Your search keyword '"Sura T"' showing total 72 results

1. A Haplotype of the Human CXCR1 Gene Protective against Rapid Disease Progression in HIV-1⁺ Patients

Author

Vasilescu, A., Terashima, Y., Enomoto, M., Heath, S., Poonpiriya, V., Gatanaga, H., Do, H., Diop, G., Hirtzig, T., Auewarakul, P., Lauhakirti, D., Sura, T., Charneau, P., Marullo, S., Therwath, A., Oka, S., Kanegasaki, S., Lathrop, M., Matsushima, K., Zagury, J.-F., and Matsuda, F.

Published

2007

2. Number of Electricity Hours Generation Map for Different Wind Turbines in the Province of Wasit â€' Iraq

Author

Rawnak A. Abdul wahab, Sura T. Nassir, and Firas A. Hadi

Subjects

General Computer Science, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

Wind energy is becoming one of the renewable energy that has attracted great attention all over the world. This research work aims to build a map by which the user can have a thought about the number of generation hours of electricity from wind through all the year at the location of study (Wasit-Iraq). To interact the idea, this study included using the work included using different wind turbines at different heights. The results show that Gamesa G58-850 KW wind turbine gives more generated hours at 50 meters height.

Published

2019

3. Genome-wide SNP-based linkage analysis of tuberculosis in Thais

Author

Mahasirimongkol, S, Yanai, H, Nishida, N, Ridruechai, C, Matsushita, I, Ohashi, J, Summanapan, S, Yamada, N, Moolphate, S, Chuchotaworn, C, Chaiprasert, A, Manosuthi, W, Kantipong, P, Kanitwittaya, S, Sura, T, Khusmith, S, Tokunaga, K, Sawanpanyalert, P, and Keicho, N

Published

2009

4. The temporal and spatial distribution of wind factor in Iraq

Author

Sura T. Nassir, Azhaar K. Mishaal, Ahmed B. Khamees, and Mudar Ahmed Abdulsattar

Subjects

Factor (chord), Multidisciplinary, Physics and Astronomy (miscellaneous), Chemistry (miscellaneous), Statistics, Computer Science (miscellaneous), Environmental science, Statistical model, Autoregressive integrated moving average, Spatial distribution, Biochemistry, Genetics and Molecular Biology (miscellaneous)

Published

2020

5. HPR41 Predictors of Epidermal Growth Factor (EGFR) Testing Among Patients with Metastatic Non-Small Cell Lung Cancer (MNSCLC) Treated in the Real-World Setting

Author

Vasudevan, A., Sura, T., English, S., Wang, B., Varughese, P., and Katzen, H.

Published

2023

6. Development, testing and design optimisation of a water and R134a based thermosyphon heat exchanger for air-water heat recovery systems

Author

Kanchit Rongchai and Sura Tundee

Subjects

Thermal performance, Thermosyphons, Heat exchanger, Nusselt number, Reynolds number, Engineering (General). Civil engineering (General), TA1-2040

Abstract

Heat pipes find their increasing uses in heat recovery and energy saving in thermal systems. Our work involves the designing, building, and testing of a heat pipe heat exchanger made of 28 copper thermosyphons. We investigated the use of distilled water and R134a as the thermosyphons’ working fluid with optimisation. The thermosyphons were arranged into four rows by seven columns with a hot air flow at the evaporator and a cooling water flow at the condenser. The performance was tested in three working fluid cases: distilled water, R134a, and a hybrid. The hot air flowrate was varied and at temperatures of 80 °C, 110 °C, and 140 °C to investigate the performance. The results show that increasing the air flow temperature increased the effectiveness. Optimisation was examined using the ε-NTU analysis and revealed that R134a offered the highest effectiveness with a relatively small NTU. Tested using three values of Cr, highest effectiveness of 30%, 51% and 40% for distilled water, R134a, and the hybrid respectively, was achieved across all fluid cases at Cr = 0.15. A Reynolds analysis performed to compare the effect of relative flows over the evaporator and condenser showed that increasing Reh/Rec, increased the heat transfer at the condenser and the overall effectiveness. At Reh/Rec = 2500, heat transfer was 500 W, 2000 W and 800 W for distilled water, R134a, and the hybrid respectively. Our work could potentially be useful in the designing and optimising of a thermosyphon heat exchanger for saving energy in air-water heat handling applications.

Published

2022

7. Search for anomalous production of events with a photon, jet, b-quark jet, and missing transverse energy RID G-1087-2011 RID E-4473-2011

