Volume Expansion with Albumin Compared to Gelofusine in Children with Severe Malaria: Results of a Controlled Trial

Akech, Samuel; Gwer, Samson; Idro, Richard; Fegan, Greg; Eziefula, Alice C; Newton, Charles R.; Levin, Michael; Maitland, Kathryn

doi:10.1371/journal.pctr.0010021

Cited by 102 publications

(87 citation statements)

References 40 publications

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“…The participants in the trial were therefore comparable to study cohorts enrolled in our previous fluid resuscitation trials [3,15,19], with one exception [16].…”

Section: Participantsmentioning

confidence: 99%

“…We aimed to recruit 80 children: 40 to receive Dextran and 40 to receive HES which would give sufficient data on the frequency of serious adverse events and clinical data on correction of hypovolaemic shock. Our previous experience suggested that this number was sufficient to provide information on these key endpoints [3,10,15,16]. Additional new data generated by the study included bolus volumes required of Dextran and HES to achieve satisfactory improvements in haemodynamic features of shock (primary endpoint).…”

Section: Sample Sizementioning

confidence: 99%

“…Additional new data generated by the study included bolus volumes required of Dextran and HES to achieve satisfactory improvements in haemodynamic features of shock (primary endpoint). The trial had a similar design to previously published trials [3,10,15,16] but differed since children with decompensated shock (low systolic blood pressure) were excluded in the current trial since ethical approval to defer consent for these cases, permitted in the previous studies, was declined. The ethics committee raised concerns over the safety of the Dextrans -which in a previous trial had resulted in acute febrile reactions [23].…”

Section: Sample Sizementioning

confidence: 99%

“…In a series of trials we have established that fluid resuscitation with 5% human albumin solution (HAS) results in a lower mortality than either 0.9% saline or Gelofusine ® (a gelatin polymer) [3,10,15,16]. The greatest benefit was seen in the high risk group with acidosis and coma [10].…”

Section: Introductionmentioning

confidence: 99%

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Phase II trial on the use of Dextran 70 or starch for supportive therapy in Kenyan children with severe malaria*

Akech

Jemutai

Timbwa

et al. 2010

Critical Care Medicine

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Objective: A previous meta-analysis has shown a consistent survival benefit in children with severe malaria receiving human albumin solution (HAS) compared to other resuscitation fluids.HAS is expensive and not readily available in Africa. We examined the safety and efficacy of the fluid resuscitation with two synthetic colloids, Dextran 70 and hydroxyethyl starch to inform future trial design.Design: An open-label randomised controlled, phase II safety and efficacy trial. 23/37 (62%) and 25/39 (64%) respectively (p=0.99). Acidosis resolution and respiratory distress was marginally superior in HES group: 3/39 (8%) remained acidotic at 8 hours versus 10/37 (27%) in Dextran arm (p=0.05). There were 4 deaths (5%), two per arm; including 3 deaths in the coma subgroup (3/39, 8%). No other new adverse event was reported. Conclusions:Correction of shock by volume expansion with either Dextran or HES in children with severe malaria acidosis is safe with low mortality, including the highest risk cases admitted in coma. Both solutions present an attractive and practical option for consideration in future volume resuscitation trials in severe malaria.3

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“…The participants in the trial were therefore comparable to study cohorts enrolled in our previous fluid resuscitation trials [3,15,19], with one exception [16].…”

Section: Participantsmentioning

confidence: 99%

Section: Sample Sizementioning

confidence: 99%

Section: Sample Sizementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Phase II trial on the use of Dextran 70 or starch for supportive therapy in Kenyan children with severe malaria*

