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1. Prevalence, Trajectory, and Predictors of Poststroke Pain: Retrospective Analysis of Pooled Clinical Trial Data Set

Author

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.

Published
2023
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2. The protocol for an observational Australian cohort study of CADASIL: The AusCADASIL study.

Author

Saks, DG, Bajorek, B, Catts, VS, Bentvelzen, AC, Jiang, J, Wen, W, Mather, KA, Thalamuthu, A, Huang-Lung, J, Nivison-Smith, L, Griffiths, LR, Smith, RA, Sexton, A, James, P, Jayasena, T, Poljak, A, Hansra, GK, Hosoki, S, Park, A, Hillenbrand, CM, van Wijngaarden, P, Chander, RJ, Humphrey, S, Chen, R, Kochan, NA, Helman, TJ, Levi, C, Brodtmann, A, O'Sullivan, MJ, Markus, R, Butcher, K, Parsons, M, Kovacic, JC, Sachdev, PS, Saks, DG, Bajorek, B, Catts, VS, Bentvelzen, AC, Jiang, J, Wen, W, Mather, KA, Thalamuthu, A, Huang-Lung, J, Nivison-Smith, L, Griffiths, LR, Smith, RA, Sexton, A, James, P, Jayasena, T, Poljak, A, Hansra, GK, Hosoki, S, Park, A, Hillenbrand, CM, van Wijngaarden, P, Chander, RJ, Humphrey, S, Chen, R, Kochan, NA, Helman, TJ, Levi, C, Brodtmann, A, O'Sullivan, MJ, Markus, R, Butcher, K, Parsons, M, Kovacic, JC, and Sachdev, PS

Abstract

INTRODUCTION: Cerebral Autosomal Dominant Arteriopathy with Subcortical Infarcts and Leukoencephalopathy (CADASIL) is a rare genetic condition with a broad phenotypic presentation. This study aims to establish the first Australian cohort of individuals affected by CADASIL (AusCADASIL) and examine its clinical features and longitudinal course, and to investigate neuroimaging and blood biomarkers to assist in early diagnosis and identify disease progression. METHODS: Participants will be recruited from six study centres across Australia for an observational study of CADASIL. We aim to recruit 150 participants with diagnosed CADASIL, family history of CADASIL or suspected CADASIL symptoms, and 150 cognitively normal NOTCH3 negative individuals as controls. Participants will complete: 1) online questionnaires on medical and family history, mental health, and wellbeing; 2) neuropsychological evaluation; 3) neurological examination and brain MRI; 4) ocular examination and 5) blood sample donation. Participants will have annual follow-up for 4 years to assess their progression and will be asked to invite a study partner to corroborate their self-reported cognitive and functional abilities.Primary outcomes include cognitive function and neuroimaging abnormalities. Secondary outcomes include investigation of genetics and blood and ocular biomarkers. Data from the cohort will contribute to an international consortium, and cohort participants will be invited to access future treatment/health intervention trials. DISCUSSION: AusCADASIL will be the first study of an Australian cohort of individuals with CADASIL. The study will identify common pathogenic variants in this cohort, and characterise the pattern of clinical presentation and longitudinal progression, including imaging features, blood and ocular biomarkers and cognitive profile.

Published
2024

3. Outcomes following small bowel obstruction due to malignancy in the national audit of small bowel obstruction

Author

Drake, Thomas M., Lee, Matthew J., Sayers, Adele E., Abercrombie, John, Acheson, Austin, Alderson, Derek, Anderson, Iain, Bradburn, Mike, Davies, Michael, Hamady, Zaed, Hind, Daniel, Hollyman, Marianne, Hare, Sarah, Lee, Ellen, Northover, John, Lewis, Christopher, Marriott, Paul J., Maynard, Nick, McFall, Malcolm, Muragananthan, Aravinth, Murray, David, Singh, Pritam, Tierney, Gillian, Verjee, Azmina, Walsh, Ciaran, Wild, Jonathan RL., Wilson, Timothy, Abbott, S., Abdulaal, Y., Afshar, S., Akhtar, M., Anderson, D., Appleton, S., Bandyopadhyay, D., Bashir, G., Behar, N., Bhandari, S., Branagan, G., Boulton, R., Borg, C., Bouras, G., Boyle, J., Brewer, H., Brown, L., Briggs, C., Cartmell, M., Chan, S., Chandratreya, N., Conaghan, P., Cornish, J., Cotton, D., Coyne, P., Crozier, J., Cook, T., Cunha, P., Curtis, N., Day, A., Dayal, S., Dennis, R., Dent, P., Dowson, H., Fallaize, R., Farag, S., El Farran, M., Faulkner, G., Giordano, P., Grey, T., Halahakoon, V., Hannay, J., Harikrishnan, A., Holtham, S., Hawkin, P., Hall, C., Hancock, L., Hartley, J., Howse, F., Kallam, R., Kakaniaris, G., Kelly, S., Lockwood, S., Leinhardt, D., Levy, B., Lal, R., Lazim, T., Lund, J., Lunevicius, R., Mathur, P., Maude, K., McArthur, D., McIlroy, B., Miles, A., Moug, S., Mondragon-Pritchard, M., Messenger, D., Mullan, M., Myers, A., Muhammad, K., Mason, C., Sarveswaran, J., Shatkar, V., Singh, B., Skelly, B., Subramonia, S., Swinscoe, M., Thava, B., Thorn, C., Panagiotopoulos, S., Patel, P., Phillips, J., Peristerakis, I., Qureshi, A., Saunders, M., Shah, P., Sheel, A., Siddiqui, S., Skaife, P., Smart, N., Smith, I., Stevenson, L., Stylianides, N., Steinke, J., Stubbs, B., Thompson, R., Varcada, M., Vimalachandran, D., Virlos, I., Watfah, J., Watson, N., Walker, M., Ventham, N., West, H., Wilson, J., Wijeyekoon, S., Ah-Chuen, J., Ahmed, T., Akram, F., Aldred, E., Ali, A., Aly, M., Amajuoyi, A., Amin, V., Andreou, A., Ansari, A., Ardley, R., Arshad, F., Ashour, O., Asour, A., Ayoub, F., Azeem, H., Azhar, B., Baillie, C., Barker, J., Barkham, B., Baron, R., Barrie, J., Barry-Yarrow, E., Battersby, N., Bazoua, G., Berger, C., Bhasin, S., Biggs, S., Bisset, C., Blencowe, N., Boddy, A., Boereboom, C., Bogdan, M., Bogle, R., Bohra, P., Bolkan, H., Boyer, M., Broadhurst, J., Brown, E., Brown, J., Burns, K., Butcher, K., Capper, C., Cash, T., Chapman, J., Chapman, S., Charalabopoulos, A., Cheek, C., Chok, S., Choong, W., Chowdhury, J., Coe, P., Conn, G., Cook, N., Cooper, S., Cox, C., Crook, R., Cuffolo, G., da Silva, L., Das, B., Davenport, M., Davies, J., Davies, T., Dean, S., Demetriou, G., Dengu, F., Dent, H., Di Benedetto, G., Dindyal, S., Donnelly, E., Douka, E., Downham, C., Edent, H., Edgerton, K., El-Sharif, M., Elamin, O., Elsaid, N., Evans, J., Evans, M., Ewe, R., Ewing, A., Ferguson, H., Fisher, O., Fletcher, J., Forouzanfar, A., Foster, A., Fox, R., Francis, N., Fretwell, V., Fung, D., Gammeri, E., Garnham, J., Geraghty, A., Gilbert, A., Gill, M., Gillespie, M., Glasbey, J., Golder, A., Green, N., Groundwater, E., Grove, T., Habib, H., Haddow, J., Halkias, C., Hampson, A., Hanna, T., Harries, R., Harvey, K., Hawkins, J., Healy, R., Heartshorne, R., Heller, S., Hendra, L., Herrod, P., Heywood, N., Hicks, G., Ng, P., Hope, C., Hopley, P., Hossain, T., Hossaini, S., Hubbard, T., Humphreys, A., Ikram, H., Ioannis, M., Iqbal, M., Jatania, J., Jenkinson, P., Jokhan, S., Jones, A., Jones, C., Jones, L., Joshi, H., Joshi, K., Joy, M., Jull, P., Kane, E., Kanitkar, R., Kauser, S., Kazmi, F., Kedrzycki, M., Kendall, J., Khan, T., King, G., Kisiel, A., Kitsis, C., Kolawole, I., Kosasih, S., Kosti, A., Kotb, A., Lau, A., Lafaurie, G., Lazzaro, A., Lefroy, R., Lennon, H., Leong, K., Lim, E., Lim, J., Lindley, S., Liu, D., Lloyd, P., Locker, D., Lowe, C., Lunt, A., Lutfi, S., Luther, A., Luwemba, S., Mahankali-Rao, P., Mai, D., Majid, S., Malik, A., Manu, N., Mapara, R., Martin, C., Martin, J., Massey, L., Mathias, J., McCain, S., McCluney, S., McNair, A., Mekhail, P., Merchant, J., Merker, L., Mir, S., Mistry, P., Miu, V., Moat, M., Mohamed, E., Mohamed, I., Moore, N., Moretti, L., Morris, H., Morrison, T., Moss, J., Mountford, D., Moynihan, R., Muldoon-Smith, D., Mulholland, J., Murgitroyd, E., Murugaiyan, K., Mykoniatis, I., Nana, G., Nash, T., Nassar, A., Newton, R., Nguyen, K., Nicholas, F., Noor, M., Nowers, J., Nugent, C., Nunn, A., O'Callaghan, J., O'Hara, R., O'Neill, A., Olivier, J., Osei-Bordom, D., Osgood, L., Panchasara, B., Parks, R., Patel, H., Pawelec, K., Payne, C., Pearson, K., Perin, G., Petronio, B., Phelan, L., Pisaneschi, C., Pitt, J., Ponchietti, L., Powell, A., Powell-Chandler, A., Pranesh, N., Proctor, V., Qureshi, N., Rahman, M., Rai, Z., Ramcharan, S., Rangarajan, K., Rashid, M., Reader, H., Rehman, A., Rehan, S., Rengifo, C., Richardson, N., Robinson, A., Robinson, D., Rossi, B., Rutherford, F., Sadien, I., Saghir, T., Sahnan, K., Salahia, G., Scott, B., Scott, K., Seager, A., Seal, S., Sezen, E., Shaban, F., Shahmohammadi, M., Shamsiddinova, A., Shankar, S., Sharpe, A., Shields, T., Shinkwin, M., Shurmer, J., Siddika, A., Simson, R., Singh, S., Sivaraj, J., Skinner, A., Smart, C., Smith, F., Smith, R., Sreedhar, A., Stewart-Parker, E., Stott, M., Symons, N., Taj, T., Tam, J., Tan, K., Tani, S., Tao, D., Thippeswamy, K., Thomas, C., Thompson, E., Thompson-Reil, C., Tongo, F., Toth, G., Turnbull, A., Turnbull, J., Wade, T., Wafi, A., Waite, K., Walker, N., Walker, T., Walsh, U., Wardle, S., Warner, R., Watt, J., Watts, J., Wayman, J., Weegenaar, C., West, M., Whyler, M., Whitehurst, L., Wiggans, M., Williams, G., Williams, R., Williamson, A., Williamson, J., Winter, A., Wolpert, L., Wong, J., van Boxel, G., Yeap, E., Zaman, S., Zappa, B., Zosimas, D., Anderson, O., Athem, A., Athersmith, M., Badenoch, T., Barker, S., Bellam, S., Boam, T., Boland, M., Blake, L., Brown, O., Butler, M., Byrne, B., Campbell, L., Chow, M., Da Costa, K., Cutting, J., Deputy, M., Devoto, L., Doody, P., Ekpete, N., Eljaafari, M., Exarchou, K., Faoury, M., Farinella, E., Gill, C., Goh, M., Gregoir, T., Growcott, S., Gunasekaran, S., Harris, G., Heard, R., Hobson, B., Iqbal, N., Jain, R., Kang, P., Khan, M., Korambayil, S., Kouris, S., Kshatriya, K., Kumar, S., Lee, K., Mahroof, S., Malik, K., Mann, K., Mansour, S., Martin, R., McKay, S., McKinley, N., McWhirter, D., Mellor, K., Mishra, A., Mockford, K., Morrison-Jones, V., Ng, C., Nunn, R., O'Neill, S., Oke, O., Obeid, N., Patel, R., Patel, S., Plunkett-Reed, K., Pouzi, M., Pywell, S., Richards, E., Sinclair, P., Slim, N., Spence, G., Swinkin, M., Tahir, W., Takacs, K., Tanner, N., Taylor, M., Valero, C., Venn, M., Venza, M., Yeong, T., and Fearnhead, Nicola S.

