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Does the addition of dextrose to IV crystalloid therapy provide clinical benefit in acute dehydration? A systematic review and meta-analysis

Published online by Cambridge University Press:  30 January 2019

Ashley Grigsby
Affiliation:
Department of Pediatrics, Indiana University School of Medicine, Indianapolis, IN Department of Emergency Medicine, Indiana University School of Medicine, Indianapolis, IN
Jennifer Herron
Affiliation:
Ruth Lilly Medical Library, Indiana University School of Medicine, Indianapolis, IN
Benton R. Hunter*
Affiliation:
Department of Emergency Medicine, Indiana University School of Medicine, Indianapolis, IN
*
Correspondence to: Dr. Benton R. Hunter, Indiana University School of Medicine, Department of Emergency Medicine, 1701 N. Senate Ave., Indianapolis, IN 46202; Email: [email protected]

Abstract

Objectives

Intravenous dextrose aids in the resolution of ketosis in dehydrated patients not tolerating oral glucose and is often recommended in this clinical scenario. Our aim was to determine whether the addition of dextrose to intravenous rehydration solutions results in decreased hospital admissions or other clinically important benefits among dehydrated children or adults.

Methods

MEDLINE, EMBASE, Web of Science, SCOPUS, and the Cochrane Library were searched by a medical librarian from inception through November 2017. The inclusion criteria were randomized controlled trials comparing dextrose containing intravenous solutions with intravenous solutions without dextrose in patients being treated for dehydration, and not already hospitalized.

Results

The database and bibliographies search identified 1,472 unique citations. Only two trials (N = 333) met the inclusion criteria. Both compared normal saline with solutions of dextrose in normal saline. There was no statistically significant difference in admission rates (relative risk = 0.83; 95% confidence interval = 0.62 to 1.10) or revisits (relative risk = 0.54; 95% confidence interval = 0.24 to 1.22). Heterogeneity was low (I2 = 0). No other outcome results were eligible for pooling, but neither study found differences in any clinical outcomes. No adverse events were reported in either trial.

Conclusions

The addition of dextrose to intravenous saline has not been shown to improve clinical outcomes in dehydrated children presenting to the emergency department with gastroenteritis, but the confidence intervals around the estimate of effect are wide and include the possibility of substantial benefit.

Résumé

Objectif

Les perfusions de dextrose aident à neutraliser la cétose chez les patients en état de déshydratation qui ne tolèrent pas la prise orale de glucose, et le traitement est souvent recommandé dans ces situations cliniques. L’étude visait donc à déterminer si l'adjonction de dextrose aux solutions de réhydratation intraveineuse se traduisait par une réduction du nombre d'hospitalisations ou offrait d'autres avantages cliniques importants chez les enfants et les adultes.

Méthode

Une recherche a été menée dans les bases de données MEDLINE, EMBASE, SCOPUS, la plateforme Web of Science et la bibliothèque Cochrane Library par un bibliothécaire spécialisé dans le domaine médical, depuis leur mise sur pied jusqu’à novembre 2017. Les critères de sélection consistaient en la recherche d'essais à répartition aléatoire, dans lesquels étaient comparées des solutions de perfusion additionnées de dextrose à celles n'en contenant pas chez les patients externes, traités pour de la déshydratation.

Résultats

La recherche documentaire dans les bibliographies et les bases de données a permis de relever 1472 citations uniques; toutefois, 2 essais (n = 333) seulement satisfaisaient aux critères de sélection. Dans les deux cas, on comparait des solutions physiologiques salées à des solutions physiologiques salées additionnées de dextrose. Il n'est ressorti aucun écart significatif en ce qui concerne le taux d'hospitalisation (taux relatif [TR] = 0,83; intervalle de confiance [IC] à 95% = 0,62–1,10) ou de reconsultation (TR = 0,54; IC à 95% = 0,24–1,22). Quant à l'hétérogénéité, elle était faible (I2 = 0). Aucun autre résultat ne se prêtait à une mise en commun, mais il ne s'est pas dégagé non plus de différence entre les deux études à l’égard de quelque résultat clinique que ce soit. Enfin, aucun événement indésirable n'a été signalé dans l'un ou l'autre des essais.

