Your search keyword '"Toner, Aileen"' showing total 7 results

1. A systematic review of urine biomarkers in children with IgA vasculitis nephritis

Author

Williams, Chloe E. C., Toner, Aileen, Wright, Rachael D., and Oni, Louise

Subjects

Vasculitis -- Diagnosis -- Physiological aspects, IgA glomerulonephritis -- Diagnosis -- Physiological aspects, Biological markers -- Identification and classification, Health

Abstract

Background Nephritis is a recognised complication of IgA vasculitis (IgAV, Henoch-Schönlein purpura) contributing to 1-2% of all chronic kidney disease (CKD) stage 5. Improved understanding may reduce irreversible damage in IgAV nephritis (IgAV-N). Objective The aim of this study was to perform a comprehensive systematic literature review to identify promising clinical and pre-clinical urine biomarkers in children with IgAV-N that could predict the presence of nephritis and/or determine its severity. Methods A systematic literature review was performed using four search engines and a predefined search term strategy. Promising biomarkers were divided in terms of clinical or pre-clinical and ability to predict the presence of nephritis or determine its severity. Results were described using statistical significance (p < 0.05) and area under the curve (AUC) values. Results One hundred twenty-one studies were identified; 13 were eligible. A total of 2446 paediatric patients were included: healthy controls (n = 761), children with IgAV-N (n = 1236) and children with IgAV without nephritis (IgAV-noN, n = 449). Fifty-one percent were male, median age 7.9 years. The clinical markers, 24-h protein quantity and urine protein:creatinine ratio, were deemed acceptable for assessing severity of nephritis (AUC < 0.8). Urinary albumin concentration (Malb) performed well (AUC 0.81-0.98). The most promising pre-clinical urinary biomarkers in predicting presence of nephritis were as follows: kidney injury molecule-1 (KIM-1) (AUC 0.93), monocyte chemotactic protein-1 (MCP-1) (AUC 0.83), N-acetyl-[beta]-glucosaminidase (NAG) (0.76-0.96), and angiotensinogen (AGT) (AUC not available). Urinary KIM-1, MCP-1, and NAG appeared to correlate with disease severity. Conclusions Longitudinal studies are needed to assess whether pre-clinical biomarkers enhance standard of care in IgAV-N., Author(s): Chloe E. C. Williams [sup.1] [sup.2] , Aileen Toner [sup.1] , Rachael D. Wright [sup.2] , Louise Oni [sup.2] [sup.3] Author Affiliations: (1) grid.10025.36, 0000 0004 1936 8470, School [...]

Published

2021

2. Methods of measuring disease activity in paediatric IgA vasculitis

Author

Williams, Chloe, Toner, Aileen, Dowsett, Tom, Murphy, Jared, and Oni, Louise

Abstract

Introduction: IgA vasculitis (IgAV, Henoch-Schönlein purpura, HSP) is the most common vasculitis of childhood and currently contributes to 1-2% of all chronic kidney disease (CKD) stage 5. New methods of measuring disease activity are required to improve the standard of care given. The aim of this thesis is to evaluate methods of measuring disease activity in IgAV using urine biomarkers and a disease-specific scoring tool. Methods: Firstly, a systematic literature review was performed using 4 search engines and a search term strategy with predefined inclusion and exclusion criteria. Promising biomarkers were divided in terms of traditional or novel and described using statistical significance and area under the curve (AUC) values. Secondly, a specific disease activity scoring tool (the IgA-VAS) was developed and preliminarily validated in a cohort of paediatric patients with IgAV. Test validity, concurrent validity and inter-rater agreement were assessed retrospectively. A randomly selected subgroup were also scored using a visual analogue scale. Results: The systematic review identified 13 eligible studies. A total of 2,446 paediatric patients were included: healthy controls (n=761), children with IgAV-N (n=1,236) and children with IgAV without nephritis (IgAV-noN, n=449). 51% were male, median age 7.9 years. The traditional markers, 24-hour protein quantity and urine protein:creatinine ratio were deemed acceptable for assessing severity of nephritis (AUC 0.5, p