Published
2019
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4. Amelogenins in human developing and mature dental pulp.

Author

Ye, L, Le, TQ, Zhu, L, Butcher, K, Schneider, RA, Li, W, and Besten, PK Den

Subjects
Cells, Cultured, Odontoblasts, Dental Pulp, Dentin, Dental Papilla, Humans, Cell Cycle Proteins, Recombinant Proteins, Oligonucleotide Array Sequence Analysis, Cell Differentiation, Cell Proliferation, Alternative Splicing, Odontogenesis, Molecular Weight, Amelogenin, amelogenin, alternative splicing, proliferation, dental papilla cells, dental pulp cells, odontoblasts, dentin, Cells, Cultured, Dentistry
Abstract

Amelogenins are a group of heterogenous proteins first identified in developing tooth enamel and reported to be present in odontoblasts. The objective of this study was to elucidate the expression and function of amelogenins in the human dentin-pulp complex. Developing human tooth buds were immunostained for amelogenin, and mRNA was detected by in situ hybridization. The effects of recombinant amelogenins on pulp and papilla cell proliferation were measured by Brd U immunoassay, and differentiation was monitored by alkaline phosphatase expression. Amelogenin protein was found in the forming dentin matrix, and amelogenin mRNA was localized in the dentin, presumably in the odontoblast processes. Proliferation of papilla cells was enhanced by recombinant human amelogenin rH72 (LRAP+ exon 4), while pulp cells responded to both rH72 and rH58 (LRAP), with no effect by rH174. These studies suggest that odontoblasts actively synthesize and secrete amelogenin protein during human tooth development, and that low-molecular-weight amelogenins can enhance pulp cell proliferation.

Published
2006

5. A Pragmatic Randomized Trial Comparing Surgical Clipping and Endovascular Treatment of Unruptured Intracranial Aneurysms

Author

Darsaut, T.E., primary, Findlay, J.M., additional, Bojanowski, M.W., additional, Chalaala, C., additional, Iancu, D., additional, Roy, D., additional, Weill, A., additional, Boisseau, W., additional, Diouf, A., additional, Magro, E., additional, Kotowski, M., additional, Keough, M.B., additional, Estrade, L., additional, Bricout, N., additional, Lejeune, J.-P., additional, Chow, M.M.C., additional, O’Kelly, C.J., additional, Rempel, J.L., additional, Ashforth, R.A., additional, Lesiuk, H., additional, Sinclair, J., additional, Erdenebold, U.-E., additional, Wong, J.H., additional, Scholtes, F., additional, Martin, D., additional, Otto, B., additional, Bilocq, A., additional, Truffer, E., additional, Butcher, K., additional, Fox, A.J., additional, Arthur, A.S., additional, Létourneau-Guillon, L., additional, Guilbert, F., additional, Chagnon, M., additional, Zehr, J., additional, Farzin, B., additional, Gevry, G., additional, and Raymond, J., additional

Published
2023
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9. TACTICS-Trial of Advanced CT Imaging and Combined Education Support for Drip and Ship: evaluating the effectiveness of an 'implementation intervention' in providing better patient access to reperfusion therapies: protocol for a non-randomised controlled stepped wedge cluster trial in acute stroke

Author

Ryan, A, Paul, CL, Cox, M, Whalen, O, Bivard, A, Attia, J, Bladin, C, Davis, SM, Campbell, BC, Parsons, M, Grimley, RS, Anderson, C, Donnan, GA, Oldmeadow, C, Kuhle, S, Walker, FR, Hood, RJ, Maltby, S, Keynes, A, Delcourt, C, Hatchwell, L, Malavera, A, Yang, Q, Wong, A, Muller, C, Sabet, A, Garcia-Esperon, C, Brown, H, Spratt, N, Kleinig, T, Butcher, K, Levi, CR, Ryan, A, Paul, CL, Cox, M, Whalen, O, Bivard, A, Attia, J, Bladin, C, Davis, SM, Campbell, BC, Parsons, M, Grimley, RS, Anderson, C, Donnan, GA, Oldmeadow, C, Kuhle, S, Walker, FR, Hood, RJ, Maltby, S, Keynes, A, Delcourt, C, Hatchwell, L, Malavera, A, Yang, Q, Wong, A, Muller, C, Sabet, A, Garcia-Esperon, C, Brown, H, Spratt, N, Kleinig, T, Butcher, K, and Levi, CR

Abstract

INTRODUCTION: Stroke reperfusion therapies, comprising intravenous thrombolysis (IVT) and/or endovascular thrombectomy (EVT), are best practice treatments for eligible acute ischemic stroke patients. In Australia, EVT is provided at few, mainly metropolitan, comprehensive stroke centres (CSC). There are significant challenges for Australia's rural and remote populations in accessing EVT, but improved access can be facilitated by a 'drip and ship' approach. TACTICS (Trial of Advanced CT Imaging and Combined Education Support for Drip and Ship) aims to test whether a multicomponent, multidisciplinary implementation intervention can increase the proportion of stroke patients receiving EVT. METHODS AND ANALYSIS: This is a non-randomised controlled, stepped wedge trial involving six clusters across three Australian states. Each cluster comprises one CSC hub and a minimum of three primary stroke centre (PSC) spokes. Hospitals will work in a hub and spoke model of care with access to a multislice CT scanner and CT perfusion image processing software (MIStar, Apollo Medical Imaging). The intervention, underpinned by behavioural theory and technical assistance, will be allocated sequentially, and clusters will move from the preintervention (control) period to the postintervention period. PRIMARY OUTCOME: Proportion of all stroke patients receiving EVT, accounting for clustering. SECONDARY OUTCOMES: Proportion of patients receiving IVT at PSCs, proportion of treated patients (IVT and/or EVT) with good (modified Rankin Scale (mRS) score 0-2) or poor (mRS score 5-6) functional outcomes and European Quality of Life Scale scores 3 months postintervention, proportion of EVT-treated patients with symptomatic haemorrhage, and proportion of reperfusion therapy-treated patients with good versus poor outcome who presented with large vessel occlusion at spokes. ETHICS AND DISSEMINATION: Ethical approval has been obtained from the Hunter New England Human Research Ethics Committee (18/09

Published
2022

10. Association of Endovascular Thrombectomy With Functional Outcome in Patients With Acute Stroke With a Large Ischemic Core

Author

Garcia-Esperon, C, Bivard, A, Johns, H, Chen, C, Churilov, L, Lin, L, Butcher, K, Kleinig, TJ, Choi, PMC, Cheng, X, Dong, Q, Aviv, R, Miteff, F, Spratt, NJ, Levi, CR, Parsons, MW, Garcia-Esperon, C, Bivard, A, Johns, H, Chen, C, Churilov, L, Lin, L, Butcher, K, Kleinig, TJ, Choi, PMC, Cheng, X, Dong, Q, Aviv, R, Miteff, F, Spratt, NJ, Levi, CR, and Parsons, MW

Abstract

BACKGROUND AND OBJECTIVES: Endovascular thrombectomy (EVT) is effective for patients with large vessel occlusion (LVO) stroke with smaller volumes of CT perfusion (CTP)-defined ischemic core. However, the benefit of EVT is unclear in those with a core volume >70 mL. We aimed to compare outcomes of EVT and non-EVT patients with an ischemic core volume ≥70 mL, hypothesizing that there would be a benefit from EVT for fair outcome (3-month modified Rankin scale [mRS] 0-3) after stroke. METHODS: A retrospective analysis of patients enrolled into a multicenter (Australia, China, and Canada) registry (2012-2020) who underwent CTP within 24 hours of stroke onset and had a baseline ischemic core volume ≥70 mL was performed. The primary outcome was the estimation of the association of EVT in patients with core volume ≥70 mL and within 70-100 and ≥100 mL subgroups with fair outcome. RESULTS: Of the 3,283 patients in the registry, 299 had CTP core volume ≥70 mL and 269 complete data (135 had core volume between 70 and 100 mL and 134 had core volume ≥100 mL). EVT was performed in 121 (45%) patients. EVT-treated patients were younger (median 69 vs 75 years; p = 0.011), had lower prestroke mRS, and smaller median core volumes (92 [79-116.5] mL vs 105.5 [85.75-138] mL, p = 0.004). EVT-treated patients had higher odds of achieving fair outcome in adjusted analysis (30% vs 13.9% in the non-EVT group; adjusted odds ratio [aOR] 2.1, 95% CI 1-4.2, p = 0.038). The benefit was seen predominantly in those with 70-100 mL core volume (71/135 [52.6%] EVT-treated), with 54.3% in the EVT-treated vs 21% in the non-EVT group achieving a fair outcome (aOR 2.5, 95% CI 1-6.2, p = 0.005). Of those with a core volume ≥100 mL, 50 of the 134 (37.3%) underwent EVT. Proportions of fair outcome were very low in both groups (8.1% vs 8.7%; p = 0.908). DISCUSSION: We found a positive association of EVT with the 3-month outcome after stroke in patients with a baseline CTP ischemic core volume 70-100 mL but not

