Your search keyword '"K. Lung"' showing total 80 results

1. B03 CARFILZOMIB AND LENALIDOMIDE FOR PRIMARY PLASMA CELL LEUKEMIA: FINAL RESULTS OF THE PROSPECTIVE PHASE 2 EMN12/HOVON-129 STUDY FOR PATIENTS AGED ≥66 YEARS

Author

P. Musto, M.C. Minnema, W.W.H. Roeloffzen, A. Capra, B. van der Holt, A. Juul Vangsted, A. Broyl, F. Schjesvold, T. Lund, T. Silkjaer, R. Benjamin, M. Grasso, K. Lung Wu, J. Caers, M. Cavo, R. Hájek, B. Bruno, A. Gadisseur, G. Pietrantuono, M. Offidani, L. Pour, P. Sonneveld, M. Boccadoro, and N. van de Donk

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2023

2. Enhancing the Physical, Antimicrobial, and Osteo/Odontogenic Properties of a Sol–Gel-Derived Tricalcium Silicate by Graphene Oxide for Vital Pulp Therapies

Author

Mohamed Mahmoud Abdalla, Mohammed Zahedul Islam Nizami, Vidhyashree Rajasekar, Mohammed Basabrain, Christie Y. K. Lung, and Cynthia Kar Yung Yiu

Subjects

sol–gel, tricalcium silicate, graphene oxide, vital pulp therapy, human dental pulp stem cells, Biotechnology, TP248.13-248.65, Medicine (General), R5-920

Abstract

Objectives: This study developed a sol–gel tricalcium silicate/graphene oxide (TCS-GO) composite and examined its physicochemical properties, antimicrobial activity, and osteo/odontogenic effect on dental pulp stem cells. Methods: Tricalcium silicate was synthesized and combined with graphene oxide at three different concentrations, namely 0.02%, 0.04%, and 0.08% w/w, while tricalcium silicate and mineral trioxide aggregate served as controls. The setting time, compressive strength, pH, and calcium ion release of the composites were evaluated, as well as antimicrobial properties against Streptococcus mutans and Lactobacillus acidophilus. Additionally, the viability of dental pulp stem cells; apatite forming ability; and the gene expression of Alkaline phosphatase, Dentin sialophosphoprotein, and Runt-related transcription factor 2 were assessed. Results: TCS-GO (0.08%) showed a significantly shorter setting time and higher compressive strength when compared to MTA (p < 0.05). Additionally, tricalcium silicate and TCS-GO groups showed a higher release of Ca ions than MTA, with no significant difference in pH values among the different groups. TCS-GO (0.08%) also demonstrated a significantly stronger antimicrobial effect against Lactobacillus acidophilus compared to MTA (p < 0.05). ALP expression was higher in TCS-GO (0.08%) than MTA on days 3 and 7, while DSPP expression was higher in TCS-GO (0.08%) than MTA on day 3 but reversed on day 7. There was no significant difference in RUNX2 expression between TCS-GO (0.08%) and MTA on days 3 and 7. Conclusions: The TCS-GO (0.08%) composite demonstrated superior physicochemical characteristics and antimicrobial properties compared to MTA. Moreover, the early upregulation of ALP and DSPP markers in TCS-GO (0.08%) indicates that it has the potential to promote and enhance the osteo/odontogenic differentiation of DPSCs.

Published

2024

3. Physicochemical Properties and Inductive Effect of Calcium Strontium Silicate on the Differentiation of Human Dental Pulp Stem Cells for Vital Pulp Therapies: An In Vitro Study

Author

Mohamed Mahmoud Abdalla, Christie Y. K. Lung, Mohammed Nadeem Bijle, and Cynthia Kar Yung Yiu

Subjects

calcium strontium silicate, setting time, bioactivity, dental pulp stem cells, sol–gel, differentiation, Technology, Electrical engineering. Electronics. Nuclear engineering, TK1-9971, Engineering (General). Civil engineering (General), TA1-2040, Microscopy, QH201-278.5, Descriptive and experimental mechanics, QC120-168.85

Abstract

The development of biomaterials that exhibit profound bioactivity and stimulate stem cell differentiation is imperative for the success and prognosis of vital pulp therapies. The objectives were to (1) synthesize calcium strontium silicate (CSR) ceramic through the sol–gel process (2) investigate its physicochemical properties, bioactivity, cytocompatibility, and its stimulatory effect on the differentiation of human dental pulp stem cells (HDPSC). Calcium silicate (CS) and calcium strontium silicate (CSR) were synthesized by the sol–gel method and characterized by x-ray diffraction (XRD). Setting time, compressive strength, and pH were measured. The in vitro apatite formation was evaluated by SEM-EDX and FTIR. The NIH/3T3 cell viability was assessed using an MTT assay. The differentiation of HDPSC was evaluated using alkaline phosphatase activity (ALP), and Alizarin red staining (ARS). Ion release of Ca, Sr, and Si was measured using inductive coupled plasma optical emission spectroscopy (ICP-OES). XRD showed the synthesis of (CaSrSiO4). The initial and final setting times were significantly shorter in CSR (5 ± 0.75 min, 29 ± 1.9 min) than in CS (8 ± 0.77 min, 31 ± 1.39 min), respectively (p < 0.05). No significant difference in compressive strength was found between CS and CSR (p > 0.05). CSR demonstrated higher apatite formation and cell viability than CS. The ALP activity was significantly higher in CSR 1.16 ± 0.12 than CS 0.92 ± 0.15 after 14 d of culture (p < 0.05). ARS showed higher mineralization in CSR than CS after 14 and 21 d culture times. CSR revealed enhanced differentiation of HDPSC, physicochemical properties, and bioactivity compared to CS.

Published

2022

4. Krüppel-like factor 2 is required for normal mouse cardiac development.

Author

Aditi R Chiplunkar, Tina K Lung, Yousef Alhashem, Benjamin A Koppenhaver, Fadi N Salloum, Rakesh C Kukreja, Jack L Haar, and Joyce A Lloyd

Subjects

Medicine, Science

Abstract

Krüppel-like factor 2 (KLF2) is expressed in endothelial cells in the developing heart, particularly in areas of high shear stress, such as the atrioventricular (AV) canal. KLF2 ablation leads to myocardial thinning, high output cardiac failure and death by mouse embryonic day 14.5 (E14.5) in a mixed genetic background. This work identifies an earlier and more fundamental role for KLF2 in mouse cardiac development in FVB/N mice. FVB/N KLF2-/- embryos die earlier, by E11.5. E9.5 FVB/N KLF2-/- hearts have multiple, disorganized cell layers lining the AV cushions, the primordia of the AV valves, rather than the normal single layer. By E10.5, traditional and endothelial-specific FVB/N KLF2-/- AV cushions are hypocellular, suggesting that the cells accumulating at the AV canal have a defect in endothelial to mesenchymal transformation (EMT). E10.5 FVB/N KLF2-/- hearts have reduced glycosaminoglycans in the cardiac jelly, correlating with the reduced EMT. However, the number of mesenchymal cells migrating from FVB/N KLF2-/- AV explants into a collagen matrix is reduced considerably compared to wild-type, suggesting that the EMT defect is not due solely to abnormal cardiac jelly. Echocardiography of E10.5 FVB/N KLF2-/- embryos indicates that they have abnormal heart function compared to wild-type. E10.5 C57BL/6 KLF2-/- hearts have largely normal AV cushions. However, E10.5 FVB/N and C57BL/6 KLF2-/- embryos have a delay in the formation of the atrial septum that is not observed in a defined mixed background. KLF2 ablation results in reduced Sox9, UDP-glucose dehydrogenase (Ugdh), Gata4 and Tbx5 mRNA in FVB/N AV canals. KLF2 binds to the Gata4, Tbx5 and Ugdh promoters in chromatin immunoprecipitation assays, indicating that KLF2 could directly regulate these genes. In conclusion, KLF2-/- heart phenotypes are genetic background-dependent. KLF2 plays a role in EMT through its regulation of important cardiovascular genes.

Published

2013

5. Canadian Surgery Forum 2018: St. John’s, NL Sept. 13–15, 2018

Author

S, Jayaraman, L, Lee, J, Mata, R, Droeser, P, Kaneva, S, Liberman, P, Charlebois, B, Stein, G, Fried, L, Feldman, M, Schellenberg, K, Inaba, V, Cheng, J, Bardes, L, Lam, E, Benjamin, K, Matsushima, D, Demetriades, J, Cho, A, Strumwasser, D, Grabo, C, Bir, A, Eastman, N, Orozco, J, Chen, C, Park, T, Kang, J, Jung, J, Elfassy, T, Grantcharov, J, Taylor, M, Stem, D, Yu, S, Chen, S, Fang, S, Gearhart, B, Safar, J, Efron, P, Serrano, S, Parpia, D, McCarty, N, Solis, M, Valencia, S, Jibrael, A, Wei, S, Gallinger, M, Simunovic, A, Hummadi, M, Rabie, M, Al Skaini, H, Shamshad, S, Shah, K, Verhoeff, P, Glen, A, Taheri, B, Min, B, Tsang, V, Fawcett, S, Widder, M, Yang, K, Wanis, O, Gilani, K, Vogt, M, Ott, J, VanKoughnett, C, Vinden, S, Balvardi, E, St Louis, Y, Yousef, A, Toobaie, E, Guadagno, R, Baird, D, Poenaru, A, Kleiman, B, Mador, C, Moulton, E, Lee, C, Li, K, Beyfuss, H, Solomon, N, Sela, V, McAlister, A, Ritter, J, Hallet, M, Tsang, G, Martel, D, Jalink, M, Husien, C, Gu, M, Levine, S, Otiti, J, Nginyangi, C, Yeo, J, Ring, M, Holden, T, Ungi, G, Fichtinger, B, Zevin, B, Fang, J, Dang, S, Karmali, M, Kim, B, Zhang, E, Duceppe, S, Rieder, A, Maeda, A, Okrainec, T, Jackson, F, Kegel, S, Lachance, T, Landry, C, Mueller, S, Joharifard, E, Nyiemah, C, Howe, C, Dobboh, L Gizzie, Kortimai, A, Kabeto, J, Beste, N, Garraway, R, Riviello, S, Hameed, S, Shinde, G, Marcil, S, Prasad, J, Arminan, E, Debru, N, Church, R, Gill, P, Mitchell, M, Delisle, C, Chernos, J, Park, K, Hardy, A, Vergis, M, Guez, D, Hong, J, Koichopolos, R, Hilsden, D, Thompson, F, Myslik, J, Vandeline, R, Leeper, A, Doumouras, S, Govind, S, Valanci, N, Alhassan, T, Wong, N, Nadkarni, S, Chia, D, Seow, D, Carter, L, Ruo, O, Levine, L, Allen, P, Murphy, R, van Heest, F, Saleh, S, Minor, P, Engels, E, Joos, C, Wang, R, Nenshi, M, Meschino, C, Laane, N, Parry, M, Hameed, A, Lacoul, C, Chrystoja, J, Ramjist, R, Sutradhar, L, Lix, N, Baxter, D, Urbach, J, Ahlin, S, Patel, S, Nanji, S, Merchant, K, Lajkosz, S, Brogly, P, Groome, J, Sutherland, G, Liu, T, Crump, M, Bair, A, Karimuddin, A, Peterson, J, Hawel, E, Shlomovitz, I, Habaz, A, Elnahas, N, Alkhamesi, C, Schlachta, G, Akhtar-Danesh, T, Daodu, V, Nguyen, R, Dearden, I, Datta, L, Hampton, A, Kirkpatrick, J, McKee, J, Regehr, P, Brindley, D, Martin, A, LaPorta, L, Gillman, K, DeGirolamo, K, D'Souza, L, Hartford, D, Gray, C, Clarke, R, Wigen, C, Garcia-Ochoa, S, Gray, A, Maciver, J, Van Koughnett, K, Leslie, T, Zwiep, S, Ahn, J, Greenberg, F, Balaa, D, McIsaac, R, Musselman, I, Raiche, L, Williams, H, Moloo, M, Nguyen, D, Naidu, P, Karanicolas, A, Nadler, R, Raskin, V, Khokhotva, R, Poirier, C, Plourde, A, Paré, M, Marchand, M, Leclair, J, Deshaies, P, Hebbard, I, Ratnayake, K, Decker, E, MacIntosh, Z, Najarali, A, Alhusaini, A, McClure, M, Dakouo, R, Behman, A, Nathens, N Look, Hong, P, Pechlivanoglou, K, Lung, P, Simone, E, Schemitsch, L, Chen, L, Rosenkrantz, N, Schuurman, R, George, E, Shavit, A, Pawliwec, Z, Rana, D, Evans, P, Dawe, R, Brown, G, Lefebvre, K, Devenny, D, Héroux, C, Bowman, R, Mimeault, L, Calder, L, Baker, R, Winter, C, Cahill, D, Fergusson, T, Schroeder, K, Kahnamoui, S, Elkheir, F, Farrokhyar, B, Wainman, O, Hershorn, S, Lim, A, Arora, F, Wright, J, Escallon, L, Gotlib, M, Allen, N, Gawad, I, Raîche, G, Jeyakumar, D, Li, M, Aarts, A, Giles, T, Dumitra, R, Alam, J, Fiore, M, Vassiliou, O, Al Busaidi, A, Brobbey, T, Stelfox, T, Chowdhury, J, Kortbeek, C, Ball, N, AlShahwan, S, Fraser, A, Tran, A, Martel, N, Manhas, D, Mannina, A, Behman, B, Haas, A, Fowler, L, Findlay-Shirras, H, Singh, N, Biswanger, A, Gosselin-Tardif, M Abou, Khalil, J Mata, Gutierrez, A, Guigui, L, Ferri, D, Roberts, L, Moore, J, Holcomb, J, Harvin, J, Sadek, P, Belanger, K, Nadeau, K, Mullen, D, Aitkens, K, Foss, D, MacIsaac, S, Zhang, M, Methot, L, Hookey, J, Yates, I, Perelman, E, Saidenberg, S, Khair, J, Lampron, A, Tinmouth, S, Hammond, D, Hochman, M, Lê, R, Rabbani, A, Abou-Setta, R, Zarychanski, B, Elsoh, B, Goldacre, G, Nash, M, Trepanier, N, Wong-Chong, C, Sabapathy, P, Chaudhury, N, Bradley, C, Dakin, N, Holm, W, Henderson, M, Roche, A, Sawka, E, Tang, B, Huang, T, Gimon, R, Rochon, M, Lipson, W, Buie, A, MacLean, E, Lau, V, Mocanu, I, Tavakoli, N, Switzer, C, Tian, C, de Gara, D, Birch, P, Young, C, Chiu, A, Meneghetti, G, Warnock, M, Meloche, O, Panton, A, Istl, A, Gan, P, Colquhoun, R, Habashi, S, Stogryn, J, Metcalfe, K, Clouston, N, Zondervan, K, McLaughlin, J, Springer, J, Lee, N, Amin, M, Caddedu, C, Eskicioglu, A, Warraich, D, Keren, N, Kloos, S, Gregg, R, Mohamed, E, Dixon, R, Rochan, A, Domouras, S, Kelly, I, Yang, S, Forbes, R, Garfinkle, S, Bhatnagar, G, Ghitulescu, C, Vasilevsky, N, Morin, M, Boutros, A, Petrucci, P, Sylla, S, Wexner, G, Sigler, J, Faria, P, Gordon, L, Azoulay, A, Liberman, S, Khorasani, A, de Buck van Overstraeten, E, Kennedy, N, Pecorelli, D, Mouldoveanu, A, Gosselin-Tardiff, J, Chau, F Rouleau, Fournier, P, Bouchard, J Abou, Khalil, J, Motter, J, Mottl, G, Hwang, J, Kelly, G, Nassif, M, Albert, J, Monson, J, McLeod, J, Cha, M, Raval, T, Phang, C, Brown, R, Robertson, F, Letarte, A, Antoun, V, Pelsser, E, Hyun, K, Clouston-Chambers, R, Helewa, S, Candy, Z, Mir, N, Hanna, A, Azin, D, Hirpara, F, Quereshy, C, O'Brien, S, Chadi, S, Punnen, H, Yoon, W, Xiong, H, Stuart, J, Andrews, R, Selvam, S, Wong, W, Hopman, P, MacDonald, F, Dossa, B, Medeiros, C, Keng, S, Acuna, J, Hamid, A, Ghuman, N, Kasteel, D, Buie, T, McMullen, A, Elwi, T, MacLean, H, Wang, F, Coutinho, Q, Le, L, Shack, H, Roy, R, Kennedy, J, Bunn, W, Chung, M, Elmi, E, Wakeam, R, Presutti, S, Keshavjee, T, Cil, D, McCready, V, Cheung, C, Schieman, J, Bailey, G, Nelson, T, Batchelor, S, Grondin, A, Graham, N, Safieddine, S, Johnson, W, Hanna, D, Low, A, Seely, E, Bedard, C, Finley, R, Nayak, D, Lougheed, D, Petsikas, A, Kinio, V Ferreira, Resende, C, Anstee, D, Maziak, S, Gilbert, F, Shamji, S, Sundaresan, P, Villeneuve, J, Ojah, A, Ashrafi, A, Najjar, I, Yamani, S, Sersar, A, Batouk, D, Parente, A, Laliberte, M, McInnis, C, McDonald, Y, Hasnain, K, Yasufuku, T, Waddell, N, Chopra, C, Nicholson-Smith, R, Malthaner, R, Patel, M, Doubova, H, Robaidi, E, Delic, A, Fazekas, K, Hughes, P, Pinkney, Y, Lopez-Hernandez, M, Coret, L, Schneider, J, Agzarian, Y, Shargall, M, Mehta, K, Pearce, V, Gupta, N, Coburn, B, Kidane, K, Hess, C, Compton, J, Ringash, G, Darling, A, Mahar, P, Thomas, J, Vernon, J, Spicer, S, Renaud, J, Seitlinger, Y, Al Lawati, F, Guerrera, P, Falcoz, G, Massard, D, Hylton, J, Huang, S, Turner, D, French, C, Wen, J, Masters, C, Fahim, D, St-Pierre, E, Ruffini, M, Inra, Z, Abdelsattar, S, Cassivi, F, Nichols, D, Wigle, S, Blackmon, K, Shen, S, Gowing, F Sadegh, Beigee, K, Sheikhy, A Abbasi, Dezfouli, T, Schnurr, L, Linkins, M, Crowther, M, de Perrot, S, Uddin, J, Douketis, L, Angka, A, Jeong, M, Sadiq, M, Kilgour, C Tanese, de Souza, M, Kennedy, R, Auer, R, Adam, R, Memeo, D, Goéré, T, Piardi, E, Lermite, O, Turrini, M, Lemke, J, Li, M, Tun-Abraham, R, Hernandez-Alejandro, S, Bennett, F, Navarro, A, Sa Cunha, P, Pessaux, E, Isenberg-Grzeda, J, Kazdan, S, Myrehaug, S, Singh, D, Chan, C, Law, C, Nessim, G, Paull, A, Ibrahim, E, Sabri, S, Rodriguez-Qizilbash, D, Berger-Richardson, R, Younan, J, Hétu, S, Johnson-Obaseki, F, Angarita, Y, Zhang, A, Govindarajan, E, Taylor, Z, Bayat, D, Bischof, A, McCart, S, Sequeira, S, Samman, S, Cornacchi, G, Foster, L, Thabane, S, Thomson, O, Lovrics, S, Martin, P, Lovrics, N, Latchana, L, Davis, Y, Liu, A, Hammad, D, Kagedan, C, Earle, G, Pang, S, Kupper, M, Quan, R, Hsiao, P, Bongers, M, Lustgarten, D, Goldstein, P, Dhar, L, Rotstein, J, Pasternak, J, Nostedt, L, Gibson-Brokop, M, McCall, D, Schiller, S, Mukhi, L, Mack, N, Singh, M, Chanco, A, Hilchie-Pye, C, Kenyon, A, Mathieson, J, Burke, R, Nason, J, Austin, M, Brar, S, Hurton, S, Kong, Y, Xu, M, Thibedeau, W, Cheung, J, Dort, S, Karim, A, Bouchard-Fortier, Y, Jeong, Q, Li, L, Bubis, C, O'Rourke, N, Dharampal, K, Smith, A, Harvey, R, Pashcke, L, Rudmik, S, Chandarana, S, Buac, S, Latosinsky, N, Shahvary, M, Gervais, G, Leblanc, M, Brackstone, K, Guidolin, B, Yaremko, S, Gaede, K, Lynn, A, Kornecki, G, Muscedere, O, Shmuilovich, I, BenNachum, M, Mouawad, N, Gelman, M, Lock, J, Daza, M, Horkoff, F, Sutherland, O, Bathe, M, Moser, J, Shaw, G, Beck, Y, Luo, S, Ahmed, C, Wall, T, Domes, K, Jana, E, Waugh, J, Baird, P, Newell, P, Hansen, M, Gough, E, McArthur, A, Skaro, G, Gauvin, N, Goel, D, Mutabdzic, F, Lambreton, M, Kilcoyne, K, Ang, A, Karachristos, H, Cooper, J, Hoffman, S, Reddy, L, Park, R, Gilbert, R, Shorr, A, Workneh, K, Bertens, J, Abou-Khalil, H, Smith, J, Levy, J, Ellis, B, Bakanisi, M, Sadeghi, S, Michaelson, V, Tandan, M, Marcaccio, D, Dath, M, Connell, A, Bennett, N, Wasey, R, Sorial, S, Macdonald, D, Johnson, D, Klassen, C, Leung, C, Botkin, M, Bahasadri, S, MacLellan, J, Tan, H, Jun, H, Cheah, K, Wong, N, Harvey, A, Smith, S, Cassie, S, Sun, J, Vallis, L, Twells, K, Lester, D, Gregory, W, Sun, F, Raghavji, M, Laffin, J, Bourget-Murray, A, Reso, A, Jarrar, N, Eipe, A, Budiansky, C, Walsh, J, Mamazza, and M, Rashid

