PROLONGATION OF ALLOGRAFT AND XENOGRAFT SURVIVAL IN MICE BY ANTI-CD2 MONOCLONAL-ANTIBODIES

被引：59

作者：

CHAVIN, KD

LAU, HT

BROMBERG, JS

机构：

[1] MED UNIV S CAROLINA, DEPT SURG, TRANSPLANT PROGRAM 404 CSB, 171 ASHLEY AVE, CHARLESTON, SC 29425 USA

[2] MED UNIV S CAROLINA, DEPT MICROBIOL & IMMUNOL, CHARLESTON, SC 29425 USA

[3] CHILDRENS HOSP PHILADELPHIA, DEPT SURG, PHILADELPHIA, PA 19104 USA

来源：

TRANSPLANTATION | 1992年 / 54卷 / 02期

关键词：

D O I：

10.1097/00007890-199208000-00018

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Anti-CD2 monoclonal antibodies (mAb) were used to influence graft survival in two transplantation models. Xenogeneic rat islets were transplanted intraportally into mice. Anti-CD2 mAb prolonged xenograft survival and was synergistic with UVB irradiation in prolonging survival. Anti-CD2 mAb was also more potent than an anti-CD4 mAb in this model. Allogeneic cardiac grafts were transplanted across an entire H-2 difference and anti-CD2 mAb prolonged allograft survival in a dose-dependent fashion. Kinetic experiments revealed that anti-CD2 mAb was most potent when administered at the time of allografting. A delay in administration of mAb markedly reduced its immunosuppressive effects. Furthermore, additional doses of mAb given after the initial doses provided no increased immunosuppression and anti-CD2 mAbs did not delay rejection of second-set allografts. These findings support the notion that anti-CD2 mAbs interfere with afferent immunity and that CD2 is most important during the initial steps of an immune response. Investigation of the effect of anti-CD2 mAb on cellular immune functions demonstrated, in agreement with previous results, that it caused antigenic down-modulation of CD2 with relative sparing of CD3, CD4, and CD8 cell surface expression. Concommitantly the MLR, CTL, and NK responses were suppressed.

引用

页码：286 / 291

页数：6

共 38 条

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