Conclusion

L'adjonction de dextrose aux solutions physiologiques salées ne s'est pas traduite par une amélioration des résultats cliniques chez les enfants en état de déshydratation, traités au service des urgences pour une gastroentérite; toutefois, les intervalles de confiance entourant l'estimation des effets sont larges et pourraient comporter des avantages importants.

Type
Original Research
Copyright
Copyright © Canadian Association of Emergency Physicians 2019 

CLINICIAN'S CAPSULE

What is known about the topic?

Intravenous dextrose halts endogenous ketone production and is commonly recommended in dehydrated patients unable to tolerate oral intake.

What did this study ask?

Is there evidence that the addition of dextrose to intravenous fluids provides a clinically meaningful benefit in dehydrated patients?

What did this study find?

Intravenous dextrose has not been shown to provide any important benefit to patients in this setting, but further research is needed.

Why does this study matter to clinicians?

In dehydrated patients, clinicians should not feel obligated towards dextrose containing solutions, which may be more expensive and less readily available.

INTRODUCTION

Vomiting, diarrhea, and dehydration are common reasons for emergency department (ED) visits and hospitalizations, especially in pediatric patients.Reference Gindi and Jones1Reference Schappert and Burt3 Dehydration is often secondary to gastrointestinal losses but can occur from renal dysfunction, skin losses such as sweat and burns, and third space sequestration.Reference Better4, Reference Reid and Losek5 Gastroenteritis accounts for 10 percent of pediatric admissions and approximately 300 deaths in children under age 5 in the United States annually, with a similar disease burden in Europe.2, Reference Elliott6 Oral rehydration is widely recommended for mild to moderate dehydration.Reference Farthing, Salam and Lindberg7, Reference King, Glass, Bresee and Duggan8 However, some patients are unable to tolerate oral rehydration, and IV crystalloid is frequently used.Reference King, Glass, Bresee and Duggan8Reference Simpson and Teach11

Ketosis may complicate dehydration when illness prevents the intake of adequate carbohydrates, leading to increased free fatty acid breakdown and ketogenesis.Reference Reid and Losek5, Reference Levy and Bachur12 Ketoacidosis occurs when there is no carbohydrate substrate and thus no insulin secretion, triggering lipolysis and ketogenesis to prevent hypoglycemia.Reference Toth and Greenbaum13 Patients with lower serum bicarbonate levels are less likely to tolerate oral fluids,Reference Reid and Losek5, Reference Colletti, Brown and Sharieff14 leading to the belief that acidosis contributes to failure of oral rehydration. Because the administration of carbohydrate substrate limits fatty acid oxidation and ketone production, IV glucose should encourage the resolution of ketosis and acidosis, hastening the tolerance of oral intake and speeding recovery.Reference Reid and Losek5, Reference Bai, Fu and Liu15

Children are at increased risk for dehydrationReference Reid and Losek5 and ketosis, due to higher brain energy requirements and lower glycogen stores to produce glucose in times of decreased carbohydrate intake.Reference Toth and Greenbaum13 Acute dehydration thus leads to ketonemia sooner in children than adults (1 day v. 3 days).Reference Toth and Greenbaum13, Reference Owen, Caprio and Reichard16 These pathophysiologic features suggest that pediatric patients with dehydration, particularly from vomiting and diarrhea, should be most likely to benefit from IV dextrose.

The objective of this review was to determine whether existing evidence from randomized controlled trials (RCTs) supports the common teaching that the addition of dextrose to IV rehydration solution improves clinical outcomes in dehydrated patients not already admitted to the hospital. We planned a subgroup analysis to determine whether the evidence supports a larger effect size in children than adults.

METHODS

This systematic review follows the PRISMA guidelines for performing and reporting systematic reviews.

