Acute Renal Failure Clinical Trial
Official title:
Prospective Multicenter Study to Assess the Predictive Value of PIIINP and Urinary NGAL in Renal Function Recovery During Acute Tubular Necrosis
Acute Renal Failure (ARF) is defined by a severe, and usually reversible, glomerular
filtration rate decreasing. Acute Tubular Necrosis (ATN) remain the major cause of ARF
involving distress and destruction of tubular cells. This specific typology of ARF may
evolve toward Chronic Renal Failure (CRF) concretizing a major public health issue.
Predict the progression of ARF towards CRF appears essential. The investigators believe that
the PIIINP and urinary NGAL biomarkers may constitute robust biomarkers of progression risk
towards CRF.
Acute Renal Failure (ARF) is defined by a severe, and usually reversible, glomerular
filtration rate decreasing. Beside its frequency, ARF may be associated with severe
prognostic. Thus, patient admitted in ICU and suffering of ARF requiring dialysis, had a
higher risk of mortality up to 50%.
Tubulointerstitial nephropathies, particularly Acute Tubular Necrosis (ATN) remain the major
cause of ARF, representing 45-50% of cases. The ATN is due to suffering and destruction of
tubular cells which are very sensitive to ischemia-reperfusion lesions because tubular
reabsorption functions require significant and constant energy intake. However, ATN
represents a relatively homogeneous group in terms of acute kidney disease typology.
Homogeneity and significant frequency compels ATN as an optimal model to study function
recovery after ARF.
ARF constitutes a major public health issue. Actually, incidence of Chronic Renal Failure
(CRF) after an ARF, due to ATN, is estimated between 19% and 31%. In addition 12.5% of
patients with specific ARF presentation immediately reach End-stage Renal Disease (ESRD),
and the occurrence of ARF requiring dialysis, triples the risk of chronic renal support.
Therefore, predict the progression of ARF towards CRF appears essential.
At this time, the investigators currently lack of reliable biomarkers to predict such
progression. This pejorative kidney development is due to the persistence of intrarenal
inflammation, rapid development of interstitial fibrosis and deficiency in tubular
restoration. It involves complex mechanisms of inflammatory response, and vascular and
tubular remodeling.
Two promising biomarkers of renal fibrosis, ARF occurrence and CRF progression risk appear
in recent years: the Procollagen III N-terminal peptide (PIIINP) and the neutrophil
gelatinase associated lipocalin (NGAL). The investigators believe that the PIIINP and
urinary NGAL may constitute robust biomarkers of progression (or not) towards CRF in ARF
context. Firstly, PIIINP is a good reflection of fibrosis process inside the kidney.
Secondarily, NGAL is a marker of renal tubule remodeling after renal aggression. The
combination of these two biomarkers could therefore efficiently reflect the balance tubular
fibrosis/restoration and may allow optimal prediction of renal function recovery.
The investigators hypothesize that these two biomarkers may be used to assess the risk of
CRF progression during ARF in ATN context.
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Observational Model: Cohort, Time Perspective: Prospective
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