Published

2022

3. Continuous glucose monitoring systems for monitoring cystic fibrosis-related diabetes

Author

Toner, Aileen, additional, McCloy, Anna, additional, Dyce, Paula, additional, Nazareth, Dilip, additional, and Frost, Freddy, additional

Published

2021

4. 549 A systematic review of urine biomarkers in children with IgA vasculitis nephritis

Author

Williams, Chloe, primary, Toner, Aileen, additional, Wright, Rachael, additional, and Oni, Louise, additional

Published

2021

5. Continuous glucose monitoring systems for monitoring cystic fibrosis-related diabetes

Author

Toner, Aileen, additional, McCloy, Anna, additional, Dyce, Paula, additional, Nazareth, Dilip, additional, and Frost, Freddy, additional

Published

2020

6. The impact of continuous glucose monitoring on the management of people with cystic fibrosis-related diabetes

Author

Toner, Aileen and Southern, Kevin

Abstract

Background Cystic fibrosis-related diabetes (CFRD) is the most common comorbidity found in people with cystic fibrosis (pwCF). CFRD is associated with increased adverse outcomes and burden of treatment in pwCF as well as reduced quality of life. People with CFRD (pwCFRD) must measure their blood glucose levels several times per day to monitor their diabetes and so that treatment can be tailored to individuals. Continuous glucose monitoring systems (CGMS) are a relatively new technology that have been shown to be useful in diagnosing CFRD, but the impact of CGM on the monitoring and subsequent management of CFRD remains undetermined. This application of CGM has previously been approved in people with other forms of diabetes. Method For this work, engagement with stakeholders was undertaken to devise outcomes of interest that would make a meaningful impact on the lives and wellbeing of pwCFRD and those involved with their care. A protocol for an original Cochrane systematic review on the impact of CGM on pwCFRD was then created and the review itself was conducted. This included performing a comprehensive search of five major databases and assessing the eligibility of the results for inclusion in the study. A suggested framework for future research in this area was then created. Results Out of a total of 1768 studies, once duplicates were eliminated, there were found to be no completed RCT studies that appropriately fitted the protocol’s criteria for inclusion in the review. The only study that did meet the criteria was a single RCT protocol registered at clinicaltrials.gov (NCT03939065) which had not yet been undertaken, and thus, presented no data to be analysed for the review at this time. However, once this trial is completed, it may be eligible for inclusion in an update of this review. Discussion There is currently no evidence to support the costly implementation of CGM to manage CFRD, although there are indications that CGMS are already being used in this context. CFRD is becoming more prevalent because of a range of factors including the improved life expectancy of pwCF. The impact of CFRD on peoples’ lives is of ever-growing importance and so it is now more pressing than ever to conduct research into ways to help alleviate both the treatment and disease burden for pwCFRD. Ensuring new technologies are properly evaluated will contribute to the provision of a growing and robust body of evidence which in turn will support the decision-making of policy makers, clinicians, and patients alike. As discussed, there is currently no data available on the impact of CGM on the management of pwCFRD. However, it is noted that the absence of evidence is not evidence of absence of effect. It is hoped that publication of this review will raise the profile of the question at hand and generate sufficient research to provide a route map to find the answers.

