke, an age-related disorder involving degeneration of neurons resulting from cerebral ischemia, is a major cause of disability and mortality. Although dietary restriction (DR) extends lifespan and reduces levels of cellular oxidative stress in several different organ systems including the brain, the impact of DR on ischemic brain injury is unknown. We report that maintenance of adult rats on a DR regimen resulted in reduced brain damage and improved behavioral outcome in a middle cerebral artery occlusion-reperfusion (MCAO-R) stroke model. Administration of 2-deoxyglucose (2-DG), a nonmetabolizable analogue of glucose, to rats fed ad libitum resulted in reduced ischemic brain damage and improved behavioral outcome following MCAO-R. 2-DG protected cultured hippocampal neurons against chemical hypoxia, demonstrating a direct protective action on neurons. DR and 2-DG administration resulted in an increase in the level of the stress protein heat-shock protein 70 (HSP-70) in striatal cells in vivo, and 2-DG treatment induced HSP-70 in cultured neurons suggesting involvement of a preconditioning stress response in the neuroprotective actions of DR and 2-DG. The neuroprotective effect of DR and 2-DG in this focal cerebral ischemia model suggests that outcome following stroke may be improved in individuals who follow a regimen of reduced food intake., (Copyright 1999 Wiley-Liss, Inc.)

Published
1999

37. Uric acid protects neurons against excitotoxic and metabolic insults in cell culture, and against focal ischemic brain injury in vivo.

Author

Yu ZF, Bruce-Keller AJ, Goodman Y, and Mattson MP

Subjects
Animals, Calcium metabolism, Cell Death drug effects, Cells, Cultured, Cerebral Cortex drug effects, Glutamic Acid toxicity, Hippocampus, Ischemic Attack, Transient physiopathology, Lipid Peroxidation drug effects, Male, Membrane Potentials drug effects, Microscopy, Confocal, Mitochondria drug effects, Mitochondria physiology, Neostriatum drug effects, Neurons metabolism, Neuroprotective Agents therapeutic use, Oxidative Stress drug effects, Rats, Rats, Sprague-Dawley, Reactive Oxygen Species metabolism, Sodium Cyanide toxicity, Uric Acid administration & dosage, Uric Acid therapeutic use, Ischemic Attack, Transient drug therapy, Neurons drug effects, Neuroprotective Agents pharmacology, Uric Acid pharmacology
Abstract

Uric acid is a well-known natural antioxidant present in fluids and tissues throughout the body. Oxyradical production and cellular calcium overload are believed to contribute to the damage and death of neurons that occurs following cerebral ischemia in victims of stroke. We now report that uric acid protects cultured rat hippocampal neurons against cell death induced by insults relevant to the pathogenesis of cerebral ischemia, including exposure to the excitatory amino acid glutamate and the metabolic poison cyanide. Confocal laser scanning microscope analyses showed that uric acid suppresses the accumulation of reactive oxygen species (hydrogen peroxide and peroxynitrite), and lipid peroxidation, associated with each insult. Mitochondrial function was compromised by the excitotoxic and metabolic insults, and was preserved in neurons treated with uric acid. Delayed elevations of intracellular free calcium levels induced by glutamate and cyanide were significantly attenuated in neurons treated with uric acid. These data demonstrate a neuroprotective action of uric acid that involves suppression of oxyradical accumulation, stabilization of calcium homeostasis, and preservation of mitochondrial function. Administration of uric acid to adult rats either 24 hr prior to middle cerebral artery occlusion (62.5 mg uric acid/kg, intraperitoneally) or 1 hr following reperfusion (16 mg uric acid/kg, intravenously) resulted in a highly significant reduction in ischemic damage to cerebral cortex and striatum, and improved behavioral outcome. These findings support a central role for oxyradicals in excitotoxic and ischemic neuronal injury, and suggest a potential therapeutic use for uric acid in ischemic stroke and related neurodegenerative conditions.

Published
1998
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38. [Studies on desensitization of GABAB receptor coupled adenylate cyclase].

Author

Yu ZF, Cheng GJ, and Hu BR

Subjects
Animals, Binding Sites physiology, GTP-Binding Proteins metabolism, Male, Mice, Protein Kinase C metabolism, Synaptic Membranes metabolism, Adenylyl Cyclases metabolism, Baclofen pharmacology, GABA Agonists pharmacology, Receptors, GABA-B metabolism
Abstract

After preincubation of crude synaptic membranes (P2 membranes) with phorber ester (PMA) or GABAB receptor agonist baclofen (BAL), the rate of inhibition of BAL on basal adenylate cyclase (AC) activity and forskolin-stimulated AC activity significantly reduced (desensitized). This effect of BAL did not change after preincubation with forskolin suggesting that the desensitization mechanism of GABAB receptor coupled AC is related with activation of protein kinase C (PKC), but not with protein kinase A. It was further found that the equilibrium dissociation constant (Kd) of GABAB receptor was increased during desensitization. Our results suggest that PKC activation may cause some structural or conformational changes of GABAB receptor, resulting in an uncoupling from G protein and desensitization of GABAB receptor-coupled AC.

