235 results on '"Gregson, B A"'
Search Results
2. Prevalence, Trajectory, and Predictors of Poststroke Pain: Retrospective Analysis of Pooled Clinical Trial Data Set
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Ali, Myzoon, Tibble, Holly, Brady, Marian C., Quinn, Terence J., Sunnerhagen, Katharina S., Venketasubramanian, Narayanaswamy, Shuaib, Ashfaq, Pandyan, Anand, Mead, Gillian, Lees, K.R., Alexandrov, A., Bath, P.M., Bluhmki, E., Bornstein, N., Chen, C., Claesson, L., Curram, J., Davis, S.M., Diener, H-C., Donnan, G., Fisher, M., Ginsberg, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M.G., Hommel, M., Kaste (Emeritus), M., Lyden, P., Marler, J., Muir, K., Roffe, C., Teal, P., Wahlgren, N.G., Warach, S., Ali, M., Ashburn, A., Barer, D., Barzel, A., Bernhardt, J., Bowen, A., Drummond, A., Edmans, J., English, C., Gladman (Emeritus), J., Godecke, E., Hiekkala, S., Hoffman, T., Kalra, L., Kuys, S., Langhorne, P., Laska, A.C., Lees, K.R., Logan, P., Machner, B., Morris, J., Pollock, A., Pomeroy, V., Rodgers, H., Sackley, C., Shaw, L., Stott, D.J., Tyson, S., van Vliet, P., Walker, M., Whiteley, W., Hanley, D.F., Butcher, K., Davis, S., Gregson, B., Lees, K.R., Lyden, P., Mayer, S., Muir, K., and Steiner, T.
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- 2023
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3. Forewarning of hypotensive events using a Bayesian artificial neural network in neurocritical care
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Donald, Rob, Howells, Tim, Piper, Ian, Enblad, P., Nilsson, P., Chambers, I., Gregson, B., Citerio, G., Kiening, K., Neumann, J., Ragauskas, A., Sahuquillo, J., Sinnott, R., Stell, A., and the BrainIT Group
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- 2019
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4. Decompressive craniectomy as a second/third-tier intervention in traumatic brain injury: A multicenter observational study
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Decraene, B, Klein, S, Piper, I, Gregson, B, Enblad, P, Ragauskas, A, Citerio, G, Chambers, I, Neumann, J, Sahuquillo, J, Kiening, K, Moss, L, Nilsson, P, Donald, R, Howells, T, Lo, M, Depreitere, B, Decraene, Brecht, Klein, Samuel P, Piper, Ian, Gregson, Barbara, Enblad, Per, Ragauskas, Arminas, Citerio, Giuseppe, Chambers, Iain, Neumann, Jan-Oliver, Sahuquillo, Juan, Kiening, Karl, Moss, Laura, Nilsson, Pelle, Donald, Rob, Howells, Tim, Lo, Milly, Depreitere, Bart, Decraene, B, Klein, S, Piper, I, Gregson, B, Enblad, P, Ragauskas, A, Citerio, G, Chambers, I, Neumann, J, Sahuquillo, J, Kiening, K, Moss, L, Nilsson, P, Donald, R, Howells, T, Lo, M, Depreitere, B, Decraene, Brecht, Klein, Samuel P, Piper, Ian, Gregson, Barbara, Enblad, Per, Ragauskas, Arminas, Citerio, Giuseppe, Chambers, Iain, Neumann, Jan-Oliver, Sahuquillo, Juan, Kiening, Karl, Moss, Laura, Nilsson, Pelle, Donald, Rob, Howells, Tim, Lo, Milly, and Depreitere, Bart
- Abstract
Objectives: RESCUEicp studied decompressive craniectomy (DC) applied as third-tier option in severe traumatic brain injury (TBI) patients in a randomized controlled setting and demonstrated a decrease in mortality with similar rates of favorable outcome in the DC group compared to the medical management group. In many centers, DC is being used in combination with other second/third-tier therapies. The aim of the present study is to investigate outcomes from DC in a prospective non-RCT context. Methods: This is a prospective observational study of 2 patient cohorts: one from the University Hospitals Leuven (2008–2016) and one from the Brain-IT study, a European multicenter database (2003–2005). In thirty-seven patients with refractory elevated intracranial pressure who underwent DC as a second/third-tier intervention, patient, injury and management variables including physiological monitoring data and administration of thiopental were analysed, as well as Extended Glasgow Outcome score (GOSE) at 6 months. Results: In the current cohorts, patients were older than in the surgical RESCUEicp cohort (mean 39.6 vs. 32.3; p < 0.001), had higher Glasgow Motor Score on admission (GMS < 3 in 24.3% vs. 53.0%; p = 0.003) and 37.8% received thiopental (vs. 9.4%; p < 0.001). Other variables were not significantly different. GOSE distribution was: death 24.3%; vegetative 2.7%; lower severe disability 10.8%; upper severe disability 13.5%; lower moderate disability 5.4%; upper moderate disability 2.7%, lower good recovery 35.1%; and upper good recovery 5.4%. The outcome was unfavorable in 51.4% and favorable in 48.6%, as opposed to 72.6% and 27.4% respectively in RESCUEicp (p = 0.02). Conclusion: Outcomes in DC patients from two prospective cohorts reflecting everyday practice were better than in RESCUEicp surgical patients. Mortality was similar, but fewer patients remained vegetative or severely disabled and more patients had a good recovery. Although patients were older a
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- 2023
5. Antiplatelet Therapy After Spontaneous Intracerebral Hemorrhage and Functional Outcomes
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Murthy, Santosh B., Biffi, Alessandro, Falcone, Guido J., Sansing, Lauren H., Torres Lopez, Victor, Navi, Babak B., Roh, David J., Mandava, Pitchaiah, Hanley, Daniel F., Ziai, Wendy C., Kamel, Hooman, Rosand, Jonathan, Sheth, Kevin N., Butcher, K., Davis, S., Gregson, B., Lees, K.R., Lyden, P., Mayer, S., Muir, K., and Steiner, T.
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- 2019
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6. Trigger Characteristics of EUSIG-Defined Hypotensive Events
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Donald, Rob, Howells, Tim, Piper, Ian, Chambers, I., Citerio, G., Enblad, P., Gregson, B., Kiening, K., Mattern, J., Nilsson, P., Ragauskas, A., Sahuquillo, Juan, Sinnott, R., Stell, A., Schuhmann, Martin U., editor, and Czosnyka, Marek, editor
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- 2012
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7. Early Warning of EUSIG-Defined Hypotensive Events Using a Bayesian Artificial Neural Network
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Donald, Rob, Howells, Tim, Piper, Ian, Chambers, I., Citerio, G., Enblad, P., Gregson, B., Kiening, K., Mattern, J., Nilsson, P., Ragauskas, A., Sahuquillo, Juan, Sinnott, R., Stell, A., Schuhmann, Martin U., editor, and Czosnyka, Marek, editor
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- 2012
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8. Intraventricular hemorrhage and hydrocephalus after spontaneous intracerebral hemorrhage: results from the STICH trial
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Bhattathiri, P. S., Gregson, B., Prasad, K. S. M., Mendelow, A. D., Steiger, H. -J., editor, Hoff, Julian T., editor, Keep, Richard F., editor, Xi, Guohua, editor, and Hua, Ya, editor
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- 2006
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9. The significance of crossovers after randomization in the STICH trial
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Prasad, K. S. M., Gregson, B. A., Bhattathiri, P. S., Mitchell, P., Mendelow, A. D., Steiger, H. -J., editor, Hoff, Julian T., editor, Keep, Richard F., editor, Xi, Guohua, editor, and Hua, Ya, editor
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- 2006
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10. Sex and Stroke in Thrombolyzed Patients and Controls
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Hametner, Christian, MacIsaac, Rachael L., Kellert, Lars, Abdul-Rahim, Azmil H., Ringleb, Peter A., Lees, Kennedy R., Alexandrov, A., Bath, P.M., Bluhmki, E., Bornstein, N., Chen, C., Claesson, L., Davis, S.M., Donnan, G., Diener, H.C., Fisher, M., Ginsberg, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M.G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Venketasubramanian, N., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N.G., Warach, S., and Weimar, C.
