Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT04005105 |
| Other study ID # |
PrevHemAKI |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
October 14, 2019 |
| Est. completion date |
September 1, 2023 |
Study information
| Verified date |
February 2024 |
| Source |
Hospital Clinic of Barcelona |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
BACKGROUND: The incidence of acute kidney injury (AKI) in patients undergoing cardiac surgery
can reach 35% and between 2 and 5% require kidney replacement therapy during the AKI episode.
The development of AKI n this context is independently associated with higher long-term
mortality (5-10 years). In addition, there is strong evidence that an episode of AKI in the
hospital increases the risk of developing chronic kidney disease in the medium-long term. On
the other hand, once AKI has been recovered according to creatinine values, there are no
established biomarkers to predict patients at risk of progression to chronic kidney disease,
which will allow us to increase nephroprotection and surveillance measures in this group of
patients.
STUDY DESIGN: Open-label randomized unicentric prospective study of patients undergoing
valvular replacement heart surgery ± coronary bypass with acute kidney injury (AKI) risk >30%
according to the Leicester Cardiosurgery scale. Patients will be randomized 1:1 in two
groups: standard hemodynamic management or intensive hemodynamic management based on
premorbid mean perfusion pressure (MPP). The interventional period will span from
intra-operation until the first 24 hours postoperative. The incidence of AKI will be
evaluated according to KDIGO criteria between 48 hours and 7 days after surgery. Patients
will be followed for one year. Biomarkers of mitochondrial damage will be analyzed at various
points during the follow-up to patients presenting AKI.
INTERVENTIONS:
A) Group 1/Intensive management: Intra-surgical values of ± 25% basal MAP will be maintained
and once in the ICU an algorithm corresponding to group 1 based on cardiac index and ± 25%
MPP will be followed for 24 hours.
B) Group 2/Standard management: MAP during surgery will be maintained > 60 mmHg according to
usual protocol. Once in ICU, during the first 24 hours an algorithm corresponding to group 2
based on cardiac index, MAP and CVP will be followed.
Biomarkers of mitochondrial damage will be determined in urine in patients in both groups
only in patients developing AKI according to KDIGO guidelines between 48h and 7 days.
EXPECTED RESULTS:A 50% reduction in the incidence of AKI in the intervention group compared
to the control group is expected. At the same time, markers of mitochondrial damage are
expected to be validated in our cohort as biomarkers of AKI progression and to investigate
its usefulness as biomarkers of transition to Chronic kidney disease.
Description:
BACKGROUND:
The incidence of acute kidney injury (AKI) in patients undergoing cardiac surgery can reach
35% and between 2 and 5% require kidney replacement therapy during the AKI episode. The
development of AKI n this context is independently associated with higher long-term mortality
(5-10 years). In addition, there is strong evidence that an episode of AKI in the hospital
increases the risk of developing chronic kidney disease in the medium-long term. That is why
the prevention of AKI is essential to reduce the morbidity that these patients suffer in the
hospital and out-of-hospital environment. On the other hand, once AKI has been recovered
according to creatinine values, there are no established biomarkers to predict patients at
risk of progression to chronic kidney disease, which will allow us to increase
nephroprotection and surveillance measures in this group of patients.
STUDY DESIGN:
Open-label randomized unicentric prospective study of patients undergoing valvular
replacement heart surgery ± coronary bypass with acute kidney injury (AKI) risk >30%
according to the Leicester Cardiosurgery scale. Patients will be randomized 1:1 in two
groups: standard hemodynamic management or intensive hemodynamic management based on
premorbid mean perfusion pressure (MPP). The interventional period will span from
intra-operation until the first 24 hours postoperative. The incidence of AKI will be
evaluated according to KDIGO criteria between 48 hours and 7 days after surgery. Patients
will be followed for one year. Biomarkers of mitochondrial damage will be analyzed at various
points during the follow-up to patients presenting AKI. Intention to treat population will be
defined as patients who sign informed consent and undergo planned surgery.
INTERVENTIONS-ANALYSIS:
A) Group 1/Intensive management: Baseline mean blood pressure (MAP) and central venous
pressure (CVP) will be measured to calculate baseline mean perfusion pressure (MPP).
Intra-surgical values of ± 25% basal MAP will be maintained and once in the ICU an algorithm
corresponding to group 1 based on cardiac index and ± 25% MPP will be followed for 24 hours.
B) Group 2/Standard management: MAP during surgery will be maintained > 60 mmHg according to
usual protocol. Once in ICU, during the first 24 hours an algorithm corresponding to group 2
based on cardiac index, MAP and CVP will be followed. Biomarkers of mitochondrial damage will
be determined in urine in patients in both groups only in patients developing AKI according
to KDIGO guidelines between 48h and 7 days. The following variables will be assessed in both
groups: accumulated fluid balance in first 24 hours, ICU /hospitalization length of stay,
days with vasoactive support, MAKE (Major Adverse Kidney Events: mortality, need for renal
replacement therapy, persistent renal dysfunction) at 30, 90 and 365 days and other AKI
episodes at one year. In the patients who develop AKI, urinary markers of mitochondrial
injury will also be measured at 30 days.
EXPECTED RESULTS:
A 50% reduction in the incidence of AKI in the intervention group compared to the control
group is expected. At the same time, markers of mitochondrial damage are expected to be
validated in our cohort as biomarkers of AKI progression and to investigate its usefulness as
biomarkers of transition to Chronic kidney disease.
