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1. Post-COVID-19 Thoracic Aortic Rupture with an Unforeseen Spinal Epidural Hematoma

Author

Kush R. Lohani, Vikram V. Sannasi, Harvinder R. S. Sidhu, Oon C. Ooi, Wu P. Hung, and Min Q. Chen

Subjects
Radiology, Nuclear Medicine and imaging, Surgery, Cardiology and Cardiovascular Medicine
Abstract

The importance of prompt diagnosis and early stenting of an aortic rupture cannot be overemphasized. We present a case of thoracic aortic rupture in a middle-aged gentleman who had recently suffered coronavirus disease 2019. The case was further complicated by the development of an unexpected spinal epidural hematoma.

Published
2023

2. STCF Conceptual Design Report: Volume 1 -- Physics & Detector

Author

Achasov, M., Ai, X. C., Aliberti, R., An, Q., Bai, X. Z., Bai, Y., Bakina, O., Barnyakov, A., Blinov, V., Bobrovnikov, V., Bodrov, D., Bogomyagkov, A., Bondar, A., Boyko, I., Bu, Z. H., Cai, F. M., Cai, H., Cao, J. J., Cao, Q. H., Cao, Z., Chang, Q., Chao, K. T., Chen, D. Y., Chen, H., Chen, H. X., Chen, J. F., Chen, K., Chen, L. L., Chen, P., Chen, S. L., Chen, S. M., Chen, S., Chen, S. P., Chen, W., Chen, X. F., Chen, X., Chen, Y., Chen, Y. Q., Cheng, H. Y., Cheng, J., Cheng, S., Dai, J. P., Dai, L. Y., Dai, X. C., Dedovich, D., Denig, A., Denisenko, I., Ding, D. Z., Dong, L. Y., Dong, W. H., Druzhinin, V., Du, D. S., Du, Y. J., Du, Z. G., Duan, L. M., Epifanov, D., Fan, Y. L., Fang, S. S., Fang, Z. J., Fedotovich, G., Feng, C. Q., Feng, X., Feng, Y. T., Fu, J. L., Gao, J., Ge, P. S., Geng, C. Q., Geng, L. S., Gilman, A., Gong, L., Gong, T., Gradl, W., Gu, J. L., Escalante, A. G., Gui, L. C., Guo, F. K., Guo, J. C., Guo, J., Guo, Y. P., Guo, Z. H., Guskov, A., Han, K. L., Han, L., Han, M., Hao, X. Q., He, J. B., He, S. Q., He, X. G., He, Y. L., He, Z. B., Heng, Z. X., Hou, B. L., Hou, T. J., Hou, Y. R., Hu, C. Y., Hu, H. M., Hu, K., Hu, R. J., Hu, X. H., Hu, Y. C., Hua, J., Huang, G. S., Huang, J. S., Huang, M., Huang, Q. Y., Huang, W. Q., Huang, X. T., Huang, X. J., Huang, Y. B., Huang, Y. S., Hüsken, N., Ivanov, V., Ji, Q. P., Jia, J. J., Jia, S., Jia, Z. K., Jiang, H. B., Jiang, J., Jiang, S. Z., Jiao, J. B., Jiao, Z., Jing, H. J., Kang, X. L., Kang, X. S., Ke, B. C., Kenzie, M., Khoukaz, A., Koop, I., Kravchenko, E., Kuzmin, A., Lei, Y., Levichev, E., Li, C. H., Li, C., Li, D. Y., Li, F., Li, G., Li, H. B., Li, H., Li, H. N., Li, H. J., Li, H. L., Li, J. M., Li, J., Li, L., Li, L. Y., Li, N., Li, P. R., Li, R. H., Li, S., Li, T., Li, W. J., Li, X. H., Li, X. Q., Li, Y., Li, Y. Y., Li, Z. J., Liang, H., Liang, J. H., Liao, G. R., Liao, L. Z., Liao, Y., Lin, C. X., Lin, X. S., Liu, B. J., Liu, C. W., Liu, D., Liu, F., Liu, G. M., Liu, H. B., Liu, J., Liu, J. J., Liu, J. B., Liu, K., Liu, K. Y., Liu, L., Liu, Q., Liu, S. B., Liu, T., Liu, X., Liu, Y. W., Liu, Y., Liu, Y. L., Liu, Z. Q., Liu, Z. Y., Liu, Z. W., Logashenko, I., Long, Y., Lu, C. G., Lu, N., Lü, Q. F., Lu, Y., Lv, Z., Lukin, P., Luo, F. J., Luo, T., Luo, X. F., Lyu, H. J., Lyu, X. R., Ma, J. P., Ma, P., Ma, Y., Maas, F., Malde, S., Matvienko, D., Meng, Z. X., Mitchell, R., Dias, J. M., Nefediev, A., Nefedov, Y., Olsen, S. L., Ouyang, Q., Pakhlov, P., Pakhlova, G., Pan, X., Pan, Y., Passemar, E., Pei, Y. P., Peng, H. P., Peng, L., Peng, X. Y., Peng, X. J., Peters, K., Pivovarov, S., Pyata, E., Qi, B. B., Qi, Y. Q., Qian, W. B., Qian, Y., Qiao, C. F., Qin, J. J., Qin, L. Q., Qin, X. S., Qiu, T. L., Rademacker, J., Redmer, C. F., Sang, H. Y., Saur, M., Shan, W., Shan, X. Y., Shang, L. L., Shao, M., Shekhtman, L., Shen, C. P., Shen, J. M., Shen, Z. T., Shi, H. C., Shi, X. D., Shwartz, B., Sokolov, A., Song, J. J., Song, W. M., Song, Y., Song, Y. X., Sukharev, A., Sun, J. F., Sun, L., Sun, X. M., Sun, Y. J., Sun, Z. P., Tang, J., Tang, S. S., Tang, Z. B., Tian, C. H., Tian, J. S., Tikhonov, Y., Todyshev, K., Uglov, T., Vorobyev, V., Wan, B. D., Wang, B. L., Wang, B., Wang, D. Y., Wang, G. Y., Wang, G. L., Wang, H. L., Wang, J., Wang, J. H., Wang, J. C., Wang, M. L., Wang, R., Wang, S. B., Wang, W., Wang, W. P., Wang, X. C., Wang, X. D., Wang, X. L., Wang, X. P., Wang, X. F., Wang, Y. D., Wang, Y. P., Wang, Y. Q., Wang, Y. L., Wang, Y. G., Wang, Z. Y., Wang, Z. L., Wang, Z. G., Wei, D. H., Wei, X. L., Wei, X. M., Wen, Q. G., Wen, X. J., Wilkinson, G., Wu, B., Wu, J. J., Wu, L., Wu, P. W., Wu, T. W., Wu, Y. S., Xia, L., Xiang, T., Xiao, C. W., Xiao, D., Xiao, M., Xie, Y. H., Xing, Y., Xing, Z. Z., Xiong, X. N., Xu, F. R., Xu, J., Xu, L. L., Xu, Q. N., Xu, X. C., Xu, X. P., Xu, Y. C., Xu, Y. P., Xu, Y., Xu, Z. Z., Xuan, D. W., Xue, F. F., Yan, L., Yan, M. J., Yan, W. B., Yan, W. C., Yan, X. S., Yang, B. F., Yang, C., Yang, H. J., Yang, H. R., Yang, H. T., Yang, J. F., Yang, S. L., Yang, Y. D., Yang, Y. H., Yang, Y. S., Yang, Y. L., Yang, Z. Y., Yao, D. L., Yin, H., Yin, X. H., Yokozaki, N., You, S. Y., You, Z. Y., Yu, C. X., Yu, F. S., Yu, G. L., Yu, H. L., Yu, J. S., Yu, J. Q., Yuan, L., Yuan, X. B., Yue, Y. F., Zeng, M., Zeng, S., Zhang, A. L., Zhang, B. W., Zhang, G. Y., Zhang, G. Q., Zhang, H. J., Zhang, H. B., Zhang, J. Y., Zhang, J. L., Zhang, J., Zhang, L., Zhang, L. M., Zhang, R., Zhang, S. L., Zhang, T., Zhang, X., Zhang, Y., Zhang, Y. X., Zhang, Y. T., Zhang, Y. F., Zhang, Y. C., Zhang, Y. M., Zhang, Y. L., Zhang, Z. H., Zhang, Z. Y., Zhao, H. Y., Zhao, J., Zhao, L., Zhao, M. G., Zhao, Q., Zhao, R. G., Zhao, R. P., Zhao, Z. G., Zhao, Z. X., Zhemchugov, A., Zheng, B., Zheng, L., Zheng, Q. B., Zheng, R., Zheng, Y. H., Zhong, X. H., Zhou, H. J., Zhou, H. Q., Zhou, H., Zhou, S. H., Zhou, X., Zhou, X. K., Zhou, X. R., Zhou, Y. L., Zhou, Y., Zhou, Y. X., Zhou, Z. Y., Zhu, J. Y., Zhu, K., Zhu, R. D., Zhu, R. L., Zhu, S. H., Zhu, Y. C., Zhu, Z. A., Zhukova, V., Zhulanov, V., Zou, B. S., and Zuo, Y. B.

Subjects
High Energy Physics - Phenomenology, High Energy Physics - Experiment (hep-ex), Physics - Instrumentation and Detectors, High Energy Physics - Phenomenology (hep-ph), FOS: Physical sciences, Instrumentation and Detectors (physics.ins-det), High Energy Physics - Experiment
Abstract

The Super $τ$-Charm facility (STCF) is an electron-positron collider proposed by the Chinese particle physics community. It is designed to operate in a center-of-mass energy range from 2 to 7 GeV with a peak luminosity of $0.5\times 10^{35}{\rm cm}^{-2}{\rm s}^{-1}$ or higher. The STCF will produce a data sample about a factor of 100 larger than that by the present $τ$-Charm factory -- the BEPCII, providing a unique platform for exploring the asymmetry of matter-antimatter (charge-parity violation), in-depth studies of the internal structure of hadrons and the nature of non-perturbative strong interactions, as well as searching for exotic hadrons and physics beyond the Standard Model. The STCF project in China is under development with an extensive R\&D program. This document presents the physics opportunities at the STCF, describes conceptual designs of the STCF detector system, and discusses future plans for detector R\&D and physics case studies.

Published
2023
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3. Glacial Isostatic Adjustment and sea-level change in Singapore and Southeast Asia: Implications from past to future

Author

Li, T., Shaw, T., Kim, H., Chua, S., Wu, P., and Horton, B.

Abstract

Over 400 million people in Southeast Asia live in low elevation coastal zones and are susceptible to future relative sea-level (RSL) rise. Projections of future RSL rely on an accurate understanding of sea-level driving processes such as Glacial Isostatic Adjustment (GIA). Here we apply GIA models, paleo RSL records and instrumental data to demonstrate the evolution of RSL changes in Singapore and Southeast Asia and the associated impacts.We reconstructed RSL since the Last Glacial Maximum (LGM) to quantify magnitudes and rates of RSL changes through time and used GIA model to assess paleotopography changes and impacts to human populations. We applied the Intergovernmental Panel on Climate Change (IPCC) RSL projections and used the geological past to provide probabilityperspectives when IPCC future projections were last exceeded in Singapore. Future projections under a moderate emissions scenario show RSL rising 0.95 m at a rate of 7.3 mm/yr by 2150 which was only exceeded (> 99% probability) during rapid ice melting events (MWPs) ~14.5 and ~9 ka BP. We inferred the human population history using 763 high-coverage whole-genome datasets. Integrated paleotopographic and population genomic analysis demonstrates the earliest documented instance of forced human migration driven by rapid sea-level rise (e.g., WMPs). We investigated the mid-Holocene highstand sensitivity revealing that Earth model variation affects the magnitude and ice model variation changes both the timing and magnitude of the highstand. Lastly, we produced a highstand “treasure map” to guide future highstand data collection efforts as the highstand is poorly constrained currently.&nbsp, The 28th IUGG General Assembly (IUGG2023) (Berlin 2023)

Published
2023
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4. A Next-Generation Liquid Xenon Observatory for Dark Matter and Neutrino Physics