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- 2017
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11. Continuous Monitoring of ICP and CPP Following ICH and its Relationship to Clinical, Radiological and Surgical Parameters
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Fernandes, H. M., Siddique, S., Banister, K., Chambers, I., Wooldridge, T., Gregson, B., Mendelow, A. D., Reulen, H.-J., editor, Steiger, H.-J., editor, Mendelow, A. David, editor, Baethmann, Alexander, editor, Czernicki, Zbigniew, editor, Hoff, Julian T., editor, Ito, Umeo, editor, James, Hector E., editor, Kuroiwa, Toshihika, editor, Marmarou, Anthony, editor, Marshall, Lawrence F., editor, and Reulen, Hans-Jürgen, editor
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- 2000
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12. The Selectin Superfamily: The Role of Selectin Adhesion Molecules in Delayed Cerebral Ischaemia After Aneurysmal Subarachnoid Haemorrhage
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Nissen, J. J., Mantle, D., Blackburn, A., Barnes, J., Wooldridge, T., Gregson, B., Mendelow, A. D., Reulen, H.-J., editor, Steiger, H.-J., editor, Mendelow, A. David, editor, Baethmann, Alexander, editor, Czernicki, Zbigniew, editor, Hoff, Julian T., editor, Ito, Umeo, editor, James, Hector E., editor, Kuroiwa, Toshihika, editor, Marmarou, Anthony, editor, Marshall, Lawrence F., editor, and Reulen, Hans-Jürgen, editor
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- 2000
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13. Temporal Profile of Pneumonia After Stroke
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de Jonge, Jeroen C., primary, van de Beek, Diederik, additional, Lyden, Patrick, additional, Brady, Marian C., additional, Bath, Philip M., additional, van der Worp, H. Bart, additional, Lees, K.R., additional, Alexandrov, A., additional, Berge, E., additional, Bluhmki, E., additional, Bornstein, N., additional, Chen, C., additional, Claesson, L., additional, Davis, S.M., additional, Donnan, G., additional, Diener, H.C., additional, Fisher, M., additional, Ginsberg, M., additional, Gregson, B., additional, Grotta, J., additional, Hacke, W., additional, Hennerici, M.G., additional, Hommel, M., additional, Kaste, M., additional, Marler, J., additional, Muir, K., additional, Venketasubramanian, N., additional, Sacco, R., additional, Shuaib, A., additional, Teal, P., additional, Wahlgren, N.G., additional, Warach, S., additional, and Weimar, C., additional
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- 2022
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14. Regional differences in outcome from subarachnoid haemorrhage: comparative audit
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Mitchell, P, Hope, T, Gregson, B A, and Mendelow, A David
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- 2004
15. How Well Do Standard Stroke Outcome Measures Reflect Quality of Life?: A Retrospective Analysis of Clinical Trial Data
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Ali, Myzoon, Fulton, Rachael, Quinn, Terry, Brady, Marian, Lees, K. R., Alexandrov, A., Bath, P. M., Bluhmki, E., Bornstein, N., Claesson, L., Davis, S. M., Donnan, G., Diener, H. C., Fisher, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M. G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N. G., Warach, S., Weimar, C., Brady, M., Ali, M., Ashburn, A., Barer, D., Bernhardt, J., Bowen, A., Brodie, E., Corr, S., Drummond, A., Edmans, J., English, C., Gladman, J., Godecke, E., Hoffmann, T., Kalra, L., Kuys, S., Langhorne, P., Laska, A. C., Lees, K. R., Lincoln, N., Logan, P., Jongbloed, L., Mead, G., Pollock, A., Pomeroy, V., Rodgers, H., Sackley, C., Shaw, L., Stott, D. J., Sunnerhagen, K. S., Tyson, S., van Vliet, P., Walker, M., Whiteley, W., Warach, S., Albers, G., Davis, S., Donnan, G., Fisher, M., Furlan, T., Grotta, J., Hacke, W., Kidwell, C., Koroshetz, W., Lees, K. R., Lev, M., Liebeskind, D., Sorensen, G., Thijs, V., Thomalla, G., Wardlaw, J., Wintermark, M., Hanley, D. F., Gregson, B., Davis, S., Lees, K. R., Lyden, P., Muir, K., Steiner, T., Mayer, S., Wahlgren, N. G., Molina, C., Numminen, H., Lees, K. R., Tsivgoulis, G., Weimar, C., Diener, H. -C., Hankey, G., Lees, K. R., Ovbiagele, B., and Weir, C.
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- 2013
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16. CRASH Trial Is Based on Problematic Meta-Analysis
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Gregson, B., Todd, N. V., Crawford, D., Gerber, C. J., Fulton, B., Tacconi, L., Crawford, P. J., and Sengupta, R. P.
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- 1999
17. β-Blockers, Pneumonia, and Outcome After Ischemic Stroke: Evidence From Virtual International Stroke Trials Archive
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Sykora, Marek, Siarnik, Pavel, Diedler, Jennifer, Lees, K.R., Alexandrov, A., Bath, P.M., Bluhmki, E., Bornstein, N., Claesson, L., Davis, S.M., Donnan, G., Diener, H. C., Fisher, M., Ginsberg, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M.G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N.G., Warach, S., and Weimar, C.
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- 2015
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18. National Institutes of Health Stroke Scale Item Profiles as Predictor of Patient Outcome: External Validation on Independent Trial Data
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Abdul-Rahim, Azmil H., Fulton, Rachael L., Sucharew, Heidi, Kleindorfer, Dawn, Khatri, Pooja, Broderick, Joseph P., Lees, Kennedy R., Alexandrov, A., Bath, P.M., Bluhmki, E., Bornstein, N., Claesson, L., Curram, J., Davis, S.M., Donnan, G., Diener, H.C., Fisher, M., Ginsberg, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M.G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N.G., Warach, S., and Weimar, C.
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- 2015
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19. Associations of chronic heart failure with outcome in acute ischaemic stroke patients who received systemic thrombolysis: analysis from VISTA
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Abdul-Rahim, A. H., Fulton, R. L., Frank, B., McMurray, J. J. V., Lees, K. R., Alexandrov, A. V., Bath, P. W., Bluhmki, E., Claesson, L., Curram, J., Davis, S. M., Donnan, G., Diener, H. C., Fisher, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M. G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N. G., Warach, S., and Weimar, C.
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- 2015
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20. Characteristic Adverse Events and Their Incidence Among Patients Participating in Acute Ischemic Stroke Trials
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Hesse, Kerrick, Fulton, Rachael L., Abdul-Rahim, Azmil H., Lees, Kennedy R., Alexandrov, A.V., Bath, P.W., Bluhmki, E., Claesson, L., Curram, J., Davis, S.M., Donnan, G., Diener, H.C., Fisher, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M.G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N.G., Warach, S., and Weimar, C.
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- 2014
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21. THRIVE Score Predicts Ischemic Stroke Outcomes and Thrombolytic Hemorrhage Risk in VISTA
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Flint, Alexander C., Faigeles, Bonnie S., Cullen, Sean P., Kamel, Hooman, Rao, Vivek A., Gupta, Rishi, Smith, Wade S., Bath, Philip M., Donnan, Geoffrey A., Lees, K.R., Alexandrov, A., Bath, P.M., Bluhmki, E., Bornstein, N., Claesson, L., Davis, S.M., Donnan, G., Diener, H.C., Fisher, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M.G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N.G., Warach, S., and Weimar, C.
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- 2013
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22. Does the cognitive measure Cog-4 show improvement among patients treated with thrombolysis after acute stroke?
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Hajjar, Karim, Fulton, Rachael L., Diener, Hans-Christoph, Lees, Kennedy R., Alexandrov, A, Bath, PMW, Bluhmki, E, Claesson, L, Curram, J, Davis, SM, Donnan, G, Diener, HC, Fisher, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, MG, Hommel, M, Kaste, M, Lees, KR, Lyden, P, Marler, J, Muir, K, Sacco, R, Shuaib, A, Teal, P, Wahlgren, NG, Warach, S, and Weimar, C
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- 2013
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23. The use of hyperventilation therapy after traumatic brain injury in Europe: an analysis of the BrainIT database
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Neumann, J.-O., Chambers, I. R., Citerio, G., Enblad, P., Gregson, B. A., Howells, T., Mattern, J., Nilsson, P., Piper, I., Ragauskas, A., Sahuquillo, J., Yau, Y. H., and Kiening, K.
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Artificial respiration -- Usage ,Artificial respiration -- Standards ,Artificial respiration -- Research ,Practice guidelines (Medicine) -- Research ,Practice guidelines (Medicine) -- Usage ,Brain -- Injuries ,Brain -- Care and treatment ,Health care industry - Abstract
Byline: J.-O. Neumann (1), I. R. Chambers (2), G. Citerio (3), P. Enblad (4), B. A. Gregson (5), T. Howells (4), J. Mattern (1), P. Nilsson (4), I. Piper (6), A. Ragauskas (7), J. Sahuquillo (8), Y. H. Yau (9), K. Kiening (1) Keywords: Traumatic brain injury; Hyperventilation Abstract: Objective To assess the use of hyperventilation and the adherence to Brain Trauma Foundation-Guidelines (BTF-G) after traumatic brain injury (TBI). Setting Twenty-two European centers are participating in the BrainIT initiative. Design Retrospective analysis of monitoring data. Patients and participants One hundred and fifty-one patients with a known time of trauma and at least one recorded arterial blood--gas (ABG) analysis. Measurements and results A total number of 7,703 ABGs, representing 2,269 ventilation episodes (VE) were included in the analysis. Related minute-by-minute ICP data were taken from a 30 min time window around each ABG collection. Data are given as mean with standard deviation. (1) Patients without elevated intracranial pressure (ICP) ( Conclusion While overall adherence to current BTF-G seems to be the rule, its recommendations on early prophylactic hyperventilation as well as the use of additional cerebral oxygenation monitoring during forced hyperventilation are not followed in this sample of European TBI centers. Descriptor Neurotrauma Author Affiliation: (1) Department of Neurosurgery, Universitatsklinikum Heidelberg, Im Neuenheimer Feld 400, 69120, Heidelberg, Germany (2) Regional Medical Physics Department, James Cook University Hospital, Middlesborough, UK (3) Department of Perioperative Medicine and Intensive Care, NeuroICU, Hospital San Gerardo, Monza, Italy (4) Department of Clinical Neurosciences, Section of Neurosurgery, Uppsala University Hospital, Uppsala, Sweden (5) Department of Neurosurgery, Newcastle General Hospital, Newcastle upon Tyne, UK (6) Department of Clinical Physics, Institute of Neurological Sciences, Southern General Hospital, Glasgow, Scotland (7) Telematics Science Laboratory, Kaunas University of Technology, Kaunas, Lithuania (8) Department of Neurosurgery, Neurotraumatology Research Unit, Vall d'Hebron University Hospital, Barcelona, Spain (9) Department of Neurosurgery, Western General Hospital, Edinburgh, Scotland Article History: Registration Date: 11/04/2008 Received Date: 29/07/2007 Accepted Date: 01/04/2008 Online Date: 01/05/2008
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- 2008
24. Effect of awake Carotid Endarterectomy under local anaesthesia on peri-operative blood pressure: blood pressure is normalised when carotid stenosis is treated under local anaesthesia
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Bhattathiri, P. S., Ramakrishnan, Y., Vivar, R. A., Bell, K., Bullock, R. E., Mitchell, P., Gregson, B., and Mendelow, A. D.
