Do tissue damage biomarkers used to assess machine-perfused NHBD kidneys predict long-term renal function post-transplant?

Background: Renal transplantation in many units is limited by the availability of donor organs. Kidneys obtained from non-heart-beating donors (NHBD) represent an important resource, with the potential to substantially increase the available donor organ pool. Such kidneys are associated with increas...

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Bibliographic Details
Published in:Clinica chimica acta 2003-12, Vol.338 (1), p.33-43
Main Authors: Gok, Muhammed A., Pelzers, Maurice, Glatz, Jan F.C., Shenton, Brian K., Buckley, Pamela E., Peaston, Robert, Cornell, Chris, Mantle, Dave, Soomro, Naeem, Jaques, Bryon C., Manas, Derek M., Talbot, David
Format: Article
Language:English
Subjects:
Alanine aminopeptidase
Biological and medical sciences
Biomarkers
Biomarkers - blood
Carrier Proteins - blood
CD13 Antigens - blood
Creatinine - blood
Fatty acid binding protein
Fatty Acid-Binding Proteins
Follow-Up Studies
Glutathione S-transferase
Glutathione Transferase - blood
Graft Survival
Humans
Investigative techniques, diagnostic techniques (general aspects)
Kidney - pathology
Kidney - physiology
Kidney - physiopathology
Kidney - surgery
Kidney transplantation
Kidney Transplantation - methods
Long-term function
Medical sciences
Non-heart-beating donors
Perfusion
Survival Rate
Time Factors
Tissue Donors
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Summary:Background: Renal transplantation in many units is limited by the availability of donor organs. Kidneys obtained from non-heart-beating donors (NHBD) represent an important resource, with the potential to substantially increase the available donor organ pool. Such kidneys are associated with increased warm ischaemic tissue injury which may be assessed by hypothermic machine perfusion. Within our transplant centre, a key component of such damage assessment and viability screening involves the quantification of the tissue damage biomarkers glutathione S-transferase in kidney perfusates. Methods: Since 1998, 126 NHBD kidneys were machine-perfused prior to implantation, resulting in 74 transplants. Kidney perfusate samples were assayed for glutathione S-transferase in “real time”, and alanine aminopeptidase and fatty acid binding protein in “retrospect”. Results: The pre-transplant concentration of these tissue injury biomarkers determined pre-transplant did not correlate with subsequent longer-term renal function, as assessed by measurement of serum creatinine (tGST: Spearman correlation r=−0.02; Ala-AP: r=0.02; H-FABP: r=−0.05) and creatinine clearance (tGST: r=0.08; Ala-AP: r=−0.02; H-FABP: r=0.14) for those kidneys that had passed their viability tests. Conclusions: Thus whilst these biomarkers may represent reliable pre-transplant indicators of immediate kidney viability and short-term kidney function, they do not predict the efficacy of renal function in the longer term.
ISSN:0009-8981
1873-3492
DOI:10.1016/j.cccn.2003.07.023