Author

Aalbers, J, AbdusSalam, SS, Abe, K, Aerne, V, Agostini, F, Ahmed Maouloud, S, Akerib, DS, Akimov, DY, Akshat, J, Al Musalhi, AK, Alder, F, Alsum, SK, Althueser, L, Amarasinghe, CS, Amaro, FD, Ames, A, Anderson, TJ, Andrieu, B, Angelides, N, Angelino, E, Angevaare, J, Antochi, VC, Antón Martin, D, Antunovic, B, Aprile, E, Araújo, HM, Armstrong, JE, Arneodo, F, Arthurs, M, Asadi, P, Baek, S, Bai, X, Bajpai, D, Baker, A, Balajthy, J, Balashov, S, Balzer, M, Bandyopadhyay, A, Bang, J, Barberio, E, Bargemann, JW, Baudis, L, Bauer, D, Baur, D, Baxter, A, Baxter, AL, Bazyk, M, Beattie, K, Behrens, J, Bell, NF, Bellagamba, L, Beltrame, P, Benabderrahmane, M, Bernard, EP, Bertone, GF, Bhattacharjee, P, Bhatti, A, Biekert, A, Biesiadzinski, TP, Binau, AR, Biondi, R, Biondi, Y, Birch, HJ, Bishara, F, Bismark, A, Blanco, C, Blockinger, GM, Bodnia, E, Boehm, C, Bolozdynya, AI, Bolton, PD, Bottaro, S, Bourgeois, C, Boxer, B, Brás, P, Breskin, A, Breur, PA, Brew, CAJ, Brod, J, Brookes, E, Brown, A, Brown, E, Bruenner, S, Bruno, G, Budnik, R, Bui, TK, Burdin, S, Buse, S, Busenitz, JK, Buttazzo, D, Buuck, M, Buzulutskov, A, Cabrita, R, Cai, C, Cai, D, Capelli, C, Cardoso, JMR, Carmona-Benitez, MC, Cascella, M, Catena, R, Chakraborty, S, Chan, C, Chang, S, Chauvin, A, Chawla, A, Chen, H, Chepel, V, Chott, NI, Cichon, D, Cimental Chavez, A, Cimmino, B, Clark, M, Co, RT, Colijn, AP, Conrad, J, Converse, MV, Costa, M, Cottle, A, Cox, G, Creaner, O, Cuenca Garcia, JJ, Cussonneau, JP, Cutter, JE, Dahl, CE, D’Andrea, V, David, A, Decowski, MP, Dent, JB, Deppisch, FF, De Viveiros, L, Di Gangi, P, Di Giovanni, A, Di Pede, S, Dierle, J, Diglio, S, Dobson, JEY, Doerenkamp, M, Douillet, D, Drexlin, G, Druszkiewicz, E, Dunsky, D, Eitel, K, Elykov, A, Emken, T, Engel, R, Eriksen, Fairbairn, M, Fan, A, Fan, JJ, Farrell, SJ, Fayer, S, Fearon, NM, Ferella, A, Ferrari, C, Fieguth, A, Fiorucci, S, Fischer, H, Flaecher, H, Flierman, M, Florek, T, Foot, R, Fox, PJ, Franceschini, R, Fraser, ED, Frenk, CS, Frohlich, S, Fruth, T, Fulgione, W, Fuselli, C, Gaemers, P, Gaior, R, Gaitskell, RJ, Galloway, M, Gao, F, Garcia Garcia, I, Genovesi, J, Ghag, C, Ghosh, S, Gibson, E, Gil, W, Giovagnoli, D, Girard, F, Glade-Beucke, R, Glück, F, Gokhale, S, De Gouvêa, A, Gráf, L, Grandi, L, Grigat, J, Grinstein, B, Van Der Grinten, MGD, Grössle, R, Guan, H, Guida, M, Gumbsheimer, R, Gwilliam, CB, Hall, CR, Hall, LJ, Hammann, R, Han, K, Hannen, V, Hansmann-Menzemer, S, Harata, R, Hardin, SP, Hardy, E, Hardy, CA, Harigaya, K, Harnik, R, Haselschwardt, SJ, Hernandez, M, Hertel, SA, Higuera, A, Hils, C, Hochrein, S, Hoetzsch, L, Hoferichter, M, Hood, N, Hooper, D, Horn, M, Howlett, J, Huang, DQ, Huang, Y, Hunt, D, Iacovacci, M, Iaquaniello, G, Ide, R, Ignarra, CM, Iloglu, G, Itow, Y, Jacquet, E, Jahangir, O, Jakob, J, James, RS, Jansen, A, Ji, W, Ji, X, Joerg, F, Johnson, J, Joy, A, Kaboth, AC, Kalhor, L, Kamaha, AC, Kanezaki, K, Kar, K, Kara, M, Kato, N, Kavrigin, P, Kazama, S, Keaveney, AW, Kellerer, J, Khaitan, D, Khazov, A, Khundzakishvili, G, Khurana, I, Kilminster, B, Kleifges, M, Ko, P, Kobayashi, M, Kodroff, D, Koltmann, G, Kopec, A, Kopmann, A, Kopp, J, Korley, L, Kornoukhov, VN, Korolkova, EV, Kraus, H, Krauss, LM, Kravitz, S, Kreczko, L, Kudryavtsev, VA, Kuger, F, Kumar, J, López Paredes, B, LaCascio, L, Laha, R, Laine, Q, Landsman, H, Lang, RF, Leason, EA, Lee, J, Leonard, DS, Lesko, KT, Levinson, L, Levy, C, Li, I, Li, SC, Li, T, Liang, S, Liebenthal, CS, Lin, J, Lin, Q, Lindemann, S, Lindner, M, Lindote, A, Linehan, R, Lippincott, WH, Liu, X, Liu, K, Liu, J, Loizeau, J, Lombardi, F, Long, J, Lopes, MI, Lopez Asamar, E, Lorenzon, W, Lu, C, Luitz, S, Ma, Y, Machado, PAN, Macolino, C, Maeda, T, Mahlstedt, J, Majewski, PA, Manalaysay, A, Mancuso, A, Manenti, L, Manfredini, A, Mannino, RL, Marangou, N, March-Russell, J, Marignetti, F, Marrodán Undagoitia, T, Martens, K, Martin, R, Martinez-Soler, I, Masbou, J, Masson, D, Masson, E, Mastroianni, S, Mastronardi, M, Matias-Lopes, JA, McCarthy, ME, McFadden, N, McGinness, E, McKinsey, DN, McLaughlin, J, McMichael, K, Meinhardt, P, Menéndez, J, Meng, Y, Messina, M, Midha, R, Milisavljevic, D, Miller, EH, Milosevic, B, Milutinovic, S, Mitra, SA, Miuchi, K, Mizrachi, E, Mizukoshi, K, Molinario, A, Monte, A, Monteiro, CMB, Monzani, ME, Moore, JS, Morå, K, Morad, JA, Morales Mendoza, JD, Moriyama, S, Morrison, E, Morteau, E, Mosbacher, Y, Mount, BJ, Mueller, J, Murphy, A St J, Murra, M, Naim, D, Nakamura, S, Nash, E, Navaieelavasani, N, Naylor, A, Nedlik, C, Nelson, HN, Neves, F, Newstead, JL, Ni, K, Nikoleyczik, JA, Niro, V, Oberlack, UG, Obradovic, M, Odgers, K, O’Hare, CAJ, Oikonomou, P, Olcina, I, Oliver-Mallory, K, Oranday, A, Orpwood, J, Ostrovskiy, I, Ozaki, K, Paetsch, B, Pal, S, Palacio, J, Palladino, KJ, Palmer, J, Panci, P, Pandurovic, M, Parlati, A, Parveen, N, Patton, SJ, Pěč, V, Pellegrini, Q, Penning, B, Pereira, G, Peres, R, Perez-Gonzalez, Y, Perry, E, Pershing, T, Petrossian-Byrne, R, Pienaar, J, Piepke, A, Pieramico, G, Pierre, M, Piotter, M, Pizzella, V, Plante, G, Pollmann, T, Porzio, D, Qi, J, Qie, Y, Qin, J, Quevedo, F, Raj, N, Rajado Silva, M, Ramanathan, K, Ramírez García, D, Ravanis, J, Redard-Jacot, L, Redigolo, D, Reichard, S, Reichenbacher, J, Rhyne, CA, Richards, A, Riffard, Q, Rischbieter, GRC, Rocchetti, A, Rosenfeld, SL, Rosero, R, Rupp, N, Rushton, T, Saha, S, Salucci, P, Sanchez, L, Sanchez-Lucas, P, Santone, D, Dos Santos, JMF, Sarnoff, I, Sartorelli, G, Sazzad, ABMR, Scheibelhut, M, Schnee, RW, Schrank, M, Schreiner, J, Schulte, P, Schulte, D, Schulze Eissing, H, Schumann, M, Schwemberger, T, Schwenk, A, Schwetz, T, Scotto Lavina, L, Scovell, PR, Sekiya, H, Selvi, M, Semenov, E, Semeria, F, Shagin, P, Shaw, S, Shi, S, Shockley, E, Shutt, TA, Si-Ahmed, R, Silk, JJ, Silva, C, Silva, MC, Simgen, H, Šimkovic, F, Sinev, G, Singh, R, Skulski, W, Smirnov, J, Smith, R, Solmaz, M, Solovov, VN, Sorensen, P, Soria, J, Sparmann, TJ, Stancu, I, Steidl, M, Stevens, A, Stifter, K, Strigari, LE, Subotic, D, Suerfu, B, Suliga, AM, Sumner, TJ, Szabo, P, Szydagis, M, Takeda, A, Takeuchi, Y, Tan, P-L, Taricco, C, Taylor, WC, Temples, DJ, Terliuk, A, Terman, PA, Thers, D, Thieme, K, Thümmler, T, Tiedt, DR, Timalsina, M, To, WH, Toennies, F, Tong, Z, Toschi, F, Tovey, DR, Tranter, J, Trask, M, Trinchero, GC, Tripathi, M, Tronstad, DR, Trotta, R, Tsai, YD, Tunnell, CD, Turner, WG, Ueno, R, Urquijo, P, Utku, U, Vaitkus, A, Valerius, K, Vassilev, E, Vecchi, S, Velan, V, Vetter, S, Vincent, AC, Vittorio, L, Volta, G, Von Krosigk, B, Von Piechowski, M, Vorkapic, D, Wagner, CEM, Wang, AM, Wang, B, Wang, Y, Wang, W, Wang, JJ, Wang, L-T, Wang, M, Watson, Wei, Y, Weinheimer, C, Weisman, E, Weiss, M, Wenz, D, West, SM, Whitis, TJ, Williams, M, Wilson, MJ, Winkler, D, Wittweg, C, Wolf, J, Wolf, T, Wolfs, FLH, Woodford, S, Woodward, D, Wright, CJ, Wu, VHS, Wu, P, Wüstling, S, Wurm, M, Xia, Q, Xiang, X, Xing, Y, Xu, J, Xu, Z, Xu, D, Yamashita, M, Yamazaki, R, Yan, H, Yang, L, Yang, Y, Ye, J, Yeh, M, Young, I, Yu, HB, Yu, TT, Yuan, L, Zavattini, G, Zerbo, S, Zhang, Y, Zhong, M, Zhou, N, Zhou, X, Zhu, T, Zhu, Y, Zhuang, Y, Zopounidis, JP, Zuber, K, Zupan, J, Aalbers, J, S AbdusSalam, S, Abe, K, Aerne, V, Agostini, F, Ahmed Maouloud, S, S Akerib, D, Y Akimov, D, Akshat, J, K Al Musalhi, A, Alder, F, K Alsum, S, Althueser, L, S Amarasinghe, C, D Amaro, F, Ames, A, J Anderson, T, Andrieu, B, Angelides, N, Angelino, E, Angevaare, J, C Antochi, V, Ant??n Martin, D, Antunovic, B, Aprile, E, M Ara??jo, H, E Armstrong, J, Arneodo, F, Arthurs, M, Asadi, P, Baek, S, Bai, X, Bajpai, D, Baker, A, Balajthy, J, Balashov, S, Balzer, M, Bandyopadhyay, A, Bang, J, Barberio, E, W Bargemann, J, Baudis, L, Bauer, D, Baur, D, Baxter, A, L Baxter, A, Bazyk, M, Beattie, K, Behrens, J, F Bell, N, Bellagamba, L, Beltrame, P, Benabderrahmane, M, P Bernard, E, F Bertone, G, Bhattacharjee, P, Bhatti, A, Biekert, A, P Biesiadzinski, T, R Binau, A, Biondi, R, Biondi, Y, J Birch, H, Bishara, F, Bismark, A, Blanco, C, M Blockinger, G, Bodnia, E, Boehm, C, I Bolozdynya, A, D Bolton, P, Bottaro, S, Bourgeois, C, Boxer, B, Br??s, P, Breskin, A, A Breur, P, J Brew, C A, Brod, J, Brookes, E, Brown, A, Brown, E, Bruenner, S, Bruno, G, Budnik, R, K Bui, T, Burdin, S, Buse, S, K Busenitz, J, Buttazzo, D, Buuck, M, Buzulutskov, A, Cabrita, R, Cai, C, Cai, D, Capelli, C, R Cardoso, J M, C Carmona-Benitez, M, Cascella, M, Catena, R, Chakraborty, S, Chan, C, Chang, S, Chauvin, A, Chawla, A, Chen, H, Chepel, V, I Chott, N, Cichon, D, Cimental Chavez, A, Cimmino, B, Clark, M, T Co, R, P Colijn, A, Conrad, J, V Converse, M, Costa, M, Cottle, A, Cox, G, Creaner, O, J Cuenca Garcia, J, P Cussonneau, J, E Cutter, J, E Dahl, C, D???andrea, V, David, A, P Decowski, M, B Dent, J, F Deppisch, F, de Viveiros, L, Di Gangi, P, Di Giovanni, A, Di Pede, S, Dierle, J, Diglio, S, Y Dobson, J E, Doerenkamp, M, Douillet, D, Drexlin, G, Druszkiewicz, E, Dunsky, D, Eitel, K, Elykov, A, Emken, T, Engel, R, R Eriksen, S, Fairbairn, M, Fan, A, J Fan, J, J Farrell, S, Fayer, S, M Fearon, N, Ferella, A, Ferrari, C, Fieguth, A, Fiorucci, S, Fischer, H, Flaecher, H, Flierman, M, Florek, T, Foot, R, J Fox, P, Franceschini, R, D Fraser, E, S Frenk, C, Frohlich, S, Fruth, T, Fulgione, W, Fuselli, C, Gaemers, P, Gaior, R, J Gaitskell, R, Galloway, M, Gao, F, Garcia Garcia, I, Genovesi, J, Ghag, C, Ghosh, S, Gibson, E, Gil, W, Giovagnoli, D, Girard, F, Glade-Beucke, R, Gl??ck, F, Gokhale, S, de Gouv??a, A, Gr??f, L, Grandi, L, Grigat, J, Grinstein, B, D van der Grinten, M G, Gr??ssle, R, Guan, H, Guida, M, Gumbsheimer, R, B Gwilliam, C, R Hall, C, J Hall, L, Hammann, R, Han, K, Hannen, V, Hansmann-Menzemer, S, Harata, R, P Hardin, S, Hardy, E, A Hardy, C, Harigaya, K, Harnik, R, J Haselschwardt, S, Hernandez, M, A Hertel, S, Higuera, A, Hils, C, Hochrein, S, Hoetzsch, L, Hoferichter, M, Hood, N, Hooper, D, Horn, M, Howlett, J, Q Huang, D, Huang, Y, Hunt, D, Iacovacci, M, Iaquaniello, G, Ide, R, M Ignarra, C, Iloglu, G, Itow, Y, Jacquet, E, Jahangir, O, Jakob, J, S James, R, Jansen, A, Ji, W, Ji, X, Joerg, F, Johnson, J, Joy, A, C Kaboth, A, Kalhor, L, C Kamaha, A, Kanezaki, K, Kar, K, Kara, M, Kato, N, Kavrigin, P, Kazama, S, W Keaveney, A, Kellerer, J, Khaitan, D, Khazov, A, Khundzakishvili, G, Khurana, I, Kilminster, B, Kleifges, M, Ko, P, Kobayashi, M, Kodroff, D, Koltmann, G, Kopec, A, Kopmann, A, Kopp, J, Korley, L, N Kornoukhov, V, V Korolkova, E, Kraus, H, M Krauss, L, Kravitz, S, Kreczko, L, A Kudryavtsev, V, Kuger, F, Kumar, J, L??pez Paredes, B, Lacascio, L, Laha, R, Laine, Q, Landsman, H, F Lang, R, A Leason, E, Lee, J, S Leonard, D, T Lesko, K, Levinson, L, Levy, C, I, Li, C Li, S, Li, T, Liang, S, S Liebenthal, C, Lin, J, Lin, Q, Lindemann, S, Lindner, M, Lindote, A, Linehan, R, H Lippincott, W, Liu, X, Liu, K, Liu, J, Loizeau, J, Lombardi, F, Long, J, I Lopes, M, Lopez Asamar, E, Lorenzon, W, Lu, C, Luitz, S, Ma, Y, N Machado, P A, Macolino, C, Maeda, T, Mahlstedt, J, A Majewski, P, Manalaysay, A, Mancuso, A, Manenti, L, Manfredini, A, L Mannino, R, Marangou, N, March-Russell, J, Marignetti, F, Marrod??n Undagoitia, T, Martens, K, Martin, R, Martinez-Soler, I, Masbou, J, Masson, D, Masson, E, Mastroianni, S, Mastronardi, M, A Matias-Lopes, J, E McCarthy, M, Mcfadden, N, Mcginness, E, N McKinsey, D, Mclaughlin, J, Mcmichael, K, Meinhardt, P, Men??ndez, J, Meng, Y, Messina, M, Midha, R, Milisavljevic, D, H Miller, E, Milosevic, B, Milutinovic, S, A Mitra, S, Miuchi, K, Mizrachi, E, Mizukoshi, K, Molinario, A, Monte, A, B Monteiro, C M, E Monzani, M, S Moore, J, Mor??, K, A Morad, J, D Morales Mendoza, J, Moriyama, S, Morrison, E, Morteau, E, Mosbacher, Y, J Mount, B, Mueller, J, J Murphy, A St, Murra, M, Naim, D, Nakamura, S, Nash, E, Navaieelavasani, N, Naylor, A, Nedlik, C, N Nelson, H, Neves, F, L Newstead, J, Ni, K, A Nikoleyczik, J, Niro, V, G Oberlack, U, Obradovic, M, Odgers, K, J O???Hare, C A, Oikonomou, P, Olcina, I, Oliver-Mallory, K, Oranday, A, Orpwood, J, Ostrovskiy, I, Ozaki, K, Paetsch, B, Pal, S, Palacio, J, J Palladino, K, Palmer, J, Panci, P, Pandurovic, M, Parlati, A, Parveen, N, J Patton, S, P????, V, Pellegrini, Q, Penning, B, Pereira, G, Peres, R, Perez-Gonzalez, Y, Perry, E, Pershing, T, Petrossian-Byrne, R, Pienaar, J, Piepke, A, Pieramico, G, Pierre, M, Piotter, M, Pizzella, V, Plante, G, Pollmann, T, Porzio, D, Qi, J, Qie, Y, Qin, J, Quevedo, F, Raj, N, Rajado Silva, M, Ramanathan, K, Ram??rez Garc??a, D, Ravanis, J, Redard-Jacot, L, Redigolo, D, Reichard, S, Reichenbacher, J, A Rhyne, C, Richards, A, Riffard, Q, C Rischbieter, G R, Rocchetti, A, L Rosenfeld, S, Rosero, R, Rupp, N, Rushton, T, Saha, S, Salucci, P, Sanchez, L, Sanchez-Lucas, P, Santone, D, F dos Santos, J M, Sarnoff, I, Sartorelli, G, R Sazzad, A B M, Scheibelhut, M, W Schnee, R, Schrank, M, Schreiner, J, Schulte, P, Schulte, D, Schulze Eissing, H, Schumann, M, Schwemberger, T, Schwenk, A, Schwetz, T, Scotto Lavina, L, R Scovell, P, Sekiya, H, Selvi, M, Semenov, E, Semeria, F, Shagin, P, Shaw, S, Shi, S, Shockley, E, A Shutt, T, Si-Ahmed, R, J Silk, J, Silva, C, C Silva, M, Simgen, H, imkovic, F, Sinev, G, Singh, R, Skulski, W, Smirnov, J, Smith, R, Solmaz, M, N Solovov, V, Sorensen, P, Soria, J, J Sparmann, T, Stancu, I, Steidl, M, Stevens, A, Stifter, K, E Strigari, L, Subotic, D, Suerfu, B, M Suliga, A, J Sumner, T, Szabo, P, Szydagis, M, Takeda, A, Takeuchi, Y, Tan, P-L, Taricco, C, C Taylor, W, J Temples, D, Terliuk, A, A Terman, P, Thers, D, Thieme, K, Th??mmler, T, R Tiedt, D, Timalsina, M, H To, W, Toennies, F, Tong, Z, Toschi, F, R Tovey, D, Tranter, J, Trask, M, C Trinchero, G, Tripathi, M, R Tronstad, D, Trotta, R, D Tsai, Y, D Tunnell, C, G Turner, W, Ueno, R, Urquijo, P, Utku, U, Vaitkus, A, Valerius, K, Vassilev, E, Vecchi, S, Velan, V, Vetter, S, C Vincent, A, Vittorio, L, Volta, G, von Krosigk, B, von Piechowski, M, Vorkapic, D, M Wagner, C E, M Wang, A, Wang, B, Wang, Y, Wang, W, J Wang, J, Wang, L-T, Wang, M, R Watson, J, Wei, Y, Weinheimer, C, Weisman, E, Weiss, M, Wenz, D, M West, S, J Whitis, T, Williams, M, J Wilson, M, Winkler, D, Wittweg, C, Wolf, J, Wolf, T, H Wolfs, F L, Woodford, S, Woodward, D, J Wright, C, S Wu, V H, Wu, P, W??stling, S, Wurm, M, Xia, Q, Xiang, X, Xing, Y, Xu, J, Xu, Z, Xu, D, Yamashita, M, Yamazaki, R, Yan, H, Yang, L, Yang, Y, Ye, J, Yeh, M, Young, I, B Yu, H, T Yu, T, Yuan, L, Zavattini, G, Zerbo, S, Zhang, Y, Zhong, M, Zhou, N, Zhou, X, Zhu, T, Zhu, Y, Zhuang, Y, P Zopounidis, J, Zuber, K, Zupan, J, Laboratoire de Physique Nucléaire et de Hautes Énergies (LPNHE (UMR_7585)), Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Laboratoire de physique subatomique et des technologies associées (SUBATECH), Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS)-IMT Atlantique (IMT Atlantique), Institut Mines-Télécom [Paris] (IMT)-Institut Mines-Télécom [Paris] (IMT)-Nantes université - UFR des Sciences et des Techniques (Nantes univ - UFR ST), Nantes Université - pôle Sciences et technologie, Nantes Université (Nantes Univ)-Nantes Université (Nantes Univ)-Nantes Université - pôle Sciences et technologie, Nantes Université (Nantes Univ)-Nantes Université (Nantes Univ), Laboratoire de l'Accélérateur Linéaire (LAL), Université Paris-Sud - Paris 11 (UP11)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), Institut Pluridisciplinaire Hubert Curien (IPHC), Université de Strasbourg (UNISTRA)-Université de Haute-Alsace (UHA) Mulhouse - Colmar (Université de Haute-Alsace (UHA))-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), AstroParticule et Cosmologie (APC (UMR_7164)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Observatoire de Paris, Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), HEP, INSPIRE, Lang, RF [0000-0001-7594-2746], Schumann, M [0000-0002-5036-1256], and Apollo - University of Cambridge Repository

Subjects
detector: technology, Nuclear and High Energy Physics, Astrophysics and Astronomy, Cosmology and Nongalactic Astrophysics (astro-ph.CO), Physics - Instrumentation and Detectors, [PHYS.HEXP] Physics [physics]/High Energy Physics - Experiment [hep-ex], [PHYS.NEXP] Physics [physics]/Nuclear Experiment [nucl-ex], Physics::Instrumentation and Detectors, 530 Physics, FOS: Physical sciences, dark matter, neutrinoless double-beta decay, neutrinos, supernova, direct detection, astroparticle physics, xenon, [PHYS.NEXP]Physics [physics]/Nuclear Experiment [nucl-ex], nucl-ex, High Energy Physics - Experiment, High Energy Physics - Experiment (hep-ex), double-beta decay: (0neutrino), [PHYS.HEXP]Physics [physics]/High Energy Physics - Experiment [hep-ex], Nuclear Physics - Experiment, [PHYS.PHYS.PHYS-INS-DET]Physics [physics]/Physics [physics]/Instrumentation and Detectors [physics.ins-det], Topical Review, Nuclear Experiment (nucl-ex), Detectors and Experimental Techniques, physics.ins-det, Nuclear Experiment, Engineering & allied operations, activity report, xenon: liquid, hep-ex, Astrophysics::Instrumentation and Methods for Astrophysics, Instrumentation and Detectors (physics.ins-det), dark matter: detector, [PHYS.PHYS.PHYS-INS-DET] Physics [physics]/Physics [physics]/Instrumentation and Detectors [physics.ins-det], astro-ph.CO, time projection chamber: xenon, High Energy Physics::Experiment, ddc:620, [PHYS.ASTR] Physics [physics]/Astrophysics [astro-ph], [PHYS.ASTR]Physics [physics]/Astrophysics [astro-ph], Particle Physics - Experiment, Astrophysics - Cosmology and Nongalactic Astrophysics
Abstract

The nature of dark matter and properties of neutrinos are among the most pressing issues in contemporary particle physics. The dual-phase xenon time-projection chamber is the leading technology to cover the available parameter space for Weakly Interacting Massive Particles (WIMPs), while featuring extensive sensitivity to many alternative dark matter candidates. These detectors can also study neutrinos through neutrinoless double-beta decay and through a variety of astrophysical sources. A next-generation xenon-based detector will therefore be a true multi-purpose observatory to significantly advance particle physics, nuclear physics, astrophysics, solar physics, and cosmology. This review article presents the science cases for such a detector., 77 pages, 40 figures, 1262 references

Published
2022

5. On the Opportunity of Causal Learning in Recommendation Systems: Foundation, Estimation, Prediction and Challenges

Author

Wu, P., Li, H., Deng, Y., Hu, W., Dai, Q., Dong, Z., Sun, J., Zhang, R., and Xiaohua Zhou

Subjects
FOS: Computer and information sciences, Information Retrieval (cs.IR), Computer Science - Information Retrieval
Abstract

Recently, recommender system (RS) based on causal inference has gained much attention in the industrial community, as well as the states of the art performance in many prediction and debiasing tasks. Nevertheless, a unified causal analysis framework has not been established yet. Many causal-based prediction and debiasing studies rarely discuss the causal interpretation of various biases and the rationality of the corresponding causal assumptions. In this paper, we first provide a formal causal analysis framework to survey and unify the existing causal-inspired recommendation methods, which can accommodate different scenarios in RS. Then we propose a new taxonomy and give formal causal definitions of various biases in RS from the perspective of violating the assumptions adopted in causal analysis. Finally, we formalize many debiasing and prediction tasks in RS, and summarize the statistical and machine learning-based causal estimation methods, expecting to provide new research opportunities and perspectives to the causal RS community.

Published
2022

6. Seroepidemiology of enterovirus A71 infection in prospective cohort studies of children in southern China, 2013-2018

Author

Yang, J, Liao, Q, Luo, K, Liu, F, Zhou, Y, Zou, G, Huang, W, Yu, S, Wei, X, Zhou, J, Dai, B, Qiu, Q, Altmeyer, R, Hu, H, Paireau, J, Luo, L, Gao, L, Nikolay, B, Hu, S, Xing, W, Wu, P, van Doorn, HR, Horby, PW, Simmonds, P, Leung, GM, Cowling, BJ, Cauchemez, S, Yu, H, Fudan University [Shanghai], Chinese Center for Disease Control and Prevention, Hunan provincial center for disease control and prevention, Institut Pasteur de Shanghai, Académie des Sciences de Chine - Chinese Academy of Sciences (IPS-CAS), Réseau International des Instituts Pasteur (RIIP), Direction des maladies infectieuses - Infectious Diseases Division [Saint-Maurice], Santé publique France - French National Public Health Agency [Saint-Maurice, France], Modélisation mathématique des maladies infectieuses - Mathematical modelling of Infectious Diseases, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Shandong First Medical University, Shandong Academy of Medical Sciences, The University of Hong Kong (HKU), Oxford University Clinical Research Unit [Ho Chi Minh City] (OUCRU), University of Oxford, ANR-10-LABX-0062,IBEID,Integrative Biology of Emerging Infectious Diseases(2010), and ANR-16-CONV-0005,INCEPTION,Institut Convergences pour l'étude de l'Emergence des Pathologies au Travers des Individus et des populatiONs(2016)

Subjects
China, Multidisciplinary, Infant, Newborn, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology, Enterovirus A, Human, Seroepidemiologic Studies, Child, Preschool, Enterovirus Infections, Humans, [SDV.SPEE]Life Sciences [q-bio]/Santé publique et épidémiologie, Prospective Studies, Child, Hand, Foot and Mouth Disease, Antigens, Viral, Enterovirus
Abstract

Enterovirus A71 (EV-A71)–related hand, foot, and mouth disease (HFMD) imposes a substantial clinical burden in the Asia Pacific region. To inform policy on the introduction of the EV-A71 vaccine into the National Immunization Programme, we investigated the seroepidemiological characteristics of EV-A71 in two prospective cohorts of children in southern China conducted between 2013 and 2018. Our results show that maternal antibody titres declined rapidly in neonates, with over half becoming susceptible to EV-A71 at 1 month of age. Between 6 months and 2 years of age, over 80% of study participants were susceptible, while one third remained susceptible at 5 years old. The highest incidence of EV-A71 infections was observed in children aged 5-6 months. Our findings support EV-A71 vaccination before 6 months for birth cohorts in southern China, potentially with a one-time catch-up vaccination for children 6 months-5 years old. More regionally representative longitudinal seroepidemiological studies are needed to further validate these findings.

