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Peripheral phenotype and gene expression profiles of combined liver–kidney transplant patients
- Dumontet, Erwan;
- Danger, Richard;
- Vagefi, Parsia A;
- Londoño, Maria-Carlota;
- Pallier, Annaïck;
- Lozano, Juan José;
- Giral, Magali;
- Degauque, Nicolas;
- Soulillou, Jean-Paul;
- Martínez-Llordella, Marc;
- Lee, Herman;
- Latournerie, Marianne;
- Boudjema, Karim;
- Dulong, Joelle;
- Tarte, Karin;
- Sanchez-Fueyo, Alberto;
- Feng, Sandy;
- Brouard, Sophie;
- Conchon, Sophie
- et al.
Published Web Location
https://doi.org/10.1111/liv.12917Abstract
Background and aims
The beneficial effect of one graft on another has been reported in combined transplantation but the associated mechanisms and biological influence of each graft have not yet been established.Methods
In multiple analyses, we explored the PBMC phenotype and signature of 45 immune-related messenger RNAs and 754 microRNAs from a total of 235 patients, including combined liver-kidney transplant recipients (CLK), patients with a liver (L-STA) or kidney (K-STA) graft only under classical immunosuppression and patients with tolerated liver (L-TOL) or kidney grafts (K-TOL).Results
CLK show an intermediary phenotype with a higher percentage of peripheral CD19(+) CD24(+) CD38(Low) memory B cells and Helios(+) Treg cells, two features associated with tolerance profiles, compared to L-STA and K-STA (P < 0.05, P < 0.01). Very few miRNA were significantly differentially expressed in CLK vs. K-STA and even fewer when compared to L-STA (35 and 8, P < 0.05). Finally, CLK are predicted to share common miRNA targets with K-TOL and even more with L-TOL (344 and 411, P = 0.005). Altogether CLK display an intermediary phenotype and gene profile, which is closer to that of liver transplant patients, with possible similarities with the profiles of tolerant patients.Conclusion
These data suggest that CLK patients show the immunological influence of both allografts with liver having a greater influence.Many UC-authored scholarly publications are freely available on this site because of the UC's open access policies. Let us know how this access is important for you.
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