Subjects

Abstracts

Published

2018

6. Analysis of the XENON100 dark matter search data

Author

S. E. A. Orrigo, Marc Schumann, P. Shagin, J. A. M. Lopes, A. Kish, Luke Goetzke, Jean-Pierre Cussonneau, K. E. Lim, Elena Aprile, E. Nativ, W. Hampel, M. Selvi, Ehud Duchovni, K. Bokeloh, E. K. U. Gross, João Cardoso, Hui Wang, Uwe Oberlack, Jochen Schreiner, M. Weber, F. Gao, A. Behrens, T. Marrodán Undagoitia, F. V. Massoli, Qing Lin, M. Le Calloch, J.M.F. dos Santos, O. Vitells, Ch. Weinheimer, A. Rizzo, P. Beltrame, W. Fulgione, N. Priel, C. Grignon, A. J. Melgarejo Fernandez, A. Teymourian, M. Garbini, K. Arisaka, S. Rosendahl, Sebastian Lindemann, M. Alfonsi, F. Arneodo, W. T. Chen, Ran Budnik, Kaixuan Ni, R. Persiani, Karl Giboni, David B. Cline, G. Sartorelli, Laura Baudis, C. Balan, Giacomo Bruno, Hardy Simgen, A. D. Ferella, H. Contreras, E. Pantic, K. Lung, Ethan Brown, M. P. Decowski, Manfred Lindner, Y. Mei, P. R. Scovell, Guillaume Plante, Y. Meng, A. Molinario, S. Fattori, C. Levy, B. Choi, D. Thers, R. F. Lang, J. Lamblin, H. Landsman, L. Scotto Lavina, The XENON100 Collaboration, Astroparticle Physics (IHEF, IoP, FNWI), Aprile, E., Alfonsi, M., Arisaka, K., Arneodo, F., Balan, C., Baudis, L., Behrens, A., Beltrame, P., Bokeloh, K., Brown, E., Bruno, G., Budnik, R., Cardoso, J.M.R., Chen, W.-T., Choi, B., Cline, D.B., Contreras, H., Cussonneau, J.P., Decowski, M.P., Duchovni, E., Fattori, S., Ferella, A.D., Fulgione, W., Gao, F., Garbini, M., Giboni, K.-L., Goetzke, L.W., Grignon, C., Gross, E., Hampel, W., Kish, A., Lamblin, J., Landsman, H., Lang, R.F., Le Calloch, M., Levy, C., Lim, K.E., Lin, Q., Lindemann, S., Lindner, M., Lopes, J.A.M., Lung, K., Marrodán Undagoitia, T., Massoli, F.V., Mei, Y., Melgarejo Fernandez, A.J., Meng, Y., Molinario, A., Nativ, E., Ni, K., Oberlack, U., Orrigo, S.E.A., Pantic, E., Persiani, R., Plante, G., Priel, N., Rizzo, A., Rosendahl, S., Dos Santos, J.M.F., Sartorelli, G., Schreiner, J., Schumann, M., Scotto Lavina, L., Scovell, P.R., Selvi, M., Shagin, P., Simgen, H., Teymourian, A., Thers, D., Vitells, O., Wang, H., Weber, M., and Weinheimer, C.

Subjects

Large Underground Xenon experiment, Physics - Instrumentation and Detectors, Xenon, WIMP, Physics::Instrumentation and Detectors, Direct detection, Dark matter, chemistry.chemical_element, FOS: Physical sciences, DarkSide, WIMP Argon Programme, Nuclear physics, Statistical analysis, Nuclear Experiment, Instrumentation and Methods for Astrophysics (astro-ph.IM), Physics, Time projection chamber, Astrophysics::Instrumentation and Methods for Astrophysics, Astronomy and Astrophysics, Instrumentation and Detectors (physics.ins-det), WIMPs, chemistry, Weakly interacting massive particles, Astrophysics - Instrumentation and Methods for Astrophysics

Abstract

The XENON100 experiment, situated in the Laboratori Nazionali del Gran Sasso, aims at the direct detection of dark matter in the form of weakly interacting massive particles (WIMPs), based on their interactions with xenon nuclei in an ultra low background dual-phase time projection chamber. This paper describes the general methods developed for the analysis of the XENON100 data. These methods have been used in the 100.9 and 224.6 live days science runs from which results on spin-independent elastic, spin-dependent elastic and inelastic WIMP-nucleon cross-sections have already been reported., Comment: 18 pages, 17 figures, information for the 224.6 live days run included

Published

2014

7. DarkSide search for dark matter

Author

I. N. Machulin, R. Klemmer, Marco Pallavicini, N. Rossi, G. Forster, K. Fomenko, W. Sands, G. Di Pietro, H. Cao, D. D'Angelo, M. Komor, A. Razeto, N. N. Nurakhov, R. Saldanha, S. Parmeggiano, A. Nemtzow, E. Shields, F. Perfetto, Min-Xin Guan, M. Gromov, K. Randle, E. V. Unzhakov, S. Bussino, M. Orsini, M. Montuschi, E. Meroni, G. Korga, Austin P. Lund, Marc S. Seigar, A. Tonazzo, E. de Haas, G. Testera, L. Lukyanchenko, S. Gazzana, M. D. Skorokhvatov, B. Rossi, M. De Vincenzi, J. Maricic, L. Grandi, G. Zuzel, Laura Cadonati, M. E. Monzani, Yanhui Ma, D. Durben, M. Zehfus, B. J. Mount, Chung-Yao Yang, Augusto Brigatti, Lawrence Pinsky, A. Kayunov, R. B. Vogelaar, A. Meregaglia, S. Chidzik, C. Joliet, C. Condon, C. Ghiano, A. Pocar, N. Pelliccia, C. L. Kendziora, P. Saggese, A. Nelson, Sandra Zavatarelli, P. X. Li, O. Smirnov, S. Westerdale, Livia Ludhova, A. M. Goretti, A. S. Chepurnov, Thomas Alexander, S. Pordes, E. V. Hungerford, G. Koh, G. Guray, A. Sotnikov, Fausto Ortica, C. Guo, D. A. Semenov, R. Tartaglia, E. Pantic, K. Arisaka, G. Fiorillo, D. Korablev, I. Dratchnev, C. J. Martoff, Frank Calaprice, J. Brodsky, J. Tatarowicz, K. Keeter, Gioacchino Ranucci, Marcin Wójcik, D. Franco, W. Zhong, P. Cavalcante, Henning O. Back, G. Bonfini, P. Beltrame, P. D. Meyers, J. Thompson, An. Ianni, V. N. Muratova, L. Perasso, D. Alton, C. Salvo, S. Perasso, A.V. Etenko, R. Parsells, S. Davini, A. G. Cocco, Al. Ianni, Stefano Maria Mari, S. Luitz, Han Wang, P. J. Mosteiro, F. Gabriele, Jingke Xu, Cristiano Galbiati, D. Montanari, A. Fan, A. Empl, S. Kidner, S. V. Sukhotin, A. Wright, V. V. Kobychev, K. Lung, C. Love, T. Mohayai, A. Candela, S. D. Rountree, Paolo Lombardi, Aldo Romani, B Loer, A. V. Derbin, Y Suvarov, Jay Burton Benziger, T., Alexander, D., Alton, K., Arisaka, H. O., Back, P., Beltrame, J., Benziger, G., Bonfini, A., Brigatti, J., Brodsky, S., Bussino, L., Cadonati, F., Calaprice, A., Candela, H., Cao, P., Cavalcante, A., Chepurnov, S., Chidzik, A. G., Cocco, C., Condon, D., D'Angelo, S., Davini, M. D., Vincenzi, E. D., Haa, A., Derbin, G. D., Pietro, I., Dratchnev, D., Durben, A., Empl, A., Etenko, A., Fan, Fiorillo, Giuliana, D., Franco, K., Fomenko, G., Forster, F., Gabriele, C., Galbiati, S., Gazzana, C., Ghiano, A., Goretti, L., Grandi, M., Gromov, M., Guan, C., Guo, G., Guray, E. V., Hungerford, A., Ianni, C., Joliet, A., Kayunov, K., Keeter, C., Kendziora, S., Kidner, R., Klemmer, V., Kobychev, G., Koh, M., Komor, D., Korablev, G., Korga, P., Li, B., Loer, P., Lombardi, C., Love, L., Ludhova, S., Luitz, L., Lukyanchenko, A., Lund, K., Lung, Y., Ma, I., Machulin, S., Mari, J., Maricic, C. J., Martoff, A., Meregaglia, E., Meroni, P., Meyer, T., Mohayai, D., Montanari, M., Montuschi, M. E., Monzani, P., Mosteiro, B., Mount, V., Muratova, A., Nelson, A., Nemtzow, N., Nurakhov, M., Orsini, F., Ortica, M., Pallavicini, E., Pantic, S., Parmeggiano, R., Parsell, N., Pelliccia, L., Perasso, S., Perasso, Perfetto, Francesco, L., Pinsky, A., Pocar, S., Porde, K., Randle, G., Ranucci, A., Razeto, A., Romani, B., Rossi, N., Rossi, S. D., Rountree, P., Saggese, R., Saldanha, C., Salvo, W., Sand, M., Seigar, D., Semenov, E., Shield, M., Skorokhvatov, O., Smirnov, A., Sotnikov, S., Sukhotin, Y., Suvarov, R., Tartaglia, J., Tatarowicz, G., Testera, J., Thompson, A., Tonazzo, E., Unzhakov, R. B., Vogelaar, H., Wang, S., Westerdale, M., Wojcik, A., Wright, J., Xu, C., Yang, S., Zavatarelli, M., Zehfu, W., Zhong, G., Zuzel, Physics Department, Amherst U., University of Massachusetts System (UMASS), Biomécanique et Bioingénierie (BMBI), Université de Technologie de Compiègne (UTC)-Centre National de la Recherche Scientifique (CNRS), Régulation de l'expression génétique chez les microorganismes (REGCM), 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), Laboratoire Kastler Brossel (LKB (Jussieu)), Fédération de recherche du Département de physique de l'Ecole Normale Supérieure - ENS Paris (FRDPENS), École normale supérieure - Paris (ENS-PSL), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-École normale supérieure - Paris (ENS-PSL), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Université Pierre et Marie Curie - Paris 6 (UPMC)-Centre National de la Recherche Scientifique (CNRS), departement de physique, Albert-Ludwigs-Universität Freiburg, SLAC National Accelerator Laboratory (SLAC), Stanford University, Anhui University [Hefei], Physics Department, Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome] (UNIROMA), Département Recherches Subatomiques (DRS-IPHC), Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université Louis Pasteur - Strasbourg I-Centre National de la Recherche Scientifique (CNRS), Department of Geological Sciences, University of Michigan [Ann Arbor], University of Michigan System-University of Michigan System, 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), Kavli Institute for Particle Astrophysics and Cosmology (KIPAC), Università degli studi di Genova = University of Genoa (UniGe), Departamento de Engenharia Elétrica [Minas Gerais] (DEE - UFMG), Universidade Federal de Minas Gerais, Max-Planck-Institut für Astronomie (MPIA), Max-Planck-Gesellschaft, Rhodes University, Grahamstown, EAST CHINA UNIVERSITY, KEY LAB, Institute of Physics, Polish Academy of Sciences, Polska Akademia Nauk = Polish Academy of Sciences (PAN), International Iberian Nanotechnology Laboratory (INL), Centre de Recherche en Information Biomédicale sino-français (CRIBS), Université de Rennes (UR)-Southeast University [Jiangsu]-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut Européen des membranes (IEM), Université Montpellier 2 - Sciences et Techniques (UM2)-Ecole Nationale Supérieure de Chimie de Montpellier (ENSCM)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Alexander, T, Alton, D, Arisaka, K, Back, Ho, Beltrame, P, Benziger, J, Bonfini, G, Brigatti, A, Brodsky, J, Bussino, Severino Angelo Maria, Cadonati, L, Calaprice, F, Candela, A, Cao, H, Cavalcante, P, Chepurnov, A, Chidzik, S, Cocco, Ag, Condon, C, D'Angelo, D, Davini, S, DE VINCENZI, Mario, De Haas, E, Derbin, A, Di Pietro, G, Dratchnev, I, Durben, D, Empl, A, Etenko, A, Fan, A, Fiorillo, G, Franco, D, Fomenko, K, Forster, G, Gabriele, F, Galbiati, C, Gazzana, S, Ghiano, C, Goretti, A, Grandi, L, Gromov, M, Guan, M, Guo, C, Guray, G, Hungerford, Ev, Ianni, Al, Ianni, An, Joliet, C, Kayunov, A, Keeter, K, Kendziora, C, Kidner, S, Klemmer, R, Kobychev, V, Koh, G, Komor, M, Korablev, D, Korga, G, Li, P, Loer, B, Lombardi, P, Love, C, Ludhova, L, Luitz, S, Lukyanchenko, L, Lund, A, Lung, K, Ma, Y, Machulin, I, Mari, Stefano Maria, Maricic, J, Martoff, Cj, Meregaglia, A, Meroni, E, Meyers, P, Mohayai, T, Montanari, D, Montuschi, M, Monzani, Me, Mosteiro, P, Mount, B, Muratova, V, Nelson, A, Nemtzow, A, Nurakhov, N, Orsini, M, Ortica, F, Pallavicini, M, Pantic, E, Parmeggiano, S, Parsells, R, Pelliccia, N, Perasso, L, Perasso, S, Perfetto, F, Pinsky, L, Pocar, A, Pordes, S, Randle, K, Ranucci, G, Razeto, A, Romani, A, Rossi, B, Rossi, N, Rountree, Sd, Saggese, P, Saldanha, R, Salvo, C, Sands, W, Seigar, M, Semenov, D, Shields, E, Skorokhvatov, M, Smirnov, O, Sotnikov, A, Sukhotin, S, Suvarov, Y, Tartaglia, R, Tatarowicz, J, Testera, G, Thompson, J, Tonazzo, A, Unzhakov, E, Vogelaar, Rb, Wang, H, Westerdale, S, Wojcik, M, Wright, A, Xu, J, Yang, C, Zavatarelli, S, Zehfus, M, Zhong, W, Zuzel, G., Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), Université Pierre et Marie Curie - Paris 6 (UPMC)-Fédération de recherche du Département de physique de l'Ecole Normale Supérieure - ENS Paris (FRDPENS), École normale supérieure - Paris (ENS Paris), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-École normale supérieure - Paris (ENS Paris), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS), Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Université de Strasbourg (UNISTRA)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), Dip. di Fisica dell'Università di Genova - Italy, Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-Southeast University [Jiangsu]-Institut National de la Santé et de la Recherche Médicale (INSERM), and Centre National de la Recherche Scientifique (CNRS)-Ecole Nationale Supérieure de Chimie de Montpellier (ENSCM)-Université Montpellier 2 - Sciences et Techniques (UM2)-Institut de Chimie du CNRS (INC)-Université de Montpellier (UM)

Subjects

Physics::Instrumentation and Detectors, Dark matter, chemistry.chemical_element, 7. Clean energy, 01 natural sciences, Nuclear physics, 0103 physical sciences, Neutron, Dark Matter detector, 010306 general physics, Instrumentation, Mathematical Physics, ComputingMilieux_MISCELLANEOUS, Event reconstruction, Physics, [PHYS]Physics [physics], Scintillation, Argon, Time projection chamber, 010308 nuclear & particles physics, Detector, chemistry, Scintillation counter, High Energy Physics::Experiment, Noble liquid detector, DarkSide detector, [PHYS.ASTR]Physics [physics]/Astrophysics [astro-ph]

Abstract

"The DarkSide staged program utilizes a two-phase time projection chamber (TPC) with liquid argon as the target material for the scattering of dark matter particles. Efficient background reduction is achieved using low radioactivity underground argon as well as several experimental handles such as pulse shape, ratio of ionization over scintillation signal, 3D event reconstruction, and active neutron and muon vetos. The DarkSide-10 prototype detector has proven high scintillation light yield, which is a particularly important parameter as it sets the energy threshold for the pulse shape discrimination technique. The DarkSide-50 detector system, currently in commissioning phase at the Gran Sasso Underground Laboratory, will reach a sensitivity to dark matter spin-independent scattering cross section of 10(-45) cm(2) within 3 years of operation."