Published
2022

7. Identification of Genes During the Reprogramming of Fibroblast using Bioinformatics Analysis

Author

Sai X, Guo H, Huang H, Tang X, Wu P, Nasser Mi, and Zhu P

Subjects
medicine.anatomical_structure, Bioinformatics analysis, medicine, Identification (biology), sense organs, Computational biology, Biology, Fibroblast, Reprogramming, Gene
Abstract

Bioinformatics method was used to screen Human induced pluripotent stem cells reprogrammed by Human Fibroblasts (FBs). The reprogramming efficiency was explored by difference expressed genes (DEGs) before and after the expression of hiPSCs. Likewise, microarray datasets GSE34309, GSE43996, and GSE56805 datasets were downloaded from Gene Expression Omnibus (GEO) and GEO2R to screen the differentially expressed DEGs. Further, Gene Ontology (GO) and KEGG (Kyoto Encyclopedia of Genes and Genomes (KEGG) signaling pathways were analyzed by David database. Likewise, to explore the correlation between DEGs, and the STRING database software was used to construct the protein-protein internet (PPI), and the Cytoscape_v3.7.2 Cytohubba plug-in was used to screen out the core genes. A total of 622 DEGs were identified, including 344 up regulated genes and 278 down-regulated genes. DEGs were mainly concentrated in the cell cycle and PI3K-Akt signaling pathway. Among the ten core genes screened, CDK1, IL6, EGFR, FN1, CDH1, SOX2, BRCA1, EZH2, CD44, and CCNB1 were most significant in the reprogramming of FBs into iPSCs. Regardless underline the differential of those gene expression profiles and regulatory network during FBs reprogramming could provide a theoretical basis for efficient reprogramming.

Published
2021

8. Communication Objectives Model (COM): A Taxonomy of Face-to-Face Communication Objectives to Inform Tele-Presence Technology Adoption

Author

Wu P, Brett W. Israelsen, Kaitlyn M. Ouverson, James H. Oliver, Jacklin Stonewall, Stephen B. Gilbert, Emily Oldham, Charles Peasley, and Rachel E. Dianiska

Subjects
Knowledge management, Computer science, business.industry, Taxonomy (general), Conflict management, Tele presence, Computer-mediated communication, business, Face-to-face interaction, Collective efficacy
Abstract

Computer-mediated communication (CMC) has become the new normal in the era of pandemic-induced physical distancing. CMC has dramatically reduced business travel and daily commuting for knowledge workers able to work from home, which in turn reduces carbon emissions and energy expenditure. CMC offers a different communication experience compared to in-person interactions, and its impact on the success of communication is complex. Here, we report the Communication Objectives Model (COM), a framework developed to: a) understand differences in the performance of communication objectives between CMC and face-to-face interactions, and b) guide future research on measurement of such communication objectives. Given that effective communication is essentially the result of a team activity, the psychosocial constructs that comprise our framework are derived from team research across multiple domains (e.g., social psychology, human-computer interaction, and computer supported cooperative work). Constructs of interest include trust, rapport, engagement, conflict management, collective efficacy, mental models, and shared situation awareness. For each construct, we provide a definition, empirical evidence, and theoretical bases for its observable behavioral markers, as well as potential measurement methods and analytical techniques. The contributions of this research include a framework for characterizing differences between different communication media, a hypothetical implementation demonstrating how the framework can inform the decision to travel in-person versus to deploy CMC (i.e., a travel replacement threshold), and an inventory of tools and techniques that can be used to measure and assess the psychosocial constructs involved in CMC.

Published
2021

9. Twisted oxide lateral homostructures with conjunction tunability

Author

You K, Zhong Q, Wei C, Chen Y, Zheng J, Huang R, Jan Chi Yang, Chiu Y, Chang C, Liou Y, Wu P, Hu J, Chang Yang Kuo, Ho S, Chiu C, and Chun-Gang Duan

Subjects
chemistry.chemical_compound, Materials science, chemistry, business.industry, Oxide, Optoelectronics, business, Conjunction (grammar)
Abstract

Epitaxial growth is of significant importance over the past decades, given it has been the key process of modern technology for delivering high-quality thin films. For conventional heteroepitaxy, the selection of proper single crystal substrates not only facilitates the integration of different materials but also fulfills interface and strain engineering upon a wide spectrum of functionalities. Nevertheless, the lattice structures, regularity and crystalline orientation are determined once a specific substrate is chosen. In this work, we reveal the growth of twisted oxide lateral homostructures with multiple conjunction degree of freedom. The twisted lateral homostructures with atomically sharp interfaces can be composed of epitaxial “blocks” with different crystalline orientations, ferroic orders and phases. We further demonstrate that this approach is universal for fabricating various complex systems. Our results establish an efficient pathway towards twisted lateral homostructures, allowing epitaxial films to be arbitrarily tailored at designated positions with unbounded in-plane conjunction tunability.

Published
2021

11. Pooling Samples as an Efficient Approach to Regular SARS-CoV-2 Testing in Residential Care Facilities

Author

BJ Cowling, Wu P, and McMenamin M

Subjects
medicine.medical_specialty, Government, Isolation (health care), Family medicine, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Pooling, Declaration, medicine, Business, Commission, Institutional review board, Decision analysis
Abstract

Background: Residents of care facilities for the elderly have accounted for a large proportion of all deaths due to COVID-19 globally. In Hong Kong, care home staff are required to undergo testing for SARS-CoV-2 every two weeks, regardless of symptoms. We aimed to optimize testing strategies in order to improve on existing screening programs. Methods: We estimated the reduced sensitivity of pooled PCR testing and used a decision analysis to determine the expected number of tests required. We assumed transmission occurred according to a time-varying Poisson process and that the time from infection to isolation followed a time-varying geometric distribution. We estimated the cumulative number of cases expected under syndromic surveillance, testing without pooling and pooled testing with pool sizes 2, 5 and 10 using an age of infection model. Findings: Assuming a prevalence of 0.02%, pooling 10 samples and conducting testing every two days instead of testing without pooling every 14 days could reduce the average size of an outbreak from between 2 and 14 cases (median 7 cases) to between 1 and 6 cases (median 2 cases). Pooling to allow for daily testing further reduced the average size of an outbreak from 4 cases to 1 case compared to weekly testing. Interpretation: Health authorities can improve on existing screening programs by employing pooled testing procedures and testing individuals more frequently to make the most use of available testing resources. Funding Information: This project was supported by a commissioned grant from the Health and Medical Research Fund, Food and Health Bureau, Government of the Hong Kong Special Administrative Region, and the Theme-based Research Scheme (Project No. T11-712/19-N) of the Research Grants Council of the Hong Kong SAR Government. Declaration of Interests: BJC consults for Roche, GSK, Moderna, AstraZeneca and Sanofi Pasteur and is supported by the AIR@innoHK program of the Innovation and Technology Commission of the Hong Kong SAR Government. The authors report no other potential conflicts of interest. Ethics Approval Statement: The study was approved by the Institutional Review Board of the University of Hong Kong.

Published
2021

12. Controlling Cellular Arrangements via Stretched Bioprinting

Author

Longbin Huang, Tao Liang, Deming Jiang, Hsia Kj, Chengyang Han, Minliang Liu, Ping Wang, Wu P, Chunlian Qin, and Chuanjiang He

Subjects
Computer science, Common method, Process (anatomy), Biomedical engineering
Abstract

Bioprinting is a common method to replicate geometrical architecture of native tissues. However, it usually fails to modulate cellular arrangements, which is critical for the tissue’s functionality. To our knowledge, no method has successfully addressed this challenge. Here, we report a method of controlling cellular orientation during the bioprinting process by integrating a stretch process into a modified bioprinting frame. We demonstrate that the cellular orientation is a result of cells’ sensing and responding to the tensile stress, instead of shear stress or topographical patterns. Moreover, our method shows a potent capability to induce myoblast differentiation, fusion and maturation without the presence of differentiation medium. As a potential clinical application, we demonstrate that aligned myofibers directly printed onto injured muscle in vivo, can not only repair the structure of damaged tissue, but also recover the muscle functionalities effectively. This study shows that the new method can produce tissues with precise control of cellular arrangements and more clinically viable functionalities.Significance StatementDue to no method could reproduce the exact cellular arrangements of native tissues in engineered tissues, tissue engineering facing difficult in fabricating 3D tissues that possess desirable biological and mechanical functionalities for biomedical applications. For the first time, we report a method of controlling cellular orientation during 3D bio-printing process. This method can be used to produce engineered tissues with controlled cellular arrangement with several different cell types. Moreover, this method shows a potent capability of fabricating fully mature and aligned myofibers in vitro in the absence of differentiation medium. As potential clinical applications, with this method, engineered tissues could be directly printed in vivo with high efficacy of tissue repair and function recovery.

Published
2020

14. The role of procalcitonin in early differential diagnosis of suspected children with COVID-19

Author

Peng D, Liu Z, Jie Zhang, Wu P, and Yun Xu

Subjects
medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), animal diseases, viruses, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), chemical and pharmacologic phenomena, Asymptomatic, Procalcitonin, Immune system, Internal medicine, Epidemiology, medicine, Respiratory system, Pathogen, business.industry, Respiratory infection, General Medicine, biochemical phenomena, metabolism, and nutrition, medicine.disease, Pneumonia, Viral pneumonia, Immunology, Coinfection, bacteria, Family cluster, Differential diagnosis, medicine.symptom, business
Abstract

BackgroundWe aimed to identify clinical features of coronavirus disease 2019 (COVID-19) in children and evaluate the role of procalcitonin in early differential diagnosis.MethodsA retrospective analysis was performed on all suspected pediatric cases.Results39 (50.6%) of 77 suspected cases were comfirmed, 4 (5.2%) of them had viral coinfection. Compared with non-COVID-19 group (n=33), COVID-19 confirmed group (n=39) had fewer fever(OR[95% CI]0.467[0.314-0.694]; P=.000) and symptoms of acute respiratory infection (0.533[0.36–0.788]; P=.001), more asymptomatic (13.568[1.895-96.729]; P=.000), and more family cluster infections (5.077[2.224-11.591]; P=.000), while computed tomography had more positive findings of viral pneumonia (1.822[1.143-2.906]; P=.008). Age (6.9[3.6-10.5] vs 5[2.1-7.6]; P=. 088) and gender were statistically insignificant. Procalcitonin (0.05[0.029-0.076] vs 0.103[0.053-0.21]; P= 000) of COVID-19 alone group (n=35) was significantly reduced. While compared with coinfection group (n=4), procalcitonin (0.05[0.029-0.076] vs 0.144[0.109-2.26]; P=.010) was also reduced. The area under curve of model is 0.834 ([95% CI][0.741-0.926]; P=.000). Procalcitonin as a differential indicator of COVID-19 alone, its area under curve is 0.809 ([0.710-0.909]; P=.000). The optimal cut-off value is 0.1 ng/mL, the sensitivity, specificity, positive and negative predictive value of differentiating are 65.9%, 78.6%, 82.9%, and 59.2%, respectively.ConclusionsAsymptoms or mild symptoms, positive computed tomography findings and family cluster infection are the main clinical features of COVID-19 in children. With good performance, procalcitonin can provide an important basis for differentiating COVID-19 alone and other viral infection or viral coinfection.

Published
2020

15. Comparison of transcriptomic and proteomic analyses to construct a model for the promotion of starch synthesis by ABA in Euryale ferox Salisb. seeds

Author

Liu X, Li X, Wu P, Li L, Zhang Y, and Xu X

Subjects
Starch synthesis, Transcriptome, Promotion (rank), media_common.quotation_subject, Botany, Biology, biology.organism_classification, Euryale ferox, media_common
Abstract

Background: Euryale ferox Salisb. is an annual aquatic herb and the only species belonging to the genus Euryale in the Nymphaeaceae family. E. ferox seeds are used in medicine and diets. Starch is the main factor affecting E. ferox seed quality, but its regulatory mechanism has not been elucidated. Results: Herein, four time points of seed development, including after flowering T1 (10 days), T2 (20 days), T3 (30 days) and T4 (40 days), were investigated by using RNA-Seq and iTRAQ technology. Using weighted gene co-expression network analyses (WGCNAs), co-expressed genes and hub genes were identified for each module. Of particular importance are the discoveries of specific modules for seed starch during the seed developmental stages. The candidate regulators of seed starch are involved in the hormonal signaling pathways. Three ABA signaling receptor kinases, EfPYR1, EfSnRK2.1 and EfSnRK2.2, were identified as hub genes functioning in starch synthesis during the seed maturation process. The changes in expression pattern, ABA and starch content also indicated that ABA is positively correlated with starch. Conclusions: Together, these results indicate that E. ferox seed accumulation of starch is promoted by ABA, providing new insights into the regulatory mechanism of starch synthesis in E. ferox seeds.

Published
2020

16. Studying the mix design and investigating the photocatalytic performance of pervious concrete containing TiO2-Soaked recycled aggregates

Author

Xu, Y, Jin, R, Hu, L, Li, B, Chen, W, Shen, J, Wu, P, and Fang, J

Subjects
Pervious concreteMechanical properties, Photocatalytic effects, Recycled aggregate, Titanium dioxide, Recycled aggregate concrete
Abstract

Demolished concrete, as one main form of construction and demolition wastes, has been widely studied of being utilized as recycled aggregates (RAs) in new concrete production. However, existing studies of applying RAs have been limited to the mechanical and durability issues of cementitious composites containing RAs.

Published
2020

17. Epigenetic Silencing of CDR1as Drives IGF2BP3-Mediated Melanoma Invasion and Metastasis

Author

Hanniford D, Ulloa-Morales A, Karz A, Berzoti-Coelho M, Moubarak R, Sanchez-Sendra B, Kloetgen A, Davalos V, Imig J, Wu P, Vasudevaraja V, Argibay D, Lilja K, Tabaglio T, Monteagudo C, Guccione E, Tsirigos A, Osman I, Aifantis I, and Hernando E

Abstract

Metastasis is the primary cause of death of cancer patients. Dissecting mechanisms governing metastatic spread may uncover important tumor biology and/or yield promising therapeutic insights. Here, we investigated the role of circular RNAs (circRNA) in metastasis, using melanoma as a model aggressive tumor. We identified silencing of cerebellar degeneration-related 1 antisense (CDR1as), a regulator of miR-7, as a hallmark of melanoma progression. CDR1as depletion results from epigenetic silencing of LINC00632, its originating long non-coding RNA (lncRNA) and promotes invasion in vitro and metastasis in vivo through a miR-7-independent, IGF2BP3-mediated mechanism. Moreover, CDR1as levels reflect cellular states associated with distinct therapeutic responses. Our study reveals functional, prognostic, and predictive roles for CDR1as and expose circRNAs as key players in metastasis.

Published
2020

18. Genomic Epidemiology of SARS-CoV-2 in the United Arab Emirates Reveals Novel Insights into the Virus Mutation, Co-Infection and Host-Dependent RNA Editing

Author

Jun Wang, Xavier Anton, Xin Meng, Pauline Ogrodzki, Kusuma, Lin Lin, Kaabi Nama, Javier Quilez, Shanshan Liu, Xun Xu, Rong Liu, Sally Mahmoud, Junhua Li, Walid Abbas Zaher, Huang X, Xin Jin, Xiao P, Zhaorong Yuan, Liu W, Budoor Alqarni, Huanming Yang, Wenjun He, Hanif Khalak, Liang K, Ashish Koshy, Wu P, Liu P, Nan Qiao, Ma T, Fang Chen, Stephen S. Francis, Mohammed Saifuddin Fasihuddin, Denghui Liu, and Hosani Fia

Subjects
Genetics, Genetic diversity, education.field_of_study, RNA editing, Transmission (medicine), Genetic variation, Pandemic, Population, Subclade, Biology, education, Viral load
Abstract

Background: The United Arab Emirates is a major business hub with substantial amount of international travel. Like many other countries, it was greatly affected by the COVID-19 pandemic since late January 2020, with recurring waves of infection. This study aimed at combining genomic and epidemiological data to unravel the source of SARS-CoV-2 introduction, transmission and evolution in the country. Methods: We performed meta-transcriptomic sequencing of 1,067 nasopharyngeal swab samples collected from qRT-PCR positive COVID-19 patients in Abu Dhabi, UAE, between May 9th and June 29th 2020. We investigated the genetic diversity and transmission dynamics of the viral population and analyzed the infection and transmission potential of novel genomic clusters. Within-host SARS-CoV-2 genetic variation was analyzed to determine the occurrence and prevalence of multiple infections. Finally, we evaluated innate host responses during the prolonged period of local infection. Findings: All globally known SARS-CoV-2 clades were identified within the UAE sequenced strains, with a higher occurrence of European and East Asian clades. We defined 5 subclades based on 11 unique genetic variants within the UAE strains, which were associated with higher viral loads (p

Published
2020

19. Effect of hydrolyzed infant formula vs conventional formula on risk of type 1 diabetes the TRIGR randomized clinical trial

