Methylprednisolone prevents rejection of intrastriatal grafts of xenogeneic embryonic neural tissue in adult rats

被引:22
作者
Duan, WM
Brundin, P
GrasbonFrodl, EM
Widner, H
机构
[1] Section for Neuronal Survival, Dept. of Physiology and Neuroscience, S-223 62 Lund
关键词
methylprednisolone; cyclosporin A; neural transplantation; xenograft; immunology; inflammation; cytokine; brain; rat;
D O I
10.1016/0006-8993(95)01409-8
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
We studied the effects of high-dose methylprednisolone on the survival of intrastriatal neural xenografts and the host responses against them. Dissociated mesencephalic tissue from inbred mouse (CBA-strain) embryos was transplanted to the intact striatum of adult Sprague-Dawley rats. The rats received either daily injections of methylprednisolone (30 mg/kg), or cyclosporin A (10 mg/kg), or no immunosuppressive treatment. Two or six weeks after transplantation, there was good survival of xenografts in both the methylprednisolone- and cyclosporin A-treated rats. In contrast, the xenografts in untreated control rats were all rejected by six weeks. There was no marked difference in the degree of expression of MHC class I and II antigens and the accumulation of activated astrocytes and microglial cells/macrophages between the three groups. However, both methylprednisolone and cyclosporin A reduced infiltration of T lymphocytes to the transplantation sites. The expression of pro-inflammatory cytokines (interferon-gamma, tumour necrosis factor-alpha, interleukin-6) in and around the grafts was lower in the methylprednisolone- and cyclosporin A-treated groups than in untreated control rats. Although high-dose methylprednisolone caused significant body weight loss, we conclude that this treatment can prevent rejection of intrastriatal grafts of xenogeneic embryonic neural tissue in the adult.
引用
收藏
页码:199 / 212
页数:14
相关论文
共 58 条
[1]   ESTIMATION OF NUCLEAR POPULATION FROM MICROTOME SECTIONS [J].
ABERCROMBIE, M .
ANATOMICAL RECORD, 1946, 94 (02) :239-247
[2]   ENDOTHELIAL-CELL ACTIVATION AND THROMBOREGULATION DURING XENOGRAFT REJECTION [J].
BACH, FH ;
ROBSON, SC ;
FERRAN, C ;
WINKLER, H ;
MILLAN, MT ;
STUHLMEIER, KM ;
VANHOVE, B ;
BLAKELY, ML ;
VANDERWERF, WJ ;
HOFER, E ;
DEMARTIN, R ;
HANCOCK, WW .
IMMUNOLOGICAL REVIEWS, 1994, 141 :5-30
[3]  
BARKER CF, 1977, ADV IMMUNOL, V25, P1
[4]   METHYLPREDNISOLONE INHIBITS EARLY INFLAMMATORY PROCESSES BUT NOT ISCHEMIC CELL-DEATH AFTER EXPERIMENTAL SPINAL-CORD LESION IN THE RAT [J].
BARTHOLDI, D ;
SCHWAB, ME .
BRAIN RESEARCH, 1995, 672 (1-2) :177-186
[5]  
BENVENISTE EN, 1994, J IMMUNOL, V153, P5210
[6]   CONTROL OF CACHECTIN (TUMOR-NECROSIS-FACTOR) SYNTHESIS - MECHANISMS OF ENDOTOXIN RESISTANCE [J].
BEUTLER, B ;
KROCHIN, N ;
MILSARK, IW ;
LUEDKE, C ;
CERAMI, A .
SCIENCE, 1986, 232 (4753) :977-980
[7]   CROSS-SPECIES NEURAL GRAFTING IN A RAT MODEL OF PARKINSONS-DISEASE [J].
BJORKLUND, A ;
STENEVI, U ;
DUNNETT, SB ;
GAGE, FH .
NATURE, 1982, 298 (5875) :652-654
[8]  
BRUNDIN P, 1985, EXP BRAIN RES, V60, P204
[9]  
BRUNDIN P, 1989, EXP BRAIN RES, V75, P195
[10]   THE EFFECTS OF METHYLPREDNISOLONE AND THE GANGLIOSIDE GM1 ON ACUTE SPINAL-CORD INJURY IN RATS [J].
CONSTANTINI, S ;
YOUNG, W .
JOURNAL OF NEUROSURGERY, 1994, 80 (01) :97-111