The role of novel therapeutic approaches for prevention of allosensitization and antibody-mediated rejection

Jordan, Stanley C.; Ammerman, Noriko; Choi, Jua; Huang, Edmund; Peng, Alice; Sethi, Supreet; Najjar, Reiad; Kim, Irene; Toyoda, Mieko; Kumar, Sanjeev; Lim, Kathlyn; Vo, Ashley

doi:10.1111/ajt.15913

Cited by 28 publications

(32 citation statements)

References 72 publications

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“…A single-center, phase I/II investigator-initiated study (NCT03380377) aims to evaluate the safety and tolerability of monthly clazakizumab administration in 10 DSApositive kidney transplant recipients with biopsy-proven cAMR and transplant glomerulopathy [121,129]. At 18month follow-up, there were sustained reductions in mean DSA relative intensity scores, stabilization of renal function, and increased Tregs, without drug-related serious Abbreviations: TCZ, tocilizumab; cPRA, calculated panel reactive antibody; DES, desensitization; ESRD, end-stage renal disease; DSA, donor-specific antibody; AMR, antibody-mediated rejection; TG, transplant glomerulopathy; ACR, acute cellular rejection; AE, adverse event; SAE, serious adverse event; cAMR, chronic antibody-mediated rejection; Treg, regulatory T-cell; MFI, mean fluorescence intensity adverse events.…”

Section: Clazakizumabmentioning

confidence: 99%

IL-6 Directed Therapy in Transplantation

Miller

Madsen

2021

Curr Transpl Rep

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Purpose of Review IL-6 is a pleiotropic, pro-inflammatory cytokine that plays an integral role in the development of acute and chronic rejection after solid organ transplantation. This article reviews the experimental evidence and current clinical application of IL-6/IL-6 receptor (IL-6R) signaling inhibition for the prevention and treatment of allograft injury. Recent Findings There exists a robust body of evidence linking IL-6 to allograft injury mediated by acute inflammation, adaptive cellular/humoral responses, innate immunity, and fibrosis. IL-6 promotes the acute phase reaction, induces B cell maturation/antibody formation, directs cytotoxic T-cell differentiation, and inhibits regulatory T-cell development. Importantly, blockade of the IL-6/IL-6R signaling pathway has been shown to mitigate its harmful effects in experimental studies, particularly in models of kidney and heart transplant rejection. Currently, available agents for IL-6 signaling inhibition include monoclonal antibodies against IL-6 or IL-6R and janus kinase inhibitors. Recent clinical trials have investigated the use of tocilizumab, an anti-IL-6R mAb, for desensitization and treatment of antibody-mediated rejection (AMR) in kidney transplant recipients, with promising initial results. Further studies are underway investigating the use of alternative agents including clazakizumab, an anti-IL-6 mAb, and application of IL-6 signaling blockade to clinical cardiac transplantation. Summary IL-6/IL-6R signaling inhibition provides a novel therapeutic option for the prevention and treatment of allograft injury. To date, evidence from clinical trials supports the use of IL-6 blockade for desensitization and treatment of AMR in kidney transplant recipients. Ongoing and future clinical trials will further elucidate the role of IL-6 signaling inhibition in other types of solid organ transplantation.

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Section: Clazakizumabmentioning

confidence: 99%

IL-6 Directed Therapy in Transplantation

Miller

Madsen

2021

Curr Transpl Rep

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“…Indeed, antibody rebound due to plasma cells (PC), which do not express CD20, limit the efficacy of the most commonly used strategy combining IGIV, plasmapheresis and B cell depletion by anti-CD20 depleting agent. Targeting PC with new pharmacological tool from autoimmunity and cancer research could allow a better management of the humoral response in desensitization protocols ( 37 ). In the germinal center, after the enhancement of alloantigen responses by T follicular helper (Tfh), activated B cells develop into memory-B cells, progress to plasmablasts and ultimately to antibody-producing PC ( 38 , 39 ).…”

Section: Introductionmentioning

confidence: 99%

“…These PC are the long-lived mediators of lasting humoral immunity and persist in medullary niche where they can secrete high-affinity complement-activating DSAs ( 38 , 40 ). Several emerging strategies aim to deplete PCs compartment in order to prevent ABMR ( 37 , 41 ). First, Interleukin 6 (IL-6) is a cytokine promoting Tfh and enhancing the progression of B cells to high-affinity antibodies producing PC ( 42 ).…”

