Ruairi M Gallagher
University of Liverpool
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Featured researches published by Ruairi M Gallagher.
Trials | 2012
Ian Sinha; Ruairi M Gallagher; Paula Williamson; Rosalind L. Smyth
BackgroundIn clinical trials in childhood asthma, outcomes reflecting short-term disease activity are frequently measured, whilst functional status, quality of life (QoL), and long-term treatment effects are rarely assessed. There is also non-uniformity across studies in the selection and measurement of outcomes within these domains. The development of a core outcome set has the potential to reduce heterogeneity between trials, lead to research that is more likely to have measured relevant outcomes, and enhance the value of evidence synthesis by reducing the risk of outcome reporting bias and ensuring that all trials contribute usable information.MethodsPaediatricians and specialist nurses, identified through the British Paediatric Respiratory Society, completed a two-round Delphi survey. Separate cohorts of parents of children younger than 18 years, recruited in clinics, participated in each round. Young people with asthma, aged at least 13 years, participated in the first round. Outcomes were identified separately for preschool and school-aged children.We identified outcomes considered important in routine clinical assessment by clinicians and parents/young people. In round 1, 46 clinicians suggested outcomes they considered important when deciding whether to adjust a child’s asthma therapy regime, and 49 parents/young people were asked, using open questions, how they judged whether their child’s (for young people, their own) asthma therapy was appropriate. Two researchers independently classified responses into appropriate, corresponding outcomes.In round 2, 43 clinicians and 50 parents scored, from 0–4, the importance of each outcome suggested by at least 10 % of round 1 responders and selected the three most important.ResultsThe most important outcomes, when making shared decisions about regular therapies for school-aged and preschool children with asthma, were daytime and nocturnal symptoms, exacerbations, QoL, and mortality. Results from parents and clinicians were generally concordant, but parents placed more emphasis on long-term treatment effects.ConclusionsWe have developed a methodology to identify outcomes of most relevance to clinicians, parents, and young people when evaluating regularly administered therapies for asthma. Daytime and nocturnal symptoms, exacerbations, QoL, and mortality are particularly important outcomes that should be measured and reported in all clinical trials of regular therapies for children with asthma.
PLOS ONE | 2011
Ruairi M Gallagher; Jamie Kirkham; Jennifer R. Mason; Kim A Bird; Paula Williamson; Anthony J Nunn; Mark A. Turner; Rosalind L. Smyth; Munir Pirmohamed
Aim To develop and test a new adverse drug reaction (ADR) causality assessment tool (CAT). Methods A comparison between seven assessors of a new CAT, formulated by an expert focus group, compared with the Naranjo CAT in 80 cases from a prospective observational study and 37 published ADR case reports (819 causality assessments in total). Main Outcome Measures Utilisation of causality categories, measure of disagreements, inter-rater reliability (IRR). Results The Liverpool ADR CAT, using 40 cases from an observational study, showed causality categories of 1 unlikely, 62 possible, 92 probable and 125 definite (1, 62, 92, 125) and ‘moderate’ IRR (kappa 0.48), compared to Naranjo (0, 100, 172, 8) with ‘moderate’ IRR (kappa 0.45). In a further 40 cases, the Liverpool tool (0, 66, 81, 133) showed ‘good’ IRR (kappa 0.6) while Naranjo (1, 90, 185, 4) remained ‘moderate’. Conclusion The Liverpool tool assigns the full range of causality categories and shows good IRR. Further assessment by different investigators in different settings is needed to fully assess the utility of this tool.
PLOS ONE | 2012
Ruairi M Gallagher; Jennifer R. Mason; Kim A Bird; Jamie Kirkham; Matthew Peak; Paula Williamson; Anthony J Nunn; Mark A. Turner; Munir Pirmohamed; Rosalind L. Smyth
Objective(s) To obtain reliable information about the incidence of adverse drug reactions, and identify potential areas where intervention may reduce the burden of ill-health. Design Prospective observational study. Setting A large tertiary children’s hospital providing general and specialty care in the UK. Participants All acute paediatric admissions over a one year period. Main Exposure Any medication taken in the two weeks prior to admission. Outcome Measures Occurrence of adverse drug reaction. Results 240/8345 admissions in 178/6821 patients admitted acutely to a paediatric hospital were thought to be related to an adverse drug reaction, giving an estimated incidence of 2.9% (95% CI 2.5, 3.3), with the reaction directly causing, or contributing to the cause, of admission in 97.1% of cases. No deaths were attributable to an adverse drug reaction. 22.1% (95% CI 17%, 28%) of the reactions were either definitely or possibly avoidable. Prescriptions originating in the community accounted for 44/249 (17.7%) of adverse drug reactions, the remainder originating from hospital. 120/249 (48.2%) reactions resulted from treatment for malignancies. The drugs most commonly implicated in causing admissions were cytotoxic agents, corticosteroids, non-steroidal anti-inflammatory drugs, vaccines and immunosuppressants. The most common reactions were neutropenia, immunosuppression and thrombocytopenia. Conclusions Adverse drug reactions in children are an important public health problem. Most of those serious enough to require hospital admission are due to hospital-based prescribing, of which just over a fifth may be avoidable. Strategies to reduce the burden of ill-health from adverse drug reactions causing admission are needed.