Published
2022

14. What Is the “Optimal” Target Mismatch Criteria for Acute Ischemic Stroke?

Author

Chen, C, Parsons, MW, Levi, CR, Spratt, NJ, Lin, L, Kleinig, T, Butcher, K, Cheng, X, Dong, Q, O'Brien, B, Avivi, RI, Krause, M, Sylaja, PN, Choi, P, Bhuta, S, Yin, C, Yang, J, Wang, P, Qiu, W, Bivard, A, Chen, C, Parsons, MW, Levi, CR, Spratt, NJ, Lin, L, Kleinig, T, Butcher, K, Cheng, X, Dong, Q, O'Brien, B, Avivi, RI, Krause, M, Sylaja, PN, Choi, P, Bhuta, S, Yin, C, Yang, J, Wang, P, Qiu, W, and Bivard, A

Abstract

We aimed to compare Perfusion Imaging Mismatch (PIM) and Clinical Core Mismatch (CCM) criteria in ischemic stroke patients to identify the effect of these criteria on selected patient population characteristics and clinical outcomes. Patients from the INternational Stroke Perfusion Imaging REgistry (INSPIRE) who received reperfusion therapy, had pre-treatment multimodal CT, 24-h imaging, and 3 month outcomes were analyzed. Patients were divided into 3 cohorts: endovascular thrombectomy (EVT), intravenous thrombolysis alone with large vessel occlusion (IVT-LVO), and intravenous thrombolysis alone without LVO (IVT-nonLVO). Patients were classified using 6 separate mismatch criteria: PIM-using 3 different measures to define the perfusion deficit (Delay Time, Tmax, or Mean Transit Time); or CCM-mismatch between age-adjusted National Institutes of Health Stroke Scale and CT Perfusion core, defined as relative cerebral blood flow <30% within the perfusion deficit defined in three ways (as above). We assessed the eligibility rate for each mismatch criterion and its ability to identify patients likely to respond to treatment. There were 994 patients eligible for this study. PIM with delay time (PIM-DT) had the highest inclusion rate for both EVT (82.7%) and IVT-LVO (79.5%) cohorts. In PIM positive patients who received EVT, recanalization was strongly associated with achieving an excellent outcome at 90-days (e.g., PIM-DT: mRS 0-1, adjusted OR 4.27, P = 0.005), whereas there was no such association between reperfusion and an excellent outcome with any of the CCM criteria (all p > 0.05). Notably, in IVT-LVO cohort, 58.2% of the PIM-DT positive patients achieved an excellent outcome compared with 31.0% in non-mismatch patients following successful recanalization (P = 0.006). Conclusion: PIM-DT was the optimal mismatch criterion in large vessel occlusion patients, combining a high eligibility rate with better clinical response to reperfusion. No mismatch criterion was useful t

Published
2021

15. Pre-hospital triage of suspected acute stroke patients in a mobile stroke unit in the rural Alberta

Author

Kate, MP, Jeerakathil, T, Buck, BH, Khan, K, Nomani, AZ, Butt, A, Thirunavukkarasu, S, Nowacki, T, Kalashyan, H, Lloret-Villas, MI, D’Souza, A, Mishra, S, McCombe, J, Butcher, K, Jickling, G, Saqqur, M, Shuaib, A, Kate, MP, Jeerakathil, T, Buck, BH, Khan, K, Nomani, AZ, Butt, A, Thirunavukkarasu, S, Nowacki, T, Kalashyan, H, Lloret-Villas, MI, D’Souza, A, Mishra, S, McCombe, J, Butcher, K, Jickling, G, Saqqur, M, and Shuaib, A

Abstract

Mobile Stroke Unit (MSU) expedites the delivery of intravenous thrombolysis in acute stroke patients. We further evaluated the functional outcome of patients shipped to a tertiary care centre or repatriated to local hospitals after triage by MSU in acute stroke syndrome in rural northern Alberta. Consecutive patients with suspected acute stroke syndrome were included. On the basis of neurology consultation and, Computed Tomography findings, patients, who were thrombolysed or needed advanced care were transported to the Comprehensive stroke center (CSC) (Triage to CSC group). Other patients were repatriated to local hospital care (Triage to LHC group). A total of 156 patients were assessed in MSU, 73 (46.8%) were female and the mean age was 66.6 ± 15 years. One hundred and eight (69.2%) patients, including 41 (26.3%) treated with thrombolysis were transported to the CSC (Triage to CSC group) and 48 (30.8%) were repatriated to local hospital care. The diagnosis made in MSU and final diagnosis were matching in 88% (95) and 91.7% (44, p = 0.39) in Triage to CSC and Triage to LHC groups respectively. Prehospital triage by MSU of acute stroke syndrome can reliably repatriate patients to the home hospital. The proposed model has the potential to triage patients according to their medical needs by enabling treatment in home hospitals whenever reasonable.

Published
2021

16. Protocol for LASER: A Randomized Evaluation and an Associated Registry of Early Anticoagulation With Edoxaban After Ischemic Stroke in Patients With Atrial Fibrillation

Author

Alrohimi, A, Jickling, G, Jeerakathil, T, Shuaib, A, Khan, K, Kate, M, Hill, MD, Buck, B, Butcher, K, Alrohimi, A, Jickling, G, Jeerakathil, T, Shuaib, A, Khan, K, Kate, M, Hill, MD, Buck, B, and Butcher, K

Abstract

Background: The optimal timing of anticoagulation after stroke in patients with atrial fibrillation (AF) is unknown. Aim and Hypothesis: Our primary aim is to demonstrate the safety of edoxaban initiation within 5 days of AF related stroke. Our secondary aim is to determine predictors of hemorrhagic transformation (HT) after AF related stroke. We hypothesize that the rate of radiological HT will not be increased in patients starting edoxaban within 5 days of AF related stroke, relative to those in whom initiation is delayed. We hypothesize that the risk of HT in patients treated with edoxaban can be predicted using RNA expressed in leukocytes at time of stroke. Methods and Design: LASER (Lixiana Acute Stroke Evaluation Registry) is a randomized controlled trial with an associated registry (clinicaltrials.gov NCT03494530). One hundred and fifty patients with ischemic stroke and AF will undergo baseline Computed Tomography (CT) scan and will be randomized 2:1 within 5 days of symptom onset to early (≤5 days, n = 100) or delayed (6–14 days, n = 50) edoxaban initiation. Participants will undergo clinical assessment and repeat CT at 7 days and clinical assessment at 90 days. Study Outcomes: The primary outcome is the rate of incident radiological HT. Secondary outcomes include symptomatic HT, recurrent ischemic stroke, recurrent sub-clinical infarcts on follow up CT, systemic hemorrhagic complication rate, National Institute of Health Stroke Scale and modified Rankin Scale at day 7 and 90, mortality within 90 days, quality of life assessments at day 90, and predictors of HT, including RNA expression by 6 pre-selected candidate genes. Discussion: Event rates for both HT and recurrent ischemic events, in patients treated with early vs. delayed edoxaban initiation are unknown. The primary study endpoint of LASER is an objective performance criterion relevant to clinical decision making in patients with AF related stroke. This study will provide data required for a definitiv

Published
2021

17. Real-World Cost-Effectiveness of Late Time Window Thrombectomy for Patients With Ischemic Stroke

Author

Gao, Lan, Bivard, A, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Dong, Q, Cheng, X, Lou, M, Yin, C, Chen, C, Wang, P, Lin, L, Choi, P, Miteff, F, Moodie, Marj, Gao, Lan, Bivard, A, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Dong, Q, Cheng, X, Lou, M, Yin, C, Chen, C, Wang, P, Lin, L, Choi, P, Miteff, F, and Moodie, Marj

Abstract

Background: To compare the cost-effectiveness of providing endovascular thrombectomy (EVT) for patients with ischemic stroke in the >4.5h time window between patient groups who met and did not meet the perfusion imaging trial criteria. Methods: A discrete event simulation (DES) model was developed to simulate the long-term outcome post EVT in patients meeting or not meeting the extended time window clinical trial perfusion imaging criteria at presentation, vs. medical treatment alone (including intravenous thrombolysis). The effectiveness of thrombectomy in patients meeting the landmark trial criteria (DEFUSE 3 and DAWN) was derived from a prospective cohort study of Australian patients who received EVT for ischemic stroke, between 2015 and 2019, in the extended time window (>4.5 h). Results: Endovascular thrombectomy was shown to be a cost-effective treatment for patients satisfying the clinical trial criteria in our prospective cohort [incremental cost-effectiveness ratio (ICER) of $11,608/quality-adjusted life year (QALY) for DEFUSE 3-postive or $34,416/QALY for DAWN-positive]. However, offering EVT to patients outside of clinical trial criteria was associated with reduced benefit (−1.02 QALY for DEFUSE 3; −1.43 QALY for DAWN) and higher long-term patient costs ($8,955 for DEFUSE 3; $9,271 for DAWN), thereby making it unlikely to be cost-effective in Australia. Conclusions: Treating patients not meeting the DAWN or DEFUSE 3 clinical trial criteria in the extended time window for EVT was associated with less gain in QALYs and higher cost. Caution should be exercised when considering this procedure for patients not satisfying the trial perfusion imaging criteria for EVT.