Published

2013

8. Limits on spin-dependent WIMP-nucleon cross sections from 225 live days of XENON100 data

Author

Marc Schumann, P. Shagin, A. Behrens, Ehud Duchovni, E. Pantic, M. Messina, J. A. M. Lopes, A. Kish, M. Garbini, K. Arisaka, Jean-Pierre Cussonneau, Hardy Simgen, A. D. Ferella, D. Thers, Boris Bauermeister, R. F. Lang, João Cardoso, K. Lung, A. P. Colijn, T. Marrodán Undagoitia, Ch. Weinheimer, Laura Baudis, Hui Wang, F. Gao, M. P. Decowski, Manfred Lindner, C. Ghag, C. Levy, M. Selvi, W. T. Chen, J. Lamblin, H. Landsman, Daniel Lellouch, P. R. Scovell, H. Contreras, P. Beltrame, Florian Kaether, Kaixuan Ni, Ran Budnik, F. V. Massoli, A. Molinario, Qing Lin, B. Choi, J.M.F. dos Santos, L. Scotto Lavina, Sebastian Lindemann, S. Rosendahl, S. Fattori, A. Teymourian, N. Priel, C. Balan, W. Hampel, Karl Giboni, W. Fulgione, Ethan Brown, Elena Aprile, F. Arneodo, April S. Brown, Uwe Oberlack, K. E. Lim, Jochen Schreiner, C. Grignon, A. J. Melgarejo Fernandez, M. Le Calloch, M. Alfonsi, O. Vitells, A. Rizzo, S. E. A. Orrigo, Y. Meng, Giacomo Bruno, G. Sartorelli, M. Weber, G. Plante, Luke Goetzke, K. Bokeloh, E. K. U. Gross, R. Persiani, Astroparticle Physics (IHEF, IoP, FNWI), Laboratoire SUBATECH Nantes (SUBATECH), Centre National de la Recherche Scientifique (CNRS)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université de Nantes (UN)-Mines Nantes (Mines Nantes), XENON100, E. Aprile, M. Alfonsi, K. Arisaka, F. Arneodo, C. Balan, L. Baudi, B. Bauermeister, A. Behren, P. Beltrame, K. Bokeloh, A. Brown, E. Brown, G. Bruno, R. Budnik, J. M. R. Cardoso, W.-T. Chen, B. Choi, A. P. Colijn, H. Contrera, J. P. Cussonneau, M. P. Decowski, E. Duchovni, S. Fattori, A. D. Ferella, W. Fulgione, F. Gao, M. Garbini, C. Ghag, K.-L. Giboni, L. W. Goetzke, C. Grignon, E. Gro, W. Hampel, F. Kaether, A. Kish, J. Lamblin, H. Landsman, R. F. Lang, M. Le Calloch, D. Lellouch, C. Levy, K. E. Lim, Q. Lin, S. Lindemann, M. Lindner, J. A. M. Lope, K. Lung, T. Marrodán Undagoitia, F. V. Massoli, A. J. Melgarejo Fernandez, Y. Meng, M. Messina, A. Molinario, K. Ni, U. Oberlack, S. E. A. Orrigo, E. Pantic, R. Persiani, G. Plante, N. Priel, A. Rizzo, S. Rosendahl, J. M. F. dos Santo, G. Sartorelli, J. Schreiner, M. Schumann, L. Scotto Lavina, P. R. Scovell, M. Selvi, P. Shagin, H. Simgen, A. Teymourian, D. Ther, O. Vitell, H. Wang, M. Weber, C. Weinheimer, and XENON100 collaboration

Subjects

Cosmology and Nongalactic Astrophysics (astro-ph.CO), [PHYS.ASTR.IM]Physics [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], Dark matter, General Physics and Astronomy, FOS: Physical sciences, 01 natural sciences, dark matter, Particle detector, High Energy Physics - Experiment, Nuclear physics, Cross section (physics), High Energy Physics - Experiment (hep-ex), High Energy Physics - Phenomenology (hep-ph), WIMP, 0103 physical sciences, [PHYS.HEXP]Physics [physics]/High Energy Physics - Experiment [hep-ex], 010306 general physics, Pseudovector, Instrumentation and Methods for Astrophysics (astro-ph.IM), Spin-½, Physics, 010308 nuclear & particles physics, [SDU.ASTR.IM]Sciences of the Universe [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], High Energy Physics - Phenomenology, [PHYS.HPHE]Physics [physics]/High Energy Physics - Phenomenology [hep-ph], Astrophysics - Instrumentation and Methods for Astrophysics, Nucleon, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

We present new experimental constraints on the elastic, spin-dependent WIMP-nucleon cross section using recent data from the XENON100 experiment, operated in the Laboratori Nazionali del Gran Sasso in Italy. An analysis of 224.6 live days x 34 kg of exposure acquired during 2011 and 2012 revealed no excess signal due to axial-vector WIMP interactions with 129-Xe and 131-Xe nuclei. This leads to the most stringent upper limits on WIMP-neutron cross sections for WIMP masses above 6 GeV, with a minimum cross section of 3.5 x 10^{-40} cm^2 at a WIMP mass of 45 GeV, at 90% confidence level., Comment: 5 pages, 3 figures; corrected caption of figure 3

Published

2013

9. The distributed Slow Control System of the XENON100 experiment

Author

Y. Mei, E. Pantic, Jean-Pierre Cussonneau, F. V. Massoli, Qing Lin, A. Manzur, K. E. Lim, O. Vitells, A. C. C. Ribeiro, Giacomo Bruno, W. Fulgione, A. Rizzo, B. Choi, J. A. M. Lopes, L. Scotto Lavina, A. Kish, Ethan Brown, Gabriella Sartorelli, E. Duchovni, Laura Baudis, W. Hampel, A. D. Ferella, M. Weber, S. E. A. Orrigo, João Cardoso, M. Selvi, F. Gao, G. Plante, T. Marrodán Undagoitia, Kaixuan Ni, Ch. Weinheimer, P. Beltrame, R. Persiani, Hui Wang, W. T. Chen, S. Rosendahl, Marc Schumann, P. Shagin, A. Molinario, A. Teymourian, K. Arisaka, H. Simgen, Uwe Oberlack, P. R. Scovell, S. Fattori, Daniel McKinsey, H. Contreras, F. Arneodo, M. Garbini, Eilam Gross, Luke Goetzke, A. Behrens, K. Bokeloh, Y. Meng, Elena Aprile, E. Nativ, Ran Budnik, A. J. Melgarejo Fernandez, K. Lung, C. Levy, M. Alfonsi, J.M.F. dos Santos, R. F. Lang, M. Le Calloch, Stefan Lindemann, J. Lamblin, J. Schreiner, M. P. Decowski, Manfred Lindner, C. Balan, N. Priel, D. Thers, C. Grignon, K. L. Giboni, J. V. Patricio, E Aprile, M Alfonsi, K Arisaka, F Arneodo, C Balan, L Baudi, A Behren, P Beltrame, K Bokeloh, E Brown, G M Bruno, R Budnik, M Le Calloch, J M Cardoso, W -T Chen, B Choi, H Contrera, J -P Cussonneau, M P Decowski, E Duchovni, S Fattori, A D Ferella, W Fulgione, F Gao, M Garbini, K -L Giboni, L W Goetzke, C Grignon, E Gro, W Hampel, D N McKinsey, A Kish, J Lamblin, R F Lang, C Levy, K E Lim, Q Lin, S Lindemann, M Lindner, J A M Lope, K Lung, A Manzur, T Marrodán Undagoitia, F V Massoli, Y Mei, A J Melgarejo Fernandez, Y Meng, A Molinario, E Nativ, K Ni, U Oberlack, S E A Orrigo, E Pantic, J V Patricio, R Persiani, G Plante, N Priel, A C C Ribeiro, A Rizzo, S Rosendahl, J M F dos Santo, G Sartorelli, J Schreiner, M Schumann, L Scotto Lavina, P R Scovell, M Selvi, P Shagin, H Simgen, A Teymourian, D Ther, O Vitell, H Wang, M Weber, C Weinheimer, Laboratoire SUBATECH Nantes (SUBATECH), Centre National de la Recherche Scientifique (CNRS)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université de Nantes (UN)-Mines Nantes (Mines Nantes), XENON100, IoP (FNWI), Gravitation and Astroparticle Physics Amsterdam, GRAPPA (ITFA, IoP, FNWI), Faculty of Science, and Other Research IHEF (IoP, FNWI)

Subjects

Physics - Instrumentation and Detectors, architecture, [PHYS.ASTR.IM]Physics [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], Java, Computer science, Real-time computing, FOS: Physical sciences, chemistry.chemical_element, Control and monitor systems online, Control systems, Detector control systems (detector and experiment monitoring and slow-control systems, architecture, hardware, algorithms, databases), algorithms, 01 natural sciences, Xenon, 0103 physical sciences, hardware, DETECTOR CONTROL SYSTEMS, [PHYS.PHYS.PHYS-INS-DET]Physics [physics]/Physics [physics]/Instrumentation and Detectors [physics.ins-det], CONTROL SYSTEMS, 010306 general physics, Instrumentation and Methods for Astrophysics (astro-ph.IM), Instrumentation, Mathematical Physics, computer.programming_language, Time projection chamber, 010308 nuclear & particles physics, business.industry, Detector control systems (detector and experiment monitoring and slow-control systems, Emphasis (telecommunications), Volume (computing), Instrumentation and Detectors (physics.ins-det), Modular design, [SDU.ASTR.IM]Sciences of the Universe [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], chemistry, Control system, Astrophysics - Instrumentation and Methods for Astrophysics, databases), business, computer, System software

Abstract

The XENON100 experiment, in operation at the Laboratori Nazionali del Gran Sasso (LNGS) in Italy, was designed to search for evidence of dark matter interactions inside a volume of liquid xenon using a dual-phase time projection chamber. This paper describes the Slow Control System (SCS) of the experiment with emphasis on the distributed architecture as well as on its modular and expandable nature. The system software was designed according to the rules of Object-Oriented Programming and coded in Java, thus promoting code reusability and maximum flexibility during commissioning of the experiment. The SCS has been continuously monitoring the XENON100 detector since mid 2008, remotely recording hundreds of parameters on a few dozen instruments in real time, and setting emergency alarms for the most important variables., Comment: 12 pages, 4 figures

Published

2012

10. Dark Matter Results from 100 Live Days of XENON100 Data

Author

K. Arisaka, Marc Schumann, P. Shagin, F. Arneodo, J. A. M. Lopes, A. Kish, G. Sartorelli, K. E. Lim, R. Santorelli, Manfred Lindner, C. W. Lam, K. Bokeloh, S. Fattori, A. Behrens, M. Selvi, J. Lamblin, Eilam Gross, Elena Aprile, David B. Cline, D. Thers, Y. Mei, E. Pantic, R. F. Lang, A. Teymourian, R. Persiani, Ethan Brown, T. Bruch, K. L. Giboni, Hardy Simgen, A. D. Ferella, Hongwei Wang, M. Weber, T. Marrodán Undagoitia, C. Levy, Ch. Weinheimer, B. Choi, G. Plante, K. Lung, Laura Baudis, J.M.F. dos Santos, Sebastian Lindemann, Kaixuan Ni, A. J. Melgarejo Fernandez, S. E. A. Orrigo, A. C. C. Ribeiro, Giacomo Bruno, O. Vitells, Uwe Oberlack, Qing Lin, Ehud Duchovni, A. Askin, João Cardoso, F. Gao, W. T. Chen, E. Aprile, K. Arisaka, F. Arneodo, A. Askin, L. Baudi, A. Behren, K. Bokeloh, E. Brown, T. Bruch, G. Bruno, J. M. R. Cardoso, W.-T. Chen, B. Choi, D. Cline, E. Duchovni, S. Fattori, A. D. Ferella, F. Gao, K.-L. Giboni, E. Gro, A. Kish, C. W. Lam, J. Lamblin, R. F. Lang, C. Levy, K. E. Lim, Q. Lin, S. Lindemann, M. Lindner, J. A. M. Lope, K. Lung, T. Marrodan Undagoitia, Y. Mei, A. J. Melgarejo Fernandez, K. Ni| U. Oberlack, S. E. A. Orrigo, E. Pantic, R. Persiani, G. Plante, A. C. C. Ribeiro, R. Santorelli, J. M. F. dos Santo, G. Sartorelli, M. Schumann, M. Selvi, P. Shagin, H. Simgen, A. Teymourian, D. Ther, O. Vitell, H. Wang, M. Weber, C. Weinheimer, Laboratoire SUBATECH Nantes (SUBATECH), Mines Nantes (Mines Nantes)-Université de Nantes (UN)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), and XENON100

Subjects

Physics, Cosmology and Nongalactic Astrophysics (astro-ph.CO), Large Underground Xenon experiment, 010308 nuclear & particles physics, DARK MATTER, Dark matter, Hadron, FOS: Physical sciences, General Physics and Astronomy, Elementary particle, Fermion, 01 natural sciences, Particle detector, High Energy Physics - Experiment, WIMPS, Nuclear physics, High Energy Physics - Experiment (hep-ex), XENON, WIMP, 0103 physical sciences, [PHYS.HEXP]Physics [physics]/High Energy Physics - Experiment [hep-ex], TPC, 010306 general physics, Nucleon, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

We present results from the direct search for dark matter with the XENON100 detector, installed underground at the Laboratori Nazionali del Gran Sasso of INFN, Italy. XENON100 is a two-phase time projection chamber with a 62 kg liquid xenon target. Interaction vertex reconstruction in three dimensions with millimeter precision allows to select only the innermost 48 kg as ultra-low background fiducial target. In 100.9 live days of data, acquired between January and June 2010, no evidence for dark matter is found. Three candidate events were observed in a pre-defined signal region with an expected background of 1.8 +/- 0.6 events. This leads to the most stringent limit on dark matter interactions today, excluding spin-independent elastic WIMP-nucleon scattering cross-sections above 7.0x10^-45 cm^2 for a WIMP mass of 50 GeV/c^2 at 90% confidence level., 5 pages, 5 figures; matches accepted version

Published

2011

11. Implications on inelastic dark matter from 100 live days of XENON100 data

Author

E. Pantic, Ethan Brown, M. Selvi, David B. Cline, Y. Mei, J.M.F. dos Santos, Hui Wang, T. Marrodán Undagoitia, Manfred Lindner, Ch. Weinheimer, B. Choi, A. Behrens, Sebastian Lindemann, Karl Giboni, K. Arisaka, R. Santorelli, F. Arneodo, M. Weber, G. Plante, Hardy Simgen, A. D. Ferella, S. Fattori, J. A. M. Lopes, K. Lung, A. Kish, Laura Baudis, A. Teymourian, C. W. Lam, D. Thers, R. F. Lang, A. C. C. Ribeiro, Giacomo Bruno, Elena Aprile, C. Levy, T. Bruch, Kaixuan Ni, K. E. Lim, S. E. A. Orrigo, J. Lamblin, Uwe Oberlack, O. Vitells, Ehud Duchovni, A. J. Melgarejo Fernandez, Qing Lin, A. Askin, João Cardoso, F. Gao, W. T. Chen, Marc Schumann, P. Shagin, G. Sartorelli, R. Persiani, K. Bokeloh, E. K. U. Gross, E. Aprile, K. Arisaka, F. Arneodo, A. Askin, L. Baudi, A. Behren, K. Bokeloh, E. Brown, T. Bruch, G. Bruno, J. M. R. Cardoso, W.-T. Chen, B. Choi, D. Cline, E. Duchovni, S. Fattori, A. D. Ferella, F. Gao, K.-L. Giboni, E. Gro, A. Kish, C. W. Lam, J. Lamblin, R. F. Lang, C. Levy, K. E. Lim, Q. Lin, S. Lindemann, M. Lindner, J. A. M. Lope, K. Lung, T. Marrodán Undagoitia, Y. Mei, A. J. Melgarejo Fernandez, K. Ni, U. Oberlack, S. E. A. Orrigo, E. Pantic, R. Persiani, G. Plante, A. C. C. Ribeiro, R. Santorelli, J. M. F. dos Santo, G Sartorelli, M. Schumann, M. Selvi, P. Shagin, H. Simgen, A. Teymourian, D. Ther, O. Vitell, H. Wang, M. Weber, C. Weinheimer, Laboratoire SUBATECH Nantes (SUBATECH), Mines Nantes (Mines Nantes)-Université de Nantes (UN)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), and XENON100

Subjects

Physics, Nuclear and High Energy Physics, Cosmology and Nongalactic Astrophysics (astro-ph.CO), 010308 nuclear & particles physics, Scattering, DARK MATTER, Signal region, Dark matter, FOS: Physical sciences, 01 natural sciences, WIMPS, Nuclear physics, XENON, 0103 physical sciences, [PHYS.HEXP]Physics [physics]/High Energy Physics - Experiment [hep-ex], TPC, 010306 general physics, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

The XENON100 experiment has recently completed a dark matter run with 100.9 live-days of data, taken from January to June 2010. Events in a 48kg fiducial volume in the energy range between 8.4 and 44.6 keVnr have been analyzed. A total of three events have been found in the predefined signal region, compatible with the background prediction of (1.8 \pm 0.6) events. Based on this analysis we present limits on the WIMP-nucleon cross section for inelastic dark matter. With the present data we are able to rule out the explanation for the observed DAMA/LIBRA modulation as being due to inelastic dark matter scattering off iodine at a 90% confidence level., Comment: 3 pages, 3 figures

Published

2011

12. Light yield in DarkSide-10 : a prototype two-phase argon TPC for dark matter searches

Author

M. D. Skorokhvatov, L. Grandi, Marc S. Seigar, A. G. Cocco, A. Fan, Aldo Romani, S. Kidner, I. N. Machulin, C. Salvo, E. de Haas, D. Semenov, A. Nelson, N. Rossi, Marco Pallavicini, K. Arisaka, D. D'Angelo, E. V. Hungerford, E. V. Unzhakov, G. Fiorillo, Y. Meng, C. Ghag, G. Guray, A. Sotnikov, J. Thompson, G. Bonfini, C. L. Kendziora, W. Sands, F. Gabriele, R. B. Vogelaar, J. Brodsky, P. Saggese, C. Condon, P. Beltrame, S. Davini, B. J. Mount, C. Ghiano, M. Guan, A. Candela, P. J. Mosteiro, David B. Cline, R. Tartaglia, E. Meroni, H. O. Back, K. Keeter, S. Gazzana, M. Zehfus, Peter Daniel Meyers, An. Ianni, Laura Cadonati, F. Perfetto, A. Nemtzow, D. Korablev, Y. Suvorov, S. Westerdale, Hui Wang, A. V. Derbin, A. Brigatti, G. Koh, M. Montuschi, Livia Ludhova, V. N. Muratova, Thomas Alexander, I. Dratchnev, Y. Q. Ma, A. M. Goretti, A. Razeto, N. N. Nurakhov, R. Saldanha, A. S. Chepurnov, C. J. Martoff, J. Tatarowicz, G. Testera, Frank Calaprice, A. E. Chavarria, Cristiano Galbiati, L. Lukyanchenko, G. Zuzel, Fausto Ortica, M. Orsini, C. Guo, Al. Ianni, A. Teymourian, L. Perasso, H. Cao, Gioacchino Ranucci, W. Zhong, Sandra Zavatarelli, G. Korga, P. X. Li, D. Alton, A.V. Etenko, E. Pantic, Austin P. Lund, M. Gromov, R. Parsells, P. Cavalcante, G. Di Pietro, A. Empl, N. Pelliccia, J. Maricic, E. Shields, C. Love, T. Mohayai, Paolo Lombardi, S. V. Sukhotin, A. Wright, V. V. Kobychev, K. Lung, B. Loer, Jay Burton Benziger, Chung-Yao Yang, Lawrence Pinsky, A. Kayunov, D. Montanari, D. Durben, A. Pocar, Jilei Xu, O. Smirnov, S. Parmeggiano, Marcin Wójcik, S. Pordes, K. Fomenko, Alexander, T., Alton, D., Arisaka, K., Back, H. O., Beltrame, P., Benziger, J., Bonfini, G., Brigatti, A., Brodsky, J., Cadonati, L., Calaprice, F., Candela, A., Cao, H., Cavalcante, P., Chavarria, A., Chepurnov, A., Cline, D., Cocco, A. G., Condon, C., D'Angelo, D., Davini, S., Haas, E. D., Derbin, A., Pietro, G. D., Dratchnev, I., Durben, D., Empl, A., Etenko, A., Fan, A., Fiorillo, Giuliana, Fomenko, K., Gabriele, F., Galbiati, C., Gazzana, S., Ghag, C., Ghiano, C., Goretti, A., Grandi, L., Gromov, M., Guan, M., Guo, C., Guray, G., Hungerford, E. V., Ianni, A., Kayunov, A., Keeter, K., Kendziora, C., Kidner, S., Kobychev, V., Koh, G., Korablev, D., Korga, G., Shields, E., Li, P., Loer, B., Lombardi, P., Love, C., Ludhova, L., Lukyanchenko, L., Lund, A., Lung, K., Ma, Y., Machulin, I., Maricic, J., Martoff, C. J., Meng, Y., Meroni, E., Meyers, P. D., Mohayai, T., Montanari, D., Montuschi, M., Mosteiro, P., Mount, B., Muratova, V., Nelson, A., Nemtzow, A., Nurakhov, N., Orsini, M., Ortica, F., Pallavicini, M., Pantic, E., Parmeggiano, S., Parsells, R., Pelliccia, N., Perasso, L., Perfetto, F., Pinsky, L., Pocar, A., Pordes, S., Ranucci, G., Razeto, A., Romani, A., Rossi, N., Saggese, P., Saldanha, R., Salvo, C., Sands, W., Seigar, M., Semenov, D., Skorokhvatov, M., Smirnov, O., Sotnikov, A., Sukhotin, S., Suvorov, Y., Tartaglia, R., Tatarowicz, J., Testera, G., Teymourian, A., Thompson, J., Unzhakov, E., Vogelaar, R. B., Wang, H., Westerdale, S., Wojcik, M., Wright, A., Xu, J., Yang, C., Zavatarelli, S., Zehfus, M., Zhong, W., and Zuzel, G.