Akech

Jemutai

Timbwa

et al. 2010

Critical Care Medicine

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“…Some of the factors that may be related to the outcome in that particular group of patients include: high rates of malaria; significant anemia; lack of identification of pathogens in the majority of the patients (only 12 % had positive blood cultures and there were no other tests for bacterial or viral pathogens); lack of availability of respiratory support (ventilation was not available, and in some cases access to oxygen was extremely limited). The result was particularly surprising in light of previous studies from that region demonstrating improvements in patients with severe malaria treated with fluid boluses [74,75]. It is relevant that although early antibiotic administration, vigorous volume resuscitation, and early use of inotropic support was associated with a dramatic improvement in outcomes from severe meningococcal disease in the UK [76], early endotracheal intubation and ventilation was provided for these patients.…”

Section: Fluid Resuscitationmentioning

confidence: 96%

What’s New in the Recognition and Management of Septic Shock in Children: Dos and Don'ts

Argent

2013

Curr Pediatr Rep

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While there has been a reduction in the number of children dying of septic shock in the richer countries of the world, septic shock remains an important cause of both mortality and morbidity for children across the world. Major reduction in the incidence of septic shock will depend on the implementation of public health measures, including immunization. Improvements in outcome of pediatric septic shock have been closely linked to early recognition (although this may be challenging in many situations); early antibiotic administration; early and appropriate fluid administration and subsequent escalation of critical care. A particular challenge has been the development and implementation of systems to ensure that these elements of management are reliably and efficiently implemented in children (even in well-resourced countries). Recent studies have highlighted the complexity of caring for patients with acute severe sepsis and septic shock in countries with fewer resources, and there is an urgent need for further studies to elucidate the implications of these studies for the management of children with septic shock, particularly in settings where additional critical care support such as inotropic or ventilator support may not be readily available.

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Colloid solutions for fluid resuscitation

Bunn

Trivedi

2012

Cochrane Database of Systematic Reviews

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Background Colloids are widely used in the replacement of fluid volume. However doubts remain as to which colloid is best. Different colloids vary in their molecular weight and therefore in the length of time they remain in the circulatory system. Because of this and their other characteristics, they may differ in their safety and efficacy. Objectives To compare the effects of different colloid solutions in patients thought to need volume replacement. Search strategy We searched the Cochrane Injuries Group specialised register, the Cochrane Controlled Trials Register (2002 Issue 3), MEDLINE (1994-2002/07), EMBASE (1974-2002 August week 1), and the National Research Register (2002 issue 3). Bibliographies of trials retrieved were searched, and drug companies manufacturing colloids were contacted for information. The search was last updated in September 2002. Selection criteria Randomised and quasi-randomised trials comparing colloid solutions in critically ill and surgical patients thought to need volume replacement. The main outcomes measured were death, amount of whole blood transfused, and incidence of adverse reactions. Data collection and analysis Two authors independently extracted the data and assessed the quality of the trials. Main results Fifty-seven trials met the inclusion criteria, with a total of 3659 participants. Quality of allocation concealment was judged to be adequate in 20 trials and poor or uncertain in 37. Deaths were obtained from 36 trials. For albumin or PPF versus hydroxyethyl starch (HES) 20 trials (n=1029) reported mortality. The pooled relative risk (RR) was 1.17 (95% CI 0.91, 1.50). For albumin or PPF versus gelatin four trials (n=542) reported mortality. The RR was 0.99 (0.69, 1.42). For gelatin vs HES 11 trials (n=945) reported mortality, RR was 1.00 (0.78,1.28). RR was not estimable in the albumin vs dextran, gelatin vs dextran, and HES vs dextran groups. Thirty-six trials recorded the amount of blood transfused, however quantitative analysis was not possible due to skewness and variable reporting. Fifteen trials recorded adverse reactions, but none occurred.

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Volume Expansion with Albumin Compared to Gelofusine in Children with Severe Malaria: Results of a Controlled Trial

Cited by 102 publications

References 40 publications

Phase II trial on the use of Dextran 70 or starch for supportive therapy in Kenyan children with severe malaria*

Phase II trial on the use of Dextran 70 or starch for supportive therapy in Kenyan children with severe malaria*

What’s New in the Recognition and Management of Septic Shock in Children: Dos and Don'ts

Colloid solutions for fluid resuscitation

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