Published
2021

18. Real-World Cost-Effectiveness of Late Time Window Thrombectomy for Patients With Ischemic Stroke

Author

Gao, L, Bivard, A, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Dong, Q, Cheng, X, Lou, M, Yin, C, Chen, C, Wang, P, Lin, L, Choi, P, Miteff, F, Moodie, M, Gao, L, Bivard, A, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Dong, Q, Cheng, X, Lou, M, Yin, C, Chen, C, Wang, P, Lin, L, Choi, P, Miteff, F, and Moodie, M

Abstract

Background: To compare the cost-effectiveness of providing endovascular thrombectomy (EVT) for patients with ischemic stroke in the >4.5 h time window between patient groups who met and did not meet the perfusion imaging trial criteria. Methods: A discrete event simulation (DES) model was developed to simulate the long-term outcome post EVT in patients meeting or not meeting the extended time window clinical trial perfusion imaging criteria at presentation, vs. medical treatment alone (including intravenous thrombolysis). The effectiveness of thrombectomy in patients meeting the landmark trial criteria (DEFUSE 3 and DAWN) was derived from a prospective cohort study of Australian patients who received EVT for ischemic stroke, between 2015 and 2019, in the extended time window (>4.5 h). Results: Endovascular thrombectomy was shown to be a cost-effective treatment for patients satisfying the clinical trial criteria in our prospective cohort [incremental cost-effectiveness ratio (ICER) of $11,608/quality-adjusted life year (QALY) for DEFUSE 3-postive or $34,416/QALY for DAWN-positive]. However, offering EVT to patients outside of clinical trial criteria was associated with reduced benefit (-1.02 QALY for DEFUSE 3; -1.43 QALY for DAWN) and higher long-term patient costs ($8,955 for DEFUSE 3; $9,271 for DAWN), thereby making it unlikely to be cost-effective in Australia. Conclusions: Treating patients not meeting the DAWN or DEFUSE 3 clinical trial criteria in the extended time window for EVT was associated with less gain in QALYs and higher cost. Caution should be exercised when considering this procedure for patients not satisfying the trial perfusion imaging criteria for EVT.

Published
2021

19. Assessing the Relative Value of CT Perfusion Compared to Non-contrast CT and CT Angiography in Prognosticating Reperfusion-Eligible Acute Ischemic Stroke Patients

Author

Bivard, A, Levi, C, Lin, L, Cheng, X, Aviv, R, Spratt, NJ, Kleinig, T, Butcher, K, Chen, C, Dong, Q, Parsons, M, Bivard, A, Levi, C, Lin, L, Cheng, X, Aviv, R, Spratt, NJ, Kleinig, T, Butcher, K, Chen, C, Dong, Q, and Parsons, M

Abstract

In the present study we sought to measure the relative statistical value of various multimodal CT protocols at identifying treatment responsiveness in patients being considered for thrombolysis. We used a prospectively collected cohort of acute ischemic stroke patients being assessed for IV-alteplase, who had CT-perfusion (CTP) and CT-angiography (CTA) before a treatment decision. Linear regression and receiver operator characteristic curve analysis were performed to measure the prognostic value of models incorporating each imaging modality. One thousand five hundred and sixty-two sub-4.5 h ischemic stroke patients were included in this study. A model including clinical variables, alteplase treatment, and NCCT ASPECTS was weak (R 2 0.067, P < 0.001, AUC 0.605) at predicting 90 day mRS. A second model, including dynamic CTA variables (collateral grade, occlusion severity) showed better predictive accuracy for patient outcome (R 2 0.381, P < 0.001, AUC 0.781). A third model incorporating CTP variables showed very high predictive accuracy (R 2 0.488, P < 0.001, AUC 0.899). Combining all three imaging modalities variables also showed good predictive accuracy for outcome but did not improve on the CTP model (R 2 0.439, P < 0.001, AUC 0.825). CT perfusion predicts patient outcomes from alteplase therapy more accurately than models incorporating NCCT and/or CT angiography. This data has implications for artificial intelligence or machine learning models.

Published
2021

20. A multicentre cohort study assessing day of week effect and outcome from emergency appendicectomy

Author

Ferguson, Henry JM, Hall, Nigel J, Bhangu, Aneel, Panagiotopoulou, I G, Chatzizacharias, N, Rana, M, Rollins, K, Ejtehadi, F, Jha, B, Tan, Y W, Fanous, N, Markides, G, Tan, A, Marshal, C, Akhtar, S, Mullassery, D, Ismail, A, Hitchins, C, Sharif, S, Osborne, L, Sengupta, N, Challand, C, Pournaras, D, Bevan, K, King, J, Massey, J, Sandhu, I, Wells, J M, Teichmann, D A, Peckham-Cooper, A, Sellers, M, Folaranmi, S E, Davies, B, Potter, S, Egbeare, D, Kallaway, C, Parsons, S, Upchurch, E, Lazaridis, A, Cocker, D, King, D, Behar, N, Loukogeorgakis, S P, Kalaiselvan, R, Marzouk, S, Turner, E J H, Kaptanis, S, Kaur, V, Shingler, G, Bennett, A, Shaikh, S, Aly, M, Coad, J, Khong, T, Nouman, Z, Crawford, J, Szatmary, P, West, H, Lambert, J, Gash, K, Hanks, K A, Griggs, E, Humphreys, L, Torrance, A, Hardman, J, Taylor, L, Rex, D, Bennett, J, Crowther, N, McAree, B, Flexer, S, Mistry, P, Jain, P, Hwang, M, Oswald, N, Wells, A, Newsome, H, Martinez, P, Alvarez, C A B, León, J, Carradice, D, Gohil, R, Mount, M, Campbell, A, Iype, S, Dyson, E, Groot-Wassink, T, Ross, A R, Jones, C, Charlesworth, P, Baylem, N, Voll, J, Sian, T, Creedon, L, Hicks, G, Goring, J, Ng, V, Tiboni, S, Palser, T, Rees, B, Ravindra, P, Neophytou, C, Dent, H, Lo, T, Broom, L, OʼConnell, M, Foulkes, R, Griffith, D, Butcher, K, Mclaren, O, Tai, A, Yano, H, Torrance, H D T, Moussa, O, Mittapalli, D, Watt, D, Basson, S, Gilliland, J, Pilgrim, S, Wilkins, A, Yee, J, Cain, H, Wilson, M, Pearson, J, Turnbull, E, Brigic, A, Yassin, N A, Clarke, J, Mallappa, S, Jackson, P, Jones, C, Lakshminarayanan, B, Sharma, A, Velineni, R, Fareed, K, Yip, G, Brown, A, Patel, N, Ghisel, M, Tanner, N, Jones, H, Witherspoon, J, Phillips, M, Ho, M F, Ng, S, Mak, T, Campain, N, Mukhey, D, Mitchell, W K, Amawi, F, Dickson, E, Aggarwal, S, Satherley, L K, Asprou, F, Keys, C, Steven, M, Johnstone, M, Muhlschlegel, J, Hamilton, E, Yin, J, Dilworth, M, Wright, A, Spreadborough, P, Singh, M, Mockford, K, Morgan, J, Ball, W, Royle, J, Lacy-Colson, J, Lai, W, Griffiths, S, Mitchell, S, Parsons, C, Joel, A S, Mason, P F, Harrison, G J, Steinke, J, Rafique, H, Battersby, C, Hawkins, W, Gurram, D, Hateley, C A, Penkethman, A, Lambden, C, Conway, A, Dent, P, Yacob, D, Oshin, O A, Hargreaves, A, Gossedge, G, Long, J, Walls, M, Futaba, K, Pinkney, T, Puig, S, Boddy, A, Jones, A, Tennuci, C, Battersby, N, Wilkin, R, Lloyd, C, Sein, E, McEvoy, K, Whisker, L, Austin, S, Colori, A, Sinclair, P, Loughran, M, Lawrence, A, Horsnell, J, Bagenal, J, Pisesky, A, Mastoridis, S, Solanki, K, Siddiq, I, Merker, L, Sarmah, P, Richardson, C, Hanratty, D, Evans, L, Mortimer, M, Bhalla, A, Bartlett, D, Beral, D, Blencowe, N S, Cornish, J, Haddow, J B, Hall, N J, Johnstone, M, Pilgrim, S, Strong, S, Velineni, R, Marriot, P, Vohra, R, Patel, A, Poon, H, and Hepburn, E

Published
2014
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22. Outcomes of obstructed abdominal wall hernia: results from the UK national small bowel obstruction audit