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- 2005
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25. Logistic discriminant analysis : Applications in health care research
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Gregson, B. A.
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362.1 ,Health care logistics - Published
- 1987
26. META-ANALYSIS OF RANDOMISED CONTROLLED TRIALS (RCTS) OF SURGERY VERSUS CONSERVATIVE TREATMENT IN SPONTANEOUS SUPRATENTORIAL INTRACEREBRAL HAEMORRHAGE: 7
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Gregson, B. A. and Mendelow, A. D.
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- 2008
27. Early in-hospital exposure to statins and outcome after intracerebral haemorrhage - Results from the Virtual International Stroke Trials Archive
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Doerrfuss, J.I., Abdul-Rahim, A.H., Siegerink, B., Nolte, C.H., Lees, K.R., Endres, M., Kasner, S.E., Scheitz, J.F., Hanley, D.F., Butcher, K.S., Davis, S., Gregson, B., Lyden, P., Mayer, S., Muir, K., Sandset, E.C., Steiner, T., and VISTA Collaboration
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Intracerebral haemorrhage ,statin ,outcome ,mortality ,discontinuation - Abstract
Introduction Recent data suggest that statin use after intracerebral haemorrhage might be beneficial. However, data on the effects of early in-hospital statin exposure are lacking. Therefore, we sought to assess whether (1) early statin exposure during the acute phase after intracerebral haemorrhage and (2) early continuation of prevalent statin use are associated with favourable functional outcome. Patients and methods Data were obtained from the Virtual International Stroke Trials Archive. Patients were categorised according to use patterns of statins during this early in-hospital phase (continuation, discontinuation or new initiation of statins). Univariate and multivariable analyses were conducted to explore the association between early statin exposure and functional outcome. Results A total of 919 patients were included in the analysis. Early in-hospital statin exposure (n = 89, 9.7%) was associated with better functional outcome (modified Rankin Scale
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- 2019
28. Antibiotic Class and Outcome in Post-stroke Infections: An individual participant data pooled analysis of VISTA-acute
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Smith, Craig J., Heal, Calvin, Vail, Andy, Jeans, Adam R., Westendorp, Willeke F., Nederkoorn, Paul J., van de Beek, Diederik, Kalra, Lalit, Montaner, Joan, Woodhead, Mark, Meisel, Andreas, Lees, K. R., Alexandrov, A., Bath, P. M., Berge, E., Bluhmki, E., Bornstein, N., Chen, C., Claesson, L., Davis, S. M., Donnan, G., Diener, H. C., Fisher, M., Ginsberg, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M. G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Venketasubramanian, N., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N. G., Warach, S., Weimar, C., Graduate School, ACS - Atherosclerosis & ischemic syndromes, AII - Infectious diseases, ANS - Neurovascular Disorders, and Neurology
- Abstract
Introduction: Antibiotics used to treat post-stroke infections have differing antimicrobial and anti-inflammatory effects. Our aim was to investigate whether antibiotic class was associated with outcome after post-stroke infection. Methods: We analyzed pooled individual participant data from the Virtual International Stroke Trials Archive (VISTA)-Acute. Patients with ischemic stroke and with an infection treated with systemic antibiotic therapy during the first 2 weeks after stroke onset were eligible. Antibiotics were grouped into eight classes, according to antimicrobial mechanism and prevalence. The primary analysis investigated whether antibiotic class for any infection, or for pneumonia, was independently associated with a shift in 90 day modified Rankin Scale (mRS) using ordinal logistic regression. Results: 2,708 patients were eligible (median age [IQR] = 74 [65 to 80] y; 51% female; median [IQR] NIHSS score = 15 [11 to 19]). Pneumonia occurred in 35%. Treatment with macrolides (5% of any infections; 9% of pneumonias) was independently associated with more favorable mRS distribution for any infection [OR (95% CI) = 0.59 (0.42 to 0.83), p = 0.004] and for pneumonia [OR (95% CI) = 0.46 (0.29 to 0.73), p = 0.001]. Unfavorable mRS distribution was independently associated with treatment of any infection either with carbapenems, cephalosporins or monobactams [OR (95% CI) = 1.62 (1.33 to 1.97), p < 0.001], penicillin plus β-lactamase inhibitors [OR (95% CI) = 1.26 (1.03 to 1.54), p = 0.025] or with aminoglycosides [OR (95% CI) = 1.73 (1.22 to 2.46), p = 0.002]. Conclusion: This retrospective study has several limitations including effect modification and confounding by indication. Macrolides may have favorable immune-modulatory effects in stroke-associated infections. Prospective evaluation of the impact of antibiotic class on treatment of post-stroke infections is warranted.
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- 2019
29. Variability in pupil size estimation
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Clark, A, Clarke, T N S, Gregson, B, Hooker, P N A, and Chambers, I R
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- 2006
30. Outcome assignment in the International Surgical Trial of Intracerebral Haemorrhage
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Mendelow, A. D., Teasdale, G. M., Barer, D., Fernandes, H. M., Murray, G. D., and Gregson, B. A.
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- 2003
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31. Decompressive craniectomy as a second/third tier intervention in traumatic brain injury: a multicenter observational study
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Decraene, B, P Klein, S, Piper, I, Gregson, B, Enblad, P, Ragauskas, A, Citerio, G, Chambers, I, O Neumann, J, Sahuquillo, J, Kiening, K, Moss, L, Nilsson, P, Donald, R, Howells, T, Lo, M, Depreitere, B, B Decraene, S P Klein, I Piper, B Gregson, P Enblad, A Ragauskas, G Citerio, I Chambers, J O Neumann, J Sahuquillo, K Kiening, L Moss, P Nilsson, R Donald, T Howells, M Lo, B Depreitere, Decraene, B, P Klein, S, Piper, I, Gregson, B, Enblad, P, Ragauskas, A, Citerio, G, Chambers, I, O Neumann, J, Sahuquillo, J, Kiening, K, Moss, L, Nilsson, P, Donald, R, Howells, T, Lo, M, Depreitere, B, B Decraene, S P Klein, I Piper, B Gregson, P Enblad, A Ragauskas, G Citerio, I Chambers, J O Neumann, J Sahuquillo, K Kiening, L Moss, P Nilsson, R Donald, T Howells, M Lo, and B Depreitere
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- 2019
32. Stroke aetiological classification reliability and effect on trial sample size: systematic review, meta-analysis and statistical modelling
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Abdul-Rahim, AH, Dickie, DA, Selvarajah, JR, Lees, KR, Quinn, TJ, Alexandrov, A, Bath, PM, Berge, E, Bluhmki, E, Bornstein, N, Chen, C, Claesson, L, Davis, SM, Donnan, G, Diener, HC, Fisher, M, Ginsberg, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, MG, Hommel, M, Kaste, M, Lyden, P, Marler, J, Muir, K, Venketasubramanian, N, Sacco, R, Shuaib, A, Teal, P, Wahlgren, NG, Warach, S, Weimar, C, Abdul-Rahim, AH, Dickie, DA, Selvarajah, JR, Lees, KR, Quinn, TJ, Alexandrov, A, Bath, PM, Berge, E, Bluhmki, E, Bornstein, N, Chen, C, Claesson, L, Davis, SM, Donnan, G, Diener, HC, Fisher, M, Ginsberg, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, MG, Hommel, M, Kaste, M, Lyden, P, Marler, J, Muir, K, Venketasubramanian, N, Sacco, R, Shuaib, A, Teal, P, Wahlgren, NG, Warach, S, and Weimar, C
- Abstract
BACKGROUND: Inter-observer variability in stroke aetiological classification may have an effect on trial power and estimation of treatment effect. We modelled the effect of misclassification on required sample size in a hypothetical cardioembolic (CE) stroke trial. METHODS: We performed a systematic review to quantify the reliability (inter-observer variability) of various stroke aetiological classification systems. We then modelled the effect of this misclassification in a hypothetical trial of anticoagulant in CE stroke contaminated by patients with non-cardioembolic (non-CE) stroke aetiology. Rates of misclassification were based on the summary reliability estimates from our systematic review. We randomly sampled data from previous acute trials in CE and non-CE participants, using the Virtual International Stroke Trials Archive. We used bootstrapping to model the effect of varying misclassification rates on sample size required to detect a between-group treatment effect across 5000 permutations. We described outcomes in terms of survival and stroke recurrence censored at 90 days. RESULTS: From 4655 titles, we found 14 articles describing three stroke classification systems. The inter-observer reliability of the classification systems varied from 'fair' to 'very good' and suggested misclassification rates of 5% and 20% for our modelling. The hypothetical trial, with 80% power and alpha 0.05, was able to show a difference in survival between anticoagulant and antiplatelet in CE with a sample size of 198 in both trial arms. Contamination of both arms with 5% misclassified participants inflated the required sample size to 237 and with 20% misclassification inflated the required sample size to 352, for equivalent trial power. For an outcome of stroke recurrence using the same data, base-case estimated sample size for 80% power and alpha 0.05 was n = 502 in each arm, increasing to 605 at 5% contamination and 973 at 20% contamination. CONCLUSIONS: Stroke aetiological cl