Author

Aaltonen, T, Adelman, J, Akimoto, T, Gonzalez, Ba, Amerio, S, Amidei, D, Anastassov, A, Annovi, A, Antos, J, Apollinari, G, Apresyan, A, Arisawa, T, Artikov, A, Ashmanskas, W, Attal, A, Aurisano, A, Azfar, F, Azzurri, P, Badgett, W, Barbaro Galtieri, A, Barnes, Ve, Barnett, Ba, Bartsch, V, Bauer, G, Beauchemin, Ph, Bedeschi, F, Beecher, D, Behari, S, Bellettini, G, Bellinger, J, Benjamin, D, Beretvas, A, Beringer, J, Bhatti, A, Binkley, M, Bisello, D, Bizjak, I, Blair, Re, Blocker, C, Blumenfeld, B, Bocci, A, Bodek, A, Boisvert, V, Bolla, G, Bortoletto, D, Boudreau, J, Boveia, A, Brau, B, Bridgeman, A, Brigliadori, L, Bromberg, C, Brubaker, E, Budagov, J, Budd, Hs, Budd, S, Burke, S, Burkett, K, Busetto, G, Bussey, P, Buzatu, A, Byrum, Kl, Cabrera, S, Calancha, C, Campanelli, M, Campbell, M, Canelli, F, Canepa, A, Carls, B, Carlsmith, D, Carosi, R, Carrillo, S, Carron, S, Casal, B, Casarsa, M, Castro, A, Catastini, P, Cauz, D, Cavaliere, V, Cavalli Sforza, M, Cerri, A, Cerrito, L, Chang, Sh, Chen, Yc, Chertok, M, Chiarelli, G, Chlachidze, G, Chlebana, F, Cho, K, Chokheli, D, Chou, Jp, Choudalakis, G, Chuang, Sh, Chung, K, Chung, Wh, Chung, Ys, Chwalek, T, Ciobanu, Ci, Ciocci, Ma, Clark, A, Clark, D, Compostella, G, Convery, Me, Conway, J, Cordelli, M, Cortiana, G, Cox, Ca, Cox, Dj, Crescioli, F, Almenar, Cc, Cuevas, J, Culbertson, R, Cully, Jc, Dagenhart, D, Datta, M, Davies, T, de Barbaro, P, De Cecco, S, Deisher, A, De Lorenzo, G, Dell'Orso, Mauro, Deluca, C, Demortier, L, Deng, J, Deninno, M, Derwent, Pf, di Giovanni GP, Dionisi, C, Di Ruzza, B, Dittmann, Jr, D'Onofrio, M, Donati, Simone, Dong, P, Donini, J, Dorigo, T, Dube, S, Efron, J, Elagin, A, Erbacher, R, Errede, D, Errede, S, Eusebi, R, Fang, Hc, Farrington, S, Fedorko, Wt, Feild, Rg, Feindt, M, Fernandez, Jp, Ferrazza, C, Field, R, Flanagan, G, Forrest, R, Frank, Mj, Franklin, M, Freeman, Jc, Frisch, Hj, Furic, I, Gallinaro, M, Galyardt, J, Garberson, F, Garcia, Je, Garfinkel, Af, Genser, K, Gerberich, H, Gerdes, D, Gessler, A, Giagu, S, Giakoumopoulou, V, Giannetti, P, Gibson, K, Gimmell, Jl, Ginsburg, Cm, Giokaris, N, Giordani, M, Giromini, P, Giunta, M, Giurgiu, G, Glagolev, V, Glenzinski, D, Gold, M, Goldschmidt, N, Golossanov, A, Gomez, G, Gomez Ceballos, G, Goncharov, M, Gonzalez, O, Gorelov, I, Goshaw, At, Goulianos, K, Gresele, A, Grinstein, S, Grosso Pilcher, C, Group, Rc, Grundler, U, da Costa JG, Gunay Unalan, Z, Haber, C, Hahn, K, Hahn, Sr, Halkiadakis, E, Han, By, Han, Jy, Happacher, F, Hara, K, Hare, D, Hare, M, Harper, S, Harr, Rf, Harris, Rm, Hartz, M, Hatakeyama, K, Hays, C, Heck, M, Heijboer, A, Heinrich, J, Henderson, C, Herndon, M, Heuser, J, Hewamanage, S, Hidas, D, Hill, Cs, Hirschbuehl, D, Hocker, A, Hou, S, Houlden, M, Hsu, Sc, Huffman, Bt, Hughes, Re, Husemann, U, Hussein, M, Huston, J, Incandela, J, Introzzi, G, Iori, M, Ivanov, A, James, E, Jang, D, Jayatilaka, B, Jeon, Ej, Jha, Mk, Jindariani, S, Johnson, W, Jones, M, Joo, Kk, Jun, Sy, Jung, Je, Junk, Tr, Kamon, T, Kar, D, Karchin, Pe, Kato, Y, Kephart, R, Keung, J, Khotilovich, V, Kilminster, B, Kim, Dh, Kim, Hs, Kim, Hw, Kim, Je, Kim, Mj, Kim, Sb, Kim, Sh, Kim, Yk, Kimura, N, Kirsch, L, Klimenko, S, Knuteson, B, Ko, Br, Kondo, K, Kong, Dj, Konigsberg, J, Korytov, A, Kotwal, Av, Kreps, M, Kroll, J, Krop, D, Krumnack, N, Kruse, M, Krutelyov, V, Kubo, T, Kuhr, T, Kulkarni, Np, Kurata, M, Kwang, S, Laasanen, At, Lami, S, Lammel, S, Lancaster, M, Lander, Rl, Lannon, K, Lath, A, Latino, G, Lazzizzera, I, Lecompte, T, Lee, E, Lee, Hs, Lee, Sw, Leone, S, Lewis, Jd, Lin, Cs, Linacre, J, Lindgren, M, Lipeles, E, Lister, A, Litvintsev, Do, Liu, C, Liu, T, Lockyer, Ns, Loginov, A, Loreti, M, Lovas, L, Lucchesi, D, Luci, C, Lueck, J, Lujan, P, Lukens, P, Lungu, G, Lyons, L, Lys, J, Lysak, R, Macqueen, D, Madrak, R, Maeshima, K, Makhoul, K, Maki, T, Maksimovic, P, Malde, S, Malik, S, Manca, G, Manousakis Katsikakis, A, Margaroli, F, Marino, C, Marino, Cp, Martin, A, Martin, V, Martinez, M, Martinez Ballarin, R, Maruyama, T, Mastrandrea, P, Masubuchi, T, Mathis, M, Mattson, Me, Mazzanti, P, Mcfarland, Ks, Mcintyre, P, Mcnulty, R, Mehta, A, Mehtala, P, Menzione, A, Merkel, P, Mesropian, C, Miao, T, Miladinovic, N, Miller, R, Mills, C, Milnik, M, Mitra, A, Mitselmakher, G, Miyake, H, Moggi, N, Moon, Cs, Moore, R, Morello, Mj, Morlock, J, Fernandez, Pm, Mulmenstadt, J, Mukherjee, A, Muller, T, Mumford, R, Murat, P, Mussini, M, Nachtman, J, Nagai, Y, Nagano, A, Naganoma, J, Nakamura, K, Nakano, I, Napier, A, Necula, V, Nett, J, Neu, C, Neubauer, Ms, Neubauer, S, Nielsen, J, Nodulman, L, Norman, M, Norniella, O, Nurse, E, Oakes, L, Oh, Sh, Oh, Yd, Oksuzian, I, Okusawa, T, Orava, R, Osterberg, K, Griso, Sp, Palencia, E, Papadimitriou, V, Papaikonomou, A, Paramonov, Aa, Parks, B, Pashapour, S, Patrick, J, Pauletta, G, Paulini, M, Paus, C, Peiffer, T, Pellett, De, Penzo, A, Phillips, Tj, Piacentino, G, Pianori, E, Pinera, L, Pitts, K, Plager, C, Pondrom, L, Poukhov, O, Pounder, N, Prakoshyn, F, Pronko, A, Proudfoot, J, Ptohos, F, Pueschel, E, Punzi, Giovanni, Pursley, J, Rademacker, J, Rahaman, A, Ramakrishnan, V, Ranjan, N, Redondo, I, Renton, P, Renz, M, Rescigno, M, Richter, S, Rimondi, F, Ristori, L, Robson, A, Rodrigo, T, Rodriguez, T, Rogers, E, Rolli, S, Roser, R, Rossi, M, Rossin, R, Roy, P, Ruiz, A, Russ, J, Rusu, V, Saarikko, H, Safonov, A, Sakumoto, Wk, Salto, O, Santi, L, Sarkar, S, Sartori, L, Sato, K, Savoy Navarro, A, Schlabach, P, Schmidt, A, Schmidt, Ee, Schmidt, Ma, Schmidt, Mp, Schmitt, M, Schwarz, T, Scodellaro, L, Scribano, A, Scuri, F, Sedov, A, Seidel, S, Seiya, Y, Semenov, A, Sexton Kennedy, L, Sforza, F, Sfyrla, A, Shalhout, Sz, Shears, T, Shepard, Pf, Shimojima, M, Shiraishi, S, Shochet, M, Shon, Y, Shreyber, I, Sidoti, A, Sinervo, P, Sisakyan, A, Slaughter, Aj, Slaunwhite, J, Sliwa, K, Smith, Jr, Snider, Fd, Snihur, R, Soha, A, Somalwar, S, Sorin, V, Spalding, J, Spreitzer, T, Squillacioti, P, Stanitzki, M, St Denis, R, Stelzer, B, Stelzer Chilton, O, Stentz, D, Strologas, J, Strycker, Gl, Stuart, D, Suh, Js, Sukhanov, A, Suslov, I, Suzuki, T, Taffard, A, Takashima, R, Takeuchi, Y, Tanaka, R, Tecchio, M, Teng, Pk, Terashi, K, Thom, J, Thompson, As, Thompson, Ga, Thomson, E, Tipton, P, Ttito Guzman, P, Tkaczyk, S, Toback, D, Tokar, S, Tollefson, K, Tomura, T, Tonelli, D, Torre, S, Torretta, D, Totaro, P, Tourneur, S, Trovato, M, Tsai, Sy, Tu, Y, Turini, N, Ukegawa, F, Vallecorsa, S, van Remortel, N, Varganov, A, Vataga, E, Vazquez, F, Velev, G, Vellidis, C, Vidal, M, Vidal, R, Vila, I, Vilar, R, Vine, T, Vogel, M, Volobouev, I, Volpi, G, Wagner, P, Wagner, Rg, Wagner, Rl, Wagner, W, Wagner Kuhr, J, Wakisaka, T, Wallny, R, Wang, Sm, Warburton, A, Waters, D, Weinberger, M, Weinelt, J, Wester, Wc, Whitehouse, B, Whiteson, D, Wicklund, Ab, Wicklund, E, Wilbur, S, Williams, G, Williams, Hh, Wilson, P, Winer, Bl, Wittich, P, Wolbers, S, Wolfe, C, Wright, T, Wu, X, Wurthwein, F, Xie, S, Yagil, A, Yamamoto, K, Yamaoka, J, Yang, Uk, Yang, Yc, Yao, Wm, Yeh, Gp, Yoh, J, Yorita, K, Yoshida, T, Yu, Gb, Yu, I, Yu, Ss, Yun, Jc, Zanello, L, Zanetti, A, Zhang, X, Zheng, Y, Zucchelli Sura, T., Tonelli, D., Torre, S., Torretta, D., Totaro, P., Tourneur, S., Tu, Y., Turini, N., Ukegawa, F., Vallecorsa, S., van Remortel, N., Varganov, A., Vataga, E., Vazquez, F., Velev, G., Vellidis, C., Veszpremi, V., Vidal, M., Vidal, R., Vila, I., Vilar, R., Vine, T., Vogel, M., Volobouev, I., Volpi, G., Wuerthwein, F., Wagner, P., Wagner, R. G., Wagner, R. L., Wagner Kuhr, J., Wagner, W., Wakisaka, T., Wallny, R., Wang, S. M., Warburton, A., Waters, D., Weinberger, M., Iii, Wester W. C., Whitehouse, B., Whiteson, D., Wicklund, A. B., Wicklund, E., Williams, G., Williams, H. H., Wilson, P., Winer, B. L., Wittich, P., Wolbers, S., Wolfe, C., Wright, T., Wu, X., Wynne, S. M., Yagil, A., Yamamoto, K., Yamaoka, J., Yang, U. K., Yang, Y. C., Yao, W. M., Yeh, G. P., Yoh, J., Yorita, K., Yoshida, T., G. B., Yu, Yu, I., S. S., Yu, Yun, J. C., Zanello, L., Zanetti, A., Zaw, I., Zhang, X., Zheng, Y., Zucchelli, S., Aaltonen, T, Adelman, J, Akimoto, T, Gonzalez, Ba, Amerio, S, Amidei, D, Anastassov, A, Annovi, A, Antos, J, Apollinari, G, Apresyan, A, Arisawa, T, Artikov, A, Ashmanskas, W, Attal, A, Aurisano, A, Azfar, F, Azzurri, P, Badgett, W, Barbaro Galtieri, A, Barnes, Ve, Barnett, Ba, Bartsch, V, Bauer, G, Beauchemin, Ph, Bedeschi, F, Beecher, D, Behari, S, Bellettini, G, Bellinger, J, Benjamin, D, Beretvas, A, Beringer, J, Bhatti, A, Binkley, M, Bisello, D, Bizjak, I, Blair, Re, Blocker, C, Blumenfeld, B, Bocci, A, Bodek, A, Boisvert, V, Bolla, G, Bortoletto, D, Boudreau, J, Boveia, A, Brau, B, Bridgeman, A, Brigliadori, L, Bromberg, C, Brubaker, E, Budagov, J, Budd, H, Budd, S, Burke, S, Burkett, K, Busetto, G, Bussey, P, Buzatu, A, Byrum, Kl, Cabrera, S, Calancha, C, Campanelli, M, Campbell, M, Canelli, F, Canepa, A, Carls, B, Carlsmith, D, Carosi, R, Carrillo, S, Carron, S, Casal, B, Casarsa, M, Castro, A, Catastini, P, Cauz, D, Cavaliere, V, Cavalli Sforza, M, Cerri, A, Cerrito, L, Chang, Sh, Chen, Yc, Chertok, M, Chiarelli, G, Chlachidze, G, Chlebana, F, Cho, K, Chokheli, D, Chou, Jp, Choudalakis, G, Chuang, Sh, Chung, K, Chung, Wh, Chung, Y, Chwalek, T, Ciobanu, Ci, Ciocci, Ma, Clark, A, Clark, D, Compostella, G, Convery, Me, Conway, J, Cordelli, M, Cortiana, G, Cox, Ca, Cox, Dj, Crescioli, F, Almenar, Cc, Cuevas, J, Culbertson, R, Cully, Jc, Dagenhart, D, Datta, M, Davies, T, de Barbaro, P, De Cecco, S, Deisher, A, De Lorenzo, G, Dell'Orso, M, Deluca, C, Demortier, L, Deng, J, Deninno, M, Derwent, Pf, di Giovanni, Gp, Dionisi, C, Di Ruzza, B, Dittmann, Jr, D'Onofrio, M, Donati, S, Dong, P, Donini, J, Dorigo, T, Dube, S, Efron, J, Elagin, A, Erbacher, R, Errede, D, Errede, S, Eusebi, R, Fang, Hc, Farrington, S, Fedorko, Wt, Feild, Rg, Feindt, M, Fernandez, Jp, Ferrazza, C, Field, R, Flanagan, G, Forrest, R, Frank, Mj, Franklin, M, Freeman, Jc, Frisch, Hj, Furic, I, Gallinaro, M, Galyardt, J, Garberson, F, Garcia, Je, Garfinkel, Af, Genser, K, Gerberich, H, Gerdes, D, Gessler, A, Giagu, S, Giakoumopoulou, V, Giannetti, P, Gibson, K, Gimmell, Jl, Ginsburg, Cm, Giokaris, N, Giordani, M, Giromini, P, Giunta, M, Giurgiu, G, Glagolev, V, Glenzinski, D, Gold, M, Goldschmidt, N, Golossanov, A, Gomez, G, Gomez Ceballos, G, Goncharov, M, Gonzalez, O, Gorelov, I, Goshaw, At, Goulianos, K, Gresele, A, Grinstein, S, Grosso Pilcher, C, Group, Rc, Grundler, U, da Costa, Jg, Gunay Unalan, Z, Haber, C, Hahn, K, Hahn, Sr, Halkiadakis, E, Han, By, Han, Jy, Happacher, F, Hara, K, Hare, D, Hare, M, Harper, S, Harr, Rf, Harris, Rm, Hartz, M, Hatakeyama, K, Hays, C, Heck, M, Heijboer, A, Heinrich, J, Henderson, C, Herndon, M, Heuser, J, Hewamanage, S, Hidas, D, Hill, C, Hirschbuehl, D, Hocker, A, Hou, S, Houlden, M, Hsu, Sc, Huffman, Bt, Hughes, Re, Husemann, U, Hussein, M, Huston, J, Incandela, J, Introzzi, G, Iori, M, Ivanov, A, James, E, Jang, D, Jayatilaka, B, Jeon, Ej, Jha, Mk, Jindariani, S, Johnson, W, Jones, M, Joo, Kk, Jun, Sy, Jung, Je, Junk, Tr, Kamon, T, Kar, D, Karchin, Pe, Kato, Y, Kephart, R, Keung, J, Khotilovich, V, Kilminster, B, Kim, Dh, Kim, H, Kim, Hw, Kim, Je, Kim, Mj, Kim, Sb, Kim, Sh, Kim, Yk, Kimura, N, Kirsch, L, Klimenko, S, Knuteson, B, Ko, Br, Kondo, K, Kong, Dj, Konigsberg, J, Korytov, A, Kotwal, Av, Kreps, M, Kroll, J, Krop, D, Krumnack, N, Kruse, M, Krutelyov, V, Kubo, T, Kuhr, T, Kulkarni, Np, Kurata, M, Kwang, S, Laasanen, At, Lami, S, Lammel, S, Lancaster, M, Lander, Rl, Lannon, K, Lath, A, Latino, G, Lazzizzera, I, Lecompte, T, Lee, E, Lee, H, Lee, Sw, Leone, S, Lewis, Jd, Lin, C, Linacre, J, Lindgren, M, Lipeles, E, Lister, A, Litvintsev, Do, Liu, C, Liu, T, Lockyer, N, Loginov, A, Loreti, M, Lovas, L, Lucchesi, D, Luci, C, Lueck, J, Lujan, P, Lukens, P, Lungu, G, Lyons, L, Lys, J, Lysak, R, Macqueen, D, Madrak, R, Maeshima, K, Makhoul, K, Maki, T, Maksimovic, P, Malde, S, Malik, S, Manca, G, Manousakis Katsikakis, A, Margaroli, F, Marino, C, Marino, Cp, Martin, A, Martin, V, Martinez, M, Martinez Ballarin, R, Maruyama, T, Mastrandrea, P, Masubuchi, T, Mathis, M, Mattson, Me, Mazzanti, P, Mcfarland, K, Mcintyre, P, Mcnulty, R, Mehta, A, Mehtala, P, Menzione, A, Merkel, P, Mesropian, C, Miao, T, Miladinovic, N, Miller, R, Mills, C, Milnik, M, Mitra, A, Mitselmakher, G, Miyake, H, Moggi, N, Moon, C, Moore, R, Morello, MICHAEL JOSEPH, Morlock, J, Fernandez, Pm, Mulmenstadt, J, Mukherjee, A, Muller, T, Mumford, R, Murat, P, Mussini, M, Nachtman, J, Nagai, Y, Nagano, A, Naganoma, J, Nakamura, K, Nakano, I, Napier, A, Necula, V, Nett, J, Neu, C, Neubauer, M, Neubauer, S, Nielsen, J, Nodulman, L, Norman, M, Norniella, O, Nurse, E, Oakes, L, Oh, Sh, Oh, Yd, Oksuzian, I, Okusawa, T, Orava, R, Osterberg, K, Griso, Sp, Palencia, E, Papadimitriou, V, Papaikonomou, A, Paramonov, Aa, Parks, B, Pashapour, S, Patrick, J, Pauletta, G, Paulini, M, Paus, C, Peiffer, T, Pellett, De, Penzo, A, Phillips, Tj, Piacentino, G, Pianori, E, Pinera, L, Pitts, K, Plager, C, Pondrom, L, Poukhov, O, Pounder, N, Prakoshyn, F, Pronko, A, Proudfoot, J, Ptohos, F, Pueschel, E, Punzi, G, Pursley, J, Rademacker, J, Rahaman, A, Ramakrishnan, V, Ranjan, N, Redondo, I, Renton, P, Renz, M, Rescigno, M, Richter, S, Rimondi, F, Ristori, L, Robson, A, Rodrigo, T, Rodriguez, T, Rogers, E, Rolli, S, Roser, R, Rossi, M, Rossin, R, Roy, P, Ruiz, A, Russ, J, Rusu, V, Saarikko, H, Safonov, A, Sakumoto, Wk, Salto, O, Santi, L, Sarkar, S, Sartori, L, Sato, K, Savoy Navarro, A, Schlabach, P, Schmidt, A, Schmidt, Ee, Schmidt, Ma, Schmidt, Mp, Schmitt, M, Schwarz, T, Scodellaro, L, Scribano, A, Scuri, F, Sedov, A, Seidel, S, Seiya, Y, Semenov, A, Sexton Kennedy, L, Sforza, F, Sfyrla, A, Shalhout, Sz, Shears, T, Shepard, Pf, Shimojima, M, Shiraishi, S, Shochet, M, Shon, Y, Shreyber, I, Sidoti, A, Sinervo, P, Sisakyan, A, Slaughter, Aj, Slaunwhite, J, Sliwa, K, Smith, Jr, Snider, Fd, Snihur, R, Soha, A, Somalwar, S, Sorin, V, Spalding, J, Spreitzer, T, Squillacioti, P, Stanitzki, M, St Denis, R, Stelzer, B, Stelzer Chilton, O, Stentz, D, Strologas, J, Strycker, Gl, Stuart, D, Suh, J, Sukhanov, A, Suslov, I, Suzuki, T, Taffard, A, Takashima, R, Takeuchi, Y, Tanaka, R, Tecchio, M, Teng, Pk, Terashi, K, Thom, J, Thompson, A, Thompson, Ga, Thomson, E, Tipton, P, Ttito Guzman, P, Tkaczyk, S, Toback, D, Tokar, S, Tollefson, K, Tomura, T, Tonelli, D, Torre, S, Torretta, D, Totaro, P, Tourneur, S, Trovato, M, Tsai, Sy, Tu, Y, Turini, N, Ukegawa, F, Vallecorsa, S, van Remortel, N, Varganov, A, Vataga, E, Vazquez, F, Velev, G, Vellidis, C, Vidal, M, Vidal, R, Vila, I, Vilar, R, Vine, T, Vogel, M, Volobouev, I, Volpi, G, Wagner, P, Wagner, Rg, Wagner, Rl, Wagner, W, Wagner Kuhr, J, Wakisaka, T, Wallny, R, Wang, Sm, Warburton, A, Waters, D, Weinberger, M, Weinelt, J, Wester, Wc, Whitehouse, B, Whiteson, D, Wicklund, Ab, Wicklund, E, Wilbur, S, Williams, G, Williams, Hh, Wilson, P, Winer, Bl, Wittich, P, Wolbers, S, Wolfe, C, Wright, T, Wu, X, Wurthwein, F, Xie, S, Yagil, A, Yamamoto, K, Yamaoka, J, Yang, Uk, Yang, Yc, Yao, Wm, Yeh, Gp, Yoh, J, Yorita, K, Yoshida, T, Yu, Gb, Yu, I, Yu, S, Yun, Jc, Zanello, L, Zanetti, A, Zhang, X, Zheng, Y, and Zucchelli, S.

