Renal auto-transplantation promotes cortical microvascular network remodeling in a preclinical porcine model.

Souleymane Maïga,Geraldine Allain,Edouard Baulier,Patrick Hannaert,Luc Van Hoorebeke,Thierry Hauet,Manuel Dierick,Michel Scepi,Franck Guy,Jerome Roumy,Frederic Favreau

doi:10.1371/journal.pone.0181067

Abstract

The vascular network is a major target of ischemia-reperfusion, but has been poorly investigated in renal transplantation. The aim of this study was to characterize the remodeling of the renal vascular network that follows ischemia-reperfusion along with the most highly affected cortex section in a preclinical renal transplantation model. There were two experimental groups. The first was a grafted kidney group consisting of large white pigs for which the left kidney was harvested, cold flushed, preserved for 24 h in the University of Wisconsin’s preservation solution, and then auto-transplanted (n = 5); the right kidney was removed to mimic the situation of human kidney transplantation. The second group (uni-nephrectomized kidney group) consisted of animals that underwent only right nephrectomy, but not left renal transplantation (n = 5). Three months after autotransplantation, the kidneys were studied by X-ray microcomputed tomography. Vessel morphology and density and tortuosity of the network were analyzed using a 3D image analysis method. Cortical blood flow was determined by laser doppler analysis and renal function and tissue injury assessed by plasma creatinine levels and histological analysis. Renal ischemia-reperfusion led to decreased vascular segment volume associated with fewer vessels of less than 30 μm, particularly in the inner cortex:0.79 ± 0.54% in grafted kidneys vs. 7.06 ± 1.44% in uni-nephrectomized kidneys, p < 0.05. Vessels showed higher connectivity throughout the cortex (the arborescence factor of the whole cortex was less in grafted than uni-nephrectomized kidneys 0.90 ± 0.04 vs. 1.07 ± 0.05, p < 0.05, with an increase in the number of bifurcations). Furthermore, cortical blood flow decreased early in kidney grafts and remained low three months after auto-transplantation. The decrease in microvasculature correlated with a deterioration of renal function, proteinuria, and tubular dysfunction, and was associated with the development of fibrous tissue. This work provides new evidence concerning the impact of ischemia-reperfusion injuries on the spectrum of renal vascular diseases and could potentially guide future therapy to preserve microvessels in transplantation ischemia-reperfusion injury.

Highlights

The vascular microcirculation network is a major target in numerous cardiovascular disorders, in particular ischemia-reperfusion (IR) following renal transplantation [1]
We observed no visual signs of poor graft condition at the time of euthanasia
The density of vessels with a diameter > 30 μm did not differ between the two groups, but vessel density for segments < 30 μm in the whole cortical zone was significantly less in the grafted than uni-nephrectomized kidneys (0.55 ± 0.15% vs. 3.96 ± 0.67%, respectively, p < 0.05)

Summary

Introduction

The vascular microcirculation network is a major target in numerous cardiovascular disorders, in particular ischemia-reperfusion (IR) following renal transplantation [1]. In this condition, harvesting of the kidney induces ischemia and grafting induces reperfusion. IR syndrome can result in delayed and/or chronic graft dysfunction to nonfunctioning of the primary graft, depending on the degree of kidney damage, requiring the patient to return to dialysis [2]. During the development of chronic graft damage, renal microcirculation is affected by complex interactions between proliferation, regeneration, and capillary loss, leading to fibrosis, considered to be the major process responsible for late renal graft loss

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