Comparison of protective effects of trimetazidine against experimental warm ischemia of different durations: early and long-term effects in a pig kidney model

doi:10.1152/ajprenal.00338.2006

Comparison of protective effects of trimetazidine against experimental warm ischemia of different durations: early and long-term effects in a pig kidney model

Christophe Jayle,¹ Frederic Favreau,¹ Kequiang Zhang,¹ Carole Doucet,¹ Jean Michel Goujon,¹ William Hebrard,² Michel Carretier,¹ Michel Eugene,¹ Gerard Mauco,¹ Jean Paul Tillement,³ and Thierry Hauet¹^,2

¹Institut National de la Santé et de la Recherche Médicale E0324, Centre Hospitalier et Universitaire de Poitiers, Poitiers; ²INRA, Unité de Transplantation Expérimentale, Département de Génétique Animale, Surgères; and ³Laboratoire de Pharmacologie, Faculté de Médecine, Université Paris XII, Créteil, France

Submitted 29 August 2006 ; accepted in final form 10 October 2006

Acute renal failure (ARF) is often the consequence of an ischemia-reperfusioninjury (IRI) and associated with high mortality. Warm ischemia(WI) is a crucial factor of tissue damage, and tissue destructionled by ischemia-reperfusion (I/R) can impact the early and long-termfunctional outcome. Trimetazidine (TMZ) is an anti-ischemicdrug. Previously, we already verified its protective effecton a cold-ischemic pig kidney model by directly adding TMZ intothe preservation solution (Faure JP, Baumert H, Han Z, GoujonJM, Favreau F, Dutheil D, Petit I, Barriere M, Tallineau C,Tillement JP, Carretier M, Mauco G, Papadopoulos V, Hauet T.Biochem Pharmacol 66: 2241–2250, 2003; Faure JP, PetitI, Zhang K, Dutheil D, Doucet C, Favreau F, Eugene M, GoujonJM, Tillement JP, Mauco G, Vandewalle A, Hauet T. Am J Transplant4: 495–504, 2004). In this study, we aimed to study thepotential effect of TMZ pretreatment (5 mg/kg iv 24 h beforeWI) on the injury caused by WI for 45, 60, and 90 min and reperfusionin a WI pig kidney model. Compared with sham-operated (control)and uninephrectomized animals (UNX), TMZ pretreatment significantlyreduced deleterious effects after 45 min, and particularly 60and 90 min, of WI by improving the recovery of renal functionand minimizing the inflammatory response commonly prevalentin ischemic kidney injury. Compared with controls (control groupand UNX group), it was observed that 1) hypoxia-inducible factor-1(HIF-1 ${alpha}$ ) expression occurred earlier and with a higher intensityin the TMZ-treated groups; 2) the reduction of IRI during thefirst week following reperfusion was correlated with an earlierand greater expression of stathmin, which is involved in theprocess of tubular repair; and 3) the tubulointerstitial fibrosiswas reduced, particularly after 60 and 90 min of WI. In conclusion,TMZ made the warm-ischemic kidneys more resistant to the deleteriousimpact of a single episode of I/R and reduced early and long-termsubsequent damage.

mitochondrial damage; ischemia-reperfusion injury; stathmin; renal regeneration

Address for reprint requests and other correspondence: T. Hauet, INSERM E0324, Laboratoire de Biochimie et Toxicologie, Centre Hospitalier et Universitaire, Hôpital Jean Bernard, La Miletrie, 86000 Poitiers, France (e-mail: t.hauet{at}chu-poitiers.fr)