7. UK Foot and Ankle Thromboembolism (UK-FATE).

Author

Mangwani J, Houchen-Wolloff L, Malhotra K, Booth S, Smith A, Teece L, Mason LW, Shaikh R, Alfred W, Okhifun I, Cinar E, Bua N, Vemulapalli K, Acharya A, Gadd R, Money-Taylor J, Kantharaju R, Bhosale A, Bahri S, Broadbent R, Drummond I, Jones N, Shah S, Ravindrarjah T, Yasen Z, Singh K, Al-Habs R, Jeyaseelan L, Habbiba A, Walker T, Dewhurst M, Glasgow N, Eze D, Carter G, Rajan P, Patil V, Amer O, Malik K, Pavanerathan P, Mallick A, Seferiadis I, Currall V, Sadasivan P, Kumar S, Sanjani SR, Ciaccio M, Ayyaswamy B, Prasad P, Anand M, Sunilraj D, Lane S, Prathap S, Kankate R, Aktselis I, Davda K, Vijapur A, Tayyem M, Chau J, Azhar MS, Sturdee S, Hussain H, Sonde S, Luqman MQ, Farooq R, Wells G, Shenolikar A, Simons M, Hodgson P, Thomas R, Stevens S, Elhassan Y, Adeniyi A, Aspinall W, Joseph V, Day M, Tong A, Joyner C, Alzaranky M, Elhassan O, Chhantyal K, Arora A, Abiddin Z, Kucharski R, Ahmad I, Zeb J, Ishaq U, Thomas J, Jain K, Deol R, Faroug R, Johal K, Mordecai S, Argyropouos M, Chawla A, Ibrahim M, Pereira M, Barr L, Julies E, Hill F, Kapoor S, Bailey J, Mukhopadhyay I, Rana S, Tarig H, Qualaghassi M, Seewoonarian S, Rose B, Crate G, Abbott S, Fenner C, Geleit R, Yousaf S, Akram N, Al-Hubeshy Z, Patel B, Hussein M, Clark C, Giddie J, Dega R, Dasari K, Nandhara G, Kumar P, Gupta P, Poole H, Zace P, Alvi F, Jacob J, Reddy R, Sateesh V, Gledhill A, Craven J, Cichero M, Yates B, Newton A, Grice J, Fawcett N, Fraig H, Hamad F, Marsland D, Elliot R, Ghani Y, Chandrashekhar S, Millan RK, Clark A, Rahman K, Sykes M, Little Z, Saleem J, Jolly L, Jain A, Qadri A, Rymaruk S, Kulkarni A, Garabadi M, Akhtar M, Hossain M, Yunus S, Saleem M, Fong J, Islam A, Nusir B, Chapman J, Holmes D, Mamoowala N, Almond K, Wright C, Caruana E, Watson T, Allison G, Pillai A, Madhi I, Alsalihy M, Elamin K, Yip CR, Tew L, Dahiya R, Goff T, Bagshaw O, Slade H, Andrzejowski P, Gomati A, Drake C, Hind J, Morgan R, Khalaf A, Ditta A, Ramasamy A, McIntyre J, Blacklock C, Middleton S, Clayton R, Hrycaiczuk A, Thornhill C, Jeyakumar G, Vaithilingam D, Potter K, Jamal/Pete Chan B, Mohamed M, Fraser D, Elhalawany A, Beastall J, Cousins G, Nunag P, Loveday D, Bawa A, Gilmore R, Schankat K, Walls A, Corin N, Robinson P, Hepple S, Harries W, Riddick A, Winson I, Marsh L, Bashir MA, Saini J, Atkinson H, Limaye R, Johnson-Lynn S, Sethi M, Flanagan G, Uddin A, Reilly I, Martin R, Pujol-Nichol A, Carroll N, Boucher A, Alward M, Myint Y, Butler K, Kendal A, Bugeja M, Mooteeram J, Saedi F, Koc T, Morcos Z, Robertson G, Holmes N, Tribe H, Pearkes T, Soliman A, Prasanna A, Teoh K, Kamat S, Bajracharya A, Reeves J, Ngwayi M, Imtiaz G, Blackmore N, Lau B, Naik A, Tung E, Murhekar S, Ray R, Lyle S, Makwana N, Kaisi KA, Al-Musabi M, Dean M, Hughes A, Shuttlewood K, Welck M, Patel S, Sykes A, Thibbaiah MM, Hadi H, Haldar A, Ardakani AG, Jani P, Kutuzov V, Gibbons J, Trussler D, Hawley E, Akhtar S, Rajgor HD, Budair B, Prem H, Mckenzie J, Thurston D, O'Sullivan M, Elmajee M, Pond E, Zahra W, Heaver C, Igbagiri K, Gaukroger A, Solan M, Peacock C, Fan KS, Barton T, Robinson D, Graham S, Zeolla J, Everett S, Iqbal M, Gourbault L, Singh S, Tang C, Tarhini M, Khan S, Balasubramanian S, Lever C, Bansod V, Iyengar K, Wadood A, McMillan L, Toh E, Masunda S, Federer S, Ahmad F, Lashin A, Kaddah A, Oladeji E, Dawe E, Nolan C, El-Bayouk K, Dhukaram V, Chapman A, Beddard L, Thomas A, Garg V, Taylor H, Kelsall N, Roslee C, Akram N, Lowdon H, Kamel-Sherif A, Jones A, Best A, Zabaglo M, Sayani J, Kyaw O, Khin C, Ali R, Shaik Y, Hossain N, Valente L, Ajis A, Guha A, Pereira M, Ayoub A, Paraoan V, Hali N, Baird C, Kugan R, Abdallatif A, Blomfield M, Jackson G, Craven J, Malhotra A, Toner A, Render L, Ashley C, Limb R, Smith R, Hughes L, Matthews H, Shiers-Gelalis F, Ting J, Place S, Budgen A, Stanley J, and Jowett C

