Toward Smarter Lumping and Smarter Splitting: Rethinking Strategies for Sepsis and Acute Respiratory Distress Syndrome Clinical Trial Design

Prescott, Hallie C.; Calfee, Carolyn S.; Thompson, B. Taylor; Angus, Derek C.; Vincent, Jean‐Louis

doi:10.1164/rccm.201512-2544cp

Cited by 264 publications

(236 citation statements)

References 62 publications

(46 reference statements)

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“…in whom benefit outweighs harm) to the treatment in the included population. It is the premise of precision medicine to enrich this group as much as possible with patients with a responsive phenotype (also called predictive enrichment) [58]. The selection of the right patient for the right treatment is one the largest challenges for the coming decade [59,60].…”

Section: Ineffective Interventionsmentioning

confidence: 99%

ARDS: challenges in patient care and frontiers in research

2018

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This review discusses the clinical challenges associated with ventilatory support and pharmacological interventions in patients with acute respiratory distress syndrome (ARDS). In addition, it discusses current scientific challenges facing researchers when planning and performing trials of ventilatory support or pharmacological interventions in these patients.Noninvasive mechanical ventilation is used in some patients with ARDS. When intubated and mechanically ventilated, ARDS patients should be ventilated with low tidal volumes. A plateau pressure <30 cmH 2 O is recommended in all patients. It is suggested that a plateau pressure <15 cmH 2 O should be considered safe. Patient with moderate and severe ARDS should receive higher levels of positive endexpiratory pressure (PEEP). Rescue therapies include prone position and neuromuscular blocking agents. Extracorporeal support for decapneisation and oxygenation should only be considered when lungprotective ventilation is no longer possible, or in cases of refractory hypoxaemia, respectively. Tracheotomy is only recommended when prolonged mechanical ventilation is expected.Of all tested pharmacological interventions for ARDS, only treatment with steroids is considered to have benefit.Proper identification of phenotypes, known to respond differently to specific interventions, is increasingly considered important for clinical trials of interventions for ARDS. Such phenotypes could be defined based on clinical parameters, such as the arterial oxygen tension/inspiratory oxygen fraction ratio, but biological marker profiles could be more promising.

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Section: Ineffective Interventionsmentioning

confidence: 99%

ARDS: challenges in patient care and frontiers in research

2018

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“…To definitively evaluate the effect of balanced crystalloids versus saline on patient-centered outcomes, a large, randomized trial that carefully accounts for differences in baseline risk of AKI (8), volume of crystalloid received (7), and underlying pathophysiology (9)(10)(11)(12) among patients in the intensive care unit (ICU) is required. Such a trial faces numerous logistical challenges, including the need to enroll thousands of patients, deliver the assigned crystalloid in a time-sensitive manner, and collect detailed data on the exact amounts of crystalloid administered, the physiological effects (e.g., serum chloride), and outcomes.…”

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confidence: 99%

Balanced Crystalloids versus Saline in the Intensive Care Unit. The SALT Randomized Trial

Semler

Wang

Byrne

et al. 2017

Am J Respir Crit Care Med

214

196

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Rationale: Saline is the intravenous fluid most commonly administered to critically ill adults, but it may be associated with acute kidney injury and death. Whether use of balanced crystalloids rather than saline affects patient outcomes remains unknown.Objectives: To pilot a cluster-randomized, multiple-crossover trial using software tools within the electronic health record to compare saline to balanced crystalloids.Methods: This was a cluster-randomized, multiple-crossover trial among 974 adults admitted to a tertiary medical intensive care unit from February 3, 2015 to May 31, 2015. The intravenous crystalloid used in the unit alternated monthly between saline (0.9% sodium chloride) and balanced crystalloids (lactated Ringer's solution or PlasmaLyte A). Enrollment, fluid delivery, and data collection were performed using software tools within the electronic health record. The primary outcome was the difference between study groups in the proportion of isotonic crystalloid administered that was saline. The secondary outcome was major adverse kidney events within 30 days (MAKE30), a composite of death, dialysis, or persistent renal dysfunction.Measurements and Main Results: Patients assigned to saline (n = 454) and balanced crystalloids (n = 520) were similar at baseline and received similar volumes of crystalloid by 30 days (median [interquartile range]: 1,424 ml [500-3,377] vs. 1,617 ml [500-3,628]; P = 0.40). Saline made up a larger proportion of the isotonic crystalloid given in the saline group than in the balanced crystalloid group (91% vs. 21%; P , 0.001). MAKE30 did not differ between groups (24.7% vs. 24.6%; P = 0.98).Conclusions: An electronic health record-embedded, clusterrandomized, multiple-crossover trial comparing saline with balanced crystalloids can produce well-balanced study groups and separation in crystalloid receipt.Clinical trial registered with www.clinicaltrials.gov (NCT 02345486).

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“…Similarly, other immunomodulatory drugs such as intravenous immunoglobulins have been discarded based on lack of overall outcome effect [68]. We should re-evaluate such treatment 'failures' by using predictive or prognostic enrichment [69]. Treatment-responsive sub-phenotypes have been suggested for ARDS [70] and sepsis [71], and these need to be explored further.…”

Section: Mediator Modulationmentioning

confidence: 99%