Subjects

High Energy Physics::Experiment

Abstract

We present a signature-based search for the anomalous production of events containing a photon, two jets, of which at least one is identified as originating from a b quark, and missing transverse energy ((sic)(T)). The search uses data corresponding to 2.0 fb(-1) of integrated luminosity from p (p) over bar collisions at a center-of-mass energy of root s = 1.96 TeV, collected with the CDF II detector at the Fermilab Tevatron. From 6.697 47 x 10(6) events with a photon candidate with transverse energy E(T) > 25 GeV, we find 617 events with (sic)(T) > 25 GeV and two or more jets with E(T) > 15 GeV, at least one identified as originating from a b quark, versus an expectation of 607 +/- 113 events. Increasing the requirement on (sic)(T) to 50 GeV, we find 28 events versus an expectation of 30 +/- 11 events. We find no indications of non-standard-model phenomena.

Published

2009

8. Swimming Pool Water in Mafraq City in Northern Jordan: Quality Evaluation

Author

Sura Taha Al-Harahsheh

Subjects

swimming pools, water quality, residual chlorine, total organic carbon, trihalomethane, total coliforms, Environmental effects of industries and plants, TD194-195, Science (General), Q1-390

Abstract

The objective of this study is to examine the physical, chemical and biological characteristics of swimming pool water in Mafraq city, north of Jordan and the overall quality of the used water. Three public swimming pools were selected from Mafraq city [Areef Pool (SW1), Teachers Club Pool (SW2) and Anakeel Pool (SW3)] to analyze the physical, chemical and biological properties of their water as well as determine their compliance with the Jordanian Standards for Swimming Pools Water. Sampling was carried out weekly for eight successive weeks between July and August 2019 before bathing (after disinfection) and after bathing and analysed in Al al-Bayt University and Ministry of Environment laboratories. The parameters used to evaluate the quality of water in swimming pools were temperature, pH, electrical conductivity (EC), dissolved oxygen (DO), residual chlorine (Cl2), total organic carbon (TOC), trihalomethanes (THM), major cations and anions, selected heavy metals, and total coliform bacteria, E. coli and Pseudomonas. Most of the physical and chemical parameters analysed were within the recommended limit except for pH and EC. Residual chlorine exceeded the permissible limits in SW3 before and after bathing, recording mean values of pH, EC (4.3 ± 0.25 - 4.33 ± 0.44), (2314 ± 343 - 2453 ± 460), respectively. The dissolved oxygen was less than the recommended limit. Total coliforms, E. coli and Pseudomonas counts were < 1 before and after bathing in all the samples.

Published

2021

9. P2-285 Environmental cadmium exposure and blood pressure in the general population

Author

Sirivarasai, J., primary, Kaojarern, S., additional, Chansirikarnjana, S., additional, Sura, T., additional, Krairit, O., additional, Chunhabundit, R., additional, Chanprasertyothin, S., additional, Chotvitayataragorn, S., additional, and Prasanatikom, W., additional

Published

2011

10. Genome-wide SNP-based linkage analysis of tuberculosis in Thais

Author

Mahasirimongkol, S, primary, Yanai, H, additional, Nishida, N, additional, Ridruechai, C, additional, Matsushita, I, additional, Ohashi, J, additional, Summanapan, S, additional, Yamada, N, additional, Moolphate, S, additional, Chuchotaworn, C, additional, Chaiprasert, A, additional, Manosuthi, W, additional, Kantipong, P, additional, Kanitwittaya, S, additional, Sura, T, additional, Khusmith, S, additional, Tokunaga, K, additional, Sawanpanyalert, P, additional, and Keicho, N, additional

Published

2008

11. A haplotype of the human CXCR1 gene protective against rapid disease progression in HIV-1 + patients

Author

Vasilescu, A., primary, Terashima, Y., additional, Enomoto, M., additional, Heath, S., additional, Poonpiriya, V., additional, Gatanaga, H., additional, Do, H., additional, Diop, G., additional, Hirtzig, T., additional, Auewarakul, P., additional, Lauhakirti, D., additional, Sura, T., additional, Charneau, P., additional, Marullo, S., additional, Therwath, A., additional, Oka, S., additional, Kanegasaki, S., additional, Lathrop, M., additional, Matsushima, K., additional, Zagury, J.-F., additional, and Matsuda, F., additional

Published

2007

12. DETECTION OF SOME BIOFILM GENES RELATED WITH MULTIDRUG-RESISTANT IN ACINOBACTER BAUMANNII ISOLATED FROM CLINICAL ISOLATES

Author

Sura Talib, Thanaa Abdulrahman, and Shatha Ali

Subjects

Medicine

Abstract

Background: Acinetobacter baumannii (A. baumanii) has recently emerged as a major pathogen causing nosocomial infections in patients admitted to intensive care units with a surprisingly rapid acquisition of antibiotic resistance. Objective: To study the rate of occurrence of A. baumanii in different clinical samples and to investigate the association between biofilm formation and presence of ompA and bap genes in multi-drug resistance isolates. Methods: A total of 150 clinical samples were collected from (blood, sputum, urine, wound swab) during a period from the first of October 2017 to the end of March 2018 from Al-Imamein Al-Kadhimein City, Central Teaching Hospital of Pediatrics, Welfare Children Protection in Medical City and Al-Yarmouk Teaching Hospital and tested against 14 antibiotics by disc diffusion method. Quantitative microtiter plate assay was done for detection of biofilm formation. Polymerase chain reaction (PCR) was performed to detect ompA and bap genes. Results: There were 75 A. baumanii isolated from different clinical samples as follows: 41 from blood, 13 from wound, 12 from sputum and 9 from urine. The results of antimicrobial susceptibility test showed, high rate of resistance to Aztronem (94.7%) followed by Cefotaxime (89.3%), Cefepim (86.7%), Meropinem (86.7%), Ceftriaxone (86.7%), Ceftazidime (85%), Gentamicin (85%), and Piperacillin (82.7%) respectively. Moderate - to - low rate of resistance to Ciprofloxacin (78%), Impenim (46.7%), Levofloxacin (46%), Amikacin (44%), Tigacycline (42.3%) and Colistin (44%). The detection of biofilm formation showed that (52%) of isolate produce biofilm and the prevalence of ompA gene was 86.7% while the prevalence of Bap-gene was 34.7%. Conclusion: High frequency of A. baumannii infection was observed in different hospitals in Baghdad. More than half of the isolates were biofilm producer and there is highly significant association between the presence of bap gene and the biofilm formation but not with ompA gene. Keywords: Acinetobacter baumannii, ompA, Bap, MD Citation: Talib SS, Abdulrahman TR, Ali SH. Detection of some biofilm genes related with multidrug-resistant in Acinobacter baumannii isolated from clinical isolates. Iraqi JMS. 2018; 16(4): 430-438. doi: 10.22578/IJMS.16.4.11

Published

2018

13. A genetic association study between growth differentiation factor 5 (GDF 5) polymorphism and knee osteoarthritis in Thai population

Author

Sura Thanyachai, Trachoo Objoon, Pingsuthiwong Sarinee, Changthong Theeraroj, Tawonsawatruk Tulyapruek, and Wajanavisit Wiwat

Subjects

Osteoarthritis, Growth Differentiation Factor 5, GDF5, SNP, RFLP, Thais, Orthopedic surgery, RD701-811, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Objective Osteoarthritis (OA) is a multi-factorial disease and genetic factor is one of the important etiologic risk factors. Various genetic polymorphisms have been elucidated that they might be associated with OA. Recently, several studies have shown an association between Growth Differentiation Factor 5(GDF5) polymorphism and knee OA. However, the role of genetic predisposing factor in each ethnic group cannot be replicated to all, with conflicting data in the literatures. Therefore, the aim of this study was to investigate the association between GDF5 polymorphism and knee OA in Thai population. Materials and Methods One hundred and ninety three patients aged 54-88 years who attended Ramathibodi Hospital were enrolled. Ninety cases with knee OA according to American College of Rheumatology criteria and one hundred and three cases in control group gave informed consent. Blood sample (5 ml) were collected for identification of GDF5 (rs143383) single nucleotide polymorphism by PCR/RFLP according to a standard protocol. This study protocol was approved by the Ethics Committee on human experimentation of Ramathibodi Hospital Faculty of Medicine, Mahidol University. Odds ratios (OR) and 95% confidence intervals were calculated for the risk of knee OA by genotype (TT, TC and CC) and allele (T/C) analyses. Results The baseline characteristics between two groups including job, smoking and activity were not different, except age and BMI. The entire cases and controls were in Hardy-Weinberg equilibrium (p > 0.05). The OA knee group (n = 90) had genotypic figure which has shown by TT 42.2% (n = 38), TC 45.6% (n = 41) and CC 12% (n = 11), whereas the control group (n = 103) revealed TT 32% (n = 33), TC 45.6% (n = 47), and CC 22.3% (n = 23), respectively. Genotypic TT increased risk of knee OA as compared to CC [OR = 2.41 (P = 0.04, 95%CI = 1.02-5.67)]. In the allele analysis, the T allele was found to be significantly associated with knee OA [OR = 1.53 (P = 0.043, 95%CI = 1.01-2.30)]. Conclusion These data suggested that GDF5 polymorphism has an association with knee OA in Thai ethnic. This finding also supports the hypothesis that OA has an important genetic component in its etiology, and GDF5 protein might play important role in the pathophysiology of the disease.

Published

2011

14. Genetic Polymorphism of Zinc Transporter-8 Gene (SLC30A8), Serum Zinc Concentrations, and Proteome Profiles Related to Type 2 Diabetes in Elderly.

Author

Sirivarasai J, Tristitworn P, Shantavasinkul PC, Roytrakul S, Chansirikarnjana S, Ruangritchankul S, Chanprasertyothin S, Charernwat P, Panpunuan P, Sura T, and Sritara P

Abstract

Background and Aims : Older adults are particularly susceptible to type 2 diabetes mellitus (T2DM) due to factors such as age-related insulin resistance, decreased physical activity, and deficiency of micronutrients, especially zinc. Studies have suggested that the risk allele of the zinc transporter 8 gene (SLC30A8) single-nucleotide poly-morphism (SNP) rs13266634 may contribute to T2DM susceptibility in addition to the complex protein interactions and alterations in the protein expressions and modifications associated with T2DM. This study was implemented to study the associations between SLC30A8 polymorphism, serum zinc levels, and the profiles of proteins differentially expressed in nondiabetic ( n = 116) and prediabetic/diabetic ( n = 149) subjects. Methods : SNP genotyping using TaqMan ® assay and proteomic analysis by LC-MS/MS were performed in each group. Results : The results showed a higher risk of diabetes in individuals with the risk genotype CC accompanied by a low serum zinc level than in those with other genotypes. Profiles of proteins differentially expressed between the groups were identified and shown to be particularly associated with zinc-related functions, zinc transporter 8, and glucose metabolism. Proteins exclusively expressed in prediabetes/diabetes were assigned to a Reactome pathway related to zinc transporter and insulin processing. Conclusions : Our findings suggest that individuals carrying at least one copy of SLC30A8 rs13266634 accompanied by a low serum zinc level might be susceptible to T2DM, which could be due to alterations in insulin signaling and zinc metabolism. Understanding this relationship deepens our understanding of the genetic and molecular mechanisms underlying T2DM risk, offering potential targets for therapeutic intervention and prevention strategies.

Published

2025

15. Investigating common mutations in ATP7B gene and the prevalence of Wilson's disease in the Thai population using population-based genome-wide datasets.

Author

Own-Eium P, Dejsuphong D, Vathesatogkit P, Sritara P, Sura T, Aekplakorn W, Suktitipat B, and Eu-Ahsunthornwattana J

Subjects

Female, Humans, Male, Genetic Predisposition to Disease, Genome-Wide Association Study, Genotype, Polymorphism, Single Nucleotide, Prevalence, Southeast Asian People genetics, Thailand epidemiology, Copper-Transporting ATPases genetics, Gene Frequency, Hepatolenticular Degeneration genetics, Hepatolenticular Degeneration epidemiology, Mutation

Abstract

Wilson's disease (WD) is a rare metabolic disorder caused by variations in the ATP7B gene. It usually manifests hepatic, neurologic, and psychiatric symptoms due to excessive copper accumulation. The prevalence of WD and its common variants differ across populations. This study aimed to examine these aspects of WD within the Thai population, where information has been limited. We reviewed ClinVar and the Wilson Disease Mutation Database, organizing variants classified as pathogenic or likely pathogenic in one or both databases as "relaxed" and "strict" lists. Allele frequencies were estimated from genotyping array data (Asian Screening Array: ASA; Illumina Corp, CA) of 6291 Thai subjects, which also underwent genotype imputation. The prevalence of WD in the Thai population was estimated assuming Hardy-Weinberg Equilibrium. The strict list yielded a prevalence of 1/24,128 (carrier frequency=1/78), while the relaxed list yielded a prevalence of 1/9971 (carrier frequency=1/50). The most common WD variants in Thai subjects were c.2333 G > T, c.3443 T > C, and c.813 C > A from the strict list, and c.3316 G > A and c.2605 G > A from the relaxed list. The ASA chip covered approximately 59 and 24% of WD variants from the strict and relaxed lists, respectively. Based on the estimated prevalence, a carrier screening program for WD is not currently required in Thailand. However, as genotyping services become more affordable and accessible, such a program would facilitate early identification, treatment, and prevention of WD., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s), under exclusive licence to The Japan Society of Human Genetics.)

