Recombinant Human C1-inhibitor Prevents Acute Antibody-mediated Rejection in Alloimmunized Baboons

Overview

Journal Kidney Int

Publisher Elsevier

Specialty Nephrology

Date 2010 Mar 26

PMID 20336054

Citations 30

Authors

Xavier Tillou

Nicolas Poirier

Stephanie Le Bas-Bernardet

Jeremy Hervouet

David Minault

Karine Renaudin

Fabio Vistoli

Georges Karam

Mohamed Daha

Jean Paul Soulillou

Gilles Blancho

Affiliations

Soon will be listed here.

Abstract

Acute antibody-mediated rejection is an unsolved issue in transplantation, especially in the context of pretransplant immunization. The deleterious effect of preformed cytotoxic anti-HLA antibodies through complement activation is well proven, but very little is known concerning complement blockade to prevent/cure this rejection. Here, we used a baboon model of preimmunization to explore the prevention of acute antibody-mediated rejection by an early inhibition of the classical complement pathway using human recombinant C1-inhibitor. Baboons were immunized against peripheral blood mononuclear cells from allogeneic donors and, once a specific and stable immunization had been established, they received a kidney from the same donor. Rejection occurred at day 2 posttransplant in untreated presensitized recipients, with characteristic histological lesions and complement deposition. As recombinant human C1-inhibitor blocks in vitro cytotoxicity induced by donor-specific antibodies, other alloimmunized baboons received the drug thrice daily intravenously during the first 5 days after transplant. Rejection was prevented during this treatment but occurred after discontinuation of treatment. We show here that early blockade of complement activation by recombinant human C1-inhibitor can prevent acute antibody-mediated rejection in presensitized recipients. This treatment could also be useful in other forms of acute antibody-mediated rejection caused by induced antibodies.

Citing Articles

Complement networks in gene-edited pig xenotransplantation: enhancing transplant success and addressing organ shortage.

Yuan Y, Cui Y, Zhao D, Yuan Y, Zhao Y, Li D J Transl Med. 2024; 22(1):324.

PMID: 38566098 PMC: 10986007. DOI: 10.1186/s12967-024-05136-4.

MHC Class I Masking to Prevent AMR in a Porcine Kidney Transplantation Model in Alloimmunized Recipients.

Kervella D, Branchereau J, Prudhomme T, Nerriere-Daguin V, Renaudin K, Minault D Transplant Direct. 2023; 9(6):e1490.

PMID: 37250484 PMC: 10219698. DOI: 10.1097/TXD.0000000000001490.

Complement-targeted therapies in kidney transplantation-insights from preclinical studies.

Anwar I, DeLaura I, Ladowski J, Gao Q, Knechtle S, Kwun J Front Immunol. 2022; 13:984090.

PMID: 36311730 PMC: 9606228. DOI: 10.3389/fimmu.2022.984090.

The oxygen carrier M101 alleviates complement activation, which may be beneficial for donor organ preservation.

Puissant-Lubrano B, Bouthemy C, Congy-Jolivet N, Milhes J, Minville V, Kamar N Front Immunol. 2022; 13:1006761.

PMID: 36172347 PMC: 9511029. DOI: 10.3389/fimmu.2022.1006761.

Protection of transplants against antibody-mediated injuries: from xenotransplantation to allogeneic transplantation, mechanisms and therapeutic insights.

Kervella D, Le Bas-Bernardet S, Bruneau S, Blancho G Front Immunol. 2022; 13:932242.

PMID: 35990687 PMC: 9389360. DOI: 10.3389/fimmu.2022.932242.