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- 2019
33. Randomised evaluation of early vs late cranioplasty investigating cognitive and functional recovery: protocol for a single centre, pilot, randomised trial
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Mee, H, Kolias, A, Anwar, F, Timofeev, I, Helmy, A, Turner, C, Caldwell, K, Tarantino, S, Browne, G, Woodbury, E, Gregson, B, Warburton, E, Hutchinson, P, Mee, H, Kolias, A, Anwar, F, Timofeev, I, Helmy, A, Turner, C, Caldwell, K, Tarantino, S, Browne, G, Woodbury, E, Gregson, B, Warburton, E, and Hutchinson, P
- Published
- 2019
34. Forewarning of hypotensive events using a Bayesian artificial neural network in neurocritical care
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Donald, R, Howells, T, Piper, I, Enblad, P, Nilsson, P, Chambers, I, Gregson, B, Citerio, G, Kiening, K, Neumann, J, Ragauskas, A, Sahuquillo, J, Sinnott, R, Stell, A, Donald, R, Howells, T, Piper, I, Enblad, P, Nilsson, P, Chambers, I, Gregson, B, Citerio, G, Kiening, K, Neumann, J, Ragauskas, A, Sahuquillo, J, Sinnott, R, and Stell, A
- Abstract
Traumatically brain injured (TBI) patients are at risk from secondary insults. Arterial hypotension, critically low blood pressure, is one of the most dangerous secondary insults and is related to poor outcome in patients. The overall aim of this study was to get proof of the concept that advanced statistical techniques (machine learning) are methods that are able to provide early warning of impending hypotensive events before they occur during neuro-critical care. A Bayesian artificial neural network (BANN) model predicting episodes of hypotension was developed using data from 104 patients selected from the BrainIT multi-center database. Arterial hypotension events were recorded and defined using the Edinburgh University Secondary Insult Grades (EUSIG) physiological adverse event scoring system. The BANN was trained on a random selection of 50% of the available patients (n = 52) and validated on the remaining cohort. A multi-center prospective pilot study (Phase 1, n = 30) was then conducted with the system running live in the clinical environment, followed by a second validation pilot study (Phase 2, n = 49). From these prospectively collected data, a final evaluation study was done on 69 of these patients with 10 patients excluded from the Phase 2 study because of insufficient or invalid data. Each data collection phase was a prospective non-interventional observational study conducted in a live clinical setting to test the data collection systems and the model performance. No prediction information was available to the clinical teams during a patient’s stay in the ICU. The final cohort (n = 69), using a decision threshold of 0.4, and including false positive checks, gave a sensitivity of 39.3% (95% CI 32.9–46.1) and a specificity of 91.5% (95% CI 89.0–93.7). Using a decision threshold of 0.3, and false positive correction, gave a sensitivity of 46.6% (95% CI 40.1–53.2) and specificity of 85.6% (95% CI 82.3–88.8). With a decision threshold of 0.3, > 15 min warnin
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- 2019
35. Serum concentration of adhesion molecules in patients with delayed ischaemic neurological deficit after aneurysmal subarachnoid haemorrhage: the immunoglobulin and selectin superfamilies
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Nissen, J J, Mantle, D, Gregson, B, and Mendelow, A D
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- 2001
36. Statistics and analysis of the Camino ICP monitor
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GREGSON, B A, BANISTER, K, and CHAMBERS, I R
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- 2001
37. Surgery in Intracerebral Hemorrhage: The Uncertainty Continues
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Fernandes, H. M., Gregson, B., Siddique, S., and Mendelow, A. D.
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- 2000
38. Liver Fibrosis and Perihematomal Edema Growth in Primary Intracerebral Hemorrhage.
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Parikh, Neal S., Jesudian, Arun, Kamel, Hooman, Hanley, Daniel F., Ziai, Wendy C., Murthy, Santosh B., the VISTA-ICH Collaboration, Hanley, D. F., Butcher, K., Davis, S., Gregson, B., Lees, K. R., Lyden, P., Mayer, S., Muir, K., Steiner, T., and VISTA-ICH Collaboration
- Subjects
CEREBRAL hemorrhage ,LIVER ,FIBROSIS ,EDEMA ,ADULTS ,SECONDARY analysis ,RESEARCH ,RESEARCH methodology ,RETROSPECTIVE studies ,CIRRHOSIS of the liver ,MEDICAL cooperation ,EVALUATION research ,COMPARATIVE studies ,RESEARCH funding ,CEREBRAL edema ,DISEASE complications - Abstract
Background: Liver disease is associated with altered serum osmolality, increased thrombin generation, and systemic inflammation, all of which may contribute to perihematomal edema (PHE) after intracerebral hemorrhage (ICH). We evaluated the association between a validated liver fibrosis index and PHE growth in a cohort of patients with primary ICH.Methods: We performed a retrospective cohort study using data from the Virtual International Stroke Trials Archive-ICH. We included adult patients with primary ICH presenting within 6 h of symptom onset. The exposure of interest was the Fibrosis-4 (FIB-4) score, a validated liver fibrosis index; this was modeled as a continuous variable. The primary outcome was absolute PHE growth over 96 h. Secondary outcomes were absolute admission and 96-h PHE volumes. We used multiple linear regression models adjusted for established determinants of PHE. In a secondary analysis, the FIB-4 score was modeled as a categorical variable to compare patients with versus without liver fibrosis.Results: Among 354 patients with ICH, 8% had evidence of liver fibrosis based on a validated cutoff. The FIB-4 score was not associated with PHE growth in unadjusted (β, 0.03; 95% CI, - 0.01 to 0.12) or adjusted models (β, 0.04; 95% CI, - 0.03 to 0.13). In a secondary analysis treating FIB-4 as a categorical variable, patients with liver fibrosis did not have greater PHE growth than those without liver fibrosis. FIB-4 score was also not associated with absolute admission or 96-h PHE volumes.Conclusions: In a multicenter cohort of patients with primary intracerebral hemorrhage, a liver fibrosis score was not associated with PHE volume or growth. [ABSTRACT FROM AUTHOR]- Published
- 2021
- Full Text
- View/download PDF
39. Absolute risk and predictors of the growth of acute spontaneous intracerebral haemorrhage: a systematic review and meta-analysis of individual patient data
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Al-Shahi Salman R., Frantzias J., Lee R.J., Battey T.W.K., Ayres A.M., Goldstein J.N., Mayer S.A., Steiner T., Wang X., Arima H., Hasegawa H., Oishi M., Godoy D.A., Masotti L., Dowlatshahi D., Rodriguez-Luna D., Molina C.A., Jang D.-K., Davalos A., Castillo J., Yao X., Claassen J., Volbers B., Kazui S., Okada Y., Fujimoto S., Toyoda K., Li Q., Khoury J., Delgado P., SabÃn J.Ã., Hernández-Guillamon M., Prats-Sánchez L., Cai C., Kate M.P., McCourt R., Venkatasubramanian C., Diringer M.N., Ikeda Y., Worthmann H., Ziai W.C., d'Esterre C.D., Aviv R.I., Raab P., Murai Y., Zazulia A.R., Butcher K.S., Seyedsaadat S.M., Grotta J.C., MartÃ-Fà bregas J., Montaner J., Broderick J., Yamamoto H., Staykov D., Connolly E.S., Selim M., Leira R., Moon B.H., Demchuk A.M., Di Napoli M., Fujii Y., Anderson C.S., Rosand J., Hanley D.F., Davis S., Gregson B., Lees K.R., Lyden P.D., Muir K.W., Xie P., Bakhshayesh B., McDonald M., Brott T., Pennati P., Parry-Jones A.R., Smith C.J., Hopkins S.J., Slevin M., Campi V., Singh P., Papa F., Popa-Wagner A., Tudorica V., Takagi R., Teramoto A., Weissenborn K., and Lanfermann H.