Published

2025

16. Pharmacogenomic landscape of the Thai population from genome sequencing of 949 individuals.

Author

Piriyapongsa J, Chumnumwat S, Kaewprommal P, Triparn K, Suvichapanich S, Udomsinprasert W, Jittikoon J, Shaw PJ, Nakhonsri V, Ngamphiw C, Wangkumhang P, Pithukpakorn M, Roothumnong E, Wiboonthanasarn S, Kuptanon C, Jinawath N, Porntaveetus T, Suriyaphol P, Viprakasit V, Pisitkun P, Kantaputra P, Tim-Aroon T, Wattanasirichaigoon D, Sura T, Suphapeetiporn K, Sripichai O, Khongphatthanayothin A, Fucharoen S, Ngamphaiboon N, Shotelersuk V, Mahasirimongkol S, and Tongsima S

Subjects

Female, Humans, Male, Alleles, Polymorphism, Single Nucleotide, Southeast Asian People, Thailand, Whole Genome Sequencing, Gene Frequency, HLA Antigens genetics, Pharmacogenetics methods

Abstract

Inter-individual variability in drug responses is significantly influenced by genetic factors, underscoring the importance of population-specific pharmacogenomic studies to optimize clinical outcomes. In this study, we analyzed whole genome sequencing data from 949 unrelated Thai individuals and conducted an in-depth analysis of 3239 genes involved in drug pharmacokinetics, pharmacodynamics, or immune-mediated adverse drug reactions. We identified 43 single nucleotide polymorphisms (SNPs), 134 diplotypes, and 15 human leukocyte antigen (HLA) alleles, all with moderate to high clinical significance. On average, each Thai individual carried 14 SNPs, one to two HLA alleles, and six diplotypes with actionable phenotypic associations. Clinically important diplotypes were present in over 20% of individuals for seven genes (CYP2A6, CYP2B6, CYP2C19, CYP3A5, NAT2, SLCO1B1, and VKORC1). In addition, clinically significant SNPs with allele frequencies exceeding 20% were identified among 15 genes, including VKORC1, CYP4F2, and ABCG2. We also identified 21,211 potentially deleterious variants among 3239 genes. Of these variants, 3746 were novel. The comprehensive dataset from this study serves as a valuable resource of pharmacogenomic variants in the Thai population, which will facilitate the development of personalized drug therapies and enhance patient care in Thailand., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

17. MamF-like proteins are distant Tic20 homologs involved in organelle assembly in bacteria.

Author

Paulus A, Ahrens F, Schraut A, Hofmann H, Schiller T, Sura T, Becher D, and Uebe R

Subjects

Organelles metabolism, Protein Transport, Organelle Biogenesis, Bacterial Proteins metabolism, Bacterial Proteins genetics, Phylogeny, Magnetosomes metabolism, Magnetosomes genetics, Magnetosomes ultrastructure, Magnetospirillum metabolism, Magnetospirillum genetics

Abstract

Organelle-specific protein translocation systems are essential for organelle biogenesis and maintenance in eukaryotes but thought to be absent from prokaryotic organelles. Here, we demonstrate that MamF-like proteins are crucial for the formation and functionality of bacterial magnetosome organelles. Deletion of mamF-like genes in the Alphaproteobacterium Magnetospirillum gryphiswaldense results in severe defects in organelle positioning, biomineralization, and magnetic navigation. These phenotypic defects result from the disrupted targeting of a subset of magnetosomal proteins that contain C-terminal glycine-rich integral membrane domains. Phylogenetic analyses reveal an ancient evolutionary link between MamF-like proteins and plastidial Tic20. Our findings redefine the molecular roles of MamF-like proteins and suggest that organelle-specific protein targeting systems also play a role in bacterial organelle formation., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

18. Thai pharmacogenomics database -2 (TPGxD-2) sequel to TPGxD-1, analyzing genetic variants in 26 non-VIPGx genes within the Thai population.

Author

John S, Klumsathian S, Own-Eium P, Charoenyingwattana A, Eu-Ahsunthornwattana J, Sura T, Dejsuphong D, Sritara P, Vathesatogkit P, Thongchompoo N, Thabthimthong W, Teerakulkittipong N, Chantratita W, and Sukasem C

Subjects

Humans, Male, Alleles, Genetic Variation, High-Throughput Nucleotide Sequencing methods, Pharmacogenomic Variants, Southeast Asian People, Thailand, Databases, Genetic, Pharmacogenomic Testing methods

Abstract

Next-generation sequencing (NGS) has transformed pharmacogenomics (PGx), enabling thorough profiling of pharmacogenes using computational methods and advancing personalized medicine. The Thai Pharmacogenomic Database-2 (TPGxD-2) analyzed 948 whole genome sequences, primarily from the Electricity Generating Authority of Thailand (EGAT) cohort. This study is an extension of the previous Thai Pharmacogenomic Database (TPGxD-1) and specifically focused on 26 non-very important pharmacogenes (VIPGx) genes. Variant calling was conducted using Sentieon (version 201808.08) following GATK's best workflow practices. We then annotated variant call format (VCF) files using Golden Helix VarSeq 2.5.0. Star allele analysis was performed with Stargazer v2.0.2, which called star alleles for 22 of 26 non-VIPGx genes. The variant analysis revealed a total of 14,529 variants in 26 non-VIPGx genes, with TBXAS1 had the highest number of variants (27%). Among the 14,529 variants, 2328 were novel (without rsID), with 87 identified as clinically relevant. We also found 56 known PGx variants among the known variants (n = 12,201), with UGT2B7 (19.64%), CYP1B1 (8.9%), SLCO2B1 (8.9%), and POR (8.9%) being the most common. We reported a high frequency of intermediate metabolizers (IMs) in CYP2F1 (34.6%) and CYP4A11 (8.6%), and a high frequency of decreased functional alleles in POR (53.9%) and SLCO1B3 (34.9%) genes. This study enhances our understanding of pharmacogenomic profiling of 26 non-VIPGx genes of notable clinical importance in the Thai population. However, further validation with additional computational and reference genotyping methods is necessary, and novel alleles identified in this study should undergo further orthogonal validation., (© 2024 The Author(s). Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2024

19. A comprehensive Thai pharmacogenomics database (TPGxD-1): Phenotype prediction and variants identification in 942 whole-genome sequencing data.

Author

John S, Klumsathian S, Own-Eium P, Eu-Ahsunthornwattana J, Sura T, Dejsuphong D, Sritara P, Vathesatogkit P, Thongchompoo N, Thabthimthong W, Teerakulkittipong N, Chantratita W, and Sukasem C

Subjects

Humans, Thailand, Databases, Genetic, Pharmacogenomic Variants, Male, Female, Alleles, Southeast Asian People, Whole Genome Sequencing methods, Phenotype, Pharmacogenetics methods

Abstract

Computational methods analyze genomic data to identify genetic variants linked to drug responses, thereby guiding personalized medicine. This study analyzed 942 whole-genome sequences from the Electricity Generating Authority of Thailand (EGAT) cohort to establish a population-specific pharmacogenomic database (TPGxD-1) in the Thai population. Sentieon (version 201808.08) implemented the GATK best workflow practice for variant calling. We then annotated variant call format (VCF) files using Golden Helix VarSeq 2.5.0 and employed Stargazer v2.0.2 for star allele analysis. The analysis of 63 very important pharmacogenes (VIPGx) reveals 85,566 variants, including 13,532 novel discoveries. Notably, we identified 464 known PGx variants and 275 clinically relevant novel variants. The phenotypic prediction of 15 VIPGx demonstrated a varied metabolic profile for the Thai population. Genes like CYP2C9 (9%), CYP3A5 (45.2%), CYP2B6 (9.4%), NUDT15 (15%), CYP2D6 (47%) and CYP2C19 (43%) showed a high number of intermediate metabolizers; CYP3A5 (41%), and CYP2C19 (9.9%) showed more poor metabolizers. CYP1A2 (52.7%) and CYP2B6 (7.6%) were found to have a higher number of ultra-metabolizers. The functional prediction of the remaining 10 VIPGx genes reveals a high frequency of decreased functional alleles in SULT1A1 (12%), NAT2 (84%), and G6PD (12%). SLCO1B1 reports 20% poor functional alleles, while PTGIS (42%), SLCO1B1 (4%), and TPMT (5.96%) showed increased functional alleles. This study discovered new variants and alleles in the 63 VIPGx genes among the Thai population, offering insights into advancing clinical pharmacogenomics (PGx). However, further validation is needed using other computational and genotyping methods., (© 2024 The Author(s). Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2024

20. Alpha-glucans from bacterial necromass indicate an intra-population loop within the marine carbon cycle.

Author

Beidler I, Steinke N, Schulze T, Sidhu C, Bartosik D, Zühlke MK, Martin LT, Krull J, Dutschei T, Ferrero-Bordera B, Rielicke J, Kale V, Sura T, Trautwein-Schult A, Kirstein IV, Wiltshire KH, Teeling H, Becher D, Bengtsson MM, Hehemann JH, Bornscheuer UT, Amann RI, and Schweder T

Subjects

Phytoplankton metabolism, Biomass, Diatoms metabolism, Eutrophication, Carbon metabolism, Zooplankton metabolism, Polysaccharides, Bacterial metabolism, Polysaccharides, Bacterial chemistry, Bacterial Proteins metabolism, Carbon Cycle, Glucans metabolism, Bacteria metabolism, Bacteria classification, Bacteria genetics

Abstract

Phytoplankton blooms provoke bacterioplankton blooms, from which bacterial biomass (necromass) is released via increased zooplankton grazing and viral lysis. While bacterial consumption of algal biomass during blooms is well-studied, little is known about the concurrent recycling of these substantial amounts of bacterial necromass. We demonstrate that bacterial biomass, such as bacterial alpha-glucan storage polysaccharides, generated from the consumption of algal organic matter, is reused and thus itself a major bacterial carbon source in vitro and during a diatom-dominated bloom. We highlight conserved enzymes and binding proteins of dominant bloom-responder clades that are presumably involved in the recycling of bacterial alpha-glucan by members of the bacterial community. We furthermore demonstrate that the corresponding protein machineries can be specifically induced by extracted alpha-glucan-rich bacterial polysaccharide extracts. This recycling of bacterial necromass likely constitutes a large-scale intra-population energy conservation mechanism that keeps substantial amounts of carbon in a dedicated part of the microbial loop., (© 2024. The Author(s).)

Published

2024

21. Pressure injury treatment by intermittent electrical stimulation (PROTECT-2): protocol for a multicenter randomized clinical trial.

Author

Donaldson C, de Abreu MG, Mascha EJ, Rowbottom J, Harvester E, Khanna A, Sura T, Sessler DI, Patarroyo FR, Gulluoglu A, Zajic P, Chauhan U, Essber H, and Kurz A

Subjects

Humans, Treatment Outcome, Time Factors, Wound Healing, Pressure Ulcer therapy, Electric Stimulation Therapy methods, Multicenter Studies as Topic, Randomized Controlled Trials as Topic

Abstract

Background: Pressure ulcers account for a substantial fraction of hospital-acquired pathology, with consequent morbidity and economic cost. Treatments are largely focused on preventing further injury, whereas interventions that facilitate healing remain limited. Intermittent electrical stimulation (IES) increases local blood flow and redistributes pressure from muscle-bone interfaces, thus potentially reducing ulcer progression and facilitating healing., Methods: The Pressure Injury Treatment by Intermittent Electrical Stimulation (PROTECT-2) trial will be a parallel-arm multicenter randomized trial to test the hypothesis that IES combined with routine care reduces sacral and ischial pressure injury over time compared to routine care alone. We plan to enroll 548 patients across various centers. Hospitalized patients with stage 1 or stage 2 sacral or ischial pressure injuries will be randomized to IES and routine care or routine care alone. Wound stage will be followed until death, discharge, or the development of an exclusion criteria for up to 3 months. The primary endpoint will be pressure injury score measured over time., Discussion: Sacral and ischial pressure injuries present a burden to hospitalized patients with both clinical and economic consequences. The PROTECT-2 trial will evaluate whether IES is an effective intervention and thus reduces progression of stage 1 and stage 2 sacral and ischial pressure injuries., Trial Registration: ClinicalTrials.gov NCT05085288 Registered October 20, 2021., (© 2024. The Author(s).)

Published

2024

22. Global Protein Profiling in Processed Immunohistochemistry Tissue Sections.

Author

Venz S, von Bohlen Und Halbach V, Hentschker C, Junker H, Kuss AW, Sura T, Krüger E, Völker U, von Bohlen Und Halbach O, Jensen LR, and Hammer E

Subjects

Mice, Animals, Immunohistochemistry, Mice, Inbred C57BL, Proteins analysis, Tandem Mass Spectrometry, Paraffin Embedding, Tissue Fixation methods, Proteomics methods, Formaldehyde chemistry

Abstract

Tissue sections, which are widely used in research and diagnostic laboratories and have already been examined by immunohistochemistry (IHC), may subsequently provide a resource for proteomic studies, even though only small amount of protein is available. Therefore, we established a workflow for tandem mass spectrometry-based protein profiling of IHC specimens and characterized defined brain area sections. We investigated the CA1 region of the hippocampus dissected from brain slices of adult C57BL/6J mice. The workflow contains detailed information on sample preparation from brain slices, including removal of antibodies and cover matrices, dissection of region(s) of interest, protein extraction and digestion, mass spectrometry measurement, and data analysis. The Gene Ontology (GO) knowledge base was used for further annotation. Literature searches and Gene Ontology annotation of the detected proteins verify the applicability of this method for global protein profiling using formalin-fixed and embedded material and previously used IHC slides.

