Kidney Failure, Chronic Clinical Trial
— ENRICHOfficial title:
Intravenous vs. Oral Hydration to Reduce the Risk of Post-Contrast Acute Kidney Injury After Intravenous Contrast-Enhanced Computed Tomography in Patients With Severe Chronic Kidney Disease (ENRICH): A Randomized Controlled Trial
The use of contrast media (CM) poses a risk of post-contrast acute kidney injury (PC-AKI), especially among patients chronic kidney disease (CKD). International guidelines recommend intravenous (IV) hydration with isotonic 0.9% NaCl for three-four hours pre-contrast and four-six hours post-contrast. Recent studies have proven that oral hydration or no hydration is non-inferior to IV hydration in patients with mild to moderate CKD (eGFR 30-60 mL/min/1.73 m2). However, no randomized controlled trials have evaluated alternative hydration methods against the guideline-recommended hydration protocol for the prevention of PC-AKI in high-risk patients with severe CKD (eGFR < 30 mL/min/1.73 m2). Thus, the main focus of this trial is to evaluate IV hydration vs. oral hydration for their efficacy to prevent of PC-AKI in patients with severe CKD, who are scheduled for an elective contrast-enhanced CT-scan (CECT) with IV contrast-administration. Our research hypotheses consist of the following: 1. Oral hydration with bottled tap water is non-inferior to IV-hydration with isotonic 0.9% NaCl as renal prophylaxis to prevent PC-AKI in patients with severe CKD referred for an elective IV CECT. 2. NGAL and cfDNA are early and precise plasma and urinary biomarkers of PC-AKI with excellent diagnostic and prognostic accuracy for PC-AKI, dialysis, renal adverse events, hospitalization, progression in CKD-symptoms, and all-cause mortality.
Status | Recruiting |
Enrollment | 254 |
Est. completion date | March 16, 2026 |
Est. primary completion date | March 16, 2025 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: - eGFR < 30 mL/min/1.73 m2 - Scheduled for elective IV CECT - Age = 18 - Signed informed consent Exclusion Criteria: - Allergy to Iodine - Pregnancy - Active dialysis treatment - Acute infectious or inflammatory disease - Acute pre- and/or post-renal kidney failure - Unable to understand study information |
Country | Name | City | State |
---|---|---|---|
Denmark | Department of Cardiology | Odense C | Fyn |
Lead Sponsor | Collaborator |
---|---|
Odense University Hospital | Copenhagen University's Research Foundation for Medical Students, Department of Clinical Genetics, Odense University Hospital, Department of Nephrology, Odense University Hospital, Helen and Ejnar Bjørnow's Foundation, Novo Nordisk A/S, Open Patient data Explorative Network (OPEN), Sophus Jacobsen and Astrid Jacobsen's Foundation, The A.P. Moller Foundation, The Research Counsil of Odense University Hospital |
Denmark,
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* Note: There are 59 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Incidence of PC-AKI | The incidence of PC-AKI within the two arms | 2-5 days after IV CECT | |
Secondary | Incidence of new onset need for dialysis treatment | The incidence of patients with incident need for dialysis treatment, which is registered from the EHR and/or telephone consultation | = 30 days after IV CECT | |
Secondary | Renal adverse events | The incidence of renal adverse events defined as a relative increase in SCr > 15% and/or a decrease in eGFR > 15% and/or progression in CKD-stage from CKD-stage IV to CKD-stage Va | 25-40 days after IV CECT | |
Secondary | Hospitalization due to symptomatic heart failure | The incidence of patients hospitalized due to symptomatic heart failure, which is registered from the EHR and/or telephone consultation | = 30 days after IV CECT | |
Secondary | All-cause mortality | All-cause mortality, which is registered from the EHR | = 30 days after IV CECT | |
Secondary | Hospitalization due to suspected hydration- or contrast-related sequelae | Hospitalization due to suspected hydration- or contrast-related sequelae (e.g., arrythmias, renal insufficiency, hyponatremia or hypernatremia), which is registered from the EHR and/or telephone consultation | = 30 days after IV CECT | |
Secondary | Progression in CKD-symptoms | Progression in CKD-symptoms within 30 days after IV CECT defined as an increase in number of uremic symptoms compared to number of uremic at baseline within the two arms (see definition of "uremic symptoms" under "Variables" in the detailed description of the trial) | = 30 days after IV CECT | |
Secondary | Incidence of PC-AKI based on the criteria from the previously used and most cited definition of PC-AKI | The incidence of PC-AKI within the population and the two arms defined as a relative increase in SCr > 25% from baseline or an absolute increase > 0.5 mg/dL | 2-5 days after IV CECT | |