Subjects

Physics::Instrumentation and Detectors, Dark matter, light yield, FOS: Physical sciences, chemistry.chemical_element, dark matter, law.invention, High Energy Physics - Experiment, Nuclear physics, High Energy Physics - Experiment (hep-ex), XENON, law, DEPENDENCE, LIQUID ARGON, PARTICLES, Instrumentation and Methods for Astrophysics (astro-ph.IM), Physics, Scintillation, Time projection chamber, Argon, Gamma ray, Astronomy and Astrophysics, Laser, time projection chamber, chemistry, Yield (chemistry), Scintillation counter, argon, High Energy Physics::Experiment, Astrophysics - Instrumentation and Methods for Astrophysics, photoelectron yield

Abstract

As part of the DarkSide program of direct dark matter searches using liquid argon TPCs, a prototype detector with an active volume containing 10 kg of liquid argon, DarkSide-10, was built and operated underground in the Gran Sasso National Laboratory in Italy. A critically important parameter for such devices is the scintillation light yield, as photon statistics limits the rejection of electron-recoil backgrounds by pulse shape discrimination. We have measured the light yield of DarkSide-10 using the readily-identifiable full-absorption peaks from gamma ray sources combined with single-photoelectron calibrations using low-occupancy laser pulses. For gamma lines of energies in the range 122-1275 keV, we get consistent light yields averaging 8.887+-0.003(stat)+-0.444(sys) p.e./keVee. With additional purification, the light yield measured at 511 keV increased to 9.142+-0.006(stat) p.e./keVee., 10 pages, 7 figures, Accepted for publication in Astroparticle Physics

Published

2013

13. Krüppel-like factor 2 is required for normal mouse cardiac development

Author

Tina K. Lung, Rakesh C. Kukreja, Joyce A. Lloyd, Fadi N Salloum, Yousef N. Alhashem, Benjamin A. Koppenhaver, Aditi R. Chiplunkar, and Jack L. Haar

Subjects

Male, Embryology, Mouse, Gene Expression, lcsh:Medicine, Matrix (biology), Cardiovascular, Mice, Molecular Cell Biology, Morphogenesis, lcsh:Science, reproductive and urinary physiology, Glycosaminoglycans, Mice, Knockout, 0303 health sciences, Multidisciplinary, Cardiac Jelly, Heart development, GATA4, 030302 biochemistry & molecular biology, Gene Expression Regulation, Developmental, Embryo, Cell Differentiation, Heart, Animal Models, KLF2, embryonic structures, Heart Development, Medicine, Female, Cellular Types, Research Article, Heart Defects, Congenital, endocrine system, Kruppel-Like Transcription Factors, Mice, Transgenic, SOX9, Biology, 03 medical and health sciences, Model Organisms, Genetics, Animals, 030304 developmental biology, Myocardium, Mesenchymal stem cell, lcsh:R, Endothelial Cells, Embryo, Mammalian, Molecular biology, GATA4 Transcription Factor, Mice, Inbred C57BL, Immunology, lcsh:Q, Gene Function, T-Box Domain Proteins, Developmental Biology

Abstract

Kruppel-like factor 2 (KLF2) is expressed in endothelial cells in the developing heart, particularly in areas of high shear stress, such as the atrioventricular (AV) canal. KLF2 ablation leads to myocardial thinning, high output cardiac failure and death by mouse embryonic day 14.5 (E14.5) in a mixed genetic background. This work identifies an earlier and more fundamental role for KLF2 in mouse cardiac development in FVB/N mice. FVB/N KLF2−/− embryos die earlier, by E11.5. E9.5 FVB/N KLF2−/− hearts have multiple, disorganized cell layers lining the AV cushions, the primordia of the AV valves, rather than the normal single layer. By E10.5, traditional and endothelial-specific FVB/N KLF2−/− AV cushions are hypocellular, suggesting that the cells accumulating at the AV canal have a defect in endothelial to mesenchymal transformation (EMT). E10.5 FVB/N KLF2−/− hearts have reduced glycosaminoglycans in the cardiac jelly, correlating with the reduced EMT. However, the number of mesenchymal cells migrating from FVB/N KLF2−/− AV explants into a collagen matrix is reduced considerably compared to wild-type, suggesting that the EMT defect is not due solely to abnormal cardiac jelly. Echocardiography of E10.5 FVB/N KLF2−/− embryos indicates that they have abnormal heart function compared to wild-type. E10.5 C57BL/6 KLF2−/− hearts have largely normal AV cushions. However, E10.5 FVB/N and C57BL/6 KLF2−/− embryos have a delay in the formation of the atrial septum that is not observed in a defined mixed background. KLF2 ablation results in reduced Sox9, UDP-glucose dehydrogenase (Ugdh), Gata4 and Tbx5 mRNA in FVB/N AV canals. KLF2 binds to the Gata4, Tbx5 and Ugdh promoters in chromatin immunoprecipitation assays, indicating that KLF2 could directly regulate these genes. In conclusion, KLF2−/− heart phenotypes are genetic background-dependent. KLF2 plays a role in EMT through its regulation of important cardiovascular genes.

Published

2013

14. Study of the electromagnetic background in the XENON100 experiment

Author

Ethan Brown, R. Santorelli, A. Askin, S. Fattori, João Cardoso, F. Arneodo, E. Pantic, S. E. A. Orrigo, J. Lamblin, Marc Schumann, P. Shagin, K. Arisaka, Hardy Simgen, A. D. Ferella, Y. Mei, A. C. C. Ribeiro, Kaixuan Ni, E. Tziaferi, Laura Baudis, D. Thers, Manfred Lindner, Hongwei Wang, R. F. Lang, A. J. Melgarejo Fernandez, David B. Cline, J. A. M. Lopes, K. E. Lim, A. Kish, Qing Lin, B. Choi, J.M.F. dos Santos, K. Bokeloh, Sebastian Lindemann, Elena Aprile, T. Marrodán Undagoitia, Ch. Weinheimer, K. L. Giboni, C. W. Lam, Uwe Oberlack, K. Lung, M. Weber, G. Plante, A. Teymourian, A. Behrens, Laboratoire SUBATECH Nantes (SUBATECH), Mines Nantes (Mines Nantes)-Université de Nantes (UN)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), and XENON100

Subjects

Nuclear and High Energy Physics, Cosmology and Nongalactic Astrophysics (astro-ph.CO), [PHYS.ASTR.IM]Physics [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], Physics::Instrumentation and Detectors, Monte Carlo method, Dark matter, chemistry.chemical_element, FOS: Physical sciences, 01 natural sciences, 7. Clean energy, Particle detector, Nuclear physics, Xenon, Recoil, 0103 physical sciences, 010306 general physics, Nuclear Experiment, Instrumentation and Methods for Astrophysics (astro-ph.IM), Physics, Elastic scattering, 010308 nuclear & particles physics, Detector, Astrophysics::Instrumentation and Methods for Astrophysics, [SDU.ASTR.IM]Sciences of the Universe [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], chemistry, High Energy Physics::Experiment, Astrophysics - Instrumentation and Methods for Astrophysics, Radioactive decay, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

The XENON100 experiment, located at the Laboratori Nazionali del Gran Sasso (LNGS), aims to directly detect dark matter in the form of Weakly Interacting Massive Particles (WIMPs) via their elastic scattering off xenon nuclei. We present a comprehensive study of the predicted electronic recoil background coming from radioactive decays inside the detector and shield materials, and intrinsic contamination. Based on GEANT4 Monte Carlo simulations using a detailed geometry together with the measured radioactivity of all detector components, we predict an electronic recoil background in the WIMP-search energy range (0-100 keV) in the 30 kg fiducial mass of less than 10e-2 events/(kg-day-keV), consistent with the experiment's design goal. The predicted background spectrum is in very good agreement with the data taken during the commissioning of the detector, in Fall 2009., 10 pages, 12 figures The updated version of the paper takes into account the new measurement of $^{136}$Xe 2$\nu$ $\beta\beta$ decay by EXO-200, with a half-life of (2.11$\pm0.04\pm$0.021)$\times10^{21}$ years

Published

2011

15. Erythropoietin-Induced Phosphorylation/Degradation of BIM Contributes to Survival of Erythroid Cells

Author

Stephen T. Sawyer, Joyce A. Lloyd, Jingchun Chen, Tina K. Lung, Randolph M. Abutin, and Hisashi Harada

Subjects

MAPK/ERK pathway, Cancer Research, Programmed cell death, Cell Survival, MAP Kinase Signaling System, cells, Apoptosis, Biology, Article, Cell Line, Small hairpin RNA, Mice, Erythroid Cells, hemic and lymphatic diseases, Proto-Oncogene Proteins, Genetics, medicine, Animals, Phosphorylation, Extracellular Signal-Regulated MAP Kinases, neoplasms, Molecular Biology, Erythropoietin, Mice, Knockout, Bcl-2-Like Protein 11, Kinase, Membrane Proteins, hemic and immune systems, Cell Biology, Hematology, Cancer research, Proteasome inhibitor, biological phenomena, cell phenomena, and immunity, Apoptosis Regulatory Proteins, medicine.drug

Abstract

Objective A proapoptotic BH3-only protein BIM (BCL-2 interacting mediator of cell death) can link cytokine receptor signaling with the apoptotic machinery in hematopoietic cells. We investigated here the role of BIM in erythropoietin (EPO)-mediated survival in erythroid cells. Materials and Methods We downregulated BIM in EPO-dependent HCD57 erythroid cells with short hairpin RNA (shRNA), and used real-time polymerase chain reaction, Western blots, and flow cytometry to characterize BIM expression and apoptosis. Hematologic analyses of BIM-deficient ( Bim –/– ) mice were conducted. Results BIM expression increases in primary murine erythroid cells and HCD57 cells deprived of EPO. Whereas Bim mRNA increased less than twofold, BIM protein increased more than 10-fold after EPO withdrawal, suggesting posttranscriptional regulation of BIM. EPO treatment resulted in rapid phosphorylation of BIM at Serine 65 and phosphorylation correlated with degradation of BIM. Inhibition of extracellular signal-regulated kinase (ERK) by a MEK/ERK inhibitor, U0126, blocked both phosphorylation and degradation of BIM, resulting in apoptosis. Treatment with a proteasome inhibitor, MG-132, also blocked degradation of phosphorylated BIM. Downregulation of BIM with the shRNA resulted in HCD57 cells more resistant to apoptosis induced by either EPO withdrawal or ERK inhibition. Although we observed no significant changes in the number of erythrocytes or reticulocytes in the circulation of Bim –/– mice, erythroid progenitors from bone marrow in Bim –/– mice were reduced in number and more resistant to apoptosis induced by U0126 MEK/ERK inhibitor. Conclusion EPO protects erythroid cells from apoptosis in part through ERK-mediated phosphorylation followed by proteasomal degradation of BIM.

Published

2008

16. Dark matter results from 225 live days of XENON100 data

Author

W. Hampel, M. Garbini, J.M.F. dos Santos, J. Lamblin, K. Bokeloh, Jean-Pierre Cussonneau, S. Rosendahl, Ethan Brown, M. Selvi, Sebastian Lindemann, Eilam Gross, Boris Bauermeister, P. Beltrame, Jochen Schreiner, Luke Goetzke, Hardy Simgen, A. D. Ferella, G. Sartorelli, A. Teymourian, F. Arneodo, Laura Baudis, H. Landsman, M. Le Calloch, J. A. M. Lopes, S. Fattori, Y. Meng, O. Vitells, A. Rizzo, David B. Cline, S. E. A. Orrigo, A. Kish, João Cardoso, K. Arisaka, R. Persiani, L. Scotto Lavina, C. Grignon, K. L. Giboni, H. Contreras, F. Gao, A. Behrens, E. Pantic, C. Balan, D. Thers, Ehud Duchovni, W. T. Chen, K. E. Lim, M. Weber, Auke-Pieter Colijn, R. F. Lang, Uwe Oberlack, Elena Aprile, Kaixuan Ni, E. Nativ, T. Marrodán Undagoitia, G. Plante, B. Choi, Ch. Weinheimer, A. J. Melgarejo Fernandez, P. R. Scovell, C. Ghag, F. V. Massoli, Qing Lin, M. Alfonsi, K. Lung, A. Molinario, W. Fulgione, Giacomo Bruno, C. Levy, N. Priel, Hui Wang, Florian Kaether, M. P. Decowski, Manfred Lindner, Marc Schumann, P. Shagin, Ran Budnik, Astroparticle Physics (IHEF, IoP, FNWI), E. Aprile, M. Alfonsi, K. Arisaka, F. Arneodo, C. Balan, L. Baudi, B. Bauermeister, A. Behren, P. Beltrame, K. Bokeloh, E. Brown, G. Bruno, R. Budnik, J. M. R. Cardoso, W.-T. Chen, B. Choi, D. Cline, A. P. Colijn, H. Contrera, J. P. Cussonneau, M. P. Decowski, E. Duchovni, S. Fattori, A. D. Ferella, W. Fulgione, F. Gao, M. Garbini, C. Ghag, K.-L. Giboni, L. W. Goetzke, C. Grignon, E. Gro, W. Hampel, F. Kaether, A. Kish, J. Lamblin, H. Landsman, R. F. Lang, M. Le Calloch, C. Levy, K. E. Lim, Q. Lin, S. Lindemann, M. Lindner, J. A. M. Lope, K. Lung, T. Marrodán Undagoitia, F. V. Massoli, A. J. Melgarejo Fernandez, Y. Meng, A. Molinario, E. Nativ, K. Ni, U. Oberlack, S. E. A. Orrigo, E. Pantic, R. Persiani, G. Plante, N. Priel, A. Rizzo, S. Rosendahl, J. M. F. dos Santo, G. Sartorelli, J. Schreiner, M. Schumann, L. Scotto Lavina, P. R. Scovell, M. Selvi, P. Shagin, H. Simgen, A. Teymourian, D. Ther, O. Vitell, H. Wang, M. Weber, C. Weinheimer, Laboratoire SUBATECH Nantes (SUBATECH), Centre National de la Recherche Scientifique (CNRS)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université de Nantes (UN)-Mines Nantes (Mines Nantes), and XENON100

Subjects

Cosmology and Nongalactic Astrophysics (astro-ph.CO), Physics - Instrumentation and Detectors, Large Underground Xenon experiment, Dark matter, FOS: Physical sciences, General Physics and Astronomy, WIMP Argon Programme, 01 natural sciences, 7. Clean energy, Particle detector, High Energy Physics - Experiment, Nuclear physics, High Energy Physics - Experiment (hep-ex), High Energy Physics - Phenomenology (hep-ph), WIMP, 0103 physical sciences, [PHYS.HEXP]Physics [physics]/High Energy Physics - Experiment [hep-ex], [PHYS.PHYS.PHYS-INS-DET]Physics [physics]/Physics [physics]/Instrumentation and Detectors [physics.ins-det], 010306 general physics, Liquid Xenon, Physics, Range (particle radiation), 010308 nuclear & particles physics, DARK MATTER, Instrumentation and Detectors (physics.ins-det), High Energy Physics - Phenomenology, [PHYS.HPHE]Physics [physics]/High Energy Physics - Phenomenology [hep-ph], DAMA/NaI, TPC, PandaX, Direct search for Dark Matter, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

We report on a search for particle dark matter with the XENON100 experiment, operated at the Laboratori Nazionali del Gran Sasso (LNGS) for 13 months during 2011 and 2012. XENON100 features an ultra-low electromagnetic background of (5.3 \pm 0.6) \times 10^-3 events (kg day keVee)^-1 in the energy region of interest. A blind analysis of 224.6 live days \times 34 kg exposure has yielded no evidence for dark matter interactions. The two candidate events observed in the pre-defined nuclear recoil energy range of 6.6-30.5 keVnr are consistent with the background expectation of (1.0 \pm 0.2) events. A Profile Likelihood analysis using a 6.6-43.3 keVnr energy range sets the most stringent limit on the spin-independent elastic WIMP-nucleon scattering cross section for WIMP masses above 8 GeV/c^2, with a minimum of 2 \times 10^-45 cm^2 at 55 GeV/c^2 and 90% confidence level., 6 pages, 5 figures. Matches version accepted by PRL. Includes limits up to 10 TeV/c^2, published as supplementary material: http://prl.aps.org/supplemental/PRL/v109/i18/e181301 Please cite high mass limits as "Phys. Rev. Lett. 109, 181301 (2012), online supplementary material."

Published

2012

17. Effect of temperatures and loading rates on direct shear strength of asphaltic concrete using layer-parallel direct shear test.

