Rhabdomyolysis Clinical Trial
Official title:
A Randomized Factorial Trial of N-Acetylcysteine and Continuous Veno-Venous Hemo(Dia)Filtration for Rhabdomyolysis
Rhabdomyolysis has many causes including trauma, muscle crush injuries, lack of blood supply
to an arm or leg, burns, seizures, drugs and hereditary disorders. Rhabdomyolysis causes the
breakdown of muscle cells and the release of a molecule called myoglobin. Myoglobin is very
harmful to the kidneys and can lead to kidney failure.
Continuous dialysis has been shown to remove the myoglobin molecule from the blood in
patients with rhabdomyolysis. N-Acetylcysteine (NAC) has been used in patients receiving
contrast dye for x-rays and has shown less worsening of kidney function compared to patients
not receiving NAC.
Early and aggressive treatment of patients with rhabdomyolysis with standard therapy,
continuous dialysis and a drug called N-acetylcysteine (NAC) may prevent the development of
acute kidney failure. Patients who develop kidney failure from this disorder are often
critically ill and have a much higher chance of not surviving than those who do not develop
kidney failure.
The purpose of this study is to determine if the use of NAC and Continuous Veno-Venous
hemo(dia)filtration (CRRT)early in the course of rhabdomyolysis (in addition to standard
therapy)decreases the chance of developing acute renal failure
Rhabdomyolysis may be defined as a clinical or biochemical syndrome which may result from a
large variety of diseases, trauma, or toxic insults to skeletal muscle. The damage to the
integrity of the sarcolemma of skeletal muscle leads to the release of potentially toxic
muscle cell components into the circulation, specifically myoglobin into the plasma.
The three main principals of therapy for myoglobinuric renal failure include 1) correction
of hypovolemia/ renal ischemia, 2) increase the clearance of heme proteins from both the
circulation and the kidneys, 3) attenuate the adverse effects of heme proteins on the
proximal tubule epithelium. Consequently, therapy for rhabdomyolysis is limited to
aggressive rehydration with Ringer's lactate or normal saline, forced diuresis with
mannitol, and urinary alkalinization with intravenous bicarbonate.
Hypothesis
1. The use of N-acetylcysteine (NAC) and continuous veno-venous hemo(dia)filtration (CRRT)
early in the course of rhabdomyolysis as an adjunct to 'standard therapy' (rehydration,
mannitol diuresis, systemic alkalinization) respectively decreases the nephrotoxicity
and improves elimination of systemic myoglobin. Consequently both therapies
independently prevent the deterioration of renal glomerular and tubular function and
establishment of acute renal failure.
2. There exists a positive interaction between the use of N-acetylcysteine and CRRT in the
prevention of acute renal failure secondary to rhabdomyolysis.
Objectives Primary objective is to compare creatinine and myoglobin clearance as well as the
glomerular filtration rate over the course of 192 hours in patients with rhabdomyolysis
treated with NAC, early CRRT, both CRRT and NAC or neither of the two therapies. Secondary
objectives are to : 1) Compare excretion of urine B-NAG, B1-macroglobulin, and microalbumin,
as indicators of renal tubular and glomerular damage over the course of 192 hours in
subjects with rhabdomyolysis treated with NAC, early CRRT, both therapies, or neither
therapies 2) To compare ICU and hospital mortality and length of stay as well as the
proportion of subjects with recovery of renal function at 14 and 28 days following
randomization in patients with rhabdomyolysis treated with NAC, early CRRT, both therapies,
or neither therapies 3) To determine clinical and biochemical risk factors for renal failure
development in subjects with rhabdomyolysis.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Factorial Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Prevention
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