Combination Proteasome Inhibition and Anti-BAFF Therapy Permits Highly Sensitized Rhesus Kidney Transplantation

B. Ezekian, J. Kwun, M. Manook, P. Schroder, J. Yoon, M. Mulvihill, K. Freischlag, J. Park, J. Cochran, K. Kroning, J. Yi, S. Knechtle.

Duke Transplant Center, Duke University Medical Center, Durham, NC.

Meeting: 2018 American Transplant Congress

Abstract number: 160

Keywords: B cells, HLA antibodies, Kidney transplantation, Primates

Session Information

Session Name: Concurrent Session: Novel Therapeutics

Session Type: Concurrent Session

Date: Sunday, June 3, 2018

Session Time: 4:30pm-6:00pm

Presentation Time: 4:42pm-4:54pm

Location: Room 602/603/604

Purpose:

HLA-sensitization is a significant immunologic barrier to successful kidney transplantation (KT). We have shown that proteasome inhibition (PI) in insolation reduces plasma cells (PCs), but does not impact donor-specific antibodies (DSA) due to upstream germinal center (GC) compensation. We hypothesized that PC depletion with carfilzomib (CFZ), a 2^nd generation PI, and arrest of differentiation of upstream naive B cells with tabalumab (TAB), an anti-BAFF monoclonal antibody (mAb), would permit successful renal allotransplantation in highly sensitized nonhuman primates.

Methods:

Maximally MHC-mismatched rhesus pairs were sensitized with two sequential skin transplants and then desensitized with CFZ (20 mg/m² IV) and TAB (100 mg IV) weekly for one month. Peripheral blood, lymph node (LN), and bone marrow (BM) cells were analyzed pre- and post-desensitization. Anti-CD4 and CD8 depletion was given and swapping KT was performed. Animals were maintained on conventional triple immunosuppression post-transplant and closely monitored.

Results:

CFZ/TAB (n=6) reduced mean DSA by 57% (p=0.0173). Peripheral CD4, CD8, and CD20 counts were unchanged by desensitization treatment. However, CFZ/TAB reduced peripheral PCs (mean 4.2% to 2.4% CD3^[mdash]CD20^[mdash]CD27⁺CD38⁺ cells, p=0.0026) and LN Tfh cells (mean 4.4% to 2.7% CD3⁺CD4⁺PD1^highICOS⁺cells, p=0.0393). CFZ/TAB did not change populations of Treg, CD4 Tnaïve, CD4 Tcm, CD4 Tem, CD8 Tnaive, CD8 Tcm, or CD8 Tem cells. CFZ/TAB prolonged median survival to 61 days (vs. 5 days in controls, log rank test p=0.01). CFZ/TAB with anti-CD4/CD8 mAb induction reactivated rhCMV.

Conclusion:

CFZ/TAB was associated with a moderate reduction of DSA and prolonged graft survival in a highly sensitized rhesus model of KT. A possible mechanism for prolonged survival includes collapse of the GC by concurrently inhibiting PCs and upstream Tfh cells. This desensitization regimen in combination with T cell depletion impaired protective viral immunity.

CITATION INFORMATION: Ezekian B., Kwun J., Manook M., Schroder P., Yoon J., Mulvihill M., Freischlag K., Park J., Cochran J., Kroning K., Yi J., Knechtle S. Combination Proteasome Inhibition and Anti-BAFF Therapy Permits Highly Sensitized Rhesus Kidney Transplantation Am J Transplant. 2017;17 (suppl 3).

To cite this abstract in AMA style:

Ezekian B, Kwun J, Manook M, Schroder P, Yoon J, Mulvihill M, Freischlag K, Park J, Cochran J, Kroning K, Yi J, Knechtle S. Combination Proteasome Inhibition and Anti-BAFF Therapy Permits Highly Sensitized Rhesus Kidney Transplantation [abstract]. https://atcmeetingabstracts.com/abstract/combination-proteasome-inhibition-and-anti-baff-therapy-permits-highly-sensitized-rhesus-kidney-transplantation/. Accessed November 24, 2024.

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