Search strategy

MEDLINE (OvidSP and PubMed interfaces), EMBASE, Web of Science, SCOPUS, and the Cochrane Library were searched by a medical librarian through November 10, 2017. MeSH terms included: Glucose; Administration, Intravenous; Infusions, Intravenous; Dehydration; and Water-Electrolyte Balance. Keywords included variations of these terms and truncations to retrieve any possible alternative use of the terms. Full strategies are available in the appendix. No date or language restrictions were applied. Experts in the field were queried to identify additional trials. Titles and abstracts identified by the search were screened independently by two authors, and the full text was retrieved if either author felt the study was potentially eligible. Full text retrievals were reviewed independently by both authors to determine final eligibility for inclusion in the systematic review, with disagreements settled by discussion or adjudicated by the third author. The bibliographies of retrieved articles and related reviews were searched for additional studies. Lastly, a search was run on trial registries (e.g., ClinicalTrials.gov) to identify missed, ongoing, or unpublished trials.

Inclusion-exclusion criteria

Studies included were randomized, quasi-randomized, or cluster randomized trials comparing an IV solution containing dextrose at any concentration to an IV solution containing no dextrose in non-admitted (ED or outpatient clinic) patients with dehydration. Patients with a source of fluid losses or decreased intake and a need for rehydration therapy, in the opinion of the treating provider, were counted as dehydrated. This definition reflects how dehydration is clinically diagnosed in outpatient settings where accurate baseline body weight is usually unknown. Predefined exclusion criteria were studies of patients already admitted, those with known diabetes, hypoglycemia, underlying metabolic disorders, or known severe metabolic derangements, and patients with hemodynamic instability. Also excluded were studies of surgical patients. We chose to exclude inpatients because the intention of this review was to focus on the initial resuscitation of dehydrated patients. For similar reasons, we sought studies evaluating bolus infusions and excluded trials of maintenance or supra-maintenance intravenous infusions.

Data abstraction

Two authors independently abstracted data from each included study using standardized data abstraction forms. Abstracted information included intervention and control solutions, inclusion and exclusion criteria, setting, year and duration of study, and number of patients in the intervention and control groups meeting each of our predefined end points, if available. Any discrepancies were to be resolved by discussion and a re-evaluation of the original manuscript.

Quality appraisal of included studies

Two authors independently assessed the risk of bias (RoB) of included studies using the Cochrane RoB tool, a validated quality assessment tool for randomized trials.Reference Higgins, Altman and Gotzsche17 Discrepancies regarding RoB designation of any aspects of included studies were resolved by discussion. Colour-coded tables depicting RoB for each domain of the included studies were created using RevMan 5.3.

Outcomes

The predefined primary outcome was hospital admission during the index visit, an objective and patient-important measure of immediate treatment failure in outpatients. Several secondary clinical outcomes were identified a priori and included in the data abstraction, including 1) length of stay in the ED or clinic, 2) return visits within 1 week to the ED or necessitating IV therapy, 3) admission to the hospital within 1 week, 4) a change in dehydration scores, and 5) a patient or surrogate reported change in symptom burden.

Adverse events identified a priori and abstracted included hyperglycemia (defined as blood glucose > 200 mg/dL), symptomatic hypoglycemia (blood glucose < 70 with any symptoms), seizure, sepsis diagnosis within 1 week, and mortality.

Statistical analysis

Meta-analyses were performed using RevMan 5.3. Binary outcomes were meta-analysed using the Mantel-Haenszel method, under a fixed-effects assumption if heterogeneity was low (I 2 < 25), or random effects if heterogeneity was moderate or high (I 2 ≥ 25, or significant clinical heterogeneity). Results of binary outcomes are reported as relative risk (RR) with 95% confidence intervals (CI). Comparisons of continuous variables were to be reported as the mean difference with 95% CI and calculated using the inverse variance method. We planned three subgroup analyses: pediatric patients (age < 18 years); pregnant women of any age; and nonpregnant adults (age ≥ 18 years).

