Efficacy of Nebulised Hypertonic Saline (3%) Among Children With Bronchiolitis.

Bronchiolitis Clinical Trial

Official title:

Efficacy of Nebulised Hypertonic Saline (3%) Among Children With Mild to Moderately Severe Bronchiolitis - A Double Blind Randomized Controlled Trial.

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT01276821
• Other study ID #: PEDSTUTHIOM
• Status: Completed
• Phase: Phase 4
• First received: January 12, 2011
• Last updated: April 23, 2013
• Start date: January 2011
• Est. completion date: April 2011

Study information

• Verified date: April 2013
• Source: Tribhuvan University Teaching Hospital, Institute Of Medicine.
• Contact: n/a
• Is FDA regulated: No
• Health authority: Nepal: Health Research Council
• Study type: Interventional

Clinical Trial Summary

To assess the efficacy of nebulized 3% hypertonic saline in improving clinical severity scores among children aged 6 weeks to 24 months with bronchiolitis.

Description:

Introduction and Rationale:

Bronchiolitis is a common problem with significant morbidity, and occasional mortality among young infants. Diagnostic testing, indications for hospitalization, eligibility criteria for discharge and therefore, the length of hospital stay for bronchiolitis vary globally, suggesting a lack of consensus and an opportunity to improve care for this common disorder. Likewise, despite the frequency of this condition there is no single, widely practiced, evidence-driven and universally accepted therapeutic guidelines other than supportive care. Recent studies have shown promising results regarding the role of nebulised 3% hypertonic saline in the treatment of bronchiolitis.

This therapy might obviate the need for hospital admission and reduce the length of hospital stay, if found effective. The implications of this would be that children return home early and parents return to work earlier, resulting in reduction of the morbidity and cost associated with the disease.

Trial Design This study was a prospective, interventional, parallel-assigned, double-blind, (subject,caregiver, investigator, outcome assessor) randomized controlled trial.

Ethical Clearance The study was approved by Institutional Review Board and Ethics Committee, Tribhuvan University Teaching Hospital, Institute of Medicine as well as The Institutional Review Board of Kanti Children's Hospital.

Study Participants Subjects were recruited from previously healthy children aged 6 weeks to 24 months visiting the Emergency Room and Out-Patient Department of Kanti Children Hospital with first episode of bronchiolitis.

Bronchiolitis was clinically defined as per the AAP consensus guidelines as the first episode of acute wheezing in children less than two years of age, starting as a viral upper respiratory infection (coryza, cough or fever).

Study setting The study was carried out in the Emergency Room, Observation and Out-Patient Department of Kanti Children Hospital, Kathmandu, Nepal. Recruitment occurred at the peak of bronchiolitis season in between January 15th to April 15th for duration of 4 months.

Interventions Patient enrollment occurred on weekdays (Sunday to Friday) between approximately 08.00 and 17.00 hr when, after the initial assessment, the attending pediatrician (non-study physician) called the investigator. The investigator assessed the children for eligibility, examined the children and assigned a clinical severity score described by Wang et al.

Children meeting inclusion criteria were invited to participate in the study and written informed consent was obtained from a parent or guardian.

General condition, weight, temperature, respiratory rate, heart rate, SpO2 and presence/absence of clinical dehydration were assessed in all patients and Clinical Severity score was calculated as described by Wang et al. Patients determined to be in life threatening condition were immediately managed for same and were not further considered for study.

Preparation of study drugs was done by a faculty appointed by the Department of Child Health and administration was done by an ER/OPD nurse or the investigator, and compliance with medication administration was assured by the investigator's direct observation of each nebulization.

All eligible patients were randomly assigned to one of the two groups:

1. Group 1 (n = 50) received inhalation of L-Epinephrine 1.5 mg, diluted to 4ml with 3% Hypertonic Saline (HS) solution;

2. Group 2 (n=50) received inhalation of L-Epinephrine, 1.5 mg, diluted to 4ml with 0.9% Normal Saline solution.

The study drug was administered at 0 and 30 min by jet nebulizers using a face mask. Prior to each drug administration and at 30, 60 and 120 min, the investigator assessed the children's general condition and recorded the CS score, SpO2 in room air, respiratory rate 60 and heart rate. All patients received the first dose of nebulization within 15- 30 minutes depending upon the time required for preparation and enrollment.

Adverse events were defined as heart rate >200, tremor, withdrawal from the study due to worsening clinical status, or discontinuation of any study medications due to side effects.

Patients were excluded from the study if the administration of the 2 courses of nebulisation was not delivered, the study drug was delayed by 10 min or more (protocol deviation) or if clinical deterioration mandated escalation of therapy and/or support.

At the end of the observation period, the attending pediatrician determined the need for hospital admission.

The parents of the patients enrolled in the study were asked to follow up after 24 hours in the OPD for repeat assessment. If the parents were not available for follow up, the investigator contacted the parents or guardians via telephone 24 hours after their ED/OPD discharge to determine the need for any unscheduled hospital visit within the next 24 hours of OPD/ ER visit: their readmission (relapse) rate.In addition, they were reassessed at the end of 1 week by telephone contact . A single investigator participated in the measurement of observations to minimize inter observer variability. All calls were made from the Hospital reception Office at appropriate times 10:00a.m. - 14:00p.m NST. Patient were labeled as Lost-to-Follow up if there was failure to communicate for 3 consecutive attempts for 2 consecutive days at their 7th and 8th day of initial presentation to the OPD/ER.

Sample Size Estimation:

Sample size was determined by the following formula :

• n = [(z1 +z2)² (Ó1² + Ó2²) ] / (û1 - û2)²

• Allowing a Type1 error of 5% (α :0.05), z1 score : 1.96.

