Your search keyword '"Shokunbi T"' showing total 14 results

1. Understanding the neuroprotective effect of tranexamic acid : an exploratory analysis of the CRASH-3 randomised trial

Author

Brenner, A., Belli, A., Chaudhri, R., Coats, T., Frimley, L., Jamaluddin, S.F., Jooma, R., Mansukhani, R., Sandercock, P., Shakur-Still, H., Shokunbi, T., and Roberts, I.

Abstract

Background\ud \ud The CRASH-3 trial hypothesised that timely tranexamic acid (TXA) treatment might reduce deaths from intracranial bleeding after traumatic brain injury (TBI). To explore the mechanism of action of TXA in TBI, we examined the timing of its effect on death.\ud \ud \ud \ud Methods\ud \ud The CRASH-3 trial randomised 9202 patients within 3 h of injury with a GCS score ≤ 12 or intracranial bleeding on CT scan and no significant extracranial bleeding to receive TXA or placebo. We conducted an exploratory analysis of the effects of TXA on all-cause mortality within 24 h of injury and within 28 days, excluding patients with a GCS score of 3 or bilateral unreactive pupils, stratified by severity and country income. We pool data from the CRASH-2 and CRASH-3 trials in a one-step fixed effects individual patient data meta-analysis.\ud \ud \ud \ud Results\ud \ud There were 7637 patients for analysis after excluding patients with a GCS score of 3 or bilateral unreactive pupils. Of 1112 deaths, 23.3% were within 24 h of injury (early deaths). The risk of early death was reduced with TXA (112 (2.9%) TXA group vs 147 (3.9%) placebo group; risk ratio [RR] RR 0.74, 95% CI 0.58–0.94). There was no evidence of heterogeneity by severity (p = 0.64) or country income (p = 0.68). The risk of death beyond 24 h of injury was similar in the TXA and placebo groups (432 (11.5%) TXA group vs 421 (11.7%) placebo group; RR 0.98, 95% CI 0.69–1.12). The risk of death at 28 days was 14.0% in the TXA group versus 15.1% in the placebo group (544 vs 568 events; RR 0.93, 95% CI 0.83–1.03). When the CRASH-2 and CRASH-3 trial data were pooled, TXA reduced early death (RR 0.78, 95% CI 0.70–0.87) and death within 28 days (RR 0.88, 95% CI 0.82–0.94).\ud \ud \ud \ud Conclusions\ud \ud Tranexamic acid reduces early deaths in non-moribund TBI patients regardless of TBI severity or country income. The effect of tranexamic acid in patients with isolated TBI is similar to that in polytrauma. Treatment is safe and even severely injured patients appear to benefit when treated soon after injury.

Published

2020

2. Astrocytic responses in the striatum and corpus callosum of the brain of adult rats with focal ishaemia

Author

Femi-Akinlosotu, O., primary, Olopade, F., additional, Adekanmbi, A., additional, Oladeji, O., additional, and Shokunbi, T., additional

Published

2019

3. A qualitative and quantitative assessment of the visual cortex in kaolin-induced hydrocephalic rats

Author

Adekanmbi, A., primary, Femi-Akinlosotu, O., additional, Olopade, F., additional, Akpoke, O., additional, and Shokunbi, T., additional

Published

2019

4. Filopodia and growth cones in the vertically migrating granule cells of the postnatal mouse cerebellum

Author

Ono, K., Shokunbi, T., Nagata, Isao, Tokunaga, Akira, Yasui, Yukihiko, and Nakatsuji, Norio

Published

1997

5. Occipital encephalocoeles in 57 Nigerian children: a retrospective analysis

Author

Shokunbi, T., Adeloye, A., and Olumide, A.

