Use of a hanging-weight system for isolated renal artery occlusion during ischemic preconditioning in mice

doi:10.1152/ajprenal.00275.2006

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Am J Physiol Renal Physiol 292: F475-F485, 2007. First published August 15, 2006; doi:10.1152/ajprenal.00275.2006
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INNOVATIVE METHODOLOGY

Use of a hanging-weight system for isolated renal artery occlusion during ischemic preconditioning in mice

Almut Grenz,¹^,* Tobias Eckle,²^,* Hua Zhang,¹^,* Dan Yang Huang,¹ Manfred Wehrmann,³ Christoph Köhle,¹ Klaus Unertl,² Hartmut Osswald,¹ and Holger K. Eltzschig²

Departments of ¹Pharmacology and Toxicology, ²Anesthesiology and Intensive Care Medicine, and ³Pathology, Tübingen University Hospital, Tübingen, Germany

Submitted 19 July 2006 ; accepted in final form 10 August 2006

Renal failure from ischemia contributes to morbidity and mortality.Ischemic preconditioning (IP) represents a powerful strategyfor kidney protection, and recent advances in transgenic micemay help elucidate its molecular mechanisms. However, murineIP is technically challenging and experimental details significantlyinfluence results. Thus we developed a novel model for renalIP using a hanging-weight system for isolated renal artery occlusion.In contrast to previous models, this technique eliminates theneed for clamping the vascular pedicle (artery/vein). In fact,assessment of renal injury after different time periods of ischemia(10–60 min) revealed highly reproducible increases inplasma creatinine and potassium levels, while creatinine clearance,urinary flow and potassium/sodium excretion were significantlyattenuated. Using different numbers of IP cycles, we found maximalprotection with four cycles of 4 min of ischemia-reperfusion.In contrast, no significant renal protection was observed withIP of the vascular pedicle. To assess transcriptional responsesin this model, we isolated RNA from preconditioned kidneys andfound time-dependent induction of erythropoietin mRNA and plasmalevels with IP. Taken together, this model provides highly reproduciblerenal injury and protection by IP, thus minimizing variabilityassociated with previous techniques based on clamping of therenal pedicle. Further studies on renal ischemia/IP in micemay consider this technique.

targeted gene deletion; murine; acute renal failure; ischemia; reperfusion; kidney

Address for reprint requests and other correspondence: H. Osswald, Dept. of Pharmacology and Toxicology, Tübingen Univ. Hospital, Wilhelmstr. 56, D-72074 Tübingen, Germany (e-mail: hartmut.osswald{at}uni-tuebingen.de) or H. K. Eltzschig, Dept. of Anesthesiology and Intensive Care Medicine, Tübingen University Hospital, Zentrum für Medizinische Forschung, Waldhörnle Str. 22, D-72072 Tübingen, Germany (e-mail: heltzschig{at}partners.org)

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