Published

2023

23. Neutrophil-derived reactive agents induce a transient SpeB negative phenotype in Streptococcus pyogenes.

Author

Shumba P, Sura T, Moll K, Chakrakodi B, Tölken LA, Hoßmann J, Hoff KJ, Hyldegaard O, Nekludov M, Svensson M, Arnell P, Skrede S, Norrby-Teglund A, and Siemens N

Subjects

Bacterial Proteins, Exotoxins genetics, Streptococcus pyogenes genetics, Neutrophils

Abstract

Background: Streptococcus pyogenes (group A streptococci; GAS) is the main causative pathogen of monomicrobial necrotizing soft tissue infections (NSTIs). To resist immuno-clearance, GAS adapt their genetic information and/or phenotype to the surrounding environment. Hyper-virulent streptococcal pyrogenic exotoxin B (SpeB) negative variants caused by covRS mutations are enriched during infection. A key driving force for this process is the bacterial Sda1 DNase., Methods: Bacterial infiltration, immune cell influx, tissue necrosis and inflammation in patient´s biopsies were determined using immunohistochemistry. SpeB secretion and activity by GAS post infections or challenges with reactive agents were determined via Western blot or casein agar and proteolytic activity assays, respectively. Proteome of GAS single colonies and neutrophil secretome were profiled, using mass spectrometry., Results: Here, we identify another strategy resulting in SpeB-negative variants, namely reversible abrogation of SpeB secretion triggered by neutrophil effector molecules. Analysis of NSTI patient tissue biopsies revealed that tissue inflammation, neutrophil influx, and degranulation positively correlate with increasing frequency of SpeB-negative GAS clones. Using single colony proteomics, we show that GAS isolated directly from tissue express but do not secrete SpeB. Once the tissue pressure is lifted, GAS regain SpeB secreting function. Neutrophils were identified as the main immune cells responsible for the observed phenotype. Subsequent analyses identified hydrogen peroxide and hypochlorous acid as reactive agents driving this phenotypic GAS adaptation to the tissue environment. SpeB-negative GAS show improved survival within neutrophils and induce increased degranulation., Conclusions: Our findings provide new information about GAS fitness and heterogeneity in the soft tissue milieu and provide new potential targets for therapeutic intervention in NSTIs., (© 2023. The Author(s).)

Published

2023

24. Effect of heat inactivation and bulk lysis on real-time reverse transcription PCR detection of the SARS-COV-2: an experimental study.

Author

Leta D, Gutema G, Hagos GG, Diriba R, Bulti G, Sura T, Ayana D, Chala D, Lenjiso B, Bulti J, Abdella S, and Tola HH

Subjects

COVID-19 Testing, Hot Temperature, Humans, Real-Time Polymerase Chain Reaction, SARS-CoV-2 genetics, COVID-19 diagnosis, Reverse Transcription

Abstract

Objective: This study aimed to investigate the effect of heat inactivation and chemical bulklysis on SARS-CoV-2 detection., Results: About 6.2% (5/80) of samples were changed to negative results in heat inactivation at 60 °C and about 8.7% (7/80) of samples were changed to negative in heat inactivation at 100 °C. The Ct values of heat-inactivated samples (at 60 °C, at 100 °C, and bulk lysis) were significantly different from the temperature at 56 °C. The effect of heat on Ct value should be considered when interpreting diagnostic PCR results from clinical samples which could have an initial low virus concentration. The efficacy of heat-inactivation varies greatly depending on temperature and duration. Local validation of heat-inactivation and its effects is therefore essential for molecular testing., (© 2022. The Author(s).)

Published

2022

25. Streptococcus pneumoniae and Influenza A Virus Co-Infection Induces Altered Polyubiquitination in A549 Cells.

Author

Sura T, Gering V, Cammann C, Hammerschmidt S, Maaß S, Seifert U, and Becher D

Subjects

A549 Cells, Humans, Streptococcus pneumoniae, Ubiquitination, Coinfection microbiology, Influenza A Virus, H1N1 Subtype physiology, Influenza A virus, Influenza, Human

Abstract

Epithelial cells are an important line of defense within the lung. Disruption of the epithelial barrier by pathogens enables the systemic dissemination of bacteria or viruses within the host leading to severe diseases with fatal outcomes. Thus, the lung epithelium can be damaged by seasonal and pandemic influenza A viruses. Influenza A virus infection induced dysregulation of the immune system is beneficial for the dissemination of bacteria to the lower respiratory tract, causing bacterial and viral co-infection. Host cells regulate protein homeostasis and the response to different perturbances, for instance provoked by infections, by post translational modification of proteins. Aside from protein phosphorylation, ubiquitination of proteins is an essential regulatory tool in virtually every cellular process such as protein homeostasis, host immune response, cell morphology, and in clearing of cytosolic pathogens. Here, we analyzed the proteome and ubiquitinome of A549 alveolar lung epithelial cells in response to infection by either Streptococcus pneumoniae D39Δ cps or influenza A virus H1N1 as well as bacterial and viral co-infection. Pneumococcal infection induced alterations in the ubiquitination of proteins involved in the organization of the actin cytoskeleton and Rho GTPases, but had minor effects on the abundance of host proteins. H1N1 infection results in an anti-viral state of A549 cells. Finally, co-infection resembled the imprints of both infecting pathogens with a minor increase in the observed alterations in protein and ubiquitination abundance., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Sura, Gering, Cammann, Hammerschmidt, Maaß, Seifert and Becher.)

Published

2022

26. Cost-minimization analysis of sequential genetic testing versus targeted next-generation sequencing gene panels in patients with pheochromocytoma and paraganglioma.

Author

Pipitprapat W, Pattanaprateep O, Iemwimangsa N, Sensorn I, Panthan B, Jiaranai P, Chantratita W, Sorapipatcharoen K, Poomthavorn P, Mahachoklertwattana P, Sura T, Tunteeratum A, Srichan K, and Sriphrapradang C

Subjects

Adrenal Gland Neoplasms diagnosis, Adrenal Gland Neoplasms genetics, Costs and Cost Analysis, Genetic Predisposition to Disease, Germ-Line Mutation, Humans, Paraganglioma diagnosis, Pheochromocytoma diagnosis, Genetic Testing economics, High-Throughput Nucleotide Sequencing economics, Paraganglioma genetics, Pheochromocytoma genetics

Abstract

Introduction: Pheochromocytomas and paragangliomas (PPGLs) are highly heritable tumours, with up to 40% of cases carrying germline variants. Current guidelines recommend genetic testing for all patients with PPGLs. Next-generation sequencing (NGS) enables accurate, fast, and inexpensive genetic testing. This study aimed to compare the costs related to PPGL genetic testing between the sequential testing using the decisional algorithm proposed in the 2014 Endocrine Society guidelines and targeted NGS gene panels., Methods: Patients with proven PPGLs were enrolled. A gene list covering 17 susceptibility genes related to hereditary PPGLs was developed for targeted sequencing. Validation was carried out by Sanger sequencing. We simulated the diagnostic workflow to examine the anticipated costs based on each strategy for genetic testing., Results: Twenty-nine patients were included, among whom a germline variant was identified in 34.5%. A total of 22.7% with apparently sporadic PPGL carried a variant. Five genes were involved ( RET , n  = 3; SDHB , n  = 3; SDHD , n  = 2; EGLN1 , n  = 1; and NF1 , n  = 1). According to the diagnostic workflow, the average cost of the targeted NGS (534.7 US dollars per patient) is lower than that of the sequential testing (734.5 US dollars per patient). The targeted NGS can also reduce the number of hospital visits from 4.1 to 1 per person. The cost can be further reduced to 496.24 US dollars per person (32% reduction) if we apply a new syndromic-driven diagnostic algorithm to establish priorities for specific genetic testing for syndromic and selected cases, and targeted NGS for non-syndromic patients., Conclusions: Targeted NGS can reduce both the cost of PPGL genetic testing and the number of hospital visits, compared with the conventional approach. Our proposed algorithm is the preferred approach due to its significant reduction of the cost of genetic testing.Key messagePheochromocytomas and paragangliomas are highly heritable neoplasms.The targeted next-generation sequencing (NGS) gene panels have proven to be fast, accurate, and inexpensive for the genetic analysis.According to this cost analysis, it is economically reasonable to use targeted NGS gene panels for genetic screening.

Published

2021

27. Surviving Serum: the Escherichia coli iss Gene of Extraintestinal Pathogenic E. coli Is Required for the Synthesis of Group 4 Capsule.

Author

Biran D, Sura T, Otto A, Yair Y, Becher D, and Ron EZ

Subjects

Anti-Bacterial Agents pharmacology, Drug Resistance, Bacterial genetics, Escherichia coli Infections drug therapy, Extraintestinal Pathogenic Escherichia coli drug effects, Humans, Sepsis drug therapy, Sepsis microbiology, Escherichia coli Infections microbiology, Escherichia coli Proteins genetics, Extraintestinal Pathogenic Escherichia coli genetics, Serum microbiology

Abstract

Extraintestinal pathogenic Escherichia coli (ExPEC) strains constitute a serious and emerging clinical problem, as they cause a variety of infections and are usually highly antibiotic resistant. Many ExPEC strains are capable of evading the bactericidal effects of serum and causing sepsis. One critical factor for the development of septicemia is the increased serum survival ( iss ) gene, which is highly correlated with complement resistance and lethality. Although it is very important, the function of the iss gene has not been elucidated so far. We have been studying the serum survival of a septicemic strain of E. coli serotype O78, which has a group 4 capsule. Here, we show that the iss gene is required for the synthesis of capsules, which protect the bacteria from the bactericidal effect of complement. Moreover, we show that the deletion of the iss gene results in significantly increased binding of the complement proteins that constitute the membrane attack complex to the bacterial surface.

Published

2021

28. An Innovative Protocol for Metaproteomic Analyses of Microbial Pathogens in Cystic Fibrosis Sputum.

Author

Graf AC, Striesow J, Pané-Farré J, Sura T, Wurster M, Lalk M, Pieper DH, Becher D, Kahl BC, and Riedel K

Subjects

Bacteria genetics, Humans, Lung, Sputum, Cystic Fibrosis complications, Microbiota

Abstract

Hallmarks of cystic fibrosis (CF) are increased viscosity of mucus and impaired mucociliary clearance within the airways due to mutations of the cystic fibrosis conductance regulator gene. This facilitates the colonization of the lung by microbial pathogens and the concomitant establishment of chronic infections leading to tissue damage, reduced lung function, and decreased life expectancy. Although the interplay between key CF pathogens plays a major role during disease progression, the pathophysiology of the microbial community in CF lungs remains poorly understood. Particular challenges in the analysis of the microbial population present in CF sputum is (I) the inhomogeneous, viscous, and slimy consistence of CF sputum, and (II) the high number of human proteins masking comparably low abundant microbial proteins. To address these challenges, we used 21 CF sputum samples to develop a reliable, reproducible and widely applicable protocol for sputum processing, microbial enrichment, cell disruption, protein extraction and subsequent metaproteomic analyses. As a proof of concept, we selected three sputum samples for detailed metaproteome analyses and complemented and validated metaproteome data by 16S sequencing, metabolomic as well as microscopic analyses. Applying our protocol, the number of bacterial proteins/protein groups increased from 199-425 to 392-868 in enriched samples compared to nonenriched controls. These early microbial metaproteome data suggest that the arginine deiminase pathway and multiple proteases and peptidases identified from various bacterial genera could so far be underappreciated in their contribution to the CF pathophysiology. By providing a standardized and effective protocol for sputum processing and microbial enrichment, our study represents an important basis for future studies investigating the physiology of microbial pathogens in CF in vivo - an important prerequisite for the development of novel antimicrobial therapies to combat chronic recurrent airway infection in CF., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Graf, Striesow, Pané-Farré, Sura, Wurster, Lalk, Pieper, Becher, Kahl and Riedel.)

Published

2021

29. Changing expression patterns of TonB-dependent transporters suggest shifts in polysaccharide consumption over the course of a spring phytoplankton bloom.

Author

Francis TB, Bartosik D, Sura T, Sichert A, Hehemann JH, Markert S, Schweder T, Fuchs BM, Teeling H, Amann RI, and Becher D

Subjects

Eutrophication, North Sea, Polysaccharides, Bacterial, Phytoplankton genetics, Seawater

Abstract

Algal blooms produce large quantities of organic matter that is subsequently remineralised by bacterial heterotrophs. Polysaccharide is a primary component of algal biomass. It has been hypothesised that individual bacterial heterotrophic niches during algal blooms are in part determined by the available polysaccharide substrates present. Measurement of the expression of TonB-dependent transporters, often specific for polysaccharide uptake, might serve as a proxy for assessing bacterial polysaccharide consumption over time. To investigate this, we present here high-resolution metaproteomic and metagenomic datasets from bacterioplankton of the 2016 spring phytoplankton bloom at Helgoland island in the southern North Sea, and expression profiles of TonB-dependent transporters during the bloom, which demonstrate the importance of both the Gammaproteobacteria and the Bacteroidetes as degraders of algal polysaccharide. TonB-dependent transporters were the most highly expressed protein class, split approximately evenly between the Gammaproteobacteria and Bacteroidetes, and totalling on average 16.7% of all detected proteins during the bloom. About 93% of these were predicted to take up organic matter, and for about 12% of the TonB-dependent transporters, we predicted a specific target polysaccharide class. Most significantly, we observed a change in substrate specificities of the expressed transporters over time, which was not reflected in the corresponding metagenomic data. From this, we conclude that algal cell wall-related compounds containing fucose, mannose, and xylose were mostly utilised in later bloom stages, whereas glucose-based algal and bacterial storage molecules including laminarin, glycogen, and starch were used throughout. Quantification of transporters could therefore be key for understanding marine carbon cycling., (© 2021. The Author(s).)