- Subjects
diagnostic imaging ,clinical outcome ,Risk Assessment ,Article ,computer assisted tomography ,Outcome Assessment (Health Care) ,systematic review ,patient coding ,middle aged ,Humans ,human ,procedures ,outcome assessment ,computed tomographic angiography ,Aged ,Cerebral Hemorrhage ,neuroimaging ,anticoagulant therapy ,disease association ,prediction ,clinical practice ,priority journal ,risk factor ,disease exacerbation ,brain hemorrhage ,Disease Progression ,pathology ,meta analysis - Abstract
Background: Intracerebral haemorrhage growth is associated with poor clinical outcome and is a therapeutic target for improving outcome. We aimed to determine the absolute risk and predictors of intracerebral haemorrhage growth, develop and validate prediction models, and evaluate the added value of CT angiography. Methods: In a systematic review of OVID MEDLINE—with additional hand-searching of relevant studies' bibliographies— from Jan 1, 1970, to Dec 31, 2015, we identified observational cohorts and randomised trials with repeat scanning protocols that included at least ten patients with acute intracerebral haemorrhage. We sought individual patient-level data from corresponding authors for patients aged 18 years or older with data available from brain imaging initially done 0·5–24 h and repeated fewer than 6 days after symptom onset, who had baseline intracerebral haemorrhage volume of less than 150 mL, and did not undergo acute treatment that might reduce intracerebral haemorrhage volume. We estimated the absolute risk and predictors of the primary outcome of intracerebral haemorrhage growth (defined as >6 mL increase in intracerebral haemorrhage volume on repeat imaging) using multivariable logistic regression models in development and validation cohorts in four subgroups of patients, using a hierarchical approach: patients not taking anticoagulant therapy at intracerebral haemorrhage onset (who constituted the largest subgroup), patients taking anticoagulant therapy at intracerebral haemorrhage onset, patients from cohorts that included at least some patients taking anticoagulant therapy at intracerebral haemorrhage onset, and patients for whom both information about anticoagulant therapy at intracerebral haemorrhage onset and spot sign on acute CT angiography were known. Findings: Of 4191 studies identified, 77 were eligible for inclusion. Overall, 36 (47%) cohorts provided data on 5435 eligible patients. 5076 of these patients were not taking anticoagulant therapy at symptom onset (median age 67 years, IQR 56–76), of whom 1009 (20%) had intracerebral haemorrhage growth. Multivariable models of patients with data on antiplatelet therapy use, data on anticoagulant therapy use, and assessment of CT angiography spot sign at symptom onset showed that time from symptom onset to baseline imaging (odds ratio 0·50, 95% CI 0·36–0·70; p
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- 2018
40. Acute Risk Change: An Innovative Measure of Operative Adverse Events and Perioperative Team Performance.
- Author
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Coulson T.G., Pilcher D., Reid C.M., Bailey M., Webb S.T., Nashef S.A.M., Sandys S., Gregson B., Coulson T.G., Pilcher D., Reid C.M., Bailey M., Webb S.T., Nashef S.A.M., Sandys S., and Gregson B.
- Abstract
Objectives: Cardiac surgical risk models predict mortality preoperatively, whereas intensive care unit (ICU) models predict mortality postoperatively. Finding a large difference between the 2 (an acute risk change [ARC]) may reflect an alteration in the status of the patient related to the surgery. An adverse ARC was associated with morbidity and mortality in an Australian population. The aims of this study were to validate ARC in a UK population and to investigate the possible mechanisms behind ARC. Design(s): This was a retrospective case-control study. Setting(s): Single, high-volume cardiothoracic hospital. Participant(s): Data from 4,842 cardiac surgical patients were collected between 2013 and 2015. Intervention(s): None. Measurements and Main Results: EuroSCORE was recalibrated to each preceding year's data. ARC was defined as postoperative minus preoperative percentage mortality risk. Association among ARC, morbidity, and mortality was tested. Cases with large adverse ARC (greater than +15%) were compared with cases with large favorable ARC (less than -10%) with regard to intraoperative adverse events, unmeasured patient risk factors, and postoperative events. Adverse ARC was associated with hospital mortality, ICU stay, ICU readmission, renal support, prolonged intubation and return to the operating room (p < 0.001). Intraoperative adverse events occurred in 23 of 33 patients with adverse ARC; however, only 2 of 17 patients with favorable ARC reported adverse events (p < 0.001). Unmeasured risk factors were present in 48% of patients in the adverse ARC group. Conclusion(s): ARC is a readily available and sensitive marker that correlates strongly with morbidity and mortality. The use of ARC in local and national quality monitoring could identify areas for improvement of the quality of cardiac surgical care.Copyright © 2018 Elsevier Inc.
- Published
- 2018
41. Absolute risk and predictors of the growth of acute spontaneous intracerebral haemorrhage: a systematic review and meta-analysis of individual patient data.
- Author
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Salman, R, Frantzias, J, Lee, RJ, Lyden, PD, Battey, TWK, Ayres, AM, Goldstein, JN, Mayer, SA, Steiner, T, Wang, X, Arima, H, Hasegawa, H, Oishi, M, Godoy, DA, Masotti, L, Dowlatshahi, D, Rodriguez-Luna, D, Molina, CA, Jang, DK, Davalos, A, Castillo, J, Yao, X, Claassen, J, Volbers, B, Kazui, S, Okada, Y, Fujimoto, S, Toyoda, K, Li, Q, Khoury, J, Delgado, P, Sabín, JÁ, Hernández-Guillamon, M, Prats-Sánchez, L, Cai, C, Kate, MP, McCourt, R, Venkatasubramanian, C, Diringer, MN, Ikeda, Y, Worthmann, H, Ziai, WC, d'Esterre, CD, Aviv, RI, Raab, P, Murai, Y, Zazulia, AR, Butcher, KS, Seyedsaadat, SM, Grotta, JC, Martí-Fàbregas, J, Montaner, J, Broderick, J, Yamamoto, H, Staykov, D, Connolly, ES, Selim, M, Leira, R, Moon, BH, Demchuck, AM, Di Napoli, M, Fujii, Y, Anderson, CS, Rosand, J, Hanley, DF, Davis, S, Gregson, B, Lees, KR, Muir, KW, Xie, P, Bakhshayesh, B, McDonald, M, Brott, T, Pennati, P, Parry-Jones, AR, Smith, CJ, Hopkins, SJ, Slevin, Mark, Campi, V, Singh, P, Papa, F, Popa-Wagner, A, Tudorica, V, Takagi, R, Teramoto, A, Weissenborn, K, Lanfermann, H, Salman, R, Frantzias, J, Lee, RJ, Lyden, PD, Battey, TWK, Ayres, AM, Goldstein, JN, Mayer, SA, Steiner, T, Wang, X, Arima, H, Hasegawa, H, Oishi, M, Godoy, DA, Masotti, L, Dowlatshahi, D, Rodriguez-Luna, D, Molina, CA, Jang, DK, Davalos, A, Castillo, J, Yao, X, Claassen, J, Volbers, B, Kazui, S, Okada, Y, Fujimoto, S, Toyoda, K, Li, Q, Khoury, J, Delgado, P, Sabín, JÁ, Hernández-Guillamon, M, Prats-Sánchez, L, Cai, C, Kate, MP, McCourt, R, Venkatasubramanian, C, Diringer, MN, Ikeda, Y, Worthmann, H, Ziai, WC, d'Esterre, CD, Aviv, RI, Raab, P, Murai, Y, Zazulia, AR, Butcher, KS, Seyedsaadat, SM, Grotta, JC, Martí-Fàbregas, J, Montaner, J, Broderick, J, Yamamoto, H, Staykov, D, Connolly, ES, Selim, M, Leira, R, Moon, BH, Demchuck, AM, Di Napoli, M, Fujii, Y, Anderson, CS, Rosand, J, Hanley, DF, Davis, S, Gregson, B, Lees, KR, Muir, KW, Xie, P, Bakhshayesh, B, McDonald, M, Brott, T, Pennati, P, Parry-Jones, AR, Smith, CJ, Hopkins, SJ, Slevin, Mark, Campi, V, Singh, P, Papa, F, Popa-Wagner, A, Tudorica, V, Takagi, R, Teramoto, A, Weissenborn, K, and Lanfermann, H
- Abstract
Background Intracerebral haemorrhage growth is associated with poor clinical outcome and is a therapeutic target for improving outcome. We aimed to determine the absolute risk and predictors of intracerebral haemorrhage growth, develop and validate prediction models, and evaluate the added value of CT angiography. Methods In a systematic review of OVID MEDLINE—with additional hand-searching of relevant studies' bibliographies— from Jan 1, 1970, to Dec 31, 2015, we identified observational cohorts and randomised trials with repeat scanning protocols that included at least ten patients with acute intracerebral haemorrhage. We sought individual patient-level data from corresponding authors for patients aged 18 years or older with data available from brain imaging initially done 0·5–24 h and repeated fewer than 6 days after symptom onset, who had baseline intracerebral haemorrhage volume of less than 150 mL, and did not undergo acute treatment that might reduce intracerebral haemorrhage volume. We estimated the absolute risk and predictors of the primary outcome of intracerebral haemorrhage growth (defined as >6 mL increase in intracerebral haemorrhage volume on repeat imaging) using multivariable logistic regression models in development and validation cohorts in four subgroups of patients, using a hierarchical approach: patients not taking anticoagulant therapy at intracerebral haemorrhage onset (who constituted the largest subgroup), patients taking anticoagulant therapy at intracerebral haemorrhage onset, patients from cohorts that included at least some patients taking anticoagulant therapy at intracerebral haemorrhage onset, and patients for whom both information about anticoagulant therapy at intracerebral haemorrhage onset and spot sign on acute CT angiography were known. Findings Of 4191 studies identified, 77 were eligible for inclusion. Overall, 36 (47%) cohorts provided data on 5435 eligible patients. 5076 of these patients were not taking anticoagulant ther
- Published
- 2018
42. Acute Risk Change: An Innovative Measure of Operative Adverse Events and Perioperative Team Performance
- Author
-
Coulson, T., Gregson, B., Sandys, S., Nashef, S., Webb, S., Bailey, M., Reid, Christopher, Pilcher, D., Coulson, T., Gregson, B., Sandys, S., Nashef, S., Webb, S., Bailey, M., Reid, Christopher, and Pilcher, D.