Secondary | Timepoints of diagnosis for PC-AKI | The difference in PC-AKI diagnosed two-three days after IV CECT and four-five days after IV CECT within the population and the two arms | 2-5 days after IV CECT | |
Secondary | Number of patients with normalization of PC-AKI | Number of participants with normalization of PC-AKI within study population and the two arms defined as a decline in SCr below the criteria for PC-AKI | = 40 days after IV CECT | |
Secondary | Mean changes in SCr | Mean changes in SCr from baseline at different timepoints within the study population and the two arms | SCr is measured on the following time-points (days from baseline): -89 to -seven days, -six to -four days, -three to -one days, 0 days (baseline), +two to three days, +four to five days, and +25 to +40 days | |
Secondary | Mean changes in eGFR. | Mean changes in eGFR from baseline at different timepoints within the study population and the two arms | eGFR is measured on the following time-points (days from baseline): -89 to -seven days, -six to -four days, -three to -one days, 0 days (baseline), +two to three days, +four to five days, and +25 to +40 days | |
Secondary | The effect of hydration on standard blood parameters | Mean changes in standard blood parameters within the two arms. Standard blood parameters are the following: Hemoglobin (mM), erythrocytes (count/L), SCr (micromole/L), eGFR (mL/min/1.73 m2), albumine (micromole/L), sodium (mM), and potassium (mM) | Standard blood parameters will be obtained after IV CECT at +two to three days and/or +four to five days, and +25 to +40 days from baseline | |
Secondary | Mean values of plasma and urinary NGAL and cell-free DNA | Mean values of plasma and urinary NGAL (µg/mg) and cell-free DNA (ng/mg) at baseline and 4 hours after IV CECT | In-hospital: Before initiation of the hydration protocol and the IV CECT (baseline) and 4 hours after IV CECT | |
Secondary | Mean changes of plasma and urinary NGAL and cell-free DNA | Mean changes in plasma and urinary NGAL (µg/mg) and cell-free DNA (ng/mg) from baseline (0 hours) to four hours after IV CECT | In-hospital: Before initiation of the hydration protocol and the IV CECT (baseline) and 4 hours after IV CECT | |
Secondary | The diagnostic and prognostic accuracy of plasma and urinary NGAL and cell-free DNA | Sensitivities, specificities, negative predictive values, positive predictive values, negative likelihood-ratios, and positive likelihood-ratios of plasma and urinary NGAL (µg/mg) and cell-free DNA (ng/mg) based on the most optimal cut-off point for each biomarker based on Receiver Operating Characteristics-Curves (ROC-curves) and their corresponding Area Under Curve (AUC). The most optimal cut-off is defined as the closest point on the ROC-curves, at which the sensitivity = specificity = 1.0 | In-hospital: Before initiation of the hydration protocol and the IV CECT (baseline) and 4 hours after IV CECT | |
Secondary | The diagnostic and prognostic accuracy of plasma and urinary NGAL and cell-free DNA | Assesment of the most optimal cut-off point for each biomarker based on Receiver Operating Characteristics-Curves (ROC-curves) and their corresponding Area Under Curve (AUC). The most optimal cut-off is defined as the closest point on the ROC-curves, at which the sensitivity = specificity = 1.0 | In-hospital: Before initiation of the hydration protocol and the IV CECT (baseline) and 4 hours after IV CECT | |
Secondary | The diagnostic and prognostic accuracy of plasma and urinary NGAL and cell-free DNA | The correlation between SCr and plasma and urinary NGAL (µg/mg) and cell-free DNA (ng/mg) will be illustrated in Scatter Plots. | In-hospital: Before initiation of the hydration protocol and the IV CECT (baseline) and 4 hours after IV CECT | |
Secondary | Cost-effectiveness | The use of resources (presented in DKK, EUR, and USD) for IV-hydration and oral hydration within the two arms are calculated from the following parameters: The cost of occupying a hospital bed per hour (nursing, staff salaries etc.), IV-drip, and hydration bags with saline or bottled tap water. | 1 day (at the day of the patient's scheduled cardiac CT) | |
Secondary | Time-effectiveness of the two hydration protocols. | The two hydration methods are compared for the amount of time (hours and minutes) from initiation to completion hydration protocols. | In-hospital: Starting 1-3 hours before IV CECT and lasting maximally until 4 hours after IV CECT | |
Secondary | Risk of PC-AKI according to the size of the kidneys | The size of the right and left kidney will be measured and indexed to the body-size of the patient and analyzed as a risk factor for the occurence of PC-AKI | 2-5 days after IV CECT |
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