RESULTS

Figure 1 demonstrates the flow of study identification. The literature search identified 1,472 citations. After a review of titles and abstracts, 24 studies were retrieved for full text review. Reasons for exclusion are shown in Figure 1. Only two trials met our inclusion and exclusion criteria. Hand searching bibliographies of full text retrievals and related reviews did not identify any additional trials. Two unpublished trials (NCT01285713; NCT02054585) were identified on ClinicalTrials.gov. There were no disagreements regarding study inclusion.

Figure 1. Literature search results.

Study characteristics and RoB

The two included trialsReference Levy, Bachur, Monuteaux and Waltzman18, Reference Sendarrubias, Carron and Molina19 were similar in size and the demographics of enrolled patients. Both trials were performed in the ED and enrolled healthy children with acute gastroenteritis needing IV rehydration as determined by the treating clinician. The average age in each trial was 2–3 years, all patients were diagnosed with gastroenteritis, and children with chronic illness were excluded. The average Gorelick dehydration score was 3–4, which indicates 5%–9% loss of body weight.Reference Gorelick, Shaw and Murphy20 The control solution in both studies was 0.9% saline (NS). The intervention group in Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 received 5% dextrose in NS (D5NS), whereas Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 used 2.5% dextrose in NS (SGNS). Each trial gave a 20 mL/kg bolus of study fluid, with further hydration determined by the treating clinician. The primary outcome in both RCTs appeared to be need for hospitalization, though no outcome was specified as primary by Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 Both studies also reported return visits, change in dehydration scores, and laboratory end points. Further characteristics of each study, including specific inclusion and exclusion criteria, can be found in Table 1.

Table 1. Characteristics of included trials

Although patients and interventions were very similar between studies, the RoB of the two trials was discrepant, with Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 at generally low RoB and Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 at high RoB. Details are summarized in Table 2. Both trials were deemed unclear RoB for selective reporting because adverse events were not defined a priori. Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 was also at unclear risk of “other bias” for baseline differences between the treatment arms favouring the D5NS group, and because 55% of the patients randomized to control (NS) received IV dextrose after the initial bolus, which could bias the results towards null. The study was low RoB in all other domains.

Table 2. RoB of included studies

The study by Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 was an open label trial with unclear methods for randomization and allocation concealment. Other RoB was also rated as high because the study was stopped early after an interim analysis revealed a much lower than expected between-group difference in hospital admissions. The investigators decided to stop the trial after enrolling 145 of a planned 718 children, to propose a larger multicentre study.

Clinical results

Both studiesReference Levy, Bachur, Monuteaux and Waltzman18, Reference Sendarrubias, Carron and Molina19 reported on the primary outcome, and these results were pooled (N = 333). Dextrose containing IV fluid for dehydration did not result in a statistically significant decrease in hospitalization at the index visit when compared with NS (RR 0.83; 95% CI 0.62 to 1.10). These results are summarized in Figure 2. Heterogeneity was low (I 2 = 0), and the results were unchanged when analysed using a random effects model.

Figure 2. Effect on Hospital Admission

Both studies reported on the need for further medical care but used different outcomes. Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 used telephone follow-up at 48–72 hours after ED discharge to assess for unscheduled medical care sought for vomiting or refusal to drink in that timeframe (n = 100), with 12% lost to follow-up. Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 reported on return ED visits among those discharged from the index visit (n = 101). The reason for the return visit was not recorded, and the methods do not describe how this information was obtained. A meta-analysis of these results is displayed in Figure 3 and did not result in a statistical difference in need for additional medical care after discharge (RR 0.54; 95% CI 0.24 to 1.22).

