In this prospective randomized
controlled trial we aim to evaluate the impact of early initiation of CRRT on
outcomes in patients with acute liver failure with cerebral edema and
hyperammonemia in improving cerebral edema and clinical outcomes. We also aim
to evaluate the effects of early initiation of CRRT on systemic hemodynamics
(cardiac output and systemic vascular resistive index, extravascular lung water
and lung permeability index), endothelial function and coagulation,
microcirculation (as assessed by lactate clearance and central venous oxygen
saturation), mitochondrial function. Patients with ALF who meet the inclusion
and exclusion criteria.
Group 1: CRRT initiation within
the first 12 hours Group 2: CRRT would be initiated i) In patients with worsening
hyperammonemia despite two sessions of plasma-exchange ii) Patients meeting
renal indications (hyperkalemia, volume overload, oliguria or metabolic
acidosis etc)
Hypothesis: We hypothesize that
preemptive administration of continuous renal replacement therapy would be
synergistic to plasma-exchange in ameliorating the cytokine storm, cerebral
edema and improve outcomes in patients with non-acetaminophen ALF with cerebral
edema compared to late initiation.
Aim and Objective -
AIM:
Primary
1) 21-day transplant free
survival with Prometheus Secondary
To compare the improvement effect
in cerebral edema and hepatic encephalopathy in both groups
To study the safety of therapy
(incidence of intradialytic hypotension, impairment of coagulation,
hypothermia)
Duration of mechanical
ventilation and ICU stay in both groups
Impact on arterial lactate
Improvement in SIRS
Effect on systemic hemodynamics
and pulmonary function
Effect on endotoxin, DAMPS,
pro-inflammatory cytokines, endothelial functions and coagulation
Methodology Study Protocol
All patients will be evaluated as
follows:
Clinical history and examination
Etiology of acute event
Severity assessment indices
Complications if any
Investigations Arterial blood gas analysis
Hematology
CBC, Prothrombin time and INR
Peripheral smear, Retics
Thromboelastogram(ROTEM)
S.Fibrinogen level
Biochemistry
Liver function testing
Kidney function test
Arterial ammonia levels
Serum lactate
CRP and procalcitonin
S.Ferritin and LDH
Etiology of acute event:
Infectious etiology: IgM anti
HAV, IgM anti HEV, IgM anti HBc ( If HBsAg +ve), IgM anti HDV ( If HBsAg +ve) ,
total antiHBc, anti HCV
Non Infectious etiology: Alcohol
binging in last 4 weeks, hepatotoxic drugs, ANA (>1: 80), IgG
Non infectious etiology:
Autoimmune markers, copper studies, iron studies, HOMA IR, FBS Imaging USG
abdomen with Doppler for spleno-portal axis NCCT abdomen and brain Assessment
of cerebral edema
Optic nerve sheath diameter
Transcranial doppler
Electroechocardiogram
Study Population: 60 patients
with ALF will be randomized to two groups in 1:1 ratio.
Study Design:
A randomized controlled study.
The study will be conducted on
patients admitted to Department of Hepatology from May 2021 to March 2023 at
ILBS, New Delhi
Study group will comprise of
patients with acute liver failure (ALF) with documented cerebral edema on
CT-scan and arterial ammonia >150 ug/dl Study Period: May 2021 to March 2023
Sample Size calculation: Currently there are lack of studies investigating the
timing of CRRT in patients with ALF therefore a minimum of 60 patients 30 in
each group would be included in the current study.
The detailed cytokine profile,
endotoxin assay, markers of endothelial dysfunction and bioenergetics would be
performed in a subset of 10 patients in each group.
Intervention: Continuous renal
replacement therapy
Monitoring and Assessment: Hourly
till the patient is in the intensive care unit then every 7 days for 1 month
Statistical analysis
All variables shall be expressed
in median (range). Variables will be compared by Mann- Whitney U test. For
Categorical variables we will use Chi-Square or Fisher’s test. Survival
analysis will be done using cox-proportional regression analysis. Actuarial
probability of survival shall be calculated by Kaplan- Meier graph and compared
by log- rank test.
Standard medical treatment: All
patients will undergo plain CT-scan of the brain to screen for the presence and
severity of cerebral edema in the emergency before being shifted to the L-ICU.
In the L- ICU, patients will be managed by a multidisciplinary team. Intubation
and ventilation will be undertaken for standard indications in addition to the
development of grade 3 encephalopathy or evidence of cerebral edema on CT-scan.
