Blockade of CD40-CD154 Costimulatory Pathway Promotes Survival of Allogeneic Corneal Transplants

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Blockade of CD40-CD154 Costimulatory Pathway Promotes Survival of Allogeneic Corneal Transplants

Ying Qian, Florence Boisgerault, Gilles Benichou and M. Reza Dana

From the Schepens Eye Research Institute, Department of Ophthalmology, Harvard Medical School, Boston, Massachusetts.

PURPOSE. To determine the effect of systemic anti-CD154 monoclonalantibody on the survival of orthotopic murine corneal transplants.

METHODS. BALB/c mice were used as recipients of syngeneic, multipleminor histocompatability (H)–disparate, or major histocompatibilitycomplex MHC-mismatched corneal transplants. Recipient beds wereeither avascular (normal risk) or neovascularized (high risk).Mice were randomized to receive either anti-CD154 antibody orcontrol immunoglobulin by intraperitoneal injection at surgeryand once weekly after surgery. After orthotopic corneal transplantation,all grafts were evaluated for signs of rejection by slit lampbiomicroscopy over 8 weeks. The high-risk transplants were continuouslyobserved until week 18 after the therapy was discontinued atweek 8. Allospecific delayed-type hypersensitivity (DTH) wasevaluated after transplantation in high-risk graft recipients.Frequency of interferon (IFN)- ${gamma}$ –secreting T cells in thehosts was measured by enzyme-linked immunospot (ELISPOT) assay.

RESULTS. In normal-risk transplantation, the 8-week survivalrate improved from 25% in control mice to 88% in anti-CD154–treatedhosts of minor H–disparate grafts (P = 0.0087) and from78% in control mice to 100% in anti-CD154–treated recipientsof MHC-mismatched transplants (P = 0.177). Of particular significance,in high-risk transplantation, anti-CD154 therapy dramaticallyenhanced the survival of both minor H– and MHC-disparatecorneal transplants to 100% (P = 0.0001) and 92% (P = 0.0002),respectively. In addition, the anti-CD154–treated micedid not exhibit allospecific immunity. However, terminationof anti-CD154 led to some loss in graft survival, especiallyamong high-risk minor H–disparate grafts. The frequencyof IFN- ${gamma}$ –producing T cells was significantly reduced in anti-CD154–treatedhosts.

CONCLUSIONS. Continuous suppression of the CD40-CD154 costimulatorypathway promotes the acceptance of corneal transplants, regardlessof the degree of allodisparity or preoperative risk. The beneficialeffect of anti-CD154 treatment may be due in part to inhibitionof Th1-mediated responses.

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