Author

Lee, MJ, Drake, TM, Sayers, AE, Walsh, CJ, Davies, MM, Fearnhead, NS, Abercrombie, J, Acheson, A, Alderson, D, Anderson, I, Bach, S, Davies, M, Hamady, Z, Hind, D, Hollyman, M, Hare, S, Lee, E, Northover, J, Lewis, C, Marriott, P, Maynard, N, Murray, D, Tierney, G, Verjee, A, Wild, J, Abbott, S, Abdulaal, Y, Afshar, S, Ah‐Chuen, J, Ahmed, T, Akhtar, M, Akram, F, Aldred, E, Ali, A, Aly, M, Amajuoyi, A, Amin, V, Anderson, D, Anderson, O, Andreou, A, Ansari, A, Appleton, S, Ardley, R, Arshad, F, Ashour, O, Asour, A, Athem, A, Athersmith, M, Ayoub, F, Azeem, H, Azhar, B, Badenoch, T, Baillie, C, Bandyopadhyay, D, Barker, J, Barker, S, Barkham, B, Baron, R, Barrie, J, Barry‐Yarrow, E, Bashir, G, Battersby, N, Bazoua, G, Behar, N, Bellam, S, Berger, C, Bhandari, S, Bhasin, S, Biggs, S, Bisset, C, Blake, L, Blencowe, N, Boam, T, Boddy, A, Boereboom, C, Bogdan, M, Bogle, R, Bohra, P, Boland, M, Bolkan, H, Borg, C, Boulton, R, Bouras, G, Boyer, M, Boyle, J, Branagan, G, Brewer, H, Briggs, C, Broadhurst, J, Brown, E, Brown, J, Brown, L, Brown, O, Burns, K, Butcher, K, Butler, M, Byrne, B, Campbell, L, Capper, C, Cartmell, M, Cash, T, Chan, S, Chandratreya, N, Chapman, J, Chapman, S, Charalabopoulos, A, Cheek, C, Chok, S, Choong, W, Chow, M, Chowdhury, J, Coe, P, Conaghan, P, Conn, G, Cook, N, Cook, T, Cooper, S, Cornish, J, Cotton, D, Cox, C, Coyne, P, Crook, R, Crozier, J, Cuffolo, G, Cunha, P, Curtis, N, Cutting, J, Da Costa, K, Silva, L, Das, B, Davenport, M, Davies, J, Davies, T, Day, A, Dayal, S, Dean, S, Demetriou, G, Dengu, F, Dennis, R, Dent, H, Dent, P, Deputy, M, Devoto, L, Di Benedetto, G, Dindyal, S, Donnelly, E, Doody, P, Douka, E, Downham, C, Dowson, H, Edent, H, Edgerton, K, Ekpete, N, El Farran, M, Elamin, O, Eljaafari, M, Elsaid, N, El‐Sharif, M, Evans, J, Evans, M, Ewe, R, Ewing, A, Exarchou, K, Fallaize, R, Faoury, M, Farag, S, Farinella, E, Faulkner, G, Ferguson, H, Fisher, O, Fletcher, J, Forouzanfar, A, Foster, A, Fox, R, Francis, N, Fretwell, V, Fung, D, Gammeri, E, Garnham, J, Geraghty, A, Gilbert, A, Gill, C, Gill, M, Gillespie, M, Giordano, P, Glasbey, J, Goh, M, Golder, A, Green, N, Gregoir, T, Grey, T, Groundwater, E, Grove, T, Growcott, S, Gunasekaran, S, Habib, H, Haddow, J, Halahakoon, V, Halkias, C, Hall, C, Hampson, A, Hancock, L, Hanna, T, Hannay, J, Harikrishnan, A, Harries, R, Harris, G, Hartley, J, Harvey, K, Hawkin, P, Hawkins, J, Healy, R, Heard, R, Heartshorne, R, Heller, S, Hendra, L, Herrod, P, Heywood, N, Hicks, G, Hobson, B, Holtham, S, Hope, C, Hopley, P, Hossain, T, Hossaini, S, Howse, F, Hubbard, T, Humphreys, A, Ikram, H, Ioannis, M, Iqbal, M, Iqbal, N, Jain, R, Jatania, J, Jenkinson, P, Jokhan, S, Jones, A, Jones, C, Jones, L, Joshi, H, Joshi, K, Joy, M, Jull, P, Kakaniaris, G, Kallam, R, Kane, E, Kang, P, Kanitkar, R, Kauser, S, Kazmi, F, Kedrzycki, M, Kelly, S, Kendall, J, Khan, M, Khan, T, King, G, Kisiel, A, Kitsis, C, Kolawole, I, Korambayil, S, Kosasih, S, Kosti, A, Kotb, A, Kouris, S, Kshatriya, K, Kumar, S, Lafaurie, G, Lal, R, Lau, A, Lazim, T, Lazzaro, A, Lee, K, Lefroy, R, Leinhardt, D, Lennon, H, Leong, K, Levy, B, Lim, E, Lim, J, Lindley, S, Liu, D, Lloyd, P, Locker, D, Lockwood, S, Lowe, C, Lund, J, Lunevicius, R, Lunt, A, Lutfi, S, Luther, A, Luwemba, S, Mahankali‐Rao, P, Mahroof, S, Mai, D, Majid, S, Malik, A, Malik, K, Mann, K, Mansour, S, Manu, N, Mapara, R, Martin, C, Martin, J, Martin, R, Mason, C, Massey, L, Mathias, J, Mathur, P, Maude, K, McArthur, D, McCain, S, McCluney, S, McFall, M, McIlroy, B, McKay, S, McKinley, N, McNair, A, McWhirter, D, Mekhail, P, Mellor, K, Merchant, J, Merker, L, Messenger, D, Miles, A, Mir, S, Mishra, A, Mistry, P, Miu, V, Moat, M, Mockford, K, Mohamed, E, Mohamed, I, Mondragon‐Pritchard, M, Moore, N, Moretti, L, Morris, H, Morrison, T, Morrison‐Jones, V, Moss, J, Moug, S, Mountford, D, Moynihan, R, Muhammad, K, Muldoon‐Smith, D, Mulholland, J, Mullan, M, Murgitroyd, E, Murugaiyan, K, Myers, A, Mykoniatis, I, Nana, G, Nash, T, Nassar, A, Newton, R, Ng, C, Ng, P, Nguyen, K, Nicholas, F, Noor, M, Nowers, J, Nugent, C, Nunn, A, Nunn, R, Obeid, N, O'Callaghan, J, O'Hara, R, Oke, O, Olivier, J, O'Neill, A, O'Neill, S, Osei‐Bordom, D, Osgood, L, Panagiotopoulos, S, Panchasara, B, Parks, R, Patel, H, Patel, P, Patel, R, Patel, S, Pawelec, K, Payne, C, Pearson, K, Perin, G, Peristerakis, I, Petronio, B, Phelan, L, Phillips, J, Pisaneschi, C, Pitt, J, Plunkett‐Reed, K, Ponchietti, L, Pouzi, A, Pouzi, M, Powell, A, Powell‐Chandler, A, Pranesh, N, Proctor, V, Pywell, S, Qureshi, A, Qureshi, N, Rahman, M, Rai, Z, Ramcharan, S, Rangarajan, K, Rashid, M, Reader, H, Rehman, A, Rehman, S, Rengifo, C, Richards, E, Richardson, N, Robinson, A, Robinson, D, Rossi, B, Rutherford, F, Sadien, I, Saghir, T, Sahnan, K, Salahia, G, Sarveswaran, J, Saunders, M, Scott, B, Scott, K, Seager, A, Seal, S, Sezen, E, Shaban, F, Shah, P, Shahmohammadi, M, Shamsiddinova, A, Shankar, S, Sharpe, A, Shatkar, V, Sheel, A, Shields, T, Shinkwin, M, Shurmer, J, Siddika, A, Siddiqui, S, Simson, R, Sinclair, P, Singh, B, Singh, S, Sivaraj, J, Skaife, P, Skelly, B, Skinner, A, Slim, N, Smart, C, Smart, N, Smith, F, Smith, I, Smith, R, Spence, G, Sreedhar, A, Steinke, J, Stevenson, L, Stewart‐Parker, E, Stott, M, Stubbs, B, Stylianides, N, Subramonia, S, Swinkin, M, Swinscoe, M, Symons, N, Tahir, W, Taj, T, Takacs, K, Tam, J, Tan, K, Tani, S, Tanner, N, Tao, D, Taylor, M, Thava, B, Thippeswamy, K, Thomas, C, Thompson, E, Thompson, R, Thompson‐Reil, C, Thorn, C, Tongo, F, Toth, G, Turnbull, A, Turnbull, J, Valero, C, Boxel, G, Varcada, M, Venn, M, Ventham, N, Venza, M, Vimalachandran, D, Virlos, I, Wade, T, Wafi, A, Waite, K, Walker, M, Walker, N, Walker, T, Walsh, U, Wardle, S, Warner, R, Watfah, J, Watson, N, Watt, J, Watts, J, Wayman, J, Weegenaar, C, West, H, West, M, Whitehurst, L, Whyler, M, Wiggans, M, Wijeyekoon, S, Williams, G, Williams, R, Williamson, A, Williamson, J, Wilson, J, Winter, A, Wolpert, L, Wong, J, Yeap, E, Yeong, T, Zaman, S, Zappa, B, and Zosimas, D

Subjects
Adult, Male, medicine.medical_specialty, National Audit of Small Bowel Obstruction Steering Group and National Audit of Small Bowel Obstruction Collaborators, Incisional hernia, lcsh:Surgery, 030230 surgery, Abdominal wall, 03 medical and health sciences, 0302 clinical medicine, Postoperative Complications, NASBO Collaborators, medicine, Humans, Hernia, Hospital Mortality, General, Emergency Treatment, Aged, Proportional Hazards Models, Aged, 80 and over, Groin, business.industry, Mortality rate, Hazard ratio, West Midlands Research Collaborative, General Medicine, Odds ratio, Original Articles, lcsh:RD1-811, Middle Aged, medicine.disease, Quality Improvement, United Kingdom, Surgery, Hernia, Abdominal, Bowel obstruction, medicine.anatomical_structure, Logistic Models, 030220 oncology & carcinogenesis, Original Article, Female, business, NASBO Steering Group, Intestinal Obstruction
Abstract

Background Abdominal wall hernia is a common surgical condition. Patients may present in an emergency with bowel obstruction, incarceration or strangulation. Small bowel obstruction (SBO) is a serious surgical condition associated with significant morbidity. The aim of this study was to describe current management and outcomes of patients with obstructed hernia in the UK as identified in the National Audit of Small Bowel Obstruction (NASBO). Methods NASBO collated data on adults treated for SBO at 131 UK hospitals between January and March 2017. Those with obstruction due to abdominal wall hernia were included in this study. Demographics, co‐morbidity, imaging, operative treatment, and in‐hospital outcomes were recorded. Modelling for factors associated with mortality and complications was undertaken using Cox proportional hazards and multivariable regression modelling. Results NASBO included 2341 patients, of whom 415 (17·7 per cent) had SBO due to hernia. Surgery was performed in 312 (75·2 per cent) of the 415 patients; small bowel resection was required in 198 (63·5 per cent) of these operations. Non‐operative management was reported in 35 (54 per cent) of 65 patients with a parastomal hernia and in 34 (32·1 per cent) of 106 patients with an incisional hernia. The in‐hospital mortality rate was 9·4 per cent (39 of 415), and was highest in patients with a groin hernia (11·1 per cent, 17 of 153). Complications were common, including lower respiratory tract infection in 16·3 per cent of patients with a groin hernia. Increased age was associated with an increased risk of death (hazard ratio 1·05, 95 per cent c.i. 1·01 to 1·10; P = 0·009) and complications (odds ratio 1·05, 95 per cent c.i. 1·02 to 1·09; P = 0·001). Conclusion NASBO has highlighted poor outcomes for patients with SBO due to hernia, highlighting the need for quality improvement initiatives in this group., This study shows that small bowel obstruction due to abdominal wall hernia is common, typically involves a co‐morbid group of patients and has poor outcomes, including high mortality rates. High mortality from this problem

Published
2020

23. Permeability Measures Predict Hemorrhagic Transformation after Ischemic Stroke

Author

Bivard, A, Kleinig, T, Churilov, L, Levi, C, Lin, L, Cheng, X, Chen, C, Aviv, R, Choi, PMC, Spratt, NJ, Butcher, K, Dong, Q, Parsons, M, Bivard, A, Kleinig, T, Churilov, L, Levi, C, Lin, L, Cheng, X, Chen, C, Aviv, R, Choi, PMC, Spratt, NJ, Butcher, K, Dong, Q, and Parsons, M

Abstract

Objective: We sought to examine the diagnostic utility of existing predictors of any hemorrhagic transformation (HT) and compare them with new perfusion imaging permeability measures in ischemic stroke patients receiving alteplase only. Methods: A pixel-based analysis of pretreatment CT perfusion (CTP) was undertaken to define the optimal CTP permeability thresholds to predict the likelihood of HT. We then compared previously proposed predictors of HT using regression analyses and receiver operating characteristic curve analysis to produce an area under the curve (AUC). We compared AUCs using χ2 analysis. Results: From 5 centers, 1,407 patients were included in this study; of these, 282 had HT. The cohort was split into a derivation cohort (1,025, 70% patients) and a validation cohort (382 patients or 30%). The extraction fraction (E) permeability map at a threshold of 30% relative to contralateral had the highest AUC at predicting any HT (derivation AUC 0.85, 95% confidence interval [CI], 0.79–0.91; validation AUC 0.84, 95% CI 0.77–0.91). The AUC improved when permeability was assessed within the acute perfusion lesion for the E maps at a threshold of 30% (derivation AUC 0.91, 95% CI 0.86–0.95; validation AUC 0.89, 95% CI 0.86–0.95). Previously proposed associations with HT and parenchymal hematoma showed lower AUC values than the permeability measure. Interpretation: In this large multicenter study, we have validated a highly accurate measure of HT prediction. This measure might be useful in clinical practice to predict hemorrhagic transformation in ischemic stroke patients before receiving alteplase alone. ANN NEUROL 2020;88:466–476.