Published

1990

6. ATYPICAL IMAGING CHARACTERISTIC OF OLIGODENDROGLIOMA

Author

Baduku Ts and Shokunbi T

Subjects

Pathology, medicine.medical_specialty, business.industry, education, Medicine, Oligodendroglioma, business, medicine.disease, Industrial and Manufacturing Engineering

Abstract

Background: There has been the dearth of doctors choosing the postgraduate specialties that were outside the core clinical disciplines. This would no longer impact negatively in the distribution of Doctors in the less sought out specialties in terms of service delivery and medical education. Objectives: The present study was done to determine the career preferences of final year medical students specifically as regards to their choice of chemical pathology and factors influencing such choice. Methods: The study was a Descriptive cross sectional study. A questionnaire was self administered by the authors on all the final year medical students of Usmanu Danfodio University, Sokoto. Data was analyzed with SPSS version 20.0 Results: Out of the 60 respondents only 3(5%) had interest in pursuing chemical pathology as a postgraduate medical career. The medical students with ages ranging from 20 to 24 years were more likely to choose chemical pathology as a career using the multivariate mode

Published

2015

7. Abstracts

Author

Donat, F., Bevan, D. R., Baumgarten, R. K., Brown, J. L., Gyasi, H. K., Naguib, M., Adu-Gyamfi, Woodey, R., Morris, R., Graham, G., Torda, R., Hudson, R. J., Thomson, I. R., Cannon, J. E., Friesen, R. M., Meatherall, R. C., Chung, F., Evans, D., Stock, J., Sutherland, A. D., Coombs, R., Saunders, R., Savage, S., Jensen, L., Murphy, C., Murkin, J. M., Farrar, J. K., Tweed, W. A., Guiraudon, G., McKenzie, F. N., Tarn, S., Chung, F., Campbell, J. M., Harder, K. F., Fay, J., Shelley, E. S., Plourde, G., Hardy, J. F., MacDonald, A. I., Carle, H., Vincent, D., Legatt, D., Doyle, D. J., McCulloch, P., Milne, B., Newman, B., Lam, A. M., Cuillerier, D. J., Martin, R., Léna, P., Lamarche, Y., Black, R., Crawford, D., Froese, A. B., Butler, P., Brown, S. C., Lam, A. M., Manninen, P. H., Knill, R. L., Famewo, C. E., Naguib, M., Fleming, J., Walker, A., Lambert, T., Lah, F., Giles, W. R., Trudinger, B. J., Ahuja, B., Strunin, L., Chovaz, P. M., Sandier, A. N., Selby, D. G., Ilsley, A. H., Plummer, J., Runciman, W., Cousins, M., Ravussin, P., Archer, D., Meyer, E., Abou-Madi, M., Trop, D., Manninen, P., Ferguson, G., Blume, W., Cunningham, A. J., O’Higgins, N., McNicholas, W., Doolan, L. A., Williams, K. A., Barker, R. A., Moffitt, E. A., Imrie, D. D., Cousins, C. L., Sullivan, J. A., Kinley, C. E., Murphy, D. A., Moffitt, E. A., McIntyre, A. J., Glenn, J. J., Imrie, D. D., Cousins, C. L., Kinley, C. E., Sullivan, J. A., Murphy, D. A., James, P. D., Volgyesi, G. A., Burrows, F., Johnson, G., Loomis, C., Milne, B., Cervenko, F., Brunet, D., Fyman, P. N., Goodman, K., Hartung, J., Aaron, D., Ergin, A., Kowalski, S. E., Downs, A., Lye, C., Oppenheimer, L., Kozody, R., Duke, P. C., Wade, J. G., Kozody, R., Parrott, J., Duke, P. C., Wade, J. G., Kozody, R., Duke, P. C., Wade, J. G., Kozody, R., Parrott, J., Duke, P. C., Wade, J. G., Michoud, M. C., Amyot, R., St-Jean, S., Chapleau, D., Couture, J., Badgwell, J. M., Heavner, J. E., Cockings, E., Cooper, M. W., Maloney, L. L., Coombs, D. W., Yeager, M. P., Vanier, M., Vikis-Freiberg, V., Couture, J., Weston, G. A., Roth, S. H., James, P. D., Volgyesi, G. A., Burrows, F., Wolf, G. L., Capuano, C., Hartung, J., Selb, D. G., Ilsley, A., Runciman, W., Mather, L., Moote, C. A., Knill, R. L., Clement, J. L., Sutherland, T., Davies, J. M., Stock, J., Harpin, R. P., Wright, D. J., Hanna, M., Williams, R. T., Sutherland, T., Bradley, J. P., Marsland, A., Salkfield, I., Hardy, J. F., Girouard, G., Charest, J., Brown, M. J., Dollery, C. T., Desjardins, R., Gelb, A. W., Shokunbi, T., Floyd, P., Mervart, M., Peerless, S. J., Prideaux, P. R., Crankshaw, D. P., and Morgan, D. J.