Journal of Clinical Pharmacy and Therapeutics | 2011
Ruairi M Gallagher; Kim A Bird; Jennifer R. Mason; Matthew Peak; Paula Williamson; Anthony J Nunn; Mark A. Turner; Munir Pirmohamed; Rosalind L. Smyth
What is known and Objective: It is known that adverse drug reactions (ADRs) cause admission to hospital in adults and children. A recent adult study showed that ADRs are an important and frequent cause of hospital admission. The objective of this study is to develop methodology to ascertain the current burden of ADRs through a prospective analysis of all unplanned admissions to a paediatric hospital.
Archive | 2014
Rosalind L. Smyth; Matthew Peak; Mark A. Turner; Anthony J Nunn; Paula Williamson; Bridget Young; Janine Arnott; Jennifer R Bellis; Kim A Bird; Louise E Bracken; Elizabeth J Conroy; Lynne Cresswell; Jennifer C Duncan; Ruairi M Gallagher; Elizabeth Gargon; Hannah Hesselgreaves; Jamie Kirkham; Helena Mannix; Rebecca Md Smyth; Signe Thiesen; Munir Pirmohamed
Programme Grants for Applied Research , 2 (3) (2014) | 2014
Rosalind L Smyth; Matthew Peak; Mark A. Turner; Anthony J Nunn; Paula Williamson; Bridget Young; Janine Arnott; Jennifer R Bellis; Kim A Bird; Louise E Bracken; Elizabeth J Conroy; Lynne Cresswell; Jennifer C Duncan; Ruairi M Gallagher; Elizabeth Gargon; Hannah Hesselgreaves; Jamie Kirkham; Helena Mannix; Rebecca Md Smyth; Signe Thiesen; Munir Pirmohamed
Archives of Disease in Childhood | 2010
Ian Sinha; Ruairi M Gallagher; Paula Williamson; Rosalind L. Smyth
Archive | 2014
Rosalind L Smyth; Matthew Peak; Mark A. Turner; Anthony J Nunn; Paula Williamson; Bridget Young; Janine Arnott; Jennifer R Bellis; Kim A Bird; Louise E Bracken; Elizabeth J Conroy; Lynne Cresswell; Jennifer C Duncan; Ruairi M Gallagher; Elizabeth Gargon; Hannah Hesselgreaves; Jamie Kirkham; Helena Mannix; Rebecca Md Smyth; Signe Thiesen; Munir Pirmohamed
Archive | 2014
Rosalind L Smyth; Matthew Peak; Mark A. Turner; Anthony J Nunn; Paula Williamson; Bridget Young; Janine Arnott; Jennifer R Bellis; Kim A Bird; Louise E Bracken; Elizabeth J Conroy; Lynne Cresswell; Jennifer C Duncan; Ruairi M Gallagher; Elizabeth Gargon; Hannah Hesselgreaves; Jamie Kirkham; Helena Mannix; Rebecca Md Smyth; Signe Thiesen; Munir Pirmohamed
Archive | 2014
Rosalind L Smyth; Matthew Peak; Mark A. Turner; Anthony J Nunn; Paula Williamson; Bridget Young; Janine Arnott; Jennifer R Bellis; Kim A Bird; Louise E Bracken; Elizabeth J Conroy; Lynne Cresswell; Jennifer C Duncan; Ruairi M Gallagher; Elizabeth Gargon; Hannah Hesselgreaves; Jamie Kirkham; Helena Mannix; Rebecca Md Smyth; Signe Thiesen; Munir Pirmohamed