A randomized controlled clinical trial comparing patient/ ER physician satisfaction and ease of administration of 3 non IV routes of midazolam as a rescue medication for seizure control. Study population included children with known seizure disorder who were prescribed midazolam by pediatric neurologist at home and those presenting to ER with following inclusion and exclusion criteria
Recruited patients randomized using previously computer-generated randomization tables prepared by expert statistician. Study was approved by the faculty ethical committee prior to its start and oral informed consent was obtained from the parents. In order to simplify the administration process a reference guide was prepared for doses according to weight for each of the 3 routes. Two major groups were included (home and ER group) and each were subdivided into 3 groups according to route of administration Children was randomly assigned to receive treatment with intranasal, intramuscular or buccal midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) .Intranasal form was administered via a metered dose sprayer at 0.1 mL/spray (i.e. 0.5mg/spray). If the volume to be administered exceeded 1 mL, then the dose was divided between both nostrils to avoid runoff and swallowing. Administration was via sprays in each nostril (for nasal) or dripping between the cheek and the gum per side using insulin syringe (for buccal) or using 3 mm syringe in the front aspect of thigh for intramuscular injection. Caretakers who gave the study medication recorded their observations and answered a series of questions regarding time to drug administration, seizure cessation time, seizure recurrence, need for hospitalization or ER visits and any encountered difficulties or side effects. Ease of administration of was rated using a scale prepared by expert statistian from very easy to very difficult and overall satisfaction with the medication was rated using 10-point nominal scale (0, being not satisfied and 10, greatly satisfied). Seizures that did not cease for ten minutes after drug administration and the need to use additional medication was categorized as a treatment failure criteria. Recruited caretakers who did not spontaneously report the use of the study medication were contacted by phone monthly to address any questions and to remind them of the study. Problems with different routes of delivery were discussed, for example excessive head movements, ryle or upper respiratory tract infections and where possible suggestions and advices to help with addressed issue was provided .If a caretaker reported use of study medication at the time of the phone call, information was obtained at that time. In this group, not all children received a benzodiazepine because of different reasons: unavailability of the drug at home or at school, spontaneous resolution of seizures, difficulty in administrating the drug, or panic. ER doctor given a brief survey after the administration to evaluate sedation, discomfort and other adverse effects of the medication as well as any administration difficulties and data for other secondary outcomes (need for additional medical support, hospitalization, repeated seizures…etc).
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
305
Children from home group assigned to receive treatment with intranasal midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) via a metered dose sprayer at 0.1 mL/spray (i.e. 0.5 mg/spray). If the volume to be administered exceeded 1 mL, the dose was divided between both nostrils to avoid runoff and swallowing
Children from home group randomly assigned to receive treatment with buccal midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) via dripping between the cheek and the gum per side using insulin syringe
Ain Shams Pediatric hospital
Cairo, Egypt
Percentage of participants with therapeutic success
Percentage of participants with therapeutic success defined as cessation of visible seizure activity within 10 minutes (mins) with a sustained absence of visible seizure activity for 30 minutes following a single dose of anticonvulsant agent time frame: from start drug administration up to 30 minutes postdose \] i.e Successful responder (onset of seizure cessation within 10 minutes or duration of seizure control \>30 minutes without seizure relapse), or Unsuccessful/nonresponder (onset of seizure cessation \>10 minutes or duration of seizure control \<30 minutes
Time frame: 30 minutes post drug administration
sustained absence of seizure activity for at least 1 hour
Percentage of participants whose seizure event stopped within 10 minutes of single dose of anticonvulsant and who have sustained absence of seizure activity for at least 1 hour
Time frame: from start of study drug administration up to 1 hour postdose
sustained absence of seizure activity for 4 hour
Percentage of participants whose seizure event stopped within 10 minutes of single dose of anticonvulsant and who have sustained absence of seizure activity for at least 4 hours
Time frame: from start of study drug administration up to 4 hours postdose
sustained absence of seizure activity for 6 hour
Percentage of participants whose seizure event stopped within 10 minutes of single dose of anticonvulsant and who have sustained absence of seizure activity for at least 6 hours
Time frame: from start of study drug administration up to 6 hours postdose
Time to resolution of seizures (convulsions)
Time to resolution of seizures (convulsions) after drug administration Cessation of seizure activity was defined as caregiver/physician-confirmed cessation of abnormal motor activity with at least partial recovery of consciousness
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Children from home group randomly assigned to receive treatment with intramuscular midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) using 3 mm syringe in the front aspect of thigh
Children from the ER group assigned to receive treatment with intranasal midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) via a metered dose sprayer at 0.1 mL/spray (i.e. 0.5 mg/spray). If the volume to be administered exceeded 1 mL, the dose was divided between both nostrils to avoid runoff and swallowing
Children from ER group randomly assigned to receive treatment with buccal midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) via dripping between the cheek and the gum per side using insulin syringe
Children from ER group randomly assigned to receive treatment with intramuscular midazolam with doses of 0.2 mg/kg (maximum, 10 mg) body weight of the standard IV formulation of midazolam (5mg/mL) using 3 mm syringe in the front aspect of thigh
Time frame: 30 minutes
Time of drug preparation and administration
time taken to prepare and administer drug
Time frame: 45 minutes
Emergency department visits
Number of patients from home group who needed to go to ER after drug adminstration
Time frame: 24 hours post drug administration
percentage of patients admitted to hospital
Number of patients that were admitted to the hospital or intensive care unit after their seizure and use of study medication.
Time frame: 24 hours post drug administration
need for additional doses or additional drugs for seizure control
Percentage of participants who required additional anticonvulsant medication for ongoing status epilepticus (se) 10 minutes after single dose administration of anticonvulsant
Time frame: 10 minutes post drug administration
Seizure recurrence at 1 ,4 , 6 and 24 hrs
Seizure recurrence at 1 ,4 , 6 and 24 hrs of cessation of presenting convulsion
Time frame: 24 hours post drug administration
Respiratory depression
persistent decrease in oxygen saturation to \<92% measured at 0, 10 minutes, 30 minutes, and 1, 4 , 6 hrs postdose (ie, \<92% on room air for 2 minutes or more after dosing while monitoring aspiration pneumonia
Time frame: 6 hours post drug administration
Sedation or agitation
• Sedation or agitation measured by a 7 point nominal scale where 1 represented deep sedation and 7 sever agitation
Time frame: 4 hours post drug administration
Frequency of cardio-respiratory side effects
Frequency of cardio-respiratory side effects development of hypotension (fall of \>/= 20 mmhg systolic and/ or \>/= 10 mmhg diastolic pressure) within 0, 10 and 30 mins, 1, 4 , 6 hrs postdose of drug administration
Time frame: 6 hours post drug administration
Occurrence of route of administration and benzodiazepine related side effects
Adverse events, including but not limited nasal irritation, dizziness, Stuffy nose, headache , nausea, agitation , cardiopulmonary dysfunction, ataxia, and abnormal vital signs were recorded
Time frame: 6 hours post drug administration
Caretakers and physicians ease of administration and satisfaction with the medication
Ease of administration of was rated using a scale prepared by expert statistician from very easy to very difficult and overall satisfaction with the medication was rated using 10-point nominal scale (0, being not satisfied and 10, greatly satisfied
Time frame: up to 1 months after drug administration