Anti-lymphocyte function-associated antigen-1 monoclonal antibody inhibits CD40 ligand-independent immune responses and prevents chronic vasculopathy in CD40 ligand-deficient mice.

Matthias Corbascio, Harish Mahanty, Cecilia Österholm, Zhongquan Qi, Thomas C Pearson, Christian P Larsen, Chris E Freise, Henrik Ekberg

    Research output: Contribution to journalArticlepeer-review

    Abstract

    BACKGROUND: Blockade of CD40 ligand (CD40L; CD154, gp39) is a potential treatment for autoimmune disease and allograft rejection. However, CD40L-/- mice are capable of mobilizing cellular immune responses to viral, parasitic, and intracellular bacterial infections as well as rejecting skin grafts with nearly the same efficiency as wild-type mice. CD40L-deficient mice (CD40L-/-) or wild-type mice treated with anti-CD40L develop chronic vasculopathy only 8 weeks after allogeneic heart transplantation. To overcome CD40L-independent immune responses, we used anti-lymphocyte function-associated antigen monoclonal antibody (LFA)-1, which has previously been shown to inhibit CD8+ immune responses. METHODS: We conducted mixed lymphocyte reactions, cytotoxicity assays, skin transplantation, and vascularized heterotopic heart transplantation in wild-type B6 and CD40L-deficient mice in the presence and absence of anti-LFA-1 to study the effects of anti-LFA-1 in the absence of CD40L signaling. RESULTS: Anti-LFA-1 inhibited proliferation of naïve CD40L-/- mixed leukocyte reactions and the lysis of donor targets by CD40L-/- cytotoxic T lymphocytes. Anti-LFA-1-treated CD40L-/- mice that received fully MHC-mismatched skin grafts showed significant prolongation of graft survival, with a median survival time of 55 days (mean 66 days) compared with 13 and 21 days in wild-type and CD40L-/- controls, respectively. CD40L-/- mice that received fully MHC-mismatched vascularized heart transplants treated with four doses of 200 microg of anti-LFA-1 at the time of transplantation did not develop any signs of chronic vasculopathy 150 days after transplantation. CONCLUSION: These results indicate that anti-LFA-1 can complement CD40L inhibition in the prevention of undesirable immune responses.
    Original languageEnglish
    Pages (from-to)35-41
    JournalTransplantation
    Volume74
    Issue number1
    Publication statusPublished - 2002

    Subject classification (UKÄ)

    • Surgery

    Free keywords

    • Skin Transplantation
    • Postoperative Complications : prevention & control
    • Postoperative Complications : immunology
    • Knockout
    • Mice
    • Inbred C57BL
    • Inbred C3H
    • Inbred BALB C
    • Male
    • Heart Transplantation
    • Graft Survival : immunology
    • Graft Rejection : therapy
    • Chronic Disease
    • Cell Division : immunology
    • CD40 Ligand : immunology
    • CD40 Ligand : genetics
    • Monoclonal : pharmacology
    • Antibodies
    • Graft Rejection : immunology
    • Animal
    • Support
    • Non-U.S. Gov't
    • T-Lymphocytes
    • Cytotoxic : cytology
    • Cytotoxic : immunology
    • Transplantation
    • Homologous
    • Vascular Diseases : immunology
    • Vascular Diseases : prevention & control
    • Vascular Diseases : therapy

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