<scp>HLA‐DQ</scp> eplet mismatch load may identify kidney transplant patients eligible for tacrolimus withdrawal without donor‐specific antibody formation after mesenchymal stromal cell therapy

Bezstarosti, Suzanne; Meziyerh, Soufian; Reinders, Marlies E.J.; Voogt-Bakker, Kim; Groeneweg, Koen E.; Roelen, Dave L.; Kers, Jesper; Fijter, Johan W. de; Heidt, Sebastiaan

doi:10.1111/tan.15008

Cited by 4 publications

(1 citation statement)

References 46 publications

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“…In the TRITON trial, MSCs were administered to facilitate safe tacrolimus withdrawal. Although the MSC patients with tacrolimus withdrawal developed more dnDSA then the control group, their kidney function was not inferior and dnDSA development did not lead to more rejection episodes [13,27]. In our selection of patients from the TRITON study there was one patient in the control group with a rejection episode (mixed rejection) and two patients in the MSC group with a rejection episode (TCMR) within the first year after transplantation (Supplementary Table S1).…”

Section: Discussionmentioning

confidence: 99%

Peripheral Blood Immune Cell Composition After Autologous MSC Infusion in Kidney Transplantation Recipients

Hendriks¹,

Heidt²,

Schulz

et al. 2023

Transpl Int

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Tacrolimus is the backbone of immunosuppressive agents to prevent transplant rejection. Paradoxically, tacrolimus is nephrotoxic, causing irreversible tubulointerstitial damage. Therefore, infusion of mesenchymal stromal cells (MSC) 6 and 7 weeks post-transplantation was assessed to facilitate withdrawal of tacrolimus in the randomized phase II TRITON trial. Here, we performed detailed analysis of the peripheral blood immune composition using mass cytometry to assess potential effects of MSC therapy on the immune system. We developed two metal-conjugated antibody panels containing 40 antibodies each. PBMC samples from 21 MSC-treated patients and 13 controls, obtained pre-transplant and at 24 and 52 weeks post-transplantation, were analyzed. In the MSC group at 24 weeks, 17 CD4+ T cell clusters were increased of which 14 Th2-like clusters and three Th1/Th2-like clusters, as well as CD4+FoxP3+ Tregs. Additionally, five B cell clusters were increased, representing either class switched memory B cells or proliferating B cells. At 52 weeks, CCR7+CD38+ mature B cells were decreased. Finally, eight Tc1 (effector) memory cytotoxic T cell clusters were increased. Our work provides a comprehensive account of the peripheral blood immune cell composition in kidney transplant recipients after MSC therapy and tacrolimus withdrawal. These results may help improving therapeutic strategies using MSCs with the aim to reduce the use of calcineurin inhibitors.Clinical Trial Registration: ClinicalTrials.gov, identifier NCT02057965.

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Section: Discussionmentioning

confidence: 99%

Peripheral Blood Immune Cell Composition After Autologous MSC Infusion in Kidney Transplantation Recipients

Hendriks¹,

Heidt²,

Schulz

et al. 2023

Transpl Int

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Molecular matching tools for allocation and immunosuppression optimization. Ready for primetime?

Niemann,

Matern

2024

Current Opinion in Organ Transplantation

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Purpose of review Molecular matching continues to be an important topic in organ transplantation. Over the years, several studies – larger and smaller – supported correlations of molecular incompatibility loads and clinical outcomes. However, their practical utility for clinical decision making remains controversial and there is no consensus on the context in which they should be used. Recent findings The recent literature on molecular matching can be divided into four main areas of research: several groups present improvements of the algorithmic pipelines (1), increasing the robustness of previous findings. Further clinical evidence is reported (2) in various cohorts and other organ transplant domains, such as liver and lung transplantation. Consideration is given to the application of molecular matching in the allocation of deceased organs (3), suggesting options to improve allocation equity and utility. Furthermore, evidence is provided for personalized immunosuppression based on immunological risk (4), including infection and post graft failure management. Summary There is ample evidence that current molecular matching algorithms add value to immunologic risk stratification for organ transplant recipients. First studies on how to translate these insights into patient management with respect to organ allocation and personalized medicine are underway and require further support.

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Characterisation of the HLA‐DQ alpha eplet 52SK targeting the DQA101* alleles family

Devriese,

Lee,

Meng

et al. 2024

HLA

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Eplet 52SK is unique in the HLA eplet registry as targeting the whole family of DQA1*01 alleles. It is proposed as an antibody‐verified eplet but has not been validated enough to deserve this label. Especially, confusion can occur with reactivity targeting the 52PQ eplet which is present on the DQB1*05 and DQB1*06 alleles families, as DQ molecule stability imposes DQA1*01 to selectively associate with these DQ‐β families only. Using two Luminex single antigen (LSA) assays from two vendors, beads bearing DR‐α/DQ6 heterodimers, a special build LSA panel of additional DQ beads, and an adsorption/elution strategy relying on cells from deceased donors or recombinant cells solely expressing one DQ antigen, we definitely established the antibody‐verified status of eplet 52SK using patients' sera reacting only against the DQ5 and DQ6 beads of the One Lambda LSA panel in routine patients' follow up. We also show that reactivity against this eplet is not a rare event among anti‐DQ1 immunisation. This study further strengthens the importance of considering the DQA1 locus in immunological studies of HLA and in organ allocation strategies.

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HLA‐DQ eplet mismatch load may identify kidney transplant patients eligible for tacrolimus withdrawal without donor‐specific antibody formation after mesenchymal stromal cell therapy

Cited by 4 publications

References 46 publications

Peripheral Blood Immune Cell Composition After Autologous MSC Infusion in Kidney Transplantation Recipients

Peripheral Blood Immune Cell Composition After Autologous MSC Infusion in Kidney Transplantation Recipients

Molecular matching tools for allocation and immunosuppression optimization. Ready for primetime?

Characterisation of the HLA‐DQ alpha eplet 52SK targeting the DQA101* alleles family

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HLA‐DQ eplet mismatch load may identify kidney transplant patients eligible for tacrolimus withdrawal without donor‐specific antibody formation after mesenchymal stromal cell therapy

Cited by 4 publications

References 46 publications

Peripheral Blood Immune Cell Composition After Autologous MSC Infusion in Kidney Transplantation Recipients

Peripheral Blood Immune Cell Composition After Autologous MSC Infusion in Kidney Transplantation Recipients

Molecular matching tools for allocation and immunosuppression optimization. Ready for primetime?

Characterisation of the HLA‐DQ alpha eplet 52SK targeting the DQA1*01 alleles family

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Product

Resources

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Characterisation of the HLA‐DQ alpha eplet 52SK targeting the DQA101* alleles family