首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Increased expression of the novel molecule OX-2 is involved in prolongation of murine renal allograft survival.
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Increased expression of the novel molecule OX-2 is involved in prolongation of murine renal allograft survival.

机译:新分子OX-2的表达增加与小鼠肾脏同种异体移植物存活时间的延长有关。

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BACKGROUND: Portal venous (p.v.) peritransplant immunization with dendritic cells from bone marrow cultures, along with cyclosporine (10 mg/kg), produces antigen-specific increased renal allograft survival compared with recipients receiving intravenous (i.v.) immunization. Increased survival is associated with altered cytokine production from recipient T cells restimulated with donor antigen. We used a suppressive subtractive hybridization approach to explore a role in the regulation of transplant rejection for other genes differentially expressed after p.v. immunization. METHODS: Subtractive hybridization was performed using tissue from p.v. and i.v. immunized mice and a novel polymerase chain reaction-based approach. A gene-bank search was used to identify the source of the differentially expressed cDNAs. One product, the mouse homologue of rat OX-2, was further analyzed using Western gels and FACS analysis of dendritic cells (NLDC145+) isolated from p.v.-immunized mice. RESULTS: Eighty cDNA clones were obtained by suppressive subtractive hybridization. Differential expression was confirmed in Northern RNA blots. One clone showed sequence homology to a gene encoding a molecule on rat dendritic cells (MRC OX-2), with homology to genes encoding the costimulatory molecules CD80 (B7-1) and CD86 (B7-2). In p.v.-immunized mice, a monoclonal antibody to the rat OX-2 molecule identified, by Western blot analysis, increased expression of a molecule with molecular weight (43 kDa) analogous to rat MRC-OX-2; labels (by FACS analysis) indentified increased numbers of a population of cells staining with NLDC145; and blocks indentified increased graft survival. CONCLUSION: Our data suggest that OX-2 is functionally important in the increased graft survival seen in p.v.-immunized mice receiving renal allografts.
机译:背景:与接受静脉内(i.v.)免疫的接受者相比,用来自骨髓培养物的树突状细胞与环孢菌素(10 mg / kg)进行的门静脉(p.v.)移植前免疫可产生抗原特异性的肾脏同种异体移植存活率。存活率的提高与受体T细胞再注入供体抗原后细胞因子产生的改变有关。我们使用抑制性消减杂交方法探讨了在p.v.之后差异表达的其他基因在移植排斥调节中的作用。免疫。方法:利用p.v.的组织进行减性杂交。和i.v.免疫小鼠和一种新型的基于聚合酶链反应的方法。基因库搜索用于鉴定差异表达cDNA的来源。使用蛋白质凝胶和从p.v.免疫小鼠中分离的树突状细胞(NLDC145 +)的FACS分析进一步分析了一种产品,即大鼠OX-2的小鼠同源物。结果:通过抑制性消减杂交获得了80个cDNA克隆。在Northern RNA印迹中证实了差异表达。一个克隆显示与编码大鼠树突状细胞上的分子的基因(MRC OX-2)具有序列同源性,与编码共刺激分子CD80(B7-1)和CD86(B7-2)的基因具有同源性。在经p.v.免疫的小鼠中,通过Western blot分析鉴定的针对大鼠OX-2分子的单克隆抗体可增加分子量(43 kDa)的分子与大鼠MRC-OX-2相似的分子的表达。标签(通过FACS分析)鉴定出用NLDC145染色的细胞群数目增加;并鉴定出增加的移植物存活率。结论:我们的数据表明,在接受肾同种异体移植的经pv免疫的小鼠中,OX-2在提高移植存活率方面具有重要的功能。

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