Long-term kidney graft survival by delayed T cell ablative treatment in rhesus monkeys

M Jonker; J Ringers; Miriam Ossevoort; W Slingerland; Y van den Hout; K Haanstra; J Wubben; E Kuhn; P Friend; R Calne

Long-term kidney graft survival by delayed T cell ablative treatment in rhesus monkeys

M Jonker^*, J Ringers, Miriam Ossevoort, W Slingerland, Y van den Hout, K Haanstra, J Wubben, E Kuhn, P Friend, R Calne

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

17 Citations (Scopus)

Abstract

Background. Tolerance to organ allografts in primates including man has been elusive, although in rodents and pigs tolerance can be achieved to organ allografts with relatively short courses of immunosuppressive treatment. In all varieties of graft acceptance that do not require full-dose maintenance immunosuppression, immunological engagement of donor and recipient and an early unstable period have been observed. On the basis of the hypothesis that elimination of aggressive T cell function should tip the balance in favor of an operationally tolerant state, experiments have been performed in monkeys allowing recipient-donor interaction before T-cell ablation and a short course of immunosuppression.

Methods. Rhesus monkeys received an allogeneic kidney graft from a MHC-mismatched donor. The animals either received anti-CD3 immunotoxin (FN18-CRM9) alone, started 2 days after transplantation, or in combination with a short course of cyclosporine (CsA) and/or rapamycin (RAPA), started at 5 days after transplantation. Kidney function was followed by monitoring serum creatinine levels and regular biopsies. Humoral and cellular antidonor immunity was tested in vitro before and at several time points after transplantation.

Results. Graft survival of monkeys that received CsA alone (mean survival time (MST)=29.3) was significantly prolonged compared with the controls (MST=6). FN18-CRM9 treatment alone also resulted in prolonged graft survival (MST=29.4). The combined treatment of FN18-CRM9 and CsA and/or RAPA resulted in prolonged graft survival after all immunosuppression was stopped (MST=207.8).

Conclusions. It seems feasible to postpone immunosuppression posttransplantation and yet prevent allograft rejection without the need of permanent immunosuppression.

Original language	English
Article number	UNSP 0041-1337/02/7306-874/0
Pages (from-to)	874-880
Number of pages	7
Journal	Transplantation
Volume	73
Issue number	6
Publication status	Published - 27-Mar-2002
Externally published	Yes
Event	Congress on New Dimensions in Transplantation - Weaving the Future - , Italy Duration: 16-Feb-1998 → 19-Feb-1998

Keywords

DOSE CYCLOSPORINE MONOTHERAPY
RENAL-TRANSPLANT RECIPIENTS
IMMUNOSUPPRESSANT SDZ-RAD
ALLOGRAFT RECIPIENTS
MONOCLONAL-ANTIBODY
COMPLETE WITHDRAWAL
PROPE TOLERANCE
CAMPATH 1H
PRIMATES
SIROLIMUS

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@article{9cae93e15cf64a4183ef6ba7d87aab6b,

title = "Long-term kidney graft survival by delayed T cell ablative treatment in rhesus monkeys",

abstract = "Background. Tolerance to organ allografts in primates including man has been elusive, although in rodents and pigs tolerance can be achieved to organ allografts with relatively short courses of immunosuppressive treatment. In all varieties of graft acceptance that do not require full-dose maintenance immunosuppression, immunological engagement of donor and recipient and an early unstable period have been observed. On the basis of the hypothesis that elimination of aggressive T cell function should tip the balance in favor of an operationally tolerant state, experiments have been performed in monkeys allowing recipient-donor interaction before T-cell ablation and a short course of immunosuppression.Methods. Rhesus monkeys received an allogeneic kidney graft from a MHC-mismatched donor. The animals either received anti-CD3 immunotoxin (FN18-CRM9) alone, started 2 days after transplantation, or in combination with a short course of cyclosporine (CsA) and/or rapamycin (RAPA), started at 5 days after transplantation. Kidney function was followed by monitoring serum creatinine levels and regular biopsies. Humoral and cellular antidonor immunity was tested in vitro before and at several time points after transplantation.Results. Graft survival of monkeys that received CsA alone (mean survival time (MST)=29.3) was significantly prolonged compared with the controls (MST=6). FN18-CRM9 treatment alone also resulted in prolonged graft survival (MST=29.4). The combined treatment of FN18-CRM9 and CsA and/or RAPA resulted in prolonged graft survival after all immunosuppression was stopped (MST=207.8).Conclusions. It seems feasible to postpone immunosuppression posttransplantation and yet prevent allograft rejection without the need of permanent immunosuppression.",

keywords = "DOSE CYCLOSPORINE MONOTHERAPY, RENAL-TRANSPLANT RECIPIENTS, IMMUNOSUPPRESSANT SDZ-RAD, ALLOGRAFT RECIPIENTS, MONOCLONAL-ANTIBODY, COMPLETE WITHDRAWAL, PROPE TOLERANCE, CAMPATH 1H, PRIMATES, SIROLIMUS",

author = "M Jonker and J Ringers and Miriam Ossevoort and W Slingerland and {van den Hout}, Y and K Haanstra and J Wubben and E Kuhn and P Friend and R Calne",

year = "2002",

month = mar,

day = "27",

language = "English",

volume = "73",

pages = "874--880",

journal = "Transplantation",

issn = "0041-1337",

publisher = "Lippincott Williams and Wilkins",

number = "6",

note = "Congress on New Dimensions in Transplantation - Weaving the Future ; Conference date: 16-02-1998 Through 19-02-1998",