Subjects

Humans, Male, Female, United Kingdom epidemiology, Middle Aged, Prospective Studies, Risk Factors, Adult, Incidence, Aged, Postoperative Complications epidemiology, Postoperative Complications prevention & control, Rupture surgery, Venous Thromboembolism prevention & control, Venous Thromboembolism epidemiology, Venous Thromboembolism etiology, Achilles Tendon injuries, Achilles Tendon surgery, Anticoagulants therapeutic use

Abstract

Aims: Venous thromboembolism (VTE) is a potential complication of foot and ankle surgery. There is a lack of agreement on contributing risk factors and chemical prophylaxis requirements. The primary outcome of this study was to analyze the 90-day incidence of symptomatic VTE and VTE-related mortality in patients undergoing foot and ankle surgery and Achilles tendon (TA) rupture. Secondary aims were to assess the variation in the provision of chemical prophylaxis and risk factors for VTE., Methods: This was a multicentre, prospective national collaborative audit with data collection over nine months for all patients undergoing foot and ankle surgery in an operating theatre or TA rupture treatment, within participating UK hospitals. The association between VTE and thromboprophylaxis was assessed with a univariable logistic regression model. A multivariable logistic regression model was used to identify key predictors for the risk of VTE., Results: A total of 13,569 patients were included from 68 sites. Overall, 11,363 patients were available for analysis: 44.79% were elective (n = 5,090), 42.16% were trauma excluding TA ruptures (n = 4,791), 3.50% were acute diabetic procedures (n = 398), 2.44% were TA ruptures undergoing surgery (n = 277), and 7.10% were TA ruptures treated nonoperatively (n = 807). In total, 11 chemical anticoagulants were recorded, with the most common agent being low-molecular-weight heparin (n = 6,303; 56.79%). A total of 32.71% received no chemical prophylaxis. There were 99 cases of VTE (incidence 0.87% (95% CI 0.71 to 1.06)). VTE-related mortality was 0.03% (95% CI 0.005 to 0.080). Univariable analysis showed that increased age and American Society of Anesthesiologists (ASA) grade had higher odds of VTE, as did having previous cancer, stroke, or history of VTE. On multivariable analysis, the strongest predictors for VTE were the type of foot and ankle procedure and ASA grade., Conclusion: The 90-day incidence of symptomatic VTE and mortality related to VTE is low in foot and ankle surgery and TA management. There was notable variability in the chemical prophylaxis used. The significant risk factors associated with 90-day symptomatic VTE were TA rupture and high ASA grade., Competing Interests: J. Mangwani reports support from the Leicester Hospitals Charity, related to this study. J. Mangwani reports payment or honoraria for lectures, presentations, educational events from Orthosolutions, and royalties from Meshworks, unrelated to this study. K. Malhotra reports payment or honoraria for lectures, presentations, speaker bureaus, manuscript writing or educational events from NewClip Technics, unrelated to this study. L. W. Mason reports royalties or licenses, consulting fees, and patents planned, issued or pending from Orthosolutions, unrelated to this study., (© 2024 The British Editorial Society of Bone & Joint Surgery.)

Published

2024