Published
2020

24. Reduced Impact of Endovascular Thrombectomy on Disability in Real-World Practice, Relative to Randomized Controlled Trial Evidence in Australia

Author

Gao, L, Tan, E, Moodie, M, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Chen, C, Lin, L, Choi, P, Bivard, A, Gao, L, Tan, E, Moodie, M, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Chen, C, Lin, L, Choi, P, and Bivard, A

Abstract

Background and Aims: Disability-adjusted life years (DALYs) are an important measure of the global burden of disease that informs patient outcomes and policy decision-making. Our study aimed to compare the DALYs saved by endovascular thrombectomy (EVT) in the Australasian-based EXTEND-IA trial vs. clinical registry data from EVT in Australian routine clinical practice. Methods: The 3-month modified Rankin scale (mRS) outcome and treatment status of consecutively enrolled Australian patients with large vessel occlusion (LVO) stroke were taken from the International Stroke Perfusion Imaging Registry (INSPIRE). DALYs were calculated as the summation of years of life lost (YLL) due to premature death and years lived with a disability (YLD). A generalized linear model (GLM) with gamma family and log link was used to compare the difference in DALYs for patients receiving/not receiving EVT while controlling for key covariates. Ordered logit regression model was utilized to compare the difference in functional outcome at 3 months between the treatment groups. Cox regression analysis was undertaken to compare the difference in survival over an 18-year time horizon. Estimated long-term DALYs saved based on the EXTEND-IA randomized controlled trial (RCT) results were used as the comparator. Results: INSPIRE patients who received EVT treatment only achieved nominally better functional outcomes than the non-EVT group (p = 0.181) at 3 months. There was no significant survival gain from EVT over the first 3 months of stroke in both INSPIRE and EXTEND-IA patients. However, measured against no EVT in the long-term, EVT in INSPIRE was associated with no significant survival gain [hazard ratio (HR): 0.92, 95% confidence interval (CI): 0.78–1.08, p = 0.287] compared with the survival benefit extrapolated from the EXTEND-IA trial (HR: 0.42, 95% CI: 0.22–0.82, p = 0.01]. Offering EVT to patients with LVO stroke was also associated with fewer DALYs lost (11.04, 95% CI: 10.45–11.62) than t

Published
2020

25. Successful dabigatran reversal after subdural hemorrhage using idarucizumab in a mobile stroke unit: A case report

Author

Thirunavukkarasu, S, Kalashyan, H, Jickling, G, Jeerakathil, TJ, Jayaprakash, HK, Buck, BH, Shuaib, A, Butcher, K, Thirunavukkarasu, S, Kalashyan, H, Jickling, G, Jeerakathil, TJ, Jayaprakash, HK, Buck, BH, Shuaib, A, and Butcher, K

Abstract

RATIONALE: Idarucizumab is a specific reversal agent for patients with bleeding related to the anticoagulant dabigatran. There are no prior descriptions of Idarucizumab administration in the prehospital setting for intracranial hemorrhage. PATIENT CONCERNS: An 82-year-old woman treated with dabigatran for atrial fibrillation developed acute focal weakness. This led to activation of emergency medical services and assessment in the mobile stroke unit (MSU). DIAGNOSIS: Computed tomography of the brain performed in the MSU revealed an acute subdural hematoma. INTERVENTIONS: The patient was treated with Idarucizumab in the MSU. OUTCOMES: The subdural hematoma was treated with a burr hole evacuation and the patient was discharged to a rehabilitation facility without residual focal neurological deficits. LESSONS: Idarucizumab can be used safely and effectively to treat dabigatran-associated intracranial hemorrhage in the prehospital setting.

Published
2020

26. Reduced Impact of Endovascular Thrombectomy on Disability in Real-World Practice, Relative to Randomized Controlled Trial Evidence in Australia

Author

Gao, Lan, Tan, Elise, Moodie, Marjory, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Chen, C, Lin, L, Choi, P, Bivard, A, Gao, Lan, Tan, Elise, Moodie, Marjory, Parsons, M, Spratt, NJ, Levi, C, Butcher, K, Kleinig, T, Yan, B, Chen, C, Lin, L, Choi, P, and Bivard, A

Abstract

Background and Aims: Disability-adjusted life years (DALYs) are an important measure of the global burden of disease that informs patient outcomes and policy decision-making. Our study aimed to compare the DALYs saved by endovascular thrombectomy (EVT) in the Australasian-based EXTEND-IA trial vs. clinical registry data from EVT in Australian routine clinical practice.Methods: The 3-month modified Rankin scale (mRS) outcome and treatment status of consecutively enrolled Australian patients with large vessel occlusion (LVO) stroke were taken from the International Stroke Perfusion Imaging Registry (INSPIRE). DALYs were calculated as the summation of years of life lost (YLL) due to premature death and years lived with a disability (YLD). A generalized linear model (GLM) with gamma family and log link was used to compare the difference in DALYs for patients receiving/not receiving EVT while controlling for key covariates. Ordered logit regression model was utilized to compare the difference in functional outcome at 3 months between the treatment groups. Cox regression analysis was undertaken to compare the difference in survival over an 18-year time horizon. Estimated long-term DALYs saved based on the EXTEND-IA randomized controlled trial (RCT) results were used as the comparator.Results: INSPIRE patients who received EVT treatment only achieved nominally better functional outcomes than the non-EVT group (p = 0.181) at 3 months. There was no significant survival gain from EVT over the first 3 months of stroke in both INSPIRE and EXTEND-IA patients. However, measured against no EVT in the long-term, EVT in INSPIRE was associated with no significant survival gain [hazard ratio (HR): 0.92, 95% confidence interval (CI): 0.78–1.08, p = 0.287] compared with the survival benefit extrapolated from the EXTEND-IA trial (HR: 0.42, 95% CI: 0.22–0.82, p = 0.01]. Offering EVT to patients with LVO stroke was also associated with fewer DALYs lost (11.04, 95% CI: 10.45&nda

Published
2020

28. DC voltage fields generated by RF plasmas and their influence on film growth morphology through static attraction to metal wetting layers: Beyond ion bombardment effects.

Author

Butcher, K. S. A., Terziyska, P. T., Gergova, R., Georgiev, V., Georgieva, D., Binsted, P. W., and Skerget, S.

Subjects
*PLASMA dynamics, *RADIO frequency, *SURFACE morphology, *ION bombardment, *DIRECT currents
Abstract

It is shown that attractive electrostatic interactions between regions of positive charge in RF plasmas and the negative charge of metal wetting layers, present during compound semiconductor film growth, can have a greater influence than substrate temperature on film morphology. Using GaN and InN film growth as examples, the DC field component of a remote RF plasma is demonstrated to electrostatically affect metal wetting layers to the point of actually determining the mode of film growth. Examples of enhanced self-seeded nanopillar growth are provided in the case where the substrate is directly exposed to the DC field generated by the plasma. In another case, we show that electrostatic shielding of the DC field from the substrate can result in the growth of Ga-face GaN layers from gallium metal wetting layers at 490 °C with root-mean-square roughness values as low as 0.6 nm. This study has been carried out using a migration enhanced deposition technique with pulsed delivery of the metal precursor allowing the identification of metal wetting layers versus metal droplets as a function of the quantity of metal source delivered per cycle. It is also shown that electrostatic interactions with the plasma can affect metal rich growth limits, causing metal droplet formation for lower metal flux than would otherwise occur. Accordingly, film growth rates can be increased when shielding the substrate from the positive charge region of the plasma. For the example shown here, growth rates were more than doubled using a shielding grid. [ABSTRACT FROM AUTHOR]

Published
2017
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43. National prospective cohort study of the burden of acute small bowel obstruction