Author

Knip M., Akerblom H. K., Altaji E., Becker D., Bruining J., Castano L., Danne T., De Beaufort C., Dosch H. -M., Dupre J., Fraser W. D., Howard N., Ilonen J., Konrad D., Kordonouri O., Krischer J. P., Lawson M. L., Ludvigsson J., Madacsy L., Mahon J. L., Ormisson A., Palmer J. P., Pozzilli P., Savilahti E., Serrano-Rios M., Songini M., Taback S., Vaarala O., White N. H., Virtanen S. M., Wasikowa R., Mandrup-Poulsen T., Arjas E., Lernmark A., Laara E., Schmidt B., Hyytinen M., Koski K., Koski M., Merentie K., Pajakkala E., Reunanen A., Salonen M., Terhonen T., Virkkunen S., Cuthbertson D., Gainer B., Hadley D., Malloy J., Nallamshetty L., Shanker L., Bradley B., Lough G., Fraser W., Sermer M., Taback S. P., Franciscus M., Nucci A., Palmer J., Alahuhta K., Barlund S., Korhonen T., Kovanen L., Lehtonen E., Niinisto S., Pekkala M., Sorkio S., Toivanen L., Vahatalo L., Uusitalo U., Ohman T., Bongiorno R., Catteau J., Fraser G., Lloyd M., Crock P., Giles M., Siech K., See D. W., Brown C., Craig M., Johnston A., Bere L. J., Clarson C. L., Jenner M., McManus R., Renato N., Lovell M., Higo D., Kent N., Kwan J., Marshall C., Metzger D., Chanoine J. -P., Stewart L., Thompson D., Edwards A., Lange I., Mercer J., Pacaud D., Josephine H., Schwarz W., Stephure D. K., Boer J., Chatur T., Chick C., Couch B., Demianczuk N., Girgis R., Marks S., Ryan E., Thompson M., Dean H. J., Grant L., Hamelin K., LaForte J., Murphy L., Catte D., Schneider C., Sellers E. A. C., Woo V., Boland A., Clark H. D., Cooper T., Gruslin A., Karovitch A., Keely E., Malcolm J. C., Sauro V., Tawagi G. F., Andrighetti S., Arnold G., Barrett J., Blumer I., Daneman D., Donat D., Ehrlich R., Feig D., Gottesman I., Gysler M., Karkanis S., Kenshole A., Knight B., Lackie E., Lewis V., Martin M. J., Maxwell C., Oliver G., Panchum P., Shilletto N., Simone A., Skidmore M., Turrini T., Wong S., Allen C., Belanger L., Bouchard I., Ferland S., Frenette L., Garrido-Russo M., Leblanc M., Imbeault J., Morin V., Olivier G., Weisnagell J., Costain G., Dornan J., Heath K., MacSween M. -C., McGibbon A., Ramsay C., Sanderson F., Sanderson S., Benabdesselam L., Gonthier M., Huot C., Thibeault M., Laforte D., Legault L., Perron P., Armson A., Canning P., Cummings E. A., Ivanko V., McLeod L., Mokashi A., Scott K., Bridger T., Crane J., Crummell C., Curtis J. C., Dawson C., Joyce C., Newhook L. A., Newman S., Druken E., Begum-Hasan J., Breen A., Houlden R., Woods M., Carrson G., Kelly S., Martel M. J., Penner M., Sankaran K., Hardy-Brown K., King N., White R. A., Park M., Popkin J., Robson L., Coles K., Al Taji E., Cerna M., Cerny M., Francova H., Hainerova I., Kothankova H., Koukalova R., Krakorova V., Mendlova P., Sitova R., Stechova K., Vavrinec J., Vosahlo J., Zlatohlavkova B., Brazdova L., Faksova P., Gregorova D., Kantor L., Malkova K., Venhacova J., Venhacova P., Cipra A., Skvor J., Budejovice C., Tomsikova Z., Botkova-Krauseova H., Mockova A., Paterova P., Gogelova P., Kandrnalova J., Einberg U., Jakovlev U., Posiadlo S., Rannaste E., Raukas R., Riikjarv M. -A., Valla K., Astover V., Kirss A., Retpap J., Taht E., Tillmann V., Vahtra S., Heikkila M., Hirvasniemi M., Luopajarvi K., Johansson S., Kleemola P., Laukkanen E., Parkkola A., Pigg H. -M., Puttonen H., Renlund M., Salonen K., Suomalainen H., Tenkula T., Teramo K., Jarvenpaa A. -L., Hamalainen A. -M., Jussila R., Kiiveri S., Haavisto H., Holopainen S., Kupiainen H., Leeve T., Lumme K., Nironen T., Tenhola S., Tiilikainen T., Keinonen H., Lautala P., Salonen P., Vesanto M., Aspholm A. S., Asunta P., Ikavalko H., Jason E., Jaminki S., Kekki P., Koskinen M., Lehtimaki S., Lahde J., Makela M., Peltoniemi S., Poutiainen L., Ranta K., Salonsaari T., Sarviharju-Tujula S. -L., Selvenius J., Siljander H., Haanpaa P. -L., Holm C., Juutilainen A., Jarvelainen V., Kangaskolkka-Keskilohko A. -M., Laino E., Marjamaki L., Suominen E., Ylitalo S., Hokkanen M., Lounamaa R., Matikainen M., Nuuja A., Paalanen I., Puupponen A. R., Salo-Edwards H., Alanne S., Kultti T., Linjama H., Muhonen K., Vaaraniemi M., Talvitie T., Backman M., Hanhijarvi R., Koivula P., Lindstrom K., Martikainen A., Nurmi P., Bjork A., Huopio H., Komulainen J., Lehtomaki S., Muikku E., Pesola J., Sankilampi U., Arkkola T., Hekkala A., Jurvakainen S., Koivikko M. -L., Kahonen M., Leinonen E., Mykkanen T., Pohjola H., Riikonen K., Niittyvuopio A., Stenius A., Tapanainen P., Veijola R., Alar A., Jovio S., Korpela P., Makinen E., Hietanen L., Kivisto J., Kaar M. -L., Lehtimaki P., Mustila T., Popov E., Saatela S., Taittonen L., Ahtiainen K., Laaksonen N., Luoto M., Viitala J., Virransalo R., Nykanen P., Paajanen S., Parkkinen S., Pyrhonen H., Sarkka T., Aschemeier B., Bektas S., Biester T., Datz N., Deiss D., Fath M., Lupke K., Muller B., Nestoris C., Rothes S., Sadeghian E., Semler K., Arato A., Krikovszky D., Nobilis A., Szenasi J., Benevento D., Anguissola G. B., Biagioni M., Bizzarri C., Cherubini V., Ferrito L., Giordano C., Giorgetti C., Khazrai Y. M., Kyanvash S., Maddaloni E., Napoli A., Piergiovanni F., Pitocco D., Suraci T., Tabacco G., Valente L., Visalli N., Carboni M. B., Cavallo R., Cau V., Isola C., Ledda A., Loddo M., Mannu C., Pettinau M., Pisano S., Porceddu M., Putzu C., Rita A., Peters D., Schierloh U., Bisschoff M., Blonk L., Lappenschaar T., Manai B., Seesink M., Sperling-Conrad M., Verhagen M., Zoethout J. A., Basiak A., Chalas M., Chesiak M., Gramza A., Iwankiewicz J., Sieradzan E., Wikiera B., Ciechanowska M., Dziatkowiak H., Futona B., Gorska A., Glowacka-Wony M., Kaim I., Klich B., Starzyk J., Wolanin M., Tokarska L., Chucherco D., Deja G., Firek-Pedras M., Jarosz-Chobot P., Kalina M., Kutrowska-Adamusiak K., Minkina-Pedras M., Muchaka-Bianga M., Bodalski J., Mlynarski W., Szadkowska A., Cieslak A., Cypryk K., Dziatosz K., Jastzebowska J., Krysiak A., Szymanska U., Wilcznski J., Zawodniak-Szalapska M., Aguay A., Bilbao J. R., Chueca M., Cortazar A., Echarte G., Frutos T. G., Jimenez P., Martul P., Moreno A., Oyarzabal M., Rica I., Salgado Y., Martinez-Larrad M. T., Hawkins F. G., Hernandez R., Herranz L., Pallardo L. F., Deibarra L. S., Fernandez B. H., Luis J. L., Ortiz-Quintana L., Recarte P. P., Arnau D. R., Aronsson L., Boden S., Fredriksson J., Isacsson E., Johansson I., Karlsson E., Lock C., Sandstrom A. -M., Konefal M. S., Andreasson C., Dahlstrom U., Hanas R., Lundqvist K., Windell L., Jansson I., Karlsson A. -K., Lindbladh B., Odenman I., Pettersson C., Sundberg F., Sundqvist M., Aronsson S., Bellman I., Bengtsson A. -B., Lyden G. -B., Nilsson N. -O., Soderblom M., Unt C., Augustsson M., Bengtsson M., Fors H., Helmrich A., Johansson T. O., Andersson A. -C., Boiard-Stomlid A., Hellgren G., Kallsholm H., Lindqvist J., Nilsson M., Nordwall M., Stromstedt C., Ahsberg C., Lindh A., Lindhe C., Samuelsson C., Wiik A., Edenwall H., Ljumgcrantz M., Persson I. -B., Strigard E., Svensson B. -L., Aman J., Breivik G. -E., Detlofsson I. -L., Kroon M., Sarnblad S., Johansson C., Ilvered R., Lundberg A., Akesson K., Beccarelli A., Gadient M., Rappold-Amrein C., Schoenle E., Daftary A., Damagro-Elias M. E., Gilmour C., Klein M. B., Lain C., Salerno D., Smith M. E., Vats K., Pfaff D. J., Malone P., Mansfield P., Munns M., Nickel K., Pompilio K., Siemion W., Taculad R., Van Horn K., Zdanadewic M., Chambliss C., Jones J., Sadler M., Tanner-Blasiar M., Bell C., Camper N., Devaskar S., Devaskar U., Horowitz H., Rogers L., Shannahan R., Silk K., Bermudez Z., Colon R., Frazer T., Martinez-Nieves B., Torres J., Vega J., Chan M., Cook S., Goland R., Greenberg E., Jules N., Montes J., Nelson M., Parra-Valencia Z., Schachner H., Softness B., Kiviniemi M., Suomenin R., Alexander A., Hyrckowian E., Nichol L., Trucco M., Karjalainen E., Louhio T., Sarnesto A., Valtonen E., Davydova B., Helander S., Hamalainen J., Harkonen T., Joutsjoki L., Kararic M., Latva-Koivisto M., Lonn E., Nurmi T., Ollila I., Rinkinen J., Ronkainen M., Tukiainen H., Cederlof A., Kiikeri M., Tsupari S., Cheng R., Bryant K., Chan Y., Maezawa Y., Paltser G., Rasavi R., Tsui H., Winer S., Wu P., Yantha J., Pediatrics, Knip M., Akerblom H.K., Altaji E., Becker D., Bruining J., Castano L., Danne T., De Beaufort C., Dosch H.-M., Dupre J., Fraser W.D., Howard N., Ilonen J., Konrad D., Kordonouri O., Krischer J.P., Lawson M.L., Ludvigsson J., Madacsy L., Mahon J.L., Ormisson A., Palmer J.P., Pozzilli P., Savilahti E., Serrano-Rios M., Songini M., Taback S., Vaarala O., White N.H., Virtanen S.M., Wasikowa R., Mandrup-Poulsen T., Arjas E., Lernmark A., Laara E., Schmidt B., Hyytinen M., Koski K., Koski M., Merentie K., Pajakkala E., Reunanen A., Salonen M., Terhonen T., Virkkunen S., Cuthbertson D., Gainer B., Hadley D., Malloy J., Nallamshetty L., Shanker L., Bradley B., Lough G., Fraser W., Sermer M., Taback S.P., Franciscus M., Nucci A., Palmer J., Alahuhta K., Barlund S., Korhonen T., Kovanen L., Lehtonen E., Niinisto S., Pekkala M., Sorkio S., Toivanen L., Vahatalo L., Uusitalo U., Ohman T., Bongiorno R., Catteau J., Fraser G., Lloyd M., Crock P., Giles M., Siech K., See D.W., Brown C., Craig M., Johnston A., Bere L.J., Clarson C.L., Jenner M., McManus R., Renato N., Lovell M., Higo D., Kent N., Kwan J., Marshall C., Metzger D., Chanoine J.-P., Stewart L., Thompson D., Edwards A., Lange I., Mercer J., Pacaud D., Josephine H., Schwarz W., Stephure D.K., Boer J., Chatur T., Chick C., Couch B., Demianczuk N., Girgis R., Marks S., Ryan E., Thompson M., Dean H.J., Grant L., Hamelin K., LaForte J., Murphy L., Catte D., Schneider C., Sellers E.A.C., Woo V., Boland A., Clark H.D., Cooper T., Gruslin A., Karovitch A., Keely E., Malcolm J.C., Sauro V., Tawagi G.F., Andrighetti S., Arnold G., Barrett J., Blumer I., Daneman D., Donat D., Ehrlich R., Feig D., Gottesman I., Gysler M., Karkanis S., Kenshole A., Knight B., Lackie E., Lewis V., Martin M.J., Maxwell C., Oliver G., Panchum P., Shilletto N., Simone A., Skidmore M., Turrini T., Wong S., Allen C., Belanger L., Bouchard I., Ferland S., Frenette L., Garrido-Russo M., Leblanc M., Imbeault J., Morin V., Olivier G., Weisnagell J., Costain G., Dornan J., Heath K., MacSween M.-C., McGibbon A., Ramsay C., Sanderson F., Sanderson S., Benabdesselam L., Gonthier M., Huot C., Thibeault M., Laforte D., Legault L., Perron P., Armson A., Canning P., Cummings E.A., Ivanko V., McLeod L., Mokashi A., Scott K., Bridger T., Crane J., Crummell C., Curtis J.C., Dawson C., Joyce C., Newhook L.A., Newman S., Druken E., Begum-Hasan J., Breen A., Houlden R., Woods M., Carrson G., Kelly S., Martel M.J., Penner M., Sankaran K., Hardy-Brown K., King N., White R.A., Park M., Popkin J., Robson L., Coles K., Al Taji E., Cerna M., Cerny M., Francova H., Hainerova I., Kothankova H., Koukalova R., Krakorova V., Mendlova P., Sitova R., Stechova K., Vavrinec J., Vosahlo J., Zlatohlavkova B., Brazdova L., Faksova P., Gregorova D., Kantor L., Malkova K., Venhacova J., Venhacova P., Cipra A., Skvor J., Budejovice C., Tomsikova Z., Botkova-Krauseova H., Mockova A., Paterova P., Gogelova P., Kandrnalova J., Einberg U., Jakovlev U., Posiadlo S., Rannaste E., Raukas R., Riikjarv M.-A., Valla K., Astover V., Kirss A., Retpap J., Taht E., Tillmann V., Vahtra S., Heikkila M., Hirvasniemi M., Luopajarvi K., Johansson S., Kleemola P., Laukkanen E., Parkkola A., Pigg H.-M., Puttonen H., Renlund M., Salonen K., Suomalainen H., Tenkula T., Teramo K., Jarvenpaa A.-L., Hamalainen A.-M., Jussila R., Kiiveri S., Haavisto H., Holopainen S., Kupiainen H., Leeve T., Lumme K., Nironen T., Tenhola S., Tiilikainen T., Keinonen H., Lautala P., Salonen P., Vesanto M., Aspholm A.S., Asunta P., Ikavalko H., Jason E., Jaminki S., Kekki P., Koskinen M., Lehtimaki S., Lahde J., Makela M., Peltoniemi S., Poutiainen L., Ranta K., Salonsaari T., Sarviharju-Tujula S.-L., Selvenius J., Siljander H., Haanpaa P.-L., Holm C., Juutilainen A., Jarvelainen V., Kangaskolkka-Keskilohko A.-M., Laino E., Marjamaki L., Suominen E., Ylitalo S., Hokkanen M., Lounamaa R., Matikainen M., Nuuja A., Paalanen I., Puupponen A.R., Salo-Edwards H., Alanne S., Kultti T., Linjama H., Muhonen K., Vaaraniemi M., Talvitie T., Backman M., Hanhijarvi R., Koivula P., Lindstrom K., Martikainen A., Nurmi P., Bjork A., Huopio H., Komulainen J., Lehtomaki S., Muikku E., Pesola J., Sankilampi U., Arkkola T., Hekkala A., Jurvakainen S., Koivikko M.-L., Kahonen M., Leinonen E., Mykkanen T., Pohjola H., Riikonen K., Niittyvuopio A., Stenius A., Tapanainen P., Veijola R., Alar A., Jovio S., Korpela P., Makinen E., Hietanen L., Kivisto J., Kaar M.-L., Lehtimaki P., Mustila T., Popov E., Saatela S., Taittonen L., Ahtiainen K., Laaksonen N., Luoto M., Viitala J., Virransalo R., Nykanen P., Paajanen S., Parkkinen S., Pyrhonen H., Sarkka T., Aschemeier B., Bektas S., Biester T., Datz N., Deiss D., Fath M., Lupke K., Muller B., Nestoris C., Rothes S., Sadeghian E., Semler K., Arato A., Krikovszky D., Nobilis A., Szenasi J., Benevento D., Anguissola G.B., Biagioni M., Bizzarri C., Cherubini V., Ferrito L., Giordano C., Giorgetti C., Khazrai Y.M., Kyanvash S., Maddaloni E., Napoli A., Piergiovanni F., Pitocco D., Suraci T., Tabacco G., Valente L., Visalli N., Carboni M.B., Cavallo R., Cau V., Isola C., Ledda A., Loddo M., Mannu C., Pettinau M., Pisano S., Porceddu M., Putzu C., Rita A., Peters D., Schierloh U., Bisschoff M., Blonk L., Lappenschaar T., Manai B., Seesink M., Sperling-Conrad M., Verhagen M., Zoethout J.A., Basiak A., Chalas M., Chesiak M., Gramza A., Iwankiewicz J., Sieradzan E., Wikiera B., Ciechanowska M., Dziatkowiak H., Futona B., Gorska A., Glowacka-Wony M., Kaim I., Klich B., Starzyk J., Wolanin M., Tokarska L., Chucherco D., Deja G., Firek-Pedras M., Jarosz-Chobot P., Kalina M., Kutrowska-Adamusiak K., Minkina-Pedras M., Muchaka-Bianga M., Bodalski J., Mlynarski W., Szadkowska A., Cieslak A., Cypryk K., Dziatosz K., Jastzebowska J., Krysiak A., Szymanska U., Wilcznski J., Zawodniak-Szalapska M., Aguay A., Bilbao J.R., Chueca M., Cortazar A., Echarte G., Frutos T.G., Jimenez P., Martul P., Moreno A., Oyarzabal M., Rica I., Salgado Y., Martinez-Larrad M.T., Hawkins F.G., Hernandez R., Herranz L., Pallardo L.F., Deibarra L.S., Fernandez B.H., Luis J.L., Ortiz-Quintana L., Recarte P.P., Arnau D.R., Aronsson L., Boden S., Fredriksson J., Isacsson E., Johansson I., Karlsson E., Lock C., Sandstrom A.-M., Konefal M.S., Andreasson C., Dahlstrom U., Hanas R., Lundqvist K., Windell L., Jansson I., Karlsson A.-K., Lindbladh B., Odenman I., Pettersson C., Sundberg F., Sundqvist M., Aronsson S., Bellman I., Bengtsson A.-B., Lyden G.-B., Nilsson N.-O., Soderblom M., Unt C., Augustsson M., Bengtsson M., Fors H., Helmrich A., Johansson T.O., Andersson A.-C., Boiard-Stomlid A., Hellgren G., Kallsholm H., Lindqvist J., Nilsson M., Nordwall M., Stromstedt C., Ahsberg C., Lindh A., Lindhe C., Samuelsson C., Wiik A., Edenwall H., Ljumgcrantz M., Persson I.-B., Strigard E., Svensson B.-L., Aman J., Breivik G.-E., Detlofsson I.-L., Kroon M., Sarnblad S., Johansson C., Ilvered R., Lundberg A., Akesson K., Beccarelli A., Gadient M., Rappold-Amrein C., Schoenle E., Daftary A., Damagro-Elias M.E., Gilmour C., Klein M.B., Lain C., Salerno D., Smith M.E., Vats K., Pfaff D.J., Malone P., Mansfield P., Munns M., Nickel K., Pompilio K., Siemion W., Taculad R., Van Horn K., Zdanadewic M., Chambliss C., Jones J., Sadler M., Tanner-Blasiar M., Bell C., Camper N., Devaskar S., Devaskar U., Horowitz H., Rogers L., Shannahan R., Silk K., Bermudez Z., Colon R., Frazer T., Martinez-Nieves B., Torres J., Vega J., Chan M., Cook S., Goland R., Greenberg E., Jules N., Montes J., Nelson M., Parra-Valencia Z., Schachner H., Softness B., Kiviniemi M., Suomenin R., Alexander A., Hyrckowian E., Nichol L., Trucco M., Karjalainen E., Louhio T., Sarnesto A., Valtonen E., Davydova B., Helander S., Hamalainen J., Harkonen T., Joutsjoki L., Kararic M., Latva-Koivisto M., Lonn E., Nurmi T., Ollila I., Rinkinen J., Ronkainen M., Tukiainen H., Cederlof A., Kiikeri M., Tsupari S., Cheng R., Bryant K., Chan Y., Maezawa Y., Paltser G., Rasavi R., Tsui H., Winer S., Wu P., Yantha J., University of Zurich, and Knip, Mikael

Subjects
Male, Risk, medicine.medical_specialty, Casein, Breastfeeding, 030209 endocrinology & metabolism, 610 Medicine & health, 2700 General Medicine, Endocrinology and Diabetes, Disease-Free Survival, law.invention, Follow-Up Studie, Nutrition Policy, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, Double-Blind Method, SDG 3 - Good Health and Well-being, law, Internal medicine, Diabetes mellitus, medicine, Humans, Cumulative incidence, 030212 general & internal medicine, Child, Infant Nutritional Physiological Phenomena, Original Investigation, 2. Zero hunger, Type 1 diabetes, business.industry, Hazard ratio, Absolute risk reduction, Infant, Newborn, Caseins, General Medicine, ta3121, medicine.disease, Infant Formula, 3. Good health, Diabetes Mellitus, Type 1, Infant formula, 10036 Medical Clinic, Endokrinologi och diabetes, Female, business, Human, Follow-Up Studies
Abstract

IMPORTANCE Early exposure to complex dietary proteins may increase the risk of type 1 diabetes in children with genetic disease susceptibility. There are no intact proteins in extensively hydrolyzed formulas. OBJECTIVE To test the hypothesis that weaning to an extensively hydrolyzed formula decreases the cumulative incidence of type 1 diabetes in young children. DESIGN, SETTING, AND PARTICIPANTS An international double-blind randomized clinical trial of 2159 infants with human leukocyte antigen-conferred disease susceptibility and a first-degree relative with type 1 diabetes recruited from May 2002 to January 2007 in 78 study centers in 15 countries; 1081 were randomized to be weaned to the extensively hydrolyzed casein formula and 1078 to a conventional formula. The follow-up of the participants ended on February 28, 2017. INTERVENTIONS The participants received either a casein hydrolysate or a conventional adapted cows milk formula supplemented with 20% of the casein hydrolysate. The minimum duration of study formula exposure was 60 days by 6 to 8 months of age. MAIN OUTCOMES AND MEASURES Primary outcome was type 1 diabetes diagnosed according to World Health Organization criteria. Secondary outcomes included age at diabetes diagnosis and safety (adverse events). RESULTS Among 2159 newborn infants (1021 female [47.3%]) who were randomized, 1744 (80.8%) completed the trial. The participants were observed for a median of 11.5 years (quartile [Q] 1-Q3, 10.2-12.8). The absolute risk of type 1 diabetes was 8.4% among those randomized to the casein hydrolysate (n = 91) vs 7.6% among those randomized to the conventional formula (n = 82) (difference, 0.8%[95% CI, -1.6% to 3.2%]). The hazard ratio for type 1 diabetes adjusted for human leukocyte antigen risk group, duration of breastfeeding, duration of study formula consumption, sex, and region while treating study center as a random effect was 1.1 (95% CI, 0.8 to 1.5; P = .46). The median age at diagnosis of type 1 diabetes was similar in the 2 groups (6.0 years [Q1-Q3, 3.1-8.9] vs 5.8 years [Q1-Q3, 2.6-9.1]; difference, 0.2 years [95% CI, -0.9 to 1.2]). Upper respiratory infections were the most common adverse event reported (frequency, 0.48 events/year in the hydrolysate group and 0.50 events/year in the control group). CONCLUSIONS AND RELEVANCE Among infants at risk for type 1 diabetes, weaning to a hydrolyzed formula compared with a conventional formula did not reduce the cumulative incidence of type 1 diabetes after median follow-up for 11.5 years. These findings do not support a need to revise the dietary recommendations for infants at risk for type 1 diabetes. Funding Agencies|Eunice Kennedy Shriver National Institute of Child Health and Development (NICHD); National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health [HD040364, HD042444, HD051997]; Canadian Institutes of Health Research; Commission of the European Communities [QLK1-2002-00372]; European Foundation for the Study of Diabates/JDRF/Novo Nordisk; Academy of Finland (Centre of Excellence in Molecular Systems Immunology and Physiology Research) [250114]; Dutch Diabetes Research Foundation; Finnish Diabetes Research Foundation; JDRF

