CD4 AND CD8 MONOCLONAL-ANTIBODY THERAPY - STRATEGIES TO PROLONG RENAL-ALLOGRAFT SURVIVAL IN THE DOG

被引：6

作者：

WATSON, CJE ^{[1
]}

COBBOLD, SP ^{[1
]}

DAVIES, HFS ^{[1
]}

REBELLO, PRUB ^{[1
]}

WALDMANN, H ^{[1
]}

CALNE, RY ^{[1
]}

METCALFE, SM ^{[1
]}

机构：

[1] ADDENBROOKES HOSP,DEPT IMMUNOL,CAMBRIDGE CB2 2QQ,ENGLAND

来源：

BRITISH JOURNAL OF SURGERY | 1993年 / 80卷 / 11期

关键词：

D O I：

10.1002/bjs.1800801111

中图分类号：

R61 [外科手术学];

学科分类号：

摘要：

The value of CD4 and CD8 monoclonal antibody therapy in tolerance induction has been demonstrated in rodent transplant models. In this paper the immunosuppressive potential of CD4 and CD8 monoclonal antibodies for dog renal allografts was evaluated as a preliminary fo tolerogenic studies in this large animal model. Monoclonal antibodies were given for a maximum of 10 days after transplantation. Therapy was stopped prematurely following adverse reactions associated with the recipient developing an antibody response against the foreign (rat) therapeutic monoclonal antibody. Blood trough levels of CD4 and CD8 antibodies indicated that saturating doses were achieved. Although neither CD4 nor CD8 alone prolonged allograft survival (rejection by day 7), combination of CD4 and CD8 antibodies resulted in good graft function for a median of 14 days. The effect of removing circulating T lymphocytes was also assessed using a lytic Thy-1 monoclonal antibody. Alone Thy-1 had little effect but, when combined with CD4, the median allograft survival time was increased to 15.5 days. Reduction of the number of circulating T lymphocytes appears complementary to blockade of CD4 for immunosuppression, while blockade of CD4 combined with removal of CD8 also favours allograft survival.

引用

页码：1389 / 1392

页数：4

共 16 条

[1]

ABAZA H. M., 1966, TRANSPLANTATION, V4, P618, DOI 10.1097/00007890-196609000-00008

[2] INDUCTION OF TOLERANCE BY MONOCLONAL-ANTIBODY THERAPY [J].

BENJAMIN, RJ ;

WALDMANN, H .

NATURE, 1986, 320 (6061) :449-451

[3]

CALNE R Y, 1977, IRCS (International Research Communications System) Medical Science Library Compendium, V5, P595

[4]

CALNE R Y, 1961, Surg Forum, V12, P118

[5] TOLERANCE IN THE MOUSE TO MAJOR HISTOCOMPATIBILITY COMPLEX-MISMATCHED HEART ALLOGRAFTS, AND TO RAT-HEART XENOGRAFTS, USING MONOCLONAL-ANTIBODIES TO CD4 AND CD8 [J].

CHEN, ZH ;

COBBOLD, S ;

METCALFE, S ;

WALDMANN, H .

EUROPEAN JOURNAL OF IMMUNOLOGY, 1992, 22 (03) :805-810

[6] A SIMPLE METHOD FOR MEASURING PATIENT ANTI-GLOBULIN RESPONSES AGAINST ISOTYPIC OR IDIOTYPIC DETERMINANTS [J].

COBBOLD, SP ;

REBELLO, PRUB ;

DAVIES, HFS ;

FRIEND, PJ ;

CLARK, MR .

JOURNAL OF IMMUNOLOGICAL METHODS, 1990, 127 (01) :19-24

[7] THE INDUCTION OF SKIN-GRAFT TOLERANCE IN MAJOR HISTOCOMPATIBILITY COMPLEX-MISMATCHED OR PRIMED RECIPIENTS - PRIMED T-CELLS CAN BE TOLERIZED IN THE PERIPHERY WITH ANTI-CD4 AND ANTI-CD8 ANTIBODIES [J].

COBBOLD, SP ;

MARTIN, G ;

WALDMANN, H .

EUROPEAN JOURNAL OF IMMUNOLOGY, 1990, 20 (12) :2747-2755

[8]

COSIMI AB, 1990, SURGERY, V108, P406

[9] EVIDENCE THAT LONG-TERM CARDIAC ALLOGRAFT SURVIVAL INDUCED BY ANTI-CD4 MONOCLONAL-ANTIBODY DOES NOT REQUIRE DEPLETION OF CD4+ T-CELLS [J].

DARBY, CR ;

MORRIS, PJ ;

WOOD, KJ .

TRANSPLANTATION, 1992, 54 (03) :483-490

[10] ADOPTIVE TRANSFER OF FIRST-SET ALLOGRAFT RESPONSES BY RECIRCULATING SMALL LYMPHOCYTES IN RAT [J].

DORSCH, S ;

ROSER, B .

AUSTRALIAN JOURNAL OF EXPERIMENTAL BIOLOGY AND MEDICAL SCIENCE, 1974, 52 (FEB) :33-44

← 1 2 →