Targeted Deletion of Fgl-2/Fibroleukin in the Donor Modulates Immunologic Response and Acute Vascular Rejection in Cardiac Xenografts

Author:

Mendicino Michael1,Liu MingFeng1,Ghanekar Anand1,He Wei1,Koscik Cheryl1,Shalev Itay1,Javadi Mojib1,Turnbull Julie1,Chen Wenhao1,Fung Laisum1,Sakamoto Seisuke1,Marsden Phillip1,Waddell Thomas K.1,Phillips M. James1,Gorczynski Reginald1,Levy Gary A.1,Grant David1

Affiliation:

1. From the Multi Organ Transplant Program, University Health Network (M.M., M.L., A.G., W.H., C.K., I.S., M.J., J.T., W.C., L.F., S.S., P.M., T.K.W., M.J.P., R.G., G.A.L., D.G.); Canadian Institutes of Health Research Group on Cellular and Molecular Mechanisms of Organ Injury (M.M., M.L., A.G., C.K., I.S., W.C., P.M., M.J.P., R.G., G.A.L.); Departments of Immunology (M.M., C.K., I.S., M.J., R.G., G.A.L.) and Surgery (A.G., T.K.W., R.G., D.G.), Faculty of Medicine, University of Toronto; Department of...

Abstract

Background— Xenografts ultimately fail as a result of acute vascular rejection (AVR), a process characterized by intravascular thrombosis, fibrin deposition, and endothelial cell activation. Methods and Results— We studied whether targeted deletion of Fgl-2, an inducible endothelial cell procoagulant, (Fgl-2 −/− ) in the donor prevents AVR in a mouse-to-rat cardiac xenotransplantation model. By 3 days after transplant, Fgl-2 +/+ grafts developed typical features of AVR associated with increased levels of donor Fgl-2 mRNA. Grafts from Fgl-2 −/− mice had reduced fibrin deposition but developed cellular rejection. Treatment with a short course of cobra venom factor and maintenance cyclosporine resulted in long-term acceptance of both Fgl-2 +/+ and Fgl-2 −/− grafts. On withdrawal of cyclosporine, Fgl-2 +/+ grafts developed features of AVR; in contrast, Fgl-2 −/− grafts again developed acute cellular rejection. Rejecting Fgl-2 +/+ hearts stained positively for IgG, IgM, C3, and C5b-9, whereas rejecting Fgl-2 −/− hearts had minimal Ig and complement deposition despite xenoantibodies in the serum. Furthermore, serum containing xenoantibodies failed to stain Fgl-2 −/− long-term treated hearts but did stain wild-type heart tissues. Treatment of Fgl-2 −/− xenografts with mycophenolate mofetil and tacrolimus, a clinically relevant immune suppression protocol, led to long-term graft acceptance. Conclusions— Deletion of Fgl-2 ameliorates AVR by downregulation of xenoantigens and may facilitate successful clinical heart xenotransplantation.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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