Published
2018

20. Enhanced bulk conductivity of A-site divalent acceptor-doped non-stoichiometric sodium bismuth titanate

Author

Yang, F., Wu, P., Sinclair, D., and Kilner, J

Subjects
Materials Science(all), Chemistry(all), Non-stoichiometry, Doping, Oxide-ion conductors, Sodium bismuth titanate, Condensed Matter Physics
Abstract

Bismuth-deficient sodium bismuth titanate (nominally Na0.5Bi0.49TiO2.985, NB0.49T) is a good oxide-ion conductor. Here we report the influence of A-site divalent ions, M2 + = Ca2 +, Sr2 + and Ba2 +, on the electrical properties of NB0.49T. A-site divalent doping for Bi3 + enhances the bulk (grain) conductivity by ~ one order of magnitude without changing the conduction mechanism, which is attributed to an increase in the oxygen vacancy concentration based on the doping mechanism Bi3 + + ½ O2 − → M2 +. Among these three dopants, Sr2 + is the most effective in increasing the bulk conductivity due to a combination of its smaller mismatch in ion size with Bi3 +, its intermediate polarisability and lower bond strength to oxygen compared to Ca2 + and Ba2 +. Doping strategies for further improvements to bulk conductivity of NBT materials are discussed based on these results. Comparison with other oxide-ion conductors and initial stability test under reducing atmosphere show the doped non-stoichiometric NBT materials are promising for low and intermediate temperature applications.\ud \ud

Published
2017
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21. Dissimilation of synonymous codon usage bias in virus-host coevolution due to translational selection

Author

Wu P, Xiaoyun Chen, Hou Y, Hao Zhang, Shaozhi Deng, Chen F, Zheng Hu, Yang, and Jianzhi Zhang

Subjects
Genetics, 0303 health sciences, Ecology, Translational efficiency, Host (biology), fungi, Translation (biology), Biology, Virus, Article, 03 medical and health sciences, 0302 clinical medicine, RNA, Transfer, Codon usage bias, Transfer RNA, Viruses, Selection, Genetic, Codon, Codon Usage, Gene, 030217 neurology & neurosurgery, Ecology, Evolution, Behavior and Systematics, Coevolution, 030304 developmental biology
Abstract

Eighteen of the 20 amino acids are each encoded by more than one synonymous codon. Due to differential transfer RNA supply within the cell, synonymous codons are not used with equal frequency, a phenomenon termed codon usage bias (CUB). Previous studies have demonstrated that CUB of endogenous genes trans-regulates the translational efficiency of other genes. We hypothesized similar effects for CUB of exogenous genes on host translation, and tested it in the case of viral infection, a common form of naturally occurring exogenous gene translation. We analysed public Ribo-Seq datasets from virus-infected yeast and human cells and showed that virus CUB trans-regulated tRNA availability, and therefore the relative decoding time of codons. Manipulative experiments in yeast using 37 synonymous fluorescent proteins confirmed that an exogenous gene with CUB more similar to that of the host would apply decreased translational load on the host per unit of expression, whereas expression of the exogenous gene was elevated. The combination of these two effects was that exogenous genes with CUB overly similar to that of the host severely impeded host translation. Finally, using a manually curated list of viruses and natural and symptomatic hosts, we found that virus CUB tended to be more similar to that of symptomatic hosts than that of natural hosts, supporting a general deleterious effect of excessive CUB similarity between virus and host. Our work revealed repulsion between virus and host CUBs when they are overly similar, a previously unrecognized complexity in the coevolution of virus and host. This study shows repulsion between virus and host codon usage bias when they are too similar, due to increased viral expression leading to levels of tRNA consumption that impede host translation.

Published
2019

22. Factors associated with overall survival and relief of dysphagia in advanced esophageal cancer patients after 125I seed-loaded stent placement: a multicenter retrospective analysis

Author

Guo Jh, Teng Gj, Qin J, Ai-Wu Mao, Su C, Lu J, Hao Xu, Cai-Fang Ni, Wu P, and Zhu Hd

Subjects
Male, China, medicine.medical_specialty, Esophageal Neoplasms, medicine.medical_treatment, Adenocarcinoma, Gastroenterology, Iodine Radioisotopes, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Aged, Neoplasm Staging, Proportional Hazards Models, Retrospective Studies, Performance status, business.industry, Proportional hazards model, Palliative Care, Hazard ratio, Stent, Retrospective cohort study, General Medicine, Middle Aged, Esophageal cancer, Prognosis, medicine.disease, Dysphagia, Treatment Outcome, 030220 oncology & carcinogenesis, Carcinoma, Squamous Cell, Female, Stents, 030211 gastroenterology & hepatology, medicine.symptom, Deglutition Disorders, business
Abstract

Iodine-125 (125I) seed-loaded stent placement has served as an effective palliation for malignant esophageal strictures in China. We performed a retrospective study to identify the prognostic factors of this irradiation stent placement in advanced esophageal cancer patients. A total of 201 patients who underwent 125I seed-loaded stent placement were included in this study from June 2012 to March 2016 at five hospitals in China. The Cox regression models adjusted for stratification factors were used, and a stepwise multivariate analysis was performed to predict the overall survival and relief of dysphagia on the basis of pretreatment clinical characteristics, respectively. Three independent prognostic factors were identified for overall survival: histopathological subtype (squamous cell carcinoma vs. adenocarcinoma, hazard ratio [HR] 1.45, 95% confidence interval [CI95%]: 1.01-2.09, P = 0.046), serum total protein (≥66 g/L vs.

Published
2019

23. Linagliptin Effects on Heart Failure and Related Outcomes in Individuals With Type 2 Diabetes Mellitus at High Cardiovascular and Renal Risk in CARMELINA

Author

McGuire D, Alexander J, Johansen O, Perkovic V, Rosenstock J, Cooper M, Wanner C, Kahn S, Toto R, Zinman B, Baanstra D, Pfarr E, Schnaidt S, Meinicke T, George J, von Eynatten M, Marx N, Aizenberg D, Fiorella A, Edgardo N, Belen C, Alonso P, Walter M, Maia K, Guillermo S, Leandro B, Constanza R, Alejandra N, Melina C, Ariel I, Rodrigo C, Alvarez C, Jorge M, Gabriel C, German S, Bartolacci I, Bolobanich G, Tale T, Meritano M, Echeverria M, Gerrini S, Alvarez M, Torrijos N, Berli M, Coggiola J, Castaneda G, Rode R, Milessi R, Roude A, Bono J, Caresani J, Arias V, Westberg J, Allende G, Liberman A, Bordonava A, Almagro S, Gerbaudo C, Schiavi L, Budassi N, Cecilia M, Buncuga M, Carlos S, Osvaldo T, Mercedes S, Calella P, Agustina V, Aljandro M, Alberto D, Fiorella M, Cantero M, Cariganano M, Anadon P, Cartasegna L, Gabriela M, Fernanda A, Alberto R, Chacon C, Jazmin F, Colombo H, Coni E, Mattausch S, Thomsenhall K, della Torre M, Morandini M, Berra F, Margarita H, Commendatore V, Tedesco J, Bolzan P, Cuneo C, Narcisa G, Caputi V, Pablo S, Sandra G, Pacora F, Tinari M, Jure H, Parody M, Toranzo A, Frechtel G, Yohena S, Lovecchio S, Muller C, Martin S, Olivera C, Breyaui M, Bianchi G, Garcia C, Luciana V, Florencia F, Ruben G, Gelersztein E, Rey G, Sanchez C, Fornasari L, Di Pierro L, Giacomi G, Miguel S, Laura T, Gonzalo C, Ramon C, Glenny J, Koretzky M, Porto A, Tiberio O, Ellenberg A, Saurral R, Igarzabal C, Vilamajo O, Matkovich J, de Lapertosa S, Villagra M, Cuzziol G, de la Cruz M, Pinchetti R, Mierez M, Lopez C, Gorosito V, Gabito A, Kleiban A, Grosembacher L, Adrian P, Paula R, Javier G, Kraft F, Andres F, Krynski F, Nicolas P, Marcelo F, Alfredo F, de la Fuente R, Natalia C, Luquez H, Recuero Y, Becchetti N, Ruiz M, Costantino M, Vazquez G, Guzman C, Pelatia P, Maffei L, Sassone S, Yantorno M, Prado G, Khron B, Maldonado N, Gustavo L, Veronica V, Marino J, Elizabeth A, Alejandra C, Oscar R, Azize G, Gallardo M, Escudero M, Vargas E, Ramos H, Lucero C, Najenson M, Crocci I, Chiesa A, Nardone L, Dominguez S, Zanini A, Manghi F, Grossman M, Giudice G, Romeo A, Piskorz D, Miguel C, Susana D, Noeli U, Rosa S, Martin V, Soledad A, Virginia M, Lorena G, Prado A, Veronica L, Eduardo H, Adolfo P, Florencia W, Rista L, Scolari C, Rojas N, Bertolio V, Zarandon R, Jair S, Orlando C, Sanabria H, Ignacio D, Viviana C, Marina R, Sarjanovich R, Scaro G, Huerta C, Mana M, Gutierrez M, Dain A, Gavicola R, Sessa H, Sacripanti J, Felman R, Vilarino P, Sicer M, Lagrutta M, Sala J, Casabella T, Cecilia H, Carlos B, Vines G, Javier R, Vico M, Lanchiotti P, Martella C, Torres L, Villarino A, Molina M, Martinez J, Farias C, Bertola S, Rojas M, Guzman P, Nisi J, Martinez D, Barrionuevo M, Vita N, Lopez A, Vottero E, Giuliano M, Paron L, Vogel D, Mele P, Imposti H, Dominguez A, Zaidman C, Fernando G, Beck M, Beltrame P, Chemello D, Junior R, Abreu A, Fernandes V, Saboia J, Rodrigues L, Carvalho M, Gurgel M, Gadelha D, Ramos C, Borba V, Golbert M, Pitthan M, Golbert L, Valentini R, Canani L, Gross J, Valenti A, Sartori C, Dutra O, Azevedo E, Azevedo A, Vaz R, Vaz H, da Costa F, da Costa L, Panarotto D, Lain F, Camazzola F, Dellomea B, Rech R, Pizzato P, Nunes C, Jaeger C, Silveira D, Wagner L, Machado L, Rea R, de Bem A, Alves J, Jonasson T, Malucelli F, Betti R, Lerario A, Lisboa H, Bem J, Tres G, Tavares C, Nardi A, Pozzatto M, Backes L, Reolao J, Scariot E, Ziguer E, Baldissera D, Griz L, Antunes D, Victor F, Freire K, Barros A, Costi B, Sa M, Carneiro A, Felicio J, Felicio K, Penha P, Ferreira J, Melo F, Alves A, Souza A, Costa L, Pinheiro D, Turatti L, Augusto G, Leanca C, Santomauro A, Forti A, Sena R, Marinho A, Facanha C, de Souza K, de Souza A, de Queiroz W, Leite S, Vieira S, Gubert L, Olsen A, Piazzetta G, Fuck A, Ferreira M, Fortes J, Brandao T, Alves F, Radice E, dos Santos J, de Almeida R, Franco D, Saporito W, Eliaschewitz F, de Siqueira K, Bona R, Genestreti P, de Castro D, Visconti G, Sampaio C, Palhares F, Konigsfeld H, Alves E, Feder C, Leao B, Saraiva J, Rodovalho S, Costa M, Pires N, Figueiredo E, Werner G, Garcia J, de Paiva I, Quirino B, Botelho R, da Silva R, Navarro A, Lourenco C, Pereira A, Arantes F, Boner D, Saad J, Falchetto E, Washizu E, Mandil A, Pimenta N, Tofani F, Fonseca T, Teixeira L, Maia L, Lemos M, Mouco O, Nakazone M, Weiand L, Bohn J, Hissa M, Araripe F, Carvalho F, Cancado G, Wang R, Chacra A, Fusaro A, de Mendonca E, Cercato C, Halpern A, Alves B, Braile M, Sestito R, Mustafa E, Ferreira V, Sbardellini B, de Almeida P, Guimaraes F, Piedade M, Bienert I, Braga J, Daher R, Hirakawa T, Terra E, Farias E, Figueiredo M, Lima L, Moraes K, Avelino I, Flato U, Plavnik F, Portes E, Moreira M, Vendramini M, Veloso R, Padilha M, Rodrigues A, Adam R, Santos S, Sayeg N, Guerrero D, Madeira M, Siqueira J, Pinheiro R, Villacorta A, Mellazi A, Braga T, Kaiser S, Paolino B, Lefterov I, Marinchev A, Angelova S, Klyuchkova N, Lybomirova Z, Kerekovski Y, Kuneva T, Penkova D, Levterov G, Videnova E, Georgieva P, Shinkov A, Borissova A, Vlahov J, Dakovska-Dekova L, Lucheva M, Luchev P, Temelkova M, Borisova K, Tsenov S, Andreeva V, Margaritov V, Arasheva G, Lozanov L, Borisov R, Gorcheva D, Henein S, Whatley S, Boutros M, Kalyniuk N, Berlingieri J, Nisker W, Hoag G, Hepburn D, Harvey M, Manjoo P, Yale J, Sherman M, Tsoukas M, Rehman W, Mason M, Santerre M, De Kock J, Barkhuizen F, Rooke C, Gill C, Kooy J, Burgoyne G, de Kock J, Degen G, Hockman L, Invik R, Roberts P, Ward K, Alasaad H, Susan A, Davies V, Gupta N, Milhalidis J, Grossman L, Agawal N, Yared Z, Rwaheed, Nouhad S, Nahla A, Khandwala H, Warwick A, Wadehra D, Manan A, Vecchiarelli J, Aslam N, Ferrao A, St-Maurice F, Collette R, Davey B, Nawaz S, Coutu B, Costi P, Greiss I, Mansour F, Raymond J, St-Phard W, Nadra I, Della Siega A, Barahona L, Klinke P, Contractor H, Fryer M, Chandra N, Conti B, Telzer L, Sorensen S, Lounsbury N, Martin E, Mitchell L, Pelzer E, Nelson S, Jones M, Cox J, Luco G, Trhoughton T, Labonte R, Chouinard G, Frechette A, Rheaume M, Cusson J, Faucher J, Dery V, Kelly A, Miranda B, Al-Kayssi N, Malette P, Rheault P, Fredette P, Dumas R, Palardy J, Belanger A, Boucher P, Doyon B, Charbonneau J, Bailey G, Odendaal M, Stephan K, Badenhorst J, Knight D, Thurgood A, Johnston M, Cooper-Rosen E, Jagger R, Green M, Weisnagel S, Gangloff A, Bergeron J, Pesant Y, Chevalier P, Woo V, Hurd C, Ruckert G, Lira J, Navarro G, Venegas M, Gonzalez P, Montecinos H, Vidal G, Fernandez M, Varas J, Fernandez C, Aguilar J, Marin R, Kindel C, Yovaniniz P, Gherman O, Aravena M, Carvajal J, Macias E, Corrado P, Lazcano M, Garrido B, Charme G, Carrasco J, Vignolo P, Saavedra S, Gajardo V, Saavedra C, Santamaria D, del Castillo B, Balda I, Zurvarra V, Fu G, Jiang D, Huang H, Wang M, Song J, Lu W, Lin Y, Lu Z, Shi Y, Zhong M, Zhao X, Chen D, Zhang G, He Y, Shi P, Chu K, Gao Q, Deng W, Zhang J, Zhang Y, Chen H, Liu E, Xie Y, Lin R, Tan W, Yuan Z, Wang Y, Ren J, Yu H, Luo M, Ma W, Shi W, Xu H, Xu M, Liu G, Dong Y, Bai B, Guo R, Liu X, Gao Y, Li S, Xu X, Liu P, Dong X, Wang S, Fu F, Jiang Q, Meng C, Yin X, Lu Y, Cui Y, Su G, Miao W, Wei F, Zhao Q, Li Z, Gao X, Lozno H, Prada W, Figueroa W, Ordonez A, Quintero E, Vallejo G, Contreras C, Escobar J, Alvaran J, Ortiz L, Marin M, Montoya C, Mendoza J, Manjarres J, Navarro B, Martinez G, Bonfanti A, Perci X, de la Hoz L, Arroyo J, Rendon C, Lopez J, Escobar N, Franco J, Lozano M, Zapata C, Ibarra L, Barrero A, Sarmiento A, Lozada H, Olitte M, Florez L, Munoz C, Quintero G, Correa G, Ruiz S, Dorado A, Causa A, Palma E, Morales A, Arteaga J, Beltran J, Granados M, Rubio A, Dada F, Bueno W, Rivera R, Corredor K, Romero V, Accini F, Palmera J, Ruiz G, Ortega M, Sanchez A, Lora Y, Cano J, Duque S, Thiriez S, Castano M, Giraldo P, Boljkovac Z, Grcic I, Balen M, Zukanovic S, Jeric M, Dvorscak D, Car S, Knezevic A, Herceg D, Franov B, Miskovic V, Bakula M, Hadak A, Superba M, Rubes J, Gornik I, Hamzic J, Ballek L, Sedlackova L, Hejlova J, Galatikova D, Huskova A, Zak P, Flekac M, Mraz M, Potuznik P, Palova S, Novak P, Okenka L, Matuska J, Rohac F, Vondrak K, Reichert P, Shamasna A, Skopek J, Lejskova M, Jiruska M, Lang P, Podoubsky R, Svobodova J, Cifkova R, Jozifova M, Krajcoviechova A, Wolfhart P, Sulc P, Silhova E, Cechakova M, Machova V, Balkova J, Peterka M, Votocek S, Prosecky R, Valis M, Barton P, Tomek J, Pumprla J, Axmannova M, Vitaskova R, Sincl F, Horanska P, Richter B, Malicherova E, Roderova E, Jenickova P, Winkelmann B, Finger C, Klausmann G, Milek K, Schwabe M, Weiss N, Mahlmann A, Werth S, Schmidt C, Schoell I, London M, Steidl E, Orban K, Taeschner H, Bonigut S, Schiefke I, Schwittay A, Kornmann O, Eich A, Franke S, Kis J, Szobota E, Danos P, Beke E, Grosz A, Csecsei G, Ferenczy J, Filo A, Ferencz I, Mihaly E, Baranyi T, Revesz K, Schlezak J, Harcsa E, Dombroczki Z, Kocsis I, Juhasz E, Literati-Nagy B, Kulcsar E, Bezzeg K, Kemeny V, Peterfai E, Buday B, Keltai K, Balo T, Somogyi A, Nagy G, Oroszlan T, Bagosi Z, Bujtor Z, Tabak A, Ferencz V, Domjan B, Tanczer T, Palinkas A, Karolyi H, Kovacs K, Csaszar I, Palhegyi E, Engelhalter G, Horthy R, Vanko E, Szabo G, Sipos G, Szigyarto M, Sebo N, Paragh G, Zsiros N, Szentimrei R, Pal D, Kobling T, Szanto I, Varadi Z, Bajnok L, Szujo S, Nemes O, Bajnok A, Mezosi E, Bodis B, Marton Z, Konyves L, Farago M, Kiss G, Kiss O, Nagy E, Takacs R, Nyitray S, Abraham G, Fehertemplomi K, Deak L, Dezso E, Karneili E, Deeb D, Zloczower M, Mahmid R, Zolotov S, Hochberg I, Elias M, Goldstein L, Poletaev V, Rock W, Koren O, Saliba W, Wolf F, Adawi F, Nimer A, Mosenzon O, Raz I, Potekhin M, Cahn A, Yulian T, Zvulunov E, Israel H, Shpitz D, Bar-Or I, Chananashvili L, Irena L, Dessau H, Halabe A, Vishlitzky V, Nabriski D, Baraf L, Itelman M, Schiff E, Willner N, Fireman-Klein E, Svistunov V, Dotan Y, Pavlichev O, Saig L, Bashkin A, Kuyantseva E, Gershkov S, Nodelman M, Arbel Y, Bogomolny N, Leshem-Rubinow E, Rofe M, Chorin E, Havkuk O, Wainstein J, Feldman D, Fujino Y, 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Ocicka-Kozakiewicz A, Jurowiecki J, Stasinska T, Karczewicz-Janowska J, Jaruga J, ZytkiewiczJaruga D, Krupinska E, Pupek-Musialik D, Bogdanski P, Szulinska M, Skrypnik D, Skokowska E, Bojarska-Los M, Giermkowska-Samek M, Pirog M, Wojnowski L, Jelinska A, Gradzka M, Danyluk A, Lysek R, Sliwinska T, Podrazka-Szczepaniak A, Barney M, Tomczyk A, Necki M, Malicka J, Dudzinska M, KiszczakBochynska E, Markiewicz A, Galbas K, Paciorkowski A, Mazur S, Mazur M, Chmielowski A, Swiatek A, Sobocka B, Wis J, Jozefowska M, Kaczmarek M, Timler M, Cieplucha Z, Lazuka L, Lazuka N, Wittek A, Spyra J, Jasiel-Wojculewicz H, Stefanski A, Wierucki L, Hanczuk A, Misiura M, Szmygel K, Kolcowa O, Orlowska-Kunikowska E, Rutkowski M, Ignaszewska-Wyrzykowska A, Popenda G, Maciejewska J, Mostowy A, WojteckaGrabka M, Grazyna M, Wieslaw K, Barbara K, Kramarczuk E, Wojciech C, Jaroslaw H, Ewa B, Karas P, Agnieszka S, Hanna C, Justyna S, Piotr K, Wozniak I, Mateusz W, Katarzyna W, Jacek F, Andrzej J, Cymerman K, Gmytrasiewicz M, Zambrzycki J, Krysiak-Kowaluk H, Klodawska K, Klszczewski Z, Zieleniewski J, Opadczuk P, Urbanska K, Faran-Grabowska K, Szczepanik T, Siegel A, Kleczek A, Kincel K, Nowak D, Slowik-Gomulka L, Watemborska-Matuszyk G, Lampart J, Strozik-Krecichwost A, Dziewit T, Broncel M, Wojcik-Odyniec J, Jakubczyk E, Wierzbicka K, Witowicz A, Jedrych B, Korczyk P, Socik-Pojawa M, Monteiro P, Monteiro S, Mendes P, Soares F, Mendes S, Leite L, Vicente J, Santos M, Ferreira A, Alves P, Rosario F, Garrao A, Duarte L, Rogado C, Duarte R, Laginha T, Matos P, Raposo J, Mariz J, Teixeira J, Capela C, Leitao A, Cardiga R, Alface M, Augusto S, Basto L, Cunha A, Rei D, Dantas J, Verdasca I, Andrade L, Silva A, Suarez M, Dias V, Silva J, Pereira N, Goncalves M, Goncalves A, Silveira A, Sampaio A, Dias A, Diogo M, Vilaca C, Cif A, Calin T, Elena S, Crisan C, Adina S, Ramona S, Anghel V, Simona C, Turcu L, Mihaela V, Cosma D, Cristina H, Marius-Calin H, Negrisanu G, Andreea-Andrada M, Maria-Mihaela 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M, Rebecca J, Barker T, Seaton B, Campbell E, Kompanik H, Jayson L, Huffman C, Bialow M, McDonnell G, McCaffrey J, Manis C, DeLuca E, Levins J, Bartlett M, Anorga K, Franco M, Gentry P, Hodge D, Pohil R, Rschultz, Leggett R, Blair L, Gisler J, Niegos F, Osburn M, Parma K, Schendel S, Stines L, Winnie M, Wu P, Canales J, Yu J, Cornett G, Beavins J, Hyde D, Zapinski D, Johnson T, Levinson D, Ahmed A, Kenny B, Kuehl A, Bates C, Jantzi C, Ananthula P, Shafer J, Louthan J, Bays A, Stapleton A, Staton P, Strum D, Taylor P, Smith A, Rapp R, Bao S, Randolph C, MacGillivray B, Schuster R, Harden T, Barnella C, Dunnam T, Whiles R, Bolick C, Brockmyre A, Plucker S, Marshall C, Poteet C, Morin D, Tavel E, Averill N, McFann A, Purcell D, Dixon T, Corey E, Goss J, Drescher R, Irfan M, Naeem M, Egelhof R, Mehta P, Koehler T, Walia J, Fernandez J, Bedel G, Preet R, Bhuchar S, Ahmed F, Onyema D, Benchabbat A, Kohanbash L, Miller P, Lalinde M, Carrithers E, Patterson R, Raube-Miceli A, Martinez A, 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Earl J, McNeill R, Farrington C, Carr K, Nabat M, Matthew S, Yvette E, Handelsman Y, Delkhah S, Ismail Y, Janna C, Akhtar A, Neiman A, Blumenthal S, Colleen V, Schmidt D, Ashraf E, Bhargava A, Khoo T, Langel C, Theuma P, Wright D, Fitzgerald K, Hitchcock J, Capasso-Gulve E, Wolff E, Umpierrez G, Priyathama V, Francisco P, Dawn S, Quraishi A, Kahn B, Ferro F, Hertz B, Phelps J, Campbell A, Downing J, Pangtay D, Pangatay S, Villagran-Solis K, Haseeb M, Rettig K, Kwan R, Cox R, Slimak V, So A, Schmedtje J, Chang A, Douglas Z, McGarity W, Jestel J, Kanade P, Julie J, Asher R, Canaan Y, Perez A, Alonso I, Cutchin R, Koser A, Adeola Y, Brito S, Stocks J, Frandsen B, Weigelt M, Stehouwer E, Ince C, Stephen P, Shadi B, Jeffrey C, Thethi T, Carpio G, McDuffie R, Moreau C, Stell C, Katalenich B, McKendall-Lewis C, Htun W, Conroy K, Lovre D, Galagan R, Olmeda C, Sihota A, Barton A, Beasley R, Nankivel P, Aberle M, Machin I, Porras J, Rodriguez D, Albornoz A, Haidar A, Lopez-Santini R, Rivero G, 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Colfer H, Kane L, Teklinski A, Gadowski G, Levanovich P, Saba F, Confident L, Hossain S, Steinberg B, Philippe B, Choroenthkongtrakal S, Boccalano F, Anand R, Syam V, Manohar A, Suresh P, Madhusudhan P, Patel P, Cambier P, Klonaris J, Cheng W, Fisher S, Schelle M, Reese L, McLean S, Poock J, Hoens J, Rosie A, Welshons R, Dean J, Kuhlman P, Luke R, Lohrbauer L, Cunningham M, Buday P, Lehmann M, Chrzanowski K, Fletcher A, Hargrove J, Harris F, Debs-Perez G, Maiquez A, Cordoves L, Georgescu M, Tayoun H, Munoz F, Ortiz D, Munoz G, Hamzeh I, Misra A, Zhang L, Forgosh L, Loria K, Roncari C, Hommerding J, Morris G, Lebron C, Blake K, LaVenture K, Lange C, Levinson L, Baungarten T, Edevante S, Shawley S, Moyer H, Elliott K, Iachini K, Rajan R, Davis C, Shattuck A, Simon W, Lakin G, Secrist N, Buth D, Steere D, Talbot K, Singh N, Mascolo R, Sloan S, Kmetzo J, Brown J, Carter L, Lawrence M, Arauz-Pacheco C, Lender D, Kozlow W, Cavanaugh L, Wilson J, Gujja P, Akhter F, Khan M, Mohammed A, Satyavolu S, Dev D, Yalamanchili H, Sumeyye C, Fernandes H, Chaleff F, Jancko M, Trenche S, Kaplan W, Wilcox S, Goisse M, Rua M, Black J, Chapman K, Suh D, Yan L, Song D, Chanara S, Houchin V, McKeinness A, Sotolongo R, Gutierrez K, Miranda-Palma B, Solano M, Jain M, Needell J, Banerjee A, Jarratt M, Hantel S, Lees K, Welty F, Freedman S, Parhofer K, Birkeland K, McGill J, Tijssen J, Clemmensen P, Pehrson S, Grande P, Januzzi J, Wood M, Petrie M, Sairanen T, Tatlisumak T, Soinne L, Kase C, Turan T, Mann J, Agarwal R, Fogarty D, Navaneethan S, Srinivas T, Forsmark C, Frossard J, Gelrud A, Mayerle J, Lee R, Heist R, Sullivan R, Buchbinder E, Chodak G, Edelman M, Thompson V, Coles A, and CARMELINA Investigators