Published
1997

39. [Improvement of learning and memory functions by GABAB receptor antagonists in mice].

Author

Yu ZF, Hu BR, and Cheng GJ

Subjects
Animals, Baclofen antagonists & inhibitors, Baclofen pharmacology, Female, Male, Mice, GABA Antagonists pharmacology, Learning drug effects, Memory drug effects, Organophosphorus Compounds pharmacology
Abstract

In one trial passive avoidance response in mice, the effects of gamma-aminobutyric acid (GABA)B receptor agonist baclofen and antagonist CGP35348 and CGP36742 on acquisition, consolidation and retrieval of memory were observed. The results showed that the antagonists could significantly promote the acquisition impairment induced by baclofen, the consolidation impairment induced by baclofen and NaNO2, and the retrieval impairment induced by baclofen and 30% alcohol. These results suggest that the GABAB receptor antagonists may become a novel type of drug for the treatment of Alzheimer's disease.

Published
1996

40. [32 cases of sudden deafness treated with sequential external counterpulsation in addition to combined traditional Chinese medicine and Western medicine therapy].

Author

Yu ZF

Subjects
Adenosine Triphosphate therapeutic use, Adolescent, Adult, Aged, Combined Modality Therapy, Female, Humans, Lidocaine therapeutic use, Male, Middle Aged, Plant Extracts, Salvia miltiorrhiza, Counterpulsation, Drugs, Chinese Herbal therapeutic use, Hearing Loss, Sudden therapy
Abstract

The present study includes 32 cases of sudden deafness treated with Sequential External Counterpulsation in addition to combined TCM-WM therapy, 30 cases treated with combined TCM-WM, and 30 cases treated with WM alone. The clinical findings of these 3 groups were quite similar, hence they were comparable. The mean duration of treatment, percentage of effectiveness and percentage of recurrence within 3 years were 13 days, 75% and 16.6% respectively in the first group; 19 days, 56.6% and 29.4% in the second group; and 21 days, 53.2% and 37.5% in the third group. The first group showed shorter duration of treatment higher effective rate and lower recurrence rate; and all their differences were statistically significant (P < 0.05). The data revealed that, the treatment of sudden deafness with Sequential External Counterpulsation in addition to combined TCM-WM has great advantage over treatment with combined TCM-WM or WM alone.

Published
1993

41. [Studies of the spasm-relieving effect of Glycyrrhiza uralensis Fisch.--Aster tataricus L.F. pulvis mixture on the trachea in guinea pigs].

Author

Liu LM, Yu ZF, and Wu CY

Subjects
Acetylcholine antagonists & inhibitors, Animals, Drug Synergism, Guinea Pigs, Histamine Antagonists pharmacology, In Vitro Techniques, Male, Muscle Relaxation drug effects, Trachea drug effects, Drugs, Chinese Herbal pharmacology, Glycyrrhiza, Muscle, Smooth drug effects, Plants, Medicinal
Abstract

The experiment shows that high concentration of Aster tataricus plus Glycyrrhiza uralensis Fisch. can inhibit the tracheal systoliea caused by histamine, but for tracheal systoliea caused by acetylcholine the inhibition is indistinct. The experiment also shows that Aster tataricus, glycyrrhiza uralensis and Tussilago far fara L. combined have coordinated inhibiting effect on the tracheal systoliea caused by histamine and acetylcholine.

Published
1993

42. Infiltrating lymphocytes and accessory cells in nasopharyngeal carcinoma.

Author

Zong YS, Zhang CQ, Zhang F, Ruan JB, Chen MY, Feng KT, and Yu ZF

Subjects
Humans, Immunoenzyme Techniques, Lymphocyte Subsets, Nasopharyngeal Neoplasms mortality, Nasopharyngeal Neoplasms pathology, Neoplasm Metastasis, Antigen-Presenting Cells immunology, Lymphocytes, Tumor-Infiltrating immunology, Nasopharyngeal Neoplasms immunology
Abstract

The infiltrating lymphocytes (LCs) and accessory cells (ACs) including dendritic cells (DCs) and monocytes/macrophages in nasopharyngeal biopsies taken from 4 groups of nasopharyngeal carcinoma (NPC) patients were observed by using an immunostaining technique and the correlation of the results to the clinical manifestations and follow-up data was examined. The findings were as follows. (1) NPCs without lymph node metastasis always had marked infiltrating LCs and DCs as compared with those with lymph node(s) metastasis. (2) Advanced NPCs with lymph node(s) involvement (T1-4N1-3M0) and a rapid development of distant metastasis followed by death within 1 year after radiotherapy always showed fewer infiltrating LCs and DCs as compared with those with lymph node(s) metastasis (T1-4N1-3M0) and having longer than 5-year survival after radiotherapy. The amount of both LCs and ACs, especially DCs, infiltrating in NPC tissues appears to be an indicator of the activity of host immune defence mechanisms against cancer and influences the progression of the neoplasm as well as the prognosis.

