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Wiley InterScience

American Journal of Transplantation

American Journal of Transplantation

Volume 4 Issue 12, Pages 1972 - 1981

Published Online: 26 Aug 2004

© 2010 American Society of Transplantation and the American Society of Transplant Surgeons



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Distinct Transcriptional Changes in Donor Kidneys upon Brain Death Induction in Rats: Insights in the Processes of Brain Death
Theo A. Schuurs a,*, Frans Gerbens b , Joost A.B. van der Hoeven a , Petra J. Ottens a , Krista A. Kooi b , Henri G.D Leuvenink a , Robert M.W. Hofstra b and Rutger J. Ploeg a
  a Department of Surgery, University Hospital Groningen, Groningen, The Netherlands   b Department of Medical Genetics, University of Groningen, Groningen, The Netherlands
  *Corresponding author: Dr. Theo A. Schuurs, t.a.schuurs@med.rug.nl
Copyright Blackwell Munksgaard 2004
KEYWORDS
Brain death • donor kidney • gene expression profiling • microarray

ABSTRACT

Brain death affects hormone regulation, inflammatory reactivity and hemodynamic stability. In transplant models, donor organs retrieved from brain dead (BD) rats suffer from increased rates of primary non-function and lower graft survival. To unravel the mechanisms behind brain death we have performed DNA microarray studies with kidney-derived RNA from normo- and hypotensive BD rats, corresponding with optimal and marginal BD donors, respectively. In kidneys from normotensive donors 63 genes were identified as either up- (55) or down-regulated (8), while 90 genes were differentially expressed (67 up-regulated) in hypotensive BD donor kidneys. Most genes were categorized in different functional groups: metabolism/transport (including the down-regulated water channel Aqp-2), inflammation/coagulation (containing the largest number (16) of up-regulated genes including selectins, Il-6, α- and β-fibrinogen), cell division/fibrosis (including KIM-1 involved in tubular regeneration) and defense/repair (with the cytoprotective genes HO-1, Hsp70, MnSOD2). Also, genes encoding transcription factors (including immediate early genes as Atf-3, Egr-1) and proteins involved in signal transduction (Pik3r1) were identified. Summarizing, the use of DNA microarrays has clarified parts of the process of brain death: Brain-death-induced effects ultimately lead, via activation of transcription factors and signal transduction cascades, to differential expression of different "effector" genes. Not only deleterious processes such as inflammation and fibrosis occur in brain dead donor kidneys but genes involved in protection and early repair processes are activated as well. These findings can be used to introduce specific cytoprotective interventions in the brain dead donor to better maintain or even increase organ viability.


Received 29 April 2004, revised and accepted for publication 9 July 2004

DIGITAL OBJECT IDENTIFIER (DOI)
10.1111/j.1600-6143.2004.00607.x About DOI

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