Published

1985

8. Effect of early tranexamic acid treatment on fatigue in patients with mild traumatic brain injury: data from the CRASH-3 clinical trial.

Author

Mansukhani R, Belli A, Brenner A, Chaudhri R, Frimley L, Faizah Jamaluddin S, Jooma R, Shakur-Still H, Shokunbi T, and Roberts I

Abstract

Background: Each year world-wide about 65 million people sustain a mild traumatic brain injury (mTBI). Fatigue is a common and distressing symptom after mTBI. We examine the effect of tranexamic acid (TXA) on fatigue in patients with mTBI using data from the CRASH-3 trial., Methods: The CRASH-3 trial randomised 9,202 patients with traumatic brain injury and no significant extracranial bleeding to receive TXA or placebo within 3 hours of injury. The primary outcome was death from head injury within 28 days of injury. The methods and results are presented elsewhere. Fatigue was recorded as "None", "Moderate" or "Extreme." This study examines the effect of TXA on extreme fatigue in the 2,632 patients with mTBI (Glasgow Coma Scale [GCS] score≥13). Our analyses were not prespecified., Results: Our study primary outcome, extreme fatigue, was reported for 10 (0.8%) of 1,328 patients receiving TXA and 19 (1.5%) of 1,288 patients receiving placebo (risk ratio [RR]=0.51, 95% confidence interval [CI] 0.24-1.09). Death within 28 days of injury was reported for 34 (2.6%) of 1,328 patients receiving TXA versus 47 (3.6%) of 1,288 patients receiving placebo (RR=0.70, 95% CI 0.45-1.08). Among patients allocated to TXA, 44 (3.3%) patients either died or reported extreme fatigue versus 66 (5.1%) patients among those allocated to placebo (RR=0.65, 95% CI 0.44-0.94). This composite outcome is disproportionately influenced by deaths which account for 74% (81 from 110) of events., Conclusions: We found no evidence that tranexamic acid reduces fatigue in patients with mTBI. Given, 1) our analyses were not prespecified, 2) our outcome measure is not based on a validated fatigue severity scale, and 3) TBI patients can suffer from hospital-induced delirium, which hinders clinician assessment, these results need to be replicated in another study., Registration: ISRCTN (ISRCTN15088122, 19/07/2011), ClinicalTrials.gov (NCT01402882, 26/07/2011), EudraCT (2011-003669-14, 25/07/2011), Pan African Clinical Trial Registry (PACTR20121000441277, 30/10/2012)., Competing Interests: No competing interests were disclosed., (Copyright: © 2024 Mansukhani R et al.)

Published

2024

9. Probing Caffeine Administration as a Medical Management for Hydrocephalus: An Experimental Study.

Author

Olopade F, Femi-Akinlosotu O, Ibitoye C, and Shokunbi T

Subjects

Animals, Cerebral Ventricles, Humans, Kaolin adverse effects, Mice, Water adverse effects, Caffeine adverse effects, Hydrocephalus complications, Hydrocephalus drug therapy

Abstract

Background: Hydrocephalus is currently managed by cerebrospinal fluid diversion from the cerebral ventricles to other body sites, but this is complicated by obstruction and infection in young infants, thus adding to morbidity and mortality. Studies have reported caffeine to be a pleiotropic neuroprotective drug in the developing brain due to its antioxidant, anti-inflammatory, and antiapoptotic properties, with improved white matter microstructural development. In this study, we investigate the use of caffeine administration as a possible means of pharmacological management for hydrocephalus., Methods: A total of 76 three-day-old mice pups from 10 dams were divided into four groups: hydrocephalus was induced in the pups in two groups by intracisternal injection of kaolin suspension, and their dams were given either caffeine (50 mg/kg by gavage) or water daily for 21 days; the dams in the other 2 (non-hydrocephalic) groups similarly had either caffeine or water; the pups received caffeine administered via lactation. Developmental neurobehavioral tests were performed until day 21, when the pups were sacrificed. Their brains were removed and processed for Cresyl and Golgi staining; both quantitative and qualitative analyses were then carried out., Results: Improved developmental motor activities and reflexes were observed in the hydrocephalus + caffeine-treated pups. Caffeine administration was associated with reduced cell death and increased dendritic arborization of the neurons in the sensorimotor cortex and striatum of hydrocephalic mice pups., Conclusion: Caffeine administration appears to have promise as an adjunct in hydrocephalus management, and its use needs to be further explored., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