- Abstract
Objectives: Cardiac surgical risk models predict mortality preoperatively, whereas intensive care unit (ICU) models predict mortality postoperatively. Finding a large difference between the 2 (an acute risk change [ARC]) may reflect an alteration in the status of the patient related to the surgery. An adverse ARC was associated with morbidity and mortality in an Australian population. The aims of this study were to validate ARC in a UK population and to investigate the possible mechanisms behind ARC. Design: This was a retrospective case-control study. Setting: Single, high-volume cardiothoracic hospital. Participants: Data from 4,842 cardiac surgical patients were collected between 2013 and 2015. Interventions: None. Measurements and main results: EuroSCORE was recalibrated to each preceding year's data. ARC was defined as postoperative minus preoperative percentage mortality risk. Association among ARC, morbidity, and mortality was tested. Cases with large adverse ARC (greater than +15%) were compared with cases with large favorable ARC (less than -10%) with regard to intraoperative adverse events, unmeasured patient risk factors, and postoperative events. Adverse ARC was associated with hospital mortality, ICU stay, ICU readmission, renal support, prolonged intubation and return to the operating room (p < 0.001). Intraoperative adverse events occurred in 23 of 33 patients with adverse ARC; however, only 2 of 17 patients with favorable ARC reported adverse events (p < 0.001). Unmeasured risk factors were present in 48% of patients in the adverse ARC group. Conclusion: ARC is a readily available and sensitive marker that correlates strongly with morbidity and mortality. The use of ARC in local and national quality monitoring could identify areas for improvement of the quality of cardiac surgical care.
- Published
- 2018
43. Interdependence of Stroke Outcome Scales: Reliable Estimates from the Virtual International Stroke Trials Archive (VISTA)
- Author
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Goldie, F. C., Fulton, R. L., Frank, Benedikt, Lees, K. R., Alexandrov, A., Bath, P. W., Bluhmki, E., Claesson, L., Curram, J., Davis, S. M., Donnan, G., Diener, Hans Christoph, Fisher, M., Gregson, B., Grotta, J., Hacke, W., Hennerici, M. G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N. G., Warach, S., and Weimar, Christian
- Subjects
medicine.medical_specialty ,Archives ,business.industry ,medicine.medical_treatment ,Treatment outcome ,Medizin ,Outcome assessment ,medicine.disease ,Outcome (game theory) ,Clinical neurology ,Stroke ,Clinical trial ,User-Computer Interface ,Treatment Outcome ,Neurology ,Outcome Assessment, Health Care ,Stroke outcome ,Physical therapy ,Humans ,Medicine ,cardiovascular diseases ,business ,Stroke recovery - Abstract
Background and Purpose Clinical deficits from stroke are diverse, prompting measurement in trials by a range of outcome scales. Statistical and clinical advantage can be gained by combining scales into a global outcome provided combinations are chosen with limited correlations. We aimed to clarify the interdependence of outcome scales by systematic review of published data and by novel analysis of data from completed acute trials. Summary of Review We systematically searched ScienceDirect and PubMed to summarize published data on correlations between stroke outcome scales. We generated new data on correlations among salient scales at 90 days poststroke in patients from the Virtual International Stroke Trials Archive (VISTA). We calculated Pearson and Spearman-Rank correlation coefficients for continuous and ordinal measures, respectively. We also assessed partial correlations, adjusted for baseline National Institute of Health Stroke Scale (NIHSS), and age. Published estimates of interdependence were limited to small single-trial cohorts and gave divergent results. From the more extensive VISTA dataset, we found that the modified Rankin Scale at 90 days poststroke explained 80.8% of the National Institute of Health Stroke Scale at 90 days poststroke and 86·5% of the European Stroke Scale. National Institute of Health Stroke Scale explained 75.9% of the Barthel Index and 81·2% of the Scandinavian Stroke Scale. After adjustment, modified Rankin Scale explained 56.6% of National Institute of Health Stroke Scale, 75.2% of Barthel Index. National Institute of Health Stroke Scale explained 60.2% of Barthel Index. Conclusion Correlations and partial correlations among stroke outcome scales in trial datasets are higher than previously reported. The new estimates are more reliable for trial planning due to the sample size and diversity.
- Published
- 2013
44. Selection for Delayed Intravenous Alteplase Treatment Based on a Prognostic Score
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Fulton, R. L., Lees, K. R., Bluhmki, E., Biegert, G., Albers, G. W., Davis, S. M., Donnan, G. A., Grotta, J. C., Hacke, W., Kaste, M., Von Kummer, R., Shuaib, A., Toni, Danilo, Alexandrov, A., Bath, P. W., Claesson, L., Curram, J., Diener, H. C., Fisher, M., Gregson, B., Hennerici, M. G., Hommel, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Teal, P., Wahlgren, N. G., Warach, S., Weimar, C., Collaboration, Vista, Ecass Atlantis Ninds, and Epithet, Investigators
- Subjects
medicine.medical_specialty ,medicine.medical_treatment ,Population ,law.invention ,03 medical and health sciences ,0302 clinical medicine ,Fibrinolytic Agents ,Randomized controlled trial ,law ,Internal medicine ,Odds Ratio ,Humans ,Medicine ,030212 general & internal medicine ,education ,Stroke ,Randomized Controlled Trials as Topic ,education.field_of_study ,business.industry ,Patient Selection ,Thrombolysis ,Odds ratio ,Prognosis ,medicine.disease ,Confidence interval ,3. Good health ,Clinical trial ,Treatment Outcome ,Neurology ,Tissue Plasminogen Activator ,Medical emergency ,business ,030217 neurology & neurosurgery ,Fibrinolytic agent - Abstract
Background and Purpose Approved use of intravenous alteplase for ischemic stroke offers net benefit. Pooled randomized controlled trial analysis suggests additional patients could benefit but others be harmed with treatment initiated beyond 4·5 h after stroke onset. We proposed prognostic scoring methods to identify a strategy for patient selection. Methods We selected 500 patients treated by intravenous alteplase and 500 controls from Virtual International Stroke Trials Archive, matching modified Rankin score outcomes to those from pooled randomized controlled trial 4·5–6 h data. We ranked patients by prognostic score. We chose limits to optimize our sample for a net treatment benefit significant at P = 0·01 by Cochran–Mantel–Haenszel test and by ordinal regression. For validation, we had these applied to the pooled randomized controlled trial data for 4·5–6 h, testing for net benefit by Cochran–Mantel–Haenszel test, ordinal regression, and also by dichotomized outcomes: modified Rankin score 0–1, mortality and parenchymal hemorrhage type 2 bleeds. All analyses were adjusted for age and National Institutes of Health Stroke Scale. Results In the training dataset, limits of 56–95 on a prognostic score retained 714 patients in whom there was net benefit significant at P = 0·01. When applied to the 1120 patients in the pooled randomized controlled trial 4·5–6 h dataset, score limits of 56–95 retained 711 patients and gave odds ratio for improved modified Rankin score distribution of 1·13, 95% confidence interval 0·87–1·47, Cochran–Mantel–Haenszel P = 0·89. More patients achieved modified Rankin score 0–1 (odds ratio 1·44, 1·02–2·05, P = 0·04) but mortality and parenchymal hemorrhage type 2 bleeds were increased: odds ratio 1·56, 1·01–2·40, P = 0·04; odds ratio 15·6, 3·7–65·8, P = 0·0002, respectively. Conclusion Selection of patients between 4·5 and 6 h based on simple clinical measures failed to deliver a population in whom the alteplase effect would be safe and effective.
- Published
- 2013
45. Predicting disability after ischemic stroke based on comorbidity index and stroke severity-from the virtual international stroke trials archive-acute collaboration.
