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Neurostorming is a sudden and exaggerated stress response as a result of damage to the brain. With appropriate treatment and time, there is hope for individuals to overcome storming, regain consciousness, and work towards successfully recovering from brain injury. Most treatments for neurostorming involve the use of medications only such as dexmedetomidine, opioids, gabapentin and propofol to address secondary complications like high blood pressure and fever. These medications focus on slowing the body's stress response or relaxing the body. Stellate ganglion block (SGB) is a promising therapy for paroxysmal sympathetic hyperactivity (PSH), overcoming the limitations of systemic medications and may serve to recalibrate aberrant autonomic states. Ketamine is a potent dissociative agent which has sedative, analgesic and anesthetic properties beside its sympathomimetic effect. Its combination with stellate ganglion block is to oppose its sympathomimetic effect. Dexmedetomidine has analgesic and sedative effect which inhibits the sympathetic nerve activity through its action on the α2 receptor in the spinal cord. Hypothesis: Null hypothesis: There is no difference between the effects of stellate ganglion block combined with dexmedetomidine or subanesthetic ketamine infusion for treatment of neurostorm after traumatic brain injury in critically ill patients.Alternative hypothesis: There is a difference between the effects of stellate ganglion block combined with dexmedetomidine or subanesthetic ketamine infusion for treatment of neurostorm after traumatic brain injury in critically ill patients.which has sedative, analgesic and anesthetic properties beside its sympathomimetic effect. Aim of the work is achievement of effective treatment for the neurostorm after traumatic brain injury in critically ill patients with better outcomes and decrease intensive care unit (ICU) stay.
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PATIENTS AND METHODS
I. Technical Design:
Site of study:
This study will be carried out in the emergency intensive Care unit (ICU) of Zagazig University Hospitals within 6 months.
Sample size:
The sample size was collected using G power version 3.1.9.7 according to the following expected moderate effect size between stellate ganglion plus dexmedetomidine group (SD group) and stellate ganglion block plus ketamine group (SK group) (d=0.5) CI 95% and power 80% the sample size was calculated to be 102,51 in each group.
Patients included in this study:
Inclusion criteria:
Exclusion criteria:
Withdrawal criteria:
The patient has the right to withdraw from the study at any time without any negative consequence on their medical treatment plan.
II. Operational Design:
Type of study:
Double-blinded randomized clinical trial.
Parameters of the study will include:
All patients suspected of having PSH will underwent detailed clinical history and physical examination. Hemodynamics monitoring including heart rate and mean arterial pressure (MAP) also temperature monitoring will be done as base line before the block and after stellate ganglion block every one hour over 24 hours until remission (till return to normal values for age and sex). These patients will be also subjected to routine hematological investigations including, complete blood count, kidney and liver function test, coagulation profile, urine analysis for myoglobinuria and thyroid profile. septic screening including, blood, urine, tracheal aspirate and sputum culture and radiological assessment by using chest x-ray.
All patients developing PSH will be randomly allocated by using computerized generated randomization table into two groups:
SD group: Stellate ganglion block and 1 ug/kg/h intravenous Dexmedetomidine infusion.
SK group: Stellate ganglion block and 0.5 mg/kg/h intravenous ketamine infusion.
Stellate ganglion block :
Patients will undergo an ultrasonography-guided SGB at bedside under standard American Society of Anesthesiologists monitoring standards. The patient will be placed in supine position with the head turn to the opposite side. The anterior and lateral parts of the neck will be prepped with chlorhexidine, and a linear (13-6 MHz) ultrasound probe will be applied to the anterolateral neck at the cricoid cartilage level to identify the transverse process of C6 and C7, anterior tubercle of C6 (Chassaignac tubercle), longus colli muscle and surrounding neurovascular structure. The needle will be advanced with an in-plane technique and aimed to deposit the local anesthetics medial to the Chassaignac tubercle and anterior to pre-vertebral fascia of longus colli muscle. After that, a catheter will be advanced through the needle and secured in place. After aspiration, 10 ml of bupivacaine 0.25% solution will be injected through the catheter and repeated every 48 hours till time of remission.
a. Data to be measured:
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Inclusion criteria
Exclusion criteria
Known hypersensitivity to study drugs. 2) Patients with primary brain stem injury or brain stem hemorrhage 3) Severe systemic organ diseases. 4) GCS score =3 points 5) Patients complicated with severe coagulation abnormalities, hemorrhagic shock, multiple organ failure.
Patients with a history of cerebral hemorrhage or cerebral infarction within the past 3 months. 7) Patients complicated with a history of end stage malignancy.
Patients complicated with a history of uncontrolled epilepsy.
Primary purpose
Allocation
Interventional model
Masking
205 participants in 2 patient groups
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Data sourced from clinicaltrials.gov
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