Published
1993
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43. Ultrasonic studies of the effect of artemisia decoction on the volume and dynamics of gallbladder.

Author

Yu ZF and Wu XS

Subjects
Adolescent, Adult, Child, Female, Gallbladder physiology, Humans, Male, Middle Aged, Muscle Contraction drug effects, Muscle, Smooth drug effects, Ultrasonography, Cholagogues and Choleretics pharmacology, Drugs, Chinese Herbal pharmacology, Gallbladder diagnostic imaging, Gallbladder drug effects
Abstract

This paper deals with the ultrasonic studies of the effect of artemisia decoction (AD) on the volume and motion of gallbladder in 33 cases. Ultrasonic examination shows that AD intravenous infusion has remarkable effects on the contractility of gallbladder. There are 4 patterns of phasic changes in the motion of gallbladder and an increase in frequency of its contraction and relaxation. AD has also certain contraction effects on the gallbladders which can not contract after a fatty meal. The above findings indicate that AD is a good choleretic and has a definite regulating effect on the motility of the gallbladder. The clinical use of AD is conducive to bile flow, stone expelling, inhibiting the deposition of bile solids and reducing the possibility of stone formation.

Published
1993

45. Elimination of malignant clonogenic cells from human bone marrow using multiple myeloid cell-specific monoclonal antibodies and complement.

Author

Hu ZB, Yu ZF, Qiao CN, and Ma WL

Subjects
Animals, Antibodies, Monoclonal, Antibodies, Neoplasm immunology, Bone Marrow pathology, Colony-Forming Units Assay, Humans, Leukemia, Myeloid immunology, Leukemia, Promyelocytic, Acute immunology, Mice, Rabbits, Tumor Cells, Cultured, Tumor Stem Cell Assay, Complement System Proteins immunology, Leukemia, Myeloid pathology, Leukemia, Promyelocytic, Acute pathology
Abstract

Single or combined monoclonal antibodies (McAbs) Zh53, Zh820, and Zh2-1 have been used to eliminate malignant clonogenic cells from human bone marrow. The test of cytotoxicity showed that all of these McAbs could express high specific cytotoxic action against HL-60 cells and were selectively complement-dependent cytotoxic to various types of fresh leukemic cells. Clonogenic assay detected that single treatment with antibody and rabbit complement (RC) could reduce clonogenic units of HL-60 cells by more than 2 logs and two treatments reduced clonogenic units by more than 4 logs. However, combination of 2 McAbs could reduce clonogenic units by 4-5 logs. The data suggest that multiple treatments with McAbs and RC or a combination of 2 McAbs are more effective than a single treatment in eliminating clonogenic tumor cells. Treatment of normal human bone marrow with Zh53, Zh2-1 and RC did not produce a loss of normal CFU-GM, but treatment with Zh820 reduced the clonic units of normal CFU-GM by 24%.

Published
1991

47. [Advances in research on the relation between the kidney and the ear].

Author

Yu ZF

Subjects
Aldosterone pharmacology, Animals, Anti-Bacterial Agents adverse effects, Bone Diseases complications, Ear, Inner drug effects, Ear, Inner physiopathology, Hearing Disorders complications, Humans, Kidney Diseases complications, Water-Electrolyte Balance, Ear physiopathology, Kidney physiopathology, Medicine, Chinese Traditional, Medicine, East Asian Traditional
Published
1985

48. Chemo-immunotherapy versus chemotherapy in acute leukemia remission induction.

Author

Yu ZF, Lin MF, Wang BC, Lin XJ, and Lin XH

Subjects
Acute Disease, Adolescent, Adult, BCG Vaccine therapeutic use, Child, Humans, Leukemia immunology, Measles Vaccine therapeutic use, Middle Aged, Antineoplastic Agents administration & dosage, Immunotherapy methods, Leukemia therapy
Published
1981

50. Experimental research on Artemisia decoction and general attack therapy in cholelithiasis.

Author

Yu ZF and Guo ZG

Subjects
Animals, Bile physiology, Blood Pressure drug effects, Dogs, Humans, Morphine pharmacology, Muscle Contraction drug effects, Muscle Relaxation drug effects, Plant Extracts therapeutic use, Sphincter of Oddi drug effects, Sphincter of Oddi physiology, Cholelithiasis drug therapy, Medicine, Chinese Traditional, Medicine, East Asian Traditional
Published
1980

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