Subjects
cardiovascular disease, type 2 diabetes mellitus, heart failure, chronic kidney diseases
Abstract

Background: Individuals with type 2 diabetes mellitus are at increased risk for heart failure (HF), particularly those with coexisting atherosclerotic cardiovascular disease and/or kidney disease. Some but not all dipeptidyl peptidase-4 inhibitors have been associated with increased HF risk. We performed secondary analyses of HF and related outcomes with the dipeptidyl peptidase-4 inhibitor linagliptin versus placebo in CARMELINA (The Cardiovascular and Renal Microvascular Outcome Study With Linagliptin), a cardiovascular outcomes trial that enrolled participants with type 2 diabetes mellitus and atherosclerotic cardiovascular disease and/or kidney disease. Methods: Participants in 27 countries with type 2 diabetes mellitus and concomitant atherosclerotic cardiovascular disease and/or kidney disease were randomized 1:1 to receive once daily oral linagliptin 5 mg or placebo, on top of standard of care. All hospitalization for HF (hHF), cardiovascular outcomes, and deaths were prospectively captured and centrally adjudicated. In prespecified and post hoc analyses of HF and related events, Cox proportional hazards models adjusting for region and baseline history of HF were used. Recurrent hHF events were analyzed using a negative binomial model. In a subset of participants with left ventricular ejection fraction captured within the year before randomization, HF-related outcomes were assessed in subgroups stratified by left ventricular ejection fraction > or 50%. Results: CARMELINA enrolled 6979 participants (mean age, 65.9 years; estimated glomerular filtration rate, mL/min per 1.73m(2); hemoglobin A1c, 8.0%; 62.9% men; diabetes mellitus duration, 14.8 years), including 1873 (26.8%) with a history of HF at baseline. Median follow-up was 2.2 years. Linagliptin versus placebo did not affect the incidence of hHF (209/3494 [6.0%] versus 226/3485 [6.5%], respectively; hazard ratio [HR], 0.90; 95% CI, 0.74-1.08), the composite of cardiovascular death/hHF (HR, 0.94; 95% CI, 0.82-1.08), or risk for recurrent hHF events (326 versus 359 events, respectively; rate ratio, 0.94; 95% CI, 0.75-1.20). There was no heterogeneity of linagliptin effects on hHF by history of HF at baseline, baseline estimated glomerular filtration rate or urine albumin-creatinine ratio, or prerandomization left ventricular ejection fraction. Conclusions: In a large, international cardiovascular outcome trial in participants with type 2 diabetes mellitus and concomitant atherosclerotic cardiovascular disease and/or kidney disease, linagliptin did not affect the risk of hHF or other selected HF-related outcomes, including among participants with and without a history of HF, across the spectrum of kidney disease, and independent of previous left ventricular ejection fraction. Clinical Trial Registration: URL: https://www.clinicaltrials.gov. Unique identifier: NCT01897532.

Published
2019

24. Assessing China's agricultural water use efficiency in a green-blue water perspective: A study based on data envelopment analysis

Author

Geng, Q, Ren, Q, Nolan, RH, Wu, P, and Yu, Q

Subjects
Ecology
Abstract

© 2018 Uneven water resources and growing food demand due to an increasing population bring challenges to China. One important mechanism to address these challenges is to enhance water use efficiency (WUE). This requires information on current efficiencies in water use for agricultural production. In this study, we provide a benchmarking tool to assess relative agricultural WUE in 31 provinces in China during 2003-2013. Data Envelopment Analysis (DEA) was used with both green-blue water and blue-only scenarios. Results show that China's agricultural WUE has improved evidently after 2008. Overall technical efficiency (TE) and the pure technical efficiency (PTE) in China based on the green-blue scenario are relatively high, with the average potential increase less than 10% (8% and 4%, respectively). However, there is a larger potential for blue water use efficiency (14% and 7% respectively). The PTE in Northern China (NC) is higher than that in Southern China (SC) while the TE in NC is lower under green-blue scenario. Moreover, the TE and PTE in NC are lower than that in SC under blue-only scenario. These results indicate that green water management techniques in NC are superior to SC but the scale efficiency (SE) in NC is lower. There are four provinces where the efficiency values are on the frontier in four cases, i.e. two scenarios (green-blue and blue-only) and two assumptions in DEA, but fourteen provinces where the efficiency values are not on the frontier in any case and most of them were located in SC. Our results also suggest that improving SE can substantially contribute to national WUE, but exploring the solutions to enhance blue water use efficiency in China is also a key task in the future works. The research results have important implications for China and different provinces to improve agricultural WUE by water policies and management.

Published
2019

25. Effect of Linagliptin vs Placebo on Major Cardiovascular Events in Adults With Type 2 Diabetes and High Cardiovascular and Renal Risk The CARMELINA Randomized Clinical Trial

Author

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Satyavolu S, Dev D, Yalamanchili H, Sumeyye C, Fernandes H, Chaleff F, Jancko M, Trenche S, Kaplan W, Wilcox S, Goisse M, Rua M, Black J, Chapman K, Suh D, Yan L, Song D, Chanara S, Houchin V, McKeinness A, Sotolongo R, Gutierrez K, Miranda-Palma B, Solano M, Jain M, Needell J, Banerjee A, Jarratt M, Hantel S, Lees K, Welty F, Freedman S, Parhofer K, Birkeland K, McGill J, Tijssen J, Clemmensen P, Pehrson S, Grande P, Januzzi J, Wood M, Petrie M, Sairanen T, Tatlisumak T, Soinne L, Kase C, Turan T, Mann J, Agarwal R, Fogarty D, Navaneethan S, Srinivas T, Forsmark C, Frossard J, Gelrud A, Mayerle J, Lee R, Heist R, Sullivan R, Buchbinder E, Chodak G, Edelman M, Thompson V, Coles A, and CARMELINA Investigators

Abstract

IMPORTANCE Type 2 diabetes is associated with increased cardiovascular (CV) risk. Prior trials have demonstrated CV safety of 3 dipeptidyl peptidase 4 (DPP-4) inhibitors but have included limited numbers of patients with high CV risk and chronic kidney disease. OBJECTIVE To evaluate the effect of linagliptin, a selective DPP-4 inhibitor, on CV outcomes and kidney outcomes in patients with type 2 diabetes at high risk of CV and kidney events. DESIGN, SETTING, AND PARTICIPANTS Randomized, placebo-controlled, multicenter noninferiority trial conducted from August 2013 to August 2016 at 605 clinic sites in 27 countries among adults with type 2 diabetes, hemoglobin A(1c) of 6.5% to 10.0%, high CV risk (history of vascular disease and urine-albumin creatinine ratio [UACR] > 200mg/g), and high renal risk (reduced eGFR and micro-or macroalbuminuria). Participants with end-stage renal disease (ESRD) were excluded. Final follow-up occurred on January 18, 2018. INTERVENTIONS Patients were randomized to receive linagliptin, 5 mg once daily (n = 3494), or placebo once daily (n = 3485) added to usual care. Other glucose-lowering medications or insulin could be added based on clinical need and local clinical guidelines. MAIN OUTCOMES AND MEASURES Primary outcomewas time to first occurrence of the composite of CV death, nonfatalmyocardial infarction, or nonfatal stroke. Criteria for noninferiority of linagliptin vs placebo was defined by the upper limit of the 2-sided 95% CI for the hazard ratio (HR) of linagliptin relative to placebo being less than 1.3. Secondary outcome was time to first occurrence of adjudicated death due to renal failure, ESRD, or sustained 40% or higher decrease in eGFR from baseline. RESULTS Of 6991 enrollees, 6979 (mean age, 65.9 years; eGFR, 54.6 mL/min/1.73m2; 80.1% with UACR > 30mg/g) received at least 1 dose of study medication and 98.7% completed the study. During a median follow-up of 2.2 years, the primary outcome occurred in 434 of 3494 (12.4%) and 420 of 3485 (12.1%) in the linagliptin and placebo groups, respectively, (absolute incidence rate difference, 0.13 [95% CI,-0.63 to 0.90] per 100 person-years) (HR, 1.02; 95% CI, 0.89-1.17; P

Published
2019

26. A Physics-based Approach to Assess Critical Load Cases for Landing Gears within Aircraft Conceptual Design

Author

Wu, P., Veldhuis, L.L.M., Voskuijl, M., and Delft University of Technology

Subjects
Analysis and Optimization, Landing Gear, Flight Dynamics and Loads, Multidisciplinary Design, Load Cases
Abstract

The European Union and the United States are proposing to bring in more strict flight vehicle emission criteria in their reports of the high‐level groups on aviation research, i.e. EU Flightpath 2050 and US Destination 2025. More fuel‐efficient aircraft must be developed to achieve this target. Moreover, the increasingly competitive aviation market also expects more fuel‐efficient aircraft to be designed. An efficient and reliable aircraft design with a decreased weight could significantly contribute to the improvement of aircraft economical and environmental performance. Various research studies have highlighted the potential for significant weight savings on the landing gear system. In general, the landing gear accounts for around 5% of aircraft Maximum Landing Weight. In the aircraft conceptual design stage, there are two methods to achieve weight savings on the landing gear system: 1. Investigation of conventional designs 2. Introduction of innovative designs In the use of these two methods, a key step is to verify the design of the landing gear w.r.t certain critical load cases. A landing gear critical load case is defined as a set of combinations of aircraft flight attitudes and motions, control surfaces and engine throttle settings, and environmental conditions that could lead to damage and failure of the landing gear structure. These critical load cases reflect the possible extreme conditions that might occur in operation. These critical load cases are traditionally obtained by utilizing the methods based on statistical data while ignoring specific flight dynamics and landing gear characteristics. These methods could lead to three problems.

Published
2019
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27. Comparison of Kaposi Sarcoma Risk in Human Immunodeficiency Virus-Positive Adults Across 5 Continents: A Multiregional Multicohort Study

