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首页> 外文期刊>Transplant immunology >Isogeneic MSC application in a rat model of acute renal allograft rejection modulates immune response but does not prolong allograft survival.
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Isogeneic MSC application in a rat model of acute renal allograft rejection modulates immune response but does not prolong allograft survival.

机译:同种MSC在急性肾移植排斥反应大鼠模型中的应用可调节免疫反应,但不能延长同种异体移植的存活时间。

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Application of mesenchymal stromal cells (MSCs) has been proposed for solid organ transplantation based on their potent immuno-modulatory effects in vitro and in vivo. We investigated the potential of MSCs to improve acceptance of kidney transplants in an MHC-incompatible rat model including isogeneic kidney transplantation (RTx) as control. MSCs were administered i.v. or i.a. at time of transplantation. No immunosuppression was applied. Renal function was monitored by serum-creatinine, histopathology, immunochemistry for graft infiltrating cells and expressions of inflammatory genes. We demonstrated the short-term beneficial effects of MSC injection. In the long term, however, MSC-related life-threatening/shortening events (thrombotic microangiopathy, infarctions, infections) were evident despite decreased T- and B-cell infiltration, lower interstitial inflammation and downregulated inflammatory genes particularly after i.a. MSC injection. We conclude that i.a. MSC administration provides efficient immunomodulation after allogeneic RTx, although timing and co-treatment strategies need further fine-tuning to develop the full potential of powerful cell therapy in solid organ transplantation.
机译:基于间充质基质细胞(MSC)在体内和体外的强力免疫调节作用,已经提出了它们在实体器官移植中的应用。我们调查了骨髓间充质干细胞在不兼容MHC的大鼠模型(包括同种肾移植(RTx))中改善肾移植接受度的潜力。通过静脉内施用MSC。或i.a.在移植时。没有应用免疫抑制。通过血清肌酐,组织病理学,免疫化学检测移植肾浸润细胞和炎症基因表达来监测肾功能。我们证明了MSC注射的短期有益作用。从长远来看,尽管T细胞和B细胞浸润​​减少,间质炎症降低和炎症基因下调,尤其是在i.a之后,但与MSC相关的威胁生命/缩短生命的事件(血栓性微血管病,梗塞,感染)仍然很明显。 MSC注射。我们得出的结论是异源RTx给药后,MSC的给药可提供有效的免疫调节作用,尽管时间安排和共同治疗策略需要进一步调整以开发出强大的细胞疗法在实体器官移植中的全部潜力。

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