10. Tranexamic acid to reduce head injury death in people with traumatic brain injury: the CRASH-3 international RCT.

Author

Roberts I, Shakur-Still H, Aeron-Thomas A, Beaumont D, Belli A, Brenner A, Cargill M, Chaudhri R, Douglas N, Frimley L, Gilliam C, Geer A, Jamal Z, Jooma R, Mansukhani R, Miners A, Pott J, Prowse D, Shokunbi T, and Williams J

Subjects

Adult, Cost-Benefit Analysis, Glasgow Coma Scale, Humans, Antifibrinolytic Agents therapeutic use, Brain Injuries, Traumatic complications, Brain Injuries, Traumatic drug therapy, Craniocerebral Trauma, Tranexamic Acid therapeutic use

Abstract

Background: Tranexamic acid safely reduces mortality in traumatic extracranial bleeding. Intracranial bleeding is common after traumatic brain injury and can cause brain herniation and death. We assessed the effects of tranexamic acid in traumatic brain injury patients., Objective: To assess the effects of tranexamic acid on death, disability and vascular occlusive events in traumatic brain injury patients. We also assessed cost-effectiveness., Design: Randomised trial and economic evaluation. Patients were assigned by selecting a numbered treatment pack from a box containing eight packs that were identical apart from the pack number. Patients, caregivers and those assessing outcomes were masked to allocation. All analyses were by intention to treat. We assessed the cost-effectiveness of tranexamic acid versus no treatment from a UK NHS perspective using the trial results and a Markov model., Setting: 175 hospitals in 29 countries., Participants: Adults with traumatic brain injury within 3 hours of injury with a Glasgow Coma Scale score of ≤ 12 or any intracranial bleeding on computerised tomography scan, and no major extracranial bleeding, were eligible., Intervention: Tranexamic acid (loading dose 1 g over 10 minutes then infusion of 1 g over 8 hours) or matching placebo., Main Outcome Measures: Head injury death in hospital within 28 days of injury in patients treated within 3 hours of injury. Secondary outcomes were early head injury deaths, all-cause and cause-specific mortality, disability, vascular occlusive events, seizures, complications and adverse events., Results: Among patients treated within 3 hours of injury ( n  = 9127), the risk of head injury death was 18.5% in the tranexamic acid group versus 19.8% in the placebo group (855/4613 vs. 892/4514; risk ratio 0.94, 95% confidence interval 0.86 to 1.02). In a prespecified analysis excluding patients with a Glasgow Coma Scale score of 3 or bilateral unreactive pupils at baseline, the results were 12.5% in the tranexamic acid group versus 14.0% in the placebo group (485/3880 vs. 525/3757; risk ratio 0.89, 95% confidence interval 0.80 to 1.00). There was a reduction in the risk of head injury death with tranexamic acid in those with mild to moderate head injury (166/2846 vs. 207/2769; risk ratio 0.78, 95% confidence interval 0.64 to 0.95), but in those with severe head injury (689/1739 vs. 685/1710; risk ratio 0.99, 95% confidence interval 0.91 to 1.07) there was no apparent reduction ( p -value for heterogeneity = 0.030). Early treatment was more effective in mild and moderate head injury ( p  = 0.005), but there was no obvious impact of time to treatment in cases of severe head injury ( p  = 0.73). The risk of disability, vascular occlusive events and seizures was similar in both groups. Tranexamic acid is highly cost-effective for mild and moderate traumatic brain injury (base case of £4288 per quality-adjusted life-year gained)., Conclusion: Early tranexamic acid treatment reduces head injury deaths. Treatment is cost-effective for patients with mild or moderate traumatic brain injury, or those with both pupils reactive., Future Work: Further trials should examine early tranexamic acid treatment in mild head injury. Research on alternative routes of administration is needed., Limitations: Time to treatment may have been underestimated., Trial Registration: Current Controlled Trials ISRCTN15088122, ClinicalTrials.gov NCT01402882, EudraCT 2011-003669-14, Pan African Clinical Trial Registry PACTR20121000441277., Funding: The project was funded by the National Institute for Health Research (NIHR) Health Technology Assessment programme and will be published in full in Health Technology Assessment ; Vol. 25, No. 26. See the NIHR Journals Library website for further project information. In addition, funding was provided by JP Moulton Charitable Trust, Joint Global Health Trials (Medical Research Council, Department for International Development and the Wellcome Trust). This project was funded by the NIHR Global Health Trials programme.