Figure 3. Effect on Revisits

Both studies reported on changes in dehydration scores but used different scales. Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 found no difference in improvement on a “general appearance score” from 1–5. On average, children in both arms of the study improved by 1 point at 3 hours. Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 reported that there was no difference in the change in Gorelick dehydration score between study groups, with children in both arms of the trial improving by 2 points on average after 2 hours. These results could not be pooled. Length of ED stay was reported only in Levy et al.,Reference Levy, Bachur, Monuteaux and Waltzman18 who found no difference between those randomized to D5NS (280 minutes) versus those randomized to NS (288 minutes). None of the other predefined clinical outcomes of this review were reported in either study. Both studies reported that there were no adverse events, but these were not well defined in either trial.

Laboratory results

No cases of symptomatic hypoglycemia were reported, and Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 states that “hypoglycemia was not reported” at all. Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 found that hypoglycemia (blood sugar < 60 mg/dL) was more common in the NS group at 1 hour, but by 2 hours there was no difference, with three patients in each group who were hypoglycemic. None were reported to be symptomatic.

Hyperglycemia (blood sugar > 200 mg/dL) was reported in four SGNS patients and 0 NS patients by Sendarrubias et al.,Reference Sendarrubias, Carron and Molina19 with the timeframe not specified. Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 did not report hyperglycemic events, but the median blood glucose in the intervention arm at 1 hour was 272 mg/dL (interquartile range [IQR] = 221–361). By 2 hours, this had decreased to 154 (IQR = 121–221). No cases were reported to be symptomatic.

Both studies reported change in serum ketones as a secondary outcome. In both trials, dextrose containing fluid resulted in significantly more rapid clearance of serum ketones. Sendarrubias et al.Reference Sendarrubias, Carron and Molina19 found that serum ketones had decreased significantly more at 2 hours in SGNS treated patients than in NS treated controls (p < 0.001). By 4 hours, the difference had diminished and was no longer statistically significantly different (p = 0.08). Levy et al.Reference Levy, Bachur, Monuteaux and Waltzman18 found that D5NS-treated patients had a larger decrease in ketonemia at 2 hours (mean difference 1.6 mmol/L; 95% CI 0.9 to 2.3 mmol/L).

DISCUSSION

This systematic review found that current evidence does not support the addition of dextrose to IV solutions to improve clinical outcomes in healthy dehydrated children with acute gastroenteritis. Due to the limitations of the available evidence, however, no firm recommendations can be made for or against its use. Confidence in the effect estimate of our primary outcome is low and was downgraded for imprecision and RoB. For the outcome of repeat visits, confidence is very low and was downgraded for imprecision, high RoB, and clinical heterogeneity. We suggest that, pending the results of ongoing trials, the use of IV rehydration with or without dextrose is reasonable in this setting.

The two included trialsReference Levy, Bachur, Monuteaux and Waltzman18, Reference Sendarrubias, Carron and Molina19 were performed in the patient group most likely to benefit according to pathophysiology (vomiting children) and did confirm that ketone clearance was faster in dextrose-treated patients. Why this did not result in a clinical benefit is uncertain. It is possible that the improved ketone clearance is too brief to make a clinical impact. This theory is supported by the finding that there was no longer any difference in ketone clearance by 4 hours.Reference Sendarrubias, Carron and Molina19 It is also possible that ketone clearance rate is wholly unimportant, or that the meta-analysis was underpowered to find clinical differences.

Although our review included only two trials,Reference Levy, Bachur, Monuteaux and Waltzman18, Reference Sendarrubias, Carron and Molina19 additional data from RCTs do exist. Seven RCTs have evaluated IV glucose in admitted nonsurgical patients.Reference Akech, Karisa and Nakamya21Reference Tan, Norazilah and Omar27 While none of these trials suggested any clinical benefit with dextrose solutions, most did not report specifics of clinical outcomes. Five of these trials enrolled severely dehydrated children with presumed cholera diarrhea.Reference Gutman, Drutz, Whalen and Watten22Reference Rahman, Bennish, Alam and Salam26 All five reported that time to rehydration was similar between groups, but only one trialReference Juca, Rey and Martins23 gave specific numbers (2.3 v. 2.4 hours). All five studies reported that all patients made a complete recovery. In a very different patient population, Akech et al.Reference Akech, Karisa and Nakamya21 found no difference in outcomes between Ringer's lactate (RL) or half strength Darrow's solution with 5% dextrose (HSD/D5) among malnourished Kenyan children with shock mostly due to diarrhea (mortality 58% HSD/D5 v. 45% RL [p = 0.42]). Tan et al.Reference Tan, Norazilah and Omar27 performed the only trial in any adult population, enrolling 202 patients admitted for hyperemesis gravidarum, and found that D5NS produced similar clinical results to NS. While these inpatient RCTs included almost no quantitative results and were not included in the review, they all support our findings of no benefit with the addition of dextrose.