Author

Lee, M. J., Sayers, A. E., Drake, T. M., Marriott, P. J., Anderson, I. D., Bach, S. P., Bradburn, M., Hind, D., Verjee, A., Fearnhead, N. S., Abercrombie, John, Acheson, Austin, Alderson, Derek, Anderson, Iain, Davies, Michael, Hamady, Zaed, Hollyman, Marianne, Hare, Sarah, Lee, Ellen, Northover, John, Lewis, Christopher, McFall, Malcolm, Murugananthan, Aravinth, Murray, David, Singh, Pritam, Tierney, Gillian, Walsh, Ciaran, Wild, Jonathan, Wilson, Timothy, Abbott, S, Abdulaal, Y, Afshar, S, Ah‐Chuen, J, Ahmed, T, Akhtar, M, Akram, F, Aldred, E, Ali, A, Aly, M, Amajuoyi, A, Amin, V, Anderson, D, Anderson, O, Andreou, A, Ansari, A, Appleton, S, Ardley, R, Arshad, F, Ashour, O, Asour, A, Athem, A, Athersmith, M, Ayoub, F, Azeem, H, Azhar, B, Badenoch, T, Baillie, C, Bandyopadhyay, D, Barker, J, Barker, S, Barkham, B, Baron, R, Barrie, J, Barry‐Yarrow, E, Bashir, G, Battersby, N, Bazoua, G, Behar, N, Bellam, S, Berger, C, Bhandari, S, Bhasin, S, Biggs, S, Bisset, C, Blake, L, Blencowe, N, Boam, T, Boddy, A, Boereboom, C, Bogdan, M, Bogle, R, Bohra, P, Boland, M, Bolkan, H, Borg, C, Boulton, R, Bouras, G, Boyer, M, Boyle, J, Branagan, G, Brewer, H, Briggs, C, Broadhurst, J, Brown, E, Brown, J, Brown, L, Brown, O, Burns, K, Butcher, K, Butler, M, Byrne, B, Campbell, L, Capper, C, Cartmell, M, Cash, T, Chan, S, Chandratreya, N, Chapman, J, Chapman, S, Charalabopoulos, A, Cheek, C, Chok, S, Choong, W, Chow, M, Chowdhury, J, Coe, P, Conaghan, P, Conn, G, Cook, N, Cook, T, Cooper, S, Cornish, J, Cotton, D, Cox, C, Coyne, P, Crook, R, Crozier, J, Cuffolo, G, Cunha, P, Curtis, N, Cutting, J, Da Costa, K, Silva, L, Das, B, Davenport, M, Davies, J, Davies, T, Day, A, Dayal, S, Dean, S, Demetriou, G, Dengu, F, Dennis, R, Dent, H, Dent, P, Deputy, M, Devoto, L, Di Benedetto, G, Dindyal, S, Donnelly, E, Doody, P, Douka, E, Downham, C, Dowson, H, Edent, H, Edgerton, K, Ekpete, N, El Farran, M, Elamin, O, Eljaafari, M, Elsaid, N, El‐Sharif, M, Evans, J, Evans, M, Ewe, R, Ewing, A, Exarchou, K, Fallaize, R, Faoury, M, Farag, S, Farinella, E, Faulkner, G, Ferguson, H, Fisher, O, Fletcher, J, Forouzanfar, A, Foster, A, Fox, R, Francis, N, Fretwell, V, Fung, D, Gammeri, E, Garnham, J, Geraghty, A, Gilbert, A, Gill, C, Gill, M, Gillespie, M, Giordano, P, Glasbey, J, Goh, M, Golder, A, Green, N, Gregoir, T, Grey, T, Groundwater, E, Grove, T, Growcott, S, Gunasekaran, S, Habib, H, Haddow, J, Halahakoon, V, Halkias, C, Hall, C, Hampson, A, Hancock, L, Hanna, T, Hannay, J, Harikrishnan, A, Harries, R, Harris, G, Hartley, J, Harvey, K, Hawkin, P, Hawkins, J, Healy, R, Heard, R, Heartshorne, R, Heller, S, Hendra, L, Herrod, P, Heywood, N, Hicks, G, Hobson, B, Holtham, S, Hope, C, Hopley, P, Hossain, T, Hossaini, S, Howse, F, Hubbard, T, Humphreys, A, Ikram, H, Ioannis, M, Iqbal, M, Iqbal, N, Jain, R, Jatania, J, Jenkinson, P, Jokhan, S, Jones, A, Jones, C, Jones, L, Joshi, H, Joshi, K, Joy, M, Jull, P, Kakaniaris, G, Kallam, R, Kane, E, Kang, P, Kanitkar, R, Kauser, S, Kazmi, F, Kedrzycki, M, Kelly, S, Kendall, J, Khan, M, Khan, T, King, G, Kisiel, A, Kitsis, C, Kolawole, I, Korambayil, S, Kosasih, S, Kosti, A, Kotb, A, Kouris, S, Kshatriya, K, Kumar, S, Lafaurie, G, Lal, R, Lau, A, Lazim, T, Lazzaro, A, Lee, K, Lefroy, R, Leinhardt, D, Lennon, H, Leong, K, Levy, B, Lim, E, Lim, J, Lindley, S, Liu, D, Lloyd, P, Locker, D, Lockwood, S, Lowe, C, Lund, J, Lunevicius, R, Lunt, A, Lutfi, S, Luther, A, Luwemba, S, Mahankali‐Rao, P, Mahroof, S, Mai, D, Majid, S, Malik, A, Malik, K, Mann, K, Mansour, S, Manu, N, Mapara, R, Martin, C, Martin, J, Martin, R, Mason, C, Massey, L, Mathias, J, Mathur, P, Maude, K, McArthur, D, McCain, S, McCluney, S, McIlroy, B, McKay, S, McKinley, N, McNair, A, McWhirter, D, Mekhail, P, Mellor, K, Merchant, J, Merker, L, Messenger, D, Miles, A, Mir, S, Mishra, A, Mistry, P, Miu, V, Moat, M, Mockford, K, Mohamed, E, Mohamed, I, Mondragon‐Pritchard, M, Moore, N, Moretti, L, Morris, H, Morrison, T, Morrison‐Jones, V, Moss, J, Moug, S, Mountford, D, Moynihan, R, Muhammad, K, Muldoon‐Smith, D, Mulholland, J, Mullan, M, Murgitroyd, E, Murugaiyan, K, Myers, A, Mykoniatis, I, Nana, G, Nash, T, Nassar, A, Newton, R, Ng, C, Ng, P, Nguyen, K, Nicholas, F, Noor, M, Nowers, J, Nugent, C, Nunn, A, Nunn, R, Obeid, N, O'Callaghan, J, O'Hara, R, Oke, O, Olivier, J, O'Neill, A, O'Neill, S, Osei‐Bordom, D, Osgood, L, Panagiotopoulos, S, Panchasara, B, Parks, R, Patel, H, Patel, P, Patel, R, Patel, S, Pawelec, K, Payne, C, Pearson, K, Perin, G, Peristerakis, I, Petronio, B, Phelan, L, Phillips, J, Pisaneschi, C, Pitt, J, Plunkett‐Reed, K, Ponchietti, L, Pouzi, A, Pouzi, M, Powell, A, Powell‐Chandler, A, Pranesh, N, Proctor, V, Pywell, S, Qureshi, A, Qureshi, N, Rahman, M, Rai, Z, Ramcharan, S, Rangarajan, K, Rashid, M, Reader, H, Rehman, A, Rehman, S, Rengifo, C, Richards, E, Richardson, N, Robinson, A, Robinson, D, Rossi, B, Rutherford, F, Sadien, I, Saghir, T, Sahnan, K, Salahia, G, Sarveswaran, J, Saunders, M, Scott, B, Scott, K, Seager, A, Seal, S, Sezen, E, Shaban, F, Shah, P, Shahmohammadi, M, Shamsiddinova, A, Shankar, S, Sharpe, A, Shatkar, V, Sheel, A, Shields, T, Shinkwin, M, Shurmer, J, Siddika, A, Siddiqui, S, Simson, R, Sinclair, P, Singh, B, Singh, S, Sivaraj, J, Skaife, P, Skelly, B, Skinner, A, Slim, N, Smart, C, Smart, N, Smith, F, Smith, I, Smith, R, Spence, G, Sreedhar, A, Steinke, J, Stevenson, L, Stewart‐Parker, E, Stott, M, Stubbs, B, Stylianides, N, Subramonia, S, Swinkin, M, Swinscoe, M, Symons, N, Tahir, W, Taj, T, Takacs, K, Tam, J, Tan, K, Tani, S, Tanner, N, Tao, D, Taylor, M, Thava, B, Thippeswamy, K, Thomas, C, Thompson, E, Thompson, R, Thompson‐Reil, C, Thorn, C, Tongo, F, Toth, G, Turnbull, A, Turnbull, J, Valero, C, Boxel, G, Varcada, M, Venn, M, Ventham, N, Venza, M, Vimalachandran, D, Virlos, I, Wade, T, Wafi, A, Waite, K, Walker, M, Walker, N, Walker, T, Walsh, U, Wardle, S, Warner, R, Watfah, J, Watson, N, Watt, J, Watts, J, Wayman, J, Weegenaar, C, West, H, West, M, Whitehurst, L, Whyler, M, Wiggans, M, Wijeyekoon, S, Williams, G, Williams, R, Williamson, A, Williamson, J, Wilson, J, Winter, A, Wolpert, L, Wong, J, Yeap, E, Yeong, T, Zaman, S, Zappa, B, Zosimas, D, Moug S Mondragon‐Pritchard, M, Rehan, S, and van Boxel, G

Abstract

Background: \ud Small bowel obstruction is a common surgical emergency, and is associated with high levels of morbidity and mortality across the world. The literature provides little information on the conservatively managed group. The aim of this study was to describe the burden of small bowel obstruction in the UK.\ud \ud Methods: \ud This prospective cohort study was conducted in 131 acute hospitals in the UK between January and April 2017, delivered by trainee research collaboratives. Adult patients with a diagnosis of mechanical small bowel obstruction were included. The primary outcome was in‐hospital mortality. Secondary outcomes included complications, unplanned intensive care admission and readmission within 30 days of discharge. Practice measures, including use of radiological investigations, water soluble contrast, operative and nutritional interventions, were collected.\ud \ud Results: \ud Of 2341 patients identified, 693 (29·6 per cent) underwent immediate surgery (within 24 h of admission), 500 (21·4 per cent) had delayed surgery after initial conservative management, and 1148 (49·0 per cent) were managed non‐operatively. The mortality rate was 6·6 per cent (6·4 per cent for non‐operative management, 6·8 per cent for immediate surgery, 6·8 per cent for delayed surgery; P = 0·911). The major complication rate was 14·4 per cent overall, affecting 19·0 per cent in the immediate surgery, 23·6 per cent in the delayed surgery and 7·7 per cent in the non‐operative management groups (P < 0·001). Cox regression found hernia or malignant aetiology and malnutrition to be associated with higher rates of death. Malignant aetiology, operative intervention, acute kidney injury and malnutrition were associated with increased risk of major complication.\ud \ud Conclusion: \ud Small bowel obstruction represents a significant healthcare burden. Patient‐level factors such as timing of surgery, acute kidney injury and nutritional status are factors that might be modified to improve outcomes.

Published
2019

44. Community exercise is feasible for neuromuscular diseases and can improve aerobic capacity

Author

Wallace, A, Pietrusz, A, Dewar, E, Dudziec, M, Jones, K, Hennis, P, Sterr, A, Baio, G, Machado, P, Laurá, M, Skorupinska, I, Skorupinska, M, Butcher, K, Trenell, M, Reilly, MM, Hanna, M, and Ramdharry, GM

Subjects
education, alliedhealth, human activities
Abstract

Objective: The aim of this phase 2 trial was to ascertain the feasibility and effect of community based aerobic exercise training for people with two of the more common neuromuscular diseases: Charcot-Marie-Tooth disease type 1A (CMT) and Inclusion Body Myositis (IBM). \ud \ud Methods: A randomised single blinded cross over trial design was used to compare a 12-week aerobic training programme using recombinant exercise bicycles compared to a control period. The training occurred three times per week in community gyms local to the participants. Support was available from trained gym staff and a research physiotherapist. The two disease groups were analysed separately. The primary outcome measure was peak oxygen uptake (VO2 peak) during a maximal exercise test, with secondary measures of muscle strength, function and patient reported measures. \ud \ud Results: Data from 23 people with CMT and 17 people with IBM was included in the analysis. Both disease groups had high levels of participation and demonstrated improvements in VO2 peak, with a moderate effect size in the CMT participants (Cohen’s d = 0.53) and a strong effect size in the IBM group (Cohen’s d = 1.72). No major changes were observed in the secondary outcome measures. Qualitative interviews revealed that participants valued the support of gym instructors and the research physiotherapists in overcoming challenges to participation. \ud \ud Conclusion: Twelve weeks of aerobic training in community gyms was feasible, safe and improved aerobic capacity in people with CMT and IBM. \ud \ud Classification of Evidence: This study provides Class II evidence that for patients with CMT type 1A and IBM, an aerobic training program increases aerobic capacity.

