Ischemia Reperfusion Injury Clinical Trial
Official title:
The Renal Transplant Outcome Prediction and Validation Study (TOPVAS)
The number of patients with end stage renal disease is increasing continuously and kidney
transplantation is the preferred treatment modality. Modern immunosuppressive therapy has
reduced the number of acute rejection episodes and increased one year allograft survival
dramatically. Nonetheless, 4% of allografts are lost beyond the first year annually due to a
multifactorial process and the latter number has not changed for decades. One of the most
important factors to determine long-term success after kidney transplantation is the quality
of the donor organ. For example, transplantation of organs from elderly or extended criteria
donors results in reduced allograft and patient survival.
In previous work, the investigators specifically focused on age-associated molecular
signatures including telomere length and mRNA expression levels of the cell cycle inhibitors
CDKN2A (p16INK4a) and CDKN1A (p21WAF1) and assessed these parameters in pre-implantation
biopsies of 54 patients. In a linear regression analysis CDKN2A turned out to be the best
single predictor for serum creatinine after 1 year followed by donor age and telomere length.
A multiple linear regression analysis revealed that the combination of CDKN2A values and
donor age yielded even higher predictive values. In another study the investigators were able
to show an interaction between donor age and use of calcineurin inhibitors with regard to
outcome after renal transplantation.
During these past activities an extensive set of whole genome transcriptomics profile
information from zero hour biopsies and clinical follow-up data has been collected. In the
TOPVAS study, existing data derived from 72 of the above mentioned set of biopsies (exclusion
of live donor grafts) will be analysed with state of the art bioinformatical/system biology
tools to derive a general (not purely age associated) prognostic biomarker panel for
functional transplant outcome two years after transplantation. This marker panel will also be
used to define organs preferentially suitable for MMF/tacrolimus based immunosuppression.
Both panels will then be validated for their prognostic and predictive information on the
long-term outcome after transplantation in a new independent patient population treated with
tacrolimus and MMF. In addition to biomarker assessment and in pursue of identifying
alternative and/or complementary parameters with predictive value , an advanced morphological
investigation of tissue biopsy life stains will be performed employing an innovative cell
viability staining technology ("BIOPSYCHRONOLOGY").
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