Author

C K Lung, M R Mohd Hasan, M O Hamzah, A Sani, S Poovaneshvaran, and P J Ramadhansyah

Published

2020

18. A Multi-Element-Doped Porous Bioactive Glass Coating for Implant Applications

Author

Christie Y. K. Lung, Mohamed M. Abdalla, Chun Hung Chu, Iris Yin, Sofiya-Roksolana Got, and Jukka P. Matinlinna

Subjects

titanium, bioactive glass, implant coating, antibacterial, cell cytotoxicity, Technology, Electrical engineering. Electronics. Nuclear engineering, TK1-9971, Engineering (General). Civil engineering (General), TA1-2040, Microscopy, QH201-278.5, Descriptive and experimental mechanics, QC120-168.85

Abstract

Objectives: The objectives of the study were (1) to develop a novel multi-element-doped porous 58S bioactive glass coating for titanium implants and (2) to investigate the physiochemical, cell cytotoxic and antibacterial properties of this novel coating for titanium implants. Methods: This study employed the sol–gel method to develop a silver-, cobalt (II) oxide- and titanium dioxide-doped 58S bioactive glass coating. The surface topography and in vitro bioactivity of the new bioactive glass-coated implants were studied using scanning electron microscopy (SEM) and energy-dispersive X-ray spectroscopy. The surface nanohardness and coating degradation were evaluated using atomic force microscopy (AFM) and inductively coupled plasma atomic emission spectroscopy (ICP-AES), respectively. The cell cytotoxicity was assessed using cell viability of osteoblast-like mouse cells. The antibacterial property was examined using colony-forming units (CFUs) of the implant coating against Porphyromonas gingivalis. Results: The multi-element-doped porous 58S bioactive glass-coated titanium implant was synthesized. SEM showed that calcium phosphate was formed on the novel coating but not on the 58S bioactive glass coating. The mean surface nanohardness of the novel coating and the 58S coating were 124 ± 24 and 50 ± 17 MPa, respectively (p < 0.001). ICP-AES showed that the releases of Si, Ca and P ions of the novel coating were significantly higher than that of a 58S bioactive glass-coated implant. No significant difference in cell cytotoxicity was found between the novel coating and the 58S coating (p > 0.1). The mean CFUs of the novel coating and the conventional coating were 120 × 106 and 49 × 106 /mL. Conclusion: A novel multielement-doped porous bioactive glass coating for titanium implants was developed. The coating displays promising biocompatibility and antibacterial activity. Clinical significance: the coating can be used to improve the clinical success of dental implants for patient care if it shows success in clinical trials.

Published

2021

19. First Axion Results from the XENON100 Experiment

Author

Xenon, The Collaboration, Aprile, E., Agostini, F., Alfonsi, M., Arisaka, K., Arneodo, F., Auger, M., Balan, C., Barrow, P., Baudis, L., Bauermeister, B., Behrens, A., Beltrame, P., Bokeloh, K., Brown, A., Brown, E., Bruenner, S., Bruno, G., Budnik, R., Cardoso, J. M. R., Colijn, A. P., Contreras, H., Cussonneau, J. P., Decowski, M. P., Duchovni, E., Fattori, S., Ferella, A. D., Fulgione, W., Gao, F., Garbini, M., Geis, C., Goetzke, L. W., Grignon, C., Gross, E., Hampel, W., Itay, R., Kaether, F., Kessler, G., Kish, A., Landsman, H., Lang, R. F., Le Calloch, M., Lellouch, D., Levy, C., Lindemann, S., Lindner, M., Lopes, J. A. M., Lung, K., Lyashenko, A., Macmullin, S., Marrodan Undagoitia, T., Masbou, J., Massoli, F. V., Mayani Paras, D., Melgarejo Fernandez, A. J., Meng, Y., Messina, M., Miguez, B., Molinario, A., Murra, M., Naganoma, J., Oberlack, U., Orrigo, S. E. A., Pantic, E., Persiani, R., Piastra, F., Pienaar, J., Plante, G., Priel, N., Reichard, S., Reuter, C., Rizzo, A., Rosendahl, S., Dos Santos, J. M. F., Sartorelli, G., Schindler, S., Schreiner, J., Schumann, M., Scotto Lavina, L., Selvi, M., Shagin, P., Simgen, H., Teymourian, A., Thers, D., Tiseni, A., Gian Carlo Trinchero, Vitells, O., Wang, H., Weber, M., Weinheimer, C., Laboratoire SUBATECH Nantes (SUBATECH), Centre National de la Recherche Scientifique (CNRS)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université de Nantes (UN)-Mines Nantes (Mines Nantes), XENON100, Astroparticle Physics (IHEF, IoP, FNWI), E. Aprile, F. Agostini, M. Alfonsi, K. Arisaka, F. Arneodo, M. Auger, C. Balan, P. Barrow, L. Baudi, B. Bauermeister, A. Behren, P. Beltrame, K. Bokeloh, A. Brown, E. Brown, S. Bruenner, G. Bruno, R. Budnik, J. M. R. Cardoso, A. P. Colijn, H. Contrera, J. P. Cussonneau, M. P. Decowski, E. Duchovni, S. Fattori, A. D. Ferella, W. Fulgione, F. Gao, M. Garbini, C. Gei, L. W. Goetzke, C. Grignon, E. Gro, W. Hampel, R. Itay, F. Kaether, G. Kessler, A. Kish, H. Landsman, R. F. Lang, M. Le Calloch, D. Lellouch, C. Levy, S. Lindemann, M. Lindner, J. A. M. Lope, K. Lung, A. Lyashenko, S. MacMullin, T. Marrodán Undagoitia, J. Masbou, F. V. Massoli, D. Mayani Para, A. J. Melgarejo Fernandez, Y. Meng, M. Messina, B. Miguez, A. Molinario, M. Murra, J. Naganoma, K. Ni, U. Oberlack, S. E. A. Orrigo, E. Pantic, R. Persiani, F. Piastra, J. Pienaar, G. Plante, N. Priel, S. Reichard, C. Reuter, A. Rizzo, S. Rosendahl, J. M. F. dos Santo, G. Sartorelli, S. Schindler, J. Schreiner, M. Schumann, L. Scotto Lavina, M. Selvi, P. Shagin, H. Simgen, A. Teymourian, D. Ther, A. Tiseni, G. Trinchero, O. Vitell, H. Wang, M. Weber, C. Weinheimer, and The XENON100 Collaboration

Subjects

Nuclear and High Energy Physics, Particle physics, Astrophysics and Astronomy, Cosmology and Nongalactic Astrophysics (astro-ph.CO), astro-ph.GA, Dark matter, chemistry.chemical_element, FOS: Physical sciences, Astrophysics, 01 natural sciences, Cosmology, dark matter, Xenon, High Energy Physics - Phenomenology (hep-ph), Assioni, 0103 physical sciences, 010306 general physics, Axion, Liquid Xenon, Coupling, Coupling constant, Quantum chromodynamics, Physics, 010308 nuclear & particles physics, hep-ph, Astrophysics - Astrophysics of Galaxies, Galaxy, High Energy Physics - Phenomenology, chemistry, [PHYS.HPHE]Physics [physics]/High Energy Physics - Phenomenology [hep-ph], Astrophysics of Galaxies (astro-ph.GA), astro-ph.CO, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

We present the first results of searches for axions and axion-like-particles with the XENON100 experiment. The axion-electron coupling constant, $g_{Ae}$, has been tested by exploiting the axio-electric effect in liquid xenon. A profile likelihood analysis of 224.6 live days $\times$ 34 kg exposure has shown no evidence for a signal. By rejecting $g_{Ae}$, larger than $7.7 \times 10^{-12}$ (90% CL) in the solar axion search, we set the best limit to date on this coupling. In the frame of the DFSZ and KSVZ models, we exclude QCD axions heavier than 0.3 eV/c$^2$ and 80 eV/c$^2$, respectively. For axion-like-particles, under the assumption that they constitute the whole abundance of dark matter in our galaxy, we constrain $g_{Ae}$, to be lower than $1 \times 10^{-12}$ (90% CL) for masses between 5 and 10 keV/c$^2$. We present the first results of searches for axions and axionlike particles with the XENON100 experiment. The axion-electron coupling constant, gAe, has been probed by exploiting the axioelectric effect in liquid xenon. A profile likelihood analysis of 224.6 live days × 34-kg exposure has shown no evidence for a signal. By rejecting gAe larger than 7.7×10-12 (90% C.L.) in the solar axion search, we set the best limit to date on this coupling. In the frame of the DFSZ and KSVZ models, we exclude QCD axions heavier than 0.3 and 80 eV/c2, respectively. For axionlike particles, under the assumption that they constitute the whole abundance of dark matter in our galaxy, we constrain gAe to be lower than 1×10-12 (90% C.L.) for masses between 5 and 10 keV/c2. We present the first results of searches for axions and axion-like-particles with the XENON100 experiment. The axion-electron coupling constant, $g_{Ae}$, has been probed by exploiting the axio-electric effect in liquid xenon. A profile likelihood analysis of 224.6 live days $\times$ 34 kg exposure has shown no evidence for a signal. By rejecting $g_{Ae}$, larger than $7.7 \times 10^{-12}$ (90\% CL) in the solar axion search, we set the best limit to date on this coupling. In the frame of the DFSZ and KSVZ models, we exclude QCD axions heavier than 0.3 eV/c$^2$ and 80 eV/c$^2$, respectively. For axion-like-particles, under the assumption that they constitute the whole abundance of dark matter in our galaxy, we constrain $g_{Ae}$, to be lower than $1 \times 10^{-12}$ (90\% CL) for mass range from 1 to 40 keV/c$^2$, and set the best limit to date as well.

Published

2014

20. Response of the XENON100 dark matter detector to nuclear recoils

Author

Aprile, E., Alfonsi, M., Arisaka, K., Arneodo, F., Balan, C., Baudis, L., Bauermeister, B., Behrens, A., Beltrame, P., Bokeloh, K., Brown, A., Brown, E., Brünner, S., Bruno, G., Budnik, R., Cardoso, J., Chen, W., Choi, B., Colijn, A., Contreras, H., Cussonneau, J., Decowski, M., Duchovni, E., Fattori, S., Ferella, A., Fulgione, W., Gao, F., Garbini, M., Geis, C., Ghag, C., Giboni, K., Goetzke, L., Grignon, C., Gross, E., Hampel, W., Itay, R., Kaether, F., Kessler, G., Kish, A., Lamblin, J., Landsman, H., Lang, R., Calloch, M., Levy, C., Lim, K., Lin, Q., Lindemann, S., Lindner, M., Lopes, J., Lung, K., Marrodan Undagoitia, T., Undagoitia, T., Fernandez, A., Meng, Y., Messina, M., Molinario, A., Ni, K., Oberlack, U., Orrigo, S., Pantic, E., Persiani, R., Plante, G., Priel, N., Rizzo, A., Rosendahl, S., Santos, J., Sartorelli, G., Schreiner, J., Schumann, M., Lavina, L., Scovell, P., Selvi, M., Shagin, P., Simgen, H., Teymourian, A., Thers, D., Vitells, O., Wang, H., Weber, M., Weinheimer, C., Schuhmacher, H., Wiegel, B., Astroparticle Physics (IHEF, IoP, FNWI), Laboratoire SUBATECH Nantes (SUBATECH), Centre National de la Recherche Scientifique (CNRS)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université de Nantes (UN)-Mines Nantes (Mines Nantes), XENON100, E. Aprile, M. Alfonsi, K. Arisaka, F. Arneodo, C. Balan, L. Baudi, B. Bauermeister, A. Behren, P. Beltrame, K. Bokeloh, A. Brown, E. Brown, S. Bruenner, G. Bruno, R. Budnik, J. M. R. Cardoso, W.-T. Chen, B. Choi, A. P. Colijn, H. Contrera, J. P. Cussonneau, M. P. Decowski, E. Duchovni, S. Fattori, A. D. Ferella, W. Fulgione, F. Gao, M. Garbini, C. Gei, C. Ghag, K.-L. Giboni, L. W. Goetzke, C. Grignon, E. Gro, W. Hampel, R. Itay, F. Kaether, G. Kessler, A. Kish, H. Landsman, R. F. Lang, M. Le Calloch, C. Levy, K. E. Lim, Q. Lin, S. Lindemann, M. Lindner, J. A. M. Lope, K. Lung, T. Marrodán Undagoitia, F. V. Massoli, A. J. Melgarejo Fernandez, Y. Meng, M. Messina, A. Molinario, K. Ni, U. Oberlack, S. E. A. Orrigo, E. Pantic, R. Persiani, G. Plante, N. Priel, A. Rizzo, S. Rosendahl, J. M. F. dos Santo, G. Sartorelli, J. Schreiner, M. Schumann, L. Scotto Lavina, P. R. Scovell, M. Selvi, P. Shagin, H. Simgen, A. Teymourian, D. Ther, O. Vitell, H. Wang, M. Weber, C. Weinheimer, H. Schuhmacher, B. Wiegel, and XENON Collaboration

Subjects

Nuclear and High Energy Physics, [PHYS.ASTR.IM]Physics [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], Cosmology and Nongalactic Astrophysics (astro-ph.CO), [SDU.ASTR.CO]Sciences of the Universe [physics]/Astrophysics [astro-ph]/Cosmology and Extra-Galactic Astrophysics [astro-ph.CO], Physics::Instrumentation and Detectors, Monte Carlo method, Dark matter, FOS: Physical sciences, 01 natural sciences, dark matter, Particle detector, Nuclear physics, [PHYS.ASTR.CO]Physics [physics]/Astrophysics [astro-ph]/Cosmology and Extra-Galactic Astrophysics [astro-ph.CO], Recoil, Ionization, 0103 physical sciences, 010306 general physics, Nuclear Experiment, Instrumentation and Methods for Astrophysics (astro-ph.IM), Physics, Scintillation, 010308 nuclear & particles physics, Detector, Astrophysics::Instrumentation and Methods for Astrophysics, [SDU.ASTR.IM]Sciences of the Universe [physics]/Astrophysics [astro-ph]/Instrumentation and Methods for Astrophysic [astro-ph.IM], Neutron source, Astrophysics - Instrumentation and Methods for Astrophysics, Astrophysics - Cosmology and Nongalactic Astrophysics

Abstract

Results from the nuclear recoil calibration of the XENON100 dark matter detector installed underground at the Laboratori Nazionali del Gran Sasso (LNGS), Italy are presented. Data from measurements with an external 241AmBe neutron source are compared with a detailed Monte Carlo simulation which is used to extract the energy dependent charge-yield Qy and relative scintillation efficiency Leff. A very good level of absolute spectral matching is achieved in both observable signal channels - scintillation S1 and ionization S2 - along with agreement in the 2-dimensional particle discrimination space. The results confirm the validity of the derived signal acceptance in earlier reported dark matter searches of the XENON100 experiment., Comment: 10 pages, 10 figures. Matches version accepted by PRD. Contains revised representation of expected WIMP event signature. Conclusions remain unaffected

Published

2013

21. The burden of all-cause mortality following influenza-associated hospitalizations, FluSurv-NET, 2010-2019.

Author

O'Halloran AC, Millman AJ, Holstein R, Olsen SJ, Cummings C, Chai SJ, Kirley PD, Alden NB, Yousey-Hindes K, Meek J, Openo KP, Fawcett E, Ryan PA, Leegwater L, Henderson J, McMahon M, Lynfield R, Angeles KM, Bleecker M, McGuire S, Spina NL, Tesini BL, Gaitan MA, Lung K, Shiltz E, Thomas A, Talbott HK, Schaffner W, Hill M, Reed C, and Garg S

Abstract

Background: While the estimated number of U.S. influenza-associated deaths is reported annually, detailed data on the epidemiology of influenza-associated deaths, including the burden of in-hospital versus post-hospital discharge deaths are limited., Methods: Using data from the 2010-11 through 2018-19 seasons from the Influenza Hospitalization Surveillance Network, we linked cases to death certificates to identify patients who died from any cause during their influenza hospital stay or within 30 days post discharge. We described demographic and clinical characteristics of patients who died in hospital versus post discharge and characterized locations and causes of death (COD)., Results: Among 121,390 cases hospitalized with laboratory-confirmed influenza over 9 seasons, 5.5% died; 76% of deaths were in patients ≥65 years, 71% were non-Hispanic White, and 34% had ≥4 underlying medical conditions. Among all patients with an influenza-associated hospitalization who died, 48% of deaths occurred after hospital discharge; the median days from discharge to death was 9 days (IQR 3-19 days). Post-discharge deaths more often occurred in older patients and among those with underlying medical conditions. Only 37% of patients who died had "influenza" as a COD on their death certificate. Influenza was more frequently listed as a COD among persons who died in-hospital compared with cardiovascular disease among those who died after discharge., Conclusions: All-cause mortality burden is substantial among patients hospitalized with influenza, with almost 50% of deaths occurring within 30 days after hospital discharge. Surveillance systems should consider capture of post-discharge outcomes to better characterize the impact of influenza on all-cause mortality., (Published by Oxford University Press on behalf of Infectious Diseases Society of America 2024.)

Published

2024

22. Laboratory-Confirmed Influenza-Associated Hospitalizations Among Children and Adults - Influenza Hospitalization Surveillance Network, United States, 2010-2023.

Author

Naquin A, O'Halloran A, Ujamaa D, Sundaresan D, Masalovich S, Cummings CN, Noah K, Jain S, Kirley PD, Alden NB, Austin E, Meek J, Yousey-Hindes K, Openo K, Witt L, Monroe ML, Henderson J, Nunez VT, Lynfield R, McMahon M, Shaw YP, McCahon C, Spina N, Engesser K, Tesini BL, Gaitan MA, Shiltz E, Lung K, Sutton M, Hendrick MA, Schaffner W, Talbot HK, George A, Zahid H, Reed C, Garg S, and Bozio CH

Subjects

Humans, United States epidemiology, Adult, Middle Aged, Adolescent, Child, Young Adult, Child, Preschool, Infant, Aged, Female, Male, Infant, Newborn, Hospitalization statistics & numerical data, Influenza, Human epidemiology, Population Surveillance, Seasons

