Kidney Injury Clinical Trial
Official title:
Early Diagnosis as a Strategy in Reducing the Incidence of Acute Renal Failure and Mortality Associated With Contrast Media Administration in Cardiovascular Procedures
Renal damage due to contrast media (CM) administration is one of the main complications of
cardiac intervention and is called contrast-induced nephropathy (CIN). Patients suffering
from CIN have a high probability of developing acute renal failure. Today there is no
treatment capable of reversing kidney damage, so the best strategy is prevention, by early
diagnosis. In this regard, a line of research is currently being carried out focused on the
identification of new markers capable of detecting susceptibility/predisposition to renal
damage before the administration of a potentially nephrotoxic drug, even at doses that alone
should not produce Kidney damage. This concept has been called predisposition to kidney
damage.
Taking into account all of the above, the objective of this work is to evaluate the ability
of the new markers (previously identified in preclinical models) to detect the predisposition
to the CIN before administering the CM.
Kidney damage is one of the most frequent complications of cardiac intervention. This
pathology is called contrast-induced nephropathy (CIN) and is defined as an increase in
plasma creatinine greater than or equal to 0.5 mg/dL, or greater than or equal to 25% with
respect to baseline, during the 5 days after contrast medium (CM) administration.
The appearance of acute renal damage significantly increases the health costs associated with
interventional procedures. This is derived from the increase in the length of hospital stay,
in care units, and from the application of dialysis as the only existing treatment. In the
United States, it has been estimated that the development of acute in-hospital renal damage
increases health expenditure by $ 7933 per patient per day, mainly due to the increase in
hospitalization time. Thus, not only the very early detection, but especially the prevention
of acute renal damage are key aspects for the prognosis of the patients, and for the control
of the health expenditure associated with them.
Iodized CMs are the leading cause of acute renal damage of toxic origin in humans. CMs
produce renal ischemia derived from a vasoconstriction that has two effects: on the one hand
reduction of glomerular filtration, and on the other, tubular ischemic damage that amplifies
the reduction of filtrate and, with it, renal dysfunction.
Different scales have been proposed to determine the risk of developing CIN, which include
different variables such as the presence of arterial hypotension, the use of counterpulsation
balloon, the age over 75 years, the presence of anaemia, diabetes, the amount of CM used and
renal function. Each item is assigned a certain score in the case of being present in the
patient and depending on the final score, the possible risk of contrast nephropathy after the
procedure and even the risk of dialysis is estimated. However, these scales are not widely
used in clinical practice and their usefulness is doubtful.
Currently the detection of renal damage associated with CM is performed using the plasma
creatinine marker. The main drawback of this detection mode is that creatinine levels
increase when renal functionality is already altered. In other words, detection occurs when
renal functionality has decreased by approximately 70%. This is why new markers capable of
detecting damage in their earliest stages are currently being evaluated, when the damage is
less widespread. Also in the last decade a new concept of biomarker called a marker of
predisposition to kidney damage has emerged. This concept has been revealed after verifying
that certain treatments significantly increase the risk of suffering an acute renal failure,
and do so in a hidden and silent way.
This susceptibility can be detected by certain markers, which if its usefulness is validated
in clinical practice, this assessment would be a very useful tool to classify the risk of
patients, individually. Thus the information provided by the predisposition markers would
allow a preventive and personalized medicine to be carried out when subjecting patients to a
new procedure or treatment potentially harmful to their kidneys.
Taking into account all of the above, the objective of this work is to evaluate the ability
of the new predisposition markers (previously identified in preclinical models) to detect
patients at risk of suffering CIN before CM administration.
To carry out this purpose, patients who are going to receive an CM will be recruited from the
Cardiology Service of the University Assistance Complex of Salamanca (CAUSA). Patients who
agree to be part of the study must sign an informed consent.
DATA COLLECTION, SAMPLES AND PROCESSING Each patient is assigned an alphanumeric code,
therefore their identity will only be known by the cardiology staff.
At the time of inclusion in the study, the following information will be collected for each
patient: date of sample collection, general data, anthropometric data, risk factors,
prescribed drugs.
Both before the CM administration and daily for the next 5 days, the plasma creatinine value
obtained through the patient's medical history will be collected, since this is a
determination that is made as part of the care procedure.
A urine sample will be collected before the CM administration. This sample will be coded with
the code mentioned above and will be taken to the CAUSA Sample Bank, where it will be
centrifuged, aliquoted and stored at -80 degrees Celsius.
URINE SAMPLES ANALYSIS The following determinations will be made: Proteinuria: marker used in
the clinic, the Bradford colorimetric technique will be used; Early kidney damage markers and
predisposition markers using colorimetric methods, ELISAs and Western Blot STATISTIC ANALYSIS
A significance level of 0.05 will be used. The data analysis will be performed with STATA 10
and Statistical Package for the Social Sciences (SPSS) 23.0. Different contrast will be
applied depending on the association that is to be studied in each case, and the type of
variables such as: normality test (Kolmogorov-Smirnov, Shapiro-Wilk), frequency comparison
(X2), correlation test (Pearson, Spearman), comparison of means for independent data (ANOVA
and Kruskal-Wallis) and repeated measures ANOVA and Wilcoxon test for paired data.
STUDY LIMITATIONS Although the study follows all the recommendations for observational
studies considered in the STORBE statement (STregthening the Reporting of OBservational
studies in Epidemiology), there is a possibility that there are factors that have not been
considered. On the other hand, the included variables are biomarkers of early kidney damage
and predisposition to acute renal damage induced by certain renal toxins. It is possible that
there are other markers (unknown), that there are not being analysed, and that can predict
the kidney damage.
CONCLUSION In summary, this project focuses on finding a solution to a problem of high
clinical relevance: to diagnose patients at risk of suffering CIN before CM administration.
Therefore, it proposes an objective focused on personalized medicine.
This project will be carried out through the generation of a consortium of professionals from
different fields, on the one hand researchers, experts in markers of renal damage and on the
other, clinicians specialized in the realization of vascular catheterizations.
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