• For a Power of 95%, z2=1.64.

• Standard deviation of the Clinical Severity Score : 1.3

• Mean Change in Clinical Severity Score between the two interventions to consider clinically significant : Change in Clinical Severity Score of 1

• The study proposed that a difference of 1 point in the Clinical Severity Score between the two intervention groups would be considered Clinically Significant.

• To detect this mean difference of 1 unit in the Clinical severity score, with a Power of 95%, a Sample size of 44 in each intervention group were required.This made a total of 88 patients to be enrolled in the study.Considering the drop out/ lost to follow up to be approximately 10%, 100 patients were enrolled, allowing 50 in each group.

• Standard deviation of the Change in clinical severity score was derived from previous studies and taken as 1.3 .

Randomization

1. Sequence Generation A Random Allocation Software generated by computer, identified patients by a triple digit mixed numeric code was used by the study coordinator to allocate patients to treatment groups, and the study coordinator was the only person with access to the randomization.

2. Type of Randomization Block Randomization method was used to stratify patients into blocks of 10 each, each comprising of 10 patients.

Allocation Concealment After preparation, the study solutions were labeled with the codes and wrapped in an envelope with the respective codes and attached with the proforma bearing the respective codes.Study solutions were identical in appearance and odor. The identity of the study solutions was blinded to all participants, care providers, and investigators and outcome assessor.

Implementation The randomization process was done by the study coordinator (not involved in the study) and he was the only person to have access to the codes.

The study solutions were stored in the non-freezer compartment of the refrigerator at a temperature of 2-8*C and were discarded if not used within 72 hours of preparation.

Blinding The study was a Double Blind Randomized Controlled Trial with the investigator, the participants, the nurses who delivered the drug, and the outcome assessor being blinded to the therapeutic option.

Statistical Methods The primary outcome was to detect the difference in mean change in Clinical Severity score between the two intervention groups. A power analysis revealed that, for detection of the difference of 1 unit in CS score between the 2 treatment groups, with α of 0.05 and power of 95%, we required 88 patients (44 per group).

A sample size of 100 patients was therefore chosen, with 50 patients in each group considering the possibility of loss to follow up.

Statistical analysis was performed using SPSS for Windows, Release 16.0 (SPSS Inc., Chicago, IL). Dichotomous events were analyzed by using the Chi-Square test.Dependent variables were compared by Student t-test. Statistical significance was defined as p-value < 0.05.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 100
• Est. completion date: April 2011
• Est. primary completion date: April 2011
• Accepts healthy volunteers: No
• Gender: Both
• Age group: 6 Weeks to 2 Years

Eligibility

Inclusion Criteria:

• Age 6 weeks to 24 Months.

• First episode of wheezing

• Fever, cough and watery nasal discharge

Exclusion Criteria :

• Any underlying cardiovascular disease.

• Prior wheezing.

• Clinical Severity Score > 9.

• Atopic dermatitis, allergic rhinitis or asthma.

• Oxygen saturation (SpO2) <85% on room air.

• Obtunded consciousness.

• Previous treatment with bronchodilators within 4 hours.

• Any steroid therapy within 48 Hours.

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment

Related Conditions & MeSH terms

• Bronchiolitis

Intervention

Drug:
• L-Epinephrine and Normal Saline (0.9%)
1.5ml of 1:1,000 L-Epinephrine and 4 ml of 0.9% Normal Saline
• L-Epinephrine and Hypertonic Saline (3%)
1.5ml of 1:1,000 L-Epinephrine and 4 ml of 3% Hypertonic Saline

Locations

Country	Name	City	State
Nepal	Out Patient Department and Emergency Department, Kanti Children Hospital	Kathmandu	Bagmati Zone

Sponsors (1)

Lead Sponsor	Collaborator
Dr. Aayush Khanal, MD

Country where clinical trial is conducted

Nepal, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Other	Average Duration of Crying (in Minutes) Among Babies Receiving Nebulisation Therapy.	The outcomes tries to compare the influence of duration of crying among babies receiving nebulization which interferes with drug delivery and henceforth might create a confounding bias while interpreting results.	2 hours	No
Primary	Mean Change in Clinical Severity Score	Mean changes in the Clinical Severity Score after 2 sessions of nebulisation as compared to baseline.; Clinical Severity Score devised by Wang et al, is an objective scoring system that measures the degree of respiratory distress in young children.; The scoring system assesses respiratory rate, wheezing, retraction, and general condition,scores ranging from 0 to 3, with higher scores indicating severe illness and vice versa.; The total scores range from 0 to 12, with increased severity receiving a higher score (Wang et al, 1992).; This scoring systems have previously been validated in a number of well designed randomized controlled trials(Anil 2010, Kuzik 2007, Sarrell 2002, and Mandelberg 2003). A 1 point improvement in the clinical severity score implies approximately 7% betterment of symptoms on the scale.	2 hours	No
Secondary	Patients Meeting Eligibility Criteria for ER/ OPD Discharge at the End of 2 Hours of Observation		At the end of 2 hours	No
Secondary	Relapse Rate	To study the number of patients in either group who need another unscheduled medical visit within the initial 24 hours of ER/ OPD visit	24 hours	No
Secondary	Need for Unscheduled Medical Visits, if Any, for Same Symptoms to Any Healthcare Facility Within 1 Week		7 days	No
Secondary	Missed Days of Work of Caregivers	Number of patients in each intervention group whose parents reported at least 1 day of missed work due to the illness of child within the week following the initial hospital visit on 7 day follow-up call.	7 days	No
Secondary	Persistence of Cough at the End of 1 Week	Number of patients in each intervention group whose parents reported the persistence of initial cough at the end of 1 week in their children.	7 days	No