Abstract

Problem/condition: Seasonal influenza accounts for 9.3 million-41 million illnesses, 100,000-710,000 hospitalizations, and 4,900-51,000 deaths annually in the United States. Since 2003, the Influenza Hospitalization Surveillance Network (FluSurv-NET) has been conducting population-based surveillance for laboratory-confirmed influenza-associated hospitalizations in the United States, including weekly rate estimations and descriptions of clinical characteristics and outcomes for hospitalized patients. However, a comprehensive summary of trends in hospitalization rates and clinical data collected from the surveillance platform has not been available., Reporting Period: 2010-11 through 2022-23 influenza seasons., Description of System: FluSurv-NET conducts population-based surveillance for laboratory-confirmed influenza-associated hospitalizations among children and adults. During the reporting period, the surveillance network included 13-16 participating sites each influenza season, with prespecified geographic catchment areas that covered 27 million-29 million persons and included an estimated 8.8%-9.5% of the U.S. population. A case was defined as a person residing in the catchment area within one of the participating states who had a positive influenza laboratory test result within 14 days before or at any time during their hospitalization. Each site abstracted case data from hospital medical records into a standardized case report form, with selected variables submitted to CDC on a weekly basis for rate estimations. Weekly and cumulative laboratory-confirmed influenza-associated hospitalization rates per 100,000 population were calculated for each season from 2010-11 through 2022-23 and stratified by patient age (0-4 years, 5-17 years, 18-49 years, 50-64 years, and ≥65 years), sex, race and ethnicity, influenza type, and influenza A subtype. During the 2020-21 season, only the overall influenza hospitalization rate was reported because case counts were insufficient to estimate stratified rates., Results: During the 2010-11 to 2022-23 influenza seasons, laboratory-confirmed influenza-associated hospitalization rates varied significantly across seasons. Before the COVID-19 pandemic, hospitalization rates per 100,000 population ranged from 8.7 (2011-12) to 102.9 (2017-18) and had consistent seasonality. After SARS-CoV-2 emerged, the hospitalization rate for 2020-21 was 0.8, and the rate did not return to recent prepandemic levels until 2022-23. Inconsistent seasonality also was observed during 2020-21 through 2022-23, with influenza activity being very low during 2020-21, extending later than usual during 2021-22, and occurring early during 2022-23. Molecular assays, particularly multiplex standard molecular assays, were the most common influenza test type in recent seasons, increasing from 12% during 2017-18 for both pediatric and adult cases to 43% and 55% during 2022-23 for pediatric and adult cases, respectively. During each season, adults aged ≥65 years consistently had the highest influenza-associated hospitalization rate across all age groups, followed in most seasons by children aged 0-4 years. Black or African American and American Indian or Alaska Native persons had the highest age-adjusted influenza-associated hospitalization rates across these seasons. Among patients hospitalized with influenza, the prevalence of at least one underlying medical condition increased with increasing age, ranging from 36.9% among children aged 0-4 years to 95.4% among adults aged ≥65 years. Consistently across each season, the most common underlying medical conditions among children and adolescents were asthma, neurologic disorders, and obesity. The most common underlying medical conditions among adults were hypertension, obesity, chronic metabolic disease, chronic lung disease, and cardiovascular disease. The proportion of FluSurv-NET patients with acute respiratory signs and symptoms at hospital admission decreased from 90.6% during 2018-19 to 83.2% during 2022-23. Although influenza antiviral use increased during the 2010-11 through the 2017-18 influenza seasons, it decreased from 90.2% during 2018-19 to 79.1% during 2022-23, particularly among children and adolescents. Admission to the intensive care unit, need for invasive mechanical ventilation, and in-hospital death ranged from 14.1% to 22.3%, 4.9% to 11.1%, and 2.2% to 3.5% of patients hospitalized with influenza, respectively, during the reported surveillance period., Interpretations: Influenza continues to cause severe morbidity and mortality, particularly in older adults, and disparities have persisted in racial and ethnic minority groups. Persons with underlying medical conditions represented a large proportion of patients hospitalized with influenza. Increased use of multiplex tests and other potential changes in facility-level influenza testing practices (e.g., influenza screening at all hospital admissions) could have implications for the detection of influenza infections among hospitalized patients. Antiviral use decreased in recent seasons, and explanations for the decrease should be further evaluated., Public Health Action: Continued robust influenza surveillance is critical to monitor progress in efforts to encourage antiviral treatment and improve clinical outcomes for persons hospitalized with influenza. In addition, robust influenza surveillance can potentially reduce disparities by informing efforts to increase access to preventive measures for influenza and monitoring any subsequent changes in hospitalization rates., Competing Interests: All authors have completed and submitted the International Committee of Medical Journal Editors form for disclosure of potential conflicts of interest. Andrea George reported that her institution (Salt Lake County Health Department) receives grant funds from Council of State and Territorial Epidemiologists. Justin Henderson reported receiving grant funds from CDC to conduct the Michigan Emerging Infections Program; grant funds from Council of State and Territorial Epidemiologists to conduct work on Respiratory Virus Hospitalization Network. Ruth Lynfield reported receiving grant funds for a cooperative agreement between CDC and Minnesota Department of Health to conduct Minnesota Emerging Infections Program; attendance at Council of State and Territorial Epidemiologists, American Academy of Pediatrics Committee on Infections Diseases, National Foundation for Infectious Diseases, and Infectious Diseases Week meetings with support from Council of State and Territorial Epidemiologists, National Foundation for Infectious Diseases, and Infectious Diseases Society of America; voluntary positions of Council of State and Territorial Epidemiologists executive officer, American Academy of Pediatrics Red Book associate editor, National Foundation for Infectious Diseases secretary, and Infectious Diseases Week Program Committee; received fee for work as American Academy of Pediatrics Red Book associate editor; donated to Minnesota Department of Health. James Meek reported receiving grant funds from CDC to conduct the Connecticut Emerging Infections Program. Maya L. Monroe reported receiving grant funds from CDC to conduct the Maryland Emerging Infections Program. Angelle Naquin reported one-time funding support for attending meetings, travel, or both from Council of State and Territorial Epidemiologists. William Schaffner reported his institution receiving grant funds for a cooperative agreement between CDC and Vanderbilt University Medical Center to conduct Tennessee Emerging Infections Program. Yomei P. Shaw reported receiving grant funds from CDC to conduct the New Mexico Emerging Infections Program at New Mexico Department of Health; receives funding from CDC to attend annual surveillance officer and principal investigator meetings. Eli Shiltz reported grant funding for the population-based Influenza Hospitalization Surveillance Project and COVID-NET activities from Council of State and Territorial Epidemiologists; recipient of Epidemiology and Laboratory Capacity and Immunizations and Vaccines for Children grant funding from CDC. Devi Sundaresan reported one-time funding support for attending meetings, travel, or both from Council of State and Territorial Epidemiologists. H. Keipp Talbot reported receiving CDC research grants. Val Tellez Nunez reported receiving grant funds from Council of State and Territorial Epidemiologists. Brenda L. Tesini reported receiving a stipend for participation on Merck Manuals editorial board, independent from pharmaceutical branch of company. Dawud Ujamaa reported one-time funding support for attending meetings, travel, or both from Council of State and Territorial Epidemiologists. Lucy Witt reported participation as a site investigator for Merck & Co. from February 2022 through February 2024 for work not related to this report; unpaid participation on Infection Control Today editorial advisory board, MJH Life Sciences. Kimberly Yousey-Hindes reported receiving grant funds from CDC to conduct the Connecticut Emerging Infections Program. No other conflicts of interest were reported.

Published

2024

23. Contrasting predictors of severe primary graft dysfunction following transplant for chronic and acute respiratory failure.

Author

Kurihara C, Kaiho T, Thomae B, Cerier E, Lung K, Avella Patino D, Toyoda T, Yan Y, Budinger GRS, and Bharat A

Abstract

Background: Lung transplantation represents a pivotal intervention for individuals grappling with end-stage lung diseases, and the role of lung transplantation in acute respiratory distress syndrome (ARDS) patients has garnered increased attention especially after the coronavirus disease 2019 (COVID-19) pandemic. Multiple studies have demonstrated a high incidence of primary graft dysfunction (PGD) in patients with ARDS compared to contemporaneous controls undergoing transplantation for chronic end-stage lung diseases although underlying mechanisms or risk factors remain unknown. This retrospective study investigates the contrasting risk factors for PGD grade 3 in patients with ARDS and chronic respiratory failure undergoing lung transplantation., Methods: The study included 293 patients who underwent lung transplantation from January 2018 through June 2023. We performed a multivariate logistic regression analysis using variables from the univariate logistic regression analyses to predict PGD grade 3., Results: Our findings reveal distinct predictors for PGD grade 3 in the two cohorts. ARDS patients had higher incidence of PGD grade 3 than non-ARDS patients (30.2% vs. 9.6%, P<0.001). Multivariate logistic regression analysis showed ischemic time [odds ratio (OR) =0.60; 95% confidence interval (CI): 0.40-0.90; P=0.01] as predictor of PGD grade 3 for non-ARDS patients, and age (OR =0.72; 95% CI: 0.52-0.99; P=0.048), pre-operative albumin (OR <0.01; 95% CI: <0.01-0.74; P=0.042) for ARDS patients. Interestingly, there was no notable difference in post-transplant survival between the two groups., Conclusions: This study highlights differing risk profiles for severe PGD in ARDS and non-ARDS lung transplant recipients, underscoring the need for tailored approaches in managing these patients. It paves the way for further research to refine strategies aimed at reducing PGD incidence and enhancing transplant outcomes in these distinct populations., Competing Interests: Conflicts of Interest: All authors have completed the ICMJE uniform disclosure form (available at https://jtd.amegroups.com/article/view/10.21037/jtd-24-100/coif). The authors have no conflicts of interest to declare., (2024 Journal of Thoracic Disease. All rights reserved.)

Published

2024

24. Timing of influenza antiviral therapy and risk of death in adults hospitalized with influenza-associated pneumonia, FluSurv-NET, 2012-2019.

Author

Tenforde MW, Noah KP, O'Halloran AC, Kirley PD, Hoover C, Alden NB, Armistead I, Meek J, Yousey-Hindes K, Openo KP, Witt LS, Monroe ML, Ryan PA, Falkowski A, Reeg L, Lynfield R, McMahon M, Hancock EB, Hoffman MR, McGuire S, Spina NL, Felsen CB, Gaitan MA, Lung K, Shiltz E, Thomas A, Schaffner W, Talbot HK, Crossland MT, Price A, Masalovich S, Adams K, Holstein R, Sundaresan D, Uyeki TM, Reed C, Bozio CH, and Garg S

Abstract

Background: Pneumonia is common in adults hospitalized with laboratory-confirmed influenza, but the association between timeliness of influenza antiviral treatment and severe clinical outcomes in patients with influenza-associated pneumonia is not well characterized., Methods: We included adults aged ≥18 years hospitalized with laboratory-confirmed influenza and a discharge diagnosis of pneumonia over 7 influenza seasons (2012-2019) sampled from a multi-state population-based surveillance network. We evaluated 3 treatment groups based on timing of influenza antiviral initiation relative to admission date (day 0, day 1, days 2-5). Baseline characteristics and clinical outcomes were compared across groups using unweighted counts and weighted percentages accounting for the complex survey design. Logistic regression models were generated to evaluate the association between delayed treatment and 30-day all-cause mortality., Results: 26,233 adults were sampled in the analysis. Median age was 71 years and most (92.2%) had ≥1 non-immunocompromising condition. Overall, 60.9% started antiviral treatment on day 0, 29.5% on day 1, and 9.7% on days 2-5 (median 2 days). Baseline characteristics were similar across groups. Thirty-day mortality occurred in 7.5%, 8.5%, and 10.2% of patients who started treatment on day 0, day 1, and days 2-5, respectively. Compared to those treated on day 0, adjusted OR for death was 1.14 (95%CI: 1.01-1.27) in those starting treatment on day 1 and 1.40 (95%CI: 1.17-1.66) in those starting on days 2-5., Discussion: Delayed initiation of antiviral treatment in patients hospitalized with influenza-associated pneumonia was associated with higher risk of death, highlighting the importance of timely initiation of antiviral treatment at admission., (Published by Oxford University Press on behalf of Infectious Diseases Society of America 2024.)

Published

2024

25. Patterns and Disparities in Recorded Gonioscopy During Initial Glaucoma Evaluations in the United States.

Author

Lee JH, Yoo K, Lung K, Apolo G, Toy B, Sanvicente C, and Xu B

Subjects

Humans, Male, Female, Retrospective Studies, United States epidemiology, Aged, Middle Aged, Case-Control Studies, Tomography, Optical Coherence methods, Visual Fields physiology, Healthcare Disparities, Aged, 80 and over, Gonioscopy, Intraocular Pressure physiology, Glaucoma diagnosis, Glaucoma ethnology

Abstract

Purpose: To assess patterns in gonioscopy during initial glaucoma evaluations in the United States., Design: Retrospective, case-control study., Methods: Patients undergoing initial glaucoma evaluation between 2009-2020 were identified in the Optum Clinformatics DataMart. Initial evaluation was defined as follows: (1) glaucoma suspect, anatomical narrow angle (ANA), or primary/secondary glaucoma diagnosed by an ophthalmologist; (2) continuously observable during a 36-month lookback period; (3) no history of glaucoma medications, laser, or surgical procedures; and (4) optical coherence tomography (OCT) or visual field performed within 6 months of initial diagnosis. Logistic regression models were developed to identify factors associated with no record of gonioscopy based on Current Procedural Terminology (CPT) codes., Results: Among 198,995 patients, 20.4% and 29.5% had recorded gonioscopy on the day of diagnosis or within 6 months, respectively. On multivariable analysis, odds of recorded gonioscopy within 6 months of initial evaluation was lower (P < .001) among non-Hispanic Whites (OR=0.84) but similar for Blacks (OR=1.02) and Hispanics (OR=0.96) compared with Asians. Age ≥60 years (OR<0.82), pseudophakia/aphakia (OR=0.58), or residence outside of the Northeast region (OR=0.66-0.84) conferred lower odds of recorded gonioscopy (P < .001). Angle closure glaucoma (OR=0.85), secondary glaucoma (OR=0.31), or open angle glaucoma/suspect (OR=0.12/0.24, respectively) patients were less likely to have recorded gonioscopy compared to ANA patients (P < .01)., Conclusions: More than 70% patients undergoing initial glaucoma evaluation in the United States do not have a record of gonioscopy, especially elderly, non-Hispanic White, and pseudophakic patients in non-Northeast regions. This pattern does not conform to current practice guidelines and could contribute to misdiagnosed disease and suboptimal outcomes., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

26. Atopic Dermatitis and the Risk of Actinic Keratosis Development: A Population-Based Study.

Author

Huang MY, Peterson H, Yee D, Lee K, Korouri E, Kingston P, Agüero R, Lung K, and Armstrong AW

Subjects

Humans, Female, Male, Middle Aged, Risk Factors, Aged, Adult, Keratosis, Actinic etiology, Keratosis, Actinic epidemiology, Dermatitis, Atopic epidemiology, Dermatitis, Atopic etiology

Published

2024

27. Practice Patterns and Sociodemographic Disparities in the Clinical Care of Anatomical Narrow Angles in the United States.

Author

Yoo K, Apolo G, Lung K, Toy B, and Xu B

Subjects

Humans, United States epidemiology, Iridectomy, Retrospective Studies, Intraocular Pressure, Iris surgery, Glaucoma, Angle-Closure diagnosis, Ocular Hypertension etiology, Laser Therapy adverse effects, Cataract etiology

Abstract

Purpose: To assess treatment and visit patterns among patients with newly diagnosed anatomical narrow angle (ANA) and identify sociodemographic factors associated with disparities in care., Design: Retrospective practice pattern evaluation study., Methods: A total of 263,422 patients diagnosed with ANA between 2007 and 2019 were identified in the Optum Clinformatics Data Mart. Inclusion was limited to newly diagnosed ANA, defined as (1) continuous enrollment during a 2-year lookback period and 1-year study period from first diagnosis; (2) diagnosis by an ophthalmologist or optometrist; and (3) no history of pseudophakia, ANA treatments, or prior primary angle closure glaucoma diagnosis. Outcome measures were treatment with laser peripheral iridotomy (LPI), cataract surgery, or intraocular pressure-lowering medications and number of eye care visits. Logistic and Poisson regression were performed to assess factors associated with treatment and eye care visits, respectively., Results: Among 52,405 eligible cases, 27.7% received LPI, 13.9% received drops, and 15.1% received cataract surgery. Odds of LPI were higher in Asians and Hispanics (odds ratio [OR] ≥ 1.16, P < .001). Non-Whites had higher odds of drops (OR ≥ 1.19, P < .001), but Hispanics had lower odds of cataract surgery (OR = 0.79, P < .001). The mean number of eye care visits was 2.6±2.1 including the day of diagnosis. Older age and treatment were associated with higher rates of eye care visits (rate ratio > 1.15, P < .001)., Conclusion: More than a quarter of patients with newly diagnosed ANA receive treatment with LPI. Racial minorities are more likely to receive ANA-specific treatments but less likely to receive cataract surgery. These differences may reflect racial differences in disease severity and the need for clearer practice guidelines in ANA care., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

28. Chemical Localization With Robotic Bronchoscopy: Can It Aid Resection of Subsolid Lung Nodules?

Author

Dolan DP, Lee DN, Bharat A, Lung K, Odell D, and Kim S

Subjects

Humans, Bronchoscopy methods, Retrospective Studies, Thoracic Surgery, Video-Assisted methods, Lung diagnostic imaging, Lung surgery, Lung pathology, Multiple Pulmonary Nodules diagnostic imaging, Multiple Pulmonary Nodules surgery, Robotic Surgical Procedures, Lung Neoplasms diagnostic imaging, Lung Neoplasms surgery, Lung Neoplasms pathology, Precancerous Conditions

Abstract

Introduction: Subsolid nodules or those located deep in lung parenchyma are difficult to localize using minimally invasive thoracic surgery. While image-guided percutaneous needle localization has been performed, it is inconvenient and has potential complications. In this study, the role of chemical localization using robotic bronchoscopy to facilitate resection was evaluated., Methods: Consecutive patients undergoing surgical resection for lung nodules between 8/2019-3/2022 were included. Patients with subsolid lung nodules, or small nodules deep in lung parenchyma that were deemed difficult to localize, were chemically localized (CL) using robotic bronchoscopy before resection. Clinico-demographic data were obtained retrospectively using a prospectively maintained database., Results: Localization of lung nodules before resection was performed in 139 patients while 110 patients were not localized. Daily activity score was higher for localized patients. Nodules in the localized group were smaller (P < 0.001) and had similar solid:ground glass ratio. In the localized group, larger margins were observed, and no re-resection of the parenchymal margin was required. Twenty patients in the non-localized group required re-resection intraoperatively due to close pathological margins or inability to locate the nodule in the resected specimen. Operative time was a median of 10-15 min longer for localized patients, P < 0.001. Length of stay was shorter in the localized group (P < 0.05)., Conclusions: Chemical localization of lung nodules using robotic bronchoscopy appears to be a safe and effective method of identifying the location of nodules with small size and less density and aids increased tumor margins intraoperatively., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2024

29. Temporal correlation between postreperfusion complement deposition and severe primary graft dysfunction in lung allografts.

Author

Cerier E, Kurihara C, Kaiho T, Toyoda T, Manerikar A, Kandula V, Thomae B, Yagi Y, Yeldandi A, Kim S, Avella-Patino D, Pandolfino J, Perlman H, Singer B, Scott Budinger GR, Lung K, Alexiev B, and Bharat A

Subjects

Humans, Complement C4b, Retrospective Studies, Lung, Complement System Proteins, Allografts, Graft Rejection etiology, Graft Rejection pathology, Primary Graft Dysfunction etiology, Lung Transplantation adverse effects

Abstract

Growing evidence implicates complement in the pathogenesis of primary graft dysfunction (PGD). We hypothesized that early complement activation postreperfusion could predispose to severe PGD grade 3 (PGD-3) at 72 hours, which is associated with worst posttransplant outcomes. Consecutive lung transplant patients (n = 253) from January 2018 through June 2023 underwent timed open allograft biopsies at the end of cold ischemia (internal control) and 30 minutes postreperfusion. PGD-3 at 72 hours occurred in 14% (35/253) of patients; 17% (44/253) revealed positive C4d staining on postreperfusion allograft biopsy, and no biopsy-related complications were encountered. Significantly more patients with PGD-3 at 72 hours had positive C4d staining at 30 minutes postreperfusion compared with those without (51% vs 12%, P < .001). Conversely, patients with positive C4d staining were significantly more likely to develop PGD-3 at 72 hours (41% vs 8%, P < .001) and experienced worse long-term outcomes. In multivariate logistic regression, positive C4d staining remained highly predictive of PGD-3 (odds ratio 7.92, 95% confidence interval 2.97-21.1, P < .001). Hence, early complement deposition in allografts is highly predictive of PGD-3 at 72 hours. Our data support future studies to evaluate the role of complement inhibition in patients with early postreperfusion complement activation to mitigate PGD and improve transplant outcomes., (Copyright © 2023 American Society of Transplantation & American Society of Transplant Surgeons. Published by Elsevier Inc. All rights reserved.)