Author

Rohner E., Butikofer L., Schmidlin K., Sengayi M., Maskew M., Giddy J., Garone D., Moore R. D., D'Souza G., Goedert J. J., Achenbach C., Gill M. J., Kitahata M. M., Patel P., Silverberg M. J., Castilho J., McGowan C., Chen Y. -M. A., Law M., Taylor N., Paparizos V., Bonnet F., Verbon A., Fatkenheuer G., Post F. A., Sabin C., Mocroft A., Le Moing V., Dronda F., Obel N., Grabar S., Spagnuolo V., Antinori A., Quiros-Roldan E., Mussini C., Miro J. M., Meyer L., Hasse B., Konopnicki D., Roca B., Barger D., Raben D., Clifford G. M., Franceschi S., Brockmeyer N., Chakraborty R., Egger M., Bohlius J., Judd A., Zangerle R., Touloumi G., Warszawski J., Dabis F., Krause M. M., Ghosn J., Leport C., Wittkop L., Reiss P., Wit F., Prins M., Bucher H., Gibb D., Del Amo J., Thorne C., Kirk O., Stephan C., Perez-Hoyos S., Hamouda O., Bartmeyer B., Chkhartishvili N., Noguera-Julian A., Monforte A. D., Prieto L., Conejo P. R., Soriano-Arandes A., Battegay M., Kouyos R., Tookey P., Casabona J., Castagna A., Konopnick D., Goetghebuer T., Sonnerborg A., Teira R., Garrido M., Haerry D., De Wit S., Costagliola D., D'Arminio-Monforte A., Chene G., Schwimmer C., Termote M., Campbell M., Frederiksen C. M., Friis-Moller N., Kjaer J., Brandt R. S., Berenguer J., Bouteloup V., Cozzi-Lepri A., Davies M. -A., Dorrucci M., Dunn D., Furrer H., Guiguet M., Lambotte O., Leroy V., Lodi S., Matheron S., Monge S., Nakagawa F., Paredes R., Phillips A., Puoti M., Schomaker M., Smit C., Sterne J., Thiebaut R., Torti C., Van Der Valk M., Tanser F., Vinikoor M., MacEte E., Wood R., Stinson K., Fatti G., Phiri S., Chimbetete C., Malisita K., Eley B., Fritz C., Hobbins M., Kamenova K., Fox M., Prozesky H., Technau K., Sawry S., Benson C. A., Bosch R. J., Kirk G. D., Boswell S., Mayer K. H., Grasso C., Hogg R. S., Harrigan P. R., Montaner J. S. G., Yip B., Zhu J., Salters K., Gabler K., Buchacz K., Brooks J. T., Gebo K. A., Carey J. T., Rodriguez B., Horberg M. A., Thorne J. E., Rabkin C., Margolick J. B., Jacobson L. P., Klein M. B., Rourke S. B., Rachlis A. R., Cupido P., Hunter-Mellado R. F., Mayor A. M., Deeks S. G., Martin J. N., Saag M. S., Mugavero M. J., Willig J., Eron J. J., Napravnik S., Crane H. M., Drozd D. R., Haas D., Rebeiro P., Turner M., Bebawy S., Rogers B., Justice A. C., Dubrow R., Fiellin D., Gange S. J., Anastos K., Althoff K. N., McKaig R. G., Freeman A. M., Lent C., Van Rompaey S. E., Morton L., McReynolds J., Lober W. B., Abraham A. G., Lau B., Zhang J., Jing J., Modur S., Wong C., Hogan B., Desir F., Liu B., You B., Cahn P., Cesar C., Fink V., Sued O., Dell'Isola E., Perez H., Valiente J., Yamamoto C., Grinsztejn B., Veloso V., Luz P., De Boni R., Wagner S. C., Friedman R., Moreira R., Pinto J., Ferreira F., Maia M., De Menezes Succi R. C., MacHado D. M., De Fatima Barbosa Gouvea A., Wolff M., Cortes C., Rodriguez M. F., Allendes G., Pape J. W., Rouzier V., Marcelin A., Perodin C., Luque M. T., Padgett D., Madero J. S., Ramirez B. C., Belaunzaran P., Vega Y. C., Gotuzzo E., Mejia F., Carriquiry G., McGowan C. C., Shepherd B. E., Sterling T., Jayathilake K., Person A. K., Rebeiro P. F., Giganti M., Duda S. N., Maruri F., Vansell H., Ly P. S., Khol V., Zhang F. J., Zhao H. X., Han N., Lee M. P., Li P. C. K., Lam W., Chan Y. T., Kumarasamy N., Saghayam S., Ezhilarasi C., Pujari S., Joshi K., Gaikwad S., Chitalikar A., Merati T. P., Wirawan D. N., Yuliana F., Yunihastuti E., Imran D., Widhani A., Tanuma J., Oka S., Nishijima T., Choi J. Y., Na S., Kim J. M., Sim B. L. H., Gani Y. M., David R., Kamarulzaman A., Syed Omar S. F., Ponnampalavanar S., Azwa I., Ditangco R., Uy E., Bantique R., Wong W. W., Ku W. W., Wu P. C., Ng O. T., Lim P. L., Lee L. S., Ohnmar P. S., Avihingsanon A., Gatechompol S., Phanuphak P., Phadungphon C., Kiertiburanakul S., Sungkanuparph S., Chumla L., Sanmeema N., Chaiwarith R., Sirisanthana T., Kotarathititum W., Praparattanapan J., Kantipong P., Kambua P., Ratanasuwan W., Sriondee R., Nguyen K. V., Bui H. V., Nguyen D. T. H., Nguyen D. T., Cuong D. D., An N. V., Luan N. T., Sohn A. H., Ross J. L., Petersen B., Cooper D. A., Law M. G., Jiamsakul A., Boettiger D. C., Ellis D., Bloch M., Agrawal S., Vincent T., Allen D., Smith D., Rankin A., Baker D., Templeton D. J., Jackson E., McCallum K., Ryder N., Sweeney G., Cooper D., Carr A., MacRae K., Hesse K., Finlayson R., Gupta S., Langton-Lockton J., Shakeshaft J., Brown K., Idle S., Arvela N., Varma R., Lu H., Couldwell D., Eswarappa S., Smith D. E., Furner V., Cabrera G., Fernando S., Cogle A., Lawrence C., Mulhall B., Boyd M., Petoumenos K., Puhr R., Huang R., Han A., Gunathilake M., Payne R., O'Sullivan M., Croydon A., Russell D., Cashman C., Roberts C., Sowden D., Taing K., Marshall P., Orth D., Youds D., Rowling D., Latch N., Warzywoda E., Dickson B., Donohue W., Moore R., Edwards S., Boyd S., Roth N. J., Lau H., Read T., Silvers J., Zeng W., Hoy J., Watson K., Bryant M., Price S., Woolley I., Giles M., Korman T., Williams J., Nolan D., Allen A., Guelfi G., Mills G., Wharry C., Raymond N., Bargh K., Templeton D., Medical Microbiology & Infectious Diseases, Global Health, Infectious diseases, APH - Aging & Later Life, AII - Infectious diseases, APH - Global Health, Graduate School, APH - Digital Health, APH - Personalized Medicine, Bohlius, Julia, Cohere In, Eurocoord, Castagna, Antonella, Rohner, E, Butikofer, L, Schmidlin, K, Sengayi, M, Maskew, M, Giddy, J, Garone, D, Moore, R, D'Souza, G, Goedert, J, Achenbach, C, Gill, M, Kitahata, M, Patel, P, Silverberg, M, Castilho, J, Mcgowan, C, Chen, Y, Law, M, Taylor, N, Paparizos, V, Bonnet, F, Verbon, A, Fatkenheuer, G, Post, F, Sabin, C, Mocroft, A, Le Moing, V, Dronda, F, Obel, N, Grabar, S, Spagnuolo, V, Antinori, A, Quiros-Roldan, E, Mussini, C, Miro, J, Meyer, L, Hasse, B, Konopnicki, D, Roca, B, Barger, D, Raben, D, Clifford, G, Franceschi, S, Brockmeyer, N, Chakraborty, R, Egger, M, Bohlius, J, Judd, A, Zangerle, R, Touloumi, G, Warszawski, J, Dabis, F, Krause, M, Ghosn, J, Leport, C, Wittkop, L, Reiss, P, Wit, F, Prins, M, Bucher, H, Gibb, D, Del Amo, J, Thorne, C, Kirk, O, Stephan, C, Perez-Hoyos, S, Hamouda, O, Bartmeyer, B, Chkhartishvili, N, Noguera-Julian, A, Monforte, A, Prieto, L, Conejo, P, Soriano-Arandes, A, Battegay, M, Kouyos, R, Tookey, P, Casabona, J, Castagna, A, Konopnick, D, Goetghebuer, T, Sonnerborg, A, Teira, R, Garrido, M, Haerry, D, De Wit, S, Costagliola, D, D'Arminio-Monforte, A, Chene, G, Schwimmer, C, Termote, M, Campbell, M, Frederiksen, C, Friis-Moller, N, Kjaer, J, Brandt, R, Berenguer, J, Bouteloup, V, Cozzi-Lepri, A, Davies, M, Dorrucci, M, Dunn, D, Furrer, H, Guiguet, M, Lambotte, O, Leroy, V, Lodi, S, Matheron, S, Monge, S, Nakagawa, F, Paredes, R, Phillips, A, Puoti, M, Schomaker, M, Smit, C, Sterne, J, Thiebaut, R, Torti, C, Van Der Valk, M, Tanser, F, Vinikoor, M, Macete, E, Wood, R, Stinson, K, Fatti, G, Phiri, S, Chimbetete, C, Malisita, K, Eley, B, Fritz, C, Hobbins, M, Kamenova, K, Fox, M, Prozesky, H, Technau, K, Sawry, S, Benson, C, Bosch, R, Kirk, G, Boswell, S, Mayer, K, Grasso, C, Hogg, R, Harrigan, P, Montaner, J, Yip, B, Zhu, J, Salters, K, Gabler, K, Buchacz, K, Brooks, J, Gebo, K, Carey, J, Rodriguez, B, Horberg, M, Thorne, J, Rabkin, C, Margolick, J, Jacobson, L, Klein, M, Rourke, S, Rachlis, A, Cupido, P, Hunter-Mellado, R, Mayor, A, Deeks, S, Martin, J, Saag, M, Mugavero, M, Willig, J, Eron, J, Napravnik, S, Crane, H, Drozd, D, Haas, D, Rebeiro, P, Turner, M, Bebawy, S, Rogers, B, Justice, A, Dubrow, R, Fiellin, D, Gange, S, Anastos, K, Althoff, K, Mckaig, R, Freeman, A, Lent, C, Van Rompaey, S, Morton, L, Mcreynolds, J, Lober, W, Abraham, A, Lau, B, Zhang, J, Jing, J, Modur, S, Wong, C, Hogan, B, Desir, F, Liu, B, You, B, Cahn, P, Cesar, C, Fink, V, Sued, O, Dell'Isola, E, Perez, H, Valiente, J, Yamamoto, C, Grinsztejn, B, Veloso, V, Luz, P, De Boni, R, Wagner, S, Friedman, R, Moreira, R, Pinto, J, Ferreira, F, Maia, M, De Menezes Succi, R, Machado, D, De Fatima Barbosa Gouvea, A, Wolff, M, Cortes, C, Rodriguez, M, Allendes, G, Pape, J, Rouzier, V, Marcelin, A, Perodin, C, Luque, M, Padgett, D, Madero, J, Ramirez, B, Belaunzaran, P, Vega, Y, Gotuzzo, E, Mejia, F, Carriquiry, G, Shepherd, B, Sterling, T, Jayathilake, K, Person, A, Giganti, M, Duda, S, Maruri, F, Vansell, H, Ly, P, Khol, V, Zhang, F, Zhao, H, Han, N, Lee, M, Li, P, Lam, W, Chan, Y, Kumarasamy, N, Saghayam, S, Ezhilarasi, C, Pujari, S, Joshi, K, Gaikwad, S, Chitalikar, A, Merati, T, Wirawan, D, Yuliana, F, Yunihastuti, E, Imran, D, Widhani, A, Tanuma, J, Oka, S, Nishijima, T, Choi, J, Na, S, Kim, J, Sim, B, Gani, Y, David, R, Kamarulzaman, A, Syed Omar, S, Ponnampalavanar, S, Azwa, I, Ditangco, R, Uy, E, Bantique, R, Wong, W, Ku, W, Wu, P, Ng, O, Lim, P, Lee, L, Ohnmar, P, Avihingsanon, A, Gatechompol, S, Phanuphak, P, Phadungphon, C, Kiertiburanakul, S, Sungkanuparph, S, Chumla, L, Sanmeema, N, Chaiwarith, R, Sirisanthana, T, Kotarathititum, W, Praparattanapan, J, Kantipong, P, Kambua, P, Ratanasuwan, W, Sriondee, R, Nguyen, K, Bui, H, Nguyen, D, Cuong, D, An, N, Luan, N, Sohn, A, Ross, J, Petersen, B, Cooper, D, Jiamsakul, A, Boettiger, D, Ellis, D, Bloch, M, Agrawal, S, Vincent, T, Allen, D, Smith, D, Rankin, A, Baker, D, Templeton, D, Jackson, E, Mccallum, K, Ryder, N, Sweeney, G, Carr, A, Macrae, K, Hesse, K, Finlayson, R, Gupta, S, Langton-Lockton, J, Shakeshaft, J, Brown, K, Idle, S, Arvela, N, Varma, R, Lu, H, Couldwell, D, Eswarappa, S, Furner, V, Cabrera, G, Fernando, S, Cogle, A, Lawrence, C, Mulhall, B, Boyd, M, Petoumenos, K, Puhr, R, Huang, R, Han, A, Gunathilake, M, Payne, R, O'Sullivan, M, Croydon, A, Russell, D, Cashman, C, Roberts, C, Sowden, D, Taing, K, Marshall, P, Orth, D, Youds, D, Rowling, D, Latch, N, Warzywoda, E, Dickson, B, Donohue, W, Edwards, S, Boyd, S, Roth, N, Lau, H, Read, T, Silvers, J, Zeng, W, Hoy, J, Watson, K, Bryant, M, Price, S, Woolley, I, Giles, M, Korman, T, Williams, J, Nolan, D, Allen, A, Guelfi, G, Mills, G, Wharry, C, Raymond, N, and Bargh, K

Subjects
Male, viruses, HIV Infections, Men who have sex with men, Cohort Studies, 0302 clinical medicine, Risk Factors, Antiretroviral therapy, Cohort study, HIV, Kaposi sarcoma, Adolescent, Adult, Anti-Retroviral Agents, CD4 Lymphocyte Count, Female, HIV-1, Humans, Middle Aged, Sarcoma, Kaposi, Viral Load, Young Adult, 030212 general & internal medicine, Articles and Commentaries, Incidence (epidemiology), Hazard ratio, virus diseases, Sarcoma, 3. Good health, Infectious Diseases, 030220 oncology & carcinogenesis, Cohort, Coinfection, Microbiology (medical), antiretroviral therapy, 610 Medicine & health, Kaposi, 03 medical and health sciences, SDG 3 - Good Health and Well-being, 360 Social problems & social services, medicine, cohort study, business.industry, medicine.disease, Confidence interval, business, Demography
Abstract

Background We compared Kaposi sarcoma (KS) risk in adults who started antiretroviral therapy (ART) across the Asia-Pacific, South Africa, Europe, Latin, and North America. Methods We included cohort data of human immunodeficiency virus (HIV)-positive adults who started ART after 1995 within the framework of 2 large collaborations of observational HIV cohorts. We present incidence rates and adjusted hazard ratios (aHRs). Results We included 208140 patients from 57 countries. Over a period of 1066572 person-years, 2046 KS cases were diagnosed. KS incidence rates per 100000 person-years were 52 in the Asia-Pacific and ranged between 180 and 280 in the other regions. KS risk was 5 times higher in South African women (aHR, 4.56; 95% confidence intervals [CI], 2.73-7.62) than in their European counterparts, and 2 times higher in South African men (2.21; 1.34-3.63). In Europe, Latin, and North America KS risk was 6 times higher in men who have sex with men (aHR, 5.95; 95% CI, 5.09-6.96) than in women. Comparing patients with current CD4 cell counts ≥700 cells/µL with those whose counts were

Published
2017

28. Ecological occurrence and plant regeneration of embryoid of the endangered and endemic plantDysosma versipellisin China

Author

Wu P, Hong-Zhen Tang, Yuming Wei, Yang S, Xiao-Ming Tan, and Ya-Qin Zhou

Subjects
chemistry.chemical_compound, Horticulture, Podophyllotoxin, chemistry, Somatic embryogenesis, Callus formation, Callus, Regeneration (biology), medicine, Dysosma versipellis, Kinetin, Explant culture, medicine.drug
Abstract

In this study, the effective callus culture, somatic embryogenesis, and plant regeneration system ofDysosma versipellis, which is an endangered and endemic plant in China, were established under specific culture conditions. Using theD.versipellisleaves, petioles, and roots as explants, DPS software orthogonal design method and SPSS Duncan’s multiple range test were used to investigate their effects ofD.versipellison callus formation, embryoid induction, and plant regeneration by adding different phytohormones. Results showed that leaves and petioles were the most suitable materials in inducing callus. The effect of phytohormone on callus formation followed the order of 2,4-dichlorophenoxyacetic acid (2,4-D)>thidiazuron (TDZ)> kinetin>naphthylacetic acid (NAA)>2-ip. The best medium for callus formation was MS+2,4-D 1 mg/L+NAA 0.05 mg/L+TDZ 0.5 mg/L+2-ip 1 mg/L. The optimal medium to induce the formation of granular callus embryoid was MS+0.5 mg/L 6-BA+0.1 mg/L NAA, and the induction rate was 71.33%. The embryoid rooting and plant regeneration medium was MS+0.5 mg/L IBA+0.5 mg/L GA3. The optimal medium formula obtained in this study was suitable for the rapid induction of callus, embryoid, and plant regeneration ofD. versipellisunder in vitro culture conditions. Further study on the action mechanism, signal regulation mechanism, and artificial seed production of fungal elicitors affecting the accumulation of podophyllotoxin is important.

Published
2018

31. Stellar Populations of over 1000 z ̃ 0.8 Galaxies from LEGA-C: Ages and Star Formation Histories from D n 4000 and Hδ

Author

Wu, P., van der Wel, A., Gallazzi, A., Bezanson, R., Pacifici, C., Straatman, C., Franx, M., Barišić, I., Bell, E., Brammer, G., Calhau, J., Chauke, P., van Houdt, J., Maseda, M., Muzzin, A., Rix, H., Sobral, D., Spilker, J., van de Sande, J., van Dokkum, P., and Wild, V.

Abstract

Drawing from the LEGA-C data set, we present the spectroscopic view of the stellar population across a large volume- and mass-selected sample of galaxies at large look-back time. We measure the 4000 Å break (D n 4000) and Balmer absorption line strengths (probed by Hδ) from 1019 high-quality spectra of z = 0.6-1.0 galaxies with M * = 2 × 1010 M ☉ to 3 × 1011 M ☉. Our analysis serves as a first illustration of the power of high-resolution, high signal-to-noise ratio continuum spectroscopy at intermediate redshifts as a qualitatively new tool to constrain galaxy formation models. The observed D n 4000-EW(Hδ) distribution of our sample overlaps with the distribution traced by present-day galaxies, but z ̃ 0.8 galaxies populate that locus in a fundamentally different manner. While old galaxies dominate the present-day population at all stellar masses >2 × 1010 M ☉, we see a bimodal D n 4000-EW(Hδ) distribution at z ̃ 0.8, implying a bimodal light-weighted age distribution. The light-weighted age depends strongly on stellar mass, with the most massive galaxies >1 × 1011 M ☉ being almost all older than 2 Gyr. At the same time, we estimate that galaxies in this high-mass range are only ̃3 Gyr younger than their z ̃ 0.1 counterparts, at odds with purely passive evolution given a difference in look-back time of >5 Gyr; younger galaxies must grow to >1011 M ☉ in the meantime, or small amounts of young stars must keep the light-weighted ages young. Star-forming galaxies at z ̃ 0.8 have stronger Hδ absorption than present-day galaxies with the same D n 4000, implying larger short-term variations in star formation activity.

Published
2018

32. The impact of carbon emission costs on manufacturers' production and location decision

Author

Wu, P, Jin, Y, Shi, Y, Shyu, H, Jin, Ying [0000-0003-2683-6829], Shi, Yongjiang [0000-0001-8739-6244], and Apollo - University of Cambridge Repository

Subjects
Economic Order Quantity (EOQ) model, carbon emission, location modelling
Abstract

This paper investigates how emerging carbon emission costs may affect the joint production and location decisions for a manufacturer across the world's regions. Specifically, we develop a new theoretical model which explicitly links product demand, production costs and carbon emission levels to location decisions, and investigate the manufacturer's optimal decisions between two distinct regions. The results show that the influence of carbon emissions on manufacturers' decisions can vary greatly under different circumstances: both off-shoring and near-shoring are possible under rising carbon emission costs; manufacturers with high or low demand have different tolerance levels to the rising carbon emission costs when considering an alternative location; trade costs can change the pattern of relocation. To gain policy insights for those who pursue reducing carbon emissions, different product examples are used to calculate the critical carbon price which triggers different location choices. The results suggest that if production technology is stable, raising carbon cost itself has only limited effects on reducing total carbon emissions, especially for high-value-low-emission industries. The location shift, which is more sensitive to changes in variable carbon emissions, may lead to a significant emission reduction when completed. Additional pricing decision from the manufacturer shows no significant effect on the location decisions; however, if demand is linked directly to carbon emission footprint of the product, then it is more hopeful that a raised carbon price would reduce the carbon emissions significantly through relocation.

Published
2017
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33. Influence of Steel Fibre on Dynamic Compressive Properties of Ultra-High Performance Concrete

Author

Wu, P, Liu, Z, Wu, C, Zhang, H, Xu, S, and Su, Y

Subjects
General Science & Technology
Abstract

© 2017, Editorial Board of Journal of Tianjin University(Science and Technology). All right reserved. The dynamic and static compressive experiments on ultra-high performance concrete(UHPC)were carried out, including five sets of specimens with different mixtures, by utilizing the 75 mm split Hopkinson pressure bar (SHPB) system and the YAW-3000 electro-hydraulic servo testing machine, respectively. The effects of types and volume ratios of steel fibers on dynamic compressive strength were analyzed in detail. The dynamic increase factors of UHPC for different mixtures were calculated and the diagram of dynamic increase factors was further obtained. The results indicate that the dynamic compressive strength and peak strain of the UHPC increase significantly with the increase of strain rates; the types and volume ratios of steel fibers have great effect on the dynamic properties of the UHPC but little effect on the dynamic increase factor; a better improvement effect of fibers with greater length-diameter ratios on the dynamic compressive strength of the UHPC was also clearly observed.

Published
2017

34. Self-organization process in newborn skin organoid formation inspires novel strategy for hair regeneration of adult cells

Author

Lei, M, Schumacher, LJ, Lai, YC, Juan, WT, Yeh, CY, Wu, P, Jian, TX, Baker, RE, Widelitz, RB, Yang, L, and Chuong, CM

Subjects
hair neogenesis, phase transition, stem cells, environmental reprogramming, tissue engineering, MD Multidisciplinary
Abstract

Organoids made from dissociated progenitor cells undergo tissue-like organization. This in vitro self-organization process is not identical to embryonic organ formation, but it achieves a similar phenotype in vivo. This implies genetic codes do not specify morphology directly; instead, complex tissue architectures may be achieved through several intermediate layers of cross talk between genetic information and biophysical processes. Here we use newborn and adult skin organoids for analyses. Dissociated cells from newborn mouse skin form hair primordia-bearing organoids that grow hairs robustly in vivo after transplantation to nude mice. Detailed time-lapse imaging of 3D cultures revealed unexpected morphological transitions between six distinct phases: dissociated cells, cell aggregates, polarized cysts, cyst coalescence, planar skin, and hair-bearing skin. Transcriptome profiling reveals the sequential expression of adhesion molecules, growth factors, Wnts, and matrix metalloproteinases (MMPs). Functional perturbations at different times discern their roles in regulating the switch from one phase to another. In contrast, adult cells form small aggregates, but then development stalls in vitro. Comparative transcriptome analyses suggest suppressing epidermal differentiation in adult cells is critical. These results inspire a strategy that can restore morphological transitions and rescue the hair-forming ability of adult organoids: (i) continuous PKC inhibition and (ii) timely supply of growth factors (IGF, VEGF), Wnts, and MMPs. This comprehensive study demonstrates that alternating molecular events and physical processes are in action during organoid morphogenesis and that the self-organizing processes can be restored via environmental reprogramming. This tissue-level phase transition could drive self-organization behavior in organoid morphogenies beyond the skin.

