Christina M. Katsios scite author profile

Objective To assess the reporting, extent, and handling of loss to follow-up and its potential impact on the estimates of the effect of treatment in randomised controlled trials.Design Systematic review. We calculated the percentage of trials for which the relative risk would no longer be significant under a number of assumptions about the outcomes of participants lost to follow-up. Data sources Medline search of five top general medical journals, 2005-07.Eligibility criteria Randomised controlled trials that reported a significant binary primary patient important outcome. ResultsOf the 235 eligible reports identified, 31 (13%) did not report whether or not loss to follow-up occurred. In reports that did give the relevant information, the median percentage of participants lost to follow-up was 6% (interquartile range 2-14%). The method by which loss to follow-up was handled was unclear in 37 studies (19%); the most commonly used method was survival analysis (66, 35%). When we varied assumptions about loss to follow-up, results of 19% of trials were no longer significant if we assumed no participants lost to follow-up had the event of interest, 17% if we assumed that all participants lost to RESEARCHfollow-up had the event, and 58% if we assumed a worst case scenario (all participants lost to follow-up in the treatment group and none of those in the control group had the event). Under more plausible assumptions, in which the incidence of events in those lost to follow-up relative to those followed-up is higher in the intervention than control group, results of 0% to 33% trials were no longer significant. ConclusionPlausible assumptions regarding outcomes of patients lost to follow-up could change the interpretation of results of randomised controlled trials published in top medical journals. IntroductionLoss to follow-up in randomised controlled trials could bias results if the unavailability of data is associated with the likelihood of outcome events. For example, patients might fail to return for assessment because of deterioration in their medical condition, resulting in a higher frequency of adverse outcomes of interest associated with that condition. If the distribution of such patients differs between study arms, the prognostic balance created by randomisation will be disturbed. 1 2 Although analysis of patients for whom outcome data are available in the groups to which they are randomised will avoid bias as a result of factors such as non-adherence, it will not protect against potential bias associated with loss to follow-up. 3Although investigators strive to reduce the amount of missing data, in most instances they will fail to achieve complete follow-up.3-5 Indeed, 60-89% of randomised controlled trials have some missing outcome data.6-8 Interpretation of results is compromised when, as is often the case, investigators do not report strategies for handling such data.8 9 The most commonly reported strategy among trials that do report their approach is to restrict analyses to participants with ful...

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Specific instructions for estimating unclearly reported blinding status in randomized trials were reliable and valid

Akl

Sun

Busse

et al. 2012

Journal of Clinical Epidemiology

146

115

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Extracorporeal carbon dioxide removal in patients with chronic obstructive pulmonary disease: a systematic review

et al. 2015

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Pressure-Controlled vs Volume-Controlled Ventilation in Acute Respiratory Failure

Rittayamai

Katsios

Beloncle

et al. 2015

Chest

120

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An antimicrobial stewardship program improves antimicrobial treatment by culture site and the quality of antimicrobial prescribing in critically ill patients

et al. 2012

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IntroductionIncreasing antimicrobial costs, reduced development of novel antimicrobials, and growing antimicrobial resistance necessitate judicious use of available agents. Antimicrobial stewardship programs (ASPs) may improve antimicrobial use in intensive care units (ICUs). Our objective was to determine whether the introduction of an ASP in an ICU altered the decision to treat cultures from sterile sites compared with nonsterile sites (which may represent colonization or contamination). We also sought to determine whether ASP education improved documentation of antimicrobial use, including an explicit statement of antimicrobial regimen, indication, duration, and de-escalation.MethodsWe retrospectively analyzed consecutive patients with positive bacterial cultures admitted to a 16-bed medical-surgical ICU over 2-month periods before and after ASP introduction (April through May 2008 and 2009, respectively). We evaluated the antimicrobial treatment of positive sterile- versus nonsterile-site cultures, specified a priori. We reviewed patient charts for clinician documentation of three specific details regarding antimicrobials: an explicit statement of antimicrobial regimen/indication, duration, and de-escalation. We also analyzed cost and defined daily doses (DDDs) (a World Health Organization (WHO) standardized metric of use) before and after ASP.ResultsPatient demographic data between the pre-ASP (n = 139) and post-ASP (n = 130) periods were similar. No difference was found in the percentage of positive cultures from sterile sites between the pre-ASP period and post-ASP period (44.9% versus 40.2%; P = 0.401). A significant increase was noted in the treatment of sterile-site cultures after ASP (64% versus 83%; P = 0.01) and a reduction in the treatment of nonsterile-site cultures (71% versus 46%; P = 0.0002). These differences were statistically significant when treatment decisions were analyzed both at an individual patient level and at an individual culture level. Increased explicit antimicrobial regimen documentation was observed after ASP (26% versus 71%; P < 0.0001). Also observed were increases in formally documented stop dates (53% versus 71%; P < 0.0001), regimen de-escalation (15% versus 23%; P = 0.026), and an overall reduction in cost and mean DDDs after ASP implementation.ConclusionsIntroduction of an ASP in the ICU was associated with improved microbiologically targeted therapy based on sterile or nonsterile cultures and improved documentation of antimicrobial use in the medical record.

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