Published

2024

30. Postreperfusion Pulmonary Artery Pressure Indicates Primary Graft Dysfunction After Lung Transplant.

Author

Cerier E, Manerikar A, Kandula V, Toyoda T, Thomae B, Yagi Y, Patino DMA, Lung K, Garza-Castillon R Jr, Bharat A, and Kurihara C

Subjects

Humans, Pulmonary Artery, Lung, Risk Factors, Retrospective Studies, Primary Graft Dysfunction etiology, Lung Transplantation adverse effects

Abstract

Background: Primary graft dysfunction is a risk factor of early mortality after lung transplant. Models identifying patients at high risk for primary graft dysfunction are limited. We hypothesize high postreperfusion systolic pulmonary artery pressure is a clinical marker for primary graft dysfunction., Methods: This is a retrospective review of 158 consecutive lung transplants performed at a single academic center from January 2020 through July 2022. Only bilateral lung transplants were included and patients with pretransplant extracorporeal life support were excluded., Results: Primary graft dysfunction occurred in 42.3% (n = 30). Patients with primary graft dysfunction had higher postreperfusion systolic pulmonary artery pressure (41 ± 9.1 mm Hg) than those without (31.5 ± 8.8 mm Hg) (P < .001). Logistic regression showed postreperfusion systolic pulmonary artery pressure is a predictor for primary graft dysfunction (odds ratio 1.14, 95% CI 1.06-1.24, P < .001). Postreperfusion systolic pulmonary artery pressure of 37 mm Hg was optimal for predicting primary graft dysfunction by Youden index. The receiver operating characteristic curve of postreperfusion systolic pulmonary artery pressure at 37 mm Hg (sensitivity 0.77, specificity 0.78, area under the curve 0.81), was superior to the prereperfusion pressure curve at 36 mm Hg (sensitivity 0.77, specificity 0.39, area under the curve 0.57) (P < .01)., Conclusions: Elevated postreperfusion systolic pulmonary artery pressure after lung transplant is predictive of primary graft dysfunction. Postreperfusion systolic pulmonary artery pressure is more indicative of primary graft dysfunction than prereperfusion systolic pulmonary artery pressure. Using postreperfusion systolic pulmonary artery pressure as a positive signal of primary graft dysfunction allows earlier intervention, which could improve outcomes., (Copyright © 2024 The Society of Thoracic Surgeons. Published by Elsevier Inc. All rights reserved.)

Published

2024

31. Association of Chronic Medical Conditions With Severe Outcomes Among Nonpregnant Adults 18-49 Years Old Hospitalized With Influenza, FluSurv-NET, 2011-2019.

Author

Famati EA, Ujamaa D, O'Halloran A, Kirley PD, Chai SJ, Armistead I, Alden NB, Yousey-Hindes K, Openo KP, Ryan PA, Monroe ML, Falkowski A, Kim S, Lynfield R, McMahon M, Angeles KM, Khanlian SA, Spina NL, Bennett NM, Gaitán MA, Shiltz E, Lung K, Thomas A, Talbot HK, Schaffner W, George A, Staten H, Bozio CH, and Garg S

Abstract

Background: Older age and chronic conditions are associated with severe influenza outcomes; however, data are only comprehensively available for adults ≥65 years old. Using data from the Influenza Hospitalization Surveillance Network (FluSurv-NET), we identified characteristics associated with severe outcomes in adults 18-49 years old hospitalized with influenza., Methods: We included FluSurv-NET data from nonpregnant adults 18-49 years old hospitalized with laboratory-confirmed influenza during the 2011-2012 through 2018-2019 seasons. We used bivariate and multivariable logistic regression to determine associations between select characteristics and severe outcomes including intensive care unit (ICU) admission, invasive mechanical ventilation (IMV), and in-hospital death., Results: A total of 16 140 patients aged 18-49 years and hospitalized with influenza were included in the analysis; the median age was 39 years, and 26% received current-season influenza vaccine before hospitalization. Obesity, asthma, and diabetes mellitus were the most common chronic conditions. Conditions associated with a significantly increased risk of severe outcomes included age group 30-39 or 40-49 years (IMV, age group 30-39 years: adjusted odds ratio [aOR], 1.25; IMV, age group 40-49 years: aOR, 1.36; death, age group 30-39 years: aOR, 1.28; death, age group 40-49 years: aOR, 1.69), being unvaccinated (ICU: aOR, 1.18; IMV: aOR, 1.25; death: aOR, 1.48), and having chronic conditions including extreme obesity and chronic lung, cardiovascular, metabolic, neurologic, or liver diseases (ICU: range aOR, 1.22-1.56; IMV: range aOR, 1.17-1.54; death: range aOR, 1.43-2.36)., Conclusions: To reduce the morbidity and mortality associated with influenza among adults aged 18-49 years, health care providers should strongly encourage receipt of annual influenza vaccine and lifestyle/behavioral modifications, particularly among those with chronic medical conditions., Competing Interests: Potential conflicts of interest. D.U. reports that he is a contract employee of GDIT. K.Y.H. reports grants from the CDC for the Connecticut Emerging Infections Program. M.M. reports grants from the CDC for the Emerging Infections Program. P.R. reports funding support from the Emerging Infections Program Cooperative agreement. A.F. reports grants from the Michigan Department of Health and Human Services from the CSTE Federal Grand. S.K. reports grants from the Michigan Department of Health and Human Services from the CSTE Federal Grand. R.L. reports grants from the CDC Emerging Infections Cooperative Agreement to the MN Department of Health. S.K. reports salary and data collection for the manuscript supported by a grant received from the CDC Emerging Infections Program. K.A. reports salary and data collection for the manuscript supported by a grant received from the CDC Emerging Infections Program. N.B. reports an agreement to consult for the GSK. E.S. reports grant funding for the population-based Influenza Hospitalization Surveillance Project (IHSP) and COVID-Net activities, including support for personnel and equipment for data collection activities from the Council for State and Territorial Epidemiologists (CSTE). W.S. reports a grant from the CDC Emerging Infections Program. H.K.T. reports a grant from the CDC. A.G. reports a grant from the CSTE. All other authors report no potential conflicts., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published

2023

32. Severity of influenza-associated hospitalisations by influenza virus type and subtype in the USA, 2010-19: a repeated cross-sectional study.

Author

Sumner KM, Masalovich S, O'Halloran A, Holstein R, Reingold A, Kirley PD, Alden NB, Herlihy RK, Meek J, Yousey-Hindes K, Anderson EJ, Openo KP, Monroe ML, Leegwater L, Henderson J, Lynfield R, McMahon M, McMullen C, Angeles KM, Spina NL, Engesser K, Bennett NM, Felsen CB, Lung K, Shiltz E, Thomas A, Talbot HK, Schaffner W, Swain A, George A, Rolfes MA, Reed C, and Garg S

Subjects

Humans, United States epidemiology, Cross-Sectional Studies, Influenza A Virus, H3N2 Subtype, Influenza B virus, Hospitalization, Influenza, Human therapy, Influenza, Human prevention & control, Influenza Vaccines, Influenza A Virus, H1N1 Subtype, Influenza A virus

Abstract

Background: Influenza burden varies across seasons, partly due to differences in circulating influenza virus types or subtypes. Using data from the US population-based surveillance system, Influenza Hospitalization Surveillance Network (FluSurv-NET), we aimed to assess the severity of influenza-associated outcomes in individuals hospitalised with laboratory-confirmed influenza virus infections during the 2010-11 to 2018-19 influenza seasons., Methods: To evaluate the association between influenza virus type or subtype causing the infection (influenza A H3N2, A H1N1pdm09, and B viruses) and in-hospital severity outcomes (intensive care unit [ICU] admission, use of mechanical ventilation or extracorporeal membrane oxygenation [ECMO], and death), we used FluSurv-NET to capture data for laboratory-confirmed influenza-associated hospitalisations from the 2010-11 to 2018-19 influenza seasons for individuals of all ages living in select counties in 13 US states. All individuals had to have an influenza virus test within 14 days before or during their hospital stay and an admission date between Oct 1 and April 30 of an influenza season. Exclusion criteria were individuals who did not have a complete chart review; cases from sites that contributed data for three or fewer seasons; hospital-onset cases; cases with unidentified influenza type; cases of multiple influenza virus type or subtype co-infection; or individuals younger than 6 months and ineligible for the influenza vaccine. Logistic regression models adjusted for influenza season, influenza vaccination status, age, and FluSurv-NET site compared odds of in-hospital severity by virus type or subtype. When missing, influenza A subtypes were imputed using chained equations of known subtypes by season., Findings: Data for 122 941 individuals hospitalised with influenza were captured in FluSurv-NET from the 2010-11 to 2018-19 seasons; after exclusions were applied, 107 941 individuals remained and underwent influenza A virus imputation when missing A subtype (43·4%). After imputation, data for 104 969 remained and were included in the final analytic sample. Averaging across imputed datasets, 57·7% (weighted percentage) had influenza A H3N2, 24·6% had influenza A H1N1pdm09, and 17·7% had influenza B virus infections; 16·7% required ICU admission, 6·5% received mechanical ventilation or ECMO, and 3·0% died (95% CIs had a range of less than 0·1% and are not displayed). Individuals with A H1N1pdm09 had higher odds of in-hospital severe outcomes than those with A H3N2: adjusted odds ratios (ORs) for A H1N1pdm09 versus A H3N2 were 1·42 (95% CI 1·32-1·52) for ICU admission; 1·79 (1·60-2·00) for mechanical ventilation or ECMO use; and 1·25 (1·07-1·46) for death. The adjusted ORs for individuals infected with influenza B versus influenza A H3N2 were 1·06 (95% CI 1·01-1·12) for ICU admission, 1·14 (1·05-1·24) for mechanical ventilation or ECMO use, and 1·18 (1·07-1·31) for death., Interpretation: Despite a higher burden of hospitalisations with influenza A H3N2, we found an increased likelihood of in-hospital severe outcomes in individuals hospitalised with influenza A H1N1pdm09 or influenza B virus. Thus, it is important for individuals to receive an annual influenza vaccine and for health-care providers to provide early antiviral treatment for patients with suspected influenza who are at increased risk of severe outcomes, not only when there is high influenza A H3N2 virus circulation but also when influenza A H1N1pdm09 and influenza B viruses are circulating., Funding: The US Centers for Disease Control and Prevention., Competing Interests: Declaration of interests EJA has consulted for Pfizer, Sanofi Pasteur, GlaxoSmithKline (GSK), Janssen, Moderna, and Medscape; serves on a safety monitoring board for Kentucky BioProcessing and Sanofi Pasteur; and serves on a data adjudication board for WCG and ACI Clinical. EJA's institution receives funds to conduct clinical research unrelated to this manuscript from MedImmune, Regeneron, PaxVax, Pfizer, GSK, Merck, Sanofi Pasteur, Janssen, and Micron, and has also received funding from the US National Institutes of Health to conduct clinical trials of COVID-19 vaccines. ES notes the agency grant funding supporting the data collection for this project, and agency grant funding from the US Centers for Disease Control and Prevention (CDC) to support other epidemiology projects. HKT, WS, NBA, JM, KY-H, RKH, and RL have received CDC grant funding. JH and LL have received grants from the Michigan Department of Health and Human Services. ES reports grants from the Council for State and Territorial Epidemiologists (CSTE) during the conduct of the study and grants from CDC outside the submitted work. AG reports grants from CSTE. All other authors declare no competing interests., (Copyright © 2023 Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2023

33. Lung Transplantation in Coronavirus-19 Patients: What We Have Learned So Far.

Author

Cerier E, Lung K, Kurihara C, and Bharat A

Subjects

Humans, SARS-CoV-2, Follow-Up Studies, COVID-19, Respiratory Distress Syndrome surgery, Lung Transplantation

Abstract

Coronavirus-19 (COVID-19) can result in irrecoverable acute respiratory distress syndrome (ARDS) or life-limiting fibrosis for which lung transplantation is currently the only viable treatment. COVID-19 lung transplantation has transformed the field of lung transplantation, as before the pandemic, few transplants had been performed in the setting of infectious disease or ARDS. Given the complexities associated with COVID-19 lung transplantation, it requires strict patient selection with an experienced multidisciplinary team in a high-resource hospital setting. Current short-term outcomes of COVID-19 lung transplantation are promising. However, follow-up studies are needed to determine long-term outcomes and whether these patients may be predisposed to unique complications., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

34. Rural-Urban Disparities in Receipt of Surgery for Potentially Resectable Non-Small Cell Lung Cancer.

Author

Logan CD, Feinglass J, Halverson AL, Durst D, Lung K, Kim S, Bharat A, Merkow RP, Bentrem DJ, and Odell DD

Subjects

Humans, Rural Population, Healthcare Disparities, Carcinoma, Non-Small-Cell Lung surgery, Lung Neoplasms surgery

Abstract

Introduction: Access to cancer care, especially surgery, is limited in rural areas. However, the specific reasons rural patient populations do not receive surgery for non-small cell lung cancer (NSCLC) is unknown. We investigated geographic disparities in reasons for failure to receive guideline-indicated surgical treatment for patients with potentially resectable NSCLC., Methods: The National Cancer Database was used to identify patients with clinical stage I-IIIA (N0-N1) NSCLC between 2004 and 2018. Patients from rural areas were compared to urban areas, and the reason for nonreceipt of surgery was evaluated. Adjusted odds of (1) primary nonsurgical management, (2) surgery being deemed contraindicated due to risk, (3) surgery being recommended but not performed, and (4) overall failure to receive surgery were determined., Results: The study included 324,785 patients with NSCLC with 42,361 (13.0%) from rural areas. Overall, 62.4% of patients from urban areas and 58.8% of patients from rural areas underwent surgery (P < 0.001). Patients from rural areas had increased odds of (1) being recommended primary nonsurgical management (adjusted odds ratio [aOR]: 1.14, 95% confidence interval [CI]: 1.05-1.23), (2) surgery being deemed contraindicated due to risk (aOR: 1.19, 95% CI: 1.07-1.33), (3) surgery being recommended but not performed (aOR: 1.13, 95% CI: 1.01-1.26), and (4) overall failure to receive surgery (aOR: 1.21, 95% CI: 1.13-1.29; all P < 0.001)., Conclusions: There are geographic disparities in the management of NSCLC. Rural patient populations are more likely to fail to undergo surgery for potentially resectable disease for every reason examined., (Copyright © 2022. Published by Elsevier Inc.)

Published

2023

35. Rates and Patterns of Diagnostic Conversion from Anatomical Narrow Angle to Primary Angle-Closure Glaucoma in the United States.

Author

Yoo K, Apolo G, Zhou S, Burkemper B, Lung K, Song B, Wong B, Toy B, Camp A, and Xu B

Subjects

Humans, United States epidemiology, Aged, Retrospective Studies, Case-Control Studies, Intraocular Pressure, Glaucoma, Angle-Closure diagnosis, Glaucoma, Angle-Closure epidemiology, Glaucoma, Angle-Closure surgery, Cataract

Abstract

Purpose: To assess rates of diagnostic conversion from anatomical narrow angle (ANA) to primary angle-closure glaucoma (PACG) in the United States and identify factors associated with diagnostic conversion., Design: Retrospective case-control study., Participants: Patients diagnosed with ANA between the years 2007 and 2019 were identified based on International Classification of Diseases (ICD) codes in the Optum Clinformatics Data Mart Database. Inclusion was limited to newly diagnosed ANA, defined as the following: (1) continuous enrollment during a 2-year look back period and 6-year study period from index (first) date of ANA diagnosis; (2) diagnosis by an ophthalmologist or optometrist and record of gonioscopy; and (3) no history of intraocular pressure (IOP)-lowering drops, laser peripheral iridotomy (LPI), or intraocular surgery., Methods: Cox proportional hazards models were developed to assess factors associated with diagnostic conversion, defined as a change in ICD code from ANA to PACG., Main Outcome Measures: New diagnosis of PACG within the 6-year study period recorded after an index diagnosis of ANA., Results: Among 3985 patients meeting inclusion criteria, 459 (11.52%) had detected diagnostic conversion to PACG within the study period. The conversion rate was stable at 3.54% per year after the first 6 months of ANA diagnosis. In the Cox proportional hazards model, age > 70 years and early (within 6 months of ANA diagnosis) need for LPI or IOP-lowering drops were positively associated with diagnostic conversion (hazard ratio [HR] > 1.59; P < 0.02). Cataract surgery at any time and late (after 6 months of ANA diagnosis) need for IOP-lowering drops appeared protective against diagnostic conversion (HR < 0.46; P < 0.004)., Conclusions: Annual risk of diagnostic conversion from ANA to PACG is relatively low overall; elderly patients are at higher risk whereas patients receiving cataract surgery are at lower risk. The utility of long-term monitoring seems low for most patients with ANA, highlighting the need for improved clinical methods to identify patients at higher risk for PACG., Financial Disclosure(s): Proprietary or commercial disclosure may be found after the references., (Copyright © 2022 American Academy of Ophthalmology. Published by Elsevier Inc. All rights reserved.)

Published

2023

36. National trends in the quality of segmentectomy for lung cancer.

Author

Logan CD, Jacobs RC, Feinglass J, Lung K, Kim S, Bharat A, and Odell DD

Subjects

Humans, Pneumonectomy methods, Mastectomy, Segmental, Neoplasm Staging, Treatment Outcome, Retrospective Studies, Lung Neoplasms pathology, Carcinoma, Non-Small-Cell Lung pathology

Abstract

Objective: Segmentectomy has become an accepted procedure for the treatment of non-small cell lung cancer. Adequate lymph node sampling, sufficient margins, and proper tumor size selection are factors vital for achieving outcomes comparable to lobectomy. Previous studies have demonstrated poor adherence to lymph node sampling guidelines. However, national trends in the quality of segmentectomy and implications on survival are unknown., Methods: The National Cancer Database was used to identify patients with clinical stage I to IIA non-small cell lung cancer surgically treated between 2004 and 2018. Facility-level trends in extent of resection and segmentectomy odds of adherence to (1) 2014 Commission on Cancer guidelines of sampling 10 or more lymph nodes, (2) negative (R0) resection margins, and (3) tumor size 2 cm or less were determined. Propensity score matching was based on segmentectomy adherence to (4) a composite of all measures, and survival was evaluated with Cox models and Kaplan-Meier survival estimates., Results: The study included 249,391 patients with 4.4% (n = 11,006) treated with segmentectomy. The proportion of segmentectomies performed annually increased from 3.3% in 2004 to 6.1% in 2018 (P < .001). Overall, 12.6% (n = 1385) of patients who underwent segmentectomy between 2004 and 2018 were adherent to all measures, and adherence was more likely at academic programs (odds ratio, 1.56; 95% confidence interval, 1.14-2.15) than nonacademic programs (P < .001, reference). Adherence to all measures was associated with improved survival (hazard ratio, 0.67; 95% confidence interval, 0.56-0.79)., Conclusions: As segmentectomy is increasingly established as a valid oncological option for the treatment of non-small cell lung cancer, it is important that quality remains high. This study demonstrates that continued improvement is needed., (Copyright © 2022. Published by Elsevier Inc.)

Published

2023

37. Influenza Antiviral Use in Patients Hospitalized With Laboratory-Confirmed Influenza in the United States, FluSurv-NET, 2015-2019.