Published

2021

30. Kidney Autotransplantation for Treatment of Ureteric Obstruction: A Case Report and Brief Review of the Literature.

Author

Joshi P, Lin J, Sura T, Limbu PS, Melkonian V, Bastani B, and Varma C

Abstract

Autologous kidney transplantation is a relatively rare procedure that has been used as an alternative treatment for a variety of complex genitourinary problems, in particular for the treatment of complex proximal ureteral strictures. In this case report, a 47-year-old male, who had undergone a living donor nephrectomy 14 years earlier, presented with episodes of acute kidney injury on chronic kidney disease. He was found to have a complex proximal ureter stricture of his solitary right kidney. He underwent nephrectomy with subsequent autotransplantation of the kidney into the right iliac fossa. His renal function improved significantly after surgery. Renal autotransplantation may be considered for the management of proximal ureteral obstruction when alternative options are contraindicated., Competing Interests: No conflict of interest., (Copyright © 2021 Parth Joshi et al.)

Published

2021

31. Proteomic Adaptation of Clostridioides difficile to Treatment with the Antimicrobial Peptide Nisin.

Author

Maaß S, Bartel J, Mücke PA, Schlüter R, Sura T, Zaschke-Kriesche J, Smits SHJ, and Becher D

Subjects

Bacterial Proteins metabolism, Clostridioides metabolism, Clostridioides difficile metabolism, Nisin genetics, Nisin metabolism, Pore Forming Cytotoxic Proteins genetics, Proteomics methods, Adaptation, Physiological drug effects, Anti-Bacterial Agents pharmacology, Gene Expression Regulation, Bacterial drug effects, Nisin pharmacology, Pore Forming Cytotoxic Proteins metabolism

Abstract

Clostridioides difficile is the leading cause of antibiotic-associated diarrhea but can also result in more serious, life-threatening conditions. The incidence of C. difficile infections in hospitals is increasing, both in frequency and severity, and antibiotic-resistant C. difficile strains are advancing. Against this background antimicrobial peptides (AMPs) are an interesting alternative to classic antibiotics. Information on the effects of AMPs on C. difficile will not only enhance the knowledge for possible biomedical application but may also provide insights into mechanisms of C. difficile to adapt or counteract AMPs. This study applies state-of-the-art mass spectrometry methods to quantitatively investigate the proteomic response of C. difficile 630∆ erm to sublethal concentrations of the AMP nisin allowing to follow the cellular stress adaptation in a time-resolved manner. The results do not only point at a heavy reorganization of the cellular envelope but also resulted in pronounced changes in central cellular processes such as carbohydrate metabolism. Further, the number of flagella per cell was increased during the adaptation process. The potential involvement of flagella in nisin adaptation was supported by a more resistant phenotype exhibited by a non-motile but hyper-flagellated mutant.

Published

2021

32. Treatment of Hepatitis C Post-Liver Transplantation Could Mitigate Discard Rates of Hepatitis C-Positive Deceased Donor Livers and Expand the Donor Pool.

Author

Keller J, Marklin G, Okoye O, Desai R, Sura T, Jain A, Varma C, and Nazzal M

Abstract

Background: Prior to 2014, treatment for hepatitis C was limited. However, the subsequent introduction of direct acting antiviral medications (DAA) against hepatitis C led to improvements in morbidity and better medication tolerance. DAA therapy allowed for an increase in treatment rates of hepatitis C in patients on the liver transplant waiting list. With the popularization of DAA, there became a growing concern about the utility of hepatitis C-positive (HCV+) deceased liver donors, especially after treating HCV+ potential recipients on the transplant waiting list., Methods: This is a retrospective, observational study using Mid-America Transplant Services (MTS) database from 2008 to 2017. Comparison was made before the widespread use of DAAs 2008-2013 (pre-DAA) against their common practice use 2014-2017 (post-DAA). All deceased liver donors with HCV antibody or nucleic acid positive results were evaluated., Results: Between 2008 and 2017, 96 deceased liver donors were positive for HCV. In the pre-DAA era, 47 deceased liver donors were positive for HCV, of which 32 (68.1%) were transplanted and 15 (31.9%) were discarded. In the post-DAA era, a total of 49 HCV+ organs were identified, out of which 43 (87.8%) livers were transplanted and 6 (12.2%) were discarded. Discard rate was significantly higher in the pre-DAA population (31.9% vs. 12.2%, p  = 0.026). Secondary analysis showed a distinct trend towards increased regional sharing and utilization of HCV+ donors., Conclusion: In order to reduce discard rates of HCV+ patients, our data suggest that transplant centers could potentially delay HCV treatment in patients on the transplant waitlist., Competing Interests: The authors declare that they have no conflicts of interest., (Copyright © 2021 Jennifer Keller et al.)

Published

2021

33. TRIM29 is required for efficient recruitment of 53BP1 in response to DNA double-strand breaks in vertebrate cells.

Author

Wikiniyadhanee R, Lerksuthirat T, Stitchantrakul W, Chitphuk S, Sura T, and Dejsuphong D

Subjects

Animals, Cell Line, DNA genetics, DNA Breaks, Double-Stranded, DNA End-Joining Repair genetics, DNA End-Joining Repair physiology, DNA Repair physiology, DNA-Binding Proteins physiology, Humans, Transcription Factors physiology, Tumor Suppressor p53-Binding Protein 1 metabolism, Tumor Suppressor p53-Binding Protein 1 physiology, Vertebrates genetics, DNA Repair genetics, DNA-Binding Proteins metabolism, Transcription Factors metabolism, Tumor Suppressor p53-Binding Protein 1 genetics

Abstract

Tripartite motif-containing protein 29 (TRIM29) is involved in DNA double-strand break (DSB) repair. However, the specific roles of TRIM29 in DNA repair are not clearly understood. To investigate the involvement of TRIM29 in DNA DSB repair, we disrupted TRIM29 in DT40 cells by gene targeting with homologous recombination (HR). The roles of TRIM29 were investigated by clonogenic survival assays and immunofluorescence analyses. TRIM29 triallelic knockout (TRIM29 -/-/-/+ ) cells were sensitive to etoposide, but resistant to camptothecin. Foci formation assays to assess DNA repair activities showed that the dissociation of etoposide-induced phosphorylated H2A histone family member X (ɣ-H2AX) foci was retained in TRIM29 -/-/-/+ cells, and the formation of etoposide-induced tumor suppressor p53-binding protein 1 (53BP1) foci in TRIM29 -/-/-/+ cells was slower compared with wild-type (WT) cells. Interestingly, the kinetics of camptothecin-induced RAD51 foci formation of TRIM29 -/-/-/+ cells was higher than that of WT cells. These results indicate that TRIM29 is required for efficient recruitment of 53BP1 to facilitate the nonhomologous end-joining (NHEJ) pathway and thereby suppress the HR pathway in response to DNA DSBs. TRIM29 regulates the choice of DNA DSB repair pathway by facilitating 53BP1 accumulation to promote NHEJ and may have potential for development into a therapeutic target to sensitize refractory cancers or as biomarker of personalized therapies., (© 2020 The Authors. Published by FEBS Press and John Wiley & Sons Ltd.)

Published

2020

34. Membrane Modulation of Super-Secreting "midi Bacillus " Expressing the Major Staphylococcus aureus Antigen - A Mass-Spectrometry-Based Absolute Quantification Approach.

Author

Antelo-Varela M, Aguilar Suárez R, Bartel J, Bernal-Cabas M, Stobernack T, Sura T, van Dijl JM, Maaß S, and Becher D

Abstract

Bacillus subtilis has been extensively used as a microbial cell factory for industrial enzymes due to its excellent capacities for protein secretion and large-scale fermentation. This bacterium is also an attractive host for biopharmaceutical production. However, the secretion potential of this organism is not fully utilized yet, mostly due to a limited understanding of critical rearrangements in the membrane proteome upon high-level protein secretion. Recently, it was shown that bottlenecks in heterologous protein secretion can be resolved by genome minimization. Here, we present for the first time absolute membrane protein concentrations of a genome-reduced B. subtilis strain ("midi Bacillus ") expressing the immunodominant Staphylococcus aureus antigen A (IsaA). We quantitatively characterize the membrane proteome adaptation of midi Bacillus during production stress on the level of molecules per cell for more than 400 membrane proteins, including determination of protein concentrations for ∼61% of the predicted transporters. We demonstrate that ∼30% of proteins with unknown functions display a significant increase in abundance, confirming the crucial role of membrane proteins in vital biological processes. In addition, our results show an increase of proteins dedicated to translational processes in response to IsaA induction. For the first time reported, we provide accumulation rates of a heterologous protein, demonstrating that midi Bacillus secretes 2.41 molecules of IsaA per minute. Despite the successful secretion of this protein, it was found that there is still some IsaA accumulation occurring in the cytosol and membrane fraction, leading to a severe secretion stress response, and a clear adjustment of the cell's array of transporters. This quantitative dataset offers unprecedented insights into bioproduction stress responses in a synthetic microbial cell., (Copyright © 2020 Antelo-Varela, Aguilar Suárez, Bartel, Bernal-Cabas, Stobernack, Sura, van Dijl, Maaß and Becher.)

Published

2020

35. Factors associated with dependence on smokeless tobacco, Navi Mumbai, India.

Author

Salvi A, Sura T, Karaye I, and Horney JA

Abstract

Objective: Nearly 300 million people in India use some type of tobacco product, with about 60% of those using smokeless tobacco. Smokeless tobacco use has been associated with a number adverse health outcomes in India and across South Asia., Method: A cross-sectional study of outpatients at a dental hospital in Navi Mumbai, India was conducted between January and June 2015. Trained interviewers administered a 19-item questionnaire to all patients receiving regular dental care. In addition to demographic information, data about the use of smokeless tobacco was collected. Nicotine dependence was assessed using the six-item Fagerstrom Nicotine Dependence Scale, adapted for smokeless tobacco., Results: Approximately one third of 1,067 respondents (30.55%; N = 326) reported use of smokeless tobacco. Neither use of smokeless tobacco nor nicotine dependence was associated with any demographic variables. High nicotine dependence was associated with a younger age of initiation of smokeless tobacco use (RD = 0.14; 95% CI: 0.03, 0.25) and with frequency of use, with those who reported daily use having an excess risk of high nicotine dependence of 14% (95% CI: 2%, 27%)., Conclusion: To reduce dependence on smokeless tobacco in India and subsequent adverse health outcomes, interventions should emphasize a combination of policy and public health interventions focused on increasing the age at which a person initially uses smokeless tobacco and decreasing the frequency of use.

Published

2019

36. Comparative proteome analysis in an Escherichia coli CyDisCo strain identifies stress responses related to protein production, oxidative stress and accumulation of misfolded protein.

Author

Guerrero Montero I, Dolata KM, Schlüter R, Malherbe G, Sievers S, Zühlke D, Sura T, Dave E, Riedel K, and Robinson C

Subjects

Escherichia coli metabolism, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism, Membrane Transport Proteins, Protein Sorting Signals, Protein Transport, Proteomics, Recombinant Fusion Proteins chemistry, Single-Chain Antibodies chemistry, Escherichia coli genetics, Oxidative Stress, Protein Folding, Proteome

Abstract

Background: The Twin-arginine translocation (Tat) pathway of Escherichia coli has great potential for the export of biopharmaceuticals to the periplasm due to its ability to transport folded proteins, and its proofreading mechanism that allows correctly folded proteins to translocate. Coupling the Tat-dependent protein secretion with the formation of disulfide bonds in the cytoplasm of E. coli CyDisCo provides a powerful platform for the production of industrially challenging proteins. In this study, we investigated the effects on the E. coli cells of exporting a folded substrate (scFv) to the periplasm using a Tat signal peptide, and the effects of expressing an export-incompetent misfolded variant., Results: Cell growth is decreased when either the correctly folded or misfolded scFv is expressed with a Tat signal peptide. However, only the production of misfolded scFv leads to cell aggregation and formation of inclusion bodies. The comprehensive proteomic analysis revealed that both conditions, recombinant protein overexpression and misfolded protein accumulation, lead to downregulation of membrane transporters responsible for protein folding and insertion into the membrane while upregulating the production of chaperones and proteases involved in removing aggregates. These conditions also differentially affect the production of transcription factors and proteins involved in DNA replication. The most distinct stress response observed was the cell aggregation caused by elevated levels of antigen 43. Finally, Tat-dependent secretion causes an increase in tatA expression only after induction of protein expression, while the subsequent post-induction analysis revealed lower tatA and tatB expression levels, which correlate with lowered TatA and TatB protein abundance., Conclusions: The study identified characteristic changes occurring as a result of the production of both a folded and a misfolded protein, but also highlights an exclusive unfolded stress response. Countering and compensating for these changes may result in higher yields of pharmaceutically relevant proteins exported to the periplasm.

Published

2019

37. Far-reaching cellular consequences of tat deletion in Escherichia coli revealed by comprehensive proteome analyses.

Author

Dolata KM, Montero IG, Miller W, Sievers S, Sura T, Wolff C, Schlüter R, Riedel K, and Robinson C

Subjects

Cell Membrane metabolism, Gene Deletion, Gene Expression Profiling, Periplasm metabolism, Protein Transport physiology, Proteome metabolism, Escherichia coli genetics, Escherichia coli metabolism, Protein Transport genetics, Stress, Physiological physiology, Twin-Arginine-Translocation System genetics

Abstract

In Escherichia coli, the Twin-arginine translocation (Tat) pathway secretes a set of folded proteins with important physiological functions to the periplasm and outer membrane. The loss of Tat secretion impairs outer membrane integrity and leads to decreased cell growth. Only recently, the Tat pathway has gained more attention due to its essential role in bacterial virulence and applications in the production of fully folded heterologous proteins. In this study, we investigated the influence of the deletion of all active Tat pathway components on the E. coli cells. The comprehensive proteomic analysis revealed activation of several stress responses and experimentally confirmed the dependence of certain proteins on the Tat system for export. We observed that a tat deletion triggers protein aggregation, membrane vesiculation, synthesis of colanic acid and biofilm formation. Furthermore, the mislocalization of Tat-dependent proteins disturbs iron and molybdenum homeostasis and impairs the cell envelope integrity. The results show that the functional Tat pathway is important for the physiological stability and that its dysfunction leads to a series of severe changes in E. coli cells., (Copyright © 2018 The Authors. Published by Elsevier GmbH.. All rights reserved.)

