ALPHA/BETA-T CELL RECEPTOR-DIRECTED THERAPY IN RAT CARDIAC ALLOGRAFT RECIPIENTS - TREATMENT PRIOR TO ALLOANTIGEN EXPOSURE PREVENTS SENSITIZATION AND ABROGATES ACCELERATED REJECTION

被引：22

作者：

HEIDECKE, CD

HANCOCK, WW

JAKOBS, F

ZANTL, N

KURRLE, R

WESTERHOLT, S

SEWCZIK, T

DEUSCH, K

KUPIECWEGLINSKI, J

机构：

[1] TECH UNIV MUNICH, KLINIKUM RECHTS ISAR, DEPT MED, D-81675 MUNICH, GERMANY

[2] BEHRING WERKE, D-35041 MARBURG, GERMANY

[3] MONASH UNIV SCH MED, DEPT PATHOL & IMMUNOL, PRAHRAN, VIC, AUSTRALIA

[4] HARVARD UNIV, SCH MED, SURG RES LAB, BOSTON, MA 02115 USA

来源：

TRANSPLANTATION | 1995年 / 59卷 / 01期

关键词：

D O I：

10.1097/00007890-199501150-00014

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

An mAb directed to the alpha/beta-heterodimer of the rat T cell receptor was used to prevent rejection of cardiac allografts in sensitized (accelerated rejection) recipients. Over a wide dose range, alpha/beta-TCR-directed therapy abrogated accelerated rejection at 24-36 hr and extended cardiac allograft survival in a dose-dependent fashion, both when given after heart transplantation as well as during or before the sensitizing skin transplants (8.9+/-1.0 days, 12.7+/-0.6 days, or 8.7+/-1.5 days, respectively). Pretreatment with R73 completely abrogated host sensitization induced by skin grafting. As a result, post-heart transplant cyclosporine course (15 mg/kg for 7 day) has led to long-term graft acceptance (> 90 days vs. 15.2+/-1.6 days with postoperative CsA therapy alone). Administration of R73 mAb produced incomplete depletion (CD5(+) cells) and partial modulation (alpha/beta-TCR/CD5 double-positive cells) in the peripheral blood. It suppressed in situ protein expression of many cytokines to background levels, in particular that of IL-2 and IFN-gamma, both when given after as well as before cardiac transplantation. However, only pretransplant mAb application was associated with augmented in situ elaboration of IL-4. alpha/beta-TCR-directed therapy induced strong host antiidiotypic and, to a lesser degree, anti-isotypic antibody responses. Taken together, these results provide the rationale for a novel immunosuppressive strategy involving induction of hyporesponsiveness by alpha/beta-TCR-directed therapy before the alloantigenic exposure.

引用

页码：78 / 84

页数：7

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