Nephrotoxicity Clinical Trial
Official title:
Does Ultra-High Dose i.v. N-acetylcysteine Prevent Contrast Nephropathy in Patients With Chronic Kidney Disease Undergoing Emergency Contrast Tomography.
The aim of the present study is to determine whether a high dose of intravenous NAC is efficient in preventing CN after emergency contrast injection in patients with renal failure.
Prevention of acute kidney injury (AKI) post contrast injection remains mandatory given its
association to morbidity and mortality1.
Contrast nephropathy (CN) was classically defined as an increase in 25% or more or absolute
increase of 44 umol/l of creatinine levels within three days following contrast injection2.
Markers such as cystatine C may be more sensitive to identify CN and also to correlate to
mortality8 although a definition of CN using these markers is lacking.
In patients undergoing elective radiological procedures, CN can be prevented by hydration,
withdrawal of diuretics and nephrotoxic drugs. N Acetylcysteine (NAC) has been proposed to
protect against contrast nephropathy since 200013. While hydratation is clearly beneficial
in preventing CIN14, the role of NAC administration is still uncertain and results of RCTs
gave conflicting results regarding its effect15.
Intravenous N-acetylcysteine (NAC) may be the form of choice in emergency procedures given
its rapid disponibility and its ease of administration in patients whose consciousness is
altered or who can not eat.
The aim of the present study is therefore to determine whether 6000 mg of intravenous NAC is
efficient in preventing CN after emergency contrast injection in CKD patients.
Inclusion criteria:
One hundred and thirty consecutive patients with an estimated GFR < 60 mL/min and an
indication to undergo an emergent contrast-enhanced CT will be included in the study.
Exclusion criteria: asthma, pregnancy, obstructive nephropathy and patient or family's
refusal.
Patients will be blindly randomized by computer to either placebo (0.45% saline) or high
dose (6000 mg) iv n-acétylcystéine (flumicil) iv diluted in 0.45% saline. All patients will
receive intravenous hydration (250 ml NaCl 0.45% at least) before the CT scan and 1000 ml
after the examination depending on clinical possibilities.
Creatinine and cystatine C serum levels will be collected one hour before CT scan and at day
2, 4 and 10. The T0 value will be the value measured before the CT-scan and not the baseline
admission value in order to correct for differential hydratation due to different waiting
time and hydratation before tomography. Serum Creatinine and Cystatine C will be measured by
the Jaffe method, and by a nephelometric assay respectively.
Outcome measures:
The primary endpoint of the study will be the occurrence of contrast nephropathy at day 2, 4
or 10, defined as an increase of at least 25% and/or 44 umol/l in serum creatinine level or
cystatine C levels at day 2, 4 or 10 compared to day 0. We will also assess the proportion
of patients with contrast nephropathy regarding the biomarker used and according to AKIN
criteria as well. D The AKIN criteria defined a stage 1 AKI as an increase in creatinine
between 150% and 199% from baseline or an absolute increase of at least 26.2 umol/l, a stage
2 AKI as an increase between 200% and 299% from baseline and a stage 3 AKI as an increase of
at least 300% from baseline or a creatinine concentration higher than 354 umol/l with an
acute rise of at least 44 umol/l or initiation of RRT.
Secondary endpoints will be the mean increases in creatinine and cystatin C concentrations
in days 2, 4 and 10 and the maximum increase during the time periods from day 2 to day 10
(peak increase).
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Observational Model: Case Control, Time Perspective: Prospective
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