机构地区:[1]华中科技大学同济医学院附属协和医院血液病学研究所,武汉430022 [2]武汉大学人民医院小儿科 [3]华中科技大学同济医学院免疫学研究所
出 处:《中华器官移植杂志》2001年第6期331-335,共5页Chinese Journal of Organ Transplantation
基 金:国家自然科学基金资助项目 ( 39770 76 7)
摘 要:目的 通过Fas配体 (FasL) Fas途径清除异体骨髓移植 (allo BMT)物中针对受体主要组织相容复合物 (MHC)的淋巴细胞 ,从而抑制受体发生移植物抗宿主病 (GVHD)。方法 实验组 (5组 )用磁性细胞分离系统分离BALB/C小鼠 (H 2d ,雌性 )早期造血细胞 (HC) ,经逆转录病毒法转移外源mFasLcDNA基因并扩增 1w后与BAC小鼠 (H 2d×b ,雄性 )骨髓单个核细胞 (BMMC)按 0 .6 2 5∶1混合培养 1w ,经尾静脉将 5× 10 6个混合细胞 (0 .5ml)注入经全身60 Coγ照射的BALB/C小鼠。同时设立 :1组 (空白对照组 ,未移植细胞 ) ;2组 (同基因BMT组 ) ;3组 (转染外源FasL的同基因BALB/CHC +正常BALB/C小鼠BMMC混合培养后移植组 ) ;4组 (H 2单倍型不同小鼠的allo BMT组 )。观察移植鼠的造血重建及细胞来源、GVHD、生存率和造血重建后的免疫学特征。结果 BMT后 +10d、+2 0d ,实验组、3和 4组的外周血白细胞、血小板计数均低于 2组 (P <0 .0 1) ,但 +30d后以上各组则均恢复正常。实验组中存活 2个月的 8只BALB/C小鼠 ,其BMMC中供体来源Y染色体出现率为 (81.14± 5 .3) % ,其中 1例脾细胞基因组DNA经PCR检出Neor 和mFasLcDNA整合 ;各组移植 2个月后的生存率为 :实验组 80 %、1组 0 %、2、3组均为 10 0 %、4组 2 0 % 。ObjectiveTo induce bone marrow receptor's immune priviledge against graft versus host disease (GVHD) by specific elimination of mouse aloreactive T cells through Fas ligand (FasL) Fas way. Methods irst, the stem cell antigen 1 (sca 1) + early hematopoietic cells (EHC) of BALB/C mouse (H 2d, female) were isolated by using a magnetic cell sorting syste.The exogenous mFasL cDNA gene was transferred to these cells by retrovirus gene transfer system and expanded in liquid culture system for one week. Then, in the experimental group these expanded hematopoietic cells (HC) were co cultured with bone marrow mononuclear cells (BMMC) form BAC mouse (H 2?d×b, male) at the ratio of 0.625 to l for another one week. Last, 5×10 6 ( 0.5?ml) mixed viable cells were injected into whole bodily irradiated ( 60Co γ) mice (6 to 8 week old female BALB/C) via the tail vein. The following four groups of grafted BALB/C mice were simultaneously used: (1) the mice transplanted with 0.5?ml culture medium; (2) the mice transplanted with BMMC from normal ALB/C mice; (3) the ice transplanted with mixed cells, in which exogenous mFasL gene transferred BALB/C HC were cocultured with BALB/C BMMC for one week; (4) the mice transplanted with BMMC from H 2 haplotype disparate BAC mice. The hematopoietic reconstitution, the origion of bone marrow cells responsible for the reconstitution, GVHD, the survival rate and immunological character after the reconstitution for the recipient mice were observed after bone marrow transptantation (BMT). ResultsThe counts of leukocytes and platelets in recipient mice's blood of group two on+10 day and +20 day after BMT were higher than in the experimental group, group three andgroup four(P< 0.01), but on +30?d after BMT the counts for all groups were at their normal levels. The Y chromsome from donor mice was discovered in 81.14%± 5.3% BMMC of recipient mice having survived over two months after BMT in the experimental group. The genomic integration of exogenous mFasL and Neo r
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