The goal of this clinical trial is to test the MEX-CD1 hemodialysis medical device in patients suffering from ACLF. The main questions it aims to answer are: * Is the device safe when used according to the instructions for use? * Does the device work as expected by removing the excess of free iron from the blood? Patients will receive 3 MEX-CD1 Slow Low volume CVVHD within 1 week.
This study investigates the safety and performance of the MEX-CD1 slow low volume CVVHD device in patients suffering from ACLF. Acute-on-chronic liver failure (ACLF) is defined as a syndrome in patients with acutely decompensated cirrhosis, associated with single or multiple organ failures, and characterized by a high short-term mortality. ACLF is frequently triggered by a precipitating event (alcoholic hepatitis, infection, gastrointestinal haemorrhage) and characterized by an intense systemic inflammatory response driven per pathogen-associated molecular patterns (PAMPs) and/or damage-associated molecular patterns (DAMPs) responsible of the development of organs failure through tissues hypoperfusion, immune-mediated tissue damages and mitochondrial dysfunction. Very importantly, ACLF is a very dynamic syndrome that has potential for reversibility. It is hypothesized that the extraction of non-transferrin bound iron (NTBI) could break down the vicious cycle of the excessive inflammatory responses, reduce oxidative stress and inhibit pathogen proliferation in ACLF patients. As a consequence, it is hypothesized that the extraction of NTBI could promote improvement of ACLF grade n to ACLF grade n-1 or no ACLF. It is hypothesized that the extraction of NTBI could stop the progression of ACLF by preventing further organ failures and by reducing bacterial infection. Thereby, the extraction of NTBI could restore the eligibility of ACLF patients to liver transplantation, and, with or without liver transplantation, allow an earlier discharge from intensive care and prolong survival. The proposed medical device, by combining dialysis to a hyper-chelating colloidal dialysate (MEX-CD1), specifically extracts free iron from the blood. All patients enrolled in this study will receive 3 MEX-CD1 Slow Low volume CVVHD within 1 week. The duration of each MEX-CD1 Slow Low volume CVVHD session is 3h20.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
MEX-CD1 is a hyper-chelating colloidal solution that can be added to the dialysate to be used in Slow low-volume continuous veno-venous hemodialysis. One treatment will last 3 hours and 20 minutes. Patients enrolled are hospitalized in Intensive Care Unit.
Hôpital Croix Rousse, Service d'hépatologie et gastroentérologie
Lyon, Auvergne-Rhône-Alpes, France
RECRUITINGCHU Pontchaillou
Rennes, France
RECRUITINGSADE for Safety purpose
The safety will be assessed by percentage of subjects who discontinued MexACLF due to a serious adverse device event (SADE) between Day 1 and Day 7.
Time frame: From the enrollment until the last visit, assessed up to 7 days.
SAE for Safety purpose
The safety will be assessed by the percentage of patients who experience at least one related Serious Adverse Event (SAE) between Day 1 and Day 7.
Time frame: From the start of the first MEX-CD1 treatment until the last visit, assessed up to 7 days.
Performance of MEX-CD1
The performance of the MEX-CD1 slow low-volume CVVHD treatment in terms of iron extraction will be measured by the amount of iron extracted in the dialysate bags per treatment.
Time frame: 3 hours and 20 minutes; from treatment start (0 hours) to treatment end (3h20)
Change in Acute on Chronic Liver Failure (ACLF) Grade
Assessment of the change in ACLF Grade between the baseline and the end of study Min value = 0 (no ACLF) Max value=3b (Worse outcome)
Time frame: Between the screening visit and the last visit, assessed up to 7 days.
Change in CLIF-C ACLF score
Assessment of the change in Chronic Liver Failure-Consortium (CLIF-C) ACLF score between the baseline and the end of study. CLIF-C ACLF = 10 × (0.33 × CLIF-C OFs + 0.04 x Age + 0.63 × ln (WBC count)-2) CLIF-OFs= Chronic Liver Failure Consortium Organe Failure Min value=6 (No organe Failure) Max value=18 (6 organe failures)
Time frame: Between the screening visit and the last visit, assessed up to 7 days.
Improvement in individual organ function
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TREATMENT
Masking
NONE
Enrollment
10
Assessment of the change in individual organ function by using the CLIF sequential OF score From 1 (no organe failure) to 3 (worse outcome) for the 6 organes below: Liver ; kidney ; Brain ; Coagulation ; Circulation ; Respiratory
Time frame: Between the screening visit and the last visit, assessed up to 7 days.
Development of secondary infection
Assessment of development of secondary infection by need for new antibiotic therapy
Time frame: Between the screening visit and the last visit, assessed up to 7 days.
Status of ICU
Length of stay in ICU
Time frame: Between the screening visit and the last visit, assessed up to 28 days.
hospital discharge
Length of stay at hospital
Time frame: Between the screening visit and the last visit, assessed up to 28 days.
Mortality
Assessment of the survival rate
Time frame: Between the screening visit and the last visit, assessed up to 28 days.