Published
2019

47. Who says 'no' to participating in stroke clinical trials and why: An observational study from the Vancouver Stroke Program

Author

O'Neill, ZR, Deptuck, HM, Quong, L, Maclean, G, Villaluna, K, King-Azote, P, Sharma, M, Butcher, K, Hart, RG, Field, TS, O'Neill, ZR, Deptuck, HM, Quong, L, Maclean, G, Villaluna, K, King-Azote, P, Sharma, M, Butcher, K, Hart, RG, and Field, TS

Abstract

Background: Successful stroke trials require adequate recruitment. In this observational study, we assessed reasons for refusal to provide informed consent in eligible patients approached for clinical trial participation at the Vancouver Stroke Program. Methods: We assessed screening logs from four trials that were actively recruiting at our center: three randomized trials, two of which investigated different antithrombotic strategies for secondary prevention (NAVIGATE-ESUS, NCT02313909 12/2014; DATAS-II, NCT02295826 11/2014) and one that investigated surgery plus medical management versus medical management alone for primary prevention (CREST-2, NCT02089217 03/2014). The fourth study was observational and non-randomized; all participants received an external monitoring device (PROPHECY, NCT03712865 10/2018). Screening logs from June 2015 to April 2017 were reviewed retrospectively. Subsequently, we used a prospective structured case report form for screening (May 2017-March 2018). We assessed and compared refusal rates between trials, demographics of those refusing consent, and their reasons for doing so. We used descriptive statistics, chi-square and Fisher's exact tests as appropriate for non-parametric data, and t-tests for parametric data. We examined likelihood of refusal by sex using multivariable logistic regression models including age and trial intervention as co-variables. Results: A total of 235 patients (43% women) were approached for consent. More patients refused the surgical (59%) and antithrombotic trials (53%) compared with the non-randomized external monitoring device study (13%) (p < 0.001). Surgical trial refusals were primarily due to a desire for certainty in receiving a particular intervention (39%), with the majority of those patients wanting surgery. Refusals for the antithrombotic trials were mainly due to concerns with the potential side effects of the study drug (41%); refusals in the device trial were mainly due to disinterest (46%). Wo

Published
2019

48. Aggressive blood pressure reduction is not associated with decreased perfusion in leukoaraiosis regions in acute intracerebral hemorrhage patients

Author

Kate, M, Gioia, L, Jeerakathil, T, Hill, MD, Gould, B, McCourt, R, Dowlatshahi, D, Coutts, S, Kosior, J, Demchuk, A, Buck, B, Butcher, K, Kate, M, Gioia, L, Jeerakathil, T, Hill, MD, Gould, B, McCourt, R, Dowlatshahi, D, Coutts, S, Kosior, J, Demchuk, A, Buck, B, and Butcher, K

Abstract

Leukoaraiosis regions may be more vulnerable to decreases in cerebral perfusion. We aimed to assess perfusion in leukoaraiosis regions in acute intracerebral hemorrhage (ICH) patients. We tested the hypothesis that aggressive acute BP reduction in ICH patients is associated with hypoperfusion in areas of leukoaraiosis. In the ICH Acutely Decreasing Arterial Pressure Trial (ICH ADAPT), patients with ICH <24 hours duration were randomized to two systolic BP (SBP) target groups (<150 mmHg vs. <180 mmHg). Computed tomography perfusion (CTP) imaging was performed 2h post-randomization. Leukoaraiosis tissue volumes were planimetrically measured using semi-automated threshold techniques on the acute non-contrast CT. CTP source leukoaraiosis region-of-interest object maps were co-registered with CTP post-processed maps to assess cerebral perfusion in these areas. Seventy-one patients were included with a mean age of 69±11.4 years, 52 of whom had leukoaraiosis. The mean relative Tmax (rTmax) of leukoaraiotic tissue (2.3±2s) was prolonged compared to that of normal appearing white matter in patients without leukoaraiosis (1.1 ±1.2s, p = 0.04). In the 52 patients with leukoaraiosis, SBP in the aggressive treatment group (145±20.4 mmHg, n = 27) was significantly lower than that in the conservative group (159.9±13.1 mmHg, n = 25, p = 0.001) at the time of CTP. Despite this SBP difference, mean leukoaraiosis rTmax was similar in the two treatment groups (2.6±2.3 vs. 1.8±1.6 seconds, p = 0.3). Cerebral perfusion in tissue affected by leukoaraiosis is hypoperfused in acute ICH patients. Aggressive BP reduction does not appear to acutely aggravate cerebral hypoperfusion.

Published
2019

49. The blood pressure paradox in acute ischemic stroke

Author

Hong, L, Cheng, X, Lin, L, Bivard, A, Ling, Y, Butcher, K, Dong, Q, Parsons, M, Spratt, N, Levi, C, Choi, PMC, Kleining, T, O'Brien, B, Lou, M, Hong, L, Cheng, X, Lin, L, Bivard, A, Ling, Y, Butcher, K, Dong, Q, Parsons, M, Spratt, N, Levi, C, Choi, PMC, Kleining, T, O'Brien, B, and Lou, M

Abstract

OBJECTIVE: To explore the association of poststroke baseline blood pressure with cerebral collateral flow and functional outcome in acute ischemic patients with large vessel occlusion/stenosis. METHODS: Patients identified with large vessel occlusion/stenosis with baseline multimodal computed tomography, follow-up imaging, and complete clinical profiles were included. A 90-day modified Rankin Scale of 0-1 was defined as an excellent functional outcome. Cerebral collateral flow was quantified by the volume ratio of tissue within the delay time >3 seconds perfusion lesion with severely delayed contrast transit (delay time >3 seconds/delay time >6 seconds). RESULTS: There were 306 patients included in this study. With every increase of 10 mmHg in baseline systolic blood pressure, the odds of achieving an excellent functional outcome decreased by 12% in multivariate analysis (odds ratio = 0.88, p = 0.048). Conversely, increased baseline blood pressure was associated with better collateral flow. In subgroup analysis of patients with major reperfusion, higher blood pressure was associated with decreased infarct growth and a better clinical outcome, and vice versa in patients without reperfusion. INTERPRETATION: Higher baseline blood pressure in acute ischemic stroke patients with large vessel occlusion/stenosis was associated with better collateral flow. However, for patients without reperfusion, higher baseline blood pressure was associated with increased infarct growth, leading to an unfavorable clinical outcome. The relationship between blood pressure and outcomes is highly dependent on reperfusion, and active blood pressure-lowering treatment may be inappropriate in acute ischemic stroke patients prior to reperfusion treatment. ANN NEUROL 2019;85:331-339.

Published
2019

50. Glucose Modifies the Effect of Endovascular Thrombectomy in Patients With Acute Stroke A Pooled-Data Meta-Analysis

Author

Chamorro, A., Brown, S., Amaro, S., Hill, M.D., Muir, K.W., Dippel, D.W.J., van Zwam, W., Butcher, K., Ford, G.A., den Hertog, H.M., Mitchell, P.J., Demchuk, A.M., Majoie, C.B.L.M., Bracard, S., Sibon, I., Jadhav, A.P., Lara-Rodriguez, B., van der Lugt, A., Osei, E., Renu, A., Richard, S., Rodriguez-Luna, D., Donnan, G.A., Dixit, A., Almekhlafi, M., Deltour, S., Epstein, J., Guillon, B., Bakchine, S., Gomis, M., Rochemont, R.D., Lopes, D., Reddy, V., Rudel, G., Roos, Y.B.W.E.M., Bonafe, A., Diener, H.C., Berkhemer, O.A., Cloud, G.C., Davis, S.M., van Oostenbrugge, R., Guillemin, F., Goyal, M., Campbell, B.C.V., Menon, B.K., HERMES Collaboration, Chamorro, A., Brown, S., Amaro, S., Hill, M.D., Muir, K.W., Dippel, D.W.J., van Zwam, W., Butcher, K., Ford, G.A., den Hertog, H.M., Mitchell, P.J., Demchuk, A.M., Majoie, C.B.L.M., Bracard, S., Sibon, I., Jadhav, A.P., Lara-Rodriguez, B., van der Lugt, A., Osei, E., Renu, A., Richard, S., Rodriguez-Luna, D., Donnan, G.A., Dixit, A., Almekhlafi, M., Deltour, S., Epstein, J., Guillon, B., Bakchine, S., Gomis, M., Rochemont, R.D., Lopes, D., Reddy, V., Rudel, G., Roos, Y.B.W.E.M., Bonafe, A., Diener, H.C., Berkhemer, O.A., Cloud, G.C., Davis, S.M., van Oostenbrugge, R., Guillemin, F., Goyal, M., Campbell, B.C.V., Menon, B.K., and HERMES Collaboration

Abstract

Background and Purpose-Hyperglycemia is a negative prognostic factor after acute ischemic stroke but is not known whether glucose is associated with the effects of endovascular thrombectomy (EVT) in patients with large-vessel stroke. In a pooled-data meta-analysis, we analyzed whether serum glucose is a treatment modifier of the efficacy of EVT in acute stroke.Methods-Seven randomized trials compared EVT with standard care between 2010 and 2017 (HERMES Collaboration [highly effective reperfusion using multiple endovascular devices]). One thousand seven hundred and sixty-four patients with large-vessel stroke were allocated to EVT (n=871) or standard care (n=893). Measurements included blood glucose on admission and functional outcome (modified Rankin Scale range, 0-6; lower scores indicating less disability) at 3 months. The primary analysis evaluated whether glucose modified the effect of EVT over standard care on functional outcome, using ordinal logistic regression to test the interaction between treatment and glucose level.Results-Median (interquartile range) serum glucose on admission was 120 (104-140) mg/dL (6.6 mmol/L [5.7-7.7] mmol/L). EVT was better than standard care in the overall pooled-data analysis adjusted common odds ratio (acOR), 2.00 (95% CI, 1.69-2.38); however, lower glucose levels were associated with greater effects of EVT over standard care. The interaction was nonlinear such that significant interactions were found in subgroups of patients split at glucose < or >90 mg/dL (5.0 mmol/L; P=0.019 for interaction; acOR, 3.81; 95% CI, 1.73-8.41 for patients < 90 mg/dL versus 1.83; 95% CI, 1.53-2.19 for patients >90 mg/dL), and glucose < or > 100 mg/dL (5.5 mmol/L; P=0.004 for interaction; acOR, 3.17; 95% CI, 2.04-4.93 versus acOR, 1.72; 95% CI, 1.42-2.08) but not between subgroups above these levels of glucose.Conclusions-EVT improved stroke outcomes compared with standard treatment regardless of glucose levels, but the treatment e

Published
2019

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