- Author
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Phan T.G., Ma H., Van Ly J., Srikanth V., Lees K.R., Alexandrov A., Bluhmki E., Bornstein N., Claesson L., Davis S.M., Donnan G., Diener H.C., Fisher M., Ginsberg M., Gregson B., Grotta J., Hacke W., Hennerici M.G., Hommel M., Kaste M., Lyden P., Marler J., Muir K., Venketasubramanian N., Sacco R., Shuaib A., Teal P., Wahlgren N.G., Warach S., Weimar C., Chen C., Bath P.M., Clissold B.B., Phan T.G., Ma H., Van Ly J., Srikanth V., Lees K.R., Alexandrov A., Bluhmki E., Bornstein N., Claesson L., Davis S.M., Donnan G., Diener H.C., Fisher M., Ginsberg M., Gregson B., Grotta J., Hacke W., Hennerici M.G., Hommel M., Kaste M., Lyden P., Marler J., Muir K., Venketasubramanian N., Sacco R., Shuaib A., Teal P., Wahlgren N.G., Warach S., Weimar C., Chen C., Bath P.M., and Clissold B.B.
- Abstract
Background and aim: The availability and access of hospital administrative data [coding for Charlson comorbidity index (CCI)] in large data form has resulted in a surge of interest in using this information to predict mortality from stroke. The aims of this study were to determine the minimum clinical data set to be included in models for predicting disability after ischemic stroke adjusting for CCI and clinical variables and to evaluate the impact of CCI on prediction of outcome. Method(s): We leverage anonymized clinical trial data in the Virtual International Stroke Trials Archive. This repository contains prospective data on stroke severity and outcome. The inclusion criteria were patients with available stroke severity score such as National Institutes of Health Stroke Scale (NIHSS), imaging data, and outcome disability score such as 90-day Rankin Scale. We calculate CCI based on comorbidity data in this data set. For logistic regression, we used these calibration statistics: Nagelkerke generalised R2 and Brier score; and for discrimination we used: area under the receiver operating characteristics curve (AUC) and integrated discrimination improvement (IDI). The IDI was used to evaluate improvement in disability prediction above baseline model containing age, sex, and CCI. Result(s): The clinical data among 5,206 patients (55% males) were as follows: mean age 69 +/- 13 years, CCI 4.2 +/- 0.8, and median NIHSS of 12 (IQR 8, 17) on admission and 9 (IQR 5, 15) at 24 h. In Model 2, adding admission NIHSS to the baseline model improved AUC from 0.67 (95% CI 0.65-0.68) to 0.79 (95% CI 0.78-0.81). In Model 3, adding 24-h NIHSS to the baseline model resulted in substantial improvement in AUC to 0.90 (95% CI 0.89-0.91) and increased IDI by 0.23 (95% CI 0.22-0.24). Adding the variable recombinant tissue plasminogen activator did not result in a further change in AUC or IDI to this regression model. In Model 3, the variable NIHSS at 24 h explains 87.3% of the variance of
- Published
- 2017
46. Predicting disability after ischemic stroke based on comorbidity index and stroke severity-from the virtual international stroke trials archive-acute collaboration
- Author
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Phan, TG, Clissold, Ben, Ma, H, Van Ly, J, Srikanth, V, Lees, KR, Alexandrov, A, Bath, PM, Bluhmki, E, Bornstein, N, Chen, C, Claesson, L, Davis, SM, Donnan, G, Diener, HC, Fisher, M, Ginsberg, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, MG, Hommel, M, Kaste, M, Lyden, P, Marler, J, Muir, K, Venketasubramanian, N, Sacco, R, Shuaib, A, Teal, P, Wahlgren, NG, Warach, S, Weimar, C, Phan, TG, Clissold, Ben, Ma, H, Van Ly, J, Srikanth, V, Lees, KR, Alexandrov, A, Bath, PM, Bluhmki, E, Bornstein, N, Chen, C, Claesson, L, Davis, SM, Donnan, G, Diener, HC, Fisher, M, Ginsberg, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, MG, Hommel, M, Kaste, M, Lyden, P, Marler, J, Muir, K, Venketasubramanian, N, Sacco, R, Shuaib, A, Teal, P, Wahlgren, NG, Warach, S, and Weimar, C
- Published
- 2017
47. Statins and risk of poststroke hemorrhagic complications
- Author
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Scheitz, Jan F, MacIsaac, Rachael L, Bluhmki, E., Gregson, B., Donnan, G., Diener, H. C., Grotta, J., Marler, J., Teal, P., Hennerici, M. G., Wahlgren, N. G., Lyden, P., Abdul-Rahim, Azmil H, Bath, P. W., Sacco, R., Davis, S. M., Hacke, W., Warach, S., Fisher, M., Hommel, M., Kaste, M., Muir, K., Shuaib, A., Siegerink, Bob, Weimar, C., Alexandrov, A., Bornstein, N., Ginsberg, M., Bath, Philip M, Endres, Matthias, Lees, Kennedy R, Nolte, Christian H, VISTA collaboration, and Lees, K. R.
- Subjects
Male ,Databases, Factual ,medicine.medical_treatment ,Medizin ,030204 cardiovascular system & hematology ,Severity of Illness Index ,0302 clinical medicine ,Odds Ratio ,complications [Stroke] ,mortality [Stroke] ,Stroke ,Hazard ratio ,adverse effects [Hydroxymethylglutaryl-CoA Reductase Inhibitors] ,Thrombolysis ,etiology [Cerebral Hemorrhage] ,drug therapy [Stroke] ,Treatment Outcome ,Psychotherapy, Group ,Female ,mortality [Cerebral Hemorrhage] ,Risk ,medicine.medical_specialty ,Statin ,medicine.drug_class ,Article ,03 medical and health sciences ,Internal medicine ,therapeutic use [Hydroxymethylglutaryl-CoA Reductase Inhibitors] ,Severity of illness ,medicine ,Humans ,cardiovascular diseases ,ddc:610 ,Aged ,Proportional Hazards Models ,Retrospective Studies ,Cerebral Hemorrhage ,Intracerebral hemorrhage ,business.industry ,Odds ratio ,medicine.disease ,Surgery ,Propensity score matching ,Neurology (clinical) ,Hydroxymethylglutaryl-CoA Reductase Inhibitors ,business ,030217 neurology & neurosurgery ,Follow-Up Studies - Abstract
Objective: To assess whether statin treatment before or after acute ischemic stroke (AIS) affects the risk of acute intracerebral hemorrhage (ICH), postacute ICH, and mortality within 90 days. Methods: Data were sought from the Virtual International Stroke Trials Archive, an international repository of clinical trials data. Using propensity score matching, we retrospectively compared patients with prior statin treatment and newly initiated statin within 3 days after AIS to patients without statin exposure. Outcomes of interest were acute symptomatic ICH (sICH), any acute ICH, postacute ICH, and mortality during follow-up of 3 months. Results: A total of 8,535 patients (mean age 70 years, 54% male, median baseline NIH Stroke Scale score 13) were analyzed. After propensity score matching, prior statin use was not strongly associated with sICH (adjusted odds ratio [OR] 1.33, 95% confidence interval [CI] 0.83–2.14) or any ICH (adjusted OR 1.35, 95% CI 0.92–1.98). There was no evidence of an interaction between prior statin use and thrombolysis. New initiation of statins was not associated with postacute ICH (adjusted hazard ratio [HR] 1.60, 95% CI 0.70–3.65). There was a signal towards lower 90-day mortality in patients with prior statin use (adjusted HR 0.84, 95% CI 0.70–1.00) and especially early initiation of statins (adjusted HR 0.67, 95% CI 0.46–0.97). Conclusions: Statin use prior to AIS was not associated with early hemorrhagic complications, irrespective of treatment with thrombolysis. New initiation of statin treatment early after AIS did not affect risk of postacute ICH, but might be associated with reduced mortality.
