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Low-dose Arginine-vasopressin Supplementation on Post-transplant Acute Kidney Injury After Liver Transplantation (AVENIR Trial)

Phase 3
Not yet recruiting
Conditions
Acute Kidney Injury Post Liver Transplantation
Interventions
Registration Number
NCT06344442
Lead Sponsor
Assistance Publique - Hôpitaux de Paris
Brief Summary

Liver transplantation (LT) is a high-risk surgery for hemodynamic instability and haemorrhagic shock with a high-risk of acute kidney injury (AKI). Indeed, the incidence of post-transplant AKI exceeds 50% in some series with 15% of patients requiring renal replacement therapy. Acute kidney injury after LT is a predisposing factor for chronic renal failure which is independently associated with higher morbidity and mortality.

Arginine vasopressin (AVP), an essential stress hormone released in response to hypotension, binds to AVPR1a to promote vasoconstriction. Furthermore, it may have nephroprotective effects with a preferential vasoconstriction of the post-glomerular arteriole resulting in increased glomerular filtration

The hypothesis of the present work is that low-dose arginine-vasopressin supplementation reduce posttransplant AKI in liver transplantation.

Detailed Description

Prospective, national multicenter, double-blinded, randomized , controlled superiority trial with two parallel arms : AVP vs Norepinephrine

The primary objective is to demonstrate that intraoperative low-dose supplementation of AVP induces a reduction in posttransplant AKI after liver transplantation

Investigational medicinal product: vasopressin will be administered by continuous infusion. AVP will be used to a final concentration of 0.12 U/ml. The vasopressor infusion will be titrated to maintain an MAP of at least 65 mmHg. The study-drug infusion will be started at 5 ml/h and increased by 2.5 ml/h to achieve a maximum target rate of 30 ml/h, so that AVP doses ranged from 0.01 to 0.06 U/min.

Comparator treatment : norepinephrine will be administered by continuous infusion. Norepinephrine will be used with final concentrations of 120 microg/ml. The vasopressor infusion will be titrated to maintain an MAP of at least 65 mmHg. The study-drug infusion will be started at 5 ml/h and increased by 2.5 ml/h to achieve a maximum target rate of 30 ml/h, so that NE doses ranged from10 to 60 microg/min.

Recruitment & Eligibility

Status
NOT_YET_RECRUITING
Sex
All
Target Recruitment
304
Inclusion Criteria
  • Age ≥ 18 years
  • Any adult patient with a scheduled liver transplantation
  • All participants will need to be given clear information about the study and give signed informed consent.
  • Person affiliated to the Social Security
Exclusion Criteria
  • Super-emergency for liver transplantation or fulminant hepatitis
  • Patient listed for or receiving simultaneous liver-kidney transplantation (SLKT)
  • Patients with end-stage renal disease (chronic eGFR < 15 mL/min/1.73 m2 or requiring extra-renal purification before liver transplantation
  • Patient with epilepsy
  • Hypersensitivity to arginine-vasopressin and to its excipients
  • Patient refusal
  • Patients for whom it is impossible to give informed consent (language barrier)
  • Adults under guardianship or trusteeship, persons deprived of their liberty
  • Patient enrolled in another interventional clinical study
  • Pregnancy or breastfeeding

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Arginine vasopressinArginine vasopressinlow-dose arginine-vasopressin supplementation group: Vasopressin will be administered by continuous infusion. AVP will be used to a final concentration of 0.12 U/ml. The vasopressor infusion will be titrated to maintain an MAP of at least 65 mmHg. The study-drug infusion will be started at 5 ml/h and increased by 2.5 ml/h to achieve a maximum target rate of 30 ml/h, so that AVP doses ranged from 0.01 to 0.06 U/min
NorepinephrineNorepinephrineNorepinephrine will be administered by continuous infusion. Norepinephrine will be used with final concentrations of 120 microg/ml. The vasopressor infusion will be titrated to maintain an MAP of at least 65 mmHg. The study-drug infusion will be started at 5 ml/h and increased by 2.5 ml/h to achieve a maximum target rate of 30 ml/h, so that NE doses ranged from10 to 60 microg/min.
Primary Outcome Measures
NameTimeMethod
The primary objective is to compare the effect of intraoperative low-dose supplementation of AVP vs norepinephrine infusions on post-transplant Acute Kidney Injury after liver transplantation.during the first 7 postoperative days

The stages of AKI according to AKI Network criteria (KDIGO score) determined by changes in serum creatinine and changes in urine output.

Secondary Outcome Measures
NameTimeMethod
To compare into the two arms the number of packed red blood cellsand fresh frozen plasma transfusedduring the first 12 hours postoperatively
To compare into the Number of AKI KDIGO 3during the first 7 postoperative

defined as increase in serum creatinine concentration ≥ 3 fold or ≥ 4mg/dl (or 354 micromol/L) or urine output \<0.3 ml/Kg/h for ≥24h or anuria\>12h)

To compare into the two arms the number of the Number of AKI KDIGO 11 during the first 7days

defined as increase in serum creatinine concentration by 1.5 to 1.9 fold or ≥0.3mg/dl (or 27 micromol/L) within 48h or urine output \<0.5 ml/Kg/h over a period 6-12 h)

The need for renal replacement for replacement therapy (RRT) in ICUduring the first 7 days postoperatively and on postoperative day 30
The number of patients remaining on dialysis at the end of the studyon the 30th Day
Mortalityat 30 days
To compare into the two arms the Number of AKI KDIGO 2during the first 7 postoperative

defined as increase in serum creatinine concentration by 2.0 to 2.9 fold or urine output \<0.5 ml/Kg/h over a period ≥12 h)

Average intraoperative norepinephrine concentrationsintraoperative
Number of platelets transfused intraoperativelyduring the first 12 hours postoperatively.
Average intraoperative concentrations of other vasopressors and inotropes (Adrenalin, Dobutamine)intraoperative
Amount of vascular filling solutions intraoperativelyDuring the first 12 hours postoperatively.
Number of days alive outside intensive care unitduring the 30 day post-operation
Sequential Organ Failure Assessment (SOFA score)On the third and seventh postoperative day

Sequential Organ Failure Assessment (SOFA score between 0 and 24). Zero indicates that the patient has no organ dysfunction, twenty-four is the maximum score and indicates that the patient has vinght four is the maximum score and indicates that the patient has all 6 of the organ dysfunctions explored.

(respiratory, coagulatory, liver, cardiovascular, renal, and neurologic)

Trial Locations

Locations (1)

URC Lariboisière-Fernand Widal-saint Louis

🇫🇷

Paris, France

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