}

TY - JOUR

T1 - Long-term kidney graft survival by delayed T cell ablative treatment in rhesus monkeys

AU - Jonker, M

AU - Ringers, J

AU - Ossevoort, Miriam

AU - Slingerland, W

AU - van den Hout, Y

AU - Haanstra, K

AU - Wubben, J

AU - Kuhn, E

AU - Friend, P

AU - Calne, R

PY - 2002/3/27

Y1 - 2002/3/27

N2 - Background. Tolerance to organ allografts in primates including man has been elusive, although in rodents and pigs tolerance can be achieved to organ allografts with relatively short courses of immunosuppressive treatment. In all varieties of graft acceptance that do not require full-dose maintenance immunosuppression, immunological engagement of donor and recipient and an early unstable period have been observed. On the basis of the hypothesis that elimination of aggressive T cell function should tip the balance in favor of an operationally tolerant state, experiments have been performed in monkeys allowing recipient-donor interaction before T-cell ablation and a short course of immunosuppression.Methods. Rhesus monkeys received an allogeneic kidney graft from a MHC-mismatched donor. The animals either received anti-CD3 immunotoxin (FN18-CRM9) alone, started 2 days after transplantation, or in combination with a short course of cyclosporine (CsA) and/or rapamycin (RAPA), started at 5 days after transplantation. Kidney function was followed by monitoring serum creatinine levels and regular biopsies. Humoral and cellular antidonor immunity was tested in vitro before and at several time points after transplantation.Results. Graft survival of monkeys that received CsA alone (mean survival time (MST)=29.3) was significantly prolonged compared with the controls (MST=6). FN18-CRM9 treatment alone also resulted in prolonged graft survival (MST=29.4). The combined treatment of FN18-CRM9 and CsA and/or RAPA resulted in prolonged graft survival after all immunosuppression was stopped (MST=207.8).Conclusions. It seems feasible to postpone immunosuppression posttransplantation and yet prevent allograft rejection without the need of permanent immunosuppression.

AB - Background. Tolerance to organ allografts in primates including man has been elusive, although in rodents and pigs tolerance can be achieved to organ allografts with relatively short courses of immunosuppressive treatment. In all varieties of graft acceptance that do not require full-dose maintenance immunosuppression, immunological engagement of donor and recipient and an early unstable period have been observed. On the basis of the hypothesis that elimination of aggressive T cell function should tip the balance in favor of an operationally tolerant state, experiments have been performed in monkeys allowing recipient-donor interaction before T-cell ablation and a short course of immunosuppression.Methods. Rhesus monkeys received an allogeneic kidney graft from a MHC-mismatched donor. The animals either received anti-CD3 immunotoxin (FN18-CRM9) alone, started 2 days after transplantation, or in combination with a short course of cyclosporine (CsA) and/or rapamycin (RAPA), started at 5 days after transplantation. Kidney function was followed by monitoring serum creatinine levels and regular biopsies. Humoral and cellular antidonor immunity was tested in vitro before and at several time points after transplantation.Results. Graft survival of monkeys that received CsA alone (mean survival time (MST)=29.3) was significantly prolonged compared with the controls (MST=6). FN18-CRM9 treatment alone also resulted in prolonged graft survival (MST=29.4). The combined treatment of FN18-CRM9 and CsA and/or RAPA resulted in prolonged graft survival after all immunosuppression was stopped (MST=207.8).Conclusions. It seems feasible to postpone immunosuppression posttransplantation and yet prevent allograft rejection without the need of permanent immunosuppression.

KW - DOSE CYCLOSPORINE MONOTHERAPY

KW - RENAL-TRANSPLANT RECIPIENTS

KW - IMMUNOSUPPRESSANT SDZ-RAD

KW - ALLOGRAFT RECIPIENTS

KW - MONOCLONAL-ANTIBODY

KW - COMPLETE WITHDRAWAL

KW - PROPE TOLERANCE

KW - CAMPATH 1H

KW - PRIMATES

KW - SIROLIMUS

M3 - Article

SN - 0041-1337

VL - 73

SP - 874

EP - 880

JO - Transplantation

JF - Transplantation

IS - 6

M1 - UNSP 0041-1337/02/7306-874/0

T2 - Congress on New Dimensions in Transplantation - Weaving the Future

Y2 - 16 February 1998 through 19 February 1998

ER -

Long-term kidney graft survival by delayed T cell ablative treatment in rhesus monkeys

Abstract

Keywords

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