Nonchimeric HLA-Identical Renal Transplant Tolerance: Regulatory Immunophenotypic/Genomic Biomarkers

Leventhal, Joseph R.; Mathew, James M.; Salomon, Daniel R.; Kurian, Sunil M.; Friedewald, John; Gallon, Lorenzo; Konieczna, Iwona; Tambur, Anat R.; Charette, Jane; Levitsky, Josh; Jie, Chunfa; Kanwar, Yashpal S.; Abécassis, Michaël; Miller, Joshua

doi:10.1111/ajt.13416

Cited by 53 publications

(62 citation statements)

References 33 publications

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“…We applied the cSoT in a trial of tolerance induction in which 15 renal recipients of HLA-identical living donor siblings were followed up for 5 years after transplantation 9, 10 . The protocol consisted in infusions of donor hematopoietic CD34 + stem cells with a conditioning regimen and immunosuppression was withdrawn 2 years after transplantation.…”

Section: Resultsmentioning

confidence: 99%

A composite score associated with spontaneous operational tolerance in kidney transplant recipients

Danger

Chesneau

Paul

et al. 2017

Kidney International

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New challenges in renal transplantation include using biological information to devise a useful clinical test for discerning high- and low-risk patients for individual therapy and ascertaining the best combination and appropriate dosages of drugs. Based on a 20-gene signature from a microarray meta-analysis performed on 46 operationally tolerant patients and 266 renal transplanted recipients with stable function, we applied the sparse Bolasso methodology to identify a minimal and robust combination of six genes and two demographic parameters associated with operational tolerance. This composite score of operational tolerance discriminated operationally tolerant patients with an area under the curve of 0.97 (95% confidence interval 0.94–1.00). The score was not influenced by immunosuppressive treatment, center of origin, donor type, or post-transplant lymphoproliferative disorder history of the patients. This composite score of operational tolerance was significantly associated with both de novo anti-HLA antibodies and tolerance loss. It was validated by quantitative polymerase chain reaction using independent samples and demonstrated specificity toward a model of tolerance induction. Thus, our score would allow clinicians to improve follow-up of patients, paving the way for individual therapy.

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Section: Resultsmentioning

confidence: 99%

A composite score associated with spontaneous operational tolerance in kidney transplant recipients

Danger

Chesneau

Paul

et al. 2017

Kidney International

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“…Each calf has a proportion of red cells belonging genetically to itself and that belonging to the twin. They were also shown in subsequent experiments to be able to tolerate skin grafts from each other [19]. This led to further experiments by Anderson et al, in 1951 where skin grafts were used to distinguish monozygotic from dizygotic twins [20].…”

Section: Chimerismmentioning

confidence: 95%

“…Transplantation between genetically identical monozygotic twins has shown remarkable results of tolerance [19]. However, among dizygotic (HLA non-identical) twins, the microchimerism is incomplete and hence leads to inadequate tolerance [19][20][21][22][23].…”

Section: Chimerismmentioning

confidence: 99%

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Current State of Tolerance: The Holy Grail

Rathore¹

2017

Arch Clin Nephrol

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Research in Tolerance and Chimerism by Transplant immunologists for over half a century is akin to the pursuit of the Holy Grail. Animal experiments for inducing tolerance may not have been successful initially but in that process, our knowledge of the fascinating immune system has been greatly enriched. Understanding of innate and adaptive immune systems has paved the way for development of potent immunosuppression. However, achieving clinical or operational tolerance long term in renal transplant recipients in the absence of immunosuppression is the ultimate goal for clinicians. Reduction in immunosuppression will lower morbidity and mortality associated with heavy burden of immunosuppression. This review article will be of particular interest to clinicians involved in delivering care to renal transplant recipients. We have elucidated mechanisms of self-tolerance through central and peripheral tolerance, evolution of tolerogenic strategies, difference between macro and micro-chimerism, overview of successful protocols for inducing tolerance and recent work in the development of expanding regulatory cell lines. It is most encouraging to note progress using cellular therapies as reported by Immune Tolerance Network and by Transplant Research & Immunology group at Oxford. We may not be far from achieving clinical tolerance albeit with minimal if not completely immunosuppression free regimens in the longer term. Review Article Tolerance in TransplantationThe highest result of education is toleranceHelen Keller [1], Tolerance is derived from 'tolero' in Latin, which means to endure. Achieving transplant tolerance has been the subject of research for over half a century and our current understanding of tolerance has evolved during that time. It is by no means complete and the search for true tolerance continues.Tolerance is the ability of a foreign tissue or organ to survive in a host without immunosuppression. It can be described as donor specifi c non-reactivity in experimental models [2]. "Clinical operational tolerance" is described as a well-functioning graft lacking histological signs of rejection in absence of immunosuppression for at least 1 year in an immunocompetent host capable of responding to other challenges including infections [3,4].In contrast, "Immunological tolerance" is no detectable immune reaction towards the allograft in absence of immunosuppression. It is a state of permanent and specifi c immunological acceptance of the allograft by the host immune system in the absence of immunosuppression. Self-toleranceThe concept of tolerance towards transplanted organs is best understood through learning about self-tolerance. The lymphoid system, which consists of T and B-lymphocytes, controls the immune system protecting the host from foreign pathogens. In the developmental pathway of the lymphoid system, T cells and B cells undergo education and maturation in the central lymphoid organs; the thymus and bone marrow. During this maturation process, T and B cells learn to differentiate between s...

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“…Table 2 provides a listing of these studies in which bone marrow infusions containing HSCs have been used to induce tolerance to solid organ transplants in humans (36–44). Other studies have certainly also been done support the importance of donor specific transfusions for transplant tolerance, including the Trivedi group in Hyderabad (45) and further studies on genomic markers is providing new information from groups that have been working in this area for some time (46, 47). …”

Section: Why Are Stem Cells Of Interest In Solid Organ Transplantation?mentioning

confidence: 99%

Hematopoietic stem cells and solid organ transplantation

Elahimehr

Scheinok

McKay

2016

Transplantation Reviews

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Solid organ transplantation provides life saving therapy for patients with end stage organ disease. In order that the transplanted organ survive, the recipient must take a lifelong cocktail of immunosuppressive medications that increase the risk for infections, malignancies and drug toxicities. Data from many animal studies have shown that recipients can be made tolerant of their transplanted organ by infusing stem cells, particularly hematopoietic stem cells, prior to the transplant. The animal data have been translated into humans and now several clinical trials have demonstrated that infusion of hematopoietic stem cells, along with specialized conditioning regimens, can permit solid organ allograft survival without immunosuppressive medications. This important therapeutic advance has been made possible by understanding the immunologic mechanisms by which stem cells modify the host immune system, although it must be cautioned that the conditioning regimens are often severe and associated with significant morbidity. This review discusses the role of hematopoietic stem cells in solid organ transplantation, provides an understanding of how these stem cells modify the host immune system and describes how newer information about adaptive and innate immunity might lead to improvements in the use of hematopoietic stem cells to induce tolerance to transplanted organs.

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Nonchimeric HLA-Identical Renal Transplant Tolerance: Regulatory Immunophenotypic/Genomic Biomarkers

Cited by 53 publications

References 33 publications

A composite score associated with spontaneous operational tolerance in kidney transplant recipients

A composite score associated with spontaneous operational tolerance in kidney transplant recipients

Current State of Tolerance: The Holy Grail

Hematopoietic stem cells and solid organ transplantation

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