Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT03799770 |
| Other study ID # |
R.18.12.369 - 2018/12/16 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
|
| First received |
|
| Last updated |
|
| Start date |
January 1, 2019 |
| Est. completion date |
March 23, 2021 |
Study information
| Verified date |
April 2022 |
| Source |
Mansoura University |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Observational
|
Clinical Trial Summary
This is a diagnostic test accuracy study. The investigators measure optic nerve sheath
diameter (ONSD) by ultrasound on the eye during living donor liver transplantation operation
at 5 minutes after reperfusion to predict the occurrence of early tacrolimus neurotoxicity
after liver transplantation.
We measured the ONSD at 4 timings: (T1) Post induction and before surgical incision, (T2)
Portal vein clamping, (T3) 5 minutes after reperfusion, and (T4) 30 min after reperfusion.
Description:
Neurotoxicity is mainly associated with tacrolimus and cyclosporin, amounting to 10 - 30% for
CS and up to 32% for tacrolimus.(2) . Sirolimus, everolimus, and mycophenolate mofetil lack
the neurotoxicity of calcineurin inhibitors (3-4).
Neurotoxicity mostly occurs in the early postoperative period increasing morbidity, mortality
and hospital and intensive care stay. Neurotoxicity has variable manifestations and mainly
affects the CNS. They are usually divided into minor manifestations as tremor, headache,
insomnia and paraesthesia or major encephalopathy, akinetic mutism, seizures, speech
disorders, polyneuropathy, myopathy, pseudobulbar palsy and even stroke. (2) The main
pathogenesis of calcinurin inhibitors neurotoxicity appears to be fluid extravasation
(vasogenic edema) due to disruption of blood brain barrier, not cell destruction (cytotoxic
edema).(5) During liver transplant operation there are changes in the intracranial pressure
and cerebral perfusion pressure especially during reperfusion that may affect the integrity
of blood brain barrier. (6) There are multiple methods for monitoring of intracranial
pressure invasive or non -invasive. The invasive method remains the gold standard for
monitoring of intracranial pressure but there is a controversy about its use in liver
transplantation as it may be complicated by bleeding and infections (7).
Also there are a multiple non-invasive methods for monitoring of ICP. Ultrasonographic
measurement of the optic nerve sheath diameter (ONSD) was introduced recently as a useful
noninvasive method for evaluating ICP. ONSD demonstrated a good correlation with the ICP
level in many previously published studies. (8,9) Rajajee et al. found that the optimal
cutoff of ONSD for the detection of an acutely increased ICP > 20 mm Hg was greater than 4.8
mm. (10) We hypothesize that the absolute value or the changes of ONSD during different
stages of living donor liver transplantation operation may predict occurrence of early
calcinurin inhibitor neurotoxicity (CNIN).We will investigate whether the absolute value or
changes of ONSD during different stages of living donor liver transplantation operation may
be a predictor of early calcinurin inhibitor neurotoxicity in the first month post liver
transplantation. This is a prospective observational cohort study that will be conducted to
all adult patients of both sex undergoing living donor liver transplantation operation at
Gastro-Intestinal Surgical Centre (GISC), Mansoura university Hospitals, Mansoura, Egypt over
the period covering more than 100 consecutive cases. After Institutional review board
approval, we will secure informed consents from all included patients during the preoperative
visits.
Anesthesia and surgery techniques will be done according to our center's protocol.(11)
Reperfusion:
On portal vein declamping, we will start rapid 500 ml 4% albumin infusion or packed RBCs
(according to the anhepatic hemoglobin level 5 min before declamping) through 14 Gauge
peripheral venous cannula in all patients.
For hypotension we will give norepinephrine and for resistant hypotension we will use
adrenaline as rescue.
Technique of ONSD:
Sonographic measurement of ONSD was performed with the same manner of previous studies.
Patients were placed in the supine position with their eyes closed, and a thick gel layer was
applied to the closed upper eyelid. The 7.5-MHz linear probe was placed on the gel without
excessive pressure and adjusted to the proper angle for displaying the entry of the optic
nerve into the globe. The intensity of the ultrasound was adjusted to display optimal
contrast between the retrobulbar echogenic fat tissue and the vertical hypoechoic band. An
ultrasound beam was focused on the retrobulbar area using the lowest possible acoustic power
that could measure ONSD. The ONSD was measured 3 mm behind the optic disc. Measurements were
performed in the transverse and sagittal planes of both eyes, and the final ONSD value was
calculated by averaging 4 measured values. (8)
Immunosuppression:
All patients will receive intravenous 0.5 gm methylprednisolone at the start of the warm
ischemia. After hepatic artery anastomosis and declamping, we will administer 500 mg
mycophenolate mofetil through the nasogastric tube and i.v. 20 mg basiliximab.
In the ICU, patients will receive oral tacrolimus starting the day after the operation
(adjusting the dose targeting serum level of 5-10 ng/ml) , mycophenolate mofetil 500 mg twice
per day and basiliximab 20 mg iv 4 days after.