Published

2021

11. Understanding the neuroprotective effect of tranexamic acid: an exploratory analysis of the CRASH-3 randomised trial.

Author

Brenner A, Belli A, Chaudhri R, Coats T, Frimley L, Jamaluddin SF, Jooma R, Mansukhani R, Sandercock P, Shakur-Still H, Shokunbi T, and Roberts I

Subjects

Antifibrinolytic Agents adverse effects, Antifibrinolytic Agents pharmacology, Antifibrinolytic Agents therapeutic use, Brain Injuries drug therapy, Humans, Multiple Trauma complications, Multiple Trauma drug therapy, Neuroprotective Agents adverse effects, Neuroprotective Agents pharmacology, Neuroprotective Agents therapeutic use, Tranexamic Acid adverse effects, Tranexamic Acid therapeutic use, Brain Injuries prevention & control, Protective Factors, Tranexamic Acid pharmacology

Abstract

Background: The CRASH-3 trial hypothesised that timely tranexamic acid (TXA) treatment might reduce deaths from intracranial bleeding after traumatic brain injury (TBI). To explore the mechanism of action of TXA in TBI, we examined the timing of its effect on death., Methods: The CRASH-3 trial randomised 9202 patients within 3 h of injury with a GCS score ≤ 12 or intracranial bleeding on CT scan and no significant extracranial bleeding to receive TXA or placebo. We conducted an exploratory analysis of the effects of TXA on all-cause mortality within 24 h of injury and within 28 days, excluding patients with a GCS score of 3 or bilateral unreactive pupils, stratified by severity and country income. We pool data from the CRASH-2 and CRASH-3 trials in a one-step fixed effects individual patient data meta-analysis., Results: There were 7637 patients for analysis after excluding patients with a GCS score of 3 or bilateral unreactive pupils. Of 1112 deaths, 23.3% were within 24 h of injury (early deaths). The risk of early death was reduced with TXA (112 (2.9%) TXA group vs 147 (3.9%) placebo group; risk ratio [RR] RR 0.74, 95% CI 0.58-0.94). There was no evidence of heterogeneity by severity (p = 0.64) or country income (p = 0.68). The risk of death beyond 24 h of injury was similar in the TXA and placebo groups (432 (11.5%) TXA group vs 421 (11.7%) placebo group; RR 0.98, 95% CI 0.69-1.12). The risk of death at 28 days was 14.0% in the TXA group versus 15.1% in the placebo group (544 vs 568 events; RR 0.93, 95% CI 0.83-1.03). When the CRASH-2 and CRASH-3 trial data were pooled, TXA reduced early death (RR 0.78, 95% CI 0.70-0.87) and death within 28 days (RR 0.88, 95% CI 0.82-0.94)., Conclusions: Tranexamic acid reduces early deaths in non-moribund TBI patients regardless of TBI severity or country income. The effect of tranexamic acid in patients with isolated TBI is similar to that in polytrauma. Treatment is safe and even severely injured patients appear to benefit when treated soon after injury., Trial Registration: ISRCTN15088122 , registered on 19 July 2011; NCT01402882 , registered on 26 July 2011.

Published

2020

12. Tranexamic acid for significant traumatic brain injury (The CRASH-3 trial): Statistical analysis plan for an international, randomised, double-blind, placebo-controlled trial.