Published

2019

38. A Secreted Bacterial Peptidylarginine Deiminase Can Neutralize Human Innate Immune Defenses.

Author

Stobernack T, du Teil Espina M, Mulder LM, Palma Medina LM, Piebenga DR, Gabarrini G, Zhao X, Janssen KMJ, Hulzebos J, Brouwer E, Sura T, Becher D, van Winkelhoff AJ, Götz F, Otto A, Westra J, and van Dijl JM

Subjects

Adult, Antimicrobial Cationic Peptides antagonists & inhibitors, Extracellular Traps drug effects, Female, Gingiva chemistry, Gingiva microbiology, Humans, Male, Periodontitis pathology, Phagocytosis drug effects, Porphyromonas gingivalis growth & development, Protein-Arginine Deiminases analysis, Virulence Factors analysis, Immune Evasion, Immunity, Innate drug effects, Periodontitis microbiology, Porphyromonas gingivalis enzymology, Porphyromonas gingivalis immunology, Protein-Arginine Deiminases metabolism, Virulence Factors metabolism

Abstract

The keystone oral pathogen Porphyromonas gingivalis is associated with severe periodontitis. Intriguingly, this bacterium is known to secrete large amounts of an enzyme that converts peptidylarginine into citrulline residues. The present study was aimed at identifying possible functions of this citrullinating enzyme, named Porphyromonas peptidylarginine deiminase (PPAD), in the periodontal environment. The results show that PPAD is detectable in the gingiva of patients with periodontitis, and that it literally neutralizes human innate immune defenses at three distinct levels, namely bacterial phagocytosis, capture in neutrophil extracellular traps (NETs), and killing by the lysozyme-derived cationic antimicrobial peptide LP9. As shown by mass spectrometry, exposure of neutrophils to PPAD-proficient bacteria reduces the levels of neutrophil proteins involved in phagocytosis and the bactericidal histone H2. Further, PPAD is shown to citrullinate the histone H3, thereby facilitating the bacterial escape from NETs. Last, PPAD is shown to citrullinate LP9, thereby restricting its antimicrobial activity. The importance of PPAD for immune evasion is corroborated in the infection model Galleria mellonella , which only possesses an innate immune system. Together, the present observations show that PPAD-catalyzed protein citrullination defuses innate immune responses in the oral cavity, and that the citrullinating enzyme of P. gingivalis represents a new type of bacterial immune evasion factor. IMPORTANCE Bacterial pathogens do not only succeed in breaking the barriers that protect humans from infection, but they also manage to evade insults from the human immune system. The importance of the present study resides in the fact that protein citrullination is shown to represent a new bacterial mechanism for immune evasion. In particular, the oral pathogen P. gingivalis employs this mechanism to defuse innate immune responses by secreting a protein-citrullinating enzyme. Of note, this finding impacts not only the global health problem of periodontitis, but it also extends to the prevalent autoimmune disease rheumatoid arthritis, which has been strongly associated with periodontitis, PPAD activity, and loss of tolerance against citrullinated proteins, such as the histone H3., (Copyright © 2018 Stobernack et al.)

Published

2018

39. The Escherichia coli Type III Secretion System 2 Has a Global Effect on Cell Surface.

Author

Shulman A, Yair Y, Biran D, Sura T, Otto A, Gophna U, Becher D, Hecker M, and Ron EZ

Subjects

Escherichia coli genetics, Escherichia coli physiology, Fimbriae, Bacterial metabolism, Flagella metabolism, Flagella physiology, Flagellin genetics, Flagellin metabolism, Genomic Islands, Locomotion, Multigene Family, Sequence Deletion, Type III Secretion Systems genetics, Escherichia coli enzymology, Escherichia coli Proteins metabolism, Membrane Proteins metabolism, Type III Secretion Systems metabolism

Abstract

Many strains of Escherichia coli carry a 29,250-bp ETT2 pathogenicity island (PAI), which includes genes predicted to encode type III secretion system (T3SS) components. Because it is similar to the Salmonella pathogenicity island 1 (SPI-1) system, encoding a T3SS in Salmonella enterica , it was assumed that ETT2 also encodes a secretion system injecting effectors into host cells. This assumption was checked in E. coli serotype O2-associated with urinary tract infections and septicemia-which has an intact ETT2 gene cluster, in contrast to most strains in which this cluster carries deletions and mutations. A proteomic search did not reveal any putative secreted effector. Instead, the majority of the secreted proteins were identified as flagellar proteins. A deletion of the ETT2 gene cluster significantly reduced the secretion of flagellar proteins, resulting in reduced motility. There was also a significant reduction in the transcriptional level of flagellar genes, indicating that ETT2 affects the synthesis, rather than secretion, of flagellar proteins. The ETT2 deletion also resulted in additional major changes in secretion of fimbrial proteins and cell surface proteins, resulting in relative resistance to detergents and hydrophobic antibiotics (novobiocin), secretion of large amounts of outer membrane vesicles (OMVs), and altered multicellular behavior. Most important, the ETT2 deletion mutants were sensitive to serum. These major changes indicate that the ETT2 gene cluster has a global effect on cell surface and physiology, which is especially important for pathogenicity, as it contributes to the ability of the bacteria to survive serum and cause sepsis. IMPORTANCE Drug-resistant extraintestinal pathogenic E. coli (ExPEC) strains are major pathogens, especially in hospital- and community-acquired infections. They are the major cause of urinary tract infections and are often involved in septicemia with high mortality. ExPEC strains are characterized by broad-spectrum antibiotic resistance, and development of a vaccine is not trivial because the ExPEC strains include a large number of serotypes. It is therefore important to understand the virulence factors that are involved in pathogenicity of ExPEC and identify new targets for development of antibacterial drugs or vaccines. Such a target could be ETT2, a unique type III secretion system present (complete or in parts) in many ExPEC strains. Here, we show that this system has a major effect on the bacterial surface-it affects sensitivity to drugs, motility, and secretion of extracellular proteins and outer membrane vesicles. Most importantly, this system is important for serum resistance, a prerequisite for septicemia., (Copyright © 2018 Shulman et al.)

Published

2018

40. Genotype-Phenotype Correlation in Patients With Germline Mutations of VHL, RET, SDHB , and SDHD Genes: Thai Experience.

Author

Sriphrapradang C, Choopun K, Tunteeratum A, and Sura T

Abstract

Mutations in the VHL, RET, SDHB , and SDHD genes are responsible for von Hippel-Lindau (VHL) disease, multiple endocrine neoplasia type 2 (MEN2), and familial paraganglioma, respectively. However, genotype-phenotype correlation data are lacking in Southeast Asia. A retrospective medical chart review was performed on patients referred to the genetics service. We found 35 patients diagnosed with clinical syndromes (16 VHL, 9 MEN2, 9 paragangliomas, and 1 neurofibromatosis type 1). In patients with VHL, 5 known VHL mutations were identified: p.Trp88X, p.Ile151Thr, p.Arg161X, p.Arg167Gln, and p.Leu178Arg. The most frequent RET mutations in patients with MEN2A occurred at codon 634 on exon 11: p.Cys634Tyr, p.Cys634Trp, and p.Cys634Arg. A patient with MEN2B had p.Met918Thr RET mutation. Approximately, 90% of patients with MEN2 had medullary thyroid carcinoma. Pheochromocytoma was found in 55.6% of patients with MEN2, and 60% of them had bilateral lesions. One patient with malignant thoracic paraganglioma had p.Arg46X mutation of SDHB . This study provides mutation phenotypes that offer a useful tool for clinicians and patients to stratify disease risks and tailor screening programs., Competing Interests: DECLARATION OF CONFLICTING INTERESTS: The author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2017

41. Environmental lead exposure, catalase gene, and markers of antioxidant and oxidative stress relation to hypertension: an analysis based on the EGAT study.

Author

Sirivarasai J, Kaojarern S, Chanprasertyothin S, Panpunuan P, Petchpoung K, Tatsaneeyapant A, Yoovathaworn K, Sura T, Kaojarern S, and Sritara P

Subjects

Adult, Biomarkers blood, Blood Pressure genetics, Catalase blood, Cross-Sectional Studies, Erythrocytes metabolism, Glutathione blood, Glutathione Peroxidase blood, Humans, Hydrogen Peroxide metabolism, Hypertension blood, Lipid Peroxidation genetics, Male, Malondialdehyde blood, Middle Aged, Polymorphism, Genetic genetics, Superoxide Dismutase blood, Antioxidants metabolism, Catalase genetics, Environmental Exposure adverse effects, Hypertension genetics, Lead adverse effects, Lead blood, Oxidative Stress genetics

Abstract

Lead has been linked to the development of hypertension via oxidative stress. Catalase plays an important role in the disposal of hydrogen peroxide in erythrocyte and its activity was determined by CAT gene. The aims of this study were to investigate (1) the association between blood levels of antioxidant markers such as catalase, superoxide dismutase, glutathione, glutathione peroxidase, oxidative stress-marker (malondialdehyde), and blood lead level and (2) the influence of genetic polymorphism of CAT gene (rs769217) on change in blood pressure in general population of EGAT study project. This is a cross-sectional study of 332 normotensive, 432 prehypertensive, and 222 hypertensive male subjects. Hypertensive subjects had significantly higher blood lead level (5.28 μg/dL) compared to normotensive (4.41 μg/dL) and prehypertensive (4.55 μg/dL) subjects (P < 0.05). These significant findings are also found in MDA levels. Moreover, individuals with TT genotype in hypertensive group had significantly higher blood lead and MDA levels (6.06 μg/dL and 9.67 μmol/L) than those with CC genotype (5.32 μg/dL and 8.31 μmol/L, P < 0.05). Our findings suggested that decreased blood catalase activity in this polymorphism together with low level lead exposure induced lipid peroxidation may be responsible for hypertension.

Published

2015

42. Association between inflammatory marker, environmental lead exposure, and glutathione S-transferase gene.

Author

Sirivarasai J, Wananukul W, Kaojarern S, Chanprasertyothin S, Thongmung N, Ratanachaiwong W, Sura T, and Sritara P

Subjects

Adult, Alleles, Amino Acid Substitution, Biomarkers blood, Blood Pressure drug effects, Blood Pressure genetics, C-Reactive Protein genetics, C-Reactive Protein metabolism, Glutathione S-Transferase pi blood, Glutathione Transferase blood, Humans, Male, Middle Aged, Oxidative Stress drug effects, Oxidative Stress genetics, Environmental Exposure adverse effects, Glutathione S-Transferase pi genetics, Glutathione Transferase genetics, Lead pharmacokinetics, Lead Poisoning blood, Lead Poisoning enzymology, Lead Poisoning genetics, Polymorphism, Genetic

Abstract

A number of studies suggested that lead is related to the induction of oxidative stress, and alteration of immune response. In addition, modifying these toxic effects varied partly by GST polymorphism. The objectives of this study were to assess the association between the lead-induced alteration in serum hs-CRP, with GSTM1, GSTT1, and GSTP1 Val105Ile genetic variations and the health consequence from environmental lead exposure. The 924 blood samples were analyzed for blood lead, CRP, and genotyping of three genes with real-time PCR. Means of blood lead and serum hs-CRP were 5.45 μ g/dL and 2.07 mg/L. Both CRP and systolic blood pressure levels were significantly higher for individuals with blood lead in quartile 4 (6.48-24.63 μ g/dL) compared with those in quartile 1 (1.23-3.47 μ g/dL, P < 0.01). In particular, in men with blood lead >6.47 μ g/dL the adjusted odds ratio (OR) of CRP levels for individuals with GSTP1 variants allele, GSTM1 null, GSTT1 null, double-null GSTM1, and GSTT1 compared with wild-type allele was 1.46 (95% CI; 1.05-2.20), 1.32 (95% CI; 1.03-1.69), 1.65 (95% CI; 1.17-2.35), and 1.98 (95% CI; 1.47-2.55), respectively. Our findings suggested that lead exposure is associated with adverse changes in inflammatory marker and SBP. GST polymorphisms are among the genetic determinants related to lead-induced inflammatory response.

Published

2013

43. Genetic variations of glutathione s-transferase influence on blood cadmium concentration.

Author

Khansakorn N, Wongwit W, Tharnpoophasiam P, Hengprasith B, Suwannathon L, Chanprasertyothin S, Sura T, Kaojarern S, Sritara P, and Sirivarasai J

Abstract

The glutathione S-transferases (GSTs) are involved in biotransformation and detoxification of cadmium (Cd). Genetic polymorphisms in these genes may lead to interindividual variation in Cd susceptibility. The objective of this study was to assess the association of GSTs (GSTT1, GSTM1, and GSTP1 Val105Ile) polymorphisms with blood Cd concentrations in a nonoccupationally exposed population. The 370 blood samples were analyzed for Cd concentration and polymorphisms in GSTs genes. Geometric mean of blood Cd among this population was 0.46 ± 0.02 μg/L (with 95% CI; 0.43-0.49 μg/L). Blood Cd concentrations in subjects carrying GSTP1 Val/Val genotype were significantly higher than those with Ile/Ile and Ile/Val genotypes. No significant differences in blood Cd concentrations among individual with gene deletions of GSTT1 and GSTM1 were observed. GSTP1/GSTT1 and GSTP1/GSTM1 combinations showed significantly associated with increase in blood Cd levels. This study indicated that polymorphisms of GSTP1 combined with GSTT1 and/or GSTM1 deletion are likely to influence on individual susceptibility to cadmium toxicity.

