Costimulation Blockade in Kidney Transplantation

Malvezzi, Paolo; Jouve, Thomas; Rostaing, Lionel

doi:10.1097/tp.0000000000001344

Cited by 37 publications

(22 citation statements)

References 94 publications

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“…Like current co-stimulation inhibitors, as demonstrated in primates, agents blocking CD28 might also constitute the basis of a CNI-free maintenance therapy, while reducing the rejection risk that has been attributed to the use of belatacept. 45…”

Section: A C C E P T E Dmentioning

confidence: 99%

Selective Costimulation Blockade With Antagonist Anti-CD28 Therapeutics in Transplantation

Vanhove¹,

Poirier

Soulillou

et al. 2019

Transplantation

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Nephrotoxicity of calcineurin inhibitors and uncontrolled effector function of alloreactive T lymphocytes are main drivers of transplant dysfunctions. T lymphocytes either directly damage tissues or indirectly promote inflammation and antibody responses. Beside inhibitors of calcium-dependent pathways and anti-metabolites, modulators of T cell costimulation are elected pharmacological tools to enable interference with immune-mediated transplant dysfunctions. CD28 and CTLA-4 are major co-stimulatory and co-inhibitory cell surface signaling molecules interacting with CD80/86, known to be critically important for immune response of committed T cells and regulation. Initial "bench to beside" translation, two decades ago, resulted in the development of belatacept (CTLA4-Ig), a biologic inhibiting interaction of both CD28 and CTLA-4 with CD80/86. Despite proven effectiveness in inhibiting allo-immune responses, clinical use of belatacept in kidney transplantation revealed a substantially high incidence of acute, cell-mediated rejection. The etiology of « belataceptresistant graft rejection » was allocated to elevated pretransplant frequencies of CD28+ memory T cells. Owing to different requirement in CD28 costimulatory and CTLA-4 coinhibitory signals to control naïve and memory T cells, selective antagonists of CD28-CD80/86 interactions have been developed on the rationale that preservation of CTLA4mediated regulatory mechanisms would result in a better control of alloreactivity and would represent a "Treg-compatible" immunosuppression. After the successful testing of selective CD28 antagonists in First In Human studies, this review delineates how this shift in paradigm performed in preclinical transplantation models and evaluates its clinical potential.

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Section: A C C E P T E Dmentioning

confidence: 99%

Selective Costimulation Blockade With Antagonist Anti-CD28 Therapeutics in Transplantation

Vanhove¹,

Poirier

Soulillou

et al. 2019

Transplantation

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“…The approval of belatacept in 2011 demonstrated the potential of a biological non-nephrotoxic maintenance immunosuppression by blocking co-stimulatory signals [ 41 , 42 ]. For the first time since the introduction of cyclosporine, a new immunosuppressant showed an improvement in long-term graft survival.…”

Section: New Immunosuppressive Drugs In the Pipelinementioning

confidence: 99%

Recent advances in kidney transplantation: a viewpoint from the Descartes advisory board*

Abramowicz

Oberbauer

Heemann

et al. 2018

Nephrology Dialysis Transplantation

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Transplantation medicine is a rapidly evolving field. Keeping afloat of the published literature to offer the best clinical care to our patients is a daunting task. As part of its educational mission, the Descartes advisory board identified seven topics in kidney transplantation where there has been substantial progresses over the last years: kidney allocation within Eurotransplant; kidney exchange strategies; kidney machine perfusion strategies; the changing landscape of anti-human leukocyte antigen (HLA) antibodies; the new immunosuppressive drugs in the pipeline; strategies for immunosuppression minimization; and the continuous enigma of focal segmental glomerular sclerosis recurrence after transplantation. Here, we have summarized the main knowledge and the main challenges of these seven topics with the aim to provide transplant professionals at large with key bullet points to successfully understand these new concepts.

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“…The most successful immunosuppressive protocols for xenotransplantation generally include some form of T cell costimulation blockade, by interfering with: (i) the CD28/B7 interaction using CTLA4‐Ig (belatacept) and/or (ii) the CD40/CD154 interaction using anti‐CD40 or anti‐CD154 monoclonal antibodies. Belatacept is approved for clinical solid organ transplantation, and anti‐CD40 is the subject of phase 2 clinical trials in renal transplantation . “High dose” anti‐CD40 was a key component of the protocol used to achieve long‐term cardiac xenograft survival, although some evidence suggests that anti‐CD154 may be more effective than anti‐CD40, at least in the preclinical islet model .…”

Section: Progress Towards Clinically Applicable Immunosuppressionmentioning

confidence: 99%

The 2017 IXA Presidential Lecture: Recent developments in xenotransplantation

Cowan

2018

Xenotransplantation

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The last few years have seen significant progress in xenotransplantation. Porcine xenograft survival in preclinical models continues to improve, accompanied by the adjustment of immunosuppression to more clinically realistic levels. The rapid uptake of CRISPR/Cas9 technology has accelerated the generation of new knock-in and knockout pigs, including animals null for the endogenous retrovirus PERV. This brief review presents a personal view of recent developments in the field. K E Y W O R D Sxenotransplantation in NHP models (all published 2015-2017) F I G U R E 1 Pigs will fly | 3 of 3 COWAN baboons for more than 1 year, 18 and then for more than 2 years. 2 More recently, the elimination of PERV from cultured pig cells 19 and ultimately from pigs 17 spawned numerous articles in both the popular and the scientific press, including the prestigious journal Science. 20 Although the reporting in mainstream media occasionally suggests an incomplete understanding of the science, I believe that this publicity has generally been positive for the field because it familiarizes the public with our work and overturns the previously pessimistic outlook of the broader transplant community. In summary, therefore, I feel privileged to have served as President of the IXA during this exciting period, and I remain very optimistic that "pigs will fly" (Figure 1) sooner rather than later. ORCID Peter J. Cowan

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Costimulation Blockade in Kidney Transplantation

Cited by 37 publications

References 94 publications

Selective Costimulation Blockade With Antagonist Anti-CD28 Therapeutics in Transplantation

Selective Costimulation Blockade With Antagonist Anti-CD28 Therapeutics in Transplantation

Recent advances in kidney transplantation: a viewpoint from the Descartes advisory board*

The 2017 IXA Presidential Lecture: Recent developments in xenotransplantation

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