Relevance of cytotoxic alloreactivity under different immunosuppressive regimens in clinical islet cell transplantation

Author:

Roelen D L1,Huurman V A L12,Hilbrands R3,Gillard P34,Duinkerken G1,Van Der Meer-Prins P W M1,Versteeg-van der Voort Maarschalk M F J1,Mathieu C4,Keymeulen B3,Pipeleers D G3,Roep B O1,Claas F H J1

Affiliation:

1. Department of Immunohaematology and Blood Transfusion and

2. Department of Surgery, Leiden University Medical Centre, Leiden, the Netherlands

3. Diabetes Research Centre, Brussels Free University-VUB, Brussels, Belgium

4. Laboratory for Experimental Medicine and Endocrinology (LEGENDO), University Hospital Gasthuisberg, Catholic University of Leuven-KUL, Belgium

Abstract

Summary Islet or β cell transplantation provides a promising cure for type 1 diabetes patients, but insulin-independency decreases frequently over time. Immunosuppressive regimens are implemented attempting to cope with both auto- and alloimmunity after transplantation. We analysed the influence of different immunotherapies on autoreactive and alloreactive T cell patterns and transplant outcome. Patients receiving three different immunosuppressive regimens were analysed. All patients received anti-thymocyte globulin induction therapy. Twenty-one patients received tacrolimus–mycophenolate mofetil maintenance immunosuppression, whereas the other patients received tacrolimus–sirolimus (SIR, n = 5) or SIR only (n = 5). Cellular autoreactivity and alloreactivity (CTL precursor frequency) were measured ex vivo. Clinical outcome in the first 6 months after transplantation was correlated with immunological parameters. C-peptide levels were significantly different between the three groups studied (P = 0·01). We confirm that C-peptide production was correlated negatively with pretransplant cellular autoreactivity and low graft size (P = 0·001, P = 0·007 respectively). Combining all three therapies, cellular autoimmunity after transplantation was not associated with delayed insulin-independence or C-peptide production. In combined tacrolimus–SIR and SIR-treated patients, CTL alloreactivity was associated with less insulin independence and C-peptide production (P = 0·03). The percentage of donors to whom high CTLp frequencies were measured was lower in insulin-independent recipients (P = 0·03). In this cohort of islet cell graft recipients, clinical outcome in the first 6 months after transplantation correlates with the applied immunosuppressive regimen. An association exists between insulin-independence and lower incidence of CTL alloreactivity towards donor human leucocyte antigen. This observational study demonstrates the usefulness of monitoring T cell reactivity against islet allografts to correlate immune function with graft survival.

Publisher

Oxford University Press (OUP)

Subject

Immunology,Immunology and Allergy

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