- Published
- 2016
48. Stroke Severity and Comorbidity Index for Prediction of Mortality after Ischemic Stroke from the Virtual International Stroke Trials Archive-Acute Collaboration
- Author
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Phan, Thanh G, Clissold, Benjamin, Ly, John, Ma, Henry, Moran, Chris, Srikanth, Velandai, Lees, K R, Alexandrov, A, Bath, P M, Bluhmki, E, Bornstein, N, Claesson, L, Davis, S M, Donnan, G, Diener, Hans Christoph, Fisher, M, Ginsberg, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, M G, Hommel, M, Kaste, M, Lyden, P, Marler, J, Muir, K, Sacco, R, Shuaib, A, Teal, P, Wahlgren, N G, Warach, S, Weimar, Christian, Neurologian yksikkö, and Clinicum
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medicine.medical_specialty ,Databases, Factual ,medicine.medical_treatment ,Medizin ,Severity of Illness Index ,3124 Neurology and psychiatry ,Brain Ischemia ,03 medical and health sciences ,User-Computer Interface ,0302 clinical medicine ,Interquartile range ,Predictive Value of Tests ,Risk Factors ,Severity of illness ,Medicine ,Humans ,030212 general & internal medicine ,cardiovascular diseases ,Cooperative Behavior ,Stroke ,Aged ,Aged, 80 and over ,RISK ,Ischemic stroke ,RECLASSIFICATION ,business.industry ,Rehabilitation ,Regression analysis ,Thrombolysis ,Middle Aged ,Models, Theoretical ,medicine.disease ,mortality ,Confidence interval ,3. Good health ,TISSUE ,Predictive value of tests ,Emergency medicine ,Physical therapy ,Surgery ,Neurology (clinical) ,prognosis ,Cardiology and Cardiovascular Medicine ,business ,Charlson Comorbidity Index ,030217 neurology & neurosurgery - Abstract
M. Kaste on työryhmän VISTA-Acute Collaboration jäsen. Background: There is increasing interest in the use of administrative data (incorporating comorbidity index) and stroke severity score to predict ischemic stroke mortality. The aim of this study was to determine the optimal timing for the collection of stroke severity data and the minimum clinical dataset to be included in models of stroke mortality. To address these issues, we chose the Virtual International Stroke Trials Archive (VISTA), which contains National Institutes of Health Stroke Scale (NIHSS) on admission and at 24 hours, as well as outcome at 90 days. Methods: VISTA was searched for patients who had baseline and 24-hour NIHSS. Improvement in regression models was performed by the net reclassification improvement (NRI) method. Results: The clinical data among 5206 patients were mean age, 69 +/- 13; comorbidity index, 3.3 +/- .9; median NIHSS at baseline, 12 (interquartile range [IQR] 8-17); NIHSS at 24 hours, 9 (IQR 8-15); and death at 90 days in 15%. The baseline model consists of age, gender, and comorbidity index. Adding the baseline NIHSS to model 1 improved the NRI by 0.671 (95% confidence interval [CI] 0.595-0.747) [or 67.1% correct reclassification between model 1 and model 2]. Adding the 24 hour NIHSS term to model 1 (model 3) improved the NRI by 0.929 (95% CI 0.857-1.000) for model 3 versus model 1. Adding the variable thrombolysis to model 3 (model 4) improve NRI by 0.1 (95% CI 0.023-0.178) [model 4 versus model 3]. Conclusion: The optimal model for the prediction of mortality was achieved by adding the 24-hour NIHSS and thrombolysis to the baseline model.
- Published
- 2016
49. Impact of heart rate on admission on mortality and morbidity in acute ischaemic stroke patients - results from VISTA
- Author
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Nolte, C H, Erdur, H, Grittner, U, Schneider, A, Piper, S K, Scheitz, J F, Wellwood, I, Bath, P M W, Diener, Hans Christoph, Lees, K R, Endres, M, Alexandrov, A, Bluhmki, E, Bornstein, N, Chen, C, Claesson, L, Davis, S M, Donnan, G, Fisher, M, Ginsberg, M, Gregson, B, Grotta, J, Hacke, W, Hennerici, M G, Hommel, M, Kaste, M, Lyden, P, Marler, J, Muir, K, Sacco, R, Shuaib, A, Teal, P, Venketasubramanian, N, Wahlgren, N G, Warach, S, and Weimar, Christian
- Subjects
Male ,medicine.medical_specialty ,Heart disease ,acute stroke ,recurrent stroke ,Medizin ,heart failure ,030204 cardiovascular system & hematology ,Brain Ischemia ,Coronary artery disease ,03 medical and health sciences ,0302 clinical medicine ,Patient Admission ,Modified Rankin Scale ,Heart Rate ,Internal medicine ,Atrial Fibrillation ,medicine ,Humans ,cardiovascular diseases ,Myocardial infarction ,Stroke ,Aged ,Aged, 80 and over ,business.industry ,Hazard ratio ,Atrial fibrillation ,Middle Aged ,medicine.disease ,mortality ,Neurology ,Heart failure ,Cardiology ,Female ,Neurology (clinical) ,business ,030217 neurology & neurosurgery - Abstract
BACKGROUND AND PURPOSE: Elevated heart rate (HR) is associated with worse outcomes in patients with cardiovascular disease. Its predictive value in acute stroke patients is less well established. We investigated the effects of HR on admission in acute ischaemic stroke patients. METHODS: Using the Virtual International Stroke Trials Archive (VISTA) database, the association between HR in acute stroke patients without atrial fibrillation and the pre-defined composite end-point of (recurrent) ischaemic stroke, transient ischaemic attack (TIA), myocardial infarction (MI) and vascular death within 90 days was analysed. Pre-defined secondary outcomes were the composite end-point components and any death, decompensated heart failure and degree of functional dependence according to the modified Rankin Scale after 90 days. HR was analysed as a categorical variable (quartiles). RESULTS: In all, 5606 patients were available for analysis (mean National Institutes of Health Stroke Scale 13; mean age 67 years; mean HR 77 bpm; 44% female) amongst whom the composite end-point occurred in 620 patients (11.1%). Higher HR was not associated with the composite end-point. The frequencies of secondary outcomes were 3.2% recurrent stroke (n = 179), 0.6% TIA (n = 35), 1.8% MI (n = 100), 6.8% vascular death (n = 384), 15.0% any death (n = 841) and 2.2% decompensated heart failure (n = 124). Patients in the highest quartile (HR> 86 bpm) were at increased risk for any death [adjusted hazard ratio (95% confidence interval) 1.40 (1.11-1.75)], decompensated heart failure [adjusted hazard ratio 2.20 (1.11-4.37)] and worse modified Rankin Scale [adjusted odds ratio 1.29 (1.14-1.52)]. CONCLUSIONS: In acute stroke patients, higher HR (>86 bpm) is linked to mortality, heart failure and higher degree of dependence after 90 days but not to recurrent stroke, TIA or MI.
- Published
- 2016
50. Development, Expansion, and Use of a Stroke Clinical Trials Resource for Novel Exploratory Analyses
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Ali, Myzoon, Bath, Philip, Brady, Marian, Davis, Stephen, Diener, Hans Christoph, Donnan, Geoffrey, Fisher, Marc, Hacke, Werner, Hanley, Daniel F., Luby, Marie, Tsivgoulis, G., Wahlgren, Nils, Steven Warach, Steven, Lees, Kennedy R., Lees, K. R., Alexandrov, A., Bath, P. W., Bluhmki, E., Claesson, L., Davis, S. M., Gregson, B., Grotta, J., Hennerici, M. G., Hommel, M., Kaste, M., Lyden, P., Marler, J., Muir, K., Sacco, R., Shuaib, A., Teal, P., Wahlgren, N. G., Warach, S., Weimar, Christian, Ashburn, A., Barer, D., Bowen, A., Brodie, E., Corr, S., Drummond, A., Edmans, J., English, C., Gladman, J., Kalra, L., Langhorne, P., Lincoln, N., Logan, P., Mead, G., Patchick, E., Pollock, A., Pomeroy, V., Rodgers, H., Sackley, C., Shaw, L., Sunnerhagen, K. S., Tyson, S., Vliet, P. van, Whiteley, M., Albers, G., Furlan, T., Kidwell, C., Koroshetz, W., Lev, M., Sorensen, G., Wardlaw, J., Wintermark, M., Hanley, D. F., Steiner, T., Mayer, S., Molina, C., and Numminen, H.
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Diagnostic Imaging ,medicine.medical_specialty ,Databases, Factual ,education ,Medizin ,MEDLINE ,Physical medicine and rehabilitation ,Resource (project management) ,medicine ,Humans ,Registries ,cardiovascular diseases ,Clinical care ,Stroke ,health care economics and organizations ,Cerebral Hemorrhage ,Clinical Trials as Topic ,Data collection ,business.industry ,Communication ,Data Collection ,Stroke Rehabilitation ,medicine.disease ,Test (assessment) ,Clinical trial ,Treatment Outcome ,Neurology ,Physical therapy ,Registry data ,business - Abstract
Introduction Analysis of reliable registry data can direct future research to influence clinical care. Data from the Virtual International Stroke Trials Archive have been used to test hypotheses and inform trial design. We sought to expand Virtual International Stroke Trials Archive into a broader stroke resource with new opportunities for research and international collaboration. Methods Using procedures initially developed for an acute stroke trial archive, we invited trialists to lodge data on rehabilitation, secondary prevention, intracerebral haemorrhage, imaging, and observational stroke studies. Results We have extended Virtual International Stroke Trials Archive into six subsections: Virtual International Stroke Trials Archive-Acute ( n = 28 190 patients’ data), Virtual International Stroke Trials Archive-Rehab ( n = 10 194), Virtual International Stroke Trials Archive-intracerebral haemorrhage ( n = 1829), Virtual International Stroke Trials Archive-Prevention, Virtual International Stroke Trials Archive-Imaging ( n = 1300), and Virtual International Stroke Trials Archive-Plus ( n = 6573). Enrollment continues, with commitments for the contribution of six further trials to Virtual International Stroke Trials Archive-Prevention, 13 trials to Virtual International Stroke Trials Archive-Rehab, and one registry to Virtual International Stroke Trials Archive-Plus. Data on age, type of stroke, medical history, outcomes by modified Rankin scale and Barthel Index (BI), mortality, and adverse events are available for analyses. The Virtual International Stroke Trials Archive network encourages the development of young investigators and provides opportunities for international peer review and collaboration. Conclusions Application of the original Virtual International Stroke Trials Archive concepts beyond acute stroke trials can extend the value of clinical research at low cost, without threatening commercial or intellectual property interests. This delivers valuable research output to inform the efficiency of future stroke research. We invite stroke researchers to participate actively in Virtual International Stroke Trials Archive and encourage the extension of Virtual International Stroke Trials Archive principles to other disease areas.
- Published
- 2012
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