首页> 外文期刊>Transplantation Proceedings >Blockade of both CD28/B7 and OX40/OX40L co-stimulatory signal pathways prolongs the survival of islet xenografts.
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Blockade of both CD28/B7 and OX40/OX40L co-stimulatory signal pathways prolongs the survival of islet xenografts.

机译:CD28 / B7和OX40 / OX40L共刺激信号通路的阻断延长了胰岛异种移植物的存活。

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摘要

CTLA4Ig, a recombinant fusion protein composed of the extracellular domain of human CTLA4 and the constant region of human IgG1, inhibits the interaction of CD28/B7 pathway by binding the B7 molecule. OX40Ig, a recombinant fusion protein composed of the extracellular domain of human OX40 and the constant region of human IgG1, abrogates the interaction of OX40/OX40L pathway by binding the OX40L on APCs. So blockade of CD28/B7 or OX40/OX40L co-stimulatory pathways alone in mice with CTLA4Ig or OX40Ig can result in finitely prolonging the survival of islet grafts (43.2 +/- 4.81 and 67.7 +/- 7.74 days, respectively). In this study, a novel replication-defective adenovirus containing both of the CTLA4Ig and OX40Ig genes, AdCTLA4Ig-IRES-OX40Ig, was constructed by homologous recombination and injected into the streptozocin-rendered diabetic BalB/c mouse recipients (H-2d) through the tail vein, at the same day, the freshly isolated islets from Lewis rats (RT-1) were transplanted under the left kidney capsule of the recipients. The results showed that the mean survival time of the islet xenografts in the AdCTLA4Ig-IRES-OX40Ig-treated diabetic mice was significantly prolonged (100.3 +/- 14.94 days), while those in the untreated or AdEGFP-treated mice were rejected in normal fashion (6.7 +/- 0.94 and 7.0 +/- 1.0 days, respectively). In conclusion, utilizing AdCTLA4Ig-IRES-OX40Ig in vivo which can simultaneously express CTLA4Ig and OX40Ig proteins can improve the survival of Lewis-->BalB/c islet xenografts.
机译:CTLA4Ig是由人CTLA4的胞外域和人IgG1恒定区组成的重组融合蛋白,它通过结合B7分子来抑制CD28 / B7途径的相互作用。 OX40Ig是由人OX40的胞外域和人IgG1恒定区组成的重组融合蛋白,通过将OX40L结合在APC上消除了OX40 / OX40L途径的相互作用。因此,单独用CTLA4Ig或OX40Ig阻断CD28 / B7或OX40 / OX40L共刺激途径可导致胰岛移植物的存活时间有限延长(分别为43.2 +/- 4.81和67.7 +/- 7.74天)。在这项研究中,通过同源重组构建了同时包含CTLA4Ig和OX40Ig基因AdCTLA4Ig-IRES-OX40Ig的新型复制缺陷型腺病毒,并通过链霉菌素治疗的糖尿病BalB / c小鼠受体(H-2d)将其注射入在同一天的尾静脉中,将来自Lewis大鼠(RT-1)的新鲜分离的胰岛移植到接受者的左肾荚膜下。结果表明,AdCTLA4Ig-IRES-OX40Ig治疗的糖尿病小鼠中胰岛异种移植物的平均存活时间显着延长(100.3 +/- 14.94天),而未治疗或AdEGFP治疗的小鼠中胰岛异种移植物以正常方式被拒绝(分别为6.7 +/- 0.94天和7.0 +/- 1.0天)。总之,体内利用可同时表达CTLA4Ig和OX40Ig蛋白的AdCTLA4Ig-IRES-OX40Ig可以提高Lewis-> BalB / c胰岛异种移植物的存活率。

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