Tolerance in liver transplantation: Biomarkers and clinical relevance

Baroja‐Mazo, Alberto; Revilla-Nuin, Beatriz; Parrilla, Pascual; Martı́nez-Alarcón, L.; Ramı́rez, Pablo; Pons, J.A.

doi:10.3748/wjg.v22.i34.7676

Cited by 32 publications

(23 citation statements)

References 165 publications

(158 reference statements)

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“…Many studies have emphasized the genetic and phenotypic profile of blood or tissue samples from tolerant transplant patients. This approach has given great results, overall clarifying the involvement of FOXP3 + Tregs in this phenomenon beyond other actors such as B cells, natural killer cells, and γδTCR cells as well as liver iron metabolism . However, it is well established that Tregs are not a homogeneous subset of cells.…”

Section: Discussionmentioning

confidence: 99%

Differential profile of activated regulatory T cell subsets and microRNAs in tolerant liver transplant recipients

et al. 2017

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Regulatory T cells (Tregs) play a potential role in operational tolerance in liver transplantation (LT) patients, and microRNAs (miRNAs) are known to be involved in immunological responses and tolerance. Thus, we analyzed the implication of different peripheral blood Treg subsets and miRNAs on LT tolerance in 24 tolerant (Tol) and 23 non-tolerant (non-Tol) LT recipients by cellular, genetic, and epigenetic approximation. Non-Tol patients had a lower demethylation rate of the forkhead box P3 (FOXP3) regulatory T cell-specific demethylated region (TSDR) than Tol patients that correlated with the frequency of circulating Tregs. Tol patients presented a different signature of Treg subset markers compared with non-Tol patients with increased expression of HELIOS and FOXP3 and a higher proportion of latency-associated peptide (LAP) Tregs and CD45RA human leukocyte antigen D related (HLA-DR) activated effector-memory Tregs. The expression of miR95, miR24, miR31, miR146a, and miR155 was higher in Tol than in non-Tol patients and was positively correlated with activated Treg markers. In conclusion, these data suggest that activated effector-memory Tregs and a TSDR-demethylation state of Tregs may play a role in the complex system of regulation of LT tolerance. In addition, we describe a set of miRNAs differentially expressed in human LT Tol patients providing suggestive evidence that miRNAs are implied in the preservation of self-tolerance as mediated by Tregs. Liver Transplantation 23 933-945 2017 AASLD.

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Section: Discussionmentioning

confidence: 99%

Differential profile of activated regulatory T cell subsets and microRNAs in tolerant liver transplant recipients

et al. 2017

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“…The dynamic profile of Treg in liver transplant recipients during IS weaning was explored by monitoring the frequency of Treg and Foxp3 mRNA expression in PBMC in 12 liver transplant patients undergoing IS withdrawal. A progressive increase in circulating CD4 + CD25 + Foxp3 + Treg and Foxp3 mRNA expression was associated with operational tolerance in liver transplant recipients (14,116). The expression of adenosine deaminase, which degrades adenosine to evoke stronger Treg activation, was higher in five tolerant liver transplant patients compared to the 12 non-tolerant recipients.…”

Section: Monitoring and Prediction Of Clinical Liver Transplant Tolermentioning

confidence: 96%

“…Liver pDC prevent oral T cell priming through inducing anergy or deletion of circulating T cells via a CD4 + T cell-independent mechanism (11). Monocytes cultured with hepatocyte growth factor or liver epithelial cells can differentiate into DC that release high levels of IL-10 (12, 13), suggesting that the hepatic microenvironment modulates DC differentiation into regulatory subsets (14).…”

Section: Intrahepatic Immune Cells Interact With Liver Parenchymal Cementioning

confidence: 99%

Transplant Tolerance Induction: Insights From the Liver

2020

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A comparison of pre-clinical transplant models and of solid organs transplanted in routine clinical practice demonstrates that the liver is most amenable to the development of immunological tolerance. This phenomenon arises in the absence of stringent conditioning regimens that accompany published tolerizing protocols for other organs, particularly the kidney. The unique immunologic properties of the liver have assisted our understanding of the alloimmune response and how it can be manipulated to improve graft function and survival. This review will address important findings following liver transplantation in both animals and humans, and how these have driven the understanding and development of therapeutic immunosuppressive options. We will discuss the liver's unique system of immune and non-immune cells that regulate immunity, yet maintain effective responses to pathogens, as well as mechanisms of liver transplant tolerance in pre-clinical models and humans, including current immunosuppressive drug withdrawal trials and biomarkers of tolerance. In addition, we will address innovative therapeutic strategies, including mesenchymal stem cell, regulatory T cell, and regulatory dendritic cell therapy to promote liver allograft tolerance or minimization of immunosuppression in the clinic.

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“…Tolerogenic plasmacytoid DCs have a low capacity for T cell stimulatory functions and a high capacity for inducing tolerogenicity, mainly through downregulation of MHC class II and costimulatory molecules, upregulation of inhibitory factors and secretion of effector molecules and regulatory cytokines (e.g. nitric oxide, IL-10) [47]. In the context of SOT LT recipients, plasmacytoid DCs were observed at higher frequencies in some [48], but not all analyses [44].…”

Section: Flow Cytometric Immune Cell Subset Analysesmentioning

confidence: 99%

Biomarkers of immune tolerance in liver transplantation

Vionnet

Sánchez‐Fueyo

2018

Human Immunology

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The liver exhibits intrinsic immune tolerogenic properties that contribute to a unique propensity toward spontaneous acceptance when transplanted, both in animal models and in humans. Thus, in contrast to what happens after transplantation of other solid organs, several years following liver transplantation a significant subset of patients are capable of maintaining normal allograft function with histological integrity in the absence of immunosuppressive drug treatment. Significant efforts have been put into identifying sensitive and specific biomarkers of tolerance in order to stratify liver transplant recipients according to their need for immunosuppressive medication and their likelihood of being able to completely discontinue it. These biomarkers are currently being validated in prospective clinical trials of immunosuppression withdrawal both in Europe and in the United States. These studies have the potential to transform the clinical management of liver transplant recipients by mitigating, at least in part, the burden of lifelong immunosuppression.

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Tolerance in liver transplantation: Biomarkers and clinical relevance

Cited by 32 publications

References 165 publications

Differential profile of activated regulatory T cell subsets and microRNAs in tolerant liver transplant recipients

Differential profile of activated regulatory T cell subsets and microRNAs in tolerant liver transplant recipients

Transplant Tolerance Induction: Insights From the Liver

Biomarkers of immune tolerance in liver transplantation

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