Section: Introductionmentioning

confidence: 99%

“…Clazakizumab is a humanized IgG1 mAb with specificity for IL6 which can also induce circulating DSA reduction ( 45 ). Both Tocilizumab and Clazakizumab are pharmacological agents with major interest in the development of desensitization strategies targeting PC ( 37 , 46 ). On another hand, proteasome inhibitors represent one of the most promising solution to deplete PC in the setting of desensitization, targeting more selectively PCs population.…”

Section: Introductionmentioning

confidence: 99%

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HLA Desensitization in Solid Organ Transplantation: Anti-CD38 to Across the Immunological Barriers

2021

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The presence of anti-human leucocyte antigen (HLA) antibodies in the potential solid organ transplant recipient’s blood is one of the main barriers to access to a transplantation. The HLA sensitization is associated with longer waitlist time, antibody mediated rejection and transplant lost leading to increased recipient’s morbidity and mortality. However, solid organ transplantation across the HLA immunological barriers have been reported in recipients who were highly sensitized to HLA using desensitization protocols. These desensitization regimens are focused on the reduction of circulating HLA antibodies. Despite those strategies improve rates of transplantation, it remains several limitations including persistent high rejection rate and worse long-term outcomes when compare with non-sensitized recipient population. Currently, interest is growing in the development of new desensitization approaches which, beyond targeting antibodies, would be based on the modulation of alloimmune pathways. Plasma cells appears as an interesting target given their critical role in antibody production. In the last decade, CD38-targeting immunotherapies, such as daratumumab, have been recognized as a key component in the treatment of myeloma by inducing an important plasma cell depletion. This review focuses on an emerging concept based on targeting CD38 to desensitize in the field of transplantation.

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“…A high affinity monoclonal antibody that targets the FcRn, Rozanolixizumab, has been developed and tested in cynomolgus monkeys, as well as humans ( 15 , 16 ). Therapeutically, blocking the FcRn is actively being investigated for its role in the treatment of IgG-mediated diseases, such as myasthenia gravis, and primary immune thrombocytopenia ( 17 ), and has been reported as a potential agent in the setting of AMR in transplantation both for its direct effect on lowering circulating antibody levels, and as a mechanism to be exploited with respect to maintaining circulating drug levels of IgG-based therapeutics ( 18 , 19 ). However, it has not been tested in rhesus macaque models of sensitization or IgG-mediated pathology.…”

Section: Introductionmentioning

confidence: 99%

Measuring the Impact of Targeting FcRn-Mediated IgG Recycling on Donor-Specific Alloantibodies in a Sensitized NHP Model

et al. 2021

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BackgroundIn transplantation, plasmapheresis and IVIg provide the mainstay of treatment directed at reducing or removing circulating donor-specific antibody (DSA), yet both have limitations. We sought to test the efficacy of targeting the IgG recycling mechanism of the neonatal Fc receptor (FcRn) using anti-FcRn mAb therapy in a sensitized non-human primate (NHP) model, as a pharmacological means of lowering DSA.MethodsSix (6) rhesus macaque monkeys, previously sensitized by skin transplantation, received a single dose of 30mg/kg anti-RhFcRn IV, and effects on total IgG, as well as DSA IgG, were measured, in addition to IgM and protective immunity. Subsequently, 60mg/kg IV was given in the setting of kidney transplantation from skin graft donors. Kidney transplant recipients received RhATG, and tacrolimus, MMF, and steroid for maintenance immunosuppression.ResultsCirculating total IgG was reduced from a baseline 100% on D0 to 32.0% (mean, SD ± 10.6) on d4 post infusion (p<0.05), while using a DSA assay. T-cell flow cross match (TFXM) was reduced to 40.6±12.5% of baseline, and B-cell FXCM to 52.2±19.3%. Circulating total IgM and DSA IgM were unaffected by treatment. Pathogen-specific antibodies (anti-gB and anti-tetanus toxin IgG) were significantly reduced for 14d post infusion. Post-transplant, circulating IgG responded to anti-FcRn mAb treatment, but DSA increased rapidly.ConclusionTargeting the FcRn-mediated recycling of IgG is an effective means of lowering circulating donor-specific IgG in the sensitized recipient, although in the setting of organ transplantation mechanisms of rapid antibody rise post-transplant remains unaffected.

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The role of novel therapeutic approaches for prevention of allosensitization and antibody-mediated rejection

Cited by 28 publications

References 72 publications

IL-6 Directed Therapy in Transplantation

IL-6 Directed Therapy in Transplantation

HLA Desensitization in Solid Organ Transplantation: Anti-CD38 to Across the Immunological Barriers

Measuring the Impact of Targeting FcRn-Mediated IgG Recycling on Donor-Specific Alloantibodies in a Sensitized NHP Model

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