Frontiers in Immunology (Mar 2020)

Perirenal Adipose Tissue Displays an Age-Dependent Inflammatory Signature Associated With Early Graft Dysfunction of Marginal Kidney Transplants

  • Romain Boissier,
  • Romain Boissier,
  • Pauline François,
  • Pauline François,
  • Bastien Gondran Tellier,
  • Bastien Gondran Tellier,
  • Maité Meunier,
  • Luc Lyonnet,
  • Stephanie Simoncini,
  • Jeremy Magalon,
  • Jeremy Magalon,
  • Tristan Legris,
  • Laurent Arnaud,
  • Laurent Giraudo,
  • Françoise Dignat George,
  • Françoise Dignat George,
  • Gilles Karsenty,
  • Stéphane Burtey,
  • Stéphane Burtey,
  • Eric Lechevallier,
  • Florence Sabatier,
  • Florence Sabatier,
  • Pascale Paul,
  • Pascale Paul

DOI
https://doi.org/10.3389/fimmu.2020.00445
Journal volume & issue
Vol. 11

Abstract

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Background: Better understanding of the contribution of donor aging and comorbidity factors of expanded criteria donors (ECD) to the clinical outcome of a transplant is a challenge in kidney transplantation. We investigated whether the features of donor-derived stromal vascular fraction of perirenal adipose tissue (PRAT-SVF) could be indicative of the deleterious impact of the ECD microenvironment on a renal transplant.Methods: A comparative analysis of cellular components, transcriptomic and vasculogenic profiles was performed in PRAT-SVF obtained from 22 optimal donors and 31 ECD deceased donors. We then investigated whether these parameters could be associated with donor aging and early allograft dysfunction.Results: When compared with the PRAT-SVF of non-ECD donors, ECD PRAT-SVF displayed a lower proportion of stromal cells, a higher proportion of inflammatory NK cells. The global RNA sequencing approach indicated a differential molecular signature in the PRAT-SVF of ECD donors characterized by the over-expression of CXCL1 and IL1-β inflammatory transcripts. The vasculogenic activity of PRAT-SVF was highly variable but was not significantly affected in marginal donors. Periorgan recruitment of monocytes/macrophages and NK cells in PRAT-SVF was associated with donor aging. The presence of NK cell infiltrates was associated with lower PRAT-SVF angiogenic activity and with early allograft dysfunction evaluated on day 7 and at 1 month post-transplant.Conclusions: Our results indicate that human NK cell subsets are differentially recruited in the periorgan environment of aging kidney transplants. We provide novel evidence that PRAT-SVF represents a non-invasive and timely source of donor material with potential value to assess inflammatory features that impact organ quality and function.

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