Our trial registries search identified two additional studies that appear to meet the inclusion and exclusion criteria of this review. One of these (ClinicalTrials.gov NCT01285713) is a small trial that randomized 83 children with gastroenteritis to either NS or D5NS and completed enrolment in 2012. The authors confirmed that the trial has been completed but is not yet published. Although specific results were not available, sensitivity analyses, including the plausible range of results based on information shared by the authors, found that it is very unlikely that its inclusion would change the conclusions of our review. The second trial (ClinicalTrials.gov NCT02054585) is a large multicentre study that plans to randomize 700 children with dehydration and vomiting to either D5NS or NS. It is scheduled for completion in 2019 and should add substantially to what is known about the utility of dextrose in IV rehydration in children.

Limitations

The main limitation of this review is the paucity of data meeting the inclusion criteria. The CIs around the estimate of effect are thus quite wide and include the possibility that dextrose-containing fluids provide a substantial clinical benefit that our analysis was underpowered to detect.

One of the included trials,Reference Sendarrubias, Carron and Molina19 representing almost half of the total patients in the review, was at high RoB. In addition to being an open label study, it was stopped early for futility. It is unclear what effect this may have had on the results, but the effect size of this trial was very similar to that seen in the lower RoB study.Reference Levy, Bachur, Monuteaux and Waltzman18

We chose hospital admission as our primary outcome because it is patient-important, easy to measure, and in acute dehydration, usually reflective of the response to treatment. However, it is not an entirely objective outcome. Factors other than response to rehydration therapy may play a role in the decision to admit or discharge. Social issues, patient or caregiver comfort, access to follow-up care, and financial considerations can all impact the disposition decision, and these considerations may play an even larger role in the decision-making process when dealing with pediatric patients. It is possible that unmeasured imbalances of these factors impacted the results.

We had planned to pool results for multiple clinical outcomes, but many were not reported in one or both of the included studies. Subgroup analyses also could not be performed. All included patients were children with gastroenteritis, and the included studies did not provide information to assess the effect in severe versus mild or moderate dehydration.

There is potential for publication bias. Although we could not assess for publication bias using a funnel plot with only two published studies, we did identify one small, unpublished trial that was completed several years ago. Our search of trial registries did not identify other completed and unpublished trials, but more could exist.

Finally, included studies used different concentrations of dextrose (5% v. 2.5%) in NS as their intervention. These two concentrations of dextrose could perform differently in this clinical scenario.

CONCLUSION

The addition of dextrose to IV rehydration solution has not been shown to decrease hospital admissions, repeat visits for medical care, or result in any clinical benefit among pediatric outpatients with acute dehydration. However, this conclusion is based on two small RCTs at moderate to high RoB, resulting in CIs surrounding the estimate of effect that are wide and include the possibility for substantial benefit. At least one larger trial is underway. No randomized studies in adult outpatients were identified.

SUPPLEMENTARY MATERIAL

The supplementary material for this article can be found at https://doi.org/10.1017/cem.2018.500.

Competing interests

None declared.

References

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Figure 0

Figure 1. Literature search results.

Figure 1

Table 1. Characteristics of included trials

Figure 2

Table 2. RoB of included studies

Figure 3

Figure 2. Effect on Hospital Admission

Figure 4

Figure 3. Effect on Revisits

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