Published

2012

44. Genome-wide association study identifies variations in 6p21.3 associated with nevirapine-induced rash.

Author

Chantarangsu S, Mushiroda T, Mahasirimongkol S, Kiertiburanakul S, Sungkanuparph S, Manosuthi W, Tantisiriwat W, Charoenyingwattana A, Sura T, Takahashi A, Kubo M, Kamatani N, Chantratita W, and Nakamura Y

Subjects

Anti-HIV Agents therapeutic use, Drug Eruptions etiology, Genetic Predisposition to Disease, HIV Infections drug therapy, Humans, Intracellular Signaling Peptides and Proteins genetics, Lamivudine therapeutic use, Logistic Models, Nevirapine therapeutic use, Polymorphism, Single Nucleotide, ROC Curve, Retrospective Studies, Risk Factors, Stavudine therapeutic use, Thailand, Anti-HIV Agents adverse effects, Chromosomes, Human, Pair 6, Drug Eruptions genetics, Genome-Wide Association Study methods, Nevirapine adverse effects

Abstract

Background: We aimed to identify disease-predisposing variations with nevirapine-induced rash using genome-wide single-nucleotide polymorphisms (SNPs) as genetic markers., Methods: A genome-wide association study (GWAS) was performed using ∼550000 markers in 72 human immunodeficiency virus (HIV)-infected Thai patients with nevirapine-induced rash and 77 nevirapine-tolerant patients, and then candidate SNPs were further evaluated in a replication set (88 patients with nevirapine-induced rash and 145 nevirapine-tolerant patients)., Results: The genome-wide association analysis and replication studies of candidate SNPs identified significant associations of nevirapine-induced rash with 2 SNPs (rs1265112 and rs746647) within CCHCR1 on chromosome 6p21.3 (P(GWAS) = 1.6 × 10(-4); P(replication) = 2.6 × 10(-5); P(combined) = 1.2 × 10(-8)). The odds ratio (OR) of the risk genotypes under a dominant model was 4.36 (95% confidence interval [CI], 2.58-7.36). The noncoding SNPs rs1265112 and rs746647 were in complete linkage disequilibrium with the nonsynonymous SNP rs1576 (r(2) = 1.00), which has been associated with psoriasis. The logistic regression analysis also indicated genetic variations in CCHCR1 to be significantly associated with rash, with an OR of 2.59 (95% CI, 1.82-3.68; P = .007). The receiver operating characteristic curve showed that the algorithm had an area under the curve of 76.4%, which was developed with 5 factors: rs1576*G status, HLA-B*3505 status, not receiving prescribed lead-in of nevirapine, history of drug allergy, and CD4 cell count prior to the nevirapine treatment., Conclusions: We demonstrated that genetic variations in CCHCR1 are strongly associated with nevirapine-induced rash. A predictive model that includes genetic and clinical risk factors for nevirapine-associated rash might be useful in lowering the incidence of rash associated with nevirapine initiation among HIV-infected patients.

Published

2011

45. Biochemical, environmental, and genetic factors associated with paraoxonase (PON1) activity.

Author

Sirivarasai J, Kaojarern S, Sura T, and Yoovathaworn K

Subjects

Adult, Alcohol Drinking metabolism, Aryldialkylphosphatase genetics, Carboxylic Ester Hydrolases metabolism, Enzyme Assays, Female, Genetic Association Studies, Genotype, Humans, Male, Middle Aged, Mutation, Missense, Regression Analysis, Risk Factors, Smoking metabolism, Young Adult, Aryldialkylphosphatase metabolism

Published

2011

46. The influence of metabolic gene polymorphisms on urinary 1-hydroxypyrene concentration in Thai bus drivers.

Author

Petchpoung K, Kaojarern S, Yoovathaworn K, Sura T, and Sirivarasai J

Subjects

Adult, Alcohol Drinking genetics, Alcohol Drinking metabolism, Cytochrome P-450 CYP1A1 genetics, DNA genetics, Exons genetics, Female, Genotype, Glutathione S-Transferase pi genetics, Glutathione Transferase genetics, Humans, Male, Middle Aged, Occupational Exposure analysis, Polycyclic Aromatic Hydrocarbons analysis, Polymerase Chain Reaction, Polymorphism, Restriction Fragment Length genetics, Smoking adverse effects, Thailand, Motor Vehicles, Occupational Exposure adverse effects, Polymorphism, Genetic genetics, Pyrenes metabolism

Abstract

Polycyclic aromatic hydrocarbons (PAHs) are associated with an increased cancer risk. CYP1A1 and GSTs enzymes are important in metabolism of PAHs. Genetic polymorphisms of these enzymes are responsible for enzyme activity and concentration variation. The objectives of this study were to evaluate association of 1-OHP concentration with genetic polymorphisms of CYP1A1 and GSTs in Thai bus drivers. The results showed that 1-OHP levels in bus drivers were significantly higher than that in the control group. Significant difference in 1-OHP was found between smokers and non-smokers, in only bus drivers. Significantly increasing of 1-OHP levels were observed in bus drivers with CYP1A1 MspI and exon 7 variants. Whereas, bus drivers with GSTP1 Val and GSTM1 null genotypes showed decreasing in excretion of 1-OHP. No association between 1-OHP and polymorphisms of GSTT1 was found. This study indicated that 1-OHP concentrations were associated with exposure to air pollution, cigarette smoking and polymorphisms of CYP1A1, GSTM1 and GSTP1 genes., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2011

47. Genome-wide linkage scan and association study of PARL to the expression of LHON families in Thailand.

Author

Phasukkijwatana N, Kunhapan B, Stankovich J, Chuenkongkaew WL, Thomson R, Thornton T, Bahlo M, Mushiroda T, Nakamura Y, Mahasirimongkol S, Tun AW, Srisawat C, Limwongse C, Peerapittayamongkol C, Sura T, Suthammarak W, and Lertrit P

Subjects

Adult, Female, Genetic Diseases, X-Linked genetics, Genetic Linkage, Genome-Wide Association Study, Humans, Male, Polymorphism, Single Nucleotide, Thailand, Metalloproteases genetics, Mitochondrial Proteins genetics, Optic Atrophy, Hereditary, Leber genetics

Abstract

Leber hereditary optic neuropathy (LHON) is the most common mitochondrially inherited disease causing blindness, preferentially in young adult males. Most of the patients carry the G11778A mitochondrial DNA (mtDNA) mutation. However, the marked incomplete penetrance and the gender bias indicate some additional genetic and/or environmental factors to disease expression. Herein, we first conducted a genome-wide linkage scan with 400 microsatellite markers in 9 large Thai LHON G11778A pedigrees. Using an affecteds-only nonparametric linkage analysis, 4 regions on chromosomes 3, 12, 13 and 18 showed Zlr scores greater than 2 (P < 0.025), which is consistently significant across several linkage statistics. The most suggestive marker D3S1565 (Zlr > 2 in 10 of 16 allele sharing models tested) was then expanded to include the region 3q26.2-3q28 covering SLC7A14 (3q26.2), MFN1 (3q26.32), MRPL47 (3q26.33), MCCC1 (3q27.1), PARL (3q27.1) and OPA1 (3q28-q29). All of these candidate genes were selected from the Maestro database and had known to be localized in mitochondria. Sixty tag SNPs were genotyped in 86 cases, 211 of their relatives and 32 unrelated Thai controls, by multiplex-PCR-based Invader assay. Analyses using a powerful association testing tool that adjusts for relatedness (the M(QLS) statistic) showed the most evidence of association between two SNPs, rs3749446 and rs1402000 (located in PARL presenilins-associated rhomboid-like) and LHON expression (both P = 8.8 x 10(-5)). The mitochondrial PARL protease has been recently known to play a role with a dynamin-related OPA1 protein in preventing apoptotic events by slowing down the release of cytochrome c out of mitochondrial cristae junctions. Moreover, PARL is required to activate the intramembranous proteolyses resulting in the degradation of an accumulated pro-apoptotic protein in the outer mitochondrial membrane. Under these circumstances, variants of PARL are suggested to influence cell death by apoptosis which has long been believed to intrigue the neurodegeneration of LHON.

Published

2010

48. Heritability of the human infectious reservoir of malaria parasites.

Author

Lawaly YR, Sakuntabhai A, Marrama L, Konate L, Phimpraphi W, Sokhna C, Tall A, Sarr FD, Peerapittayamongkol C, Louicharoen C, Schneider BS, Levescot A, Talman A, Casademont I, Menard D, Trape JF, Rogier C, Kaewkunwal J, Sura T, Nuchprayoon I, Ariey F, Baril L, Singhasivanon P, Mercereau-Puijalon O, and Paul R

Subjects

Anemia, Sickle Cell parasitology, Animals, Cohort Studies, Humans, Reverse Transcriptase Polymerase Chain Reaction, alpha-Thalassemia parasitology, Disease Reservoirs, Plasmodium falciparum pathogenicity, Plasmodium vivax pathogenicity

Abstract

Background: Studies on human genetic factors associated with malaria have hitherto concentrated on their role in susceptibility to and protection from disease. In contrast, virtually no attention has been paid to the role of human genetics in eliciting the production of parasite transmission stages, the gametocytes, and thus enhancing the spread of disease., Methods and Findings: We analysed four longitudinal family-based cohort studies from Senegal and Thailand followed for 2-8 years and evaluated the relative impact of the human genetic and non-genetic factors on gametocyte production in infections of Plasmodium falciparum or P. vivax. Prevalence and density of gametocyte carriage were evaluated in asymptomatic and symptomatic infections by examination of Giemsa-stained blood smears and/or RT-PCR (for falciparum in one site). A significant human genetic contribution was found to be associated with gametocyte prevalence in asymptomatic P. falciparum infections. By contrast, there was no heritability associated with the production of gametocytes for P. falciparum or P. vivax symptomatic infections. Sickle cell mutation, HbS, was associated with increased gametocyte prevalence but its contribution was small., Conclusions: The existence of a significant human genetic contribution to gametocyte prevalence in asymptomatic infections suggests that candidate gene and genome wide association approaches may be usefully applied to explore the underlying human genetics. Prospective epidemiological studies will provide an opportunity to generate novel and perhaps more epidemiologically pertinent gametocyte data with which similar analyses can be performed and the role of human genetics in parasite transmission ascertained.

Published

2010

49. Positively selected G6PD-Mahidol mutation reduces Plasmodium vivax density in Southeast Asians.

Author

Louicharoen C, Patin E, Paul R, Nuchprayoon I, Witoonpanich B, Peerapittayamongkol C, Casademont I, Sura T, Laird NM, Singhasivanon P, Quintana-Murci L, and Sakuntabhai A

Subjects

Aging, Erythrocytes metabolism, Erythrocytes parasitology, Female, Gene Dosage, Genetic Association Studies, Genetic Predisposition to Disease, Genotype, Glucosephosphate Dehydrogenase Deficiency blood, Glucosephosphate Dehydrogenase Deficiency complications, Haplotypes, Humans, Immunity, Innate, Malaria, Falciparum complications, Malaria, Falciparum genetics, Malaria, Falciparum parasitology, Malaria, Vivax complications, Malaria, Vivax genetics, Male, Plasmodium falciparum physiology, Polymorphism, Single Nucleotide, Thailand, Glucosephosphate Dehydrogenase genetics, Glucosephosphate Dehydrogenase Deficiency genetics, Malaria, Vivax parasitology, Mutation, Plasmodium vivax physiology, Selection, Genetic

Abstract

Glucose-6-phosphate dehydrogenase (G6PD) deficiency--the most common known enzymopathy--is associated with neonatal jaundice and hemolytic anemia usually after exposure to certain infections, foods, or medications. Although G6PD-deficient alleles appear to confer a protective effect against malaria, the link with clinical protection from Plasmodium infection remains unclear. We investigated the effect of a common G6PD deficiency variant in Southeast Asia--the G6PD-Mahidol(487A) variant--on human survival related to vivax and falciparum malaria. Our results show that strong and recent positive selection has targeted the Mahidol variant over the past 1500 years. We found that the G6PD-Mahidol(487A) variant reduces vivax, but not falciparum, parasite density in humans, which indicates that Plasmodium vivax has been a driving force behind the strong selective advantage conferred by this mutation.

Published

2009

50. Frequencies of spinocerebellar ataxia subtypes in Thailand: window to the population history?

Author

Sura T, Eu-Ahsunthornwattana J, Youngcharoen S, Busabaratana M, Dejsuphong D, Trachoo O, Theerasasawat S, Tunteeratum A, Noparutchanodom C, and Tunlayadechanont S

Subjects

Geography, Humans, Thailand epidemiology, Genetics, Population, Spinocerebellar Ataxias classification, Spinocerebellar Ataxias epidemiology

Abstract

Spinocerebellar ataxias (SCAs) are a heterogeneous group of disorders with almost 30 subtypes. The prevalence and relative frequency of each subtype vary among different populations. In this article, we report the relative frequency of six SCA subtypes in the Thai population and attempt to explain the observed pattern when compared with other populations in this region. We searched for SCA type 1, SCA2, SCA3, SCA6, SCA7 and dentatorubral-pallidoluysian atrophy mutations using GeneScan analysis in 340 patients from 182 families, in which at least one person had a clinical diagnosis of SCA. We analyzed the relative frequencies of SCA subtypes on a family basis, and compared these with the data in the Chinese and Indian populations. SCA3 was found in 19.2% of the patients (Agresti-Coull 95% confidence interval: 14.1-25.6%), SCA1 in 11.5% (7.6-17.1%) and SCA2 in 10.4% (6.7-15.8%). SCA6 was found in three families, with a relative frequency of 1.6% (0.3-5.0%). Compared with the related populations, the Thai SCA3 frequency was less than that of the Chinese, whereas it was higher than that in most of the Indian studies. The reverse is true for the SCA1/SCA2 frequency. A similar study in Singapore, where there was a clear history of population admixture, also showed the frequencies between those of the Chinese and the Indian populations. Although SCA3 was the most common identifiable SCA subtype in Thailand, SCA1 and SCA2 were also relatively common. Our results also supported some degree of admixture with the Indians in the Thai population and justify further study in the area.

Published

2009