Plasma cell targeting to prevent antibody-mediated rejection

Woodle, E. Steve; Tremblay, Sylvie; Rossi, Amy; Rojas, Cyd C.; Alloway, Rita R.; Roskin, Krishna M.; Allman, David; Hildeman, David

doi:10.1111/ajt.15889

Cited by 17 publications

(18 citation statements)

References 61 publications

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“…Rebound of DSA after short-term PI has been reported (136)(137)(138). This repletion of PC and DSA would be partially due to an intra-marrow PC repopulation which might be related to PC populations resistant to PI treatment.…”

Section: Costimulation Blockadementioning

confidence: 86%

Emerging New Approaches in Desensitization: Targeted Therapies for HLA Sensitization

et al. 2021

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There is an urgent need for therapeutic interventions for desensitization and antibody-mediated rejection (AMR) in sensitized patients with preformed or de novo donor-specific HLA antibodies (DSA). The risk of AMR and allograft loss in sensitized patients is increased due to preformed DSA detected at time of transplant or the reactivation of HLA memory after transplantation, causing acute and chronic AMR. Alternatively, de novo DSA that develops post-transplant due to inadequate immunosuppression and again may lead to acute and chronic AMR or even allograft loss. Circulating antibody, the final product of the humoral immune response, has been the primary target of desensitization and AMR treatment. However, in many cases these protocols fail to achieve efficient removal of all DSA and long-term outcomes of patients with persistent DSA are far worse when compared to non-sensitized patients. We believe that targeting multiple components of humoral immunity will lead to improved outcomes for such patients. In this review, we will briefly discuss conventional desensitization methods targeting antibody or B cell removal and then present a mechanistically designed desensitization regimen targeting plasma cells and the humoral response.

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Section: Costimulation Blockadementioning

confidence: 86%

Emerging New Approaches in Desensitization: Targeted Therapies for HLA Sensitization

et al. 2021

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“…After immunoglobulin class switching, they undergo affinity maturation and the cells with low affinity for foreign antigens or high affinity for self-antigens undergo apoptosis as a negative selection mechanism, followed by differentiation into MBCs or LLPCs that bind these antigens with high affinity. MBCs migrate to secondary lymphoid tissue to counter the ensuing invasion by foreign antigens, and LLPCs persist and continue to produce antibodies that induce AMR (17,18,(43)(44)(45) (Figure 1).…”

Section: Molecular Pathophysiology In Amrmentioning

confidence: 99%

“…In addition, pathological findings indicate that the CD138-positive PCs infiltrates are associated with AMR development ( 196 ). Therefore, CD138-targeting therapy may be applicable for AMR control and the maintenance of graft function after further elucidation of the involvement mechanism of CD138-mediated signaling in the activation of humoral immunity to transplanted grafts ( 43 ). However, as described in B−cell based therap y , B cells contain a subset that has an immune regulatory function.…”

Section: Development In Amr Controlmentioning

confidence: 99%

Approaches for Controlling Antibody-Mediated Allograft Rejection Through Targeting B Cells

Matsuda¹,

Watanabe²,

Li³

2021

Front. Immunol.

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Both acute and chronic antibody-mediated allograft rejection (AMR), which are directly mediated by B cells, remain difficult to treat. Long-lived plasma cells (LLPCs) in bone marrow (BM) play a crucial role in the production of the antibodies that induce AMR. However, LLPCs survive through a T cell-independent mechanism and resist conventional immunosuppressive therapy. Desensitization therapy is therefore performed, although it is accompanied by severe side effects and the pathological condition may be at an irreversible stage when these antibodies, which induce AMR development, are detected in the serum. In other words, AMR control requires the development of a diagnostic method that predicts its onset before LLPC differentiation and enables therapeutic intervention and the establishment of humoral immune monitoring methods providing more detailed information, including individual differences in the susceptibility to immunosuppressive agents and the pathological conditions. In this study, we reviewed recent studies related to the direct or indirect involvement of immunocompetent cells in the differentiation of naïve-B cells into LLPCs, the limitations of conventional methods, and the possible development of novel control methods in the context of AMR. This information will significantly contribute to the development of clinical applications for AMR and improve the prognosis of patients who undergo organ transplantation.

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“…Therefore, we initiated a desensitization trial with carfilzomib, which is an irreversible proteasome inhibitor. This trial, which is ongoing, has demonstrated increased potency and reduced toxicity compared with bortezomib 111,139,199 . Our group found >65% depletion of bone marrow plasma cells following carfilzomib treatment.…”

Section: Plasma Cell Biologymentioning

confidence: 72%

“…Research over the past several decades has uncovered factors critical for plasma cell survival and has begun to identify potential therapeutic targets to reduce or eliminate plasma cells. Here, we will focus on some of the elements, their respective therapies, and the data on their effectiveness in transplantation which should complement more mechanistic details on plasma cell homeostasis and targeting strategies in transplantation as recently reviewed 109‐115 …”

Section: Plasma Cell Biologymentioning

confidence: 99%

Plasma cell biology: Foundations for targeted therapeutic development in transplantation

Rossi

Alloway

Hildeman

et al. 2021

Immunological Reviews

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Solid organ transplantation is a life‐saving procedure for patients with end‐stage organ disease. Over the past 70 years, tremendous progress has been made in solid organ transplantation, particularly in T‐cell‐targeted immunosuppression and organ allocation systems. However, humoral alloimmune responses remain a major challenge to progress. Patients with preexisting antibodies to human leukocyte antigen (HLA) are at significant disadvantages in regard to receiving a well‐matched organ, moreover, those who develop anti‐HLA antibodies after transplantation face a significant foreshortening of renal allograft survival. Historical therapies to desensitize patients prior to transplantation or to treat posttransplant AMR have had limited effectiveness, likely because they do not significantly reduce antibody levels, as plasma cells, the source of antibody production, remain largely unaffected. Herein, we will discuss the significance of plasma cells in transplantation, aspects of their biology as potential therapeutic targets, clinical challenges in developing strategies to target plasma cells in transplantation, and lastly, novel approaches that have potential to advance the field.

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Plasma cell targeting to prevent antibody-mediated rejection

Cited by 17 publications

References 61 publications

Emerging New Approaches in Desensitization: Targeted Therapies for HLA Sensitization

Emerging New Approaches in Desensitization: Targeted Therapies for HLA Sensitization

Approaches for Controlling Antibody-Mediated Allograft Rejection Through Targeting B Cells

Plasma cell biology: Foundations for targeted therapeutic development in transplantation

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