Author

Roberts I, Belli A, Brenner A, Chaudhri R, Fawole B, Harris T, Jooma R, Mahmood A, Shokunbi T, and Shakur H

Abstract

Background: Worldwide, traumatic brain injury (TBI) kills or hospitalises over 10 million people each year. Early intracranial bleeding is common after TBI, increasing the risk of death and disability. Tranexamic acid reduces blood loss in surgery and death due to bleeding in trauma patients with extra-cranial injury. Early administration of tranexamic acid in TBI patients might limit intracranial bleeding, reducing death and disability. The CRASH-3 trial aims to provide evidence on the effect of tranexamic acid on death and disability in TBI patients. We will randomly allocate about 13,000 TBI patients (approximately 10,000 within 3 hours of injury) to an intravenous infusion of tranexamic acid or matching placebo in addition to usual care. This paper presents a protocol update (version 2.1) and statistical analysis plan for the CRASH-3 trial. Results: The primary outcome is head injury death in hospital within 28 days of injury for patients treated within 3 hours of injury (deaths in patients treated after 3 hours will also be reported). Because there are reasons to expect that tranexamic acid will be most effective in patients treated immediately after injury and less effective with increasing delay, the effect in patients treated within one hour of injury is of particular interest. Secondary outcomes are all-cause and cause-specific mortality, vascular occlusive events, disability based on the Disability Rating Scale and measures suggested by patient representatives, seizures, neurosurgical intervention, neurosurgical blood loss, days in intensive care and adverse events. Sub-group analyses will examine the effect of tranexamic acid on head injury death stratified by time to treatment, severity of TBI and baseline risk. Conclusion: The CRASH-3 trial will provide reliable evidence of the effectiveness and safety of tranexamic acid in patients with acute TBI. Registration: International Standard Randomised Controlled Trials registry ( ISRCTN15088122) 19/07/2011, and ClinicalTrials.gov ( NCT01402882) 25/07/2011., Competing Interests: No competing interests were disclosed.

Published

2018

13. Childhood head injury in Ibadan: causes, neurologic complications and outcome.

Author

Shokunbi T and Olurin O

Subjects

Age Factors, Causality, Child, Child, Preschool, Craniocerebral Trauma therapy, Female, Follow-Up Studies, Glasgow Coma Scale, Humans, Infant, Infant, Newborn, Male, Nigeria epidemiology, Prognosis, Treatment Outcome, Urban Population, Accidental Falls statistics & numerical data, Accidents, Traffic statistics & numerical data, Craniocerebral Trauma epidemiology, Craniocerebral Trauma etiology, Population Surveillance

Abstract

Ninety-nine children who suffered head injuries between January, 1988 and June, 1989 were analysed. These form approximately 60% of the total number of children with head injury seen at our institution over this period. The mean age (+/- SD) was 77.5 (+/- 53.1) months. There were more males than females (1.8:1). The two most frequent causes of head injury were pedestrian-vehicular accidents, PVA, (38%) and falls at home, FH, (40%). Fifty-two per cent of the patients sustained a loss of consciousness at presentation, 43% exhibited additional neurological deficits. Skull fractures were present in 45%. There were 2 deaths in this group. Only 8% of the patients underwent surgery which was limited to elevation of compound depressed skull fractures. By the time of discharge, neural deficits were present in 17%. 56 patients were followed-up over a mean period of 4 months. 82% of them were neurologically normal, Head injury from vehicular accidents affected older children, was more severe, but recovered as well as that from falls, except with respect to mental status function.

Published

1994

14. Ocular complications of head injury in children.

Author

Shokunbi T and Agbeja A

Subjects

Adolescent, Blindness etiology, Child, Child, Preschool, Eye Hemorrhage etiology, Eyelids injuries, Female, Humans, Infant, Male, Optic Nerve Injuries, Cranial Nerve Injuries, Craniocerebral Trauma complications, Eye Diseases etiology

Abstract

Ocular complications occurred in 28% of children with head injury. Neuro-ophthalmological lesions made up one-third of these complications, mostly involved the optic nerve, and were associated with other focal neurological signs more frequently than non-neural ocular complications. Lesions of the posterior visual pathways were rare but tended to be permanent.

Published

1991