Coronary Artery Disease Clinical Trial
Official title:
Telomere Length and Telomerase Activity as a Predictor of Acute Kidney Injury Following Cardiac
The purpose of this study is to investigate whether biomarkers of cell senescence and aging can predict the development of acute kidney injury following cardiac surgery.
Patients with pre-operative renal dysfunction are at increased risk of developing cardiac
surgery associated acute kidney injury (AKI) but a proportion of patients with normal kidney
function will also be affected. Studies show that patients developing AKI post cardiac
surgery have a poorer long term prognosis, even if their kidney function subsequently returns
to normal However, the cause for this is not currently understood. We postulate that a
unifying mechanism makes such patients more susceptible to developing post-operative AKI and
of having an overall worse long term prognosis. We suggest that this mechanism is reduced
regenerative capacity of tissues. To test this hypothesis we will measure several markers of
cell senescence and aging including telomere length, telomerase activity, and DNA methylation
status.
Previous animal studies have shown that reduced telomere length and telomerase activity in
mice increases their susceptibility to ischaemia induced renal injury. The current study will
look at whether a similar association is seen in humans, using cardiopulmonary bypass as a
mechanism for studying ischaemia/inflammatory induced kidney injury. It aims to answer the
primary research question: Are telomere length and telomerase activity related to the
development of acute kidney injury following cardiac surgery? The presence of such an
association would provide new avenues in the development of biomarkers to predict outcomes
following cardiac surgery. In addition to scoring tools currently in clinical practice, such
biomarkers might allow better risk stratification of patients undergoing cardiac surgery.
Patient Registry and sample storage: Tissue samples and patient data collected in these
patients will also form part of the Barts Cardiovascular Registry (BAR). This is a Biobank
facility run by Barts Heart Centre in collaboration with United Kingdom (UK) Biobank. All
aspects of patient recruitment, data collection, data storage, and data analysis will be
covered by Standard Operating Procedures to ensure data quality of the registry.
Quality assurance: The management team for the BAR will be responsible for auditing the
completeness and validity of the data.
Sample size: As we have no preceding data on a possible association with telomere biology and
AKI post-cardiac surgery we have been unable to perform a power calculation for sample size.
In effect, the present study will be a large pilot study looking at this association.
Previously reported studies give an incidence of AKI following cardiac surgery of between 15
and 25%. In order to have approximately 200 AKI patients to study, we will aim to recruit
1000 patients. This is realistic given that the Barts Heart Centre should be performing
approximately 50 cardiac operations per week. Once recruitment is established, an interim
analysis will be performed to allow a more accurate estimation of sample size.
Statistical analysis: All relevant clinical parameters will be analysed by frequencies,
tabulations, correlations, distributions of normality and comparisons accordingly. An array
of statistical methods will be employed for parametric and non-parametric data including
Multivariate of all factors associated with the development of acute kidney injury following
cardiac surgery. Receiver operator characteristic (ROC) curve analysis will be used to
investigate clinical outcomes and the new markers of cell senescence (telomere length,
telomerase activity, and DNA methylation status). Missing data values will be rectified where
possible by review of the primary medical records. Missing data values due to incomplete
sample collection will be dealt with by statistical modelling.
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