Author

Tenforde MW, Cummings CN, O'Halloran AC, Rothrock G, Kirley PD, Alden NB, Meek J, Yousey-Hindes K, Openo KP, Anderson EJ, Monroe ML, Kim S, Nunez VT, McMahon M, McMullen C, Khanlian SA, Spina NL, Muse A, Gaitán MA, Felsen CB, Lung K, Shiltz E, Sutton M, Thomas A, Talbot HK, Schaffner W, Price A, Chatelain R, Reed C, and Garg S

Abstract

From surveillance data of patients hospitalized with laboratory-confirmed influenza in the United States during the 2015-2016 through 2018-2019 seasons, initiation of antiviral treatment increased from 86% to 94%, with increases seen across all age groups. However, 62% started therapy ≥3 days after illness onset, driven by late presentation to care., Competing Interests: Potential conflicts of interest. E.A. has received received grants for clinical trials from Pfizer, Merck, PaxVax, Micron, Sanofi-Pasteur, Janssen, MedImmune, and GSK, has been a consultant for Sanofi-Pasteur, Pfizer, Medscape, Janssen, GSK, and Moderna, has been a member of the data safety monitoring board for Kentucky Bioprocessing and Sanofi-Pasteur, and has been a member of the endpoint adjudication committee for WCG and ACI Clinical. His institution has also received funding from the NIH to conduct clinical trials of COVID-19 vaccines. All other authors report no potential conflicts. All authors have submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest. Conflicts that the editors consider relevant to the content of the manuscript have been disclosed., (Published by Oxford University Press on behalf of Infectious Diseases Society of America 2022.)

Published

2022

38. Association of travel distance, surgical volume, and receipt of adjuvant chemotherapy with survival among patients with resectable lung cancer.

Author

Logan CD, Ellis RJ, Feinglass J, Halverson AL, Avella D, Lung K, Kim S, Bharat A, Merkow RP, Bentrem DJ, and Odell DD

Abstract

Objective: Regionalization of surgery for non-small cell lung cancer (NSCLC) to high-volume centers (HVCs) improves perioperative outcomes but frequently increases patient travel distance. Travel might decrease rates of adjuvant chemotherapy (AC) use, however, the relationship of distance, volume, and receipt of AC with outcomes is unknown. Our objective was to evaluate the association of distance, volume, and receipt of AC with overall survival among patients with NSCLC., Methods: Patients with stage I to IIIA (N0-N1) NSCLC were identified between 2004 and 2018 using the National Cancer Database. Distance to surgical facility was categorized into quartiles (<5.1, 5.1 to <11.5, 11.5 to <28.1, and ≥28.1 miles), and HVCs were defined as those that perform ≥40 annual resections. Patient characteristics and likelihood of receiving AC anywhere were determined. Propensity score-matched survival analysis was performed using Cox models and Kaplan-Meier curves., Results: Of the 131,982 patients included, 35,658 (27.0%) were stage II to IIIA. Of the stage II to IIIA cohort, 49.6% received AC, 13.1% traveled <5.1 miles to low-volume centers (LVCs), and 18.1% traveled ≥28.1 miles to HVCs ( P  < .001). Among stage II to IIIA patients who traveled ≥28.1 miles to HVCs, 45% received AC versus 51.5% who traveled <5.1 miles to LVCs (incidence rate ratio, 0.88; 95% CI, 0.83-0.94; <5.1 miles to LVC reference). Patients with stage II to IIIA NSCLC who traveled ≥28.1 miles to HVCs and did not receive AC had higher mortality rates than those who traveled <5.1 miles to LVCs and received AC (median overall survival, 52.3 vs 36.7 months; adjusted hazard ratio, 1.41; 95% CI, 1.26-1.57)., Conclusions: Increasing travel distance to surgical treatment is associated with decreased likelihood of receiving AC for patients with stage II to IIIA (N0-N1) NSCLC., (© 2022 The Author(s).)

Published

2022

39. Rural-urban survival disparities for patients with surgically treated lung cancer.

Author

Logan CD, Feinglass J, Halverson AL, Lung K, Kim S, Bharat A, and Odell DD

Subjects

Humans, Rural Population, Travel, Income, Lung Neoplasms surgery, Carcinoma, Non-Small-Cell Lung surgery

Abstract

Background: Nonsmall-cell lung cancer (NSCLC) is a common diagnosis among patients living in rural areas and small towns who face unique challenges accessing care. We examined differences in survival for surgically treated rural and small-town patients compared to those from urban and metropolitan areas., Methods: The National Cancer Database was used to identify surgically treated NSCLC patients from 2004 to 2016. Patients from rural/small-town counties were compared to urban/metro counties. Differences in patient clinical, sociodemographic, hospital, and travel characteristics were described. Survival differences were examined with Kaplan-Meier curves and Cox proportional hazards models., Results: The study included 366 373 surgically treated NSCLC patients with 12.4% (n = 45 304) categorized as rural/small-town. Rural/small-town patients traveled farther for treatment and were from areas characterized by lower income and education(all p < 0.001). Survival probabilities for rural/small-town patients were worse at 1 year (85% vs. 87%), 5 years (48% vs. 54%), and 10 years (26% vs. 31%) (p < 0.001). Travel distance >100 miles (hazard ratio [HR] = 1.11, 95% confidence interval [CI]: 1.07-1.16, vs. <25 miles) and living in a rural/small-town county (HR = 1.04, 95% CI: 1.01-1.07) were associated with increased risk for death., Conclusions: Rural and small-town patients with surgically treated NSCLC had worse survival outcomes compared to urban and metropolitan patients., (© 2022 The Authors. Journal of Surgical Oncology published by Wiley Periodicals LLC.)

Published

2022

40. Racial and Sociodemographic Disparities in the Detection of Narrow Angles before Detection of Primary Angle-Closure Glaucoma in the United States.

Author

Apolo G, Bohner A, Pardeshi A, Lung K, Toy B, Wong B, Song B, Camp A, and Xu B

Subjects

Aged, Cross-Sectional Studies, Humans, Intraocular Pressure, Male, Prevalence, Retrospective Studies, United States epidemiology, Glaucoma, Angle-Closure complications, Glaucoma, Angle-Closure diagnosis, Glaucoma, Angle-Closure epidemiology

Abstract

Purpose: To assess the proportion of newly diagnosed cases of primary angle-closure glaucoma (PACG) with and without prior diagnosis of anatomical narrow angle (ANA) and to identify sociodemographic risk factors for late detection (PACG without prior ANA diagnosis)., Design: Retrospective cohort study., Methods: One hundred two thousand six hundred seventeen patients with PACG were identified from the Optum Clinformatics Data Mart Database (2007-2019). Patients with newly diagnosed PACG met the following criteria: (1) diagnosis made by an ophthalmologist, (2) disease observable for at least 12 months before diagnosis, and (3) no history of treatment before diagnosis unless preceded by a diagnosis of ANA. Multivariate logistic regression modeling was performed to identify sociodemographic risk factors for late detection., Main Outcome Measures: Proportion of patients with newly diagnosed PACG without prior ANA diagnosis and sociodemographic factors associated with late detection., Results: Thirty-one thousand forty-four patients were eligible. More than 70% of PACG cases were detected without prior ANA diagnosis, regardless of patient age, sex, or race. The odds of late detection were significantly higher (P < 0.001) among men (odds ratio [OR], 1.32; 95% confidence interval [CI], 1.25-1.40), Black patients (OR, 1.25; 95% CI, 1.15-1.37), and patients 80 years of age or older (OR, 1.28; 95% CI, 1.11-1.47) or living in Southern (OR, 1.30; 95% CI, 1.22-1.40) or Pacific (OR, 1.27; 95% CI, 1.16-1.36) regions. Findings were similar for patients with PACG with a record of gonioscopy and treatment or with a 24-month lookback period., Conclusions: Most patients who receive a new diagnosis of PACG in the United States do not have a prior diagnosis of ANA. The elderly, men, and Black patients are at higher risk of late detection. A need exists for increased disease awareness among providers and more accessible tools to detect patients at risk of developing PACG., (Copyright © 2022 American Academy of Ophthalmology. Published by Elsevier Inc. All rights reserved.)

Published

2022

41. Commentary: Bruised donor lungs-they may not be pretty, but they will still work.

Author

Lung K and Cypel M

Subjects

Humans, Tissue Donors, Lung, Lung Transplantation adverse effects

Published

2022

42. Outcomes after extracorporeal membrane oxygenation support in COVID-19 and non-COVID-19 patients.

Author

Kurihara C, Manerikar A, Gao CA, Watanabe S, Kandula V, Klonis A, Hoppner V, Karim A, Saine M, Odell DD, Lung K, Garza-Castillon R, Kim SS, Walter JM, Wunderink RG, Budinger GRS, and Bharat A

Subjects

Hemorrhage etiology, Humans, Retrospective Studies, Time Factors, COVID-19 complications, COVID-19 therapy, Extracorporeal Membrane Oxygenation adverse effects, Respiratory Distress Syndrome etiology, Respiratory Distress Syndrome therapy

Abstract

Background: Veno-venous extracorporeal membrane oxygenation (V-V ECMO) support is increasingly used in the management of COVID-19-related acute respiratory distress syndrome (ARDS). However, the clinical decision-making to initiate V-V ECMO for severe COVID-19 still remains unclear. In order to determine the optimal timing and patient selection, we investigated the outcomes of both COVID-19 and non-COVID-19 patients undergoing V-V ECMO support., Methods: Overall, 138 patients were included in this study. Patients were stratified into two cohorts: those with COVID-19 and non-COVID-19 ARDS., Results: The survival in patients with COVID-19 was statistically similar to non-COVID-19 patients (p = .16). However, the COVID-19 group demonstrated higher rates of bleeding (p = .03) and thrombotic complications (p < .001). The duration of V-V ECMO support was longer in COVID-19 patients compared to non-COVID-19 patients (29.0 ± 27.5 vs 15.9 ± 19.6 days, p < .01). Most notably, in contrast to the non-COVID-19 group, we found that COVID-19 patients who had been on a ventilator for longer than 7 days prior to ECMO had 100% mortality without a lung transplant., Conclusions: These findings suggest that COVID-19-associated ARDS was not associated with a higher post-ECMO mortality than non-COVID-19-associated ARDS patients, despite longer duration of extracorporeal support. Early initiation of V-V ECMO is important for improved ECMO outcomes in COVID-19 ARDS patients. Since late initiation of ECMO was associated with extremely high mortality related to lack of pulmonary recovery, it should be used judiciously or as a bridge to lung transplantation., (© 2021 International Center for Artificial Organs and Transplantation and Wiley Periodicals LLC.)

Published

2022

43. Response to Comment on Gange et al. Incidence of Proliferative Diabetic Retinopathy and Other Neovascular Sequelae at 5 Years Following Diagnosis of Type 2 Diabetes. Diabetes Care 2021;44:2518-2526.

Author

Lopez J, Gange WS, Lung K, Xu BY, Seabury SA, and Toy BC

Subjects

Glycated Hemoglobin, Humans, Incidence, Diabetes Mellitus, Type 1 complications, Diabetes Mellitus, Type 2 complications, Diabetic Retinopathy complications, Diabetic Retinopathy diagnosis, Diabetic Retinopathy epidemiology

Published

2022

44. Clinical Characteristics and Outcomes of Patients With COVID-19-Associated Acute Respiratory Distress Syndrome Who Underwent Lung Transplant.

Author

Kurihara C, Manerikar A, Querrey M, Felicelli C, Yeldandi A, Garza-Castillon R Jr, Lung K, Kim S, Ho B, Tomic R, Arunachalam A, Budinger GRS, Pesce L, and Bharat A

Subjects

Adult, Aged, Extracorporeal Membrane Oxygenation, Female, Humans, Male, Middle Aged, Respiration, Artificial, Respiratory Distress Syndrome etiology, Retrospective Studies, Treatment Outcome, COVID-19 complications, Lung Transplantation mortality, Respiratory Distress Syndrome surgery

Abstract

Importance: Lung transplantation is a potentially lifesaving treatment for patients who are critically ill due to COVID-19-associated acute respiratory distress syndrome (ARDS), but there is limited information about the long-term outcome., Objective: To report the clinical characteristics and outcomes of patients who had COVID-19-associated ARDS and underwent a lung transplant at a single US hospital., Design, Setting, and Participants: Retrospective case series of 102 consecutive patients who underwent a lung transplant at Northwestern University Medical Center in Chicago, Illinois, between January 21, 2020, and September 30, 2021, including 30 patients who had COVID-19-associated ARDS. The date of final follow-up was November 15, 2021., Exposures: Lung transplant., Main Outcomes and Measures: Demographic, clinical, laboratory, and treatment data were collected and analyzed. Outcomes of lung transplant, including postoperative complications, intensive care unit and hospital length of stay, and survival, were recorded., Results: Among the 102 lung transplant recipients, 30 patients (median age, 53 years [range, 27 to 62]; 13 women [43%]) had COVID-19-associated ARDS and 72 patients (median age, 62 years [range, 22 to 74]; 32 women [44%]) had chronic end-stage lung disease without COVID-19. For lung transplant recipients with COVID-19 compared with those without COVID-19, the median lung allocation scores were 85.8 vs 46.7, the median time on the lung transplant waitlist was 11.5 vs 15 days, and preoperative venovenous extracorporeal membrane oxygenation (ECMO) was used in 56.7% vs 1.4%, respectively. During transplant, patients who had COVID-19-associated ARDS received transfusion of a median of 6.5 units of packed red blood cells vs 0 in those without COVID-19, 96.7% vs 62.5% underwent intraoperative venoarterial ECMO, and the median operative time was 8.5 vs 7.4 hours, respectively. Postoperatively, the rates of primary graft dysfunction (grades 1 to 3) within 72 hours were 70% in the COVID-19 cohort vs 20.8% in those without COVID-19, the median time receiving invasive mechanical ventilation was 6.5 vs 2.0 days, the median duration of intensive care unit stay was 18 vs 9 days, the median post-lung transplant hospitalization duration was 28.5 vs 16 days, and 13.3% vs 5.5% required permanent hemodialysis, respectively. None of the lung transplant recipients who had COVID-19-associated ARDS demonstrated antibody-mediated rejection compared with 12.5% in those without COVID-19. At follow-up, all 30 lung transplant recipients who had COVID-19-associated ARDS were alive (median follow-up, 351 days [IQR, 176-555] after transplant) vs 60 patients (83%) who were alive in the non-COVID-19 cohort (median follow-up, 488 days [IQR, 368-570] after lung transplant)., Conclusions and Relevance: In this single-center case series of 102 consecutive patients who underwent a lung transplant between January 21, 2020, and September 30, 2021, survival was 100% in the 30 patients who had COVID-19-associated ARDS as of November 15, 2021.

Published

2022

45. Anatomy, Abdomen and Pelvis, Arteries

Author

Lung K and Lui F

Abstract

The abdominal arteries arise from the abdominal aorta and are comprised of three groups of arteries: unpaired visceral arteries, paired visceral arteries, and parietal arteries. The unpaired visceral arteries supply the gastrointestinal (GI) tract, spleen, pancreas, gallbladder, and liver and are made up of the celiac trunk, superior mesenteric artery (SMA), and inferior mesenteric artery (IMA). The paired visceral arteries supply the kidneys, adrenal glands, and gonads and are made up of the middle suprarenals, renals, and gonadal branches of the abdominal aorta. The parietal arteries supply the musculoskeletal structures of the abdominal wall and are made up of the inferior phrenic, lumbar, and median sacral branches of the abdominal aorta., (Copyright © 2022, StatPearls Publishing LLC.)

Published

2022

46. Anatomy, Thorax, Long Thoracic Nerve

Author

Lung K and Lui F

Abstract

The long thoracic nerve, also referred to as the external respiratory nerve of Bell or posterior thoracic nerve, arises from the upper portion of the superior trunk of the brachial plexus and typically receives contributions from cervical nerve roots C5, C6, and C7. It is responsible for the innervation of the serratus anterior muscle; the long thoracic nerve descends posteriorly to the roots of the brachial plexus and anteriorly to the scalenus posterior muscle, and courses along the chest wall in the mid-axillary line to lie on the superficial surface of the serratus anterior muscle. Due to its long, relatively superficial course, the long thoracic nerve is susceptible to damage during certain surgical procedures or through direct trauma or stretch. When the long thoracic nerve is injured, a phenomenon known as winging of the scapula results. , (Copyright © 2022, StatPearls Publishing LLC.)

Published

2022

47. Role of Pulmonary Vasodilators in Ameliorating Primary Graft Dysfunction Following Lung Transplant.

Author

Cerier E, Lung K, and Bharat A

Subjects

Humans, Risk Factors, Vasodilator Agents therapeutic use, Lung Transplantation adverse effects, Primary Graft Dysfunction

Published

2022

48. Anatomy, Abdomen and Pelvis, Superior Gluteal Nerve

Author

Lung K and Lui F

Abstract

The superior gluteal nerve is found in the lower pelvis and arises from the dorsal divisions of the L4, L5, and S1 nerve roots of the sacral plexus. The superior gluteal nerve is responsible for innervation of the gluteus medius, gluteus minimus, and tensor fasciae latae muscles. The nerve exits the pelvis through the greater sciatic foramen superior to the piriformis muscle and accompanies the superior gluteal artery and vein. The superior gluteal nerve further divides into a superior branch and an inferior branch, with each branch following the course of the superior gluteal artery’s upper and lower portions of the deep division, respectively. Damage to the superior gluteal nerve results in paralysis of the gluteus medius muscle resulting in a characteristic gait on walking and standing known as the Trendelenburg gait.  , (Copyright © 2022, StatPearls Publishing LLC.)

Published

2022

49. Anatomy, Thorax, Serratus Anterior Muscles

Author

Lung K, St Lucia K, and Lui F

Abstract

The serratus anterior is a fan-shaped muscle that originates on the superolateral surfaces of the first to eighth ribs or the first to ninth ribs at the lateral wall of the thorax and inserts along the superior angle, medial border, and inferior angle of the scapula. The main part of the serratus anterior lies deep to the scapula and the pectoral muscles and is easily palpated between the pectoralis major and latissimus dorsi muscles. This large muscle is generally divided into three distinct parts according to the points of insertion: serratus anterior superior (insertion near the superior angle), serratus anterior intermediate (insertion along the medial border), and serratus anterior inferior (insertion near the inferior angle)., (Copyright © 2022, StatPearls Publishing LLC.)

Published

2022

50. Alternative Input for Perfusion Management Devices: Voice Recognition for Data Input and the Effects on Charting and Perioperative Calculation Use.

Author

Lung K, Brummer B, Sanderson S, and Holt DW

Subjects

Humans, Perfusion, User-Computer Interface, Voice, Voice Recognition

Abstract

Technology in healthcare has become increasingly prevalent and user friendly. In the last decade, advances in hands-free methods of data input have become more viable in a variety of medical professions. The aim of this study was to assess the advantages or disadvantages of hands-free charting through a voice-to-text app designed for perfusionists. Twelve clinical perfusion students using two different simulated bypass cases were recorded and assessed for the number of events noticed and charted, as well as the speed at which they accomplished these steps. Paper charts were compared with a custom app with voice-to-text charting capability. Data was analyzed using linear mixed models to detect differences in length of time until a chartable event was noticed, and how long after noticing an event it took to record the event. Timeliness of recording an event was made by assessing log-transformed time data. There was significantly more information recorded when charting on paper, while charting with voice-to-text resulted in significantly faster mean time from noticing an event to the recording of it. There was no significant difference between how many events were noticed and recorded. When using paper charting, a higher percentage of events that were missed were drug administration events, while voice charting had a higher percentage of missed events that were associated with cardioplegia delivery or bypass timing. With a decreased time interval between noticing an event and charting the event, speech-to-text for perfusion could be of benefit in situations where many events occur at once, such as emergency situations or highly active portions of bypass such as initiation and termination. While efforts were made to make the app as intuitive as possible, there is room for improvement., (© Copyright 2021 AMSECT.)

Published

2021