Ventilation will be managed by fentanyl and propofol along with the use of
atracurium for paralysis wherever required. All patients will be monitored
constantly for macro-hemodynamics, global tissue perfusion, and
microcirculation. The macro-hemodynamic parameters included continuous
monitoring of mean arterial pressure (MAP), heart rate and urine output per
hour. The real-time monitoring of systemic vascular resistance (SVR), stroke
volume variation (SVV), cardiac index (CI) and cardiac output (CO) will be done
by a hemodynamic monitor (FloTracâ„¢ system 4.0, Edwards Lifesciences,
California, US) wherever feasible. Global tissue perfusion adequacy and
indirect assessment of microcirculation will be done by measurement of arterial
lactate. Fluid management will be done with crystalloids, with the use of
colloids (5% albumin) in patients with severe hypoalbuminemia (serum albumin
less than 2.5gm/dl). Norepinephrine will be the primary vasopressor used to
target a mean arterial pressure of 65-70 mm of Hg. with adjunctive use of
intravenous low dose hydrocortisone and vasopressin in patients not responsive
to initial therapy.
Cerebral edema: The monitoring of
cerebral edema will be performed measuring the optic nerve sheath diameter
(ONSD) in both the eyes using a 7.5 MHz probe every 6-8 hours. Apart from this,
routine monitoring of pupillary size and reactions, extensor posturing and
plantar reflexes will be performed every 6-8 hrs. Transcranial doppler would be
done every 6-8 hours. Patients will receive 3% hypertonic saline as a
continuous infusion, initially started at 25ml /hr and titrated 6 hourly to
between 5 and 20 mL per hour (maximum 100 ml/hour) to achieve serum sodium
levels between 145-150 mmol/L. Intravenous 20% mannitol (1 g/kg IV bolus) over
20 to 30 minutes will be administered to those without renal failure. All
patients will in addition receive intravenous N-acetylcysteine for 5
day.Routine electroencephalogram (EEG) will be done for all patients daily to
screen for non-convulsive seizures which will be managed by intravenous
levetiracetam. Assessment of coagulation will be performed by ROTEM at baseline
and subsequently as required.
Protocol for standard-volume
plasma-exchange
Standard-Volume Plasma Exchange:
SVPE procedures will be performed using either Spectra Optia (SPO, Terumo BCT,
Lakewood, CO, USA) continuous-flow centrifugal apheresis system or Haemonetics
MCS+ (Braintree, MA, USA) intermittent flow centrifugal apheresis system via a
double-lumen central venous dialysis catheter. All patients will receive plasma-exchange
within first 6 hours of admission to the L-ICU along with a target volume of
1.5 to 2.0 plasma volumes per session. The replacement fluid used will be 90%
FFP and 10% normal saline.PE will be performed on consecutive days until the
desired response is achieved. [using our previously published protocol].
The number of sessions of SVPE in
each patient will be decided based on the clinical response to SVPE. Dynamic
assessment of the clinical parameters (signs of CE as assessed by pupillary
size, reaction, and optic nerve-sheath diameter), INR, lactate and arterial
ammonia will be performed at after each TPE. In patients with an improvement in
INR, and signs of CE along with a reduction in ammonia at 6 hours which was
sustained at 12 and 24 hours post-SVPE, subsequent sessions will be
discontinued. PE will also be discontinued in patients who would show worsening
in either clinical and/ or biochemical parameters. In patients who will develop
adverse events, the PE procedure will be resumed or discontinued depending on
the severity of adverse event and its resolution.
Randomization will be done by
taking 1:1 ratio by computer-generated sealed envelopes by the clinical trial
co-ordinator Group 1-Preemptive CRRT: In patients randomized to early CRRT,
CRRT would be initiated within 12 hours of randomization.
Group 2: SMT - In patients
randomized to SMT group, CRRT would be initiated as per the existing standard
protocol.
in patients with worsening
hyperammonemia despite two sessions of plasma-exchange patients meeting renal
indications (hyperkalemia, volume overload, oliguria or metabolic acidosis
etc).
The time to initiation of CRRT
would be recorded in both groups after randomization.
Continuous renal replacement
therapy will be administered as continuous venovenous hemodiafiltration
(CVVHDF) using Prisma and Prismaflex (Gambro) devices, with blood flows ranging
from 150-180 mL/hr and target effluent rates of 20 - 25 mL/kg/hr.
Anticoagulation was not used during dialysis. CRRT would be continued until
resolution of cerebral edema and in decrease in ammonia levels below 150 ug/dl
or in those who develop adverse effects of therapy.
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