Published
2017

35. Influenza vaccine effectiveness against influenza-associated hospitalization in 2015/16 season, Beijing, China

Author

Zhang Y, Wu P, Feng L, Yang P, Pan Y, Feng S, Qin Y, Zheng J, Puig-Barberà J, Muscatello D, MacIntyre R, Cowling BJ, Yu H, and Wang Q

Subjects
virus diseases
Abstract

Background: Vaccination is recommended to prevent influenza virus infection and associated complications. This study aimed to estimate the influenza vaccine effectiveness (VE) against hospitalization in the 2015/16 season in Beijing. Methods: Patients who were hospitalized in the 5 study hospitals between 1 Oct 2015 and 15 May 2016 were recruited. Influenza vaccination status was obtained for PCR-confirmed influenza patients and the selected controls who tested negative for the virus. Conditional logistic regression was used to estimate the influenza VE matching by calendar week, and adjusting for age, study sites, underlying medical conditions, smoking status, and hospital admissions over the past 12 months. Results: The overall VE was 37.9% (95% CI: -103.3, 6.5) against laboratory-confirmed influenza associated hospitalization. The 2015-16 seasonal vaccine was had 61.9% (95% CI: -211.9, 15.9), 5.4% (95% CI: -108.1, 46.6) and -45.2% (95% CI: -152.6, 16.5) effectiveness to prevent infection from A(H1N1)pdm09, A(H3N2) and influenza B, respectively. Conclusions: Influenza vaccination did not show effective protection against hospitalization with influenza in 2015/16 season in Beijing. (C) 2017 Elsevier Ltd. All rights reserved.

Published
2017

36. Tuning Thz Emission Properties Of Bi2Sr2Cacu2O8+Delta Intrinsic Josephson Junction Stacks By Charge Carrier Injection

Author

Kizilaslan, O., Rudau, F., Wieland, R., Hampp, J. S., Zhou, X. J., Ji, M., Kiselev, O., Kinev, N., Huang, Y., Hao, L. Y., Ishii, A., Aksan, M. A., Hatano, T., Koshelets, V. P., Wu, P. H., Wang, H. B., Dieter Koelle, and Kleiner, R.

Subjects
Condensed Matter::Materials Science, Condensed Matter::Superconductivity, Physics::Optics, Condensed Matter::Strongly Correlated Electrons
Abstract

We report on doping and undoping experiments of terahertz (THz) emitting intrinsic Josephson junction stacks, where the change in charge carrier concentration is achieved by heavy current injection. The experiments were performed on stand-alone structures fabricated from a Bi2Sr2CaCu2O8+delta single crystal near optimal doping. The stacks contained about 930 intrinsic Josephson junctions. On purpose, the doping and undoping experiments were performed over only a modest range of charge carrier concentrations, changing the critical temperature of the stack by less than 1 K. We show that both undoping and doping is feasible also for the large intrinsic Josephson junction stacks used for THz generation. Even moderate changes in doping introduce large changes in the THz emission properties of the stacks. The highest emission power was achieved after doping a pristine sample.

Published
2017

37. CMB Analysis of Boomerang and Maxima and the Cosmic Parameters {Omega_tot,Omega_b h^2,Omega_cdm h^2,Omega_Lambda,n_s}

Author

Bond, JR, Ade, P, Balbi, A, Bock, J, Borrill, J, Boscaleri, A, Coble, K, Crill, B, Bernardis, PD, Farese, P, Ferreira, P, Ganga, K, Giacometti, M, Hanany, S, Hivon, E, Hristov, V, Iacoangeli, A, Jaffe, A, Lange, A, Lee, A, Martinis, L, Masi, S, Mauskopf, P, Melchiorri, A, Montroy, T, Netterfield, B, Oh, S, Pascale, E, Piacentini, F, Pogosyan, D, Prunet, S, Rabii, B, Rao, S, Richards, P, Romeo, G, Ruhl, J, Scaramuzzi, F, Sforna, D, Sigurdson, K, Smoot, G, Stompor, R, Winant, C, and Wu, P

Subjects
Astrophysics::Cosmology and Extragalactic Astrophysics
Abstract

We show how estimates of parameters characterizing inflation-based theories of structure formation localized over the past year when large scale structure (LSS) information from galaxy and cluster surveys was combined with the rapidly developing cosmic microwave background (CMB) data, especially from the recent Boomerang and Maxima balloon experiments. All current CMB data plus a relatively weak prior probability on the Hubble constant, age and LSS points to little mean curvature (Omega_{tot} = 1.08\pm 0.06) and nearly scale invariant initial fluctuations (n_s =1.03\pm 0.08), both predictions of (non-baroque) inflation theory. We emphasize the role that degeneracy among parameters in the L_{pk} = 212\pm 7 position of the (first acoustic) peak plays in defining the $\Omega_{tot}$ range upon marginalization over other variables. Though the CDM density is in the expected range (\Omega_{cdm}h^2=0.17\pm 0.02), the baryon density Omega_bh^2=0.030\pm 0.005 is somewhat above the independent 0.019\pm 0.002 nucleosynthesis estimate. CMB+LSS gives independent evidence for dark energy (Omega_\Lambda=0.66\pm 0.06) at the same level as from supernova (SN1) observations, with a phenomenological quintessence equation of state limited by SN1+CMB+LSS to w_Q

Published
2016

38. The Cosmic Background Radiation circa nu2K

Author

Bond, J. R., Pogosyan, D., Prunet, S., collaboration, the MaxiBoom, Ade, P., Balbi, A., Bock, J., Borrill, J., Boscaleri, A., Coble, K., Crill, B., de Bernardis, P., Farese, P., Ferreira, P., Ganga, K., Giacometti, M., Hanany, S., Hivon, E., Hristov, V., Iacoangeli, A., Jaffe, A., Lange, A., Lee, A., Martinis, L., Masi, S., Mauskopf, P., Melchiorri, A., Montroy, T., Netterfield, B., Oh, S., Pascale, E., Piacentini, F., Rabii, B., Rao, S., Richards, P., Romeo, G., Ruhl, J., Scaramuzzi, F., Sforna, D., Smoot, G., Stompor, R., Winant, C., and Wu, P.

Subjects
Inflation (cosmology), Physics, Nuclear and High Energy Physics, Structure formation, Astrophysics (astro-ph), Cosmic microwave background, Cosmic background radiation, FOS: Physical sciences, Astrophysics, Astrophysics::Cosmology and Extragalactic Astrophysics, Omega, Atomic and Molecular Physics, and Optics, Redshift, Big Bang nucleosynthesis, High Energy Physics::Experiment, Neutrino
Abstract

We describe the implications of cosmic microwave background (CMB) observations and galaxy and cluster surveys of large scale structure (LSS) for theories of cosmic structure formation, especially emphasizing the recent Boomerang and Maxima CMB balloon experiments. The inflation-based cosmic structure formation paradigm we have been operating with for two decades has never been in better shape. Here we primarily focus on a simplified inflation parameter set, {omega_b,omega_{cdm},Omega_{tot}, Omega_\Lambda,n_s,\tau_C, \sigma_8}. Combining all of the current CMB+LSS data points to the remarkable conclusion that the local Hubble patch we can access has little mean curvature (Omega_{tot}=1.08\pm 0.06) and the initial fluctuations were nearly scale invariant (n_s=1.03\pm 0.08), both predictions of (non-baroque) inflation theory. The baryon density is found to be slightly larger than that preferred by independent Big Bang Nucleosynthesis estimates (omega_b=0.030\pm 0.005 cf. 0.019\pm 0.002). The CDM density is in the expected range (omega_{cdm}=0.17 \pm 0.02). Even stranger is the CMB+LSS evidence that the density of the universe is dominated by unclustered energy akin to the cosmological constant (Omega_\Lambda=0.66\pm 0.06), at the same level as that inferred from high redshift supernova observations. We also sketch the CMB+LSS implications for massive neutrinos., Comment: 7 pages, 4 figs., in Proc. Neutrino 2000 (Elsevier), CITA-2000-63

Published
2016

39. Constructing gene network based on biclusters of expression data

Author

Feng Liu, Sun Sl, Yang L, Tian Zz, and Wu P

Subjects
0301 basic medicine, Genetics, Correlation coefficient, Basis (linear algebra), Models, Genetic, Gene Expression Profiling, Gene regulatory network, Gene Expression, General Medicine, Computational biology, Biology, Gene expression profiling, Correlation, 03 medical and health sciences, 030104 developmental biology, Gene expression, Cluster Analysis, Gene Regulatory Networks, Molecular Biology, Gene, Function (biology), Algorithms, Oligonucleotide Array Sequence Analysis
Abstract

Two genes can be co-regulated and possibly have the similar function if they are similarly expressed, which provides a theoretical basis for construction of gene regulatory networks using gene expression data. Herein, a new method of gene regulatory network was constructed based on biclusters in this paper. Given a bicluster, this paper analyzes the correlation between genes in the clusters and then constructs the gene regulatory network by selecting genes with a correlation coefficient.

Published
2016

40. Influenza vaccine effectiveness in preventing hospitalization among Beijing residents in China, 2013-15

Author

Qin Y, Zhang Y, Wu P, Feng S, Zheng J, Yang P, Pan Y, Wang Q, Feng L, Pang X, Puig-Barberà J, Yu H, and Cowling BJ

Abstract

Background: Estimates of influenza vaccination effectiveness (VE) are valuable for populations where the vaccine has been promoted in order to support vaccination policy and to permit evaluation of vaccination strategies. Such studies would be important for China due to limited data available during seasons when the vaccine strains matched or mismatched the circulating viruses. Methods: We conducted a test-negative study in hospitals in Beijing. Patients admitted to five hospitals in the city were enrolled during the winter influenza seasons of 2013-14 and 2014-15. Influenza virus infections were determined by PCR, and influenza vaccination records were extracted from a centralized electronic immunization registry. Influenza VE was estimated by logistic regression adjusting for age group, sex and chronic conditions, and matched by calendar week. Results: A total of 2368 inpatients were recruited during the study period with a vaccination coverage in the control group of 12.8%. The overall estimate of influenza VE was 46.9% (95% CI: -20.4%, 76.6%) for the 2013-14 season and 5.0% (95% CI: -53.0%, 41.0%) for the 2014-15 season. Estimates of VE were relatively higher in children aged 6-17 years than older persons across two influenza seasons while estimates of VE for both adults and elderly were relatively low. Conclusions: Our findings were consistent with expected influenza vaccination effectiveness in seasons when the vaccine matched or mismatched circulating viruses. Strategies to increase influenza vaccine coverage could provide a public health benefit. (C) 2016 Elsevier Ltd. All rights reserved.

Published
2016

41. Design and Realization of Payload Operation and Application System of China’s Space Station

Author

Wang H, Guo L, and Wu P

Subjects
Hardware architecture, Engineering, business.industry, Payload, Human spaceflight, ComputerSystemsOrganization_COMPUTER-COMMUNICATIONNETWORKS, Avionics, ComputingMilieux_GENERAL, Flight dynamics, Systems architecture, Space Science, Aerospace engineering, business, Realization (systems), Computer hardware
Abstract

China's Space Station will be launched in the year 2018; this space station is China's largest space science experiment and application platform until now. This paper mainly introduces the function composition of payload operation and application system of China’s space station, system architecture, hardware architecture and the new technology we use to implement the payload operation and application ground system of China's space station.

Published
2016

42. Development and evaluation of a physically based multiscalar drought index: The Standardized Moisture Anomaly Index

Author

Zhang, B., Zhao, X., Jin, Jiming, Wu, P., and Blackwell Publishing Ltd

Subjects
Civil and Environmental Engineering, drought, PDSI, SPEI, SZI, the Loess Plateau, Yellow River
Abstract

In this study, a new physically based multiscalar drought index, the Standardized Moisture Anomaly Index (SZI), was developed and evaluated, which combines the advantages of the Palmer Drought Severity Index (PDSI) and the Standardized Precipitation Evapotranspiration Index (SPEI). The SZI is based on the water budget simulations produced with a sophisticated hydrological model, and it also includes a multiscalar feature to quantify drought events at different temporal scales taken from SPEI. The Chinese Loess Plateau was selected to evaluate the performance of the SZI. Our evaluation indicates that the SZI accurately captures the onset, duration, and ending of a multiyear drought event through its multiscalar feature, while the PDSI, which lacks this feature, is often unable to describe the evolution of a multiyear drought event. In addition, the variability of the SZI is more consistent with observed streamflow and the satellite normalized difference vegetation index than that of the Standardized Precipitation Index and the SPEI. Although the SPEI includes potential evapotranspiration (PE) as water demand, water demand is often unrealistically estimated based solely on PE, especially over arid and semiarid regions. The improved drought quantification with the SZI is the result of a more reasonable estimation of water demand by including evapotranspiration, runoff, and any change in soil moisture storage. In general, our newly developed SZI is physically based and includes a multiscalar feature, which enables it to provide better information for drought monitoring and identification at different temporal scales. © 2015. American Geophysical Union. All Rights Reserved.

Published
2015

43. Robust diamond-like Fe-Si network in the zero-strain NaxFeSiO4 Cathode

Author

Ye, Z., Zhao, X., Li, S. D., Wu, S. Q., Wu, P., Nguyen, M. C., Guo, J. H., Mi, J. X., Gong, Z. L., Zhu, Z. Z., Yang, Y., Wang, C. Z., and Ho, K. M.

Subjects
Condensed Matter - Materials Science, Materials Science (cond-mat.mtrl-sci), FOS: Physical sciences, Computational Physics (physics.comp-ph), Physics - Computational Physics
Abstract

Sodium orthosilicates Na2MSiO4 (M denotes transition metals) have attracted much attention due to the possibility of exchanging two electrons per formula unit. In this work, we report a group of sodium iron orthosilicates Na2FeSiO4, the crystal structures of which are characterized by a diamond-like Fe-Si network. The Fe-Si network is quite robust against the charge/discharge process, which explains the high structural stability observed in experiment. Using the density functional theory within the GGA+U framework and X-ray diffraction studies, the crystal structures and structural stabilities during the sodium insertion/deinsertion process are systematically investigated. The calculated average deintercalation voltages are in good agreement with the experimental result., Comment: 14 pages, 8 figures

Published
2015
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45. Take-off and landing using ground based power - landing simulations using multibody dynamics

Author

Wu, P., Mark Voskuijl, and Tooren, M. J. L.

Subjects
assisted takeoff and landing, multibody dynamics, field performance, aircraft landing
Abstract

A novel take-off and landing system using ground based power is proposed in the EUFP7 project GABRIEL. The proposed system has the potential benefit to reduce aircraft weight, emissions and noise. A preliminary investigation of the feasibility of the structural design of the connection mechanism between aircraft and ground system has been performed by simulating the landing procedure on a moving ground system. One of the key challenges is the landing on a moving ground system under high crosswind conditions. The main focus in the current research is the calculation of the impact loads on both aircraft and ground system for a wide range of landing conditions (sink rate, velocity differences between aircraft and ground system, etc.). For comparison, conventional landing procedures with a traditional landing gear have also been simulated. Two different aerodynamic models (empirical and vortex lattice method) have been used and compared in the simulations for verification and validation purposes. The results of this research study are a set of load cases and operational constraints that can be used for the structural design of the ground system and modifications to the aircraft. Detailed values are presented in the paper.

Published
2014

46. Thermal and electromagnetic properties of Bi$_2$Sr$_2$CaCu$_2$O$_8$ intrinsic Josephson junction stacks studied via one-dimensional coupled sine-Gordon equations

Author

Rudau, F., Tsujimoto, M., Gross, B., Judd, T. E., Wieland, R., Goldobin, E., Kinev, N., Yuan, J., Huang, Y., Ji, M., Zhou, X. J., An, D. Y., Ishii, A., Mints, R. G., Wu, P. H., Hatano, T., Wang, H. B., Koshelets, V. P., Koelle, D., and Kleiner, R.

Subjects
Superconductivity (cond-mat.supr-con), Condensed Matter - Superconductivity, Condensed Matter::Superconductivity, FOS: Physical sciences
Abstract

We used one-dimensional coupled sine-Gordon equations combined with heat diffusion equations to numerically investigate the thermal and electromagnetic properties of a $300\,\mu\mathrm{m}$ long intrinsic Josephson junction stack consisting of $N = 700$ junctions. The junctions in the stack are combined to $M$ segments where we assume that inside a segment all junctions behave identically. Most simulations are for $M = 20$. For not too high bath temperatures there is the appearence of a hot spot at high bias currents. In terms of electromagnetic properties, robust standing wave patterns appear in the current density and electric field distributions. These patterns come together with vortex/antivortex lines across the stack that correspond to $\pi$ kink states, discussed before in the literature for a homogeneous temperature distribution in the stack. We also discuss scaling of the thermal and electromagnetic properties with $M$, on the basis of simulations with $M$ between 10 and 350., Comment: 17 pages, 17 figures

Published
2014
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47. Incommensurate spin density wave as a signature of spin-orbit coupling

Author

Farrell, Aaron, Wu, P. -K., Kao, Y. -J., and Pereg-Barnea, T.

Subjects
Condensed Matter::Quantum Gases, Condensed Matter - Strongly Correlated Electrons, Strongly Correlated Electrons (cond-mat.str-el), FOS: Physical sciences, Condensed Matter::Strongly Correlated Electrons
Abstract

Close to half filling and in the limit of strong interactions the Hubbard model leads a spin Hamiltonian. In its original isotropic form this is the Heisenberg model with antiferromagnetic coupling $J$. On a square lattice there is no frustration and the ground state is a classical antiferromagnet denoted by the commensurate order vector ${\bf Q}=(\pi,\pi)$. In this work we show that the inclusion of spin orbit coupling (SOC) in the fermionic Hubbard model on a square lattice leads to an incommensurate spin density wave (ISDW) in the strong interactions limit at half filling. In this limit the Hubbard model leads to a non-diagonal and anisotropic spin Hamiltonian which exhibits the incommensurate spin order as its classical ground state. We note that an ISDW can be found in systems regardless of spin orbit-coupling due to nesting and lattice distortion. These effects, however, can usually be recognized by experimental probes., Comment: Main Text: 5 pages, 3 figures. Supplementary material: 3 pages, 2 figures

Published
2014
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48. von K��rm��n energy decay and heating of protons and electrons in a kinetic turbulent plasma

Author

Wu, P., Wan, M., Matthaeus, W. H., Shay, M. A., and Swisdak, M.

Subjects
Plasma Physics (physics.plasm-ph), Physics::Space Physics, FOS: Physical sciences, Space Physics (physics.space-ph)
Abstract

Decay in time of undriven weakly collisional kinetic plasma turbulence in systems large compared to the ion kinetic scales is investigated using fully electromagnetic particle-in-cell simulations initiated with transverse flow and magnetic disturbances, constant density, and a strong guide field. The observed energy decay is consistent with the von K��rm��n hypothesis of similarity decay, in a formulation adapted to magnetohydrodyamics (MHD). Kinetic dissipation occurs at small scales, but the overall rate is apparently controlled by large scale dynamics. At small turbulence amplitude the electrons are preferentially heated. At larger amplitudes proton heating is the dominant effect. In the solar wind and corona the protons are typically hotter, suggesting that these natural systems are in large amplitude turbulence regime., Accepted by Phys. Rev. Lett. on August 29, 2013

Published
2013
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49. Aldosterone biosynthesis and action in vascular cells

Author

Kazuhiro Iki, Ryoyu Takeda, Hiroshi Yamamoto, Yoshiyu Takeda, Isamu Miyamori, Wu P. Sheng, Haruhiko Hatakeyama, and Ivan A. Blair

Subjects
Male, medicine.medical_specialty, medicine.drug_class, Molecular Sequence Data, Clinical Biochemistry, Polymerase Chain Reaction, Biochemistry, Gas Chromatography-Mass Spectrometry, Muscle, Smooth, Vascular, chemistry.chemical_compound, Endocrinology, Mineralocorticoid receptor, Cytochrome P-450 Enzyme System, Corticosterone, Internal medicine, medicine, Animals, Cytochrome P-450 CYP11B2, Humans, Rats, Wistar, Autocrine signalling, Aldosterone, Molecular Biology, Cells, Cultured, Chromatography, High Pressure Liquid, Vascular tissue, Pharmacology, Base Sequence, biology, Organic Chemistry, Angiotensin-converting enzyme, Mesenteric Arteries, Rats, Perfusion, Receptors, Mineralocorticoid, medicine.anatomical_structure, chemistry, Mineralocorticoid, biology.protein, Steroid 11-beta-Hydroxylase, Steroids, Endothelium, Vascular, Blood vessel
Abstract

In view of the hypothetical possibility that the vascular renin-angiotensin system (RAS) might include aldosterone biosynthesis and action in the vasculature, we have undertaken a study to identify aldosterone released into the perfusion circuit from the rat mesenteric artery, and to investigate the effects of an angiotensin converting enzyme inhibition (ACEI) on aldosterone production from the vasculature. After 30 min equilibration, 240 mL of perfusate was collected and subjected to reverse-phase HPLC and subsequent mass spectrometry. Mass spectra corresponding to authentic corticosterone and aldosterone were obtained from the samples of mesenteric artery perfusate. Production of aldosterone in the mesenteric artery was not changed by adrenalectomy, although it was reduced in the arterial perfusate from rats pretreated with ACEI. By RT-PCR the expression of CYP 11B2 and mineralocorticoid receptor genes were demonstrated in both vascular endothelial and smooth muscle cells. These studies constitute indirect evidence supporting our hypothesis that locally produced aldosterone in the vascular tissue acts on vascular tone and remodeling via a paracrine or autocrine manner.

Published
1995

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